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NOXO1的可变mRNA剪接形式:Nox1和Nox3的组织差异表达及调控

Alternative mRNA splice forms of NOXO1: differential tissue expression and regulation of Nox1 and Nox3.

作者信息

Cheng Guangjie, Lambeth J David

机构信息

Department of Pathology and Laboratory Medicine, Emory University School of Medicine, Atlanta, GA 30322, USA.

出版信息

Gene. 2005 Aug 15;356:118-26. doi: 10.1016/j.gene.2005.03.008.

Abstract

The activity of gp91phox, the catalytic subunit of the superoxide-generating respiratory burst oxidase, is stimulated by the regulatory subunits p47phox, p67phox and the small GTPase Rac. Novel homologs of p47phox and p67phox (NOXO1 and NOXA1, respectively) were recently identified and are implicated in the regulation of the gp91phox homologs Nox1 and Nox3. Herein, we report four splice forms of human NOXO1. NOXO1beta is the major mRNA splice form in human colon and fetal liver while NOXO1gamma was the majority species in testis. Neither the alpha nor delta forms were expressed in significant amounts in any tissue tested. Splice forms were generated by alternative splicing of the two ends of exon 3 of the NOXO1 gene, and resulted in differences in the PX domain. The PX domain is known to bind inositol lipids, but the expressed, purified PX domains from NOXO1beta and NOXO1gamma bound these lipids with the same specificity and affinity. NOXO1beta and NOXO1gamma both activated Nox1, but NOXO1gamma showed a poorer ability to activate Nox3 compared with NOXO1beta. These data suggest different tissue localizations and functions for NOXO1beta and NOXO1gamma in regulating Nox family members.

摘要

超氧化物生成呼吸爆发氧化酶的催化亚基gp91phox的活性受调节亚基p47phox、p67phox和小GTP酶Rac的刺激。最近鉴定出了p47phox和p67phox的新型同源物(分别为NOXO1和NOXA1),它们与gp91phox同源物Nox1和Nox3的调节有关。在此,我们报告了人NOXO1的四种剪接形式。NOXO1β是人结肠和胎儿肝脏中的主要mRNA剪接形式,而NOXO1γ是睾丸中的主要类型。在任何测试组织中,α和δ形式均未大量表达。剪接形式是由NOXO1基因外显子3两端的可变剪接产生的,导致PX结构域存在差异。已知PX结构域可结合肌醇脂质,但从NOXO1β和NOXO1γ表达并纯化的PX结构域以相同的特异性和亲和力结合这些脂质。NOXO1β和NOXO1γ均激活Nox1,但与NOXO1β相比,NOXO1γ激活Nox3的能力较差。这些数据表明NOXO1β和NOXO1γ在调节Nox家族成员方面具有不同的组织定位和功能。

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