NHE4 对于啮齿动物肾脏氨的处理至关重要。

NHE4 is critical for the renal handling of ammonia in rodents.

机构信息

INSERM, Centre de Recherche des Cordeliers, UMRS872, Paris, France.

出版信息

J Clin Invest. 2010 Jun;120(6):1895-904. doi: 10.1172/JCI36581. Epub 2010 May 17.

Abstract

Ammonia absorption by the medullary thick ascending limb of Henle's loop (MTALH) is thought to be a critical step in renal ammonia handling and excretion in urine, in which it is the main acid component. Basolateral Na+/H+ exchangers have been proposed to play a role in ammonia efflux out of MTALH cells, which express 2 exchanger isoforms: Na+/H+ exchanger 1 (NHE1) and NHE4. Here, we investigated the role of NHE4 in urinary acid excretion and found that NHE4-/- mice exhibited compensated hyperchloremic metabolic acidosis, together with inappropriate urinary net acid excretion. When challenged with a 7-day HCl load, NHE4-/- mice were unable to increase their urinary ammonium and net acid excretion and displayed reduced ammonium medulla content compared with wild-type littermates. Both pharmacologic inhibition and genetic disruption of NHE4 caused a marked decrease in ammonia absorption by the MTALH. Finally, dietary induction of metabolic acidosis increased NHE4 mRNA expression in mouse MTALH cells and enhanced renal NHE4 activity in rats, as measured by in vitro microperfusion of MTALH. We therefore conclude that ammonia absorption by the MTALH requires the presence of NHE4 and that lack of NHE4 reduces the ability of MTALH epithelial cells to create the cortico-papillary gradient of NH3/NH4+ needed to excrete an acid load, contributing to systemic metabolic acidosis.

摘要

髓袢升支粗段(MTALH)对氨的吸收被认为是肾脏氨处理和尿液排泄的关键步骤,在其中它是主要的酸成分。基底外侧 Na+/H+交换器被认为在氨从 MTALH 细胞中流出中发挥作用,MTALH 细胞表达 2 种交换体同工型:Na+/H+交换器 1(NHE1)和 NHE4。在这里,我们研究了 NHE4 在尿酸性排泄中的作用,发现 NHE4-/- 小鼠表现出代偿性高氯代谢性酸中毒,同时伴有不适当的尿净酸排泄。当受到 7 天 HCl 负荷挑战时,NHE4-/- 小鼠无法增加其尿铵和净酸排泄量,与野生型同窝仔鼠相比,其髓质铵含量减少。NHE4 的药理学抑制和基因敲除都导致 MTALH 氨吸收显著减少。最后,饮食诱导的代谢性酸中毒增加了小鼠 MTALH 细胞中 NHE4 mRNA 的表达,并增强了大鼠肾 NHE4 的活性,这通过 MTALH 的体外微灌注来测量。因此,我们得出结论,MTALH 对氨的吸收需要 NHE4 的存在,而缺乏 NHE4 会降低 MTALH 上皮细胞产生排泄酸负荷所需的皮质-乳头 NH3/NH4+梯度的能力,导致全身代谢性酸中毒。

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