PO.CT01.02 · 临床试验

Initial clinical and translational results and selection of recommended phase 2 dose (RP2D) from START-002: A Phase 1b/2 study of invikafusp alfa, a first-in-class dual T-cell agonist, in combination with sacituzumab govitecan in metastatic triple-negative or HR+/HER2- breast cancer

海报缩略图:Initial clinical and translational results and selection of recommended phase 2 dose (RP2D) from START-002: A Phase 1b/2 study of invikafusp alfa, a first-in-class dual T-cell agonist, in combination with sacituzumab govitecan in metastatic triple-negative or HR+/HER2- breast cancer
编号 CT045 展板 5 时间 4/20 09:00–12:00 区域 Section 50 主讲 Steven J Isakoff, MD, PhD
分会场 First-in-Human Phase I Clinical Trials
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作者与单位

Steven J Isakoff1, Anastasia Martynova2, Philippe L Bedard3, Margaret E Gatti-Mays4, Nathalie LeVasseur5, Andreas Varkaris1, William Randolph6, Karunya Srinivasan6, Shannon McCue6, Zhenming Shun6, Ke Liu6, Zhen Su6, Kevin Chin6, Virginia Kaklamani7, Kelly McCann8, Erika Hamilton9

1Mass General Cancer Center, Boston, MA,2USC Norris Comprehensive Cancer Center, Los Angeles, MA,3Princess Margaret Cancer Centre, Toronto, ON, Canada,4The Ohio State University Comprehensive Cancer Center, Columbus, OH,5BC Cancer Vancouver Centre, Vancouver, BC, Canada,6Marengo Therapeutics, Cambridge, MA,7UT Health San Antonio, San Antonio, TX,8UCLA Health Jonsson Cancer Center, Los Angeles, CA,9Sarah Cannon Research Institute, Nashville, TN

摘要 Abstract

Background: Invikafusp alfa (invika), a first-in-class (FIC) dual T-cell agonist, as monotherapy, showed 1) selective activation and expansion of mainly CD8⁺ Vbeta6 T cells with a central memory phenotype in peripheral blood and tumor; 2) confirmed objective responses in patients with anti-PD(L)1-resistance across 7 different solid tumors including TNBC. Preclinical tumor models including breast cancer showed combining invika with cytotoxic agents enhanced antitumor activity. Sacituzumab govitecan (SG), a TROP-2-directed antibody-drug conjugate (ADC), is approved for metastatic TNBC and HR+/HER2- mBC. Published data suggest that ADCs enhance tumor immunogenicity, providing further rationale for combination with invika. Methods: START-002 is an ongoing Phase 1b/2 study evaluating invika in combination with SG in mTNBC or HR+/HER2- mBC. Phase 1b had two cohorts (invika at 0.04 or 0.08 mg/kg) in combination with SG (10 mg/kg). After recommended Phase 2 dose (RP2D) selection, Phase 2 expansion cohorts in mTNBC and HR+/HER2- mBC was initiated. Results: Translational and Clinical Pharmacology (Phase 1b; n = 8): Nanostring showed selective TRBV6 expansion (~10% to ~40% of total T cells) in all patients at both 0.04 and 0.08 mg/kg of invika peaking ~ 7 days post the 1st dose, similar to what was seen with invika monotherapy. Dose-dependent increases in Cmax and AUC similar to monotherapy were observed, indicating SG did not impact invika exposure. Initial Clinical Results (Phase 1b/2): In 22 patients (9 TNBC and 13 HR+/HER2- mBC) treated, the most common adverse events were neutropenia, diarrhea, alopecia, and stomatitis (SG-related); Grade 1& 2 cytokine release syndrome (invika-related); and fatigue and thrombocytopenia (attributed to either or both). Among 10 patients (4 TNBC and 6 HR+/HER2- mBC) who had at least 1 post treatment tumor evaluation, two HR+/HER2- patients had confirmed partial responses, one TNBC patient had an unconfirmed complete response, and six patients had stable disease (90% disease control rate). Five of 10 patients remained on treatment for ≥5 months. Invika 0.08 mg/kg in combination with SG 10 mg/kg was selected as RP2D. Conclusions: This first-in-human study demonstrates 1) the feasibility and safety of invika, a FIC dual T-cell agonist, in combination with SG, a standard-of-care ADC; 2) dose-dependent expansion of Vbeta6 T cells; 3) antitumor activity, including confirmed responses, in heavily pre-treated mBC patients. Phase 2 expansion is ongoing to further study the efficacy and safety of this novel combination in patients with mBC.
利益披露 Disclosure
S. Isakoff, None.. A. Martynova, None.. P. Bedard, None.. M. Gatti-Mays, None.. N. LeVasseur, None.. A. Varkaris, None. W. Randolph, Marengo Therapeutics Employment. K. Srinivasan, Marengo Therapeutics Employment. S. McCue, Marengo Therapeutics Employment. Z. Shun, Marengo Therapeutics Employment. K. Liu, Marengo Therapeutics Employment. Z. Su, Marengo Therapeutics Employment. K. Chin, Marengo Therapeutics Employment. V. Kaklamani, None.. K. McCann, None.. E. Hamilton, None.

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