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Loss of Zona Pellucida Binding Proteins in the Acrosomal Matrix Disrupts Acrosome Biogenesis and Sperm Morphogenesis▿ †

机译:顶体基质中Zona Pellucida结合蛋白的丢失破坏了顶体生物发生和精子形态发生▿†

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摘要

Zona pellucida binding protein 1 (ZPBP1), a spermatid and spermatozoon protein that localizes to the acrosome, was originally identified in pigs and named for its binding to the oocyte zona pellucida. In an in silico search for germ cell-specific genes, Zpbp1 and its novel paralog, Zpbp2, were discovered and confirmed to be expressed only in the testes in both mice and humans. To study the in vivo functions of both ZPBP proteins, we disrupted Zpbp1 and Zpbp2 in mice. Males lacking ZPBP1 were sterile, with abnormal round-headed sperm morphology and no forward sperm motility. Ultrastructural studies demonstrated that absence of ZPBP1 prevents proper acrosome compaction, resulting in acrosome fragmentation and disruption of the Sertoli-spermatid junctions. Males null for ZPBP2 were subfertile, demonstrated aberrant acrosomal membrane invaginations, and produced dysmorphic sperm with reduced ability to penetrate zona pellucida. Molecular phylogenetic analysis of ZPBPs from amphibians, birds, and mammals suggests that these paralogous genes coevolved to play cooperative roles during spermiogenesis. Whereas ZPBP1 was discovered for an in vitro role in sperm-egg interactions, we have shown that both ZPBP proteins play an earlier structural role during spermiogenesis.
机译:透明带结合蛋白1(ZPBP1)是一种定位于顶体的精子和精子蛋白,最初在猪中被鉴定出来,并以其与卵母细胞透明带的结合而命名。在计算机上搜索生殖细胞特异性基因时,发现Zpbp1及其新的旁系同源物Zpbp2,并证实它们仅在小鼠和人类的睾丸中表达。为了研究两种ZPBP蛋白的体内功能,我们破坏了小鼠的Zpbp1和Zpbp2。缺乏ZPBP1的雄性不育,具有圆头精子形态异常,无向前精子运动。超微结构研究表明,缺乏ZPBP1会阻止适当的顶体压实,从而导致顶体碎裂和Sertoli-精子连接的破坏。 ZPBP2无效的雄性不育,表现出顶体膜异常畸形,并产生畸形的精子,穿透透明带的能力降低。对两栖动物,鸟类和哺乳动物的ZPBP进行的分子系统发育分析表明,这些旁系同源基因共同进化,在精子发生过程中起协同作用。尽管发现ZPBP1在精卵相互作用中具有体外作用,但我们已经表明,这两种ZPBP蛋白在精子发生过程中都起着较早的结构作用。

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