Abstract 791P
Background
ASTX029 is an extracellular signal-regulated kinase 1/2 (ERK1/2) inhibitor which both prevents phosphorylation of ERK and directly inhibits ERK kinase activity. MAPK pathway genomic alterations are common in gynecological (GYN) malignancies. Here we report on the GYN cohort of an open-label Phase 2 study of ASTX029 in subjects with relapsed/refractory solid tumors (NCT03520075).
Methods
The primary objective was objective response rate (ORR) by RECIST v1.1. Subjects with relapsed/refractory GYN solid tumors with MAPK pathway genomic alterations were eligible. ASTX029 was administered continuously in 21-day cycles (once daily oral dosing at 200 mg).
Results
Thirty-two subjects were treated (mean age 64 years; 15 ovarian, 13 endometrial, 1 cervical, and 3 other). As of 05Apr2024, the only grade ≥3 AE assessed as related to ASTX029 in ≥5% of subjects was anemia (n=3; 9.4%); no SAEs (of 12; 38%) or deaths were related to ASTX029. Related grade 2 AEs in ≥5% of subjects included anemia (n=6; 19%), blurred vision (n=2; 6%), diarrhoea (n=6; 19%), nausea (n=4; 13%), fatigue (n=4; 13%), ejection fraction decreased (n=2; 6%), decreased appetite (n=2; 6%), and rash maculo-papular (n=2; 6%). Six subjects (18.8%) interrupted treatment due to a related AE but none permanently discontinued treatment for this reason. The most frequent reason for treatment discontinuation was progressive disease (n=27; 84.4%). PK exposures were in the pharmacologically active range with mean cycle 1 AUC0-24 as 10321 ng*hr/mL (76%CV) and Cmax as 3457 ng/mL (160%CV), n=11. Four subjects had a PR including: NRASQ61K ovarian adenocarcinoma who progressed on prior MEKi treatment (14+ cycles), KRASG12V cervical (mesonephric) adenocarcinoma (17+ cycles), KRASG12D endometrioid ovarian (11 cycles), and KRASG12D endometrioid endometrial (8 cycles). ORR (CR+PR) was 12.5% (% 95% CI, 1.0-24.0). Median overall survival was 11.2 months (95% CI, 8.4-NE); median duration of response was 8.5 months (95% CI, 3.4-11.1). Median follow-up on study was 7.7 months (95% CI, 5.6-13.9).
Conclusions
ASTX029 was well-tolerated and induced PR in four subjects (ORR of 12.5%). The response following MEKi therapy suggests further study in this population is warranted.
Clinical trial identification
NCT03520075.
Editorial acknowledgement
Legal entity responsible for the study
Astex Pharmaceuticals.
Funding
Astex Pharmaceuticals (now Taiho Oncology).
Disclosure
All authors have declared no conflicts of interest.
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