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Tissue-specific and SRSF1-dependent splicing of fibronectin, a matrix protein that controls host cell invasion

机译:纤连蛋白的组织特异性和SRSF1依赖性剪接,一种控制宿主细胞入侵的基质蛋白

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Cell invasion targets specific tissues in physiological placental implantation and pathological metastasis, which raises questions about how this process is controlled. We compare dermis and endometrium capacities to support trophoblast invasion, using matching sets of human primary fibroblasts in a coculture assay with human placental explants. Substituting endometrium, the natural trophoblast target, with dermis dramatically reduces trophoblast interstitial invasion. Our data reveal that endometrium expresses a higher rate of the fibronectin (FN) extra type III domain A+ (EDA+) splicing isoform, which displays stronger matrix incorporation capacity. We demonstrate that the high FN content of the endometrium matrix, and not specifically the EDA domain, supports trophoblast invasion by showing that forced incorporation of plasma FN (EDA–) promotes efficient trophoblast invasion. We further show that the serine/arginine-rich protein serine/arginine-rich splicing factor 1 (SRSF1) is more highly expressed in endometrium and, using RNA interference, that it is involved in the higher EDA exon inclusion rate in endometrium. Our data therefore show a mechanism by which tissues can be distinguished, for their capacity to support invasion, by their different rates of EDA inclusion, linked to their SRSF1 protein levels. In the broader context of cancer pathology, the results suggest that SRSF1 might play a central role not only in the tumor cells, but also in the surrounding stroma.
机译:细胞入侵针对生理性胎盘植入和病理转移中的特定组织,这引发了有关如何控制该过程的问题。我们在与人胎盘外植体共培养的实验中,使用相匹配的人类原代成纤维细胞组,比较了真皮和子宫内膜支持滋养细胞入侵的能力。用真皮替代天然的滋养层靶标子宫内膜,可显着减少滋养层间质的侵袭。我们的数据显示,子宫内膜表达更高的纤连蛋白(FN)额外的III型域A +(EDA +)剪接同工型,显示出更强的基质结合能力。我们通过显示血浆FN(EDA–)的强制掺入促进了滋养层的有效入侵,证明了子宫内膜基质的高FN含量(而不是EDA域)特别支持滋养层的入侵。我们进一步表明,富含丝氨酸/精氨酸的蛋白丝氨酸/富含精氨酸的剪接因子1(SRSF1)在子宫内膜中更高的表达,并且使用RNA干扰,它参与子宫内膜中较高的EDA外显子包涵率。因此,我们的数据显示了一种机制,通过该机制,可以通过与它们的SRSF1蛋白水平相关的不同的EDA包含率来区分组织的支持入侵能力。在更广泛的癌症病理学背景下,结果表明SRSF1可能不仅在肿瘤细胞中而且在周围的基质中都起着核心作用。

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