Phosphoproteomics of patient-derived xenografts identifies targets and markers associated with sensitivity and resistance to EGFR blockade in colorectal cancer

西妥昔单抗 磷酸蛋白质组学 癌症研究 表皮生长因子受体抑制剂 基诺美 结直肠癌 表皮生长因子受体 MAPK/ERK通路 酪氨酸激酶 受体酪氨酸激酶 蛋白激酶B 拉帕蒂尼 生物 癌症 ERBB3型 医学 激酶 信号转导 蛋白激酶A 内科学 细胞生物学 蛋白质磷酸化 曲妥珠单抗 乳腺癌
作者
Robin Beekhof,Andrea Bertotti,Franziska Böttger,Valentina Vurchio,Francesca Cottino,Eugenia R. Zanella,Giorgia Migliardi,Marco Viviani,Elena Grassi,Barbara Lupo,Alex A. Henneman,Jaco C. Knol,Thang V. Pham,Richard de Goeij-de Haas,Sander R. Piersma,Mariëtte Labots,Henk M.W. Verheul,Livio Trusolino,Connie R. Jiménez
出处
期刊:Science Translational Medicine [American Association for the Advancement of Science]
卷期号:15 (709): eabm3687-eabm3687 被引量:30
标识
DOI:10.1126/scitranslmed.abm3687
摘要

Epidermal growth factor receptor (EGFR) is a well-exploited therapeutic target in metastatic colorectal cancer (mCRC). Unfortunately, not all patients benefit from current EGFR inhibitors. Mass spectrometry-based proteomics and phosphoproteomics were performed on 30 genomically and pharmacologically characterized mCRC patient-derived xenografts (PDXs) to investigate the molecular basis of response to EGFR blockade and identify alternative drug targets to overcome resistance. Both the tyrosine and global phosphoproteome as well as the proteome harbored distinctive response signatures. We found that increased pathway activity related to mitogen-activated protein kinase (MAPK) inhibition and abundant tyrosine phosphorylation of cell junction proteins, such as CXADR and CLDN1/3, in sensitive tumors, whereas epithelial-mesenchymal transition and increased MAPK and AKT signaling were more prevalent in resistant tumors. Furthermore, the ranking of kinase activities in single samples confirmed the driver activity of ERBB2, EGFR, and MET in cetuximab-resistant tumors. This analysis also revealed high kinase activity of several members of the Src and ephrin kinase family in 2 CRC PDX models with genomically unexplained resistance. Inhibition of these hyperactive kinases, alone or in combination with cetuximab, resulted in growth inhibition of ex vivo PDX-derived organoids and in vivo PDXs. Together, these findings highlight the potential value of phosphoproteomics to improve our understanding of anti-EGFR treatment and response prediction in mCRC and bring to the forefront alternative drug targets in cetuximab-resistant tumors.
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