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Munc18b 是一种在小鼠中必不可少的基因,其表达对气道上皮细胞和肥大细胞的分泌具有限制作用。

Munc18b is an essential gene in mice whose expression is limiting for secretion by airway epithelial and mast cells.

机构信息

Department of Pulmonary Medicine, The University of Texas MD Anderson Cancer Center, Houston, TX 77030, USA.

出版信息

Biochem J. 2012 Sep 15;446(3):383-94. doi: 10.1042/BJ20120057.

Abstract

Airway mucin secretion and MC (mast cell) degranulation must be tightly controlled for homoeostasis of the lungs and immune system respectively. We found the exocytic protein Munc18b to be highly expressed in mouse airway epithelial cells and MCs, and localized to the apical pole of airway secretory cells. To address its functions, we created a mouse with a severely hypomorphic Munc18b allele such that protein expression in heterozygotes was reduced by ~50%. Homozygous mutant mice were not viable, but heterozygotes showed a ~50% reduction in stimulated release of mucin from epithelial cells and granule contents from MCs. The defect in MCs affected only regulated secretion and not constitutive or transporter-mediated secretion. The severity of passive cutaneous anaphylaxis was also reduced by ~50%, showing that reduction of Munc18b expression results in an attenuation of physiological responses dependent on MC degranulation. The Munc18b promoter is controlled by INR (initiator), Sp1 (specificity protein 1), Ets, CRE (cAMP-response element), GRE (glucocorticoid-response element), GATA and E-box elements in airway epithelial cells; however, protein levels did not change during mucous metaplasia induced by allergic inflammation. Taken together, the results of the present study identify Munc18b as an essential gene that is a limiting component of the exocytic machinery of epithelial cells and MCs.

摘要

气道黏液分泌和 MC(肥大细胞)脱颗粒必须分别受到严格控制,以维持肺部和免疫系统的稳态。我们发现外排蛋白 Munc18b 在小鼠气道上皮细胞和 MC 中高度表达,并定位于气道分泌细胞的顶端。为了研究其功能,我们创建了一种 Munc18b 严重功能缺失型的小鼠,杂合子中蛋白表达减少约 50%。纯合子突变小鼠不能存活,但杂合子小鼠刺激后上皮细胞黏液释放和 MC 颗粒内容物的释放减少约 50%。MC 中的缺陷仅影响调节性分泌,而不影响组成型或转运体介导的分泌。被动皮肤过敏反应的严重程度也降低了约 50%,表明 Munc18b 表达的减少导致依赖 MC 脱颗粒的生理反应减弱。Munc18b 启动子在气道上皮细胞中受 INR(起始)、Sp1(特异性蛋白 1)、Ets、CRE(cAMP 反应元件)、GRE(糖皮质激素反应元件)、GATA 和 E-box 元件控制;然而,在过敏炎症诱导的黏液化生过程中,蛋白水平没有发生变化。综上所述,本研究的结果表明,Munc18b 是一种必需基因,是上皮细胞和 MC 外排机制的限制组成部分。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9c5d/3430001/295bd26eed4b/bic281i001.jpg

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