Abstract P3-09-01: MYC dysregulates mitotic spindle function in triple-negative breast cancer creating a dependency on TPX2

A. Goga, Julia Rohrberg, Alexandra Corella, Moufida Taileb, S. Kilinc, Marie-Lena Jokisch, Roman Camarda, A. Zhou, S. Balakrishnan, An-Chen Chang, H. Klein-Connolly
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引用次数: 0

Abstract

Tumors that overexpress the MYC oncogene, including most receptor triple-negative breast cancers, frequently demonstrate aneuploidy, numerical chromosome alterations associated with highly aggressive cancers. Aneuploidy is also associated with rapid tumor evolution and poor patient outcome. We identify that MYC overexpression induces reversible defects in microtubule nucleation and mitotic spindle assembly, in TNBCs and other epithelial cells, promoting chromosome segregation defects, micronuclei and chromosomal instability (CIN). High TPX2 expression is permissive for mitotic spindle assembly and chromosome segregation in cells with MYC overexpression; whereas TPX2 depletion blocks mitotic progression, induces cell death and prevents tumor growth. Attenuating MYC expression reverses mitotic defects, even in established breast tumor cell lines, implicating an ongoing role for high MYC in the persistence of CIN in cancers. Our studies implicate the MYC oncogene as a regulator of spindle assembly and identify a new MYC-TPX2 synthetic-lethal interaction in TNBC that could represent a future therapeutic strategy in MYC-overexpressing cancers. Moreover, our studies suggest that blocking MYC activity can attenuate the emergence of CIN and tumor evolution. Citation Format: Goga A, Rohrberg J, Corella A, Taileb M, Kilinc S, Jokisch M-L, Camarda R, Zhou A, Balakrishnan S, Chang AN, Klein-Connolly H. MYC dysregulates mitotic spindle function in triple-negative breast cancer creating a dependency on TPX2 [abstract]. In: Proceedings of the 2018 San Antonio Breast Cancer Symposium; 2018 Dec 4-8; San Antonio, TX. Philadelphia (PA): AACR; Cancer Res 2019;79(4 Suppl):Abstract nr P3-09-01.
摘要P3-09-01: MYC在三阴性乳腺癌中有丝分裂纺锤体功能失调,产生对TPX2的依赖
过度表达MYC癌基因的肿瘤,包括大多数受体三阴性乳腺癌,经常表现出非整倍体,与高度侵袭性癌症相关的数字染色体改变。非整倍体还与肿瘤的快速演变和患者预后差有关。我们发现MYC过表达诱导tnbc和其他上皮细胞中微管成核和有丝分裂纺锤体组装的可逆缺陷,促进染色体分离缺陷、微核和染色体不稳定性(CIN)。在MYC过表达的细胞中,TPX2的高表达有利于有丝分裂纺锤体组装和染色体分离;而TPX2缺失阻断有丝分裂进程,诱导细胞死亡并阻止肿瘤生长。降低MYC表达可逆转有丝分裂缺陷,即使在已建立的乳腺肿瘤细胞系中也是如此,这意味着高MYC在癌症中CIN的持续存在中起着持续的作用。我们的研究表明MYC癌基因是纺锤体组装的调节因子,并在TNBC中发现了一种新的MYC- tpx2合成致死相互作用,这可能代表未来MYC过表达癌症的治疗策略。此外,我们的研究表明,阻断MYC活性可以减轻CIN的出现和肿瘤的发展。引用格式:Goga A, Rohrberg J, Corella A, Taileb M, Kilinc S, Jokisch M- l, Camarda R, Zhou A, Balakrishnan S, Chang AN, Klein-Connolly H.三阴性乳腺癌MYC有丝分裂纺锤体功能异常产生TPX2依赖[摘要]。2018年圣安东尼奥乳腺癌研讨会论文集;2018年12月4-8日;费城(PA): AACR;中国癌症杂志2019;79(4增刊):P3-09-01。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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