Binding of bile acids with rat colon and resultant perturbation of membrane organization as studied by uptake measurement and 31P nuclear magnetic resonance spectroscopy.

Gan Pub Date : 1984-09-01
Y Sugimoto, H Saitô, R Tabeta, M Kodama, C Nagata, M Itabashi, T Hirota, S Toyoshima
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Abstract

The mode of interaction of deoxycholate (DOC) or lithocholate (LC) with F344 rat colon was examined by measurements of uptake, 31P nuclear magnetic resonance (NMR) spectroscopy and observation of morphological changes. DOC as well as LC was taken up by the colon in a nonsaturable manner with respect to concentration and time, up to 30 min. None of several metabolic inhibitors reduced the uptake of the bile acids, nor did pretreatment of colon segments with chloroform-methanol (2:1, (v/v), heat or trypsin. Further, the bile acids were not transported by the colon against concentration gradients, and they were bound to both the mucosa and serosa equally. From these findings, it is concluded that the bile acids are transported in a passive manner, and no specific receptor for them is contained in colonic mucosa. The uptake of the bile acids by the colon varied with temperature and was related to the fluidity of the colonic membranes. The extent of uptake of dehydrocholate and taurocholate, which do not induce ornithine decarboxylase (ODC) activity, was almost the same as that of LC. The 31P NMR spectra of the colonic mucosal cells indicated that the proportion of the bilayer structure is increased by 0.5 mM DOC. Among a variety of bile acids examined, the extent of membrane alteration was in parallel with the extent of ODC induction. Treatment of the colonic mucosa with 0.5 mM DOC caused marked degeneration of the surface but not the deeper layers of the mucosa. Thus, physiological concentrations of bile acids influence the membrane organization of the colonic mucosa in a nonspecific manner that is possibly related to the tumor-promoting activity.

胆汁酸与大鼠结肠的结合及由此引起的膜组织扰动采用摄取测量和31P核磁共振波谱法研究。
采用摄食量测定、31P核磁共振(NMR)和形态变化观察等方法,探讨脱氧胆酸盐(DOC)或石胆酸盐(LC)与F344大鼠结肠的相互作用模式。DOC和LC在浓度和时间上以不饱和的方式被结肠吸收,可达30分钟。几种代谢抑制剂都不能减少胆汁酸的吸收,氯仿-甲醇(2:1,(v/v),热或胰蛋白酶预处理结肠段也不能减少胆汁酸的吸收。此外,胆汁酸不受浓度梯度的影响通过结肠运输,它们同时与粘膜和浆膜结合。由此可见,胆汁酸是一种被动的转运方式,结肠粘膜中不含胆汁酸的特异性受体。结肠对胆汁酸的吸收随温度的变化而变化,并与结肠膜的流动性有关。不诱导鸟氨酸脱羧酶(ODC)活性的去氢胆酸盐和牛磺胆酸盐的摄取程度与LC几乎相同。结肠粘膜细胞的31P核磁共振谱显示双层结构的比例增加了0.5 mM DOC。在检测的各种胆汁酸中,膜改变的程度与ODC诱导的程度平行。用0.5 mM DOC处理结肠黏膜,表面明显变性,但深层粘膜未见明显变性。因此,胆汁酸的生理浓度以一种非特异性的方式影响结肠粘膜的膜组织,这可能与促肿瘤活性有关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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