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血管灌注对3 - O - 甲基 - D - 葡萄糖在小肠内及跨小肠的积累、分布和转运的影响。

Effects of vascular perfusion on the accumulation, distribution and transfer of 3-O-methyl-D-glucose within and across the small intestine.

作者信息

Boyd C A, Parsons D S

出版信息

J Physiol. 1978 Jan;274:17-36. doi: 10.1113/jphysiol.1978.sp012131.

Abstract
  1. Factors affecting the transfer of the non-metabolized, ;actively transported' sugar, 3-O-methyl-D-glucose (3MG) across the small intestinal epithelium have been examined in vascularly perfused anuran intestine. Transfer has been studied during absorption in the steady state, and also during the period of transition from one steady state to another.2. During the steady state, the rate of absorption of 3MG from the intestinal lumen is equal to the rate of appearance in the portal venous effluent; this rate of transfer is to a small, but significant, extent directly related to the rate of arterial perfusion. With phlorizin in the intestinal lumen, transfer across the epithelium is reduced to very low rates which are independent of the rate of vascular perfusion.3. The apparent size of the tissue pool(s) of 3MG that have to be loaded to achieve the steady state rate of transfer are less than those that unload into the vascular bed after 3MG is removed from the intestinal lumen. This ;up-down asymmetry' is abolished when phlorizin is present in the intestinal lumen during the unloading phase.4. When 3MG is abruptly removed from the intestinal lumen after the tissue has been previously loaded with the sugar, the rate of washout into the vascular bed can be described by the sum of two exponential terms. The two terms differ in that the rate constant of the earlier ;fast' term is sensitive to the rate of vascular perfusion, while the later, ;slow', rate constant is insensitive to flow rate. The total quantity of 3MG that can be unloaded from the tissue into the portal venous effluent is decreased when phlorizin is present in the intestinal lumen during the unloading phase.5. Absorption from the lumen of the anuran intestine continues while the mesenteric circulation is interrupted. An estimate of the concentration of 3MG during the period of vascular stoppage can be made from the quantity recovered in the portal venous effluent when vascular perfusion is reinstituted (;vascular stop-flow'). The extent of the accumulation depends upon the duration of the vascular stoppage and the presence of Na ions in the intestinal lumen is essential for accumulation to occur.6. The findings are discussed in relation to the transfer of 3MG between various possible compartments in the tissue during absorption. Evidence is presented that a re-uptake of previously absorbed 3MG may occur across the brush border membrane. Such a recycling of 3MG across the epithelium implies that the apparent unidirectional fluxes measured across the epithelium between the bulk phase of the lumen and the blood may underestimate the size of fluxes across the epithelium at the cellular level.
摘要
  1. 研究了影响非代谢性“主动转运”糖3 - O - 甲基 - D - 葡萄糖(3MG)跨蟾蜍小肠上皮转运的因素。在血管灌注的蟾蜍小肠中进行了转运研究,包括稳态吸收期间以及从一种稳态转变到另一种稳态的过渡期间。

  2. 在稳态期间,3MG从肠腔的吸收速率等于门静脉流出液中出现的速率;这种转运速率在很小但显著的程度上与动脉灌注速率直接相关。当肠腔中有根皮苷时,跨上皮的转运速率降低到非常低的水平,且与血管灌注速率无关。

  3. 为达到稳态转运速率而必须加载的3MG组织池的表观大小小于从肠腔中去除3MG后卸载到血管床中的大小。当在卸载阶段肠腔中存在根皮苷时,这种“上下不对称”消失。

  4. 当组织预先加载该糖后,突然从肠腔中去除3MG时,进入血管床的洗脱速率可用两个指数项之和来描述。这两个项的不同之处在于,较早的“快速”项的速率常数对血管灌注速率敏感,而较晚的“缓慢”速率常数对流速不敏感。当在卸载阶段肠腔中存在根皮苷时,从组织卸载到门静脉流出液中的3MG总量会减少。

  5. 在肠系膜循环中断时,蟾蜍小肠腔的吸收仍在继续。当恢复血管灌注(“血管停流”)时,可以根据门静脉流出液中回收的量来估计血管阻断期间3MG的浓度。积累程度取决于血管阻断的持续时间,并且肠腔中钠离子的存在对于积累的发生至关重要。

  6. 结合吸收过程中3MG在组织中各种可能隔室之间的转运对这些发现进行了讨论。有证据表明,先前吸收的3MG可能会跨刷状缘膜重新摄取。这种3MG跨上皮的循环意味着,在肠腔和血液的体相之间跨上皮测量的表观单向通量可能低估了细胞水平上跨上皮通量的大小。

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