首页> 外文期刊>Biochimica et biophysica acta. Biomembranes >Modulation of Orai1 by cationic peptides triggers their direct cytosolic uptake
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Modulation of Orai1 by cationic peptides triggers their direct cytosolic uptake

机译:阳离子肽的调节术触发其直接细胞溶质摄取

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摘要

At concentrations exceeding 10 mu M, arginine-rich cell-penetrating peptides (CPPs) trigger a rapid cytoplasmic import that involves activation of acid sphingomyelinase (ASMase). ASMase activation occurs through a variety of stress signals and has also been related to the reorganization of membrane microdomains during entry of pathogens. However, in none of these cases has the initial trigger for ASMase activation been established on a molecular level. We here show that rapid cytosolic CPP import depends upon an increase in intracellular calcium, likely caused by modulation of the Orai1 calcium channel. At low peptide concentration, cytoplasmic import could be induced by thapsigargin, a known activator of Orai1. Compounds known to block Orai1 inhibited rapid uptake. Peptide-mediated modulation of Orai1 involved cell surface sialic acids as inhibition of sialylation as well as chemical blocking of sialic acids reduced rapid cytoplasmic uptake, which could be reconstituted by thapsigargin. These results establish a link between the known propensity of arginine-rich CPPs to interact with the glycocalyx and calcium influx as the initial step triggering direct cytosolic peptide uptake.
机译:在超过10μm的浓度下,富含精氨酸的细胞穿透肽(CPP)引发了一种快速的细胞质进口,涉及酸鞘氨基酶(Asmase)的激活。 ASMase激活通过各种应力信号发生,并且在病原体过程中也与膜微瘤的重组有关。然而,在这些情况下,没有在分子水平上建立ASMase活化的初始触发。我们在这里表明,快速的细胞源CPP进口取决于细胞内钙的增加,可能是由奥莱钙通道的调节引起的。在低肽浓度下,通过Thapsigargin,可通过Orai1的已知活化剂诱导细胞质进口。嵌段嵌段1的化合物抑制了快速摄取。肽介导的orai1涉及细胞表面唾液酸作为唾液酸化的抑制以及唾液酸的化学阻断减少了快速的细胞质摄取,这可以由T​​hapsigarge重构。这些结果建立了已知的富含精氨酸的CPP的倾向与甘油癌相互作用,作为初始步骤引发直接细胞溶质肽摄取的糖钙钙和钙流入。

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