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人α-乳白蛋白折叠变体HAMLET与细胞凋亡相关的构象分析。

Conformational analysis of HAMLET, the folding variant of human alpha-lactalbumin associated with apoptosis.

作者信息

Casbarra Annarita, Birolo Leila, Infusini Giuseppe, Dal Piaz Fabrizio, Svensson Malin, Pucci Piero, Svanborg Catharina, Marino Gennaro

机构信息

Dipartimento di Chimica Organica e Biochimica, Università di Napoli Federico II, I-80126 Napoli, Italy.

出版信息

Protein Sci. 2004 May;13(5):1322-30. doi: 10.1110/ps.03474704. Epub 2004 Apr 9.

DOI:10.1110/ps.03474704
PMID:15075403
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2286754/
Abstract

A combination of hydrogen/deuterium (H/D) exchange and limited proteolysis experiments coupled to mass spectrometry analysis was used to depict the conformation in solution of HAMLET, the folding variant of human alpha-lactalbumin, complexed to oleic acid, that induces apoptosis in tumor and immature cells. Although near- and far-UV CD and fluorescence spectroscopy were not able to discriminate between HAMLET and apo-alpha-lactalbumin, H/D exchange experiments clearly showed that they correspond to two distinct conformational states, with HAMLET incorporating a greater number of deuterium atoms than the apo and holo forms. Complementary proteolysis experiments revealed that HAMLET and apo are both accessible to proteases in the beta-domain but showed substantial differences in accessibility to proteases at specific sites. The overall results indicated that the conformational changes associated with the release of Ca2+ are not sufficient to induce the HAMLET conformation. Metal depletion might represent the first event to produce a partial unfolding in the beta-domain of alpha-lactalbumin, but some more unfolding is needed to generate the active conformation HAMLET, very likely allowing the protein to bind the C18:1 fatty acid moiety. On the basis of these data, a putative binding site of the oleic acid, which stabilizes the HAMLET conformation, is proposed.

摘要

将氢/氘(H/D)交换与有限蛋白酶解实验相结合,并与质谱分析联用,用于描绘人α-乳白蛋白折叠变体HAMLET(与油酸复合,可诱导肿瘤细胞和未成熟细胞凋亡)在溶液中的构象。尽管近紫外和远紫外圆二色光谱以及荧光光谱无法区分HAMLET和脱辅基α-乳白蛋白,但H/D交换实验清楚地表明它们对应于两种不同的构象状态,HAMLET比脱辅基形式和全蛋白形式掺入了更多的氘原子。补充蛋白酶解实验表明,HAMLET和脱辅基形式在β结构域中都可被蛋白酶作用,但在特定位点对蛋白酶的可及性上存在显著差异。总体结果表明,与Ca2+释放相关的构象变化不足以诱导HAMLET构象。金属离子耗竭可能是导致α-乳白蛋白β结构域部分展开的首个事件,但还需要更多的展开才能产生活性构象HAMLET,这很可能使蛋白质能够结合C18:1脂肪酸部分。基于这些数据,提出了一个稳定HAMLET构象的油酸假定结合位点。

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