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Characterization of a novel human sperm-associated antigen 9 (SPAG9) having structural homology with c-Jun N-terminal kinase-interacting protein

机译:与c-Jun N端激酶相互作用蛋白具有结构同源性的新型人类精子相关抗原9(SPAG9)的表征

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摘要

We report a novel SPAG9 (sperm-associated antigen 9) protein having structural homology with JNK (c-Jun N-terminal kinase)-interacting protein 3. SPAG9, a single copy gene mapped to the human chromosome 17q21.33 syntenic with location of mouse chromosome 11, was earlier shown to be expressed exclusively in testis [Shankar, Mohapatra and Suri (1998) Biochem. Biophys. Res. Commun. >243, 561–565]. The SPAG9 amino acid sequence analysis revealed identity with the JNK-binding domain and predicted coiled-coil, leucine zipper and transmembrane domains. The secondary structure analysis predicted an α-helical structure for SPAG9 that was confirmed by CD spectra. Microsequencing of higher-order aggregates of recombinant SPAG9 by tandem MS confirmed the amino acid sequence and mono atomic mass of 83.9 kDa. Transient expression of SPAG9 and its deletion mutants revealed that both leucine zipper with extended coiled-coil domains and transmembrane domain of SPAG9 were essential for dimerization and proper localization. Studies of MAPK (mitogenactivated protein kinase) interactions demonstrated that SPAG9 interacted with higher binding affinity to JNK3 and JNK2 compared with JNK1. No interaction was observed with p38α or extracellular-signal-regulated kinase pathways. Polyclonal antibodies raised against recombinant SPAG9 recognized native protein in human sperm extracts and localized specifically on the acrosomal compartment of intact human spermatozoa. Acrosome-reacted spermatozoa demonstrated SPAG9 immunofluorescence, indicating its retention on the equatorial segment after the acrosome reaction. Further, anti-SPAG9 antibodies inhibited the binding of human spermatozoa to intact human oocytes as well as to matched hemizona. This is the first report of sperm-associated JNK-binding protein that may have a role in spermatozoa–egg interaction.
机译:我们报告了一种新型的SPAG9(精子相关抗原9)蛋白,与JNK(c-Jun N末端激酶)相互作用蛋白3具有结构同源性。SPAG9,单拷贝基因,定位于人染色体17q21.33,与先前已证明小鼠11号染色体仅在睾丸中表达[Shankar,Mohapatra和Suri(1998)Biochem。生物物理学。 Res。公社> 243 ,561–565]。 SPAG9氨基酸序列分析显示与JNK结合结构域和预测的卷曲螺旋,亮氨酸拉链和跨膜结构域相同。二级结构分析预测SPAG9的α螺旋结构已通过CD光谱证实。通过串联质谱对重组SPAG9的高阶聚集体进行微测序,确认了83.9kDa的氨基酸序列和单原子质量。 SPAG9及其缺失突变体的瞬时表达表明,具有扩展的卷曲螺旋结构域的亮氨酸拉链和SPAG9的跨膜结构域对于二聚化和正确定位至关重要。对MAPK(促分裂原活化蛋白激酶)相互作用的研究表明,与JNK1相比,SPAG9与JNK3和JNK2的结合亲和力更高。没有观察到与p38α或细胞外信号调节的激酶途径的相互作用。产生针对重组SPAG9的多克隆抗体,可识别人精子提取物中的天然蛋白,并特异性定位于完整人精子的顶体区室。顶体反应的精子表现出SPAG9免疫荧光,表明其在顶体反应后保留在赤道片段上。此外,抗SPAG9抗体抑制人精子与完整人卵母细胞以及与之匹配的半胱氨酸的结合。这是与精子相关的JNK结合蛋白的首次报道,该蛋白可能与精子与卵的相互作用有关。

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