Mayne Pharma Pty., Ltd. 21-Nov-02

Departmentof Health and Human Services            PublicHealth Service

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Food and Drug Administration
Rockville, MD 20857

Warning Letter

WL: 320-02-01

November 21, 2002

Mr. Alexander B. Bell

Vice President Technical Operations

Mayne Pharma Pty., Ltd.

1-23 Lexia Place

Mulgrave North, Melbourne, VIC 3170

Australia

Dear Mr. Bell,

This letter is in response to an inspection of your pharmaceutical manufacturingfacility in Melbourne, Australia, by the United States Food and Drug Administration(FDA) on, April 8-16, 2002. This inspection revealed significant deviationsTom U.S. Current. Good Manufacturing Practices (CGMP) Regulations (Title 21CFR, Parts 210 and 211) in the manufacture of sterile drug products. At thecompletion of this inspection, you were issued a 46-item Inspectional Observations(FDA-483) form. These CGMP deviations cause your drug products to be adulteratedwithin the meaning of section 501(a)(2)(B) of the Federal Food, Drug, and CosmeticAct.

Our review also included your May 21, 2002, August 22, 2002 and October 11,2002 written response letters to the FDA-483 observations. We acknowledge thecommitments to correct the deficiencies; however, the response lacks sufficientdetails, explanations, and documentation to address the deviations observedduring the April 2002 inspection.

In addition, we have the following concerns that include, but are not limited to:

1. In the last two years there were 11 product sterility failures involvingthe organism [redacted]. The investigations into these routine results foundno assignable cause or the sterility failures. Some of the failures involved[redacted] sterilized products that included [redacted]. There were no correctiveactions identified in these investigations and the batches were released onthe basis of the survivor test. [21 CFR 211.192]

The production department conducted no investigations, although the productionsystem could not be ruled out as the potential cause of the product contamination.The response stated that no probable cause was identified in four investigations,i.e., no conclusive evidence that the failure was due to either laboratory orproduction error therefore corrective action could not be documented. In threeinvestigations the most probable cause for the sterility positives was deemedto be laboratory error. Further, you acknowledged at a minimum retraining ofboth production and laboratory staff should have taken place, as a correctiveaction. The response also indicated that extended review of trends for sterilityfailures was not undertaken, but will be considered as a corrective action inany future investigations.

In not addressing probable causes and not initiating corrective actions thefirm failed to identify the cause of the contamination and neglected to insurethat this type of problem would not recur. Furthermore, the drug products thatwere released failed to meet their established standards or specifications andhad no assurance to be free of objectionable microorganisms.

In the three investigations for which the sterility positives were deemed tobe laboratory errors, the investigations failed to identify the type of errorsor relate them to laboratory errors. In these three cases, the firm identifiedthe sterility positives as laboratory errors only because the product was [redacted]sterilized. The firm failed to implement any corrective actions to insure thatthe laboratory errors would not occur in the future.

2. The test methods used for sterility testing are inadequate. [21 CFR 2 11.165]There is a lack of data to demonstrate that the methods are capable of recoveringlow levels of organisms that would be found in a typical non-sterile drug product.The study summaries and raw data lacked any counts for the inoculated controlsand samples, and there is insufficient data to interpret whether the productinhibits growth of organisms. The reproducibility of the method was not demonstrated.For example, only one result following a negative recovery was used to validatethe [redacted] Method.

It was also noted that you have not completed [redacted]

Validation for 7 of 15 products with [redacted]

In the August 22, 2002 response, it states that the methodology complies withthe requirements of USP Sterility Test [redacted] Validation for [redacted].It clarified that the counts used to initially inoculate the test and controlsamples are quantified, but you don?t explain how the procedure is done. Italso states that an update to the validation requirement such that three validationtests will be performed in order to comply with the requirements of Validationof [redacted] from Pharmacopeial Articles [redacted].

Further, the response included a commitment to repeating the Validation for [redacted] testing three times for any new formulations/presentations. The validation will be performed twice on existing products the next time the batches are manufactured. As to the products requiring [redacted] inclusion in the validations, this will be scheduled for the next production batches being produced.

Until this validation is completed, the sterility test methods used are inadequatein that there is no documentation, which demonstrates the accuracy and repeatabilityfor [redacted] from Pharmacopeial Articles. Also there is no assurances thatthe sterility positive &Its identified as errors were accurate assessmentsbecause of the inadequacy of the test methods.

3. written procedures designed to prevent microbiological contamination ofsterile drug products were inadequate and resulted in: [21 CFR 211.113]

• inadequate monitoring of differential air pressures between clean rooms


• inadequate support of changes for the movement of walls and HVAC modifications made to the [redacted] facility

• inadequate controls and procedures for gowning


• inadequate validation of the sterilization process in no microbiological qualification or determination of the resistance of the biological indicator challenge system was performed for [redacted]

The responses and commitments made by the firm to correct these deficienciesin item #3 appear adequate. However, this raises concerns about the QualityControl Unit. We remind you of their responsibilities in reviewing and approvingail procedures related to production, quality control, and quality assuranceto assure the procedures are adequate for their intended use.

The CGMP deviations identified above or on the FDA-483 issued to your firmare not to be considered an all-inclusive list of the deficiencies at your facility.FDA inspections are audits, which are not intended to determine all deviationsfrom CGMPs that exist at a firm. If you wish to continue to ship your productsto the United States, it is the responsibility of your firm to assure compliancewith all U.S. standards for Current Good Manufacturing Practices.

Failure to correct these deficiencies may result in FDA denying entry of articlesmanufactured by your firm into the United States. The articles could be subjectto refusal of admission pursuant to Section 801(a)(3) of the Act in that themethods and controls used in their manufacture do not appear to conform to CurrentGood Manufacturing Practices within the meaning of Section 501(a)(2)(b) of theAct.

Please respond to this letter within 30 days and provide documentation regardingcorrections of the above deviations. Your response should include data collectedin your corrections to the deficiencies cited as well as copies of proceduresnot already included.

Please identify your response with CFN 9610999. Until FDA can confirm compliancewith CGMP?s and correction to the most recent inspection deficiencies, thisoffice will recommend disapproval of any new applications listing your firmas the manufacturer of sterile drug products.

Please contact Anthony A. Charity, Compliance Officer, at the address and telephonenumbers shown below, if you have any questions, written response or concernsregarding these decisions:

U.S. Food & Drug Administration

CDER HFD-322

7520 Standish Place

Rockville, MD 20855-2737

Tel: (301) 827-0062; FAX (301) 594-1033

To schedule a re-inspection of your facility, after corrections have been completedand your firm is in compliance with CGMP requirements, send your request to:International Operations Branch, HFC-132, 5600 Fisher?s Lane, Rockville, MD,20857. You can also contact that office by telephone at (301) 827-5655 or byfax at (301) 443-6919.

Sincerely,

/s/

Joseph C. Famulare

Director

Division of Manufacturing and Product Quality

Center for Drug Evaluation and Research

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Youth Light 2010 Inc 18-Nov-02

Departmentof Health and Human Services	Public Health Service Food and Drug Administration
	555 Winderley PI., Ste. 200 Maitland, Fl 32751

VIA CERTIFIED MAIL

WARNING LETTER

FLA-03-10

November 18, 2002

William Donaldson, President
Youth Light 2010, Inc,.
150 E. Sample Road
Pompano Beach, Florida 33064

Dear Mr. Donaldson

We are writing to you because during an inspection of your establishment located in Pompano Beach, Florida on July 10-16, 2002, Food and Drug Administration (FDA) investigators Michelle S. Dunaway and Prince Brown determined that your establishment is a specification developer and distributor of the Youth Light 2010 Intense Pulse Light System. As a specification developer, you are considered to be a manufacturer in accordance with Title 21, Code of Federal Regulations (CFR), Section 807.20(a)(1).

Under a United States law, the Federal Food, Drug, and Cosmetic Act (the Act), the Youth Light 2010 is considered to be a medical device because it is intended to be used to diagnose or treat a medical condition or to affect the structure or function of the body. The law requires that manufacturers of medical devices obtain marketing clearance for their products from the FDA before they may offer them for sale. This helps protect the public heath by ensuring that newly introduced medical devices are safe and effective or substantially equivalent to other devices already legally marketed in this country.

The inspection determined that you promote and distribute the Youth Light 2010 device for structure/function claims including the treatment of wrinkles, lines and folds, age spots and sun damage, coarse skin and large pores, and for the promotion of collagen production.

Our records do not show that you obtained marketing clearance before you began offering your product for safe. The kind of information you need to submit in order to obtain this clearance is described on FDA's medical device website at .http://www.fda.gov/cdrh/devadvice. FDA will evaluate this information and decide whether your product maybe legally marketed

Be cause you do not have marketing clearance from the FDA, marketing your product is a violation of the law. In legal terms, the product is adulterated under section 501(f)(1)(B) and misbranded under section 502(o) of the Act. Your product is misbranded under the Act because you did not submit a section 510(k) premarket notification that shows your device is substantially equivalent to other devices that are legally marketed.

Until you submit a section 510(k) premarket notification and FDA reviews it and notifies you that you may market your device, your product is also adulterated under the Act because the law requires, and you do not have, an approved premarket approval application that shows your device is safe and effective.

The above-stated inspection revealed that the device is adulterated under Section 501(h) of the Act, in that the methods used in, or the facilities or controls used for manufacturing, packing, storage, or installation are not in conformance with the current Good Manufacturing Practice (CGMP) requirements of the Quality System Regulation.

1. Your firm's management with executive responsibility failed to establish its policy and objectives for, and commitment to, quality as required by 21 CFR 820.20(a),(c), and (e). For example, you do not have any written procedures documenting any of your firm's management activities and no quality audits or management reviews have been conducted (FDA 483, Item #11, 2, and 13).

2. Your firm failed to establish procedures for quality audits and to conduct such audits to assure that the quality system is in compliance with the established quality system requirements and to determine the effectiveness of the quality system as required by 21 CFR 820.22. For example, no quality audits have been conducted and none are scheduled to assure the quality system is effective (FDA 483, Item #12).

3. Your firm failed to establish and maintain procedures to control the design of the device in order to ensure that specified requirements are met as required by 21 CFR 820.30 (f),(g), and (j). For example, no design verification confirmed that the design outputs meet design input requirements, design validation did not ensure that devices conform to defined user/patient needs and intended uses, and a design history file was not established or maintained.(FDA 483, Item #s 8,9, and 10).

4. Your firm failed to maintain records of complaint investigations by a formally designated unit as required by 21 CFR 820.198(e). Your firm received several complaints that were not documented (FDA 483, Item #11).

5. Your firm failed to establish and maintain device master records (DMRs)which include specifications (appropriate drawings composition, and/or component specifications), for maintenance and service of equipment, for production or process operations, for quality assurance, for packaging and labeling operations, and the DMR does not include or refer to the location of these records as required by 21 CFR 820.181 (a), (b), (c), and (d). For example, there are no production and process procedures/specifications, no quality assurance procedures/specifications, no packaging and labeling procedures, and there was no reference as to where these records are maintained (FDA 483, Item #s 3, 4; 5, 6, and 7).

This letter is not intended to be an all-inclusive list of deficiencies at your facility. It is your responsibility to ensure adherence to each requirement of the Act and regulations. Mr. William Chappie promised to respond in writing documenting corrective actions taken covering the observed deviations listed on the Inspectional Observations (FDA 483) and verifying that distribution of the device had been discontinued. As of this date, no response has been received.

You should know that this serious violation of the law may result in FDA taking regulatory action without further notice to you. These actions include, but are not limited to, seizing your product inventory, obtaining a court injunction against further marketing of the product, or assessing civil money penalties. Also, Federal agencies are informed about the Warning Letters we issue, such as this one, so that they may consider this information when awarding government contracts. Additionally, no requests for Certificates for Products for Export will be approved until the violations related to the subject devices have been corrected.

It is necessary to take action on this matter now. Please let this office know what steps you have taken to correct the problem within fifteen (15) working days from the date you received this letter, including: (1) the time frames within which the corrections will be completed, (2) any documentation indicating the corrections have been achieved, and (3) an explanation of each step being taken to identify and make corrections to any underlying systems problems necessary to assure that similar violations will not recur. Please adviseyour intentions to cease distribute. If you need more time, let us know why and when you expect to complete your correction. Please direct your response to Mr. Timothy J. Couzins, Compliance Officer, Food and Drug Administration, 555 Winderley Place, Suite 200, Maitland, Florida 32751, (407) 75-4728.

 

Sincerely,

/s/

 

Emma Singleton
Director, Florida District

 

 

 

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