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作为CFTR介导的阴离子跨小肠黏膜分泌的决定因素的侧向细胞间隙体积。

Lateral intercellular space volume as a determinant of CFTR-mediated anion secretion across small intestinal mucosa.

作者信息

Gawenis Lara R, Boyle Kathryn T, Palmer Bradley A, Walker Nancy M, Clarke Lane L

机构信息

Dalton Cardiovascular Research Center and the Department of Biomedical Sciences, University of Missouri-Columbia, Columbia, Missouri 65211, USA.

出版信息

Am J Physiol Gastrointest Liver Physiol. 2004 Jun;286(6):G1015-23. doi: 10.1152/ajpgi.00468.2003. Epub 2004 Feb 5.

Abstract

Studies of full-thickness, small intestinal preparations have shown that maximal anion secretion [indexed by short-circuit current (I(sc))] during intracellular cAMP (cAMP(i)) stimulation is transient and followed by a decline toward baseline. Declining I(sc) is preceded by decreases in transepithelial conductance (G(t)), which in the small intestine reflects the lateral intercellular space (LIS) volume of the paracellular pathway. We hypothesized that decreases in LIS volume limit the magnitude and duration of cAMP(i)-stimulated anion secretion. Experimental manipulations to increase the patency of the LIS (assessed by G(t) and electron microscopy) were investigated for an effect on the magnitude of cAMP(i)-stimulated anion secretion (assessed by the I(sc) and isotopic fluxes) across murine small intestine. In control studies, changes of G(t) after cAMP(i) stimulation were associated with a morphological "collapse" of the LIS, which did not occur in intestine of CFTR-null mice. Removal of the outer intestinal musculature, exposure to a serosal hypertonic solution, or increased serosal hydrostatic pressure minimized reductions in G(t) and increased the cAMP(i)-stimulated I(sc) response. Increased I(sc) primarily resulted from increased Cl(-) secretion that was largely bumetanide sensitive. However, bumetanide-insensitive I(sc) was also increased, and similar increases occurred in the Na(+)-K(+)-2Cl(-) cotransporter (NKCC1)-null intestine, indicating that activities of non-NKCC1 anion uptake proteins are also affected by LIS volume. Thus LIS patency is an important determinant of the magnitude and duration of CFTR-mediated anion secretion in murine small intestine. Decreases in LIS volume may limit the pool of available anions to basolateral transporters involved in transepithelial secretion.

摘要

对全层小肠制剂的研究表明,细胞内cAMP(cAMP(i))刺激期间的最大阴离子分泌[以短路电流(I(sc))为指标]是短暂的,随后会降至基线水平。I(sc)下降之前,跨上皮电导(G(t))会降低,在小肠中,这反映了细胞旁途径的侧向细胞间隙(LIS)体积。我们推测,LIS体积的减小限制了cAMP(i)刺激的阴离子分泌的幅度和持续时间。研究了增加LIS通畅性的实验操作(通过G(t)和电子显微镜评估)对跨小鼠小肠的cAMP(i)刺激的阴离子分泌幅度(通过I(sc)和同位素通量评估)的影响。在对照研究中,cAMP(i)刺激后G(t)的变化与LIS的形态学“塌陷”有关,而这种情况在CFTR基因敲除小鼠的肠道中并未发生。去除外层肠道肌肉组织、暴露于浆膜高渗溶液或增加浆膜静水压力可使G(t)的降低最小化,并增强cAMP(i)刺激的I(sc)反应。I(sc)的增加主要源于Cl(-)分泌的增加,而Cl(-)分泌在很大程度上对布美他尼敏感。然而,布美他尼不敏感的I(sc)也增加了,并且在Na(+)-K(+)-2Cl(-)共转运体(NKCC1)基因敲除的肠道中也出现了类似的增加,这表明非NKCC1阴离子摄取蛋白的活性也受LIS体积的影响。因此,LIS的通畅性是小鼠小肠中CFTR介导的阴离子分泌幅度和持续时间的重要决定因素。LIS体积的减小可能会限制参与跨上皮分泌的基底外侧转运体可利用阴离子的储备。

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