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Mucins, Mucus, and Goblet Cells

机译:粘蛋白,粘液和脚杯细胞

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The respiratory epithelium is lined by mucus, a gel consisting of water, ions, proteins, and macromolecules. The major macromolecular components of mucus are the mucin glycoproteins, which are critical for local defense of the airway. There are three classes of mucins in the airways: those that are secreted but do not polymerize (MUC7), those that are secreted and polymerize to form gels (MUC5AC, MUC5B), and those that have transmembrane domains and are cell surface associated (MUC1, MUC4, MUC16, MUC20). The mucins are regulated at the transcriptional, posttranscriptional, and epigenetic levels, and posttranslational modifications play an important role in mucin binding and clearance of microbes and pollutants. The development of mice deficient in specific mucins, and the cystic fibrosis pig, has greatly advanced our understanding of the role of mucins as innate immune mediators and how mucins and mucus contribute to lung disease. These observations suggest new strategies to ameliorate mucus obstruction by targeting mucociliary clearance and mucin hyperconcentration. Furthermore, a polymorphism in the promoter of MUC5B is strongly associated with risk of developing pulmonary fibrosis, supporting a novel function for MUC5B to influence interstitial lung disease. Exciting new data support the concept not only that mucins and mucus are important for lung homeostasis and protection from environmental threats but also that goblet cells play an important role as regulators of innate immune function. These insights into the innate immune properties of mucins and goblet cells support a shift from the current paradigm of repressing increased mucin expression to targeting regulation of specific mucins and the abnormal airway milieu.
机译:呼吸上皮内衬通过粘液,由水,离子,蛋白质和大分子组成的凝胶。粘液的主要大分子成分是粘蛋白糖蛋白,这对于局部防御气道至关重要。气道中有三类粘蛋白:分泌但不聚合(MUC7)的那些,它们分泌和聚合以形成凝胶(MUC5Ac,MUC5B)和具有跨膜结构域的那些,并且是相关的(MUC1 ,muc4,muc16,muc20)。粘蛋白在转录,后颅面和表观遗传水平上调节,后期修饰在粘蛋白结合和微生物和污染物的间隙中起重要作用。缺乏特定粘蛋白的小鼠和囊性纤维化猪的发展,大大提高了对粘液作为先天免疫介质的作用的理解,以及粘蛋白和粘液如何为肺病有助于肺病。这些观察结果表明,通过靶向粘液间隙和粘蛋白超复制来提出改善粘液梗阻的新策略。此外,MUC5B启动子的多态性与发育肺纤维化的风险强烈有关,支持MUC5B的新功能以影响间质性肺病。令人兴奋的新数据不仅支持粘蛋白和粘液对肺稳态和保护环境威胁重要的概念,而且还具有戈尔特细胞作为先天免疫功能的调节剂发挥重要作用。这些见解粘蛋白和杯状细胞的先天免疫特性支持从抑制粘液表达的当前范式转变,以靶向调节特定粘蛋白和异常气道Milieu。

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