ESMO Congress 2023 | OncologyPRO

Abstract 1627P

Background

Chemotherapy regimens remain the standard 1L treatment for PC, but with limited anti-tumor activity. We amid to explore the feasibility of adding the PARPi fuzuloparib to mFOLFIRINOX in pts with LA/M PC.

Methods

This was a dose escalation (ESC) and expansion (EXP) phase Ib study. Pts were given oral fuzuloparib at escalating doses starting at 30 mg bid plus intravenous mFOLFIRINOX q2w for 8–12 cycles, followed by maintenance fuzuloparib at 150 mg bid. Dose-limiting toxicities (DLTs) were observed during the first 2 cycles. At least 1 dose cohort would be selected for EXP to collect data supporting the determination of recommended phase II dose (RP2D). Primary endpoints were DLT, maximal tolerated dose (MTD), and RP2D.

Results

As of Jan 15, 2023, 39 pts were recruited. Of them, 12 pts were enrolled in ESC phase (30 mg [n=4]; 60 mg [n=6]; 100 mg [n=2]). DLT occurred in 1 pt in 60 mg cohort (grade 4 decreased platelet count and grade 4 decreased neutrophil count lasting for ≥5 d) and 1 pt in 100 mg cohort (grade 4 decreased neutrophil count lasting for ≥5 d). Based on the tolerability and safety data during ESC, 60 mg bid was determined to be the MTD. 60 and 30 mg cohorts were expanded to 22 and 15 pts, respectively. Overall, grade ≥3 treatment-related adverse events (TRAEs) were reported in 34 (87.2%) of 39 pts; the most common were decreased neutrophil count, decreased platelet count, decreased white blood cell count, and anemia. TRAEs led to discontinuation of any study agent in 5 (12.8%) pts. Efficacy in 60 mg cohort seemed to be most favorable, with ORR of 50.0%, DCR of 94.4%, median PFS of 7.2 mo, and median OS of 12.5 mo (Table). Table: 1627P

Efficacy outcomes

	30 mg	60 mg	100 mg	Overall
Confirmed ORR^∗, n/N (%; 95% CI)	2/12 (16.7%; 2.1–48.4)	9/18 (50.0%; 26.0–74.0)	0/2 (0.0%; 0.0–84.2)	11/32 (34.4%; 18.6–53.2)
Confirmed DCR^∗, n/N (%; 95% CI)	10/12 (83.3%; 51.6–97.9)	17/18 (94.4%; 72.7–99.9)	1/2 (50.0%; 1.3–98.7)	28/32 (87.5%; 71.0–96.5)
PFS^#
Events, n/N (%)	10/15 (66.7%)	12/22 (54.5%)	2/2 (100.0%)	24/39 (61.5%)
Median (95% CI), mo	7.5 (1.9–10.1)	7.2 (5.1–13.9)	7.2 (1.6–NR)	7.3 (5.3–10.1)
OS^#
Events, n/N (%)	10/15 (66.7%)	15/22 (68.2%)	1/2 (50.0%)	26/39 (66.7%)
Median (95% CI), mo	11.5 (4.0–NR)	12.5 (7.8–NR)	NR (2.0–NR)	11.5 (7.8–14.2)

^∗tumor response evaluable set;^#full analysis set.

Conclusions

1L fuzuloparib plus mFOLFIRINOX followed by maintenance fuzuloparib was generally safe, with no unexpected toxicities, and showed encouraging efficacy in pts with LA/M PC. The RP2D of fuzuloparib combination was 60 mg bid.

Clinical trial identification

NCT04228601.

Editorial acknowledgement

Legal entity responsible for the study

Jiangsu Hengrui Pharmaceuticals.

Funding

Jiangsu Hengrui Pharmaceuticals.

Disclosure

Z. Sheng, J. Lian, Q. Shi: Financial Interests, Personal, Full or part-time Employment: Jiangsu Hengrui Pharmaceuticals. All other authors have declared no conflicts of interest.

Poster session 22

1627P - First-line (1L) fuzuloparib plus mfolfirinox followed by maintenance fuzuloparib in patients (pts) with unresectable locally advanced or metastatic (LA/M) pancreatic cancer (PC): A phase Ib study

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Abstract 1627P

Background

Methods

Results

Conclusions

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

Funding

Disclosure

Abstract 1627P

Background

Methods

Results

Conclusions

Clinical trial identification

Editorial acknowledgement

Legal entity responsible for the study

Funding

Disclosure

Resources from the same session