肿瘤坏死因子-α在前列腺素E2的驱动下诱导人远端结肠分泌氯离子和钾离子。
Tumor necrosis factor-alpha induces Cl- and K+ secretion in human distal colon driven by prostaglandin E2.
作者信息
Schmitz H, Fromm M, Bode H, Scholz P, Riecken E O, Schulzke J D
机构信息
Department of Gastroenterology, Universitätsklinikum Benjamin Franklin, Freie Universität Berlin, Germany.
出版信息
Am J Physiol. 1996 Oct;271(4 Pt 1):G669-74. doi: 10.1152/ajpgi.1996.271.4.G669.
Increased levels of tumor necrosis factor-alpha (TNF-alpha) have been found in, for example, inflammatory bowel disease (IBD) and human immunodeficiency virus (HIV) infection. To investigate a possible contribution of TNF-alpha to the pathogenesis of diarrhea in these diseases, ion transport of human distal colon was studied in the Ussing chamber in vitro. Serosal addition of TNF-alpha increased short-circuit current (Isc) of partially stripped tissues in a dose-dependent manner. Maximum Isc increase of 1.8 +/- 0.2 mumol.h-1.cm-2 was reached after 60 +/- 9 min at 200 ng/ml TNF-alpha. Bidirectional tracer flux measurements revealed that TNF-alpha induced an increase in 36 Cl serosal-to-mucosal flux, a decrease in 36Cl- mucosal-to-serosal flux, and a slight increase in K+ secretion indicated by an increased secretory 86Rb net flux. In the highly differentiated colonic epithelial cell line HT-29/B6, TNF-alpha had no effect on Isc, suggesting a mediation step located in the subepithelium. This supposition was supported by measurements on totally stripped human tissues, since removal of subepithelial layers by total stripping reduced the TNF-alpha effect by 40%. Experiments with tetrodotoxin (10(-6)M) indicated that the TNF-alpha effect was not mediated by the enteric nervous system. The specific 5-lipoxygenase blocker ICI-230487 (5 x 10(-8)M) also had no effect on TNF-alpha action. In contrast, inhibition of cyclooxygenase by indomethacin (10(-6)M inhibited the effect of TNF-alpha. Radioimmunoassay of prostaglandin E2 (PGE2) in the serosal bathing solution revealed an increase in PGE2 production/release after addition of TNF-alpha, which paralleled the Isc response. We conclude that TNF-alpha changed Cl- and K+ transport toward secretion in human colon. This effect was mediated by PGE2 produced by subepithelial cells. Thus TNF-alpha could be a mediator of diarrhea during intestinal inflammation, e.g., in IBD and HIV infection.
例如,在炎症性肠病(IBD)和人类免疫缺陷病毒(HIV)感染中已发现肿瘤坏死因子-α(TNF-α)水平升高。为了研究TNF-α在这些疾病腹泻发病机制中的可能作用,在体外Ussing室中研究了人类远端结肠的离子转运。向浆膜侧添加TNF-α以剂量依赖的方式增加了部分剥离组织的短路电流(Isc)。在200 ng/ml TNF-α作用下,60±9分钟后Isc最大增加量达到1.8±0.2 μmol·h⁻¹·cm⁻²。双向示踪剂通量测量显示,TNF-α诱导36Cl从浆膜侧向黏膜侧的通量增加,36Cl⁻从黏膜侧向浆膜侧的通量减少,并且分泌性86Rb净通量增加表明K⁺分泌略有增加。在高度分化的结肠上皮细胞系HT-29/B6中,TNF-α对Isc没有影响,这表明存在一个位于上皮下的介导步骤。对完全剥离的人体组织的测量支持了这一假设,因为通过完全剥离去除上皮下层使TNF-α的作用降低了40%。用河豚毒素(10⁻⁶M)进行的实验表明,TNF-α的作用不是由肠神经系统介导的。特异性5-脂氧合酶阻断剂ICI-230487(5×10⁻⁸M)对TNF-α的作用也没有影响。相反,吲哚美辛(10⁻⁶M)抑制环氧合酶可抑制TNF-α的作用。对浆膜侧浴液中前列腺素E2(PGE2)的放射免疫分析显示,添加TNF-α后PGE2的产生/释放增加,这与Isc反应平行。我们得出结论,TNF-α改变了人类结肠中Cl⁻和K⁺的转运方向,使其向分泌方向发展。这种作用是由上皮下细胞产生的PGE2介导的。因此,TNF-α可能是肠道炎症(如IBD和HIV感染)期间腹泻的介质。
Zotero 插件