First disclosure of frontline treatment (1L tx) with the selective CDK4 inhibitor BGB-43395 in combination with letrozole for metastatic HR+/HER2− breast cancer (BC): A phase 1 safety expansion.

1066 Background: BGB-43395, a highly selective CDK4i, showed preclinical antitumor activity characterized by improved CDK4 target coverage and selectivity over CDK6. This enhanced selectivity may reduce off-target toxicity and the need for tx modifications. BGB-43395 is being evaluated as monotherapy or with endocrine therapy in patients (pts) with HR+/HER2− BC and other advanced solid tumors in an ongoing phase 1a/1b open-label, international study (NCT06120283). We report on the safety, preliminary anti-tumor activity, and pharmacodynamics (PD) of BGB-43395 + letrozole as 1L tx for BC. Methods: In safety expansion cohort 2, CDK4/6i-naive pts with advanced/metastatic HR+/HER2− BC were randomized to receive BGB-43395 240, 400, or 600 mg PO BID + letrozole to determine the recommended dose for further development. The objectives were to assess safety, preliminary anti-tumor activity, and PD. Results: As of Nov 11, 2025, 58 pts received study tx (240 mg n = 19; 400 mg n = 19; 600 mg n = 20). Treatment emergent adverse events (TEAEs) occurred in 98% of pts; grade (G)≥3 TEAEs in 32%, 37%, and 65% of pts on 240 mg, 400 mg, and 600 mg, respectively. The most common TEAEs (mostly G1/2) were (240 mg / 400 mg / 600 mg): diarrhea (79% / 95% / 90% G3 5% / 11% / 30%), nausea (53% / 68% / 85% G3 0% / 5% / 0%), and vomiting (26% / 47% / 60% G3 0% / 0% / 0%). Rates of TEAE hematologic toxicities (mostly G1/2) were low; neutrophil count decreased/neutropenia (240 mg 26% G3 0%; 400 mg 21% G3 0%; 600 mg 20% G3 10%); anemia (240 mg 5% G3 0%; 400 mg 21% G3 0%; 600 mg 20% G3 5%); platelet count decreased/thrombocytopenia (all G1 or 2 240 mg 5%; 400 mg 0%; 600 mg 5%). TEAEs led to dose modification in 53% of pts (median relative dose intensity: 240 mg 100%; 400 mg 97%; 600 mg 69%), tx discontinuation in 3% (240 mg, 1 pt; 600 mg, 1 pt), and 0 deaths. BGB-43395 + letrozole demonstrated early efficacy (Table) and strong PD effects, indicated by TK1 reduction and ctDNA decrease. Median study follow-up was 6.8 (range 3.2-9.7) mo, median time-to-response was 3.6 (range 1.6-8.4) mo, and median PFS was not reached. Conclusions: The CDK4-selective inhibitor BGB-43395, in combination with letrozole, demonstrated a favorable safety profile, with low hematologic and manageable gastrointestinal toxicity. Antitumor activity in 1L tx of pts with advanced HR+/HER2− BC was promising. Doses of 400 mg and 240 mg BID demonstrated efficacy and safety that support further development in combination with letrozole. Clinical trial information: NCT06120283 . BGB-43395 BID dose + letrozole 240 mg (n=19) 400 mg (n=19) 600 mg (n=20) Median tx follow-up, mo 7.0 7.1 5.2 Best overall response, % PR​ a 58 68 40 SD 37 32 55 PD 5 0 0 NE 0 0 5 Objective response rate (CR + PR), %(95% CI) 58(33-80) 68(43-87) 40(19-64) Disease control rate (CR + PR + SD), %(95% CI) 95(74-100) 100(82-100) 95(75-100) RECIST v1.1 (investigator). a Unconfirmed.