BBO-10203 inhibits tumor growth without inducing hyperglycemia by blocking RAS-PI3Kα interaction

Dhirendra K. Simanshu; Rui Xu; James P. Stice; Daniel J. Czyzyk; Siyu Feng; John-Paul Denson; Erin Riegler; Yue Yang; Cathy Zhang; Sofia Donovan; Bryan D. Smith; Maria Abreu Blanco; Ming Chen; Cindy Feng; Lijuan Fu; Dana Rabara; Lucy C. Young; Marcin Dyba; W. B. Yan; Kenneth Lin; Samar Ghorbanpoorvalukolaie; Erik K. Larsen; Wafa Malik; Allison Champagne; Katie Parker; Jin Hyun Ju; Stevan Jeknic; Dominic Esposito; David M. Turner; Felice C. Lightstone; Bin Wang; Paul M. Wehn; Keshi Wang; Andrew G. Stephen; Anna E. Maciag; Aaron N. Hata; Kerstin W. Sinkevicius; Dwight V. Nissley; Eli M. Wallace; Frank McCormick; Pedro J. Beltran

doi:10.1126/science.adq2004

BBO-10203 inhibits tumor growth without inducing hyperglycemia by blocking RAS-PI3Kα interaction

Dhirendra K. Simanshu(Leidos (United States)), Rui Xu(BridgeBio (United States)), James P. Stice(BridgeBio (United States)), Daniel J. Czyzyk(Leidos (United States)), Siyu Feng(BridgeBio (United States)), John-Paul Denson(Leidos (United States)), Erin Riegler(BridgeBio (United States)), Yue Yang(Lawrence Livermore National Laboratory), Cathy Zhang(BridgeBio (United States)), Sofia Donovan(BridgeBio (United States)), Bryan D. Smith(Leidos (United States)), Maria Abreu Blanco(Leidos (United States)), Ming Chen(BridgeBio (United States)), Cindy Feng(BridgeBio (United States)), Lijuan Fu(BridgeBio (United States)), Dana Rabara(Leidos (United States)), Lucy C. Young(University of California, San Francisco), Marcin Dyba(Leidos (United States)), W. B. Yan(Leidos (United States)), Kenneth Lin(BridgeBio (United States)), Samar Ghorbanpoorvalukolaie(Massachusetts General Hospital), Erik K. Larsen(Leidos (United States)), Wafa Malik(Massachusetts General Hospital), Allison Champagne(Leidos (United States)), Katie Parker(Massachusetts General Hospital), Jin Hyun Ju(Bridge Pharma (United States)), Stevan Jeknic(Bridge Pharma (United States)), Dominic Esposito(Leidos (United States)), David M. Turner(Leidos (United States)), Felice C. Lightstone(Lawrence Livermore National Laboratory), Bin Wang(BridgeBio (United States)), Paul M. Wehn(BridgeBio (United States)), Keshi Wang(BridgeBio (United States)), Andrew G. Stephen(Leidos (United States)), Anna E. Maciag(Leidos (United States)), Aaron N. Hata(Massachusetts General Hospital), Kerstin W. Sinkevicius(BridgeBio (United States)), Dwight V. Nissley(Leidos (United States)), Eli M. Wallace(BridgeBio (United States)), Frank McCormick(Leidos (United States)), Pedro J. Beltran(BridgeBio (United States))

Science

June 12, 2025

10.1126/science.adq2004

Cited by 24

Abstract

BBO-10203 is an orally available drug that covalently and specifically binds to the rat sarcoma (RAS)–binding domain of phosphoinositide 3-kinase α (PI3Kα), preventing its activation by HRAS, NRAS, and KRAS. It inhibited PI3Kα activation in tumors with oncogenic mutations in KRAS or PIK3CA and in tumors with human epidermal growth factor receptor 2 (HER2) amplification or overexpression. In preclinical models, BBO-10203 caused significant tumor growth inhibition across multiple tumor types and showed enhanced efficacy in combination with inhibitors of cyclin-dependent kinase 4/6 (CDK4/6), estrogen receptor (ER), HER2, and KRAS-G12C mutant, including in tumors harboring mutations in Kelch-like ECH-associated protein 1 (KEAP1) and serine/threonine kinase 11 (STK11). Notably, these antitumor effects occurred without inducing hyperglycemia, because insulin signaling does not depend on RAS-mediated PI3Kα activation to promote glucose uptake.

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