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上皮细胞中钙水平的升高会诱导钙结合蛋白迁移抑制因子相关蛋白8(MRP8)和MRP14转位至角蛋白中间丝。

Increase of calcium levels in epithelial cells induces translocation of calcium-binding proteins migration inhibitory factor-related protein 8 (MRP8) and MRP14 to keratin intermediate filaments.

作者信息

Goebeler M, Roth J, van den Bos C, Ader G, Sorg C

机构信息

Institute of Experimental Dermatology, University of Münster, Germany.

出版信息

Biochem J. 1995 Jul 15;309 ( Pt 2)(Pt 2):419-24. doi: 10.1042/bj3090419.

Abstract

Migration inhibitory factor-related protein 8 (MRP8) and MRP14, two S-100-like Ca(2+)-binding proteins, have been described in cells of the epithelial lineage where they are either expressed constitutively (e.g. by mucosal squamous epithelium) or induced during disease (e.g. in keratinocytes during the course of psoriasis). Their biological function, however, is not yet clear. Recent studies have provided evidence that S-100-like proteins may interact with cytoskeletal components; we have therefore studied the biochemical properties and subcellular distribution of MRP8 and MRP14 in epithelial cells. TR146 human squamous carcinoma cells, which were found to express MRP8 and MRP14 in Northern and Western blot studies, were chosen for analysis. Cross-linking experiments using bis(sulphosuccinimidyl)suberate followed by SDS/PAGE and Western blot analysis revealed formation of heteromeric MRP8-MRP14 complexes. On subjecting TR146 cell lysates to two-dimensional gel electrophoresis and Western blotting, four distinct MRP14 isoforms could be identified resembling those described earlier in macrophages. A differential centrifugation technique revealed a Ca(2+)-dependent translocation of MRP8-MRP14 from the cytoplasm to the membrane and the Nonidet P40-insoluble cytoskeletal fraction. Double-label immunofluorescence microscopy of Ca2+ ionophore A23187-stimulated TR146 cells and cytochalasin B and demecolcine cytoskeleton disruption studies identified these structures as keratin intermediate filaments. Ca(2+)-dependent binding of MRP8-MRP14 to keratin filaments was additionally confirmed by an in vitro binding assay. In conclusion, our data suggest that MRP8 and MRP14 may be involved in Ca(2+)-dependent reorganization of cytoskeletal filaments in epithelial cells, which could be of importance for events associated with differentiation and inflammatory activation.

摘要

迁移抑制因子相关蛋白8(MRP8)和MRP14是两种S-100样钙结合蛋白,已在上皮谱系细胞中被描述,它们要么组成性表达(如黏膜鳞状上皮),要么在疾病过程中被诱导表达(如银屑病病程中的角质形成细胞)。然而,它们的生物学功能尚不清楚。最近的研究提供了证据表明S-100样蛋白可能与细胞骨架成分相互作用;因此,我们研究了MRP8和MRP14在上皮细胞中的生化特性和亚细胞分布。在Northern印迹和Western印迹研究中发现表达MRP8和MRP14的TR146人鳞状癌细胞被选作分析对象。使用双(磺基琥珀酰亚胺基)辛二酸酯进行交联实验,随后进行SDS/PAGE和Western印迹分析,结果显示形成了异源二聚体MRP8-MRP14复合物。对TR146细胞裂解物进行二维凝胶电泳和Western印迹分析,可鉴定出四种不同的MRP14异构体,与先前在巨噬细胞中描述的相似。差速离心技术显示MRP8-MRP14从细胞质向膜及不溶于Nonidet P40的细胞骨架部分发生钙依赖性转运。对钙离子载体A23187刺激的TR146细胞进行双标记免疫荧光显微镜检查以及细胞松弛素B和秋水仙胺细胞骨架破坏研究,确定这些结构为角蛋白中间丝。体外结合试验进一步证实了MRP8-MRP14与角蛋白丝的钙依赖性结合。总之,我们的数据表明MRP8和MRP14可能参与上皮细胞中细胞骨架丝的钙依赖性重组,这可能与分化和炎症激活相关事件有关。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/792a/1135748/ffe29837c96a/biochemj00059-0066-a.jpg

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