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黏膜丛与电解质跨大鼠结肠黏膜的转运

Mucosal plexus and electrolyte transport across the rat colonic mucosa.

作者信息

Bridges R J, Rack M, Rummel W, Schreiner J

出版信息

J Physiol. 1986 Jul;376:531-42. doi: 10.1113/jphysiol.1986.sp016168.

Abstract

Histological and functional studies were performed on a preparation of rat colonic mucosa from which the myenteric and submucosal plexus were removed. This preparation, referred to as the mucosa preparation, was used to investigate the potential influence of the mucosal plexus on electrolyte transport. Two neuropharmacologically active agents were used: sea anemone toxin (ATX II) to stimulate the fibres of the mucosal plexus and tetrodotoxin (TTX) to block the fibres of the mucosal plexus. The morphology of the neuronal network of the mucosal plexus was visualized after the epithelium was removed and whole mount preparations of the lamina propria and circular muscle layer of muscularis mucosae were stained histochemically for acetylcholinesterase activity. Several levels of organization within the mucosal plexus were seen. Each crypt is encircled by a thin bundle of fibres near the top. These thin fibres connect with thicker bundles of fibres that encircle groups of two to five crypts in a broad band. These bundles of fibres are in turn connected to larger bundles of fibres which lie in a flat plane just below the crypts along the circular muscle layer of muscularis mucosae. In addition perikarya and ganglia were revealed within the mucosal plexus. The base-line net transport of Na+ and Cl- across the mucosa preparation was completely inhibited by ATX II (10(-6) M). This effect of ATX II on net Na+ and Cl- transport was accompanied with an increase in the short-circuit current (Isc), transmural conductance, and open-circuit potential difference across the mucosa preparation. The effect of ATX II on Isc was dose dependent with a half-maximal effective concentration at 5 X 10(-8) M-ATX II and a maximal effective concentration of 10(-7) M. ATX II was effective only when added to the serosal solution. Net Na+ and Cl- transport was restored by TTX (10(-6) M) to base-line values in ATX II-treated tissue. In addition the value of all three electrical parameters rapidly returned to the values measured before the addition of ATX II. TTX was effective in antagonizing the effects of ATX II only when added to the serosal solution. The results suggest that the regulation of electrolyte transport across the epithelium is at least one function of the mucosal plexus. Stimulation of the neurones within the mucosal plexus leads to the inhibition of electrolyte absorption.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

对去除了肌间神经丛和黏膜下神经丛的大鼠结肠黏膜标本进行了组织学和功能研究。这种标本被称为黏膜标本,用于研究黏膜神经丛对电解质转运的潜在影响。使用了两种具有神经药理学活性的药物:海葵毒素(ATX II)来刺激黏膜神经丛的纤维,河豚毒素(TTX)来阻断黏膜神经丛的纤维。在去除上皮后,对黏膜固有层和黏膜肌层环行肌层的整装标本进行乙酰胆碱酯酶活性的组织化学染色,从而观察黏膜神经丛神经元网络的形态。在黏膜神经丛内可见到几个组织层次。每个隐窝在顶部附近被一束细纤维环绕。这些细纤维与较粗的纤维束相连,较粗的纤维束在一个宽带中环绕两到五个隐窝组。这些纤维束又与更大的纤维束相连,这些更大的纤维束位于隐窝下方沿着黏膜肌层环行肌层的一个平面内。此外,在黏膜神经丛内还发现了神经细胞体和神经节。ATX II(10⁻⁶ M)完全抑制了跨黏膜标本的Na⁺和Cl⁻的基线净转运。ATX II对Na⁺和Cl⁻净转运的这种作用伴随着黏膜标本的短路电流(Isc)、跨膜电导和开路电位差的增加。ATX II对Isc的作用呈剂量依赖性,半数有效浓度为5×10⁻⁸ M - ATX II,最大有效浓度为10⁻⁷ M。ATX II仅在加入浆膜溶液时才有效。TTX(10⁻⁶ M)使ATX II处理的组织中的Na⁺和Cl⁻净转运恢复到基线值。此外,所有三个电参数的值迅速恢复到加入ATX II之前测量的值。TTX仅在加入浆膜溶液时才有效拮抗ATX II的作用。结果表明,跨上皮的电解质转运调节至少是黏膜神经丛的一项功能。刺激黏膜神经丛内的神经元会导致电解质吸收受到抑制。(摘要截断于400字)

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/7d79/1182813/9cc5d9592c4f/jphysiol00550-0547-a.jpg

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