Tumor suppressor pathways shape EGFR-driven lung tumor progression and response to treatment

肿瘤抑制通路影响EGFR驱动的肺肿瘤进展和治疗反应。

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Abstract

In vivo modeling combined with CRISPR/Cas9-mediated somatic genome editing has contributed to elucidating the functional importance of specific genetic alterations in human tumors. Our recent work uncovered tumor suppressor pathways that affect EGFR-driven lung tumor growth and sensitivity to tyrosine kinase inhibitors and reflect the mutational landscape and treatment outcomes in the human disease.

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