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感染不同毒力狂犬病病毒的鼠神经瘤细胞 N2a 的蛋白质组图谱。

Proteomic profiles of mouse neuro N2a cells infected with variant virulence of rabies viruses.

机构信息

College of Animal Science and Veterinary Medicine, Jilin University, 5333 Xi'an Road, Changchun 130062, China.

出版信息

J Microbiol Biotechnol. 2011 Apr;21(4):366-73.

Abstract

We characterized the proteomes of murine N2a cells following infection with three rabies virus (RV) strains, characterized by distinct virulence phenotypes (i.e., virulent BD06, fixed CVS-11, and attenuated SRV9 strains), and identified 35 changes to protein expression using two-dimensional gel electrophoresis in whole-cell lysates. The annotated functions of these proteins are involved in various cytoskeletal, signal transduction, stress response, and metabolic processes. Specifically, a-enolase, prx-4, vimentin, cytokine-induced apoptosis inhibitor 1 (CIAPIN1) and prx-6 were significantly up-regulated, whereas Trx like-1 and galectin-1 were down-regulated following infection of N2a cells with all three rabies virus strains. However, comparing expressions of all 35 proteins affected between BD06-, CVS-11-, and SRV9-infected cells, specific changes in expression were also observed. The up-regulation of vimentin, CIAPIN1, prx-4, and 14-3-3 theta/delta, and downregulation of NDPK-B and HSP-1 with CVS and SRV9 infection were ≥ 2 times greater than with BD06. Meanwhile, Zfp12 protein, splicing factor, and arginine/serine-rich 1 were unaltered in the cells infected with BD06 and CVS- 11, but were up-regulated in the group infected with SRV9. The proteomic alterations described here may suggest that these changes to protein expression correlate with the rabies virus' adaptability and virulence in N2a cells, and hence provides new clues as to the response of N2a host cells to rabies virus infections, and may also aid in uncovering new pathways in these cells that are involved in rabies infections. Further characterization of the functions of the affected proteins may contribute to our understanding of the mechanisms of RV infection and pathogenesis.

摘要

我们研究了感染三种不同毒力表型(即强毒 BD06、固定毒 CVS-11 和弱毒 SRV9 株)的鼠 N2a 细胞的蛋白质组,并用二维凝胶电泳在全细胞裂解物中鉴定了 35 个蛋白表达变化。这些蛋白的注释功能涉及各种细胞骨架、信号转导、应激反应和代谢过程。具体而言,感染 N2a 细胞后,a-烯醇酶、prx-4、波形蛋白、细胞因子诱导凋亡抑制剂 1(CIAPIN1)和 prx-6 显著上调,而 Trx 样蛋白-1 和半乳糖凝集素-1 下调。然而,比较 BD06、CVS-11 和 SRV9 感染的细胞之间所有 35 种受影响蛋白的表达,也观察到了特定的表达变化。与 BD06 感染相比,CVS 和 SRV9 感染引起的波形蛋白、CIAPIN1、prx-4 和 14-3-3 theta/delta 的上调以及 NDPK-B 和 HSP-1 的下调更为显著,达到 2 倍以上。同时,Zfp12 蛋白、剪接因子和富含精氨酸/丝氨酸的 1 在感染 BD06 和 CVS-11 的细胞中没有改变,但在感染 SRV9 的细胞中上调。这里描述的蛋白质组学改变可能表明,这些蛋白表达的变化与狂犬病病毒在 N2a 细胞中的适应性和毒力相关,从而为 N2a 宿主细胞对狂犬病病毒感染的反应提供了新的线索,也可能有助于揭示这些细胞中参与狂犬病感染的新途径。进一步研究受影响蛋白的功能可能有助于我们理解 RV 感染和发病机制的机制。

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