BackgroundINCB086550 is an orally administered small molecule that binds PD-L1 and inhibits PD-1/PD-L1 interaction. Translational data demonstrating markers of immune activation in patients following INCB086550 were previously reported.1 Preliminary clinical data from this phase 1 study are presented below.MethodsAdult patients (≥18 years) with advanced solid tumors were enrolled into this open-label study. Patients had disease progression after standard available therapy or were intolerant of or ineligible for standard treatment. Measurable disease was required. A modified 3+3 dose-escalation design was employed, followed by dose expansions. The primary endpoints were safety and tolerability of INCB086550, identification of a pharmacologically active dose and/or MTD, and confirmation of the RP2D. Secondary endpoints included PK, pharmacodynamics, and efficacy as assessed by investigator-determined ORR and DCR (CR, PR, or SD ≥12 weeks).ResultsAs of 9Apr2021, 79 patients received treatment (Table 1); 57.0% were female, 62.0% had ≥2 prior lines of therapy, and 16% received prior IO treatment. Forty-six (58.2%) patients had treatment-related TEAEs; those occurring in ≥5% of patients are presented in Table 2. Ten patients (12.7%) had grade ≥3 treatment-related TEAEs. Immune-related TEAEs occurred in 15 patients (19.0%); the most common (>1 patient) included peripheral sensory neuropathy (n=5), pruritus (n=3), immune-mediated neuropathy (n=2), and peripheral motor neuropathy (n=2). In total, 10 (12.7%) patients had TEAEs of peripheral neuropathy; all were grade ≤3. All grade 2 or 3 TEAEs of peripheral neuropathy resolved or improved with either study drug continuation without dose modification, dose reduction, or drug interruption/discontinuation. Patients with TEAEs leading to treatment interruption were 21 (26.6%), dose reduction 5 (6.3%), and discontinuation 13 (16.5%). Five patients (6.3%) died of a TEAE (cerebrovascular accident, dyspnea, general physical health deterioration, intestinal obstruction, intracranial hemorrhage [each n=1]); all fatal TEAEs were considered unrelated to study drug. The efficacy-evaluable population included 68 patients; ORR was 11.8% (95%CI, 5.2%–21.9%; CR, 1.5%; PR, 10.3%), and DCR was 19.1% (95%CI, 10.6%–30.5%; Table 3). Eight objective responses were observed at doses ≥400 mg BID (Table 4); 3 of these were noted among the 5 IO treatment-naive patients with MSI-H tumors who received 400 mg BID.ConclusionsImmune-related AEs observed in this ongoing phase 1 study are consistent with those seen with antibody immune checkpoint inhibitors, with the exception of peripheral neuropathy. Preliminary efficacy of INCB086550 in tumor types known to be responsive to anti-PD-(L)1 therapy is encouraging and warrants further investigation.Trial RegistrationClinicaltrials.gov identifier NCT03762447ReferencesPiha-Paul S, et al. J Immunother Cancer. 2020;8(suppl 3):A255.Ethics ApprovalThe study protocol was approved by institutional review boards (IRB) or independent ethics committees at participating centers. All study participants gave informed consent before taking part. The approval numbers were: Integ Review IRB (Austin, TX), RM 598; MD Anderson Cancer Center Office of Human Subject Protection (Houston, TX), IRB ID 2018-0765; ADVARRA (Columbia, MD), IRB# 00000971; Ethisch Comité/Comité d’ Ethique Hospital (Brussels, Belgium), A2021/085; Hôpital Saint-Louis (Paris, France), Prof Le Tourneau – 2020-118/Ref. of the Promoter 0.09.22.72214; NHS Health Research Authority London - City & East Research Ethics Committee (Bristol, UK), IRAS project ID:282291/REC reference: 20/LO/1001; Comitato Etico IRCCS Pascale (Milan, Italy), ISS Validation Protocol Number 29111(2020)-PRE21-1835; Comitato Etico Della Fondazione IRCCS ”Istituto Nazionale Dei Tumori”- Milano CE150053 (Milan, Italy), INT 230/20; Comitato Etico Regione Toscana - Area Vasta Sud Est CE150047, 18064; Comitato Etico Indipendente Istituto Clinico Humanitas CE150081, 940/20; Regulatory Pharma Net (Pisa, Italy), IEC 1393.Abstract 529 Table 1Number of patients per dose levelBID, twice daily; QD, once daily.The tumor types in the study included breast, cervical, colorectal, endometrial, esophageal, gastric, hepatocellular, melanoma, mesothelioma, ovarian, small cell lung cancer, squamous cell carcinoma of the head and neck, renal cell, urothelial, adrenal, anal, cholangiocarcinoma, gall bladder, pancreatic, penile, salivary gland, sarcoma, vaginal, prostate, basal cell, pleomorphic sarcoma, fallopian, carcinoma of parotid gland, well-differentiated liposarcoma, myoepithelial, castrate-resistant prostate cancer, cancer of unknown primary, neuroendocrine, prostate adenocarcinoma with neuroendocrine differentiation, glioblastoma, anal canal, angiosarcoma, and gastroesophageal junction.Abstract 529 Table 2Treatment-related TEAEs reported by ≥5% of patients (N=79)TEAE, treatment-emergent adverse event.Abstract 529 Table 3Summary of best overall response by RECIST v1.1 or RANO*CR, complete response; DCR, disease control rate; GBM, glioblastoma; ORR, objective response rate; PR, partial response; RANO, Response Assessment of Neuro-Oncology; RECIST, Response Evaluation Criteria in Solid Tumors; SD, stable disease.* 1 patient with GBM was assessed by RANO and had best overall response of progressive disease.† The efficacy-evaluable population included all solid tumor participants enrolled in the study who received at least 1 dose of INCB086550, completed a baseline scan, and met at least 1 of the following criteria: ≥1 postbaseline scan, participant had been on the study for a minimum of 63 days of follow-up, or participant had discontinued from treatment.‡ ”Not evaluable” indicates participants in the efficacy-evaluable population that did not have valid postbaseline overall response assessments by RECIST or RANO.§ ”Not assessed” indicates participants in the efficacy-evaluable population that did not have any postbaseline overall response assessments by RECIST or RANO.Abstract 529 Table 4Tumor types with investigator-assessed objective response per RECIST v1.1 (n=8)BID, twice daily; dMMR, deficient mismatch repair; IO, immuno-oncology; MSI-H, high microsatellite instability; RECIST, Response Evaluation Criteria in Solid Tumors.+Ongoing response.