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脊髓灰质炎病毒受体相关基因2产物的小鼠同源物,即mPRR2,介导同种细胞聚集。

Mouse homolog of poliovirus receptor-related gene 2 product, mPRR2, mediates homophilic cell aggregation.

作者信息

Aoki J, Koike S, Asou H, Ise I, Suwa H, Tanaka T, Miyasaka M, Nomoto A

机构信息

Department of Microbiology, The Tokyo Metropolitan Institute of Medical Science, Honkomagome, Japan. .

出版信息

Exp Cell Res. 1997 Sep 15;235(2):374-84. doi: 10.1006/excr.1997.3685.

Abstract

Poliovirus receptor (PVR) is a cell surface glycoprotein that belongs to the immunoglobulin superfamily. Although MPH was initially reported as the mouse homolog of human PVR, recent data strongly suggest that MPH is the mouse homolog of human PRR2, a PVR-related gene 2 product, and not that of human PVR. Thus MPH is renamed mPRR2 in this study. Physiological functions of the PVR-related gene products have not been elucidated, although PVR has been well characterized as the poliovirus receptor. In this study, a possible function of mPRR2 (MPH), which is not a functional receptor for poliovirus, was investigated. Mouse L cells expressing mPRR2 were prepared. Those mouse cells showed a higher activity of cell aggregation than the parental mouse L cells. Enhancement of cell aggregation was also observed for insect Sf9 cells infected with recombinant baculovirus carrying mPRR2 cDNA. On the other hand, L cells expressing human PVR or monkey PVR (AGM alpha1 or AGM alpha2) did not show increased cell aggregation. The cell aggregation activity of L cells expressing mPRR2 was inhibited by the addition of anti-mPRR2 monoclonal antibodies or a soluble mPRR2 molecule produced by the baculovirus expression system. An immunofluorescence study revealed that mPRR2 protein was localized to the cell-cell contact sites between cells expressing mPRR2. A similar localization of mPRR2 was observed for intrinsic mPRR2 molecules of the mouse neuroblastoma cell line NS20Y. The contact site-specific localization of mPRR2 was not observed on the border between mPRR2-expressing and nonexpressing HeLa cells. Furthermore, mPRR2 proteins directly bound to each other in vitro. mPRR2 was detected on various types of cultured cells of mouse origin and in various mouse tissues. These results suggest that mPRR2 is an intercellular adhesion molecule with a homophilic binding manner.

摘要

脊髓灰质炎病毒受体(PVR)是一种属于免疫球蛋白超家族的细胞表面糖蛋白。尽管MPH最初被报道为人PVR的小鼠同源物,但最近的数据强烈表明,MPH是人类PRR2(一种PVR相关基因2产物)的小鼠同源物,而非人类PVR的同源物。因此,在本研究中MPH被重新命名为mPRR2。尽管PVR作为脊髓灰质炎病毒受体已得到充分表征,但PVR相关基因产物的生理功能尚未阐明。在本研究中,对并非脊髓灰质炎病毒功能性受体的mPRR2(MPH)的可能功能进行了研究。制备了表达mPRR2的小鼠L细胞。那些小鼠细胞显示出比亲代小鼠L细胞更高的细胞聚集活性。在用携带mPRR2 cDNA的重组杆状病毒感染的昆虫Sf9细胞中也观察到细胞聚集增强。另一方面,表达人PVR或猴PVR(非洲绿猴α1或非洲绿猴α2)的L细胞未显示出细胞聚集增加。通过添加抗mPRR2单克隆抗体或杆状病毒表达系统产生的可溶性mPRR2分子,可抑制表达mPRR2的L细胞的细胞聚集活性。免疫荧光研究表明,mPRR2蛋白定位于表达mPRR2的细胞之间的细胞-细胞接触部位。在小鼠神经母细胞瘤细胞系NS20Y的内源性mPRR2分子中也观察到mPRR2的类似定位。在表达mPRR2和不表达mPRR2的HeLa细胞之间的边界上未观察到mPRR2的接触部位特异性定位。此外,mPRR2蛋白在体外直接相互结合。在各种小鼠来源的培养细胞和各种小鼠组织中均检测到mPRR2。这些结果表明,mPRR2是一种具有嗜同性结合方式的细胞间粘附分子。

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