蝎脂解第二激活蛋白的鉴定。

N Soudani, J Gharbi-Chihi, N Srairi-Abid, H Kaabi, A Margotat, J Torresani, M El Ayeb
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引用次数: 0

摘要

除了先前描述的LVP1蛋白外,还从蝎蝎(Buthus occitanus tunetanus)毒液中纯化了诱导脂肪细胞脂溶反应的第二种蛋白LVP2。占蛇毒总蛋白的2%,pHi = 6,分子量为16889 Da。LVP2的还原和烷基化反应显示为异二聚体结构。分离得到的LVP2 α链和β链分子量分别为8822 Da和8902。该蛋白对小鼠没有毒性,并以剂量依赖的方式刺激新解离的大鼠脂肪细胞的脂肪分解,EC50 = 2 +/- 0.75微克/毫升。LVP2亚基未表现出任何脂溶活性。如前所述的毒液和LVP1, β肾上腺素能受体(β AR)拮抗剂干扰LVP2活性。此外,研究表明LVP2与[3H] CGP 12177 (beta1/beta2 AR拮抗剂)竞争脂肪细胞膜结合,IC50约为10(-7)M。因此,这些结果为蝎子毒液中存在的蛋白质提供了原始信息,这些蛋白质可以通过β型肾上腺素受体途径对脂肪细胞脂解发挥独特的生物活性。
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Identification of second lipolysis activating protein from scorpion Buthus occitanus tunetanus.

Besides the previously described LVP1, a second protein, LVP2, inducing a lipolytic response in adipose cells, was purified from scorpion Buthus occitanus tunetanus venom. It represented 2% of crude venom proteins, with pHi = 6 and molecular mass of 16889 Da. The reduction and the alkylation of LVP2 revealed an heterodimeric structure. Isolated alpha and beta chains of LVP2 have a molecular weight (MW) of 8822 Da and 8902, respectively. This protein was not toxic to mice and stimulated lipolysis on freshly dissociated rat adipocytes in a dose-dependent manner with EC50 = 2 +/- 0.75 microg/ml. LVP2 subunits did not display any lipolytic activity. As previously described for venom and LVP1, beta adrenergic receptor (beta AR) antagonists interfere with LVP2 activity. Furthermore, it is shown that LVP2 competes with [3H] CGP 12177 (beta1/beta2 AR antagonist) for binding to adipocyte plasma membrane with an IC50 of about 10(-7)M. Thus, these results bring original information on the existence of proteins that are present in scorpion venoms and can exert a distinct biological activity on adipocyte lipolysis through a beta-type adreno-receptor pathway.

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