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从MPC - 11和克雷布斯II腹水癌细胞中分离出的游离、细胞骨架结合和膜结合多核糖体,其多聚腺苷酸结合蛋白的组成有所不同。

Free, cytoskeletal-bound and membrane-bound polysomes isolated from MPC-11 and Krebs II ascites cells differ in their complement of poly(A) binding proteins.

作者信息

Moss R, Pryme I F, Vedeler A

机构信息

Department of Biochemistry and Molecular Biology, University of Bergen, Norway.

出版信息

Mol Cell Biochem. 1994 Feb 23;131(2):131-9. doi: 10.1007/BF00925949.

Abstract

A three-step detergent/salt extraction procedure (Vedeler et al., Mol Cell Biochem 100: 183-193, 1991) was used to isolate free polysomes (FP), cytoskeletal-bound polysomes (CBP) and membrane-bound polysomes (MBP) from MPC-11 and Krebs II ascites cells. Polysomes were pelleted, washed with high salt buffer and re-pelleted. Proteins in the dialysed high-salt extracts were subjected to poly(A) Sepharose chromatography and poly(A) binding and non-binding proteins were separated by SDS-PAGE. In MPC-11 cells the FP fraction contains thirteen poly(A) binding proteins and four non-poly(A) binding proteins while the corresponding fraction in Krebs II ascites cells has four poly(A) binding proteins and six proteins which do not bind poly(A). The CBP fraction isolated from MPC-11 cells has a complement of ten poly(A) binding proteins, four which are non-poly(A) binding, and a protein of 105 kDa which has both poly(A) binding and non-poly(A) binding properties. In the CBP fraction prepared from Krebs II ascites cells a protein band at 32 kDa exhibits both poly(A) binding and non-poly(A) binding properties. In this fraction there are six poly(A) binding proteins and an additional eight which do not bind poly(A). Of the total number of proteins eight of these have a molecular weight below 40 kDa. The MBP fraction in MPC-11 cells contains three poly(A) binding proteins and eleven with non-poly(A) binding properties. In contrast this fraction in Krebs II ascites cells has a complement of thirteen poly(A) binding and ten non-poly(A) binding proteins.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

采用三步去污剂/盐提取程序(Vedeler等人,《分子与细胞生物化学》100: 183 - 193, 1991)从MPC - 11细胞和克雷布斯II腹水癌细胞中分离游离多核糖体(FP)、细胞骨架结合多核糖体(CBP)和膜结合多核糖体(MBP)。将多核糖体沉淀,用高盐缓冲液洗涤并再次沉淀。对透析后的高盐提取物中的蛋白质进行聚(A)琼脂糖凝胶层析,通过SDS - PAGE分离聚(A)结合蛋白和非聚(A)结合蛋白。在MPC - 11细胞中,FP组分包含13种聚(A)结合蛋白和4种非聚(A)结合蛋白,而在克雷布斯II腹水癌细胞中的相应组分有4种聚(A)结合蛋白和6种不结合聚(A)的蛋白。从MPC - 11细胞中分离的CBP组分有10种聚(A)结合蛋白,其中4种是非聚(A)结合蛋白,还有一种105 kDa的蛋白同时具有聚(A)结合和非聚(A)结合特性。在从克雷布斯II腹水癌细胞制备的CBP组分中,一条32 kDa的蛋白带同时具有聚(A)结合和非聚(A)结合特性。该组分中有6种聚(A)结合蛋白和另外8种不结合聚(A)的蛋白。在这些蛋白总数中,有8种分子量低于40 kDa。MPC - 11细胞中的MBP组分包含3种聚(A)结合蛋白和11种具有非聚(A)结合特性的蛋白。相比之下,克雷布斯II腹水癌细胞中的该组分有13种聚(A)结合蛋白和10种非聚(A)结合蛋白。(摘要截短至2

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