Abstract 39TiP
Background
HCC recurs in 50%∼70% of patients within 5 years following potentially curative resection. Adjuvant therapies are expected to prevent early recurrence in high risk patients, however till now there is no solid evidence and consensus. The immune component of the liver microenvironment has been reported to play a key role in HCC recurrence. Sitravatinib is a selective tyrosine kinase inhibitor targeting TAM (TYRO3, AXL, MER) and split tyrosine-kinase domain-containing receptors (VEGFR2, KIT) that may help overcome the immunosuppressive tumor microenvironment and augment antitumor responses. TIS, an anti-PD-1 antibody, has shown encouraging and durable clinical antitumor activity in advanced HCC. An early trial showed that TIS plus sitravatinib was well-tolerated and had preliminary antitumor activity in previously treated advanced HCC. This open-label, multicenter, phase II study (NCT05407519) aims to evaluate the efficacy and safety of TIS plus sitravatinib as adjuvant therapy in patients with HCC at high risk of recurrence after curative resection.
Trial design
Eligible patients are aged from 18∼70 years and have HCC confirmed by histopathology or cytology; ECOG PS 0/1; Child-Pugh class A liver score; no prior systematic treatment and locoregional therapy; no invasion or tumor thrombus in portal vein, hepatic vein or bile duct and no extrahepatic metastasis or lymph node metastasis. Patients have undergone a curative resection, and those at high-risk of HCC recurrence will be eligible by fulfilling at least one of the following criteria: 1) a solitary tumor>5 cm; 2) solitary tumor>2cm and ≤5cm with microvascular invasion; and 3) 2∼3 lesions. Forty patients will receive TIS (200mg, IV, Q3W) combined with sitravatinib (100mg, PO, QD). TIS and sitravatinib will be administered until disease progression, intolerable toxicity, withdrawal of consent or death, with a maximum 17 cycles for TIS. Primary endpoint is 2-year recurrence-free survival (RFS) rate. Secondary endpoints include RFS, time to recurrence, overall survival (OS), 1-year RFS rate, 1-year and 2-year OS rate, and safety.
Clinical trial identification
NCT05407519.
Legal entity responsible for the study
The authors.
Funding
BeiGene, Ltd.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
28P - Development 68Ga trastuzumab Fab and bioevaluation by PET imaging in HER2/neu-expressing breast cancer patients
Presenter: Yogesh Rathore
Session: Poster viewing 01
29P - Targeting CXCR4 promotes antitumor immunity through TOX-mediated CD8+ T cell activation
Presenter: Canhui Cao
Session: Poster viewing 01
30P - Investigation of KRAS G12C inhibitor JAB-21822 as a single agent and in combination with SHP2 inhibitor JAB-3312 in preclinical cancer models
Presenter: Peng Wang
Session: Poster viewing 01
31P - Photothermal responsive, nucleolin-targeted bimetallic nano-vehicle delivered the combinational therapeutics for improved pancreatic cancer treatment
Presenter: Kandasamy Saravanakumar
Session: Poster viewing 01
32P - Tumor growth inhibition effect of PLAG by regulation of neutrophil infiltration in ICI insensitivity B16F10 melanoma
Presenter: Guen Tae Kim
Session: Poster viewing 01
33P - Establishment of personalized therapeutic for salivary gland cancers based on patients-derived salivary tumoroid model
Presenter: Yoonjin Roh
Session: Poster viewing 01
34P - Association of ACRBP gene polymorphism (+26A/G) to liver cancer and diabetes leads to novel biomarker discovery
Presenter: Md Shariful Islam
Session: Poster viewing 01
35P - Exploring plerixafor as a vector molecule in nuclear medicine for targeting CXCR4 receptor overexpression in vivo
Presenter: Tamanna Lakhanpal
Session: Poster viewing 01
36P - Preclinical evaluation of novel MCL-1 degrader in in vitro and in vivo cancer models
Presenter: Piotr Kowalczyk
Session: Poster viewing 01
37P - Development of splice switching antisense oligonucleotides targeting midkine
Presenter: Graham Robertson
Session: Poster viewing 01