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Friday, May 28, 2010

Yancey, Samuel DVM 5/28/10

  

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

Public Health Service
Food and Drug Administration
 

New York District
158-15 Liberty Avenue

Jamaica, NY 11433


 

May 28, 2010

 

WARNING LETTER NYK 2010-20


VIA UNITED PARCEL SERVICE


Samuel Yancey, DVM
9430 State Route 812
Croghan, New York 13327


Dear Dr. Yancey:


On February 12 and 22, 2010, investigators from the U.S. Food and Drug Administration (FDA) conducted an investigation involving the use of drugs in your veterinary practice. That revealed that you caused the animal drug Phenylbute Injection 20% (phenylbutazone), ANADA 200-371, to be unsafe under section 512(a) of the Federal Food, and Cosmetic Act (the U.S.C. § 360b(a), and adulterated within the meaning of section 501(a)(5) of the Act, 21 U.S.C. § 351 (a)(5), because the drug was used in a manner that did not conform with its approved uses the regulations for Extralabel Drug Use in Animals, Title 21, Code of Federal Regulations, Part 530 (21 C.F.R. Part 530). In addition, your actions caused a cow sold for slaughter as food to become adulterated within the meaning of section 402(2)(C)(ii) of the Act, 21 U.S.C. § 342(2)(C)(ii). You can find the Act and its associated regulations on through on the FDA's web page at www.fda.gov.


The extralabel use of approved veterinary or human drugs in animals is permitted only if it complies with sections 512(a)(4) and 512(a)(5) of the Act, 21 U.S.C. § 360b(a)(4) and (5), and the implementing regulations at 21 C.F.R Part 530. Our investigation found that you failed to comply with 21 C.F.R. 530.41(a)(12) in that you prescribed Phenylbute Injection 20% (phenylbutazone), ANADA 200-371, a drug approved for use in horses only, for use in female dairy cattle20 months age or older under the terms of extralabel use and for the use in downer animals at the (b)(4), without meeting the requirements of 21 C.F.R. Part C.F.R. Part 530.41(a)(12) prohibits phenylbutazone from extralabel use in female dairy cattle months of age or older.


In addition, even if phenylbutazone was not on the list drugs prohibited from extralabel use C.F.R. Part 530.41(a)(12), you did not comply with the requirements of 21 C.F.R. 530.12 (a),(c),(d), and (e) which require that any animal drug prescribed and dispensed for extralabel use by a veterinarian shall bear or be accompanied by labeling information adequate to assure the safe and proper use of the product. The required labeling information includes:


(1) The name and address of the prescribing veterinarian.


(2) Any directions for use specified by the veterinarian including the identification of the animal, condition to be treated, dosage, frequency, route of administration, and duration of therapy. 


(3) Any cautionary statements.


(4) The veterinarian's specified withdrawal time for meat which might be derived from the treated animal.


Your prescription for extralabel use also did not meet the requirements of 21 C.F.R. 530.20(a)(2)(i), (iii), and (iv), which require that prior to prescribing or dispensing an approved new animal drug for an extralabel use in food animals, the veterinarian must:


(1) Make a careful diagnosis and evaluation of the condition for which the drug is to be used.


(2) Institute procedures to assure that the identity of the treated animal is carefully maintained.


(3) Take appropriate measures to assure that assigned timeframes for withdrawal are met and no illegal residues occur in any food-producing animals subject to extralabel treatment.


The above is not intended to be an all-inclusive list of violations. You are responsible for complying with the requirements of the Act, including the extralabel use regulations promulgated under the Act.You should take prompt action to correct the above violations and to establish procedures whereby such violations do not recur. Failure to do so may result in regulatory action without further notice, such as seizure and/or injunction.


We have enclosed a copy of 21 C.F.R. Part 530 for your reference. We strongly suggest that you review this document and become familiar with all of the requirements concerning extralabel use of new animal and human drugs so that you can prevent future violations of the Act.

You should notify this office in writing within fifteen (15) working days of receiving this letter of the specific steps you have taken to correct the noted violations, including an explanation of each step being taken to prevent the recurrence of similar violations. If corrective action cannot be completed within fifteen (15) working days of receiving this letter, state the reason for the delay and the time frame within which the corrections will be completed. Also, include copies of any available documentation demonstrating that corrections have been made.


Your response should be sent to Patricia A. Clark, Compliance Officer, U.S. Food and Drug Administration, 300 Pearl St, Suite 100, Buffalo,New York 14202. If you have any questions about this letter, please contact Compliance Officer Patricia A. Clark at 716-551-4461. ext 3168.
 

Sincerely yours,

/S/
Ronald M. Pace
District Director
New York District

 

-

American Sea Food Company, Inc. 5/28/10












  

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 

 

W/L 24-10



May 28, 2010

David E. Arpia, President/Owner

American Sea Food Company, Inc.

4904 North Harbor Drive #201

San Diego, CA 92106



Dear Mr. Arpia:



On February 1st - 18th, 2010 we inspected your seafood processing facility, located in 4904 North Harbor Drive #201, San Diego, CA 92106. We found that you have serious deviations from the seafood HACCP Regulations, Title 21, Code of Federal Regulations, Part 123 (21 CFR 123). In accordance with 21 CFR 123.6(g), failure of a processor to have and implement a HACCP plan that complies with this section or otherwise operate in accordance with the requirements of this part, renders the fishery products adulterated within the meaning of Section 402(a)(4) of the Federal Food, Drug and Cosmetic Act (the Act), 21 U.S.C § 342(a)(4). Accordingly your scombroid-forming fishes are adulterated, in that these fishes have been prepared, packed, or held under insanitary conditions whereby they may have become contaminated with filth, or whereby it may have been rendered injurious to health. You may find the Act and the Seafood HACCP Regulations through links in FDA's home page at www.fda.gov.



We acknowledge your written responses to the February 2010 FDA inspection. Two written responses were received by Los Angeles District Office; one on April 7th 2010 and the second on April 13th 2010. We have reviewed your responses, which included an updated HACCP plan. However, based on your response, your scombroid-forming fish continue to be adulterated. The deviations are as follows:



1. You must have a HACCP plan that at a minimum, lists critical limits that must be met, to comply with 21 CFR 123.6(c)(3). A critical limit is defined in 21 CFR 123.3 (c) as the "maximum or minimum value to which a physical, biological or chemical parameter must be controlled at a critical control point to prevent, eliminate or reduce to an acceptable level the occurrence of the identified food safety hazard." However, your undated HACCP plan for "Fresh and Frozen Tuna," received on April 13, 2010, does not list adequate critical limits at the Receiving critical control point (CCP) to ensure that scombroid species received directly from the harvest vessel have been handled properly in order to control histamine formation. We note that your firm is occasionally the primary processor of tuna that is received directly from fishing vessels. 

 

Your current critical limit, i.e. "All lots received are accompanied by harvest vessel records" is insufficient for controlling the hazard of scombrotoxin formation. In addition to collecting harvest vessel records for each, you should also conduct a sensory examination of at least 118 fish per lot and use a thermometer to the measure the internal temperature of a representative number of fish at receipt (minimum of 12 fish). Alternatively, if you receive scombroid species fish from vendors, other than harvest vessels, you must ensure that the fish is delivered with transportation records that show the fish was held at or below 40° F throughout transit or held under an adequate quantity of ice or chemical cooling media at the time of delivery. Please refer to the Fish and Fishery Products Hazard and Controls Guidance, chapter 7 - "Histamine Control" for more information on primary and secondary processor monitoring requirements.



In addition, we note that your firm processes other scombroid species fish, in addition to tuna, such as Mahi-Mahi. Your HACCP plan should reflect all your scombroid fish species.



2. You must implement the monitoring procedures and frequency that you have listed in your HACCP plan, to comply with 21 CPR 123.6(b) and (c)(4). However, your film did not follow the monitoring procedure of 1) internal temperature taken for each receipt of scombroid fish transported for 4 hours or less, and 2) checking the suppliers certification that they are following their HACCP plan at the Receiving critical control point to control histamine formation listed in your HACCP plan for "Fresh and Frozen Tuna," received on April 13, 2010. For example, your firm did not document product temperature or certificate information upon receipt for Tuna, Mahi-Mahi, and other histamine species on its receiving records for the months of Oct. 2009 to January 2010 as per the HACCP plan.



In addition, on 2/1/2010 at approximately 8:00 am, you received Tuna, Albacore, and Mahi-Mahi without checking the temperature or the adequacy of ice on receipt. This product was seen strapped closed in the cooler, on the a.m. of 2/2/10 and management stated that it still had not been monitored for its receipt. In addition, you did not assess the suppliers certificate that the product was handled correctly as per their HACCP plan as stated in your critical limits at Receiving.



3. 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 CPR 123.6(c)(4). However, your film's HACCP plan for "Fresh and Frozen Tuna," received on April 13, 2010, lists a monitoring procedure at the "Storage of fresh tuna in the plant" critical control point that is not adequate to control scombrotoxin formation. Specifically, your HACCP plan states that you will monitor the "icing of fish and/or storage in cooler." Your monitoring procedure, as written, allows you to alternate between checking that the fish is stored in the cooler and/or stored on ice. When scombrotoxin fish are stored in the cooler you will need to ensure that the fish is continuously held at the temperature specified in your critical limit and have equipment capable of providing a continuous record of the time/temperatures on a 24 hour a day/7 day a week basis.



4. You must maintain sanitation control records in accordance with 21 CPR 123.11(c) per the recordkeeping requirements detailed in 21 CFR 123.9(a). However, we observed that on 2/01/10, your firm did not accurately record your sanitation records with the actual date and time that the data was obtained. For example, the aforementioned record had data marked for the "6 AM" and "10 AM" checklist columns; however, it was determined that you were not able to record the "10 AM" data due to the fact that you were with the CSOs in another capacity at the time. At 11:00A, when the daily sanitation monitoring record was reviewed, it was determined that the data had been prefilled. Your sanitation records should reflect the accurate conditions in the plant, and must be recorded at the date and time when the activity actually took place. [FDA-483 item #9]



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. In addition, we may not provide certificates to your film for export of your products to European Union (EU) countries if you do not correct these deviations.



Please respond in writing within 15 working days from your receipt of this letter. Your response should outline the specific things you are doing to correct these deviations. You may wish to include in your response documentation such as revised HACCP planes), HACCP and sanitation monitoring records or other useful information that would assist us in evaluating your corrections. If you cannot complete all corrections before you respond, we expect that you will explain the reason for your delay and state when you will correct any remaining deviations.



This letter may not list all the deviations at your facility. You are responsible for ensuring that your processing plant operates in compliance with the Act, the Seafood HACCP Regulations and the Good Manufacturing Practice regulations (21 CFR Part 110). You also have a responsibility to use procedures to prevent further violations of the Federal Food, Drug, and Cosmetic Act and all applicable regulations.



Your written reply should be addressed to:



Blake Bevill

Director, Compliance Branch

Food and Drug Administration

19701 Fairchild

Irvine, CA 92612-2506



If you have any questions regarding this letter, please contact Mr. Robert B. McNab, Compliance Officer at 949-608-4409.



Sincerely,

/S/

District Director

Cc: California Department of Public Health

Food and Drug Branch

1500 Capitol Avenue, MS-7602

P.O. Box 9974 13

Sacramento, CA 95899-7413

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Thursday, May 27, 2010

Ribbon SRL 5/27/10

  

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

May 27, 2010

Ms. Maria Gobbi
General Manager
Ribbon Pharmaceutical and Chemical Products
Via San Leonardo 23
Villadose, Rovigo
Italy

WL: 320-10-006

Dear Ms. Gobbi:

During our December 8 - 15,2009 inspection of your pharmaceutical manufacturing facility, Ribbon Pharmaceutical and Chemical Products located at Via San Leonardo 23, Villadose, Rovigo, Italy, 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. 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 December 31, 2009, 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 has not established appropriate written procedures designed to prevent microbiological contamination of drug products purporting to be sterile [21 C.F.R. § 211.113(b)].

For example, the process simulations (media fill) do not represent actual production operations for your sterile API. The process simulation performed by your firm in July 2009 failed to include simulation of the routine interventions performed in a typical campaign of 13 batches.

Your response indicates that the revised media fill protocols now include the routine interventions in a 13-batch campaign and were performed on January 4, 2010. Your response is inadequate because it does not include the results of the repeated process simulations performed. In your response to this letter, provide the finalized protocol and the summary report for all data generated during the execution of process simulations.

In addition, the process simulation procedures your firm used to evaluate state of control of sterile API manufacture are inadequate because they do not accurately simulate aseptic manufacturing operations. In addition, the test material and the validation procedures used by your firm compromise the recovery of microbial contaminates. For example:

a. Placebo mediums should be evaluated for their ability to support growth. Your response states that the placebo used in the process simulation is sodium phosphate in different forms (solution and anhydrous) and sodium chloride solution (l %). The principle of using simulation media is to create conditions representing the greatest possibility of recovering existing contaminants. Your response does not provide scientific evidence and documentation that the placebo medium (solution and anhydrous) used during process simulation adequately supports growth promotion of viable organisms. In your response to this letter, provide the rationale and the supporting study summary report for using each of the placebo growth media (including the medium in its anhydrous state) in your process simulations.

b. Placebo mediums should be evaluated for their inhibitory effect on microorganisms. Your response does not indicate that your firm uses beta-lactamase to inhibit the effect of antibiotic residue in the production line during process simulation. Media used in process simulation, sterility testing, and environmental monitoring should be evaluated for the use of beta-lactamase to neutralize antibiotics produced at your manufacturing facility. Neutralization of media makes it possible to recover the viable microorganisms that may contaminate the product. Media for environmental monitoring and microbiological testing (including process simulation) should be tested for sterility and growth promotion. You should also assure all media includes antibiotic neutralizing agents. In your response, provide documentation to support that your firm uses beta-lactamase in the media used for the environmental monitoring programs during the process simulations. Provide a copy of the test procedures for beta lactamase in media.

c. Gases used during process simulation should be evaluated for their inhibitory effect on microorganisms. Your response states that the nitrogen used in the process simulation is removed by the test membrane during filtration. Most contaminants likely to be present in pharmaceutical manufacturing environments metabolize aerobically. The creation of anaerobic conditions in the headspace above the media would decrease the probability of recovering these aerobes. Inert gas used in the process simulations should be replaced with compressed air to create worst case condition. Your response is inadequate because it does not include scientific evidence to ensure that the use of nitrogen during process simulations does not inhibit growth of aerobic organisms.

2. Controls to prevent contamination in defined (critical and support clean) areas are deficient regarding operations related to aseptic processing of product [21 C.F.R. § 211.42(c)(10)].

For example, there are no dynamic smoke study evaluations to demonstrate that the personnel activities during aseptic filling do not compromise the sterile API. The activities conducted during your documented smoke studies are not representative of actual operations.

According to your response, smoke studies were to be completed within the first two weeks of January 2010. Your response is inadequate because it does not provide an update on all airflow pattern findings and your evaluation of these study results. An in situ air pattern analysis should be conducted at all critical areas, under dynamic conditions, to demonstrate unidirectional airflow and sweeping action at critical work areas. These studies should evaluate the impact of aseptic manipulations (e.g. interventions) and equipment design, and include documentation for the activities performed with written conclusions. Provide a copy of the smoke study recordings that can be read using Windows Media Player (as an mpeg file, for example) along with supporting documentation. Please also identify the different videos by file name to indicate what is being presented in each file.

3. Your firm does not clean and maintain equipment at appropriate intervals to prevent contamination that would alter the safety, identity, strength, quality, or purity of the drug product [21 C.F.R. § 211.67(a)].

During the inspection, cleaned multi-use hoses used in the production of cephalosporin intermediates had white residue or brown rust-like residue on the connection surface and the interior of the transfer hose. The presence of rust, deterioration, and debris in product-contact equipment used to manufacture sterile drug products is unacceptable.

We acknowledge the training you provided on your procedure, PRO-SOP-010/02 "General rules of cleaning," and the associated training records. However, your response does not provide the controls implemented to ensure that contaminated hoses are not used in manufacturing. Your response also does not include evidence of corrective actions taken to remove the presence of rust, deterioration, and debris from your product-contact equipment and transfer hoses.

In your response to this letter, provide the production process steps where these hoses are used. Additionally, provide documentation to support that your firm's cleaning procedures are adequate to prevent contamination of your products. Lastly, provide the investigation report with your findings including the cleaning methods performed, as well as the corrective and preventive actions.

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 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.

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, failure to correct these violations may result in FDA refusing admission of articles manufactured at Ribbon Pharmaceutical and Chemical Products located at Via San Leonardo 23, Villadose, Rovigo, Italy 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 Current Good Manufacturing Practice 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. If you cannot complete corrective action within fifteen working days, state the reason for the delay and the date by which you will have completed the correction. Additionally, your response should state if you no longer manufacture or distribute Ceftriaxone Sodium Sterile, Cefuroxime Sodium Sterile, Cefoxitin Sodium Sterile, and Ceftazidime Buffered Sterile, and provide the dates and reasons you ceased production. Please identify your response with FEI #3005479678.

If you have questions or concerns regarding this letter, contact Maan Abduldayem, 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) 796-3916
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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Italco Food Products, Inc. 5/27/10

  

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

Public Health Service
Food and Drug Administration
 Southwest Region
Denver District Office
Bldg. 20-Denver Federal Center
P.O. Box 25087
6th Avenue & Kipling Street
Denver, Colorado 80225-0087
Telephone: 303-236-3000
FAX: 303-236-3551

May 27, 2010

Ref:DEN-10-12 WL

WARNING LETTER

VIA UPS

Mr. Michael A. Laurita, Co-Owner
Mr. Christopher J. Laurita, Co-Owner
Italco Food Products, Inc.
1340 South Cherokee Street
Denver, Colorado 80223

Dear Messrs. Laurita:

We inspected your firm, Italco Food Products, Inc., located at 1340 South Cherokee Street, Denver, Colorado, on January 20-22, 25-26, 28, 2010. Our inspection found that your firm has serious deviations from the Seafood Hazard Analysis and Critical Control Points (HACCP) Regulations, Title 21, Code of Federal Regulations, Part 123 [21 CFR Part 123]. In accordance with 21 CFR §123.6(g), failure of a processor to have and implement a HACCP plan that complies with this section or otherwise operate in accordance with the requirements of 21 CFR Part 123 renders the fishery products adulterated within the meaning of Section 402(a)(4) of the Federal Food, Drug, and Cosmetic Act (the "Act"), 21 U.S.C. §342(a). Accordingly, your vacuum packaged smoked salmon, smoked trout, and pickled seafood salad in oil 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 and the Seafood HACCP Regulations through links in FDA's home page at www.fda.gov.

The deviations that were found during the inspection were as follows:

1. You must conduct, or have conducted for you, a hazard analysis for each kind of fish and fishery product that you process 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 reasonable likely to occur, to comply with 21 CFR 123.6(a) and (b). However, your firm does not have a HACCP plan for vacuum packaged smoked salmon, smoked trout, and pickled seafood salad in oil to control the hazard of pathogen growth and toxin formation from the growth of Clostridium botulinum.

We received your written response February 16, 2010 to the FDA 483, Objectionable Observations. Our review of the information provided in that response reveals that it is inadequate. While you state that you will begin the HACCP program, you have not, as of this time, provided a HACCP plan (or plans) to address the hazards and controls associated with the above mentioned products.

You may find the Act, the seafood HACCP regulation, and FDA's, Fish and Fisheries Products Hazards and Controls Guidance: 3rd Edition (the Hazard Guide) through links in FDA's home page at www.fda.gov.

When conducting your hazard analysis, your firm should assess those steps that are reasonably likely to result in Clostridium botulinum growth and toxin formation due to time/temperature abuse. For example, receipt of refrigerated products will likely be critical to ensure that proper temperatures were maintained during the transit period to your facility. In addition, refrigerated finished product storage will likely be critical to ensure proper temperatures are maintained during extended storage periods. FDA recommends the use of equipment capable of monitoring and recording refrigerated temperatures on a 24 hour a day/7 day a week basis, with a daily check of the temperature records and a daily check of the equipment.

We may take further action if you do not promptly correct these violations. For instance, we may initiate regulatory action without further notice. Such actions may include the initiation of a seizure action against your products and/or an action to enjoin your firm from operating.

Please respond in writing within 15 working days from your receipt of this letter. Your response should outline the specific things you are doing to correct these deviations. You should include in your response documentation such as your HACCP plans, any records required to document your HACCP plan including temperature monitoring records, corrective actions, or other useful information that would assist us in evaluating your corrections. If you cannot complete all corrections before you respond, we expect that you will explain the reason for your delay and state when you will correct any remaining deviations.

This letter may not list all of the deviations at your facility. You are responsible for ensuring that your processing plant operates in compliance with the Act, the Seafood HACCP Regulations, and the Good Manufacturing Practice regulations (21 CFR Part 110). You also have a responsibility to use procedures to prevent further violations of the Act and all applicable regulations.

Please send your reply to the Food and Drug Administration, Attention: Carolyn A. Pinney, Compliance Officer, at the above letterhead address. If you have any questions regarding any issue in the letter, please contact Carolyn A. Pinney at (303) 236-3024.

Sincerely,

/s/

 

H. Thomas Warwick, Jr.
Denver District Director

 

HTW/cap

 

 

 

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Industrias Alimentarias De Navarra, S.A.U.

  

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

Public Health Service
Food and Drug Administration
 College Park, MD

WARNING LETTER
 

MAY 27, 2010
 

Mr. Alejandro Martinez Campo
General Manager
Industrias Alimentarias de Navarra, S.A.U.
Poligono Penalpons s/n 31,330
Villafranco Navarra, Spain
 

Dear Mr. Campo:

FDA inspected your low-acid canned food facility located at Barrio De La Estacion s/n, 10730 Casas del Monte, Caceres, Spain, on February 18-22, 2010. During that inspection, we found that your firm had serious deviations from the low-acid canned food regulations (21 CFR Parts 108 and 113). Failure to comply with all of the mandatory requirements of 21 CFR 108.35 and 21 CFR Part 113 constitutes a prima facie basis for the immediate application of the emergency permit control provisions of section 404 of the Act and particularly implementation of 21 CFR 108.35(k) for products offered for entry into the United States. In addition, such failure renders your low-acid canned food products adulterated within the meaning of Section 402(a)(4) of the Federal Food, Drug and Cosmetic Act (the Act), 21 U.S.C. 342(a)(4). Accordingly your product, canned black olives, is adulterated in that the product has been prepared, packed or held under insanitary conditions whereby it may have been rendered injurious to health. You can find the Act and the low-acid canned food regulations through links in FDA's home page at http://www.fda.gov.

This inspection resulted in FDA's issuance of an FDA-483, Inspectional Observations, listing the deviations found at your firm at the conclusion of the inspection. Your firm provided a response to the FDA-483 via email on February 25, 2010.
 

Upon further review of the inspectional findings and documentation provided in your February 25, 2010 response, we have the following concerns with regard to your low-acid canned food products:
 

• Your firm failed to determine and record the initial temperature of the contents of the black olives in (b)(4) prior to processing to ensure that the temperature of the product is no lower than the minimum initial temperature specified in the scheduled process as required by 21 CFR 113.87(c). Specifically, on February 18, 2010, our investigator observed no initial temperatures being recorded prior to the processing of black olives in (b)(4) In addition, your firm's thermal processing records show that no initial temperatures were recorded prior to processing black olives in December 23, 2009, respectively. Subsequently, these same records failed to contain other critical factors identified in your scheduled process, such actual processing times and the Mercury-in-glass temperatures, as required by 21 CFR 113.100(a)(7). Your firm's response included a modified blank template record to be used to record processing data including initial temperatures, size of containers, and processing times; however, we would like to review completed processing records utilizing this newly modified record template.
 

• Your firm failed to properly identify and handle temperature process deviations that occur during the thermal processing of canned black olives in your (b)(4) retorts as required by 21 CFR 113.89. Specifically, on February 18, 2010, our investigator observed the retort operation of black olives in (b)(4) being processed at (b)(4) where the scheduled process identified a processing temperature of (b)(4) Our investigator observed no corrective action taken when this process deviation occurred. Additionally, during further record review, a similar process deviation was found for (b)(4) black olives processed on November 12, 2009 in (b)(4). Your firm's temperature recording chart records for Retort #2 show that the temperature dropped to (b)(4) during one run and ranged from (b)(4) during other runs. The scheduled process for black olives in (b)(4) identifies a processing temperature of (b)(4). According to your firm's management, your method of handling these types of process deviations is to (b)(4). In addition to documenting the length of the extended cook time for these lots, the Fo values should be calculated, and these corrective actions should be documented and reviewed by your process authority. We acknowledge that your firm has provided evidence of creating a separate file detailing these process deviations and the corrective actions taken in accordance with 21 CFR 113.89, however, we would like to review actual process deviation records to ascertain how your firm handled the corrective actions.
 

You should respond in writing within thirty (30) 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 that would assist us in evaluating your corrections. If you cannot complete all corrections within thirty (30) days, you should explain the reason for your delay and state when you will correct any remaining violations.
 

If you do not respond or if we find your response inadequate, we may take further action. For instance, we may take further action to refuse admission of your imported low-acid canned food products under Section 801(a) of the Act (21 U.S.C. §381(a)), including placing them on detention without physical examination (DWPE). FDA's DWPE is an administrative procedure whereby products offered for import into the United States may be detained without physical examination upon entry. DWPE information may be conveyed in FDA's Import Alerts. For your information, an example of an Import Alert that conveys information specific to foreign firms that are not in compliance with the canned food regulations (21 CFR Part 108 and 113) is Import Alert #99-04. This alert can be found on FDA's web site at: http://www.fda.gov/ForIndustry/ImportProgram/ImportAlerts/default.htm.
 

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 low-acid canned food regulations (21 CFR Part 108 and 113), 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 Federal Food, Drug, and Cosmetic Act and all applicable regulations.
 

Please send your reply to the U.S. Food and Drug Administration, Attention: Robyn R. Jones, Consumer Safety Officer, Office of Compliance, Division of Enforcement, Manufacturing and Storage Adulteration Branch (HFS-607), 5100 Paint Branch Parkway, College Park, MD 20740 U.S.A. If you have any questions regarding any issue in this letter, you may contact Ms. Jones at (301) 436-2575 or via email at robyn.jones@fda.hhs.gov.
 

Sincerely,

/S/
Donald A. Kautter, Jr.
Acting Director
Office of Compliance
Center for Food Safety
and Applied Nutrition
 

cc:
Mr. Fernando Fernandez Jimenez
Plant Manager
Industrias Alimentarias de Navarra, S.A.U.
Barrio de la Estacion, s/n.
10730 Casas del Monte
Caceres, Spain

-

Ribbon SRL 5/27/10

  

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

May 27, 2010

Ms. Maria Gobbi
General Manager
Ribbon Pharmaceutical and Chemical Products
Via San Leonardo 23
Villadose, Rovigo
Italy

WL: 320-10-006

Dear Ms. Gobbi:

During our December 8 - 15,2009 inspection of your pharmaceutical manufacturing facility, Ribbon Pharmaceutical and Chemical Products located at Via San Leonardo 23, Villadose, Rovigo, Italy, 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. 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 December 31, 2009, 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 has not established appropriate written procedures designed to prevent microbiological contamination of drug products purporting to be sterile [21 C.F.R. § 211.113(b)].

For example, the process simulations (media fill) do not represent actual production operations for your sterile API. The process simulation performed by your firm in July 2009 failed to include simulation of the routine interventions performed in a typical campaign of 13 batches.

Your response indicates that the revised media fill protocols now include the routine interventions in a 13-batch campaign and were performed on January 4, 2010. Your response is inadequate because it does not include the results of the repeated process simulations performed. In your response to this letter, provide the finalized protocol and the summary report for all data generated during the execution of process simulations.

In addition, the process simulation procedures your firm used to evaluate state of control of sterile API manufacture are inadequate because they do not accurately simulate aseptic manufacturing operations. In addition, the test material and the validation procedures used by your firm compromise the recovery of microbial contaminates. For example:

a. Placebo mediums should be evaluated for their ability to support growth. Your response states that the placebo used in the process simulation is sodium phosphate in different forms (solution and anhydrous) and sodium chloride solution (l %). The principle of using simulation media is to create conditions representing the greatest possibility of recovering existing contaminants. Your response does not provide scientific evidence and documentation that the placebo medium (solution and anhydrous) used during process simulation adequately supports growth promotion of viable organisms. In your response to this letter, provide the rationale and the supporting study summary report for using each of the placebo growth media (including the medium in its anhydrous state) in your process simulations.

b. Placebo mediums should be evaluated for their inhibitory effect on microorganisms. Your response does not indicate that your firm uses beta-lactamase to inhibit the effect of antibiotic residue in the production line during process simulation. Media used in process simulation, sterility testing, and environmental monitoring should be evaluated for the use of beta-lactamase to neutralize antibiotics produced at your manufacturing facility. Neutralization of media makes it possible to recover the viable microorganisms that may contaminate the product. Media for environmental monitoring and microbiological testing (including process simulation) should be tested for sterility and growth promotion. You should also assure all media includes antibiotic neutralizing agents. In your response, provide documentation to support that your firm uses beta-lactamase in the media used for the environmental monitoring programs during the process simulations. Provide a copy of the test procedures for beta lactamase in media.

c. Gases used during process simulation should be evaluated for their inhibitory effect on microorganisms. Your response states that the nitrogen used in the process simulation is removed by the test membrane during filtration. Most contaminants likely to be present in pharmaceutical manufacturing environments metabolize aerobically. The creation of anaerobic conditions in the headspace above the media would decrease the probability of recovering these aerobes. Inert gas used in the process simulations should be replaced with compressed air to create worst case condition. Your response is inadequate because it does not include scientific evidence to ensure that the use of nitrogen during process simulations does not inhibit growth of aerobic organisms.

2. Controls to prevent contamination in defined (critical and support clean) areas are deficient regarding operations related to aseptic processing of product [21 C.F.R. § 211.42(c)(10)].

For example, there are no dynamic smoke study evaluations to demonstrate that the personnel activities during aseptic filling do not compromise the sterile API. The activities conducted during your documented smoke studies are not representative of actual operations.

According to your response, smoke studies were to be completed within the first two weeks of January 2010. Your response is inadequate because it does not provide an update on all airflow pattern findings and your evaluation of these study results. An in situ air pattern analysis should be conducted at all critical areas, under dynamic conditions, to demonstrate unidirectional airflow and sweeping action at critical work areas. These studies should evaluate the impact of aseptic manipulations (e.g. interventions) and equipment design, and include documentation for the activities performed with written conclusions. Provide a copy of the smoke study recordings that can be read using Windows Media Player (as an mpeg file, for example) along with supporting documentation. Please also identify the different videos by file name to indicate what is being presented in each file.

3. Your firm does not clean and maintain equipment at appropriate intervals to prevent contamination that would alter the safety, identity, strength, quality, or purity of the drug product [21 C.F.R. § 211.67(a)].

During the inspection, cleaned multi-use hoses used in the production of cephalosporin intermediates had white residue or brown rust-like residue on the connection surface and the interior of the transfer hose. The presence of rust, deterioration, and debris in product-contact equipment used to manufacture sterile drug products is unacceptable.

We acknowledge the training you provided on your procedure, PRO-SOP-010/02 "General rules of cleaning," and the associated training records. However, your response does not provide the controls implemented to ensure that contaminated hoses are not used in manufacturing. Your response also does not include evidence of corrective actions taken to remove the presence of rust, deterioration, and debris from your product-contact equipment and transfer hoses.

In your response to this letter, provide the production process steps where these hoses are used. Additionally, provide documentation to support that your firm's cleaning procedures are adequate to prevent contamination of your products. Lastly, provide the investigation report with your findings including the cleaning methods performed, as well as the corrective and preventive actions.

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 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.

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, failure to correct these violations may result in FDA refusing admission of articles manufactured at Ribbon Pharmaceutical and Chemical Products located at Via San Leonardo 23, Villadose, Rovigo, Italy 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 Current Good Manufacturing Practice 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. If you cannot complete corrective action within fifteen working days, state the reason for the delay and the date by which you will have completed the correction. Additionally, your response should state if you no longer manufacture or distribute Ceftriaxone Sodium Sterile, Cefuroxime Sodium Sterile, Cefoxitin Sodium Sterile, and Ceftazidime Buffered Sterile, and provide the dates and reasons you ceased production. Please identify your response with FEI #3005479678.

If you have questions or concerns regarding this letter, contact Maan Abduldayem, 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) 796-3916
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
 

-

Wednesday, May 26, 2010

Pfizer, Inc. 5/26/10












  

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


Public Health Service

Food and Drug Administration
 

New York District

158-15 Liberty Ave.

Jamaica, NY 11433


May 26, 2010



WARNING LETTER NYK 2010-19



VIA UPS



Jeffrey B. Kindler

Chairman and Chief Executive Officer

Pfizer, Inc.

235 East 42nd Street

New York, NY 10017



Dear Mr. Kindler:



During the period from June 29, 2009 through August 10, 2009, an inspection was conducted by investigators of the U.S. Food and Drug Administration (FDA or Agency) of your firm located at 235 East 42nd Street, New York, NY to determine your firm's compliance with the Postmarketing Adverse Drug Experience (PADE) reporting requirements of Section 505(k) of the Federal Food, Drug, and Cosmetic Act (the Act)) [21 U.S.C. § 355(k)], and Title 21, Code of Federal Regulations (21 CFR) 314.80 and 314.81.



Section 505(k)(1) of the Act [21 U.S.C. § 355(k)(1)] and 21 CFR 314.80 and 314.81 require an applicant to establish and maintain records and to report data relating to clinical experience, along with other data or information, for drugs for which an approved application is in effect. Failure to comply with Section 505(k) is a prohibited act under Section 301(e) of the Act [21 U.S.C. § 331(e)].



I. Deviations from 21 CFR 314.80 and 21 CFR 314.81 include the following:



1. Failure to submit Adverse Drug Experience (ADE) reports to FDA as required by 21 CFR 314.80(c). Specifically:



(a) The following are examples of ADEs and information regarding ADEs that were not submitted to the FDA:

 

































Report #Mfg. Report #ProductPfizer's Seriousness/Expectedness DeterminationDate Received by Pfizer
1.2009236922Dalacin (Clindamycin HCI)Serious outcome and failure to assess expectedness05/04/09
2.2009236510CamptosarSerious/unexpected12/11/08
3.2009221607LyricaSerious outcome and failure to assess expectedness06/01/09
4.2009206349LipitorSerious/unexpected04/29/09





We have reviewed your firm's response dated September 9, 2009, and have determined that it is inadequate. The response acknowledges that the above-listed reports contained serious and unexpected adverse events which were not submitted within 15 days to FDA. These reports were not submitted until they were identified during the FDA inspection. Your firm's rationale for the failure to submit these reports included a lack of file tracking control as well as a lack of adequate training in utilizing the (b)(4) system. Your firm received FDA Forms 483 on July 29, 2004 and April 18, 2006 for similar postmarketing adverse drug experience violations and your corrective actions for these observations, including training, have been shown to be ineffective. FDA expects drug manufacturers to establish and implement reasonable mechanisms to assure that all serious and unexpected experiences are promptly recorded and investigated to determine whether or not 15-day Alert reports should be submitted to FDA.



(b) FDA's Center for Drug Evaluation and Research, Division of Reproductive and Urologic Drug Products, sent you a letter dated July 14, 2005, requesting that "all manufacturers of PDE5 inhibitors for treatment of erectile dysfunction (ED) continue to submit serious reports of postmarketing ophthalmologic adverse events that might reflect non-arteritic ischemic optic neuropathy (NAION) as 15-day Alert reports." In your letter to FDA dated October 18, 2005, your firm committed to provide 15-day Alert reports for these reported outcomes.



Your firm failed to submit 15-day Alert reports for the following serious visual adverse events that met the postmarketing reporting requirement for Viagra (sildenafil citrate) by misclassifying and/or downgrading reports to non-serious without reasonable justification:

 

 

 































































 Mfg. Report No.Serious OutcomeDate Received
1.2009230915"Lost right eye vision"06/22/09
2.2009187335"Blindness"03/19/09
3.2009193299"Blind in right eye"03/27/09
4.2009213305"Decreased vision"05/12/09
5.2009213306"Decreased vision"05/12/09
6.2009202206"Decreased vision"04/22/09
7.2009179071"Visual acuity loss"02/26/09
8.2008063424"Visual acuity reduced"07/24/08
9.2008086429"Decreased vision"10/10/08
10.2008055517"Visual deficiency"07/01&10/08
11.2008071566"Difficulty seeing"8/25/08





We have reviewed your firm's response dated September 9, 2009 and have concluded that it is inadequate. Your response indicates that only four of the above reports contained serious and/or expected reports of postmarketing ophthalmologic adverse events requiring a 15-day Alert report. However, the remaining seven adverse events were deemed as non-serious although serious outcomes such as "visual acuity loss/reduction" were noted.



2. Inadequate written procedures for the surveillance, receipt, evaluation, and reporting of adverse events as required by 21 CFR 314.80(b). Specifically:



Your firm does not have adequate written procedures in place to ensure that adverse drug experiences are correctly identified, assessed, and reported to FDA in accordance with postmarketing commitments.



For fosphenytoin, in your firm's letter to FDA dated February 13, 2009, your firm agreed to develop and implement an effective plan which would include criteria to correctly identify, assess, and report cases that are not labeled as Purple Glove Syndrome (PGS), but that are suggestive of this syndrome in association with fosphenytoin sodium use. However, your firm failed to do so.



Your firm also agreed to train all pharmacovigilance staff in the worldwide affiliates by February 15, 2009. Training was to include an overview of PGS and specific directions regarding the process for expediting any adverse event reports involving fosphenytoin use to Drug Safety Surveillance (DSS).



Despite your agreement, only six out of the required sixty-three country offices worldwide were trained and some of the offices that were trained were not trained on time, including the core DSS offices. 1



Your firm's response dated September 9, 2009 remains inadequate because it fails to include an effective plan to identify cases suggestive of PGS and fails to require medical evaluation of reports suggestive of PGS. Additionally, provisions for adequate training and documentation of training were not provided.



3. Failure to submit adverse drug experiences that are both serious and unexpected to FDA 'within 15 calendar days of initial receipt of the information as required by 21 CFR 314.80(c) (1)(i). Specifically:



(a) During the time period of approximately March 1, 2006 through December 7, 2008, there were 80,560 15-day Alert Reports submitted to FDA by your firm, of which 3558 (4%) were late. Between December 8, 2008 through June 28, 2009, approximately 1508 (9%) were submitted late, a further decline in the timeliness of reporting.



The following are examples of ADE reports that contained serious and unexpected events, but were submitted late to FDA:

 































































 Mfg. Report No.ProductReason LateNo. of Days Late
1.2007039077LipitorDelay due to case processing/other1141
2.2007039077LipitorDelay due to resubmission1102
3.2007048456AzithromycinDelay forwarding to safety site687
4.2008037900AzithromycinDelay due to case revision393
5.2009229922Amlodipine BesilateDelay due to clerical/data entry issue438
6.2008040787Prostin VRDelay due to resubmission285
7.2009231444Atorvastatin CalciumDelay forwarding to safety site274
8.2009212979Epirubicin HCIDelay forwarding to safety site728
9.2009195911EplerenoneDelay due to clerical/data entry issue356

 

According to your firm's response, implementation of (b)(4) created problems for the timely submission of 15-day Alert reports. A review of the explanations for the late reports indicates reasons such as cases being initially identified as non-serious then upgraded to serious, user error in routing cases within the safety system, case distribution errors, case processing issues, and technical errors. The firm purports to have addressed these problems by updating user manuals, reinforcing training, additional prospective and retrospective quality review of cases, updating system configuration errors, and other unspecified corrective actions with supplying organizations and partners. Your response indicates reporting improved after May 2009 and that errors significantly declined once colleagues became more experienced with the new safety system. However, your firm's response did not include comparable metrics for the post-May 2009 time period. Although the Agency recognizes the benefits to implementing a new and improved computerized tracking system, such a system can only be an improvement if there is adequate staff to make accurate data entries and if the users are adequately trained in its implementation. Your firm's response also fails to address other factors that possibly contributed to the tardiness of the reports, including personnel training in the categorization of serious versus non-serious reports, training in use of the new (b)(4) system, development of SOPs, development of standardized documentation practices, and development of compliance metrics. A signed copy of your revised corrective action plan should be included in your response to this Warning Letter.



(b) On November 8, 2004, FDA granted a waiver to your firm allowing for serious and unexpected suspected adverse drug reactions for NDA 11-839 (Provera and medroxyprogesterone acetate) to be submitted no later than 30 calendar days of initial receipt of the information, instead of within 15 calendar days of receipt of the information. However, between June 8, 2005 and March 16, 2009, your firm failed to submit approximately 25 reports within 30 days. The following are examples of these late reports:

 



















 Mfg. Report No.No. of Days Late
1.20092302891720
2.2008151639128
3.20092004931641



The response comments addressed for item 3(a) also apply to this point.



(c) On August 28, 2006, FDA granted a waiver to your firm allowing for serious and unexpected suspected adverse drug reactions for Bextra (valdecoxib) to be submitted no later than 60 calendar days of initial receipt of the information, instead of within 15 calendar days of receipt of the information. The firm, however, failed to submit approximately 220 of these reports within 60 days. The following are examples of the late reports:

 

 



























 Mfg. report No.No. of Days Late
1.2006153496264
2.2006134600219
3.2007046238140
4.200700247190
5.2007098335139



The response comments addressed for item 3(a) also apply to this point.



4. Failure to submit a 15-day Alert report for adverse drug experiences obtained from postmarketing studies in which the applicant concludes that there is a reasonable possibility that the drug caused the adverse experience, as required by 21 CFR 314.80(e)(1). Specifically:



Fifteen-day Alert reports have not been submitted for all adverse drug experiences during postmarketing studies where there is a reasonable possibility that the drug caused the adverse experience. In your firm's letter dated March 18, 2008, your firm committed to submit 15-day Alert reports for Selzentry (Maraviroc) for the following events during the postmarketing period: liver-related deaths and liver failure, fatal and non-fatal myocardial infarctions, and all non-AIDS defining malignancies. The following ADE reports for Selzentry (Maraviroc) from postmarketing studies were required to be submitted to FDA as 15-day Alert reports, because they either met these criteria described in the March 18, 2008 letter, or they otherwise contain serious and unexpected events in which there is a reasonable possibility that the drug caused the event.

 

 



























 Mfg. Report No.
1.2009154994
2.2009187951
3.2007067649
4.2007076241
5.2005162672
6.2006136607
7.2008003965



Your response has been reviewed and found inadequate. In a letter to the Agency dated March 18, 2008, your firm acknowledged expedited 15-day reporting for liver-related deaths, liver failure, fatal and non-fatal myocardial infarctions and all non-AIDS defining malignancies from spontaneous and clinical trial sources. No reasons for late submission of reports 2006136607 and 2008003965 were provided in your response. Your response states that reports 2009154994, 2009187951, and 2005162672 were incorrectly not submitted due to errors in distribution. Your response further states that reports 2007067649 and 2007076241 were not submitted because they were received by the firm before clarification from the Agency advising that clinical trial cases were subject to special reporting requirements. However, after receipt of clarification that cases 2007067649 and 2007076241 were subject to reporting, your firm did not submit them to the Agency.



5. Serious and unexpected ADE reports are not promptly investigated as required by 21 CFR 314.80(c)(1)(ii). Specifically:



Adverse drug experiences that were the subject of postmarketing 15-day Alert reports were not investigated and/or documented. Specifically, in your firm's letter dated August 18, 2005, your firm submitted revised procedures to investigate all cases of postmarketing ophthalmologic ADEs that might reflect NAION involving Viagra. Your firm committed in these procedures to submit a pre-specified list of questions to reporters in order to obtain clinical and diagnostic information concerning visual symptoms and risk factors for the event. However, in cases reviewed during the inspection, your firm failed to provide documentation that adequate follow-up information had been requested. In addition, during the inspection, it was observed that some reports were either misclassified or downgraded in severity to non-serious without a reasonable justification.



Your response acknowledges that documentation of follow-up calls and the use of the questions during the calls were not handled consistently. Although the FDA does not mandate a particular method of requesting follow-up information, documentation that all postmarketing ophthalmologic events that might reflect NAION were investigated should be maintained.



6. Failure to submit 15-day Alert reports for serious adverse drug experiences as a non-applicant to the applicant within 5 calendar days of receipt as required by 21 CFR 314.80(c)(1) (iii).



Pfizer, as a non-applicant, elected to submit to the applicant (rather than to FDA) all reports of serious adverse drug experiences. However, you did not submit each report to the applicant within five calendar days of your receipt of the information.



Specifically, your firm's name is on the label of at least ten products (amoxicillin, finasteride, ondansetron, lamotrigine, metformin, penicillin V potassium, stavudine, tiotropium bromide, donepezil, interferon beta-la) for which you are required to submit serious ADE reports to the applicant within five calendar days. Of the 398 reports received by your firm for these products, 132 (33%) were sent to the applicants more than five calendar days after your receipt of them.



Your response acknowledged a need to improve on the timeliness of your submission of serious ADE reports to the applicants for products for which Pfizer does not hold the NDA or ANDA, but appears on the label as a distributor. Your response stated that activities such as targeted training and presentations have resulted in reporting timeframe improvement. However, a review of the overall time reporting for 5-day rule products in a time table provided to the investigators on July 9, 2009, for the period from December 8, 2008 to June 30, 2009, shows the contrary. As demonstrated by your report compiled for inspection entitled "5-Day Rule Products Sent to License Party between 08 Dec 2008 and 30 Jun 2009", there was a decline in the timeliness of reporting during this period.



7. Failure to promptly review all adverse drug experience information obtained or otherwise received by the applicant from any source as required by 21 CFR 314.80(b). Specifically:



Adverse drug experience information obtained or otherwise received from any source was not promptly reviewed, including information from commercial marketing experience and postmarketing epidemiological/surveillance activities.



The following are examples of serious ADEs that wvere not forwarded for case processing within 2-4 business days as required by your SOP AEM-01-02, dated July 14, 2008, pages 3 - 5:

 

















 Mfg. Report No.No. of Days Received Late
1.200920290430
2.20081508539



Your response provided an explanation for the lateness of these reports and stated that the firm has "robust quality processes in place to oversee performance ..." This response is deemed inadequate because your affiliates failed to comply with defined time fines for case processing as required by SOP AEM-01.



Your response commits the firm to implement "additional enhancements to tools enabling enhanced proactive management of case workload" to mitigate late reporting. A signed copy of your revised corrective action plan should be included in your response to this Warning Letter. Adequacy of the corrective action will be determined during subsequent inspection(s).



8. Failure to submit periodic adverse drug experience reports at quarterly intervals for each adverse drug experience which is not reported as a I5-day Alert report, for 3 years from the date of approval of the application, and then at annual intervals submitted within 60 days of the anniversary date of approval of the application as required by 21 CFR 314.80(c)(2). Specifically:



Individual ADEs which were not reported to FDA in a postmarketing IS-day Alert report have not been included in a periodic safety report.



Specifically, the following ADEs were not reported to FDA in a periodic safety report:

 

 






























 Mfg. Report No.
1.2009189370
2.2009205745
3.2009206342
4.2009211979
5.2009178032
6.2009186019
7.2009152113
8.2009166186



Your response to this observation reports a short term corrective action of nightly sweeps of the (b)(4) System with a permanent system correction to be implemented by the fourth quarter of 2009. Adequacy of the corrective action will be determined during subsequent follow-up inspection(s).



II. Deviations from 21 U.S.C. § 353(d) include the following:



In addition to the above violations of Postmarketing Adverse Drug Experience (PADE) reporting requirements, you have significant deviations from the requirements of Section 503(d) of the Federal Food, Drug, and Cosmetic Act (the Act) [21 U.S.C. § 353(d)] and Title 21, Code of Federal Regulations, Part 203. Based on the information collected during the inspection, non-compliance with the requirements of the Prescription Drug Marketing Act (PDMA), include:



1. Failure to conduct an immediate investigation, to notify FDA within 5 working days, and provide written investigation reports within 30 days of initial notification of prescription drug sample thefts, significant losses, and falsification of prescription drug sample records as required by 21 CFR 203.37(a)(1),(2), and (3) and (b)(1), (2), and (3).



21 CFR 203.37(a)(1) and (b)(1) requires a manufacturer or authorized distributor of record to notify FDA within five working days of becoming aware of a significant loss, any known theft, or suspected falsification involving drug samples. 21 CFR 203.37(a)(2) and (b)(2) requires an immediate initiation of an investigation of a suspected significant loss, any known theft, or suspected falsification. 21 CFR 203.37(a)(3) and (b)(3) requires that FDA be provided with a complete written report, including the reason for and the results of the investigation, not later than 30 days after the date of the initial notification.



The FDA 483 observations concern Pfizer's failure to notify and follow up with FDA regarding significant losses, known thefts, or suspected falsifications in accordance with these PDMA legal requirements. Pfizer's response to the FDA 483 in this regard does not address how Pfizer will meet the Section 203.37 requirements. We recognize your intent to reduce the inventory period, but the reduction you describe would still not meet the five working day reporting requirement.



Examples of incidents of significant losses and confirmed variances in drug sample annual inventory reconciliation re orts that exceeded the established threshold for significant loss in Pfizer's SOP 010 (b)(4) that were not reported to FDA are as follows:



• Employee ID (b)(6) had a total inventory loss of approximately (b)(4) on July 17, 2009. At the time of inspection, FDA had not been notified.



• Employee ID (b)(6) had a possible theft of (b)(4) totaling a loss of (b)(4) on March 11, 2008. A police report was filed on May 13, 2008, yet Pfizer did not notify FDA until May 30, 2008.



• Employee ID (b)(6) had a variance of (b)(4) on Aug 19, 2008. FDA was not notified until approximately two months later.



2. Failure to conduct, at least annually, a complete and accurate physical inventory of all drug samples distributed and to record the results of such inventory as required by 21 CFR 203.31(d).



21 CFR 203.31 (d) requires that each drug manufacturer or authorized distributor of record that distributes drug samples by means of representatives shall conduct, at least annually, a complete and accurate physical inventory of all drug samples. All drug samples in the possession or control of each manufacturer's and distributor's representatives are required to be inventoried and the results of the inventory are required to be recorded in an inventory record. In addition, manufacturers and distributors shall reconcile the results of the physical inventory with the most recently completed prior physical inventory and create a report documenting the reconciliation process.



Annual inventory reconciliations are not conducted once a year as per your SOP 010. Specifically, out of 35 inventories reviewed by FDA, the following employees did not have their inventories taken annually:















































Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)
Employee(b)(6)



Your response relays the intent to revise SOP 010 to assure that all future employee inventories are performed within 12 months from the initial inventory review rather than once each calendar year. However, we have not yet received your revised SOP and you have not addressed the status of inventories for the above employees. Therefore, the adequacy of your response cannot be determined.



The violations cited in this letter are not intended to be an all-inclusive statement of violations that exist at your firm. You are responsible for investigating and determining the causes of the violations identified above and for preventing their recurrence or the occurrence of other violations. It is your responsibility to assure that your firm complies with all requirements of federal law and FDA regulations.



You should take prompt action to correct the violations cited in this letter. Failure to promptly correct these violations may result in legal action without further notice, including, without limitation, prosecution or injunction. Other federal agencies may take this Warning Letter into account when considering the award of contracts. Additionally, FDA may withhold approval of requests for export certificates, or approval of pending new drug applications, listing your facility as a supplier or manufacturer until the above violations are corrected. A reinspection may be necessary.

You should notify this office upon receipt of this letter to arrange for a meeting to discuss the specific steps you have taken to correct the noted violations, including an explanation of each step being taken to prevent the recurrence of similar violations. If corrective action cannot be completed within 15 working days, state the reason for delay and the time within which corrections will be completed.



Your reply should be sent to Compliance Branch, Food and Drug Administration, 158-15 Liberty Avenue, Jamaica, NY 11433 Attention: Lillian C. Aveta, Compliance Officer.



Sincerely,

/S/

Ronald M. Pace

District Director

New York District

 



1 The Milan office, which is one of the core DSS offices, was not trained until July 2009.



Enclosure: Form FDA 483 dated August 10, 2009

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Tuesday, May 25, 2010

Tom Schantz Farm (d/b/a Riverview Dale Farm) 5/25/10

  

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

Public Health Service
Food and Drug Administration
 

New York District
Food & Drug Administration
158-15 Liberty Avenue
Jamaica, New York 11433-1034

 

May 25, 2010

WARNING LETTER NYK 2010-17

VIA UNITED PARCEL SERVICE

Andrew T. Schantz, Farm Manager
Thomas Schantz Farm
d/b/a Riverview Dale Farm
8841 Van Amber Road
Castorland, New York 13620

Dear Mr. Schantz:

On February 10-12, 2010, the U.S. Food and Drug Administration (FDA) conducted an investigation of your dairy farm located at 8841 Van Amber Road, Castorland, NewYork. This letter notifies you of the violations of the Federal Food, Drug, and Cosmetic Act (the Act) that we found during our investigation of your operation. You can find the Act and its associated regulations on the Internet through links on the FDA's web page at www.fda.gov.

We found that you offered an animal for sale for slaughter as food that was adulterated. Under section 402(a)(2)(C)(ii) of the Act, 21 U.S.C. § 342(a)(2)(C)(ii), a food is deemed to be adulterated if it bears or contains a new animal drug that is unsafe under section 512 of the Act, 21 U.S.C. § 360b. Further, under section 402(a)(4) of the Act, 21 U.S.C. § 342(a)(4), a food is deemed to be adulterated if it has been held under insanitary conditions whereby it may have been rendered injurious to health.

Specifically, our investigation revealed that on or about August 6, 2009, you shipped a dairy cow, identified with tag (b)(4) to an auction house, (b)(4). This dairy cow was subsequentiy slaughtered for human food on or about August 7, 2009, at (b)(4). United States Department of Agriculture, Food Safety and Inspection Service (USDA/FSIS) analysis of tissue samples collected from this animal identified the presence of phenylbutazone in the kidney at 8888.0 parts per million (ppm). FDA has not established a tolerance for phenylbutazone in animals intended for human consumption, and its use is prohibited from extralabel use in female dairy cattle 20 months of age, or older as codified in Title 21, Code of Federal Regulations (C.F.R.), 530.41(a)(12) [21 CFR 530.41(a)(12)]. The presence of this drug in tissue of this animal causes the food to be adulterated within the meaning of section 402(a)(2)(C)(ii) of the Act, 21 U.S.C. § 342(a)(2)(C)(ii).

Our investigation also found that you hold animals under conditions that are so inadequate that medicated animals bearing potentially harmful drug residues are likely to enter the food supply. For example, you failed to maintain treatment records. Food from animals held under such conditions is adulterated within the meaning of section 402(a)(4) of the Act, 21 U.S.C. § 342(a)(4).

We also found that you adulterated the new animal drugs Phenylbute Injection 20% (Phenylbutazone), ANADA 200-371 and Penicillin G Procaine Injectable Suspension USP, NADA 65-010. Specifically, our investigation revealed that you did not use phenylbutazone and penicillin G procaine as directed by their approved labeling. Use of these drugs in this matter is an extralabel use as defined in 21 C.F.R. 530.3(a).

The extralabel use of approved animal or human drugs in animals is allowed under the Act only if the extralabel use complies with sections 512(a)(4) and (5) of the Act, 21 U.S.C. § 360b(a)(4) and (5), and 21 C.F.R. Part 530, including that the use must be by or on the lawful order of a licensed veterinarian within the context of a valid veterinarian/client/patient relationship.

Our investigation found that you administered phenylbutazone to a female dairy cow approximately 58 months old without following the animal species as stated in the approved labeling. Phenylbutazone is prohibited for extralabel use in female dairy cattle 20 months or older by 21 CFR, Part 530.41(a)(12) and your extralabel use of phenylbutazone resulted in an illegal drug residue, in violation of 21 C.F.R. 530.11(c). Our investigation also found that you administered penicillin G procaine to a dairy cow without following the conditions of use stated in the approved labeling. Your extralabel use of penicillin G procaine was not under the supervision of a licensed veterinarian, in violation of 21 C.F.R. 530.11(a). Because your use of these drugs were not in conformance with their approved labeling and did not comply with 21 C.F.R., Part 530, you caused the drugs to be unsafe under section 512(a) of the Act, 21 U.S.C.§ 360b(a), and adulterated within the meaning of section 501(a)(5) of the Act, 21 U.S.C. § 351(a)(5).

The above is not intended to be an all-inclusive list of violations. As a producer of animals offered for use as food, you are responsible for ensuring that your overall operation and the food you distribute is in compliance with the law.

You should take prompt action to correct the violations described in this letter and to establish procedures to ensure that these violations do not recur. Failure to do so may result in regulatory action without further notice such as seizure and/or injunction.

In your signed affidavit dated February 10, 2010, you stated it has been your practice to feed all of your calves, including bull calves intended for slaughter, a medicated milk replacer containing the drugs neomycin and oxytetracycline. You further stated, the medicated milk replacer you use has a thirty (30) day withdrawal for meat and you have been feeding this milk replacer for years without holding the calves for the thirty (30) day withholding time. Not following the appropriate withdrawal time for a drug product (medicated feed) constitutes extralabel use. The extralabel use of an approved new animal drug (neomycin and oxytetracycline) in or on an animal feed (milk replacer) is not permitted in accordance with 21 C.F.R. 530.11(b).

You should notify this office in writing of the steps you have taken to bring your firm into compliance with the law within fifteen (15) working days of receiving this letter. Your response should include each step that has been taken or will be taken to correct the violations and prevent their recurrence. If corrective action cannot be completed within fifteen (15) working days, state the reason for the delay and the time frame within which the corrections will be completed. Please include copies of any available documentation demonstrating that corrections have been made.

Your written response should be sent to Patricia A. Clark, Compliance Officer, U.S. Food and Drug Administration, 300 Pearl Street, Suite 100, Buffalo, New York 14202. If you have any questions about this letter, please contact Compliance Officer Patricia A. Clark at 716-551-4461, extension 3168.

Sincerely yours,

/s/

Ronald M. Pace
District Director
NewYork District

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