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人生物素酶可变剪接mRNA的鉴定及内源性生物素酶的假定定位。

Identification of alternatively spliced human biotinidase mRNAs and putative localization of endogenous biotinidase.

作者信息

Stanley Christine M, Hymes Jeanne, Wolf Barry

机构信息

Department of Human Genetics, Medical College of Virginia of Virginia Commonwealth University, Richmond, VA 23298, USA.

出版信息

Mol Genet Metab. 2004 Apr;81(4):300-12. doi: 10.1016/j.ymgme.2003.12.006.

DOI:10.1016/j.ymgme.2003.12.006
PMID:15059618
Abstract

Biotinidase is essential for recycling the vitamin biotin and for transferring biotin to proteins, such as histones, suggesting that the enzyme localizes to various cellular and extracellular sites. To better understand the functions of the enzyme, we examined its gene structure and subcellular localization. Using RACE-PCR and a BLAST search, we extended the 5' sequence of the biotinidase gene. Three novel, alternatively spliced variants of biotinidase, 1a, 1b, and 1c, were identified in multiple human tissues. Exon 1c is present only in testes. The sequence of the 5' splice variants, 1a and 1b, suggest that biotinidase localizes to the mitochondria and/or ER, respectively. Using indirect immunofluorescence studies, biotinidase localizes to organelles in the cytoplasm, but not nucleus, of human fibroblasts and Hep G2 cells. Endogenous expression was examined by isopycnic gradient centrifugation of rat liver organelles, which identified an 85kDa biotinidase protein with biotinyl-hydrolase and transferase activities in microsomes and possibly lysosomes. A 48kDa protein, which also reacts with anti-biotinidase, localizes to mitochondria. The 48kDa protein is not N-glycosylated but is biotinylated, is in the inner mitochondrial matrix, but has no biotinyl-hydrolase or transferase activities. The function and validation of the mitochondrial species remains to be determined. The 5' splice variants and organelle fractionation studies indicate that biotinidase is directed to the secretory pathway and perhaps mitochondria.

摘要

生物素酶对于维生素生物素的循环利用以及将生物素转移至蛋白质(如组蛋白)至关重要,这表明该酶定位于各种细胞内和细胞外位点。为了更好地理解该酶的功能,我们研究了其基因结构和亚细胞定位。利用RACE-PCR和BLAST搜索,我们扩展了生物素酶基因的5'序列。在多种人体组织中鉴定出了生物素酶的三种新的可变剪接变体,即1a、1b和1c。外显子1c仅存在于睾丸中。5'剪接变体1a和1b的序列表明,生物素酶分别定位于线粒体和/或内质网。通过间接免疫荧光研究发现,生物素酶定位于人成纤维细胞和Hep G2细胞细胞质中的细胞器,但不在细胞核中。通过对大鼠肝脏细胞器进行等密度梯度离心来检测内源性表达,结果在微粒体以及可能的溶酶体中鉴定出一种具有生物素水解酶和转移酶活性的85kDa生物素酶蛋白。一种也与抗生物素酶反应的48kDa蛋白定位于线粒体。该48kDa蛋白未进行N-糖基化,但被生物素化,位于线粒体内膜,但没有生物素水解酶或转移酶活性。线粒体中的这种蛋白的功能及其验证仍有待确定。5'剪接变体和细胞器分级分离研究表明,生物素酶被导向分泌途径,可能还定位于线粒体。

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