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NOTCH1 PEST domain variants are responsive to standard of care treatments despite distinct transformative properties in a breast cancer model

机译:NOTCH1 PEST 结构域变体对标准护理治疗有反应尽管在乳腺癌模型中具有明显的转化特性

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摘要

Activating variants in the PEST region of NOTCH1 have been associated with aggressive phenotypes in human cancers, including triple-negative breast cancer (TNBC). Previous studies suggested that PEST domain variants in TNBC patients resulted in increased cell proliferation, invasiveness, and decreased overall survival. In this study, we assess the phenotypic transformation of activating NOTCH1 variants and their response to standard of care therapies. AAV-mediated gene targeting was used to isogenically incorporate 3 NOTCH1 variants, including a novel TNBC frameshift variant, in two non-tumorigenic breast epithelial cell lines, MCF10A and hTERT-IMEC. Two different variants at the NOTCH1 A2241 site (A2441fs and A2441T) both demonstrated increased transformative properties when compared to a non-transformative PEST domain variant (S2523L). These phenotypic changes include proliferation, migration, anchorage-independent growth, and MAPK pathway activation. In contrast to previous studies, activating NOTCH1 variants did not display sensitivity to a gamma secretase inhibitor (GSI) or resistance to chemotherapies. This study demonstrates distinct transformative phenotypes are specific to a given variant within NOTCH1 and these phenotypes do not correlate with sensitivities or resistance to chemotherapies or GSIs. Although previous studies have suggested NOTCH1 variants may be prognostic for TNBC, our study does not demonstrate prognostic ability of these variants and suggests further characterization would be required for clinical applications.
机译:NOTCH1 PEST 区域的激活变异与人类癌症(包括三阴性乳腺癌 (TNBC))中的侵袭性表型有关。先前的研究表明,TNBC 患者的 PEST 结构域变异导致细胞增殖增加、侵袭性和总生存期降低。在这项研究中,我们评估了激活 NOTCH1 变体的表型转化及其对标准护理疗法的反应。AAV 介导的基因靶向用于在两种非致瘤性乳腺上皮细胞系 MCF10A 和 hTERT-IMEC 中等基因掺入 3 个 NOTCH1 变体,包括一种新的 TNBC 移码变体。与非转化性 PEST 结构域变体 (S2523L) 相比,NOTCH1 A2241 位点的两种不同变体(A2441fs 和 A2441T)均表现出增强的转化特性。这些表型变化包括增殖、迁移、不依赖锚定的生长和 MAPK 通路激活。与以前的研究相比,激活 NOTCH1 变体未表现出对 γ 分泌酶抑制剂 (GSI) 的敏感性或对化疗的耐药性。这项研究表明,不同的转化表型对 NOTCH1 中的给定变体具有特异性,并且这些表型与对化疗或 GSI 的敏感性或耐药性无关。尽管先前的研究表明 NOTCH1 变体可能预后为 TNBC,但我们的研究并未证明这些变体的预后能力,并表明临床应用需要进一步的表征。

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