Departments of Physiology and Medicine, Gastroenterology Division, Johns Hopkins University School of Medicine, Baltimore, Maryland.
Department of Gastroenterology, Hannover Medical School, Hannover, Germany.
Am J Physiol Cell Physiol. 2019 Oct 1;317(4):C737-C748. doi: 10.1152/ajpcell.00351.2018. Epub 2019 Jul 31.
Enterotoxigenic (ETEC) is a leading cause of childhood death from diarrhea and the leading cause of Traveler's diarrhea. heat-stable enterotoxin (ST) is a major virulence factor of ETEC and inhibits the brush border Na/H exchanger NHE3 in producing diarrhea. NHE3 regulation involves multiprotein signaling complexes that form on its COOH terminus. In this study, the hypothesis was tested that ST signals via members of the Na/H exchanger regulatory factor (NHERF) family of scaffolding proteins, NHERF2, which had been previously shown to have a role, and now with concentration on a role for NHERF3. Two models were used: mouse small intestine and Caco-2/BBe cells. In both models, ST rapidly increased intracellular cGMP, inhibited NHE3 activity, and caused a quantitatively similar decrease in apical expression of NHE3. The transport effects were NHERF3 and NHERF2 dependent. Also, mutation of the COOH-terminal amino acids of NHERF3 supported that NHERF3-NHERF2 heterodimerization was likely to account for this dual dependence. The ST increase in cGMP in both models was partially dependent on NHERF3. The intracellular signaling pathways by which ST-cGMP inhibits NHE3 were different in mouse jejunum (activation of cGMP kinase II, cGKII) and Caco-2 cells, which do not express cGKII (elevation of intracellular Ca concentration [Ca]). The ST elevation of [Ca] was from intracellular stores and was dependent on NHERF3-NHERF2. This study shows that intracellular signaling in the same diarrheal model in multiple cell types may be different; this has implications for therapeutic strategies, which often assume that models have similar signaling mechanisms.
肠产毒性(ETEC)是导致儿童腹泻死亡的主要原因,也是旅行者腹泻的主要原因。热稳定肠毒素(ST)是 ETEC 的主要毒力因子,通过抑制刷状缘 Na/H 交换器 NHE3 产生腹泻。NHE3 的调节涉及到在其羧基末端形成的多蛋白信号复合物。在这项研究中,我们假设 ST 通过 Na/H 交换器调节因子(NHERF)家族的支架蛋白成员(先前已显示其具有作用,现在集中研究 NHERF3 的作用)发出信号。使用了两种模型:小鼠小肠和 Caco-2/BBe 细胞。在这两种模型中,ST 均可迅速增加细胞内 cGMP,抑制 NHE3 活性,并导致 NHE3 顶端表达的定量相似减少。这些转运效应依赖于 NHERF3 和 NHERF2。此外,NHERF3 COOH 末端氨基酸的突变支持 NHERF3-NHERF2 异二聚体可能是这种双重依赖性的原因。两种模型中 ST 引起的 cGMP 增加部分依赖于 NHERF3。ST-cGMP 抑制 NHE3 的细胞内信号通路在小鼠空肠(cGMP 激酶 II,cGKII 的激活)和不表达 cGKII 的 Caco-2 细胞中不同(细胞内 Ca 浓度[Ca]的升高)。ST 引起的 [Ca]升高来自细胞内储存库,依赖于 NHERF3-NHERF2。本研究表明,在多种细胞类型的相同腹泻模型中,细胞内信号可能不同;这对治疗策略有影响,因为治疗策略通常假设模型具有相似的信号机制。
