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溶菌酶中赖氨酸残基的化学修饰可能会显著影响其淀粉样蛋白纤维化。

Chemical modification of lysine residues in lysozyme may dramatically influence its amyloid fibrillation.

作者信息

Morshedi Dina, Ebrahim-Habibi Azadeh, Moosavi-Movahedi Ali Akbar, Nemat-Gorgani Mohsen

机构信息

Industrial and Environmental Biotechnology Department, National Institute of Genetic Engineering and Biotechnology, Tehran, Iran.

出版信息

Biochim Biophys Acta. 2010 Apr;1804(4):714-22. doi: 10.1016/j.bbapap.2009.11.012. Epub 2009 Nov 26.

DOI:10.1016/j.bbapap.2009.11.012
PMID:19945549
Abstract

Studies on the aggregation of mutant proteins have provided new insights into the genetics of amyloid diseases and the role of the net charge of the protein on the rate, extent, and type of aggregate formation. In the present work, hen egg white lysozyme (HEWL) was employed as the model protein. Acetylation and (separately) citraconylation were employed to neutralize the charge on lysine residues. Acetylation of the lysine residues promoted amyloid formation, resulting in more pronounced fibrils and a dramatic decline in the nucleation time. In contrast, citraconylation produced the opposite effect. In both cases, native secondary and tertiary structures appeared to be retained. Studies on the effect of pH on aggregation suggested greater possibilities for amorphous aggregate formation rather than fibrillation at pH values closer to neutrality, in which the protein is known to take up a conformation more similar to its native form. This is in accord with reports in the literature suggesting that formation of amorphous aggregates is more favored under relatively more native conditions. pH 5 provided a critical environment in which a mixture of amorphous and fibrillar structures were observed. Use of Tango and Aggrescan software which describe aggregation tendencies of different parts of a protein structure suggested critical importance of some of the lysine residues in the aggregation process. Results are discussed in terms of the importance of the net charge in control of protein-protein interactions leading to aggregate formation and possible specific roles of lysine residues 96 and 97.

摘要

对突变蛋白聚集的研究为淀粉样疾病的遗传学以及蛋白质净电荷对聚集形成的速率、程度和类型的作用提供了新的见解。在本研究中,使用鸡蛋清溶菌酶(HEWL)作为模型蛋白。采用乙酰化和(分别地)柠康酰化来中和赖氨酸残基上的电荷。赖氨酸残基的乙酰化促进了淀粉样蛋白的形成,导致更明显的纤维,并使成核时间急剧下降。相反,柠康酰化产生了相反的效果。在这两种情况下,天然的二级和三级结构似乎都得以保留。对pH对聚集影响的研究表明,在接近中性的pH值下,形成无定形聚集体而非纤维的可能性更大,已知在这种pH值下蛋白质会呈现出与其天然形式更相似的构象。这与文献报道一致,即无定形聚集体的形成在相对更天然的条件下更受青睐。pH 5提供了一个关键环境,在其中观察到了无定形和纤维状结构的混合物。使用描述蛋白质结构不同部分聚集倾向的Tango和Aggrescan软件表明,一些赖氨酸残基在聚集过程中至关重要。根据净电荷在控制导致聚集形成的蛋白质 - 蛋白质相互作用中的重要性以及赖氨酸残基96和97可能的特定作用对结果进行了讨论。

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