Aspartic peptidases are proteolytic enzymes present in many organisms like vertebrates, plants, fungi, protozoa and in some retroviruses such as human immunodeficiency virus (HIV). These enzymes are involved in important metabolic processes in microorganisms/virus and play major roles in infectious diseases. Although few studies have been performed in order to identify and characterize aspartic peptidase in trypanosomatids, which include the etiologic agents of leishmaniasis, Chagas’ disease and sleeping sickness, some beneficial properties of aspartic peptidase inhibitors have been described on fundamental biological events of these pathogenic agents. In this context, aspartic peptidase inhibitors (PIs) used in the current chemotherapy against HIV (e.g., amprenavir, indinavir, lopinavir, nelfinavir, ritonavir and saquinavir) were able to inhibit the aspartic peptidase activity produced by different species of Leishmania. Moreover, the treatment of Leishmania promastigotes with HIV PIs induced several perturbations on the parasite homeostasis, including loss of the motility and arrest of proliferation/growth. The HIV PIs also induced an increase in the level of reactive oxygen species and the appearance of irreversible morphological alterations, triggering parasite death pathways such as programed cell death (apoptosis) and uncontrolled autophagy. The blockage of physiological parasite events as well as the induction of death pathways culminated in its incapacity to adhere, survive and escape of phagocytic cells. Collectively, these results support the data showing that parasites treated with HIV PIs have a significant reduction in the ability to cause in vivo infection. Similarly, the treatment of Trypanosoma cruzi cells with pepstatin A showed a significant inhibition on both aspartic peptidase activity and growth as well as promoted several and irreversible morphological changes. These studies indicate that aspartic peptidases can be promising targets in trypanosomatid cells and aspartic proteolytic inhibitors can be benefic chemotherapeutic agents against these human pathogenic microorganisms.
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机译:天冬氨酸肽酶是蛋白水解酶,存在于许多生物中,例如脊椎动物,植物,真菌,原生动物和某些逆转录病毒中,例如人类免疫缺陷病毒(HIV)。这些酶参与微生物/病毒的重要代谢过程,并在传染病中起主要作用。尽管很少进行研究来鉴定和表征锥虫病中的天冬氨酸肽酶,包括利什曼病,查加斯病和昏睡病的病原体,但已针对这些病原体的基本生物学事件描述了天冬氨酸肽酶抑制剂的一些有益特性。 。在这种情况下,当前针对HIV的化学疗法中使用的天冬氨酸肽酶抑制剂(PI)(例如,氨普那韦,茚地那韦,洛匹那韦,奈非那韦,利托那韦和沙奎那韦)能够抑制利什曼原虫不同种类产生的天冬氨酸肽酶活性。此外,用HIV PIs治疗利什曼原虫前鞭毛体会引起寄生虫体内稳态的几种干扰,包括丧失活力和阻止增殖/生长。 HIV PI也诱导了活性氧水平的增加和不可逆形态变化的出现,触发了寄生虫死亡途径,如程序性细胞死亡(细胞凋亡)和自噬失控。生理寄生虫事件的阻断以及死亡途径的诱导导致其无法吞噬细胞的粘附,存活和逃逸。总的来说,这些结果支持了数据,表明用HIV PIs治疗的寄生虫导致体内感染的能力大大降低。同样,用胃抑素A处理克氏锥虫细胞对天冬氨酸肽酶活性和生长均具有显着抑制作用,并促进了几种不可逆的形态变化。这些研究表明,天冬氨酸肽酶可能是锥虫细胞中有希望的靶标,而天冬氨酸蛋白水解抑制剂可以是针对这些人类病原微生物的有益化学治疗剂。
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