throbber
CENTER FOR DRUG EVALUATION AND RESEARCH
`
`Approval Package for:
`
`Application Number: 021083
`
`Trade Name: RAPAMUNE ORAL SOLUTION 1mg/mL
`
`Generic Name: SIROLIMUS
`
`Sponsor: WYETH—AYERST RESEARCH
`
`Approval Date: 09/15/99
`
`INDICATION§s): PROPHYLAXIS OF ORGAN
`
`REJECTION IN PATIENTS RECEIVING RENAL
`
`TRANSPLANTS
`
`est-Ward Pharm.
`Exhibit 1008
`Page 001
`
`West-Ward Pharm.
`Exhibit 1008
`Page 001
`
`

`

`CENTER FOR DRUG EVALUATION AND RESEARCH
`
`APPLICATION: 021083
`
`CONTENTS
`
`Included
`
`Pending
`Completion
`
`Not
`Not
`Pregared Reguired
`
`Apgroval Letter
`Tenative Apgroval Letter
`Aggrovable Letter
`Printed Labeling
`Medical Reviewgsg
`Chemist1_'y Reviewjsg
`EA/FONSI
`
`Pharmacology Reviewgs!
`Statistical Reviewgsg
`Microbiology Reviews}
`Clinical Pharmacology
`Biogharmaceutics Reviewg s g
`Bioeguivalence Reviewgsg
`Administrative/
`
`X
`
`><><><><><><><
`
`Correspondence Documentgsg
`
`X
`
`P
`
`X
`>4
`
`X
`
`X
`
`West-Ward Pharm.
`Exhibit 1008
`Page 002
`
`West-Ward Pharm.
`Exhibit 1008
`Page 002
`
`

`

`CENTER FOR DRUG EVALUATION AND RESEARCH
`
`Application Number: 021083
`
`APPROVAL LETTER
`
`West Ward Pharm.
`Exhibit 1008
`Page 003
`
`West-Ward Pharm.
`Exhibit 1008
`Page 003
`
`

`

`NDA 2l-083
`
`Wyeth-Ayerst Research
`Attention: Maureen Skowronek
`Director, U.S. Regulatory Afiairs
`, P.O. Box 8299
`Philadelphia, PA 19101-8299
`
`Dear Ms. Skowronek:
`
`SEPl5'999
`
`Please refer to your new drug application (NDA), dated and received on December 15, 1998,
`submitted under section 505(b) ofthe Federal Food, Drug, and Cosmetic Act for Rapamune®
`(sirolirnus) Oral Solution, lmg/mL.
`.
`
`We acknowledge receipt of your submissions dated:
`
`January 6, 1999
`January 14,1999
`February 17, 1999 .
`February 19, 1999
`March ll, 1999
`March 15, 1999
`March 17, 1999
`' March 22, 1999
`March 23, 1999
`March 29, 1999
`March 31, 1999
`April 1, 1999
`April 8, 1999(2)
`
`April 12, 1999
`April 13, 1999
`, April 15, 1999
`April 21, 1999
`April 26,1999
`April 28, 1999
`April 29, 1999
`April 30, 1999
`May 4, 1999
`May 7, 1999
`May 13, 1999
`May 17, 1999
`May 21, 1999
`
`May 24, 1999 ~
`_ May 26, 1999
`May 28, 1999(2)
`June 1, I999
`June 4, 1999
`June 10, 1999
`June 11, 1999.
`June 14, 1999(2)
`June 18, 1999
`June 21, 1999
`June 25, 1999
`June 29, 1999
`July 9, 1999
`
`July 13, 1999
`July 14,- 1999
`July 28, 1999
`August 5, 1999
`August 6, 1999(3)
`August 9, 1999
`August 17, 1999
`August 19, 1999
`August 24, 1999(4)
`August 25, 1999 (2)
`August 30, 1999
`September 9, 1999
`'- September 14, 1999
`
`This new drug application provides for the use of Rapamune® (sirolimus) Oral “Solution for the
`prophylaxis of organ rejection in patients receiving renal transplants.
`
`We have completed the review ofthis application, as amended, and have concluded that adequate
`information has been presented to demonstrate that the drug product issafe and effective for use
`as recommended in the agreed upon labeling text. Accordingly, the application is approved
`efi"ective on the date of this letter.
`
`The frnalprinted labeling (FPL) must be identical to the package insert submitted September 14,
`1999, the patient package insert submitted September 14, 1999, and the irrunediate container and
`carton labels submitted August 5, 1999. Marketing the product with FPL that is not identical to
`the approved labeling text may render the product misbranded and an unapproved new drug.
`
`Please submit 20 copies ofthe FPL as soon as it is available, in no case more than 30 days afier it
`is printed. Individually mount ten of the copies on heavy-weight paper or similar material. For
`administrative purposes, this_ submission should be designated “FPL for approved NDA 21-083.”
`, Approval of this submission by FDA is not required before the labeling is used.
`’
`
`est-Ward Pharm.
`Exhibit 1008
`Page 004
`
`West-Ward Pharm.
`Exhibit 1008
`Page 004
`
`

`

`NDA 21-083
`
`Page 2
`
`We remind you of your Phase 4 commitments specified in your submission dated August 30,
`1999. These commitments, along with any completion dates agreed upon, are listed below.
`
`Clinical
`
`1.
`
`In order to evaluate the optimal dose of sirolimus in renal transplant patients, who are
`at high risk for acute rejection, you agree to conduct a well-controlled, comparative
`study or studies,'to fiirther define the optimal dose or concentration in this population.
`Patients from any or all ofthe following groups might be included:
`
`0 Black patients
`0 Patients with retransplants.
`0 Patients with high panel-reactive antibodies.
`0 Patients with greater than or equal to 4 human leukocyte antigen mismatches.
`0 Patients with multiorgan (kidney-pancreas) transplants.
`
`You will conduct an appropriate study or studies to better define the type and duration
`of hyperlipidemia associated with the use of sirolimus. In particular, you will measure
`and analyze total fasting serum cholesterol and triglycerides, as well as high-density
`lipids/low-density lipids, and lipoprotein A. Transplant recipients with and without a
`lipid disorder prior to transplant will be included, and the use of lipid-lowering agents
`and other specific interventions will be evaluated.
`
`You will create a registry for collecting safety data on pregnancies that occur during the
`use of Rapamune®.
`
`You will collect and report long-term follow-up safety and efficacy data from the
`ongoing Phase 3 studies, studies 30] and 302. Data pertaining to glomerular filtration
`rate (GFR) and serum creatinine will be included as follow-up information. These data
`should be collected throughout the entire duration of the study whether or not patients
`remain on study drug. Please note that study 301 is a 2-year study and study 302 is a 3-
`year study.
`
`As part of the continuing development of sirolimus, you will assess its efiect on long-
`tenn renal function using GFR in patients receiving kidney or other solid organ
`transplants.
`
`In your ongoing and future studies of sirolimus, you will evaluate the impact ofthis
`drug on liver function tests in recipients of kidney or liver transplants who may have
`hepatitis B virus and/or hepatitis C virus infection.
`
`Clinical Pharmacology
`
`7.
`
`In a crossover study with healthy volunteers, you will evaluate the drug-drug
`interaction potential of sirolimus when co-administered with SangCya® and
`Sandimmune®. Furthermore, you will evaluate the various administration times of
`sirolimus and cyclosporine (Neoral®), in order to determine the magnitude of the
`sirolimus concentration increase when patients do not take sirolimus 4 hours afier the
`cyclosporine dose.
`
`West Ward Pharm.
`Exhibit 1008
`Page 005
`
`West-Ward Pharm.
`Exhibit 1008
`Page 005
`
`

`

`NDA 21-083
`
`Page 3
`
`8.
`
`You will evaluate the optimum therapeutic concentration range for sirolimus and the
`value of reduced cyclosporine concentrations in combination with sirolimus. You will
`employ therapeutic drug monitoring and logistic regression modeling in both high- and
`low-risk patients.
`
`,
`
`You will evaluate the sirolimus-erythromycin pharmacokinetic interaction in a
`crossover study with healthy volunteers.
`
`10.
`
`11.
`
`You will conduct a study or studies to evaluate the effect of ethnicity on the
`pharmacokinetics of sirolimusso as to facilitate the determination of the optimum
`dosing regimen among other ethnic origins. Such a determination will be made using a
`population pharmacokinetics analysis, preferably using mixed effects modeling.
`
`You will evaluate the interactions between sirolimus and verapamil.
`
`Preclinical
`
`12.
`
`13.
`
`14.
`
`15.
`
`You will submit the report for the second carcinogenicity
`upon issuance. This is projected for the first quarter of 2000.
`
`mice to the Agency
`
`In order to qualify the degradation product WAY-126792 (seco-rapamycin), you will
`conduct the following studies: a 3-month study in monkeys, a segment I] reproductive
`study, the standard ICH battery of genotoxicity assays, and studies to further evaluate
`the irnmunosuppressive activity of seco-rapamycin.
`
`You will conduct a combination study with sirolimus and cyclosporine that will
`incorporate physiologic ‘and morphologic parameters of nephrotoxicity and a recovery
`period.
`'
`
`a) You will provide us with the data published in the literature and/or data generated
`from additional studies to better define the efi'ect of the p-glycoprotein efilux system on
`sirolimus pharmacokinetics.
`
`b) Studies are ongoing using a subclone of the human intestinal Caco-2 cell line with
`induced CYP3A4 activity to examine the combined effects of metabolism and efilux on
`sirolimus disposition. To gain a better understanding of the roles of intestinal
`metabolism and efflux, you agree to complete this in vitro study and submit the data for
`our review.
`
`Protocols, data, and final reports should be submitted to your MD for this product and a copy of
`the cover letter sent to this NDA. Ifan IND is not required to meet your Phase 4 commitments,
`please submit protocols, data, and final reports to this NDA as correspondence. In addition, as
`per 21 CFR 314.82(b)(2)(vii), we request that you include a status summary of each commitment
`in your annual report to this NDA. The status summary should include the number of patients
`entered in each study, expected completion and submission dates, and any changes in plans since
`the last annual report. For administrative purposes, all submissions, including labeling
`supplements, relating to these Phase 4 commitments must be clearly designated “Phase 4
`Commitments.”
`
`est-Ward Pharm.
`Exhibit 1008
`Page 006
`
`West-Ward Pharm.
`Exhibit 1008
`Page 006
`
`

`

`of the Center not to withhold approval because the methods are being validated. Nevertheless,
`we expect your continued cooperation to resolve any problems that may be identified.
`
`Be advised that, as of April 1, 1999, all applications for new active ingredients, new dosage
`forms, new indications, new routes of administration, and new dosing regimens are required to
`contain an assessment ofthe safety and efieetiveness ofthe product in pediatric patients unless
`this requirement is waived or deferred (63 FR 66632). We note that you have not fulfilled the
`requirements of 21 CFR 314.55. We are deferring submission of your pediatric studies until
`December 31, 2004. However, in the interim, please submit your pediatric drug development
`plans within 120 days from the date ofthis letter unless you believe a waiver is appropriate.
`
`Ifyou believe that this drug qualifies for a waiver of the pediatric study requirements, you should
`submit a request for a waiver with supporting information and documentation in accordance with
`the provisions of 21 CFR 314.55 within 60 days from the date ofthis letter. We will notify you
`within 120 days of receipt ofyour response whether a waiver is granted. If a waiver is not
`granted, we will ask you to submit your pediatric drug development plans within 120 days from
`the date of denial of the waiver.
`
`Pediatric studies conducted under the terms of section 505A ofthe Federal Food, Drug, and
`Cosmetic Act may result in additional marketing exclusivity for certain products (pediatric
`exclusivity). FDA does not necessarily ask a sponsor to complete the same scope of studies to
`qualify for pediatric exclusivity as it does to fulfill the requirements ofthe pediatric rule
`
`We remind you that you must comply with the requirements for an approved NDA set forth under
`21 CFR 314.80 and 314.81.
`
`-
`
`In addition, once the package insert has been finalized, please submit three copies ofthe
`introductory promotional materials that you propose to use for this/these product(s). All proposed
`materials should be submitted in draft or mock-up form, not final print. Please send one copy to
`the Division of Special Pathogen and Immunologic Drug Products and two copies of both the
`promotional materials and the package insert(s) directly to:
`
`Division of Drug Marketing, Advertising,
`and Communications, HFD-40
`Food and Drug Administration
`5600 Fishers Lane
`
`Rockville, Maryland 20857
`
`Please submit one market package of the drug product when it is available.
`
`If you have any questions, contact Matthew A. Bacho, Regulatory Project Manager at (301) 827-
`2127.
`
` /S/
`
`.
`
`. w er, M.
`Acting Director
`Ofiice of Drug Evaluation IV
`Center for Drug Evaluation and Research
`
`West Ward Pharm.
`Exhibit 1008
`Page 007
`
`West-Ward Pharm.
`Exhibit 1008
`Page 007
`
`

This document is available on Docket Alarm but you must sign up to view it.


Or .

Accessing this document will incur an additional charge of $.

After purchase, you can access this document again without charge.

Accept $ Charge
throbber

Still Working On It

This document is taking longer than usual to download. This can happen if we need to contact the court directly to obtain the document and their servers are running slowly.

Give it another minute or two to complete, and then try the refresh button.

throbber

A few More Minutes ... Still Working

It can take up to 5 minutes for us to download a document if the court servers are running slowly.

Thank you for your continued patience.

This document could not be displayed.

We could not find this document within its docket. Please go back to the docket page and check the link. If that does not work, go back to the docket and refresh it to pull the newest information.

Your account does not support viewing this document.

You need a Paid Account to view this document. Click here to change your account type.

Your account does not support viewing this document.

Set your membership status to view this document.

With a Docket Alarm membership, you'll get a whole lot more, including:

  • Up-to-date information for this case.
  • Email alerts whenever there is an update.
  • Full text search for other cases.
  • Get email alerts whenever a new case matches your search.

Become a Member

One Moment Please

The filing “” is large (MB) and is being downloaded.

Please refresh this page in a few minutes to see if the filing has been downloaded. The filing will also be emailed to you when the download completes.

Your document is on its way!

If you do not receive the document in five minutes, contact support at support@docketalarm.com.

Sealed Document

We are unable to display this document, it may be under a court ordered seal.

If you have proper credentials to access the file, you may proceed directly to the court's system using your government issued username and password.


Access Government Site

We are redirecting you
to a mobile optimized page.





Document Unreadable or Corrupt

Refresh this Document
Go to the Docket

We are unable to display this document.

Refresh this Document
Go to the Docket