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豚鼠胃的平滑肌细胞拥有介导舒张作用的高亲和力甘丙肽受体。

Smooth muscle cells from guinea pig stomach possess high-affinity galanin receptors that mediate relaxation.

作者信息

Gu Z F, Pradhan T K, Coy D H, Jensen R T

机构信息

Digestive Diseases Branch, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, Maryland 20892.

出版信息

Am J Physiol. 1994 May;266(5 Pt 1):G839-45. doi: 10.1152/ajpgi.1994.266.5.G839.

Abstract

Galanin-like immunoactivity occurs in nerves and plexi in muscle layers throughout gastrointestinal tract including the stomach. Galanin can affect gastric emptying and contraction or relaxation of gastric muscle in different species. The aim of this study was to investigate the direct effect of galanin on dispersed gastric smooth muscle cells and to characterize any galanin receptors that mediated any effect. Dispersed gastric smooth muscle cells were prepared from guinea pig stomach by collagenase digestion. Porcine galanin (p-galanin; 1 microM) did not stimulate contraction when present alone; however, p-galanin (1 microM) inhibited carbachol-induced contraction with a half-maximal effect at 7 nM. p-Galanin (1 microM) increased cellular adenosine 3',5'-cyclic monophosphate (cAMP) content by 10 s and caused a maximal increase of 80% over basal. 125I-galanin (porcine) bound to dispersed cells in a time- and temperature-dependent manner. Binding was saturable, reversible, and specific. Binding of 125I-galanin was inhibited almost equally by porcine and rat galanin (Ki = 6-8 nM) but was not inhibited by the galanin-associated peptide [preprogalanin-(108-123)]. The fragment galanin-(1-16) was equally potent to rat galanin; however, the fragment galanin-(9-29) was 56-fold less potent (Ki = 370 nM). Computer analysis demonstrated there were two binding sites for p-galanin on gastric smooth muscle cells, a high-affinity site (Kd = 2.6 nM) with low capacity (Bmax = 175 fmol/mg protein) and a low-affinity site (Kd = 150 nM) with large capacity (Bmax = 3,611 fmol/mg protein).(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

甘丙肽样免疫活性存在于包括胃在内的整个胃肠道肌肉层的神经和神经丛中。甘丙肽可影响不同物种的胃排空以及胃肌的收缩或舒张。本研究的目的是探讨甘丙肽对分散的胃平滑肌细胞的直接作用,并鉴定介导任何作用的甘丙肽受体。通过胶原酶消化从豚鼠胃制备分散的胃平滑肌细胞。单独存在时,猪甘丙肽(p-甘丙肽;1微摩尔)不刺激收缩;然而,p-甘丙肽(1微摩尔)抑制卡巴胆碱诱导的收缩,半数最大效应浓度为7纳摩尔。p-甘丙肽(1微摩尔)在10秒内增加细胞内环磷酸腺苷(cAMP)含量,导致比基础水平最大增加80%。125I-甘丙肽(猪)以时间和温度依赖性方式与分散细胞结合。结合具有饱和性、可逆性和特异性。猪和大鼠甘丙肽对125I-甘丙肽结合的抑制作用几乎相同(Ki = 6 - 8纳摩尔),但甘丙肽相关肽[前甘丙肽-(108 - 123)]不抑制结合。甘丙肽-(1 - 16)片段与大鼠甘丙肽的效力相同;然而,甘丙肽-(9 - 29)片段的效力低56倍(Ki = 370纳摩尔)。计算机分析表明,胃平滑肌细胞上有两个p-甘丙肽结合位点,一个高亲和力位点(Kd = 2.6纳摩尔),容量低(Bmax = 175飞摩尔/毫克蛋白质),一个低亲和力位点(Kd = 150纳摩尔),容量大(Bmax = 3,611飞摩尔/毫克蛋白质)。(摘要截断于250字)

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