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齐墩果酸作为一种抗疟天然化合物的多靶向活性。

Multi-targeted activity of maslinic acid as an antimalarial natural compound.

机构信息

Departamento de Bioquímica y Biología Molecular IV, Facultad de Veterinaria, Universidad Complutense de Madrid, Spain.

出版信息

FEBS J. 2011 Aug;278(16):2951-61. doi: 10.1111/j.1742-4658.2011.08220.x. Epub 2011 Jul 7.

DOI:10.1111/j.1742-4658.2011.08220.x
PMID:21689375
Abstract

Most drugs against malaria that are available or under development target a single process of the parasite infective cycle, favouring the appearance of resistant mutants which are easily spread in areas under chemotherapeutic treatments. Maslinic acid (MA) is a low toxic natural pentacyclic triterpene for which a wide variety of biological and therapeutic activities have been reported. Previous work revealed that Plasmodium falciparum erythrocytic cultures were inhibited by MA, which was able to hinder the maturation from ring to schizont stage and, as a consequence, prevent the release of merozoites and the subsequent invasion. We show here that MA effectively inhibits the proteolytic processing of the merozoite surface protein complex, probably by inhibition of PfSUB1. In addition, MA was also found to inhibit metalloproteases of the M16 family by a non-chelating mechanism, suggesting the possible hindrance of plasmodial metalloproteases belonging to that family, such as falcilysin and apicoplast peptide-processing proteases. Finally, in silico target screening was used to search for other potential binding targets that may have remained undetected. Among the targets identified, the method recovered two for which experimental activity could be confirmed, and suggested several putative new targets to which MA could have affinity. One of these unreported targets, phospholipase A2, was shown to be partially inhibited by MA. These results suggest that MA may behave as a multi-targeted drug against the intra-erythrocytic cycle of Plasmodium, providing a new tool to investigate the synergistic effect of inhibiting several unrelated processes with a single compound, a new concept in antimalarial research.

摘要

大多数现有的或正在开发的抗疟药物针对寄生虫感染周期的单一过程,这有利于在化学治疗处理的地区中易于传播的耐药突变体的出现。齐墩果酸(MA)是一种低毒的天然五环三萜,已有广泛的生物学和治疗活性的报道。以前的工作表明,疟原虫红细胞培养物被 MA 抑制,MA 能够阻止从环到裂殖体阶段的成熟,因此阻止裂殖体的释放和随后的入侵。我们在这里表明,MA 有效地抑制裂殖子表面蛋白复合物的蛋白水解加工,可能通过抑制 PfSUB1。此外,MA 还被发现通过非螯合机制抑制 M16 家族的金属蛋白酶,表明可能阻碍属于该家族的疟原虫金属蛋白酶,如 falcilysin 和质体肽加工蛋白酶。最后,使用计算机靶标筛选来搜索可能未被发现的其他潜在结合靶标。在所鉴定的靶标中,该方法恢复了两个可通过实验证实活性的靶标,并提出了几个可能的新靶标,MA 可能与这些靶标具有亲和力。这些未报道的靶标之一,磷脂酶 A2,被证明部分被 MA 抑制。这些结果表明,MA 可能作为一种针对疟原虫红细胞内周期的多靶药物,为用单一化合物抑制几个不相关的过程的协同作用提供了一个新的工具,这是抗疟研究中的一个新概念。

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