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IRBITs 的可变 N 端附加物在激活小鼠 NBCe1-B 中的作用:非洲爪蟾和小鼠 IRBITs 的作用。

Activation of mouse NBCe1-B by Xenopus laevis and mouse IRBITs: Role of the variable Nt appendage of IRBITs.

机构信息

Key Laboratory of Molecular Biophysics of Ministry of Education, School of Life Science & Technology, Huazhong University of Science & Technology, Wuhan, Hubei 430074, China.

Key Laboratory of Molecular Biophysics of Ministry of Education, School of Life Science & Technology, Huazhong University of Science & Technology, Wuhan, Hubei 430074, China.

出版信息

Biochim Biophys Acta Biomembr. 2020 Jun 1;1862(6):183240. doi: 10.1016/j.bbamem.2020.183240. Epub 2020 Feb 28.

Abstract

The IP3 receptor binding protein released with inositol 1,4,5-trisphosphate (IRBIT) plays important roles in the regulation of intracellular Ca signaling and intracellular pH. The mammals express two IRBIT paralogs, i.e., IRBIT1 (encoded by AHCYL1) and IRBIT2 (encoded by AHCYL2). The clawed frog Xenopus laevis oocyte is widely used for biophysical studies on ion channels and transporters. It remains unknown whether endogenous IRBIT is expressed in Xenopus oocytes. Here, we cloned from frog oocyte irbit2.L and irbit2.S, orthologs of mammalian IRBIT2. When over-expressed, the frog IRBITs powerfully stimulate the electrogenic Na/HCO cotransporter NBCe1-B as mouse IRBIT2-V2 does. Expression of an isolated Nt fragment of NBCe1-B containing the IRBIT-binding domain greatly decreases NBCe1-B activity in oocytes, suggesting that the basal activity of NBCe1-B contains a large component derived from the stimulation by endogenous frog IRBIT. The frog IRBITs are highly homologous to the mammalian ones in the carboxyl-terminal region, but varies greatly in the amino-terminal (Nt) appendage. Interestingly, truncation study showed that the Nt appendage of IRBIT1 and the long Nt appendage of IRBIT2-V2 modestly enhance, whereas the short Nt appendage of IRBIT2-V4 greatly inhibits the functional interaction between IRBIT and NBCe1-B. Finally, Ala-substitution of Ser68, a key phosphorylation site in the PEST domain of IRBIT, causes distinct functional consequences depending on the structural context of the Nt appendage in different IRBIT isoforms. We conclude that the Nt appendage of IRBITs is not necessary for, but plays an important regulatory role in the functional interaction between IRBIT and NBCe1-B.

摘要

与肌醇 1,4,5-三磷酸(IP3)结合的 IP3 受体结合蛋白(IRBIT)在调节细胞内 Ca 信号转导和细胞内 pH 方面发挥重要作用。哺乳动物表达两种 IRBIT 同源物,即 IRBIT1(由 AHCYL1 编码)和 IRBIT2(由 AHCYL2 编码)。爪蟾 Xenopus laevis 卵母细胞广泛用于离子通道和转运体的生物物理研究。目前尚不清楚内源性 IRBIT 是否在 Xenopus 卵母细胞中表达。在这里,我们从蛙卵中克隆出了 irbit2.L 和 irbit2.S,这是哺乳动物 IRBIT2 的同源物。当过度表达时,蛙类 IRBIT 像鼠类 IRBIT2-V2 一样,有力地刺激电致型 Na/HCO3 共转运体 NBCe1-B。表达含有 IRBIT 结合域的 NBCe1-B 的 Nt 片段大大降低了卵母细胞中 NBCe1-B 的活性,这表明 NBCe1-B 的基础活性包含了很大一部分来自内源性蛙类 IRBIT 的刺激。蛙类 IRBIT 在羧基末端区域与哺乳动物的高度同源,但在氨基末端(Nt)附加物上差异很大。有趣的是,截断研究表明,IRBIT1 的 Nt 附加物和 IRBIT2-V2 的长 Nt 附加物适度增强,而 IRBIT2-V4 的短 Nt 附加物则大大抑制了 IRBIT 与 NBCe1-B 之间的功能相互作用。最后,IRBIT PEST 结构域中关键磷酸化位点 Ser68 的丙氨酸取代会根据不同 IRBIT 同工型中 Nt 附加物的结构背景产生不同的功能后果。我们得出结论,IRBIT 与 NBCe1-B 之间的功能相互作用不需要 Nt 附加物,但 Nt 附加物发挥着重要的调节作用。

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