Ablation of connexin43 in smooth muscle cells of the mouse intestine: functional insights into physiology and morphology

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作者
Britta Döring
Gabriele Pfitzer
Birgit Adam
Tobias Liebregts
Dominik Eckardt
Gerald Holtmann
Franz Hofmann
Susanne Feil
Robert Feil
Klaus Willecke
机构
[1] Institut für Genetik,Abteilung Molekulargenetik
[2] Universität Bonn,Department of Gastroenterology, Hepatology and General Internal Medicine
[3] Max-Planck-Institut für Immunbiologie,Institut für Pharmakologie und Toxikologie
[4] Institut für Vegetative Physiologie,Interfakultäres Institut für Biochemie
[5] Universität Köln,undefined
[6] Royal Adelaide Hospital,undefined
[7] University of Adelaide,undefined
[8] Technische Universität München,undefined
[9] Universität Tübingen,undefined
来源
Cell and Tissue Research | 2007年 / 327卷
关键词
Gap junction; Smooth muscle cell; Cre/loxP; Gut function; Mouse (transgenic);
D O I
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中图分类号
学科分类号
摘要
Connexin43 (Cx43) gap-junction channels are highly abundant in intestinal smooth muscle but their functional impact has not been studied so far. Here, we have aimed to elucidate the functional role of Cx43 in the tunica muscularis of the mouse intestine in vivo. Transgenic mice with conditional deletion of Cx43 in smooth muscle cells (SMC) were generated. Histological investigations by immunofluorescence analyses and organ-bath recordings to assess the contractility of intestinal tissue strips were carried out. Measurements of gastrointestinal transit and of the visceromotor response by utilizing a standardized colorectal distension model to quantify alterations of visceral sensory function were also performed in SMC-specific Cx43 null mice and control littermates. Histologically, we found thickening of the tunica muscularis and a 13-fold increase of neutrophil infiltration of the gastrointestinal wall of SMC-specific Cx43 null mice. These animals also exhibited a decrease of 29% in gastrointestinal transit time. In contrast, the visceromotor response to a standardized colorectal distension was elevated, as was the contractility in SMC-specific Cx43 null mice, compared with controls. Thus, SMC-specific ablation of Cx43 in mice leads to morphological and functional alterations of the intestinal tunica muscularis, to gastrointestinal motor dysfunction and to altered visceral sensory function.
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