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首页> 外文期刊>Clinical and experimental metastasis >Mena invasive (Mena(INV)) and Mena11a isoforms play distinct roles in breast cancer cell cohesion and association with TMEM.
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Mena invasive (Mena(INV)) and Mena11a isoforms play distinct roles in breast cancer cell cohesion and association with TMEM.

机译:Mena入侵(Mena(INV))和Mena11a同工型在乳腺癌细胞凝聚力和与TMEM的关联中起不同的作用。

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摘要

Mena, an actin regulatory protein, functions at the convergence of motility pathways that drive breast cancer cell invasion and migration in vivo. The tumor microenvironment spontaneously induces both increased expression of the Mena invasive (Mena(INV)) and decreased expression of Mena11a isoforms in invasive and migratory tumor cells. Tumor cells with this Mena expression pattern participate with macrophages in migration and intravasation in mouse mammary tumors in vivo. Consistent with these findings, anatomical sites containing tumor cells with high levels of Mena expression associated with perivascular macrophages were identified in human invasive ductal breast carcinomas and called TMEM. The number of TMEM sites positively correlated with the development of distant metastasis in humans. Here we demonstrate that mouse mammary tumors generated from EGFP-Mena(INV) expressing tumor cells are significantly less cohesive and have discontinuous cell-cell contacts compared to Mena11a xenografts. Using the mouse PyMT model we show that metastatic mammary tumors express 8.7 fold more total Mena and 7.5 fold more Mena(INV) mRNA than early non-metastatic ones. Furthermore, Mena(INV) expression in fine needle aspiration biopsy (FNA) samples of human invasive ductal carcinomas correlate with TMEM score while Mena11a does not. These results suggest that Mena(INV) is the isoform associated with breast cancer cell discohesion, invasion and intravasation in mice and in humans. They also imply that Mena(INV) expression and TMEM score measure related aspects of a common tumor cell dissemination mechanism and provide new insight into metastatic risk.
机译:Mena是一种肌动蛋白调节蛋白,在促进乳腺癌细胞在体内侵袭和迁移的运动途径的融合中起作用。肿瘤微环境自发地诱导侵袭性和迁移性肿瘤细胞中侵袭性Mena(Mena(INV))表达的增加和Mena11a亚型的表达降低。具有这种Mena表达模式的肿瘤细胞与巨噬细胞在体内参与小鼠乳腺肿瘤的迁移和血管内浸润。与这些发现一致的是,在人浸润性导管乳腺癌中鉴定出包含与血管周巨噬细胞相关的高Mena表达水平的肿瘤细胞的解剖部位,称为TMEM。 TMEM位点的数量与人类远处转移的发展呈正相关。在这里,我们证明了与Mena11a异种移植物相比,从表达EGFP-Mena(INV)的肿瘤细胞产生的小鼠乳腺肿瘤的凝聚力显着降低,并且具有不连续的细胞接触。使用小鼠PyMT模型,我们发现与早期非转移性乳腺癌相比,转移性乳腺肿瘤表达的总Mena含量高8.7倍,Mena(INV)mRNA含量高7.5倍。此外,人类侵袭性导管癌的细针穿刺活检(FNA)样品中的Mena(INV)表达与TMEM评分相关,而Mena11a与TMEM得分无关。这些结果表明,Mena(INV)是与小鼠和人类的乳腺癌细胞脱落,侵袭和血管内浸润相关的同工型。他们还暗示,Mena(INV)表达和TMEM评分可衡量常见肿瘤细胞传播机制的相关方面,并提供对转移风险的新见解。

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