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Let-7 microRNA controls invasion-promoting lysosomal changes via the oncogenic transcription factor myeloid zinc finger-1

机译:Let-7 microRNA通过致癌转录因子髓样锌指1来控制促进入侵的溶酶体变化

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Cancer cells utilize lysosomes for invasion and metastasis. Myeloid Zinc Finger1 (MZF1) is an ErbB2-responsive transcription factor that promotes invasion of breast cancer cells via upregulation of lysosomal cathepsins B and L. Here we identify let-7 microRNA, a well-known tumor suppressor in breast cancer, as a direct negative regulator of MZF1. Analysis of primary breast cancer tissues reveals a gradual upregulation of MZF1 from normal breast epithelium to invasive ductal carcinoma and a negative correlation between several let-7 family members and MZF1 mRNA, suggesting that the inverse regulatory relationship between let-7 and MZF1 may play a role in the development of invasive breast cancer. Furthermore, we show that MZF1 regulates lysosome trafficking in ErbB2-positive breast cancer cells. In line with this, MZF1 depletion or let-7 expression inhibits invasion-promoting anterograde trafficking of lysosomes and invasion of ErbB2-expressing MCF7 spheres. The results presented here link MZF1 and let-7 to lysosomal processes in ErbB2-positive breast cancer cells that in non-cancerous cells have primarily been connected to the transcription factor EB. Identifying MZF1 and let-7 as regulators of lysosome distribution in invasive breast cancer cells, uncouples cancer-associated, invasion-promoting lysosomal alterations from normal lysosomal functions and thus opens up new possibilities for the therapeutic targeting of cancer lysosomes.
机译:癌细胞利用溶酶体进行侵袭和转移。髓样锌指1(MZF1)是一种ErbB2反应性转录因子,可通过上调溶酶体组织蛋白酶B和L来促进乳腺癌细胞的侵袭。在这里,我们将let-7 microRNA(一种在乳腺癌中广为人知的肿瘤抑制因子)鉴定为直接MZF1的负调节器。对原发性乳腺癌组织的分析表明,MZF1从正常乳腺上皮到浸润性导管癌逐渐上调,并且几个let-7家族成员与MZF1 mRNA之间呈负相关,这表明let-7和MZF1之间的反调控关系可能发挥了作用。在浸润性乳腺癌发展中的作用。此外,我们显示MZF1调节ErbB2阳性乳腺癌细胞中的溶酶体运输。与此相符,MZF1耗竭或let-7表达抑制溶酶体的促入侵顺行运输和表达ErbB2的MCF7球的入侵。此处显示的结果将MZF1和let-7与ErbB2阳性乳腺癌细胞的溶酶体过程联系起来,而在非癌细胞中,ErbB2阳性乳腺癌细胞主要与转录因子EB相关。将MZF1和let-7鉴定为侵袭性乳腺癌细胞中溶酶体分布的调节剂,可以将癌症相关的,促进侵袭性的溶酶体改变与正常的溶酶体功能脱钩,从而为靶向癌症溶酶体开辟了新的可能性。

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