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蛋白酶在糖基转移酶分泌中的作用:阿尔茨海默病β-分泌酶依赖性切割及随后的氨肽酶加工。

Involvement of proteases in glycosyltransferase secretion: Alzheimer's beta-secretase-dependent cleavage and a following processing by an aminopeptidase.

作者信息

Kitazume Shinobu, Suzuki Minoru, Saido Takaomi C, Hashimoto Yasuhiro

机构信息

Glyco-chain Functions Laboratory, Frontier Research System, RIKEN, 2-1 Hirosawa, Wako-shi, Saitama 351-0198, Japan.

出版信息

Glycoconj J. 2004;21(1-2):25-9. doi: 10.1023/B:GLYC.0000043743.21735.ff.

Abstract

Alzheimer's beta-secretase (BACE1) cleaves amyloid precursor protein to produce amyloid beta-peptide, which is a crucial initiation process of the pathogenesis of Alzheimer's disease. We previously found that BACE1 also cleaves a membrane-bound sialyltransferase (ST6Gal I). Here we report that, when the protein A-ST6Gal I fusion protein, or ST6Gal I-derived peptide, was used as an in vitro substrate for BACE1, it cleaved the substrates between Leu(37) and Gln(38). However, a soluble form of ST6Gal I secreted from COS cells started from Glu(41), which was three amino acids shorter than the in vitro product. The results suggested that the BACE1 product was truncated by an aminopeptidase(s) before secretion. The aminopeptidase activity was successfully detected in detergent extracts of Golgi-membrane fraction. Taken together, we concluded that BACE1 initially cleaved ST6Gal I between Leu(37) and Gln(38), and the NH(2)-terminal three amino acids of the yielded product was further trimmed by the aminopeptidase.

摘要

阿尔茨海默病β-分泌酶(BACE1)切割淀粉样前体蛋白以产生淀粉样β肽,这是阿尔茨海默病发病机制中的一个关键起始过程。我们之前发现BACE1还能切割一种膜结合唾液酸转移酶(ST6Gal I)。在此我们报告,当将蛋白A-ST6Gal I融合蛋白或ST6Gal I衍生肽用作BACE1的体外底物时,它在Leu(37)和Gln(38)之间切割底物。然而,从COS细胞分泌的可溶性ST6Gal I起始于Glu(41),比体外产物短三个氨基酸。结果表明,BACE1产物在分泌前被一种氨肽酶截短。在高尔基体膜组分的去污剂提取物中成功检测到了氨肽酶活性。综上所述,我们得出结论,BACE1最初在Leu(37)和Gln(38)之间切割ST6Gal I,产生的产物的NH(2)-末端三个氨基酸被氨肽酶进一步修剪。

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