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探索马立佐米对杜氏利什曼原虫和婴儿利什曼原虫的抗利什曼原虫潜力。

Exploring the and antileishmanial potential of Marizomib against and .

作者信息

Machado Patrícia de Almeida, Gomes Pollyanna Stephanie, Granato Juliana da Trindade, Lemos Ari Sérgio de Oliveira, Vicente Bruno, Midlej Victor do Valle, Coimbra Elaine Soares, de Matos Guedes Herbert Leonel

机构信息

Departamento de Patologia, Faculdade de Medicina, Universidade Federal Fluminense, Niterói, Brazil.

Laboratório de Imunologia Clínica, Instituto Oswaldo Cruz, Fundacao Oswaldo Cruz-Fiocruz, Rio de Janeiro, Brazil.

出版信息

Antimicrob Agents Chemother. 2025 Aug 6;69(8):e0028625. doi: 10.1128/aac.00286-25. Epub 2025 Jul 21.

Abstract

Current treatment available for leishmaniasis is fraught with numerous problems, so the search for new treatment alternatives for leishmaniasis is urgent and necessary. The proteasome has been selected as a promising target. Marizomib is a proteasome inhibitor and has shown antitumor effects, with ongoing clinical tests. In this work, we aimed to evaluate the and effects of Marizomib on and . Interestingly, Marizomib was not effective against promastigote forms of and but showed a significant effect against intracellular amastigotes of and , showing selectivity for the parasite when compared to the host cell. Furthermore, through transmission electron microscopy, it was possible to show that Marizomib induces extensive ultrastructural changes in amastigotes of and , such as the appearance of many vacuoles in the parasite cytoplasm and mitochondrial swelling. Marizomib was also shown to be effective in a murine model of cutaneous leishmaniasis, with a reduction in the size of lesions and parasite load in the footpads and draining lymph nodes of animals infected with . It is also effective in a model of visceral leishmaniasis, with a reduction in parasite load in the spleen and liver of animals infected with . Importantly, Marizomib, in the treatment regimens used, did not cause renal and hepatic acute toxicity to infected animals. These results highlight the antileishmanial potential of Marizomib, encouraging us to conduct preclinical tests in other animal models, as well as clinical trials.

摘要

目前可用于治疗利什曼病的方法存在诸多问题,因此寻找利什曼病的新治疗方案迫在眉睫且十分必要。蛋白酶体已被选为一个有前景的靶点。马里佐米布是一种蛋白酶体抑制剂,已显示出抗肿瘤作用,正在进行临床试验。在这项工作中,我们旨在评估马里佐米布对[具体寄生虫名称1]和[具体寄生虫名称2]的[具体作用1]和[具体作用2]。有趣的是,马里佐米布对[具体寄生虫名称1]和[具体寄生虫名称2]的前鞭毛体形式无效,但对[具体寄生虫名称1]和[具体寄生虫名称2]的细胞内无鞭毛体显示出显著作用,与宿主细胞相比,对寄生虫具有选择性。此外,通过透射电子显微镜可以显示,马里佐米布会在[具体寄生虫名称1]和[具体寄生虫名称2]的无鞭毛体中诱导广泛的超微结构变化,例如寄生虫细胞质中出现许多液泡以及线粒体肿胀。马里佐米布在皮肤利什曼病的小鼠模型中也显示出有效性,感染[具体寄生虫名称3]的动物脚垫和引流淋巴结中的病变大小和寄生虫载量有所减少。它在内脏利什曼病模型中也有效,感染[具体寄生虫名称4]的动物脾脏和肝脏中的寄生虫载量减少。重要的是,在所使用的治疗方案中,马里佐米布不会对感染动物造成肾和肝急性毒性。这些结果突出了马里佐米布的抗利什曼原虫潜力,鼓励我们在其他动物模型中进行临床前试验以及临床试验。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9b71/12326984/3ce3eab46527/aac.00286-25.f001.jpg

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