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The integrin cytoplasmic-tail motif EKQKVDLSTDC is sufficient to promote tumor cell invasion mediated by matrix metalloproteinase (MMP)-2 or MMP-9

机译:整合素细胞质尾基序EKQKVDLsTDC足以促进基质金属蛋白酶(mmp)-2或mmp-9介导的肿瘤细胞侵袭

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摘要

Integrins promote cellular invasion through a combination of activities, including adhesion to an extracellular matrix ligand, which result in the generation of intracellular signals that lead to changes in cell behavior. Until now, there have been no data that identify a particular region of the cytoplasmic tail of integrin subunits as being responsible specifically for promoting the invasive activity of tumor cells. In this report, we show that amino acids with the sequence EKQKVDLSTDC, which are the C-terminal residues of the integrin β6 subunit, promote αvβ6-dependent invasion in a matrix metalloproteinase (MMP)-9-dependent fashion. This same peptide sequence, when expressed at the cytoplasmic end of the β3 integrin subunit, was able to enhance αvβ3-mediated invasive and enzymatic activity of tumor cells in an MMP-2-dependent fashion. Our results show that these 11 amino acids, when expressed at the C terminus of the β subunit, are responsible for regulating the activity of invasion-promoting degradative enzymes, whereas the specific MMP involved in this cellular behavior is dependent on the context of the remainder of the β integrin subunit.
机译:整联蛋白通过包括与细胞外基质配体的粘附在内的一系列活动来促进细胞的侵袭,从而导致细胞内信号的产生,从而导致细胞行为的改变。迄今为止,还没有数据表明整联蛋白亚基的胞质尾部的特定区域特别负责促进肿瘤细胞的侵袭活性。在此报告中,我们显示了具有序列EKQKVDLSTDC的氨基酸,它们是整联蛋白β6亚基的C末端残基,以基质金属蛋白酶(MMP)-9依赖性的方式促进αvβ6依赖性入侵。当在β3整联蛋白亚基的细胞质末端表达时,相同的肽序列能够以MMP-2依赖性的方式增强肿瘤细胞的αvβ3介导的侵袭和酶促活性。我们的结果表明,这11个氨基酸在β亚基的C末端表达时,负责调节促侵袭降解酶的活性,而参与这种细胞行为的特定MMP则取决于其余的背景β整联蛋白亚基。

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