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热诱导的鸡卵清蛋白聚集表明了丝氨酸蛋白酶抑制剂聚合的一个关键因素。

Heat-Induced Aggregation of Hen Ovalbumin Suggests a Key Factor Responsible for Serpin Polymerization.

作者信息

Noji Masahiro, So Masatomo, Yamaguchi Keiichi, Hojo Hironobu, Onda Maki, Akazawa-Ogawa Yoko, Hagihara Yoshihisa, Goto Yuji

机构信息

Institute for Protein Research , Osaka University , Yamadaoka 3-2 , Suita , Osaka 565-0871 , Japan.

Department of Biological Science, Graduate School of Science , Osaka Prefecture University , Naka Ku, Sakai , Osaka 599-8570 , Japan.

出版信息

Biochemistry. 2018 Sep 18;57(37):5415-5426. doi: 10.1021/acs.biochem.8b00619. Epub 2018 Sep 6.

DOI:10.1021/acs.biochem.8b00619
PMID:30148614
Abstract

Although ovalbumin (OVA), a main component of hen egg white and a non-inhibitory serpin superfamily protein, has been reported to form fibrillar aggregates, its relationship with amyloid fibrils associated with various degenerative diseases is unclear. We studied the heat-induced aggregation of intact OVA using an amyloid-specific thioflavin T assay with a fluorometer or direct imaging with a light-emitting diode lamp and several physicochemical approaches, and the results confirmed that intact OVA forms aggregates with a small part of amyloid cores and dominantly amorphous aggregates. We isolated the amyloidogenic core peptide by proteolysis with trypsin. The isolated 23-residue peptide, pOVA, with marked amyloidogenicity, corresponded to one (β-strand 3A) of the key regions involved in serpin latency transition and domain-swap polymerization leading to serpinopathies. Although the strong amyloidogenicity of pOVA was suppressed in a mixture of tryptic digests, it was observed under acidic conditions in the presence of various salts, with which pOVA has a positive charge. Cytotoxicity measurements suggested that, although heat-treated OVA aggregates exhibited the strongest toxicity, it was attributed to a general property of amorphous aggregates rather than amyloid toxicity. Predictions indicated that the high amyloidogenicity of the β-strand 3A region is common to various serpins. This suggests that the high amyloidogenicity of β-strand 3A that is important for serpin latency transition and domain-swap polymerization is retained in OVA and constitutes β-spine amyloid cores upon heat aggregation.

摘要

虽然卵清蛋白(OVA)是鸡蛋清的主要成分,属于非抑制性丝氨酸蛋白酶抑制剂超家族蛋白,已有报道称其会形成纤维状聚集体,但其与各种退行性疾病相关的淀粉样纤维的关系尚不清楚。我们使用荧光计进行淀粉样特异性硫黄素T检测或用发光二极管灯直接成像以及几种物理化学方法研究了完整OVA的热诱导聚集,结果证实完整的OVA形成的聚集体中一小部分是淀粉样核心,主要是无定形聚集体。我们用胰蛋白酶进行蛋白水解分离出了淀粉样生成核心肽。分离出的具有显著淀粉样生成性的23个残基的肽pOVA,对应于丝氨酸蛋白酶抑制剂潜伏转变和导致丝氨酸蛋白酶病的结构域交换聚合所涉及的关键区域之一(β链3A)。虽然pOVA在胰蛋白酶消化混合物中强烈的淀粉样生成性受到抑制,但在存在各种盐的酸性条件下观察到了这种现象,此时pOVA带正电荷。细胞毒性测量表明,虽然热处理的OVA聚集体表现出最强的毒性,但这归因于无定形聚集体的一般特性而非淀粉样毒性。预测表明β链3A区域的高淀粉样生成性在各种丝氨酸蛋白酶抑制剂中是常见的。这表明对丝氨酸蛋白酶抑制剂潜伏转变和结构域交换聚合很重要的β链3A的高淀粉样生成性在OVA中得以保留,并在热聚集时构成β-脊柱淀粉样核心。

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