作者
Andreas Nicholas Saltos, Tawee Tanvetyanon, Ben C Creelan, Michael Rahman Shafique, Scott Joseph Antonia, Eric B Haura, Hong Zheng, Margaret Barlow, James Saller, Anna Castellano-Fornelli, Antoine Richards, Ram Thapa, Theresa A Boyle, Dung-Tsa Chen, Amer A Beg, Jhanelle Elaine Gray
发表日期
2020/5/20
来源
Journal of Clinical Oncology
卷号
38
期号
15_suppl
页码范围
9567-9567
出版商
American Society of Clinical Oncology
简介
9567
Background: Histone deacetylase inhibitors may enhance tumor immunogenicity through various mechanisms including induced expression of T cell chemokines. A previous phase I trial demonstrated the combination of pembrolizumab (P) with vorinostat (V) in mNSCLC was well tolerated with signals of activity in ICI-pretreated pts. We initiated a randomized trial in the first-line setting with the primary objective to determine if the combination had superior ORR compared to pembrolizumab monotherapy. Methods: Pts with treatment-naïve mNSCLC and PD-L1 expression ≥ 1% were eligible. Pts were randomized open-label 1:1 to receive P 200 mg IV q3 wk as monotherapy [Arm A] or P 200 mg IV q3 wk plus V 400 mg PO daily [Arm B]. The primary endpoint was overall response rate (ORR). Secondary endpoints included DOR, PFS and OS. Tumor biopsies were collected both pre- and on-treatment (day 15-21 …
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AN Saltos, T Tanvetyanon, BC Creelan, MR Shafique… - 2020