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首页> 外文期刊>Peptides: An International Journal >Thymosin beta4 and thymosin beta4-derived peptides induce mast cell exocytosis.
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Thymosin beta4 and thymosin beta4-derived peptides induce mast cell exocytosis.

机译:胸腺素β4和胸腺素β4衍生的肽诱导肥大细胞胞吐作用。

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摘要

The peptide thymosin beta4 (Tbeta4) promotes angiogenesis and wound healing. Mast cells are involved in these processes as well and therefore we investigated the effect of Tbeta4 on mast cells. Exposure to 0.2-2000nM Tbeta4 induced mediator release (up to 23%) in murine peritoneal and human HMC-1 mast cells in a concentration-dependent manner. While the peptide AcSDKP, matching the 4 N-terminal amino acid residues of Tbeta4, mediated low but detectable mediator release, peptides corresponding to the Tbeta4 amino acid sequences 16-38 and 17-23 stimulated mast cells mediator release on a level equal to or higher than that observed with native Tbeta4. These observations and certain characteristics of Tbeta4-mediated mast cell activation suggest that the actin-binding motif LKKTET present in Tbeta4 (amino acid 17-22) might be implicated in this process. Thus, Tbeta4 activates mediator release in mast cells by a process that possibly involves an actin-binding motif and this could be important for understanding the mechanisms of Tbeta4-mediated effects in vivo.
机译:肽胸腺素β4(Tbeta4)促进血管生成和伤口愈合。肥大细胞也参与这些过程,因此我们研究了Tbeta4对肥大细胞的作用。暴露于小鼠腹膜和人类HMC-1肥大细胞中的0.2-2000nM Tbeta4诱导介体释放(高达23%),呈浓度依赖性。虽然与Tbeta4的4个N末端氨基酸残基匹配的肽AcSDKP介导了低但可检测的介体释放,但对应于Tbeta4氨基酸序列16-38和17-23的肽刺激肥大细胞的介导剂释放水平等于或高于天然Tbeta4所观察到的。这些观察结果和Tbeta4介导的肥大细胞活化的某些特征表明,存在于Tbeta4中的肌动蛋白结合基序LKKTET(氨基酸17-22)可能与这一过程有关。因此,Tbeta4通过可能涉及肌动蛋白结合基序的过程激活肥大细胞中的介质释放,这对于理解体内Tbeta4介导的作用机制可能很重要。

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