内化
内吞作用
胞饮病
克洛丹
并行传输
细胞生物学
小窝
共域化
内体
细胞外
化学
网格蛋白
内吞循环
生物
细胞内
信号转导
紧密连接
细胞
生物化学
磁导率
膜
作者
Denise Zwanziger,Christian Staat,Anuska V. Andjelkovic,Ingolf E. Blasig
标识
DOI:10.1111/j.1749-6632.2012.06567.x
摘要
Claudin proteins are involved in the paracellular tightening of epithelia and endothelia. Their internalization, which can be modulated by extracellular stimuli, for example, proinflammatory cytokines, is a prerequisite for the regulation of the paracellular barrier to allow, for instance, cell migration or drug delivery. The internalization of peptide sequences of claudins is completely unknown. Here, we studied the internalization of two peptides, TAMRA‐claudin‐1 and TAMRA‐claudin‐5, derivatives of the extracellular loop of claudin‐1 and ‐5, respectively, in either epithelial or endothelial cells. The cellular uptake of the claudin‐1 peptide follows the clathrin‐mediated endocytosis as indicated by inhibitors and respective tracers for colocalization. In addition, macropinocytosis and caveolae‐mediated endocytosis of the peptide was observed. In contrast, the claudin‐5 peptide is mainly internalized via the caveolae‐mediated endocytosis evidenced by the colocalization with respective tracers and vesicle markers, whereas the nonselective macropinocytosis seems to be involved in a less effective manner. In conclusion, the assumption is supported that claudin peptides can be internalized by specific and nonspecific pathways.
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