Abstract 612P
Background
The fruquintinib (a highly selective, and potent oral inhibitor of VEGF receptor 1, 2, 3) plus mFOLFOX6/FOLFIRI (standard chemotherapy) in patients (pts) with advanced mCRC study was a prospective, open-label, multi-center, single-arm phase 2 study (NCT05004441). The results of this study have been previously reported at the 2023 ASCO GI (152 Poster Session) and here we updated the efficacy and safety results with more enrolled pts and longer follow-up duration.
Methods
Pts aged 18-75 years with unresectable or metastatic CRC, without prior systemic threatment were recruited. RAS/BRAF status should be detected to exclude BRAF mutations before enrollment. Pts received fruquintinib (3mg, QD, PO, Q4W) in combination with mFOLFOX6/FOLFIRI (Q2W) for up to 8 cycles. Pts with SD or above were followed by maintenance therapy (fruquintinib 3mg, QD, PO, Q4W, capecitabine 850mg/m2, BID, PO, D1-7, D15-21, Q4W) until disease progression or intolerable toxicity. The primary endpoint was ORR, secondary endpoints included DCR, PFS, OS and safety.
Results
At updated analysis (cutoff: April 20, 2023), 37 pts were enrolled (median age 56, 18 males, 6 with right half colon cancer, 15 harboring RAS mutations, 18 with liver metastases). For 30 pts who were in efficacy analysis, 23 achieved PR (76.67%), 6 achieved SD (20%), resulting in an ORR of 76.67% and a DCR of 96.67%. At a median follow-up of 7.49 mo, 2 pts underwent surgical resection, 21 pts were still in treatment, and median PFS had not yet reached. Safety profile exhibited that the regimen was tolerable and mainly grade 1/2. Grade 3 TRAEs were neutrophil count decreased (23.33%), leukopenia (10%), GGT increased and hypertension accounted for 6.67% respectively, AST increased (3.33%). No pts have serious adverse events.
Conclusions
Updated analysis of this study data further support current combination therapy with fruquintinib plus mFOLFOX6/FOLFIRI as the first-line therapy followed by fruquintinib plus capecitabine maintenance for advanced mCRC pts, which shows durable response and a favorable long-term safety profile. The study is still ongoing.
Clinical trial identification
NCT05004441.
Editorial acknowledgement
Legal entity responsible for the study
The authors.
Funding
Has not received any funding.
Disclosure
All authors have declared no conflicts of interest.
Resources from the same session
570P - Subclasses of microsatellite-instability colorectal cancer with unique molecular features and immune cell infiltration patterns
Presenter: Kui Wu
Session: Poster session 10
571P - Artificial intelligence-powered analysis of tumor lymphocytes infiltration: A translational analysis of AtezoTRIBE trial
Presenter: Martina Carullo
Session: Poster session 10
572P - Neoantigen heterogeneity among subtypes in colorectal cancer
Presenter: Fuqiang Li
Session: Poster session 10
574P - Comparative analysis of the tumor immune microenvironment (TIME) in primary and metastatic sites of microsatellite stable (MSS) and microsatellite instability-high (MSI) colorectal cancer
Presenter: Marwan Fakih
Session: Poster session 10
575P - Impact of immunological alterations and post-operative biomarkers on long-term outcomes in patients with locally advanced rectal cancer: Results from the STAR-01 study cohort
Presenter: Francesca Negri
Session: Poster session 10
576P - Prognostic values of a modified diagnostic biopsy-adapted immunoscore based on double immunohistochemical staining in patients with locally advanced rectal cancer
Presenter: Qiang Zeng
Session: Poster session 10
577P - Systematically assessing the intratissue microbiota in 937 patients with colorectal cancer
Presenter: Huanzi Zhong
Session: Poster session 10
578P - Tissue-resident microbiota characterization in colorectal cancer metastases
Presenter: Philippe Stevens
Session: Poster session 10
579P - A clinico-imaging predictive artificial intelligence model of relapse in colon cancer using baseline CT scans
Presenter: América Bueno Gómez
Session: Poster session 10