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Thursday, September 30, 2010

Qualiphar Nv

  

Department of Health and Human Services logoDepartment of Health and Human Services

Public Health Service
Food and Drug Administration
 Silver Spring MD 20993
 

Warning Letter

VIA UPS MAIL

WL: 320-10-11

September 30, 2010
 

Mr. Karl Verlinden
General Manager
Qualiphar n.v.
Rijksweg 9
B-2880 Bornem
Belgium

Dear Mr. Verlinden:

During our May 3 – 7, 2010 inspection of your pharmaceutical manufacturing facility, Qualiphar n.v., located at Rijksweg 9, B-2880 Bornem, Belgium, an investigator from the Food and Drug Administration (FDA) identified significant violations of Current Good Manufacturing Practice (CGMP) regulations for Finished Pharmaceuticals, Title 21, Code of Federal Regulations, Parts 210 and 211. These violations cause your drug products to be adulterated within the meaning of section 501(a)(2)(B) of the Federal Food, Drug, and Cosmetic Act (the Act) [21 U.S.C. § 351(a)(2)(B)] in that the methods used in, or the facilities or controls used for, their manufacture, processing, packing, or holding do not conform to, or are not operated or administered in conformity with, CGMP.

We have reviewed your firm’s response of May 28, 2010, and note that it lacks sufficient corrective actions.

Specific violations observed during the inspection include, but are not limited, to the following:

1. Your firm does not have adequate written procedures for production and process control designed to assure that the drug products you manufacture have the identity, strength, quality, and purity they purport or are represented to possess [21 C.F.R. § 211.100(a)]. Specifically, you fail to have written procedures for the manufacturing process of both the (b)(4) powder (b)(4) tablet drug products. For example:

a. Your 2002 process validation for the manufacturing of (b)(4) powder (b)(4) is deficient in that the batch production records failed to identify the specific type and sizes of equipment used and the manufacturing steps listed were minimal (i.e., (b)(4)). In addition, a comparison of the batch records for the powder (b)(4) instructions used for the 2002 validation batches with the recent 2008-2009 campaign batches showed changes in types of sugars, changes in (b)(4) time, changes in equipment and changes in order of addition of ingredients. In addition, there was no records showing these procedures had been drafted, reviewed and approved by the appropriate organizational unit. Although your quality manager informed our investigator that the changes mentioned were intended to improve content uniformity, there was no documentation to justify these changes as required by 21 CFR 211.100 (b). In addition, your firm could not provide documentation showing that any validation or testing of the powder filling operation had ever been done to ensure that the product remained homogeneous over the entire filling process. Also, a new filling machine was used (single head automatic powder filling machine, serial # 15200). However, there was no documentation of equipment qualification such as: IQ, OQ, PQ, nor documentation of machine operating parameters (i.e., agitator settings, speed, and vibration settings).

b. The only process validation study records available for the manufacture of (b)(4) tablets (b)(4) was summarized in a three page document identifying (b)(4) batches manufactured in 1997. This summary report did not include batch size, identification of equipment used, a detailed description of the manufacturing process (batch production records were not available), equipment parameters, and a description of the sampling plan used. The three-page validation record was undated, unsigned, and references (b)(4) batch numbers ((b)(4)) that are inconsistent with the coding format used in your facility.

Your firm acts as a contract manufacturer for powder (b)(4) and solid dosage drug products. It is essential that you understand your responsibility to operate in full compliance with CGMPs and to inform all of your customers of significant problems encountered during the manufacturing and testing of these products.

Your response acknowledges that the manufacturing process validation could be improved for both powder and tablets. Therefore, in collaboration with your customer, (b)(4) (the (b)(4) holder of (b)(4)), you stopped the production of your (b)(4) products in (b)(4) and dismantled the manufacturing area with the objective of (b)(4). At that time you indicated you would re-validate the entire manufacturing process for both (b)(4) tablets and powder.

The above observations are repeat observations, also cited during two previous FDA inspections of February 25-27, 1998 and November 4-8, 2002, and for which you had also promised corrections in your written responses to the FDA-483s. The February 25-27, 1998 inspection covered (b)(4) tablets and revealed that the (b)(4) process of the (b)(4) had not been validated. The November 4-8, 2002 inspection revealed several CGMP violations, including that the (b)(4) process for had not been validated. Additionally, the batch manufacturing record for (b)(4) tablets lacked detailed instructions regarding the amount of (b)(4) to be placed on the individual (b)(4) during the (b)(4) process.

This is the third occasion in which our investigators found that your facility stopped manufacturing (b)(4) the (b)(4) prior to our visit. For example, prior to our inspection of 1998, your facility last manufactured commercial (b)(4) tablets in (b)(4). Also, prior to the 2002 inspection, your facility had last manufactured (b)(4) powder (b)(4) in (b)(4). Likewise, the May 2010 inspection revealed that you stopped manufacturing both powder and tablet (b)(4) in . Therefore, the manufacture of (b)(4) was difficult to evaluate during these inspections. Your previous and current responses are similar in that your firm plans to (b)(4)

Electronic correspondence between your firm and (b)(4) obtained during the inspection reveals that you are aware of difficulties related to the manufacture of this product. Specifically, you are aware that (b)(4) is very insoluble and that the assay and dissolution results can be affected by slight variations in the manufacturing procedures.

We are concerned that you have not completed, or adequately validated the (b)(4) manufacturing process to current standards and expectations. Additionally, new equipment has not been qualified, and there is no assurance that the manufacturing process will result in a product that can consistently meet specifications. Your validation studies demonstrate yourfailure to consistently manufacture (b)(4) powder (b)(4) and tablets, as reported in this letter under item numbers two and three.

2. Failure to follow written procedures that describe the in-process controls established to be conducted on appropriate samples of in-process materials of each batch, to monitor the output and validate the performance of those manufacturing processes that may be responsible for causing variability in the characteristics of in-process material and the drug product [21 C.F.R. § 211.110(a)]. For example,

The only sample collected for (b)(4) determination after the (b)(4) of the (b)(4) used for (b)(4) tablet (b)(4) lot #(b)(4), resulted in an out-of-specification (OOS) result of (b)(4)% (batch record specification for (b)(4) is less than (b)(4)%). However, production continued and your firm released the batch without conducting an investigation as required by 21 C.F.R. § 211.192.

Your response states that there is no indication from your release and stability data that higher in-process (b)(4) content in (b)(4) had any effect on the identity, strength, quality, or purity of the finished tablets. We disagree with this conclusion in that quality must be built into the product throughout the manufacturing process. Finished product testing alone is not sufficient to demonstrate that the process is validated, particularly when discrepancies such as (b)(4) control limits are not observed during manufacturing.

Your response is inadequate in that it lacks information regarding any investigation conducted, even after the lot was released, that would explain the root cause of the problem. Your response also fails to state your rationale for releasing this batch without an investigation and the corrective actions implemented to prevent recurrence. We are concerned that other batches not meeting your in-process control procedures may have been released for distribution.

In your response, please include a list of all the products and lots manufactured by your firm within expiration that were released for distribution without meeting the established in-process specification. Also include a complete investigation of the root cause, the corrective and preventive action plan implemented, and any voluntary action necessary to address affected products in distribution.

3. Established laboratory control mechanisms are not followed [21 C.F.R. § 211.160(a)]. For example,

In 2009, various batches ((b)(4)) of (b)(4) powder (b)(4) failed either the assay or dissolution tests prior to release. Your OOS investigation reported that there were no errors related to calculations, analyst, analytical methods, or production process equipment, and that the OOS results were confirmed. However, instead of reporting the OOS as the final result, as required by your OOS investigation procedure, you invalidated the failing results, re-sampled and tested the batches. These batches were released for distribution.

Electronic correspondence collected during the inspection, related to the assay results for the 2009 powder campaign, showed (b)(4) instructed your firm to re-weigh and reject bottles found with excess fill weights because failing assay results were obtained. This practice is unacceptable regardless if requested by your customers, and is an indication of a lack of adequate controls in place to assure that (b)(4) powder (b)(4) products are manufactured in compliance with CGMP.

Your response for batches (b)(4), reports that the assay and dissolution OOS results were due to high bottle fill weights that occurred at the end-of-fill for these batches. This response is inadequate in that it does not provide any investigative report to support your conclusion and rationale. Review of production records for your in-process fill weights show no evidence of excess fill weight of bottles. The only overweight average was obtained on the (b)(4) day of a (b)(4)-day filling operation for batch (b)(4). Additionally, there were no overweight averages obtained for batch (b)(4). Therefore, your conclusion that fill weights were the problem is not supported by your batch records. Furthermore, your batch records are also not clear on how the bottles for the re-test of the “new end-of-filling” testing were selected.

Your response for batch (b)(4) indicates that you were aware of the potential problem at end of filling, and made adjustments to the filling machine to prevent overfilling. Also, overfilling and OOS results were not observed in the subsequent seven batches filled (b)(4)). This response is inadequate in that the batch record for (b)(4) contains an OOS investigation report that confirms failing results for the assay and dissolution tests. Electronic correspondence obtained during the inspection shows that following an instruction from (b)(4) you segregated, re-tested, and released the batch. The retest resulted in values within specifications, but on the lower limit for both the assay and dissolution test. (b)(4) attributed the OOS failure to a technical error in carrying out the method.

Your OOS procedure contains no provision for conducting a re-test of new samples based on a customer (b)(4) request. We are concerned that original release testing of multiple batches of powder (b)(4) yielded failing dissolution or assay results. Yet your firm released these batches for distribution based on passing repeat test results without conducting a thorough investigation as required under 21 C.F.R. § 211.192 to support your conclusion and rationale to release the affected lots. Retesting new samples without conducting a thorough investigation, after obtaining initial OOS results is an unacceptable practice.

In your response, please provide information regarding any voluntary corrective actions you intend for marketed the batches of (b)(4) that obtained an initial assay or dissolution OOS result. Also provide the root cause analysis into the actual or probable cause of the failures, investigation of the manufacturing process that may have caused the problem, and the corrective actions implemented to prevent recurrence of the problem.

Also include a list of all lots of (b)(4) powder (b)(4) manufactured by your firm, intended for shipment to the United States, that remain within expiration and for which an initial assay or dissolution OOS was obtained.

4. Failure to have adequate laboratory controls that includes sampling plans and test procedures designed to assure that your drug products conform to appropriate strength, quality and purity specifications. [21 C.F.R. § 211.160(b)].

For example, in 2009 portions of batches (b)(4) of (b)(4) powder were rejected due to fill weight OOS results. Your firm segregated only the end-of-fill portion of the batch, re-weighted the filled bottles and rejected those bottles that resulted with OOS fill weights. You re-assayed the samples found with high fill weights and reported that the excess weight caused both the assay and dissolution OOS results. However, our review found that this sampling plan and test procedure process lacked controls such as: appropriate documentation to justify your decision to re-weigh these batches, records failed to show when these batches were re-weighed, who conducted the re-weighing process, how many of the (b)(4) plus bottles from each batch were to be re-weighed, what value was to be used as a bottle tare weight, and the acceptance criteria used to release the batches.

For example, the sampling plan record for batch (b)(4) consisted of a one-page document that listed 244 handwritten bottle net weights. Some of these net weight recordings were circled, with a handwritten note at the bottom of the page reading in part, 29 pieces out-of-specification. There was a lack of consistency in identifying OOS units in that similar or higher bottle net weights were not circled and counted as OOS. Also, this record was only identified with the batch number ((b)(4) but not dated or signed by a production or quality unit representative. Furthermore there was no documentary evidence of the sampling plan for batch (b)(4)

Your response acknowledges that this process should be more clearly documented and prior to future production, procedures will be written, and personnel training documented. However, your response lacked documentation to ensure that all (b)(4) plus bottles of each batch met the fill weight specifications. We are concerned that other units from these two batches may have OOS for fill weights, which you have already reported to be associated with failing assay or dissolution results. We are also concerned with the lack of documentation, procedural controls and your determination that these batches of (b)(4) powder comply with CGMP based on your decision to reject only bottles found with excess fill weight at the end-of-fill run.

5. Records do not include the disposition of rejected filled drug product containers [21 C.F.R. § 211.184(e)].

For example, there are no records showing the final disposition of bottles containing (b)(4) powder (b)(4) from batches (b)(4) that were reportedly rejected due to excess (OOS) fill weight. Batch production records for batch (b)(4) indicate that 29 bottles were rejected on an unknown date in either February or March 2009. Batch production records for batch (b)(4) report that 144 bottles from end-of-filling were rejected prior to labeling. However, no records to confirm the final disposition of these units were available for review.

Your response acknowledges that the master record will be amended to document disposition of any rejected units and to incorporate a filling accountability record at the end of filling. You also indicate that product bottles with fill weights outside of the established specifications were rejected and destroyed. However, your response does not provide any documentation of the disposition of these rejected bottles to ensure that these defective units were not released for distribution.

6. Written procedures are not established for evaluations to be done at least annually and including provisions for a review of complaints, recalls, returned or salvaged drug products, and investigations conducted for each drug product [21 C.F.R. § 211.180(e)(2)].

For example, although your firm prepares annual product reviews for the products shipped to the United States, there were no written procedures describing who will prepare the reports, what information will be contained in the reports, or what the distribution of the reports should be. Our review of the two most recent annual reports for (b)(4) powder (b)(4) found the following discrepancies:

a. The 2008 report states that no batches were manufactured, but then lists the OOS results for batches (b)(4). Both the 2008 and 2009 reports state that there were no changes in manufacturing equipment or manufacturing process, but do not mention the new bottle filling equipment used for the batches produced in 2008 and 2009.

The 2009 report states that (b)(4) batches were released, and that none were reprocessed. It states on the next page that two batches were OOS because of the excess fill weight of bottles selected from the end of the batches had filling weight problems. The report does not mention that these two batches were reweighed and bottles found OOS were rejected.

Your failure to have written procedures as indicated in item number 6 of this letter is a repeat observation previously cited by FDA during the previous 2002 inspection for which you promised corrections in your response.

Your May 28, 2010 response acknowledges that written procedures are required for the annual review process, and that you will implement written procedures prior to any future batch production. We are concerned with the continuing failure to have written procedures for the preparation of annual review of your products.

In addition to the items listed above, the inspection brought additional matters to our attention that increase our concerns regarding the quality of drug products manufactured at your facility. These issues include, but are not limited to: lack of cleaning validation on equipment not dedicated to (b)(4) production, the use of dedicated equipment is not clear in the batch records, powder (b)(4) bottle filling records do not show the number of bottles filled or rejected for being out of weight limits, and batch records do not include a record of any sampling performed for each batch of drug product produced.

The violations cited in this letter are not intended to be an all-inclusive statement of violations that exist at your facility. You are responsible for investigating and determining the causes of the violations identified above and for preventing their recurrence and the occurrence of other violations. If you wish to ship your products to the United States, it is the responsibility of your firm to ensure compliance with all U.S. standards for CGMP and all applicable U.S. laws and regulations.

Additionally, your firm is neither registered nor has it listed every product in commercial distribution in the United States with FDA, as required by 21 C.F.R. § 207.40 and section 510(i) of the Act [21 U.S.C. § 360(i)]. Information on how to register and list is available at the following internet website: http://www.fda.gov/cder/drls/registration_listing.htm. You must complete the required registration and listing and provide evidence that you have fulfilled these requirements in your response to this letter.

Until all corrections have been completed and FDA has confirmed corrections of the violations and your firm’s compliance with CGMP, FDA may withhold approval of any new applications or supplements listing your firm as a drug product manufacturer. In addition, FDA will be refusing admission of articles manufactured at Qualiphar n.v., Rijksweg 9, B-2880 Bornem, Belgium into the United States. The articles are subject to refusal of admission pursuant to section 801(a)(3) of the Act [21 U.S.C. § 381(a)(3)], in that, the methods and controls used in their manufacture do not appear to conform to CGMP within the meaning of section 501(a)(2)(B) of the Act [21 U.S.C. § 351(a)(2)(B)].

Within fifteen working days of receipt of this letter, please notify this office in writing of the specific steps that you have taken to correct violations. Include an explanation of each step being taken to prevent the recurrence of violations and copies of supporting documentation. Also include distribution records to your U.S. customer and the current and future manufacturing status of (b)(4) products, as well as existing inventories of remaining (b)(4) products at your facility. If you cannot provide the requested information and complete corrective action within fifteen working days, state the reason for the delay and the date by which you will have complied with our requests. Please identify your response with FEI # 1000627334.
 

If you have questions or concerns regarding this letter, contact Edwin Melendez, Compliance Officer, at the below address and telephone number.
 

U.S. Food and Drug Administration
Center for Drug Evaluation and Research
Division of Manufacturing and Product Quality
International Compliance Branch
White Oak, Building 51
10903 New Hampshire Ave.
Silver Spring, MD 20993
Tel: (301) 796-3284
Fax: (301) 847-8741
 

Sincerely,
/S/
Richard L. Friedman
Director
Division of Manufacturing and Product Quality
Office of Compliance
Center for Drug Evaluation and Research

-

O'Barr, Thomas Jr., M.D. 9/30/10

  

Department of Health and Human Services logoDepartment of Health and Human Services

Public Health Service
Food and Drug Administration
 Silver Spring, MD 20993 

WARNING LETTER


CERTIFIED MAIL
RETURN RECEIPT REQUESTED

Ref: 10-HFD-45-09-05


Thomas O’Barr, Jr., M.D.
1431 White Circle NW
Marietta, GA 30066


Dear Dr. O’Barr:


Between September 16 and 30, 2009, Ms. Stephanie Hubbard, representing the Food and Drug Administration (FDA), conducted an investigation and met with you to review your conduct of the following clinical investigations of the investigational drug (b)(4), performed for (b)(4):


Protocol (b)(4), entitled (b)(4)
 

Protocol (b)(4), entitled (b)(4)

This inspection is a part of the FDA's Bioresearch Monitoring Program, which includes inspections designed to evaluate the conduct of research and to help ensure that the rights, safety, and welfare of the human subjects of those studies have been protected.


From our review of the establishment inspection report, the documents submitted with that report, and your written responses to the Form FDA 483 dated October 2, 2009, we conclude that you did not adhere to the applicable statutory requirements and FDA regulations governing the conduct of clinical investigations. We are aware that at the conclusion of the inspection, Ms. Hubbard presented and discussed with you Form FDA 483, Inspectional Observations. We wish to emphasize the following:


1. You failed to ensure that the investigation was conducted according to the investigational plan [21 CFR 312.60].


Protocol (b)(4) specified that at conclusion of the study, all primary data that are a result of the original observations and activities of the study that are necessary for the reconstruction and evaluation of any study report will be retained in a secure archive at the study site, for a period not less than two years after the last approval of a marketing application in an ICH region, and until there are no pending or contemplated marketing applications in an ICH region; or, at least two years have elapsed since the formal discontinuation of the clinical development of the investigational product. You failed to maintain all study records as required by the study protocol.


a. Specifically, during the inspection you were unable to provide case report forms for Protocol (b)(4) for any of the 20 subjects screened or 10 subjects enrolled into the study.


b. There were no source documents found for Subject 500010 during the FDA inspection.


In your written response, you stated that in your evaluation of a subject, you would take the subject’s clinical history, discuss the study with the subject, and make certain that based on the subject’s clinical history, the subject was appropriate for the study. You stated that you counted on the study coordinators to make sure that the source data adequately represented and documented this information. You further stated that you clearly should have looked at the records yourself to ensure that they had been done appropriately.


Your statement that you counted on the coordinators to be sure that the source data adequately represented and documented this information is unacceptable. As the clinical investigator, it is your ultimate responsibility to ensure that the study was conducted according to the requirements set forth in the investigational plan.


2. You failed to maintain adequate and accurate case histories that record all observations and other data pertinent to the investigation on each individual administered the investigational drug or employed as a control in the investigation [21 CFR 312.62(b)].


The following are examples of inadequate and inaccurate case histories noted for Protocol (b)(4):


a. The following was noted for Subject 500006:


i. The Clinically Significant Abnormal Lab Values form had a checkmark in a box that confirmed there were no clinically significant abnormal lab values identified for the Week 2 visit. However, the laboratory report for the Week 2 visit (June 29, 2005) and the Week 2 progress note had handwritten notes stating that you recommended that this subject be referred to his/her primary care physician due to the abnormally high glucose value of 156 mg/dL.
 

In your written response to this finding, you stated that in your review of the labs, you would sign your name indicating that you had reviewed them. If there were labs of any clinical significance, you would discuss them with the study coordinators and then with the subjects. You stated that you believed while abnormal labs were indicated, none of them are clinically significant, except patients that received specific instructions to follow up for specific values. You, however, concurred that the documentation for the lack of significance in these laboratory values was missing.


ii. There were two Visual Analog Scales for this subject for the Week 2 visit. We were unable to tell from the documents which Visual Analog Scale served as the accurate source record.


b. Subject 500008’s Clinically Significant Abnormal Lab Values form and the laboratory report for the Week 4 visit showed no information related to whether clinically significant abnormal labs were identified at this visit. In FDA’s review of the lab report for samples collected at this visit, however, there were some test measurements that were noted on the report as being outside the reference range, including the measurements for creatine kinase, potassium, and blood monocytes.


In your written response to this finding, you stated that in your review of the labs, you would sign your name indicating that you had reviewed them. If there were labs of any clinical significance, you would discuss them with the study coordinators and then with the subjects. You stated that you believed while abnormal labs were indicated, none of them are clinically significant, except patients that received specific instructions to follow up for specific values. You, however, concurred that the documentation for the lack of significance in these laboratory values was missing.


3. You failed to maintain adequate records of the disposition of the drug, including the dates, quantity, and use by subject [21 CFR 312.62(a)].


The following are examples noted for Protocol (b)(4):


a. Per the drug accountability log, Subject 500006 was dispensed 66 tablets of medication in Bottle A and 66 tablets in Bottle B on July 12, 2005, and none of these tablets were ever returned. However, the progress note dated July 22, 2005, states that the subject returned 48 tablets in Bottle A and 48 tablets in Bottle B.


b. Per the drug accountability log, on July 9, 2005, Subject 500008 returned 22 tablets of medication in Bottle A and 22 tablets in Bottle B, and was also dispensed 66 new tablets in Bottle A and 66 new tablets in Bottle B. However, a Week 4 study document shows that this exchange of study drug tablets for Subject 500008 occurred on July 12, 2005.


c. Per the drug accountability log, Subject 500013 was dispensed 66 tablets of medication in Bottle A and 66 tablets in Bottle B on June 28, 2005, and none of these tablets were ever returned. However, the progress note dated July 21, 2005, states that the subject returned 31 tablets in Bottle A and 29 tablets in Bottle B.


d. Per the drug accountability log, Subject 500015 was dispensed 66 tablets of medication in Bottle A and 66 tablets in Bottle B on July 5, 2005 (Baseline Visit); and on July 20, 2005 (Week 2 visit), 35 tablets of medication in Bottle A and 35 tablets in Bottle B were returned. The Week 1 visit (July 12, 2005) progress note, however, shows that your site identified only 33 tablets remaining in each bottle at this visit.


In your written response, you acknowledged these findings. You stated that you did not personally review the numbers for each subject in the Drug Accountability Log reports and ensure that they corresponded to the numbers entered in the progress notes in the clinical records. You also stated that counting on the work of the coordinators, which was obviously substandard, was clearly a misjudgment on your part.


Your response that you did not review the numbers for each subject in the Drug Accountability Log reports and ensure that they corresponded to the numbers entered in the progress notes in the clinical records, is unacceptable. As the clinical investigator, it is your responsibility to ensure the maintenance of adequate records of the disposition of the drug.


This letter is not intended to be an all-inclusive list of deficiencies with your clinical study of an investigational drug. It is your responsibility to ensure adherence to each requirement of the law and relevant FDA regulations. You should address these deficiencies and establish procedures to ensure that any ongoing or future studies will be in compliance with FDA regulations.


Within fifteen (15) working days of your receipt of this letter, you should notify this office in writing of the actions you have taken to prevent similar violations in the future. Failure to adequately and promptly explain the violations noted above may result in regulatory action without further notice.


If you have any questions, please contact Constance Cullity, M.D., M.P.H., at 301-796-3397; FAX 301-847-8748. Your written response and any pertinent documentation should be addressed to:


Constance Cullity (formerly Lewin), M.D., M.P.H.
Branch Chief
Good Clinical Practice Branch I
Division of Scientific Investigations
Office of Compliance
Center for Drug Evaluation and Research
Food and Drug Administration
Building 51, Room 5354
10903 New Hampshire Avenue
Silver Spring, MD 20993


Sincerely yours,
{See appended electronic signature page}
Leslie K. Ball, M.D.
Director
Division of Scientific Investigations
Office of Compliance
Center for Drug Evaluation and Research
Food and Drug Administration


Reference ID: 2842901
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This is a representation of an electronic record that was signed electronically and this page is the manifestation of the electronic signature.
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/s/
----------------------------------------------------
LESLIE K BALL
09/30/2010

-

Mutual Trading Company Inc

  

Department of Health and Human Services logoDepartment of Health and Human Services

Public Health Service
Food and Drug Administration
 Los Angeles District
Pacific Region
19701 Fairchild      
Irvine, CA 92612-2506
 
Telephone:    949-608-2900
FAX:    949-608-4415

 

 WARNING LETTER
 
CERTIFIED MAIL
RETURN RECEIPT REQUESTED
 
September 30, 2010
                                                                                                                                    W/L 46-10
Noritoshi Kanai, President
Mutual Trading Company, Inc.
431 Crocker Street
Los Angeles, California 90013-2114
 
Dear Mr. Kanai:
 
We inspected your seafood processing / importer / distribution facility, located at the above shown location, on May 17th through May 25th of 2010. We found that you have serious violations of the seafood Hazard Analysis and Critical Control Point ( henceforth “HACCP” ) regulation, Title 21, Code of Federal Regulations ( henceforth “CFR” ), Part 123, and the Current Good Manufacturing Practice ( henceforth “CGMP” ) regulation for foods in Title 21, CFR parts 110 & 123. In accordance with 21 CFR 123.6(g), failure of a processor of fish or fishery products to have and implement a HACCP plan that complies with this section or otherwise operate in accordance with the requirements of Part 123, renders the fish or fishery products adulterated within the meaning of Section 402(a)(4) of the Federal Food, Drug, and Cosmetic Act ( henceforth “the Act” ), 21 U.S.C. § 342(a)(4).
 
Accordingly, the various seafood products containing characterizing fishery products you process are adulterated, in that they have been prepared, packed, or held under insanitary conditions whereby they may have been rendered injurious to health. You may find the Act, the seafood HACCP regulation and the Fish and Fisheries Products Hazards and Controls Guidance through links at the U. S. Food and Drug Administration’s ( henceforth “FDA” ) home page at www.fda.gov.
 
Your significant violations were as follows:
 
1.  You must conduct or have conducted for you a hazard analysis for each kind fish and fishery product that you produce to determine whether there are food safety hazards that are reasonably likely to occur and you must have and implement a written HACCP plan to control any food safety hazards that are reasonably likely to occur, to comply with 21 CFR 123.6(a) and (b). However your firm does not have a HACCP plan for pasteurized refrigerated imitation crab meat in an oxygen-reduced package.
 
2.  You must have a HACCP plan that, at a minimum, lists monitoring procedures and their frequency for each critical control point, to comply with 21 CFR 123.6(c)(4). However, your firm’s HACCP plan for Mackerel with (b4) lists a CCP of (b4) and another CCP for (b4) for monitoring the refrigerator temperature to prevent C. botulinum toxin formation using a digital probe thermometer with a visual check of (b4) times a day. This method does not ensure that proper temperatures will be continuously be maintained between temperature checks and during those times when your firm is not open for business, such as overnight. FDA recommends that cooler storage temperatures be monitored with equipment that is capable of continuously monitoring temperatures and that the equipment is capable of providing a record of the temperatures or is equipped with an alarm system that provides a 24 hour alert.
 
3.  You must implement the record keeping system that you have listed in your HACCP plan, to comply with 21 CFR 123.6(b). However, your firm’s HACCP plan stated a monitoring procedure of (b4) times a day but they were only monitoring (b4) times a day from April 14 until May 3, 2010. Also this same HACCP plan for Mackerel with (b4) at the critical control point for (b4), and the critical Control Point for (b4), states a verification procedure of (b4) of recording thermometer”. The critical control point for “Finished product freezer storage” states a verification procedure of “check calibrated thermometer (b4),” and the critical point for Freezer Storage states “Check with calibrated Thermometer (b4)”, You are not calibrating your continuous recording chart thermometers or digital probe thermometers. You must implement the calibrating of your continuous recording chart thermometers and digital probe thermometers that you listed in your HACCP plans, to comply with 21 CFR 123.6(b).
 
4.  You must fully document in your records all corrective actions taken, to comply with 21 CFR 123.7(d). However, you did not document that a corrective action was taken when you deviated from your critical limit of “Maintain Refrigerator Temperature below (b4)” for Mackerel w/ (b4) at the (b4) and (b4) critical control points to control “Pathogen growth and C. botulinum toxin formation.” On numerous occasions your refrigerator temperatures were recorded above 37° F, including above 40° F.
 
5.  You must maintain sanitation control records that, at a minimum, document monitoring and corrections as set out in 21 CFR 123.11(b), to comply with 21 CFR 123.11(c). However, your firm did not maintain sanitation control records required for the processing of frozen mackerel intended to be consumed raw by the consumer. Specifically, on May 18, 2010 our investigator observed your firm’s handling of frozen mackerel; however, no sanitation control record was maintained.
 
6.  You must monitor sanitation conditions and practices during processing with sufficient frequency to ensure compliance with current good manufacturing practice requirements in 21 CFR Part 110, to comply with 21 CFR 123.1(b). However, your firm did not monitor the prevention of cross-contamination from insanitary objects to food and the exclusion of pests from the food plant with sufficient frequency to ensure compliance with the current good manufacturing practice requirements in 21 CFR Part 110 as evidenced by the following observations:
                       
a. On 5/17/10, a rusted hammer was observed in the seafood processing room. The hammer was used to break up ice which came in direct contact with frozen mackerel. The mackerel is intended to be eat raw.
 
b. On 5/17/10, a cutting board was observed to be gouged and visibly soiled with a brown organic substance. We observed the cutting board used to fillet mackerel. 
 
c. On 5/20/10, a wooden spatula was observed in the processing room. The wooden spatula had visible gouges in the wood which doesn’t allow the spatula to be cleaned. The spatula was used to manufacture various vinegar solutions which are ingredients in ready to eat seafood products.
 
d. On 5/20/10, a live cockroach was observed inside the processing room.
 
In addition, it is important that your sanitation control records accurately reflect the conditions and practices at your firm, as required by the 21 CFR 123.11(b).
 
7.  You must implement an affirmative step which ensures that the fish and fishery products you import are processed in accordance with the seafood HACCP regulation, to comply with 21 CFR 123.12.(a)(2)(ii).   However, your firm did not perform an affirmative step for (b4) tuna, (b4) mackerel, (b4) anchovy and (b4) bonito products that you import from (b4).
 
We may take further action if you do not promptly correct these violations. For instance, we may take further action to seize your product(s) and/or enjoin your firm from operating.
 
You should respond in writing within fifteen (15) working days from your receipt of this letter. Your response should outline the specific things you are doing to correct these violations. You should include in your response documentation such as HACCP and verification records, or other useful information that would assist us in evaluating your corrections. If you cannot complete all corrections before you respond, you should explain the reason for your delay and state when you will correct any remaining violations.
 
This letter may not list all the violations at your facility. You are responsible for ensuring that your processing plant operates in compliance with the Act, the seafood HACCP regulation (21 CFR Part 123) and the Current Good Manufacturing Practice regulation (21 CFR Part 110). You also have a responsibility to use procedures to prevent further violations of the Act and all applicable regulations.

 
Your written reply should be addressed to:
 
Blake Bevill
Director, Compliance Branch
U.S. Food and Drug Administration
19701 Fairchild Rd.
Irvine, California 92612-2506
 
Sincerely,
/S/
Alonza E. Cruse
Director, Los Angeles District
 
cc:     
Branch Chief
Food and Drug Branch
California Department of Public Health
1500 Capital Avenue - MS 7602
P.O. Box 997413
Sacramento, CA 95899-7413
-

Impact Instrumentation, Inc.

  

Department of Health and Human Services logoDepartment of Health and Human Services

Public Health Service
Food and Drug Administration
 

Waterview Corporate Center
10 Waterview Blvd., 3rd Floor
Parsippany, NJ 07054

Telephone (973) 331-4906 


 

September 30, 2010
 

WARNING LETTER

VIA UPS EXPRESS
AND FACSIMILE

 

10-NWJ-18
 

Leslie H. Sherman
President
Impact Instrumentation, Inc.
27 Fairfield Place
West Caldwell, NJ 07006

Dear Mr. Sherman:

During an inspection of your firm located in West Caldwell, New Jersey on February 17, 2010 through March 8, 2010, an investigator from the United States Food and Drug Administration (FDA) determined that your firm manufactures Uni-Vent® 731 Series Model EMV, Uni-Vent® 731 Series Model EMV+ (800-EMVP-01), 754 Uni-Vent Eagle Portable Ventilator, and the Special Medical Emergency Evacuation Device (SMEED). Under section 201 (h) of the Federal Food, Drug, and Cosmetic Act (the Act), 21 U.S.C. 321 (h), these products are devices because they are intended for use in the diagnosis of disease or other conditions or in the cure, mitigation, treatment, or prevention of disease, or are intended to affect the structure or function of the body.

This inspection revealed that you have not obtained marketing approval or clearance before you began offering the Uni-Vent® 731 Series Model EMV+ (800-EMVP-01) for sale, which is a violation of the law. The Act requires that manufacturers of devices that are not exempt obtain marketing approval or clearance for their products from the FDA before they may offer them for sale. This helps protect the public health by ensuring that new devices are shown to
be both safe and effective or substantially equivalent to other devices already legally marketed.

Specifically, the Uni-Vent® 731 Series Model EMV+ (800-EMVP-01) is adulterated under section 501(f)(1)(B) of the Act, 21 U.S.C. 351 (f)(1)(B), because you do not have an approved application for premarket approval (PMA) in effect pursuant to section 515(a) of the Act, 21 U.S.C. 360e(a), or an approved application for an investigational device exemption (IDE) under section 520(g) of the Act, 21 U.S.C. 360j(g). The device is also misbranded under section 502(o) the Act, 21 U.S.C. 352(o), because you did not notify the agency of your intent to introduce the device into commercial distribution, as required by section 510(k) of the Act, 21 U.S.C. 360(k).

The Uni-Vent® 731 Series Model EMV+ (800-EMVP-01) contains the following changes or modifications that were not included for the Uni-Vent® 731 Series Model EMV+ (800-EMVP-00) under 510(k) number K091238: 1) the addition of the "Pleth" waveform feature; 2) Volume Targeted Synchronized Intermittent Mandatory Ventilation (SIMV) mode; 3) Pressure Targeted SIMV mode; 4) Continuous Positive Airway Pressure (CPAP) mode; Pressure Support operating mode; and 5) an apnea alarm. These added modes and features represent significant changes or modifications in design, components, method of manufacture, or intended use that could significantly affect the safety or effectiveness of the device and represent a major change or modification in the intended use of the device. Therefore, these changes or modifications require the submission of a new 510(k). 21 C.F.R. 807.81(a)(3). For example,

1. The addition of the "Pleth" waveform feature could significantly affect the safety or effectiveness of the device as it acts as a basis on which to provide medical intervention.

2. The device is cleared to provide full ventilatory support. The addition of the Volume Targeted SIMV, Pressure Targeted SIMV, Pressure Targeted SIMV, Continuous Positive Airway Pressure, and Pressure Support, and Pressure Support modes of ventilation could significantly affect the safety or effectiveness of the device as they provide both full and partial ventilatory support.

3. The addition of the apnea alarm could significantly affect the safety or effectiveness of the device as device safety would purportedly increase.

Additionally, a new 510(k) clearance is required for changes in labeling, namely the Operator's Manual, Impact Part Number 906-EMVP-01 to incorporate the differences cited, and the Model & Serial Number Label, to differentiate between 800-EMVP-01 and 800-EMVP-00.

For a device requiring premarket approval, the notification required by section 510(k) of the Act, 21 U.S.C. 360(k), is deemed satisfied when a PMA is pending before the agency. 21 C.F.R. 807.81 (b). The kind of information you need to
submit in order to obtain approval or clearance for your device is described on the Internet at http://www.fda.gov/cdrh/devadvice/3122.html. The FDA will evaluate the information you submit and decide whether your product may be legally marketed.

This inspection also revealed that the Uni-Vent® 731 Series Model EMV, UniVent ® 731 Series Model EMV+ (800-EMVP-00), Uni-Vent® 731 Series Model EMV+ (800-EMVP-01), and 754 Uni-Vent Eagle Portable Ventilator, are adulterated within the meaning of section 501 (h) of the Act (21 U.S.C. § 351 (h)), in that the methods used in, or the facilities or controls used for, their manufacture, packing, storage, or installation are not in conformity with the Current Good Manufacturing Practice (CGMP) requirements of the Quality System (QS) regulation found at Title 21, Code of Federal Regulations (C.F.R.), Part 820. We received a response from Alan Giordano, Regulatory Affairs Manager, dated March 23, 2010, concerning our investigator's observations noted on the Form FDA 483, List of Inspectional Observations that was issued to you. We address this response below, in relation to each of the noted violations.
These violations include, but are not limited to, the following:

1. Failure to establish and maintain procedures for implementing corrective and preventive action, as required by 21 C.F.R. 820.100(a). For example:

a. Your firm's Corrective and Preventive Action procedure, QAP/0600, Rev. F, dated August 15, 2005, failed to include requirements for analyzing processes, work operations, concessions, quality audit reports, quality records, service records, complaints, returned product, and other sources of quality data to identify existing and potential causes of nonconforming product, or other quality problems, as required by 21 CFR 820.100(a)(1).

b. Your firm received complaints during the month of October, 2009 for the 754 Uni-Vent Eagle Portable Ventilators (Complaint/Serial # PC09-122/0604188, PC09-123/0504010, and PC09-135/9709011) concerning compressor motors failing to operate, ventilator displaying a code 2 alarm, and a ventilator providing a low tidal volume. As a result, your firm determined that the compressors were having intermittent output issues and performed repairs for the units returned from your customers. There was no further investigation on the root causes of the intermittent output issues, as required by 21 CFR 820.100(a)(2). Additionally, your firm failed to perform corrective and preventive actions as required in section 5 of your Complaint Resolution and Close Out form (QAP/0500-6, Rev.B) in order to prevent recurrence of nonconforming product in distribution, and those not yet distributed by your firm. Thus, your firm failed to maintain procedures for identifying the actions needed to correct and prevent recurrence of nonconforming product, as required by 21 CFR 820.100(a)(3).

c. Your firm received complaints from September 15,2008 through June 29, 2009 concerning defective transducers (b)(4) of returned 754 Uni-Vent Eagle Portable Ventilators causing insufficient tidal volumes and failure of device to operate. No corrective and preventive actions were performed for three of the complaints (Complaint/Serial # PC09-090/0711052, PC09-077/0708133, and PC09-013/9901024) received by your firm in order to prevent recurrence of nonconforming product and other quality problems, as required by 21 CFR 820.100(a)(3).

d. Your firm received complaints from June 25, 2009 through November 20, 2009 concerning defective battery packs (disconnection of battery terminal wires at the battery pack) and a vacuum gauge out of specification for returned 305 series Portable Aspirators causing failure of the aspirator to operate or failure to operate in high mode. Two of the complaints (Complaint/Serial # PC09-140/9905011 and PC09-089/ 8501107) documented that the aspirators were repaired by your firm and were later (b)(4) sent back to your firm for the same nonconforming issue. No corrective and preventive actions were performed for four of the complaints (Complaint/Serial # PC09-140/9905011, PC09-139/9605047, PC09-089/8501107, and 9404063/PC09-058) received by your firm as required by your Complaint Resolution and Close Out form. Your firm failed to prevent recurrence of nonconforming product in distribution, as required by 21 CFR 820.100(a)(3).

The adequacy of your firm's response dated March 23, 2010 cannot be determined at this time. Your firm did not submit documentation which includes a description and evidence of implementation of the correction, corrective action, and proposed preventive action. The response states that the procedures will be modified; however, no copies of the revised procedures were included. Additionally, the response does not address why corrective and preventive actions are not performed for complaints received for nonconforming product.

2. Failure to adequately review, evaluate, and investigate complaints involving the possible failure of a device, labeling, or packaging to meet any of its specifications, unless such investigation has already been performed for a similar complaint and another investigation is not necessary, as required by 21 C.F.R. 820.198(c).

Specifically, your firm's QAP/0500 Complaint Handling, Rev. K, October 9, 2008, does not require that any complaint involving the possible failure of a device to meet any of its specifications be investigated. For example, there was a lack of investigation into the following released, returned, and failed devices:

a. Complaint No. PC09-090 and Service Malfunction Record No. 090628 indicate that 754 Uni-Vent Eagle Portable Ventilator, Serial No. 0711052, had a defective transducer and was found not having any oxygen Tidal Volume and Fraction of Inspired Oxygen (FIO2) readings during service.

b. Complaint No. PC09-135 and Service Malfunction Record No. 09V1159 indicate that 754 Uni-Vent Eagle Portable Ventilator, Serial No. 9709011, had a failed compressor motor, provided low Tidal Volume, and was found having an intermittent CPU Printed Circuit Board and not having any oxygen and external air Tidal Volume and FIO2 readings during service.

c. Complaint No. PC09-140 and Service Malfunction Record No. 09A245 indicate that 305GR Portable Aspirator, Serial No. 9905011, failed to operate due to a disconnection of a battery terminal wire. The problem occurred three days after the customer received the product that was sent previously for the same problem.

The adequacy of your firm's response dated March 23, 2010 cannot be determined at this time. Your firm did not submit documentation which includes a description and evidence of implementation of the correction, corrective action, and proposed preventive action. The response states that the procedures will be modified; however, no copy of the revised procedure was included.

3. Failure to establish and maintain procedures for rework, to include retesting and reevaluation of the nonconforming product after rework, to ensure that the product meets its current approved specifications. Rework and reevaluation activities, including a determination of any adverse effect from the rework upon the product, shall be documented in the device history record (DHR), as required by 21 C.F.R. 820.90(b)(2).

For example, your firm initiated a change request order "QAP/0101-1, Rev. F, dated May 11, 2009" for your Uni-Vent® 731 Series Model EMV to alleviate a high O2 pressure leak. The change performed by your firm indicates a drawing note change that specifies (b)(4)

Your firm did not document any justification for product release until after the FDA investigator observed this deficiency during the inspection noted on Hardware Change Sheet, Rev. 3.0, dated February 23, 2010. Your firm released units with the high pressure leak nonconformities prior to determining if there were any possible adverse effects that could occur from the changes that were made to the devices.

4. Failure to establish and maintain procedures to control product that does not conform to specified requirements, as required by 21 C.F.R. 820.90(a), and failure to establish and maintain procedures that define the responsibility for review and the authority for the disposition of nonconforming product, as required by 21 C.F.R. 820.90(b)(1). For example:

a. QCP/0100 Control of Nonconformities, Rev. J, dated October 4, 2007, does not ensure that the evaluation of the nonconformance includes a determination of the need for an investigation. Additionally, the procedure does not require the documentation of justification for use of nonconforming product including the signature of the individual(s) authorizing the use.

b. Your firm had 28 Nonconforming Material Record Sheets (NCMs) for a peep leak test failure (workmanship issue for a loose zip tie on the flow manifold or another assembly) for the Model 754 ventilators. No documented investigation was conducted until after the FDA investigator observed the deficiency during the inspection.

5. Failure to adequately establish and maintain procedures for defining and documenting design output in terms that allow an adequate evaluation of conformance to design input requirements, as required by 21 C.F.R. 820.30(d). For example, your firm did not ensure that those design outputs that are essential for the proper functioning of the Uni-Vent® 731 Series Model EMV+ device are identified.

Your firm's response dated March 23, 2010 is not adequate because your firm did not submit documentation which includes evidence of implementation of the correction, corrective action, and proposed preventive action. The response states that the design output procedure will be modified to identify the assemblies which are subjected to further testing, without providing accompanying evidence.

6. Failure to establish and maintain procedures for the validation, or where appropriate verification, of design changes before their implementation, as required by 21 C.F.R. 820.30(i). For example, your firm's DES/0700 Design Change, Rev. E, December 1, 2005 does not ensure that validation, or where appropriate verification, be performed of design changes before they are implemented.

You should take prompt action to correct the violations addressed in this letter. Failure to promptly correct these violations may result in regulatory action being initiated by the Food and Drug Administration without further notice. These actions include, but are not limited to, seizure, injunction, and/or civil money penalties. Also, federal agencies are advised of the issuance of all Warning Letters about devices so that they may take this information into account when
considering the award of contracts. Additionally, premarket approval applications for Class III devices to which the Quality System regulation deviations are reasonably related will not be approved until the violations have been corrected. Requests for Certificates to Foreign Governments will not be granted until the violations related to the subject devices have been corrected.

Please notify this office in writing within fifteen (15) working days from the date you receive this letter of the specific steps you have taken to correct the noted violations, including an explanation of how you plan to prevent these violations, or similar violations, from occurring again. Include documentation of the corrective action you have taken. If your planned corrections will occur over time, please include a timetable for implementation of those corrections. If corrective action cannot be completed within 15 working days, state the reason for the delay and the time within which the corrections will be completed.

Your response should be sent to: Robert J. Maffei, Compliance Officer, U.S. Food and Drug Administration, 10 Waterview Boulevard, 3rd Floor, Parsippany, New Jersey, 07054. If you have any questions about the content of this letter, please contact Mr. Maffei via telephone at 973-331-4906 or via fax at 973-331-4969.

Finally, you should know that this letter is not intended to be an all-inclusive list of the violations at your facility. It is your responsibility to ensure compliance with applicable laws and regulations administered by FDA. The specific violations noted in this letter and in the Inspectional Observations, Form FDA 483 (FDA 483), issued at the closeout of the inspection may be symptomatic of serious problems in your firm's manufacturing and quality assurance systems. You should investigate and determine the causes of the violations, and take prompt actions to correct the violations and to bring your products into compliance.
 

Sincerely yours,
/S/
Diana Amador-Toro
District Director
 

 

-

DW Trading Inc.

  

Department of Health and Human Services logoDepartment of Health and Human Services

Public Health Service
Food and Drug Administration
 Detroit District
300 River Place
Suite 5900
Detroit, MI 48207
Telephone: 313·393·8100
FAX: 313·393·8139

 

WARNING LETTER
2010-DT-20
 
September 30, 2010
 
VIA UPS
 
 
Mr. Kai K. Wong, President and CEO
DW Trading, Inc.
3649 Lafayette Road
Indianapolis, Indiana 46222
 
Dear Mr. Kai:
 
The U.S. Food and Drug Administration (FDA) conducted an inspection of your food processing and storage facility, located at 3649 Lafayette Road, Indianapolis, Indiana, on May 18, 20-21, and 25-26, 2010. During the inspection, FDA investigators documented serious violations of the Current Good Manufacturing Practice (CGMP) regulation for foods, Title 21, Code of Federal Regulations, Part 110 (21 CFR 110).  The conditions observed during the inspection cause food products processed or stored in your facility to be adulterated under Section 402(a)(4) of the Federal Food, Drug, and Cosmetic Act (the Act) [21 U.S.C. § 342(a)(4)] in that they have been prepared, packed, or held under insanitary conditions whereby they may have been contaminated with filth or rendered injurious to health. You can find the Act and the regulations through links in FDA’s Internet Homepage at www.fda.gov.
 
Your significant violations of the CGMPs are as follows:
 
1. Failure to store finished food under conditions that will protect against physical, chemical, and microbial contamination [21 CFR 110.93]. Specifically, investigators observed rodent excreta pellets on the packaging of finished food products throughout your facility, and a field exam of two separate lots of flour found contamination of both lots by rodent excreta pellets. One of these lots of flour was also found during the field exam to be contaminated by bird-like feathers. Bird droppings, live insects, and dead insects were observed on several bags of flour. Rodent gnaw marks were found on several bags of potato starch. Investigators observed cooler condensate dripping on exposed products including ready-to-eat cabbage. A utensil used to scoop ice onto ready-to-eat vegetables was found lying on a surface contaminated with oil and a black mold-like substance.  
 
2. Failure to maintain your buildings and other physical facilities of your plant in a sanitary condition and in repair sufficient to prevent food from becoming adulterated [21 CFR 110.35 (a)]. Specifically, the roof was found leaking onto a case of mandarin oranges. Furthermore, investigators observed that the exterior of your facility was not maintained in a manner sufficient to prevent pests from entering and contaminating stored and processed foods. Specifically, holes and/or gaps were observed in exterior walls, around exterior fixtures such as air intake louvers, and under person and dock doors. Open pipes and air intake louvers and fans were not screened to prevent pests from entering the building. 
 
3. Failure to take effective measures to exclude pests from the processing areas and to protect against the contamination of food on the premises by pests [21 CFR 110.35(c)]. Specifically, investigators observed a variety of living and dead animals and insects in your facility including a mouse-like animal running through your facility; a bird flying around the facility; and, a number of dead cockroaches on a glue board. 
 
4. Failure to use insecticides or rodenticides under precautions and restrictions that will protect against the contamination of food, food-contact surfaces, and food packaging materials [21 CFR 110.35(c)]. Specifically, investigators observed poison bait boxes in close proximity to food products in your facility. 
 
5. Failure to properly store equipment, remove litter and waste, and cut weeds or grass within the immediate vicinity of your facility that may constitute an attractant, breeding place, or harborage for pests [21 CFR 110.20(a(1)]. Specifically, investigators observed mounds of trash and debris, overgrown vegetation, and standing water in the immediate vicinity of your facility. Mechanical debris, equipment, and a number of (b)(4) gallon drums were also observed against the north wall of your facility. These conditions are capable of harboring mammalian and avian pests and insects that may find access to the interior of the facility. 
 
6. Failure to handle and maintain equipment and utensils used to convey, hold, or store food during manufacturing or storage in a manner that protects against contamination [21 CFR 110.80(b)(7)]. Specifically, investigators observed that metal scoops used to repackage foods, such as spices and nuts, were not cleaned between uses and were stored in a manner that exposed them to contaminants.  
 
7. Failure to provide adequate lighting in areas where food is examined, stored, or processed [21 CFR 110.20(b)(5)]. Specifically, eight (8) overhead lights were observed to be non-functioning in the South West area of your warehouse. These conditions provide a desirable area for pests to nest and make it difficult to clean and inspect the area.
 
8. Failure to maintain plumbing in a manner that will avoid creating an unsanitary condition and that will avoid constituting a source of contamination to food, water supplies, equipment, or utensils [21 CFR 110.37(b)(3)]. Specifically, a urinal in the bathroom on the lower level of the warehouse was overflowing. Persons using the bathroom were forced to track through the standing drainage when entering or leaving.
 
This letter is not intended to be an all-inclusive list of the violations at your facility. It is your responsibility to ensure compliance with applicable laws and regulations administered by FDA. You should investigate and determine the causes of the violations and take prompt actions to correct the violations to bring your products into compliance. Failure to promptly correct these violations may result in legal action without further notice including seizure and injunction.
 
FDA notes that during the inspection the Indiana State Department of Health (ISDH) placed an embargo on two lots of contaminated product as follows:
 
1. (b)(4) bags of (b)(4) Lot (b)(4)                                                                      
2. (b)(4) bags of (b)(4) All Purpose Flour, Lot (b)(4)
 
We also acknowledge that immediately following the inspection you voluntarily destroyed these two lots of flour in addition to the following items:
           
1. (b)(4) bags of (b)(4) Flour, Lot (b)(4)
2. (b)(4) bags of (b)(4) Brand Oriental Style Noodles
3. (b)(4) bags of (b)(4)
4. (b)(4) bags of (b)(4)                                                                                    
 
During the inspection you indicated your plans to correct the violative conditions noted by investigators and listed in the FDA Form 483 which was issued to you at the conclusion of the inspection. You also indicated that many of your proposed corrective actions would be accomplished within 30 days of receiving the FDA Form 483. 
 
Please notify this office in writing within fifteen (15) working days from the date you receive this letter of the specific steps you have taken to correct the noted violations, including an explanation of how you plan to prevent these violations, or similar violations, from occurring again. Please include and explain any documentation that supports your corrective actions. If additional planned corrections will occur over time, please include a timeframe for implementation of those corrections. If corrective action cannot be completed within 15 working days, state the reason for the delay and the time in which the corrections will be completed.
 
Your written response should be sent to Tina M. Pawlowski, Ph.D., Compliance Officer, at the above address.   If you have any questions regarding this letter, please contact Compliance Officer Pawlowski at (313) 393-8217 or by e-mail at tina.pawlowski@fda.hhs.gov
 
 
Sincerely,
/S/
Joann M. Givens
Detroit District Director
Detroit District Office
 

 

-

Choksi Laboratory 9/30/10

  

Department of Health and Human Services' logoDepartment of Health and Human Services

Public Health Service
Food and Drug Administration
 Silver Spring MD 20993

Warning Letter

VIA UPS MAIL

WL: 320-10-10

September 30, 2010

Mr. Vyangesh Choksi, Director
Choksi Laboratories, Ltd.
6/3 Manoramaganj
Indore 452001 (MP)
India

Dear Mr. Choksi:

During our April 21-24, 2010 inspection of your contract testing laboratory facility, Choksi Laboratories, Ltd., located at Plot 362, Industrial Area Phase II, Panchkula, Haryana, India, investigators from the Food and Drug Administration (FDA) identified significant violations of Current Good Manufacturing Practice (CGMP) regulations for Finished Pharmaceuticals, Title 21, Code of Federal Regulations, Parts 210 and 211, as they apply to your contract testing laboratory facility. These violations cause drug product components tested by your facility to be adulterated within the meaning of section 501(a)(2)(B) of the Federal Food, Drug, and Cosmetic Act (the Act) [21 U.S.C. § 351(a)(2)(B)] in that the methods used in, or the facilities or controls used for, their manufacture, processing, packing, or holding do not conform to, or are not operated or administered in conformity with, CGMP.

We note that you did not provide a written response to the Form FDA-483, Inspectional Observations.

Specific violations observed during the inspection include, but are not limited, to the following:

1. Your firm has not established scientifically sound and appropriate specifications, standards, sampling plans, and test procedures designed to assure that tested products conform to appropriate standards of identity, strength, quality, and purity [21 C.F.R. § 211.160(b)].

For example,

a) The gas chromatographic analysis performed and the data provided to the application sponsor is not traceable to raw data. The original chromatograms could not be located during the inspection.

b) In-house laboratory procedures for various laboratory tests were either non-existent or inadequate. For example, the entire GC and HPLC test procedures address only a few precautions to be taken in running the instruments. Routine practice consisted of performing test procedures provided by customers, and then destroying these procedures as soon as the analyses were completed.

c) Your firm's standard operating procedure #CLL-PKL-SOP-10, “Maintenance of Integrity of Sample,” is inadequate in that it does not assure complete integrity of documentation related to sample analysis. It specifies the assignment of a “booking number” to each sample, but no further procedures regarding subsequent documentation are included. Certain elements of sample integrity are addressed in other SOPs, but none of the procedures explicitly call for maintaining sample integrity throughout the testing of the sample.

d) Performance of test methods such as loss on drying, residue on ignition, and sulfated ash is not adequately documented. Certain steps such as time in and time out of the oven are not recorded, and the laboratory record does not provide a format for recording such data.
e) Method verifications for compendial tests are not performed. Any method, including compendial methods, must be verified as suitable under actual conditions of use. This has not been done for any method provided by your clients.

2. Your firm has not thoroughly investigated the failure of a batch or any of its components to meet its specifications whether or not the batch has already been distributed [21 C.F.R. § 211.192].

For example,

a) Your firm's out-of-specification (OOS) procedure #CLL-PKL-SOP-01, Ver. #3 is inadequate in that the procedure for invalidation of an OOS result is inappropriate. The procedure does not specify re-analysis of the original sample solution or stock solution before re-sampling of a new portion of the original sample, or using a fresh sample obtained from a client. Additionally, the procedure specifies invalidation of an OOS result if the results of (b)(4) subsequent analyses of a new sample portion or of a fresh sample from the client are within specifications.

b) Documentation is not maintained for every OOS event. Your firm only conducts OOS investigations when the client provides additional payment for such an investigation.

3. Your quality control unit has not approved or rejected all procedures or specifications impacting the identity, strength, quality, and purity of the drug product; all procedures applicable to the quality control unit are not in writing, and all procedures are not followed [21 C.F.R. § 211.22].

For example,

a) SOP revisions are not performed and documented appropriately. For example, for SOP #CLL-PKL-SOP-01, the recorded history shows that version 02 was issued on March 10, 2009, version 03 on April 2, 2009, and version 02 again on March 14, 2009.

b) Records are issued from the record storage room without any written checkout procedures, and instead upon verbal direction by the QA manager.

c) The document control SOP lists “quality manager” and “technical manager” under“Responsibility” for document control, but does not clarify the individual roles of each.

4. Your firm has not established procedures for investigation of complaints, and for initiation of corrective and preventive actions based on results of such investigations [21 C.F.R. § 211.198].

For example,

a) Five complaints received in 2009 were related to the reporting of incorrect batch numbers. Root cause was attributed to unintelligible handwriting, but no preventive actions were taken.

b) Five complaints received in 2008 were based on incorrect or missing information on the customer analysis reports, but no corrective or preventive actions were taken.

The violations cited in this letter are not intended to be an all-inclusive statement of violations that exist at your facility. You are responsible for investigating and determining the causes of the violations identified above and for preventing their recurrence and the occurrence of other violations. If you wish to continue to test pharmaceutical components or drug products intended for distribution in the United States, it is the responsibility of your firm to ensure compliance with all U.S. standards for CGMP and all applicable U.S. laws and regulations.

Until all corrections have been completed and FDA has confirmed corrections of the violations and your firm’s compliance with CGMP, this office will recommend withholding approval of any new applications or supplements listing your firm as a contract testing laboratory.

Within fifteen working days of receipt of this letter, please notify this office in writing of the specific steps that you have taken to correct these violations. Include an explanation of each step being taken to prevent the recurrence of violations and copies of supporting documentation. If you cannot complete a corrective action within fifteen working days, state the reason for the delay and the date by which you will have completed the correction. Please identify your response with FEI # 3008299032.

If you have questions or concerns regarding this letter, contact Thomas Savage, Compliance Officer, at the below address and telephone number.

U.S. Food and Drug Administration
Center for Drug Evaluation and Research
Division of Manufacturing and Product Quality
International Compliance Branch
White Oak, Building 51
10903 New Hampshire Ave
Silver Spring, MD 20993
Tel: (301) 796-3193
Fax: (301) 847-8741


Sincerely,

/s/


/Richard L. Friedman/
Richard L. Friedman
Director
Division of Manufacturing and Product Quality
Office of Compliance
Center for Drug Evaluation and Research

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Qualiphar Nv

  

Department of Health and Human Services logoDepartment of Health and Human Services

Public Health Service
Food and Drug Administration
 Silver Spring MD 20993
 

Warning Letter

VIA UPS MAIL

WL: 320-10-11

September 30, 2010
 

Mr. Karl Verlinden
General Manager
Qualiphar n.v.
Rijksweg 9
B-2880 Bornem
Belgium

Dear Mr. Verlinden:

During our May 3 – 7, 2010 inspection of your pharmaceutical manufacturing facility, Qualiphar n.v., located at Rijksweg 9, B-2880 Bornem, Belgium, an investigator from the Food and Drug Administration (FDA) identified significant violations of Current Good Manufacturing Practice (CGMP) regulations for Finished Pharmaceuticals, Title 21, Code of Federal Regulations, Parts 210 and 211. These violations cause your drug products to be adulterated within the meaning of section 501(a)(2)(B) of the Federal Food, Drug, and Cosmetic Act (the Act) [21 U.S.C. § 351(a)(2)(B)] in that the methods used in, or the facilities or controls used for, their manufacture, processing, packing, or holding do not conform to, or are not operated or administered in conformity with, CGMP.

We have reviewed your firm’s response of May 28, 2010, and note that it lacks sufficient corrective actions.

Specific violations observed during the inspection include, but are not limited, to the following:

1. Your firm does not have adequate written procedures for production and process control designed to assure that the drug products you manufacture have the identity, strength, quality, and purity they purport or are represented to possess [21 C.F.R. § 211.100(a)]. Specifically, you fail to have written procedures for the manufacturing process of both the (b)(4) powder (b)(4) tablet drug products. For example:

a. Your 2002 process validation for the manufacturing of (b)(4) powder (b)(4) is deficient in that the batch production records failed to identify the specific type and sizes of equipment used and the manufacturing steps listed were minimal (i.e., (b)(4)). In addition, a comparison of the batch records for the powder (b)(4) instructions used for the 2002 validation batches with the recent 2008-2009 campaign batches showed changes in types of sugars, changes in (b)(4) time, changes in equipment and changes in order of addition of ingredients. In addition, there was no records showing these procedures had been drafted, reviewed and approved by the appropriate organizational unit. Although your quality manager informed our investigator that the changes mentioned were intended to improve content uniformity, there was no documentation to justify these changes as required by 21 CFR 211.100 (b). In addition, your firm could not provide documentation showing that any validation or testing of the powder filling operation had ever been done to ensure that the product remained homogeneous over the entire filling process. Also, a new filling machine was used (single head automatic powder filling machine, serial # 15200). However, there was no documentation of equipment qualification such as: IQ, OQ, PQ, nor documentation of machine operating parameters (i.e., agitator settings, speed, and vibration settings).

b. The only process validation study records available for the manufacture of (b)(4) tablets (b)(4) was summarized in a three page document identifying (b)(4) batches manufactured in 1997. This summary report did not include batch size, identification of equipment used, a detailed description of the manufacturing process (batch production records were not available), equipment parameters, and a description of the sampling plan used. The three-page validation record was undated, unsigned, and references (b)(4) batch numbers ((b)(4)) that are inconsistent with the coding format used in your facility.

Your firm acts as a contract manufacturer for powder (b)(4) and solid dosage drug products. It is essential that you understand your responsibility to operate in full compliance with CGMPs and to inform all of your customers of significant problems encountered during the manufacturing and testing of these products.

Your response acknowledges that the manufacturing process validation could be improved for both powder and tablets. Therefore, in collaboration with your customer, (b)(4) (the (b)(4) holder of (b)(4)), you stopped the production of your (b)(4) products in (b)(4) and dismantled the manufacturing area with the objective of (b)(4). At that time you indicated you would re-validate the entire manufacturing process for both (b)(4) tablets and powder.

The above observations are repeat observations, also cited during two previous FDA inspections of February 25-27, 1998 and November 4-8, 2002, and for which you had also promised corrections in your written responses to the FDA-483s. The February 25-27, 1998 inspection covered (b)(4) tablets and revealed that the (b)(4) process of the (b)(4) had not been validated. The November 4-8, 2002 inspection revealed several CGMP violations, including that the (b)(4) process for had not been validated. Additionally, the batch manufacturing record for (b)(4) tablets lacked detailed instructions regarding the amount of (b)(4) to be placed on the individual (b)(4) during the (b)(4) process.

This is the third occasion in which our investigators found that your facility stopped manufacturing (b)(4) the (b)(4) prior to our visit. For example, prior to our inspection of 1998, your facility last manufactured commercial (b)(4) tablets in (b)(4). Also, prior to the 2002 inspection, your facility had last manufactured (b)(4) powder (b)(4) in (b)(4). Likewise, the May 2010 inspection revealed that you stopped manufacturing both powder and tablet (b)(4) in . Therefore, the manufacture of (b)(4) was difficult to evaluate during these inspections. Your previous and current responses are similar in that your firm plans to (b)(4)

Electronic correspondence between your firm and (b)(4) obtained during the inspection reveals that you are aware of difficulties related to the manufacture of this product. Specifically, you are aware that (b)(4) is very insoluble and that the assay and dissolution results can be affected by slight variations in the manufacturing procedures.

We are concerned that you have not completed, or adequately validated the (b)(4) manufacturing process to current standards and expectations. Additionally, new equipment has not been qualified, and there is no assurance that the manufacturing process will result in a product that can consistently meet specifications. Your validation studies demonstrate yourfailure to consistently manufacture (b)(4) powder (b)(4) and tablets, as reported in this letter under item numbers two and three.

2. Failure to follow written procedures that describe the in-process controls established to be conducted on appropriate samples of in-process materials of each batch, to monitor the output and validate the performance of those manufacturing processes that may be responsible for causing variability in the characteristics of in-process material and the drug product [21 C.F.R. § 211.110(a)]. For example,

The only sample collected for (b)(4) determination after the (b)(4) of the (b)(4) used for (b)(4) tablet (b)(4) lot #(b)(4), resulted in an out-of-specification (OOS) result of (b)(4)% (batch record specification for (b)(4) is less than (b)(4)%). However, production continued and your firm released the batch without conducting an investigation as required by 21 C.F.R. § 211.192.

Your response states that there is no indication from your release and stability data that higher in-process (b)(4) content in (b)(4) had any effect on the identity, strength, quality, or purity of the finished tablets. We disagree with this conclusion in that quality must be built into the product throughout the manufacturing process. Finished product testing alone is not sufficient to demonstrate that the process is validated, particularly when discrepancies such as (b)(4) control limits are not observed during manufacturing.

Your response is inadequate in that it lacks information regarding any investigation conducted, even after the lot was released, that would explain the root cause of the problem. Your response also fails to state your rationale for releasing this batch without an investigation and the corrective actions implemented to prevent recurrence. We are concerned that other batches not meeting your in-process control procedures may have been released for distribution.

In your response, please include a list of all the products and lots manufactured by your firm within expiration that were released for distribution without meeting the established in-process specification. Also include a complete investigation of the root cause, the corrective and preventive action plan implemented, and any voluntary action necessary to address affected products in distribution.

3. Established laboratory control mechanisms are not followed [21 C.F.R. § 211.160(a)]. For example,

In 2009, various batches ((b)(4)) of (b)(4) powder (b)(4) failed either the assay or dissolution tests prior to release. Your OOS investigation reported that there were no errors related to calculations, analyst, analytical methods, or production process equipment, and that the OOS results were confirmed. However, instead of reporting the OOS as the final result, as required by your OOS investigation procedure, you invalidated the failing results, re-sampled and tested the batches. These batches were released for distribution.

Electronic correspondence collected during the inspection, related to the assay results for the 2009 powder campaign, showed (b)(4) instructed your firm to re-weigh and reject bottles found with excess fill weights because failing assay results were obtained. This practice is unacceptable regardless if requested by your customers, and is an indication of a lack of adequate controls in place to assure that (b)(4) powder (b)(4) products are manufactured in compliance with CGMP.

Your response for batches (b)(4), reports that the assay and dissolution OOS results were due to high bottle fill weights that occurred at the end-of-fill for these batches. This response is inadequate in that it does not provide any investigative report to support your conclusion and rationale. Review of production records for your in-process fill weights show no evidence of excess fill weight of bottles. The only overweight average was obtained on the (b)(4) day of a (b)(4)-day filling operation for batch (b)(4). Additionally, there were no overweight averages obtained for batch (b)(4). Therefore, your conclusion that fill weights were the problem is not supported by your batch records. Furthermore, your batch records are also not clear on how the bottles for the re-test of the “new end-of-filling” testing were selected.

Your response for batch (b)(4) indicates that you were aware of the potential problem at end of filling, and made adjustments to the filling machine to prevent overfilling. Also, overfilling and OOS results were not observed in the subsequent seven batches filled (b)(4)). This response is inadequate in that the batch record for (b)(4) contains an OOS investigation report that confirms failing results for the assay and dissolution tests. Electronic correspondence obtained during the inspection shows that following an instruction from (b)(4) you segregated, re-tested, and released the batch. The retest resulted in values within specifications, but on the lower limit for both the assay and dissolution test. (b)(4) attributed the OOS failure to a technical error in carrying out the method.

Your OOS procedure contains no provision for conducting a re-test of new samples based on a customer (b)(4) request. We are concerned that original release testing of multiple batches of powder (b)(4) yielded failing dissolution or assay results. Yet your firm released these batches for distribution based on passing repeat test results without conducting a thorough investigation as required under 21 C.F.R. § 211.192 to support your conclusion and rationale to release the affected lots. Retesting new samples without conducting a thorough investigation, after obtaining initial OOS results is an unacceptable practice.

In your response, please provide information regarding any voluntary corrective actions you intend for marketed the batches of (b)(4) that obtained an initial assay or dissolution OOS result. Also provide the root cause analysis into the actual or probable cause of the failures, investigation of the manufacturing process that may have caused the problem, and the corrective actions implemented to prevent recurrence of the problem.

Also include a list of all lots of (b)(4) powder (b)(4) manufactured by your firm, intended for shipment to the United States, that remain within expiration and for which an initial assay or dissolution OOS was obtained.

4. Failure to have adequate laboratory controls that includes sampling plans and test procedures designed to assure that your drug products conform to appropriate strength, quality and purity specifications. [21 C.F.R. § 211.160(b)].

For example, in 2009 portions of batches (b)(4) of (b)(4) powder were rejected due to fill weight OOS results. Your firm segregated only the end-of-fill portion of the batch, re-weighted the filled bottles and rejected those bottles that resulted with OOS fill weights. You re-assayed the samples found with high fill weights and reported that the excess weight caused both the assay and dissolution OOS results. However, our review found that this sampling plan and test procedure process lacked controls such as: appropriate documentation to justify your decision to re-weigh these batches, records failed to show when these batches were re-weighed, who conducted the re-weighing process, how many of the (b)(4) plus bottles from each batch were to be re-weighed, what value was to be used as a bottle tare weight, and the acceptance criteria used to release the batches.

For example, the sampling plan record for batch (b)(4) consisted of a one-page document that listed 244 handwritten bottle net weights. Some of these net weight recordings were circled, with a handwritten note at the bottom of the page reading in part, 29 pieces out-of-specification. There was a lack of consistency in identifying OOS units in that similar or higher bottle net weights were not circled and counted as OOS. Also, this record was only identified with the batch number ((b)(4) but not dated or signed by a production or quality unit representative. Furthermore there was no documentary evidence of the sampling plan for batch (b)(4)

Your response acknowledges that this process should be more clearly documented and prior to future production, procedures will be written, and personnel training documented. However, your response lacked documentation to ensure that all (b)(4) plus bottles of each batch met the fill weight specifications. We are concerned that other units from these two batches may have OOS for fill weights, which you have already reported to be associated with failing assay or dissolution results. We are also concerned with the lack of documentation, procedural controls and your determination that these batches of (b)(4) powder comply with CGMP based on your decision to reject only bottles found with excess fill weight at the end-of-fill run.

5. Records do not include the disposition of rejected filled drug product containers [21 C.F.R. § 211.184(e)].

For example, there are no records showing the final disposition of bottles containing (b)(4) powder (b)(4) from batches (b)(4) that were reportedly rejected due to excess (OOS) fill weight. Batch production records for batch (b)(4) indicate that 29 bottles were rejected on an unknown date in either February or March 2009. Batch production records for batch (b)(4) report that 144 bottles from end-of-filling were rejected prior to labeling. However, no records to confirm the final disposition of these units were available for review.

Your response acknowledges that the master record will be amended to document disposition of any rejected units and to incorporate a filling accountability record at the end of filling. You also indicate that product bottles with fill weights outside of the established specifications were rejected and destroyed. However, your response does not provide any documentation of the disposition of these rejected bottles to ensure that these defective units were not released for distribution.

6. Written procedures are not established for evaluations to be done at least annually and including provisions for a review of complaints, recalls, returned or salvaged drug products, and investigations conducted for each drug product [21 C.F.R. § 211.180(e)(2)].

For example, although your firm prepares annual product reviews for the products shipped to the United States, there were no written procedures describing who will prepare the reports, what information will be contained in the reports, or what the distribution of the reports should be. Our review of the two most recent annual reports for (b)(4) powder (b)(4) found the following discrepancies:

a. The 2008 report states that no batches were manufactured, but then lists the OOS results for batches (b)(4). Both the 2008 and 2009 reports state that there were no changes in manufacturing equipment or manufacturing process, but do not mention the new bottle filling equipment used for the batches produced in 2008 and 2009.

The 2009 report states that (b)(4) batches were released, and that none were reprocessed. It states on the next page that two batches were OOS because of the excess fill weight of bottles selected from the end of the batches had filling weight problems. The report does not mention that these two batches were reweighed and bottles found OOS were rejected.

Your failure to have written procedures as indicated in item number 6 of this letter is a repeat observation previously cited by FDA during the previous 2002 inspection for which you promised corrections in your response.

Your May 28, 2010 response acknowledges that written procedures are required for the annual review process, and that you will implement written procedures prior to any future batch production. We are concerned with the continuing failure to have written procedures for the preparation of annual review of your products.

In addition to the items listed above, the inspection brought additional matters to our attention that increase our concerns regarding the quality of drug products manufactured at your facility. These issues include, but are not limited to: lack of cleaning validation on equipment not dedicated to (b)(4) production, the use of dedicated equipment is not clear in the batch records, powder (b)(4) bottle filling records do not show the number of bottles filled or rejected for being out of weight limits, and batch records do not include a record of any sampling performed for each batch of drug product produced.

The violations cited in this letter are not intended to be an all-inclusive statement of violations that exist at your facility. You are responsible for investigating and determining the causes of the violations identified above and for preventing their recurrence and the occurrence of other violations. If you wish to ship your products to the United States, it is the responsibility of your firm to ensure compliance with all U.S. standards for CGMP and all applicable U.S. laws and regulations.

Additionally, your firm is neither registered nor has it listed every product in commercial distribution in the United States with FDA, as required by 21 C.F.R. § 207.40 and section 510(i) of the Act [21 U.S.C. § 360(i)]. Information on how to register and list is available at the following internet website: http://www.fda.gov/cder/drls/registration_listing.htm. You must complete the required registration and listing and provide evidence that you have fulfilled these requirements in your response to this letter.

Until all corrections have been completed and FDA has confirmed corrections of the violations and your firm’s compliance with CGMP, FDA may withhold approval of any new applications or supplements listing your firm as a drug product manufacturer. In addition, FDA will be refusing admission of articles manufactured at Qualiphar n.v., Rijksweg 9, B-2880 Bornem, Belgium into the United States. The articles are subject to refusal of admission pursuant to section 801(a)(3) of the Act [21 U.S.C. § 381(a)(3)], in that, the methods and controls used in their manufacture do not appear to conform to CGMP within the meaning of section 501(a)(2)(B) of the Act [21 U.S.C. § 351(a)(2)(B)].

Within fifteen working days of receipt of this letter, please notify this office in writing of the specific steps that you have taken to correct violations. Include an explanation of each step being taken to prevent the recurrence of violations and copies of supporting documentation. Also include distribution records to your U.S. customer and the current and future manufacturing status of (b)(4) products, as well as existing inventories of remaining (b)(4) products at your facility. If you cannot provide the requested information and complete corrective action within fifteen working days, state the reason for the delay and the date by which you will have complied with our requests. Please identify your response with FEI # 1000627334.
 

If you have questions or concerns regarding this letter, contact Edwin Melendez, Compliance Officer, at the below address and telephone number.
 

U.S. Food and Drug Administration
Center for Drug Evaluation and Research
Division of Manufacturing and Product Quality
International Compliance Branch
White Oak, Building 51
10903 New Hampshire Ave.
Silver Spring, MD 20993
Tel: (301) 796-3284
Fax: (301) 847-8741
 

Sincerely,
/S/
Richard L. Friedman
Director
Division of Manufacturing and Product Quality
Office of Compliance
Center for Drug Evaluation and Research

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