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Latrophilin 转染的肥大细胞中的拉托毒素诱导的胞吐作用。

Latrotoxin-induced exocytosis in mast cells transfected with latrophilin.

机构信息

Graduate School of Pharmaceutical Sciences, Nagoya City University, Tanabe-dori, Mizuho-ku, Nagoya 467-8603, Japan.

出版信息

Toxicon. 2010 Dec;56(8):1372-80. doi: 10.1016/j.toxicon.2010.08.002. Epub 2010 Aug 11.

Abstract

α-Latrotoxin (α-LTX) is known to cause massive exocytosis from presynaptic nerve terminals. We investigated the effects of α-LTX on exocytotic release from mast cells, typical non-neuronal secretory cells. When we transfected mast cells with latrophilin, a specific receptor for α-LTX, α-LTX caused intracellular Ca(2+) to increase and led to exocytosis in the presence of extracellular Ca(2+). On the other hand, neither Ca(2+) increase nor exocytosis was observed in the absence of extracellular Ca(2+). These results indicate that α-LTX, together with latrophilin, works as a Ca(2+) ionophore. However, α-LTX had additional effects on signal transduction in mast cells. We found that inhibitors of protein kinase C (PKC) partially suppressed exocytosis. Furthermore, several soluble N-ethylmaleimide-sensitive factor attachment protein receptor (SNARE) proteins, including SNAP-23, were phosphorylated by α-LTX. These results suggest that exocytosis induced by α-LTX can be explained by (1) elevation of intracellular Ca(2+), (2) phosphorylation of SNARE proteins including SNAP-23, syntaxin-4 and VAMP-8 through PKC-dependent and -independent pathways. Our study may provide a new system to investigate the action of α-LTX and the mechanism of exocytosis in mast cells.

摘要

α- 岩藻毒素(α-LTX)已知可引起突触前神经末梢的大量胞吐作用。我们研究了 α-LTX 对典型的非神经元分泌细胞肥大细胞胞吐释放的影响。当我们用 α-LTX 的特异性受体拉托蛋白转染肥大细胞时,α-LTX 在存在细胞外 Ca(2+)的情况下会导致细胞内 Ca(2+)增加,并导致胞吐作用。另一方面,在没有细胞外 Ca(2+)的情况下,既没有观察到 Ca(2+)增加,也没有观察到胞吐作用。这些结果表明,α-LTX 与拉托蛋白一起作为 Ca(2+)离子载体起作用。然而,α-LTX 对肥大细胞中的信号转导还有其他影响。我们发现蛋白激酶 C(PKC)抑制剂部分抑制了胞吐作用。此外,α-LTX 还使几种可溶性 N-乙基马来酰亚胺敏感因子附着蛋白受体(SNARE)蛋白,包括 SNAP-23,磷酸化。这些结果表明,α-LTX 诱导的胞吐作用可以通过以下两种途径来解释:(1)细胞内 Ca(2+)的升高;(2)通过 PKC 依赖和非依赖途径磷酸化 SNARE 蛋白,包括 SNAP-23、突触素-4 和 VAMP-8。我们的研究可能为研究 α-LTX 的作用和肥大细胞胞吐作用的机制提供了一个新的系统。

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