Real-world (RW) characteristics, treatment patterns, and outcomes of patients with cholangiocarcinoma (CCA) treated with pemigatinib.

Abstract

444 Background: Pemigatinib demonstrated efficacy in fibroblast growth factor receptor (FGFR)–altered CCA in the FIGHT-202 trial; however, limited RW evidence exists on treatment patterns and outcomes in patients (pts) with CCA treated with pemigatinib. This study assessed characteristics, FGFR2 testing patterns, treatment patterns, and outcomes of pts treated with pemigatinib for locally advanced or metastatic CCA in the United States as part of routine clinical care. Methods: This retrospective, multisite cohort study included pts with a diagnosis of unresectable locally advanced or metastatic CCA who were initially prescribed pemigatinib on or after 04/17/2020. Eligible pts were ≥18 years at pemigatinib prescription and had ≥4 months (mo) of follow-up (unless <4 mo due to death). Pts who received pemigatinib as part of a clinical trial or those who received systemic therapy for another primary malignancy (other than cancer of unknown primary or hepatic cancer) were ineligible. Participating physicians from Cardinal Health’s Oncology Provider Extended Network—approximately 72% from community oncology practices—abstracted data from the medical records of eligible patients into electronic case report forms. Results were summarized using descriptive statistics. Results: Data from 120 pts (49% male; 55% White; 19% Hispanic; median age at pemigatinib prescription, 65 years) were collected from 18 physicians/practices. Testing for FGFR2 alterations was completed in 93% (n=111) of pts; of those, all but one patient (result unknown) tested positive, and 95% were tested using next-generation sequencing. At time of pemi prescription, 90% of pts had metastatic disease. Across all pts, 94% and 6% were prescribed pemigatinib as 2nd and 3rd line of therapy, respectively. The most common starting dosage was 13.5 mg daily for 14 days of 21-day cycle (87.5% of pts). Among the 60 pts who discontinued pemi during the 6.5-month median study follow-up period, 68% discontinued due to disease progression. Median RW progression-free survival (rwPFS) from date of pemigatinib initiation was 7.4 (95% CI: 6.4–8.6) mo. Among the 116 patients with tumor response data available, RW overall response rate (rwORR) was 61% (95% CI: 52% - 71%). Conclusions: This study complements the FIGHT-202 clinical trial by assessing the use of pemigatinib among a diverse population of patients with CCA under RW conditions. Secondarily, the rwORR and rwPFS from this study support the clinical benefit of pemigatinib demonstrated in FIGHT-202.