1 / 65

Preventing OOS Deficiencies

Preventing OOS Deficiencies. Lynn Torbeck. List of Topics. Briefly review: Barr Case FDA OOS Guidance Able Laboratories Story PDA Scientific Advisory Board Committees Troublesome fundamentals Unresolved issues Preventing OOS deficiencies Final recommendations. Barr Case.

Faraday
Download Presentation

Preventing OOS Deficiencies

An Image/Link below is provided (as is) to download presentation Download Policy: Content on the Website is provided to you AS IS for your information and personal use and may not be sold / licensed / shared on other websites without getting consent from its author. Content is provided to you AS IS for your information and personal use only. Download presentation by click this link. While downloading, if for some reason you are not able to download a presentation, the publisher may have deleted the file from their server. During download, if you can't get a presentation, the file might be deleted by the publisher.

E N D

Presentation Transcript


  1. Preventing OOS Deficiencies Lynn Torbeck Preventing OOS Deficiencies

  2. List of Topics • Briefly review: • Barr Case • FDA OOS Guidance • Able Laboratories Story • PDA Scientific Advisory Board Committees • Troublesome fundamentals • Unresolved issues • Preventing OOS deficiencies • Final recommendations Preventing OOS Deficiencies

  3. Barr Case • Audited in 1989, 1991 and 1992. • Refused to accept a consent decree. • FDA was forced to go to court. • Civil action taken June 1992. • Decision in favor of the FDA on February 4, 1993. Preventing OOS Deficiencies

  4. Barr and Statistical Issues • Initial investigations • Full investigations • Testing • Retesting • Averaging • Outliers techniques Preventing OOS Deficiencies

  5. Preventing OOS Deficiencies

  6. Barr: Lessons Learned • FDA takes OOS issues very seriously. • OOS SOP’s, laboratory logs and documented investigations will be part of any Quality System review. • Companies are still getting Form 483 observations for not having an adequate SOP or for not following the SOP. Preventing OOS Deficiencies

  7. Barr: OOS Prevention • Analysts, supervisors and managers should read and discuss the Barr case and understand the OOS issues in context. Preventing OOS Deficiencies

  8. FDA Guidance • “Investigating Out of Specification (OOS) Test Results for Pharmaceutical Production.” • Issued as a draft in September 1998. • Still in draft as of today. • FDA has sent it to the attorneys. • Final version could be out this year. Preventing OOS Deficiencies

  9. Draft: OOS Prevention • All laboratory personnel, analysts, supervisors and managers should read, study and discuss in-depth, sentence by sentence if necessary, the draft OOS guidance. • Then do it again when the final guidance is released. Preventing OOS Deficiencies

  10. Able Labs – Cranbury, NJ • Massive number of OOS errors • Recall of all 46 products • 3,184 lots recalled • Five ANDA’s withdrawn • Hundreds of staff laid off • Sold to Sun Pharm in December 2005 • www.ablelabs.com Preventing OOS Deficiencies

  11. Able Labs: Lessons Learned • It is still possible to have wide spread misunderstanding of the Barr case, the OOS guidance and OOS SOPs. • Apparently the analysts felt they could not give an “incorrect result.” • Management needs to instill and cultivate a “GMP Culture” in the analytical laboratory. Preventing OOS Deficiencies

  12. Able Labs: OOS Prevention • Review the Able Labs web site. • Discuss the Able Labs story with laboratory analysts, supervisors and managers. • Discuss what a “GMP Culture” means in the analytical laboratory and how to develop and reward it. Preventing OOS Deficiencies

  13. PDA OOS Committees • Chemical OOS: • Lynn Torbeck, Chair • Eight members • Draft technical report reviewed by the FDA • Planning a PDA/FDA conference • Microbial Data Deviations: • Jeanne Moldenhauer, Chair • Draft in revision Preventing OOS Deficiencies

  14. Troublesome Fundamentals: • Outliers • Reportable Values • Averaging • Testing into compliance • Full consideration Preventing OOS Deficiencies

  15. Outliers - Defined • Extreme values vs outliers: Preventing OOS Deficiencies

  16. Outliers – Judge Wolin • "The USP expressly allows firms to apply this test (outlier) to biological and antibiotic assays, ..., but is silent on its use with chemical tests.” • "In the Court's view the silence of the USP with respect to chemical testing and outliers is prohibitory." Preventing OOS Deficiencies

  17. Outliers - Investigation • "In chemical procedures, where method accuracy variation is small, an outlier test may be appropriate as part of an OOS investigation, provided the sample and test procedure assumes homogeneity ... as in the composite strength assays. Our current thinking is that outlier tests are never appropriate where the purpose of the sample is to measure uniformity" Paul Vogel, September 10, 1993. Preventing OOS Deficiencies

  18. Outliers - Tests • Dixon's criteria, the test in USP<111>, is general in nature and not specific to biological issues. It can be used anywhere the statistical assumptions can be met. • In general, statisticians agree with the philosophy that outlier tests should be used infrequently and with great caution. Preventing OOS Deficiencies

  19. Outliers - Recommendations • Don't use any outlier rejection test for rejection of chemical test results. But it can be used as supporting information in an OOS investigation to consider retesting. • Keep all data, especially suspect data, for future review. Unusual data when seen in context and with other historical data often is not unusual at all, but in fact forms a known and well-behaved statistical distribution. Preventing OOS Deficiencies

  20. Reportable Values • “Reportable Values for Out of Specification Test Results” • Lynn Torbeck • Pharmaceutical Technology • Vol. 23, No. 2, February 1999 • Special Supplement Preventing OOS Deficiencies

  21. FDA R.V. Definition • “It should be noted that a test might consist of replicates to arrive at a result. For instance, an HPLC assay result may be determined by averaging the peak responses from a number of consecutive, replicate injections from the same preparation. The assay result would be calculated using the peak response average.” Preventing OOS Deficiencies

  22. FDA R.V. Definition • “This determination is considered one test and one result.” Preventing OOS Deficiencies

  23. Implications of FDA Definition • A reportable value is the end result of the complete measurement method as documented. • It is the value compared to the specifications. • It is the value used for official reports. • It is usually the value used for statistical analysis. Preventing OOS Deficiencies

  24. Figure 1 Preventing OOS Deficiencies

  25. Figure 2 Preventing OOS Deficiencies

  26. Figure 3 Preventing OOS Deficiencies

  27. Interpretation • The individual determinations do not have to meet the specification. • Individual determinations are not reported out of the lab. • However the variability of the determinations is a system suitability issue. • Set a limit on the standard deviation or %RSD. Preventing OOS Deficiencies

  28. R.V.: OOS Prevention • Record in writing the operational definition of the Reportable Value for each test method in the method documentation, any protocols and any reports. • Add “Only this reportable value can be compared to the specification criteria.” Preventing OOS Deficiencies

  29. Averaging • Specifically, the arithmetic mean; the sum of all of the numbers divided by the count of the numbers.  • More generally, it is a value that represents the central point of a data set. (In this sense, it can include the arithmetic average, the median, the mode, the geometric mean or the harmonic mean.) Preventing OOS Deficiencies

  30. Averaging • "... as a general rule, firms should avoid this practice, because averages hide the variability among individual test results.“ • "[Averaging] is particularly troubling if testing generates both out‑of‑specification and passing individual results which when averaged are within specification.  • "Here, relying on the average figure without examining and explaining the individual out‑of‑specification results is highly misleading and unacceptable." Preventing OOS Deficiencies

  31. Averaging • "Averaging the results of tests intended to measure the uniformity of the test article is not current good manufacturing practice ... because it may hide the variability of the sample the test procedure is intended to detect. For this reason, all individual test results must be reported and evaluated on an independent basis" Paul Vogel, September 10, 1993. Preventing OOS Deficiencies

  32. Averaging: OOS Prevention • Do not average out of specification reportable values within specification reportable values to get an in specification result. • Do not average reportable values for QA to make a decision. QA must see all individual reportable values, OOS and retests. Preventing OOS Deficiencies

  33. Testing Into Compliance • Torbeck, L., “Preventing the Practice of Testing into Compliance”, Pharmaceutical Technology, Oct 2002. • Testing into compliance is the practice of ignoring valid information that should be used to make decisions. • Such a practice is at best not scientific and at worst is fraudulent, illegal, and immoral. • Such practices if found must be stopped. Preventing OOS Deficiencies

  34. Testing Into Compliance • Averaging OOS results with in specification results to get an in specification result. • Physically averaging powers, granulations and liquids to get in specifications results. • If not part of the validated process. • Discarding data or not recording data until is known to be in specification. • Missing samples and rejected cans. • Overwriting HPLC chromatograms. Preventing OOS Deficiencies

  35. Not Testing Into Compliance • Large initial sample sizes are acceptable if all data generated is reported. • Large number of retests are acceptable if all data generated is reported. • Failing system suitability is not an OOS. • Out of limits for an in-process adjustment is not an OOS. Preventing OOS Deficiencies

  36. Compliance: OOS Prevention • Train all laboratory personnel, analysts, supervisors and managers to be able to identify specific situations of testing into compliance. • Train to be able to defend situations that are not testing into compliance during an audit. Preventing OOS Deficiencies

  37. Full Consideration • “For inconclusive investigations …. The OOS result should be retained in the record and given full consideration in the batch or lot disposition decision. • This statement has caused some discussion as it is considered to be vague and undefined. It can, I think, be defined in a simple way. Preventing OOS Deficiencies

  38. Full Consideration • First, all QA decisions are made with the Reportable Values, both OOS and retests. • Second, QA looks at the magnitude of the retest values compared to the specifications. Preventing OOS Deficiencies

  39. Full Consideration • If the retest values are close to the target, the lot can be released. • If the retest values are close to the limit that the OOS exceeded, technically the lot can be released, but QA should consider further investigation to determine why the retests are not at target. Preventing OOS Deficiencies

  40. Consideration: OOS Prevention • QA should detail and document the logic and rational for decisions based on retesting results after a OOS result is found. Preventing OOS Deficiencies

  41. Unresolved Issues • Specification Limits for OOS? • What size the retest sample? • Second analyst? • Statistical treatment of data? Preventing OOS Deficiencies

  42. Specification Limits for OOS? • Regulatory Limits • Release: accept/reject • Action limits, Cpk=1.33 • Alert, Cpk=1.0 • Warning limits • Trend • Validation limits Preventing OOS Deficiencies

  43. Specification Limits Preventing OOS Deficiencies

  44. Specification: OOS Prevention • Define in writing the levels of specification criteria. • Justify in writing which specifications are considered applicable to OOS and why or why not. Preventing OOS Deficiencies

  45. What Size the Retest Sample? • “… a matter of scientific judgment,” • “… retesting cannot continue ad infinitum.” • “Such a conclusion cannot be based on on 3 of 4 or 5 of 6 passing results, but possibly 7 of 8.” • “… will vary on a case by case basis … “ • “… an inflexible retesting rule … is inappropriate.” Preventing OOS Deficiencies

  46. What Size the Retest Sample? • “The number of retests … should be specified in advance …” • “The number of tests should not be adjusted ‘on-the-fly’, as results are being generated.” • “… a firm’s predetermined testing procedure should contain a point at which testing ends and the product is evaluated.” Preventing OOS Deficiencies

  47. What Size the Retest Sample? • This is an unresolved issue and the statisticians are still publishing journal articles and discussing it. • Barr case n=7. • Could be too much or not enough. • Currently n= 3 to n=9. • PDA OOS committee will recommend. Preventing OOS Deficiencies

  48. Retest References • Hofer, J., Considerations when determining routine sample size for a retest procedure, Pharmaceutical Technology, Nov. 2003. • Anderson, S., An alternative to the ESD approach, Pharmaceutical Technology, May 2004. Preventing OOS Deficiencies

  49. Retest: OOS Prevention • Define in writing the sample size for retests or define the procedure to be used to determine the sample size. • Provide scientific justification. Preventing OOS Deficiencies

  50. Second Analyst • Guidance suggests a second analyst. • Issues: • Added complication and variation • May not have a second analyst • May not find the root cause • Second analyst may not be as proficient • Recommend that the manager decide and justify decision in writing. Preventing OOS Deficiencies

More Related