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二硫键的裂解会导致非洲爪蟾卵母细胞中表达的IIa型而非IIb型磷酸钠共转运蛋白失活和降解。

Cleavage of disulfide bonds leads to inactivation and degradation of the type IIa, but not type IIb sodium phosphate cotransporter expressed in Xenopus laevis oocytes.

作者信息

Lambert G, Traebert M, Biber J, Murer H

机构信息

Physiologisches Institut, Universität Zürich Irchel, Winterurerstr. 190, CH-8057 Zürich, Switzerland.

出版信息

J Membr Biol. 2000 Jul 15;176(2):143-9. doi: 10.1007/s00232001083.

Abstract

Tris(2-carboxyethyl)phosphine (TCEP) reduces (cleaves) disulfide bonds of the renal proximal tubule type IIa Na/Pi- cotransporter (rat NaPi IIa) and thereby inhibits its function. We tested the effect of TCEP on the murine type IIa Na/P(i)-cotransporter and the corresponding IIb intestinal isoform both expressed in Xenopus laevis oocytes. After incubation with TCEP the function of NaPi IIa was inhibited and protein amount was decreased. Injection of the lysosomal inhibitor leupeptin prevented degradation of the protein. Exposure of oocytes to TCEP at 0 degrees C led to a reduction in transport function without concomitant loss in Na/Pi IIa protein. In contrast to NaPi type IIa, the type IIb isoform was neither inhibited, nor degraded after incubation with TCEP. These results suggest that cleavage of disulfide bonds led to changes within the confirmation of the type IIa transporter that result in (i) inhibition of the transport activity and (ii) internalization and subsequent lysosomal degradation of transporter protein. Sequence comparisons suggest the involvement/presence of different disulfide bonds in type IIa and type IIb Na/P(i)-cotransporters.

摘要

三(2-羧乙基)膦(TCEP)可还原(裂解)肾近端小管IIa型钠/磷酸共转运蛋白(大鼠NaPi IIa)的二硫键,从而抑制其功能。我们测试了TCEP对非洲爪蟾卵母细胞中表达的小鼠IIa型钠/磷酸共转运蛋白和相应的IIb型肠亚型的影响。与TCEP孵育后,NaPi IIa的功能受到抑制,蛋白质含量降低。注射溶酶体抑制剂亮抑蛋白酶肽可防止蛋白质降解。在0摄氏度下将卵母细胞暴露于TCEP会导致转运功能降低,而Na/Pi IIa蛋白不会随之损失。与IIa型钠/磷酸共转运蛋白不同,IIb型亚型在与TCEP孵育后既未受到抑制,也未发生降解。这些结果表明,二硫键的裂解导致IIa型转运蛋白构象发生变化,从而导致(i)转运活性受到抑制,以及(ii)转运蛋白内化并随后被溶酶体降解。序列比较表明,IIa型和IIb型钠/磷酸共转运蛋白中存在不同的二硫键。

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