A pilot study of durvalumab/tremelimumab (durva/treme) and radiation (XRT) for metastatic biliary tract cancer (mBTC): Preliminary safety and efficacy.

Theodore S. Hong; Lipika Goyal; Aparna R. Parikh; Beow Y. Yeap; Christine A. Ulysse; Lorraine C. Drapek; Jill N. Allen; Jeffrey W. Clark; Benjamin Christopher; Christine Bolton; David P. Ryan; Ryan B. Corcoran; Jeffrey A. Meyerhardt; Jennifer Y. Wo; Andrew X. Zhu

doi:10.1200/jco.2020.38.4_suppl.547

A pilot study of durvalumab/tremelimumab (durva/treme) and radiation (XRT) for metastatic biliary tract cancer (mBTC): Preliminary safety and efficacy.

Theodore S. Hong(Massachusetts General Hospital), Lipika Goyal(Massachusetts General Hospital), Aparna R. Parikh(University of California, San Francisco), Beow Y. Yeap(Massachusetts General Hospital), Christine A. Ulysse(Massachusetts General Hospital), Lorraine C. Drapek(Massachusetts General Hospital), Jill N. Allen(Massachusetts General Hospital), Jeffrey W. Clark(Massachusetts General Hospital), Benjamin Christopher(Massachusetts General Hospital), Christine Bolton(Massachusetts General Hospital), David P. Ryan(Massachusetts General Hospital), Ryan B. Corcoran(Massachusetts General Hospital), Jeffrey A. Meyerhardt(Dana-Farber Cancer Institute), Jennifer Y. Wo(Massachusetts General Hospital), Andrew X. Zhu(Massachusetts General Hospital)

Journal of Clinical Oncology

February 1, 2020

10.1200/jco.2020.38.4_suppl.547

Cited by 14

Abstract

547 Background: Metastatic biliary tract cancer (mBTC) is a lethal malignancy with median 5 year OS of less than 10%. Immunotherapy, particularly single agent anti-PD-1/PD-L1, has limited efficacy in mBTC with ORR~9-15%. Recently presented data shows responses in metastatic MSS pancreatic or colon cancer with combination anti-PD-1/CTLA-4 and radiation (XRT) to produce systemic response (abscopal effect) (Parikh A, GI ASCO 2019, ASCO 2019.). We evaluate safety and efficacy of dual PD-1/CTLA-4 inhibition with XRT in MSS mBTC. Methods: 15 of a planned 15 mBTC patients were enrolled. Eligible pts had histologically-confirmed mBTC, ECOG-PS 0/1, and must have progressed on at least one line of previous therapy or refused standard therapy. Safety cohort of 6 pts of durva 1500 mg/treme 75 mg q4w was enrolled. If > 2 DLTs, patients were enrolled subsequently to dose level -1 (durva 1125 mg/ treme 75 mg q4w). 3 fractions of 8 Gy of radiation at C2D1 every other day to a single metastatic site. Durva/treme continued for 4 cycles, followed by 4 cycles of maintenance durva until progressive disease, discontinuation or withdrawal. Endpoints include disease control rate (DCR (SD+PR+CR)), PFS and OS and safety. Radiological evaluations were done q2 mo. Results: 15 mBTC pts enrolled and evaluable from May 2018 to March 2019. Median age 63 years (range 48-75), 47% male. DLTs occurred in 3 patients during the safety run-in. One patient experienced DLT at dose level -1 and subsequent expansion. 3 patients did NOT reach radiation therapy. DCR was 27% with a 13% PR and 7% CR. Of those who reached radiation, DCR was 33% with a 17% PR and 8% CR. At time of analysis, median PFS was 54 days for ITT mBTC. Duration of response for 4 patients with DCR was 26, 52, 122, 254+ days. Treatment-related adverse events were reported in 12/15 patients (80%). Grade ≥3 toxicities were seen in 9/15 pts (60%) with lymphopenia (5 grade 3) and elevated LFTs (2 grade 4 and 4 grade 2) being the main adverse events. All patients with disease control were not MSI. Conclusions: Combination of durva/treme XRT is feasible and shows preliminary activity in metastatic BTC. An expansion cohort is being planned to confirm activity. Clinical trial information: NCT03482102.

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