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SNDA 20-221 ETHYOL FOR RADIATION INDUCED XEROSTOMIA.

Published byErick Preston Modified over 7 years ago

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Presentation on theme: "SNDA 20-221 ETHYOL FOR RADIATION INDUCED XEROSTOMIA."— Presentation transcript:

1 sNDA 20-221 ETHYOL FOR RADIATION INDUCED XEROSTOMIA

2 REVIEW TEAM

3 WR-0038 A Phase III Trial of Radiation Therapy  Amifostine in Patients with Head and Neck Cancer

4 PRETREATMENT CHARACTERISTICS Balanced Site of Disease Clinical Stage Nodal Status Volume of Parotid Glands for RT Type of Radiation

5 INTENDED RADIATION DOSE “Type of Radiation” Inoperable 66-70 Gy Post-Operative, High-Risk60-66 Gy Post-Operative, Low-Risk50-60 Gy

6 ACTUAL RADIATION RECEIVED Overall : p=0.056

7 PRIMARY ENDPOINTS

8 PRIMARY ENDPOINT: Acute Xerostomia Applicant: Significant Reduction of Grade 2 Xerostomia –A+RT (51%) vs. RT (78%) (p<0.0001) FDA: Agree No difference in overall incidence (Gr 1 + 2) –A+RT (90%) vs. RT (94%) (p=0.07)

9 PRIMARY ENDPOINT: Late Xerostomia Applicant: 365  31 days Significant Reduction in Grade 2 or greater –A+RT (34%) vs. RT (57%) (p<0.0019) FDA Comments: –Disagree with applicant’s definition –Reanalysis necessary

10 FDA Review (revised): Late Xerostomia

11 LATE XEROSTOMIA vs. TOTAL RADIATION DOSE

12 PRIMARY ENDPOINT: Acute Mucositis No difference (Grade 3 or greater) –A+RT (35%) vs. RT (39%) (p=0.48) Grade 1 to 4 –A+RT (95%) vs RT (99%)

13 SUMMARY OF PRIMARY EFFICACY ENDPOINT FINDINGS  Significantly lower incidence of moderate acute xerostomia  Significantly lower incidence of moderate to severe late xerostomia  No difference in the incidence of acute mucositis

14 SECONDARY ENDPOINTS Related to Efficacy: –Saliva Measurements –Patient Benefit Questionnaire Related to Non-Tumor Protection: –One Year Locoregional Control (Primary Endpoint) – DFS –Overall Survival Safety

15 Applicant: Significant difference in unstimulated saliva at one year (> 0.1 gm) –A+RT (72%) vs. RT (49%) (p=0.003) Not confirmed by stimulated saliva collections –A+RT (33%) vs. RT (41%) (p=0.3) SECONDARY ENDPOINT Saliva Measurements FDA Comments: Longitudinal analysis of unstimulated saliva production non-confirmatory Retrospective definition of time point comparisons Retrospective definition of clinically significant cut-off values

16 FDA ANALYSIS: Change from Baseline

17 SUMMARY OF SECONDARY EFFICACY ENDPOINT FINDINGS: Saliva Measurements

18 SECONDARY ENDPOINT: Patient Benefit Questionnaire Reasons for Different Analyses FDA Analysis Results Summary

19 Analysis of PBQ Data Different measures of clinical benefit –Sponsor: mean score of 8 questions –FDA: 3 individual subscales Functional well-being (speaking, eating) General condition (dryness) Use of external aids (frequency of fluid intake for eating & comfort not associated with eating) Number of data points –Sponsor: excluded data beyond the 1 year follow-up visit –FDA: all data points

20 FDA Analysis of PBQ Data Cutoff value in defining dropouts and completers: 1 year Number of Patients Method: Longitudinal analysis with GEE quadratic models

21 Functional Well-being Completers & Dropouts GEE quadratic model

22 General Condition Completers & Dropouts GEE quadratic model

23 Use of External Aids Completers & Dropouts GEE quadratic model

24 Functional Well-being All Patients

25 General Condition All Patients

26 Use of External Aids All Patients

27 SUMMARY Results: Descriptive and exploratory –Subjective nature of the questionnaire –Open-label trial design –Adjustment of multiple comparisons Trends in favor of the Ethyol: –General Condition –Use of External Aids Trend in favor of the Ethyol arm for Functional Well-being ?

28 Applicant: –Primary: no difference in locoregional control at one year (72% vs. 71%, p=1.0) –no difference in DFS, overall survival –WR-9001 in Rectal Cancer: no significant difference in overall survival SECONDARY ENDPOINT Tumor Control FDA Comments: –WR-0038: immature data, high censor rate –Selection of 0.7 as the lower limit of a 1-sided C.I. is liberal

29 Significantly greater frequency of known adverse events Large number of dropouts in A+RT –29/150 (19%) More radiotherapy doses missed in A+RT More hospitalizations in A+RT –A+RT:101 vs. RT:63 SAFETY

30 CONSIDERATIONS FOR APPROVAL Well-designed, well-controlled trials Substantial evidence of efficacy and safety

31 !Significant but expected toxicities !More drop-outs, hospitalizations, missed doses !Ability to deliver optimal doses of therapy and potential effect on the efficacy ? !Should be weighed against strength of other evidence i Safety

32  Significant difference in moderate to severe acute and late xerostomia  PBQ and Salivary Measurement data supportive ? i Efficacy

33  Single phase 3 trial i Adequate and well controlled clinical trials

34

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