ESMO Asia Virtual Congress 2020

Abstract 182P

Background

Combining LEN with anti-PD-1 antibodies (LEN+PD1) has shown promising anti-tumour effect against advanced HCC in KEYNOTE 524 and Study 117. We assessed LEN+PD1 vs LEN monotherapy in Chinese patients (Pts) with advanced HCC.

Methods

This real-world study included Pts with untreated advanced HCC who received lenvatinib (8 mg/d regardless of bodyweight) ± anti-PD-1 antibodies (q3wk) between Nov 2018 and Nov 2019, and had ≥1 efficacy and safety assessment. Endpoints included objective response rate (ORR), disease control rate (DCR) and progression free survival (PFS) evaluated using mRECIST and RECIST 1.1 every 2 months from treatment initiation, ALBI score and safety.

Results

The study included 22 patients who received LEN+PD1 and 22 who received LEN. For patients in the LEN+PD1 and LEN groups, median follow-up was 6.6 and 5.3 months, mean age was 54.8 and 53.2 years, 81.8 and 90.9% had BCLC stage C disease, and 72.7 and 68.1% were Child-Pugh A, respectively. ORR and DCR were numerically higher in the LEN+PD1 group vs the LEN group (Table) and median PFS was 12.1 (95% CI: 7.9, 16.2) vs 8.9 months (95% CI: 6.6, 11.2; HR=0.58; 95% CI: 0.17, 1.93), respectively. A similar proportion of patients in both groups decreased one ALBI level from baseline (p=0.9331). The most common AEs in the LEN+PD1 group were hypertension (22.7% [5]), decreased appetite (18.2% [4]) and ALT increase (13.6% [3]) and in the LEN group were ALT increase (31.8% [7]), proteinuria (18.2% [4]) and decreased appetite (18.2% [4]). No unexpected safety signals were observed. Table: 182P

n (%)	RECIST 1.1	mRECIST
LEN + PD1 n=22	LEN n =22	p	LEN + PD1 n=22	LEN n =22	p
ORR	10 (45.5)	4 (18.2)	0.052	11 (50.0)	7 (31.8)	0.220
DCR	20 (90.9)	17 (77.3)	0.216	20 (90.9)	17 (77.3)	0.216
Complete response	1 (4.5)	0	0.204	3 (13.6)	2 (9.1)	0.526
Partial response	9 (40.9)	4 (18.2)		8 (36.4)	5 (22.7)
Stable disease	10 (45.5)	13 (59.1)		9 (40.9)	10 (45.5)
Progressive disease	2 (9.1)	5 (22.7)		2 (9.1)	5 (22.7)

Conclusions

LEN ± anti-PD-1 antibodies was effective and well tolerated in first-line treatment of patients with advanced HCC. LEN+PD1 showed a trend towards higher ORR, DCR, and longer PFS vs LEN, with no increase in hepatotoxicity. However, further evaluation in randomized, prospective trials is required.