PO.EN01.01 · 内分泌肿瘤

TGFbeta Induction: An essential tumor suppressive arm of next generation SERDs in ER+ breast cancer models in vitro

海报缩略图:TGFbeta Induction: An essential tumor suppressive arm of next generation SERDs in ER+ breast cancer models in vitro
编号 2285 展板 7 时间 4/20 09:00–12:00 区域 Section 34 主讲 Kareem Heslop, PhD
分会场 Hormone Receptor Signaling and Therapeutic Targeting
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作者与单位

Kareem Heslop1, Jackson Liang1, Steffan Vartanian2, Jinchu Vijay1, Liang-Fu Chen1, Marc Hafner3, Michael Costa1, Ciara Metcalfe4

1Discovery Oncology, Genentech, Inc., South San Francisco, CA,2Genentech, SOUTH SAN FRANCISCO, CA,3Scientist, Genentech, South San Francisco, CA,4Genentech, Inc., South San Francisco, CA

摘要 Abstract

Breast cancer is the most diagnosed cancer globally, with a significant need for improved treatments for the most prevalent Estrogen Receptor alpha (ER)-positive subtype, where ER signaling drives cell proliferation.The next-generation oral Selective ER antagonist and degrader (SERD), giredestrant, is a potent investigational agent that robustly suppresses tumor cell proliferation. However, primary and acquired resistance pose a major challenge to all endocrine therapies including oral SERDs, necessitating a deeper understanding of resistance mechanisms. In a comprehensive whole-genome CRISPR screen, we sought to identify genetic perturbations that confer a growth advantage in the presence of giredestrant. Notably, knockout of multiple TGFbeta signaling components (TGFbeta3, SMAD4, IPO8, TGFbetaR2) consistently freed ER+ cells from giredestrant-induced cell cycle arrest. We establish an unexpected autocrine mechanism: by suppressing the ER pathway, giredestrant induces the expression and signaling of the tumor suppressor TGFbeta3. This induced TGFbeta signaling then elevates CDKN1A (p21) levels, which precedes the inhibition of its natural target, CDK2. We demonstrate that this TGFbeta→p21-|CDK2 axis is necessary for giredestrant to achieve its maximal inhibitory effect in vitro. Molecular profiling confirmed CDKN1A was among the most significantly suppressed genes when TGFbeta signaling was inhibited in combination with giredestrant. Crucially, combining giredestrant and a TGFbeta inhibitor led to resistance, but this was partially overcome by a combination of CDK4/6 and CDK2 inhibition. This finding shows that CDK4/6/2 blockade can bypass, in-part, the requirement for the p21 cell cycle brake. Collectively, our results reveal that giredestrant's in vitro efficacy relies on an autocrine TGFbeta loop to mediate the necessary G1 arrest. The inhibition of TGFbeta creates a resistance mechanism by neutralizing this essential tumor-suppressive signaling component.
利益披露 Disclosure
K. Heslop, Genentech Employment. J. Liang, Genentech Employment. J. Vijay, Genentech Employment. L. Chen, Genentech Employment. M. Costa, Genentech Employment.

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