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公猪前顶体蛋白酶的定点诱变揭示了与透明带糖蛋白结合相关的残基。

Site-directed mutagenesis of boar proacrosin reveals residues involved in binding of zona pellucida glycoproteins.

作者信息

Jansen S, Jones R, Jenneckens I, Marschall B, Kriegesmann B, Coadwell J, Brenig B

机构信息

Veterinary Institute of Göttingen, Germany.

出版信息

Mol Reprod Dev. 1998 Oct;51(2):184-92. doi: 10.1002/(SICI)1098-2795(199810)51:2<184::AID-MRD8>3.0.CO;2-M.

DOI:10.1002/(SICI)1098-2795(199810)51:2<184::AID-MRD8>3.0.CO;2-M
PMID:9740326
Abstract

Proacrosin, the zymogen form of the serine protease beta-acrosin, is thought to function as a secondary binding molecule between mammalian gametes during fertilization (Jansen et al., 1995: Int J Dev Biol 39, 501-510). The interaction involves strong ionic bonds between positively charged amino acids on proacrosin and negatively charged polysulphate groups on zona pellucida glycoproteins. In this investigation, we identified the basic residues on proacrosin that are important for this binding. Site-directed mutagenesis shows that two groups of amino acids comprising His47, Arg50, and Arg51 together with Arg250, Lys252, and Arg253 are crucial because their deletion or replacement severely reduces affinity for zona glycoproteins. Molecular models of proacrosin reveal that these residues are located along one face of the protein on two exposed surface loops that project over and around the catalytic site. These findings support the hypothesis that polysulphate binding sites on proacrosin are formed by a restricted number of basic amino acids on the surface of the protein, presenting a specific orientation that is complementary to negatively charged sulphate groups on zona glycoproteins. Identification and elucidation of the stereochemistry of these charged moieties will aid design of new kinds of nonsteroidal antifertility agents.

摘要

前顶体蛋白酶是丝氨酸蛋白酶β-顶体蛋白酶的酶原形式,被认为在受精过程中作为哺乳动物配子之间的二级结合分子发挥作用(扬森等人,1995年:《国际发育生物学杂志》39卷,501 - 510页)。这种相互作用涉及前顶体蛋白酶上带正电荷的氨基酸与透明带糖蛋白上带负电荷的多硫酸基团之间的强离子键。在本研究中,我们确定了前顶体蛋白酶上对这种结合重要的碱性残基。定点诱变表明,由His47、Arg50和Arg51以及Arg250、Lys252和Arg253组成的两组氨基酸至关重要,因为它们的缺失或替换会严重降低对透明带糖蛋白的亲和力。前顶体蛋白酶的分子模型显示,这些残基位于蛋白质的一个面上的两个暴露表面环上,这些环在催化位点上方和周围突出。这些发现支持了这样的假设,即前顶体蛋白酶上的多硫酸结合位点由蛋白质表面数量有限的碱性氨基酸形成,呈现出与透明带糖蛋白上带负电荷的硫酸基团互补的特定取向。对这些带电部分的立体化学的鉴定和阐明将有助于新型非甾体抗生育剂的设计。

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