Kinome-Focused CRISPR-Cas9 Screens in African Ancestry Patient-Derived Breast Cancer Organoids Identify Essential Kinases and Synergy of EGFR and FGFR1 Inhibition

基诺美 清脆的 类有机物 生物 靶向治疗 癌症 遗传筛选 癌症研究 生命银行 激酶 乳腺癌 曲美替尼 计算生物学 生物信息学 医学 MAPK/ERK通路 遗传学 基因 表型
作者
Florencia P. Madorsky Rowdo,Rachel Martini,Sarah Ackermann,Colin P. Tang,Marvel Tranquille,Adriana Irizarry,Ilkay Us,Omar Alawa,Jenna E. Moyer,Michael Sigouros,John Nguyen,Majd Al Assaad,Esther Cheng,Paula S. Ginter,Jyothi Manohar,Brian Stonaker,Richard Boateng,Joseph K. Oppong,Ernest Adjei,Baffour Awuah,Ishmael Kyei,Francis Aitpillah,Michael O. Adinku,Kwasi Ankomah,Ernest Osei‐Bonsu,Kofi K. Gyan,Syed A. Hoda,Lisa A. Newman,Juan Miguel Mosquera,Andrea Sboner,Olivier Elemento,Lukas E. Dow,Melissa B. Davis,M. Laura Martín
出处
期刊:Cancer Research [American Association for Cancer Research]
卷期号:85 (3): 551-566 被引量:1
标识
DOI:10.1158/0008-5472.can-24-0775
摘要

Abstract Precision medicine approaches to cancer treatment aim to exploit genomic alterations that are specific to individual patients to tailor therapeutic strategies. Yet, some targetable genes and pathways are essential for tumor cell viability even in the absence of direct genomic alterations. In underrepresented populations, the mutational landscape and determinants of response to existing therapies are poorly characterized because of limited inclusion in clinical trials and studies. One way to reveal tumor essential genes is with genetic screens. Most screens are conducted on cell lines that bear little resemblance to patient tumors, after years of culture under nonphysiologic conditions. To address this problem, we aimed to develop a CRISPR screening pipeline in three-dimensionally grown patient-derived tumor organoid (PDTO) models. A breast cancer PDTO biobank that focused on underrepresented populations, including West African patients, was established and used to conduct a negative-selection kinome-focused CRISPR screen to identify kinases essential for organoid growth and potential targets for combination therapy with EGFR or MEK inhibitors. The screen identified several previously unidentified kinase targets, and the combination of FGFR1 and EGFR inhibitors synergized to block organoid proliferation. Together, these data demonstrate the feasibility of CRISPR-based genetic screens in patient-derived tumor models, including PDTOs from underrepresented patients with cancer, and identify targets for cancer therapy. Significance: Generation of a breast cancer patient-derived tumor organoid biobank focused on underrepresented populations enabled kinome-focused CRISPR screening that identified essential kinases and potential targets for combination therapy with EGFR or MEK inhibitors. See related commentary by Trembath and Spanheimer, p. 407
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