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A holistic approach to dissecting SPARC family protein complexity reveals FSTL-1 as an inhibitor of pancreatic cancer cell growth

机译:剖析SPARC家庭蛋白质复杂性的整体方法显示FSTL-1可作为胰腺癌细胞生长的抑制剂

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摘要

SPARC is a matricellular protein that is involved in both pancreatic cancer and diabetes. It belongs to a wider family of proteins that share structural and functional similarities. Relatively little is known about this extended family, but evidence of regulatory interactions suggests the importance of a holistic approach to their study. We show that Hevin, SPOCKs, and SMOCs are strongly expressed within islets, ducts, and blood vessels, suggesting important roles for these proteins in the normal pancreas, while FSTL-1 expression is localised to the stromal compartment reminiscent of SPARC. In direct contrast to SPARC, however, FSTL-1 expression is reduced in pancreatic cancer. Consistent with this, FSTL-1 inhibited pancreatic cancer cell proliferation. The complexity of SPARC family proteins is further revealed by the detection of multiple cell-type specific isoforms that arise due to a combination of post-translational modification and alternative splicing. Identification of splice variants lacking a signal peptide suggests the existence of novel intracellular isoforms. This study underlines the importance of addressing the complexity of the SPARC family and provides a new framework to explain their controversial and contradictory effects. We also demonstrate for the first time that FSTL-1 suppresses pancreatic cancer cell growth.
机译:SPARC是一种参与胰腺癌和糖尿病的母体细胞蛋白。它属于共享结构和功能相似性的更广泛的蛋白质家族。对这个大家庭了解的相对较少,但是监管相互作用的证据表明,采用整体方法进行研究非常重要。我们显示,Hevin,SPOCK和SMOC在胰岛,导管和血管中强烈表达,表明这些蛋白质在正常胰腺中起着重要作用,而FSTL-1表达则局限于SPARC的间质隔室。与SPARC直接相反,在胰腺癌中FSTL-1表达降低。与此相一致,FSTL-1抑制胰腺癌细胞的增殖。通过检测由于翻译后修饰和选择性剪接相结合而产生的多种细胞类型特异性同工型,进一步揭示了SPARC家族蛋白的复杂性。缺乏信号肽的剪接变体的鉴定表明存在新的细胞内亚型。这项研究强调了解决SPARC系列复杂性的重要性,并提供了一个新的框架来解释其争议性和矛盾性的影响。我们还首次证明FSTL-1抑制胰腺癌细胞的生长。

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