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克氏锥虫基因组中的 DNA G-四链体作为恰加斯病的潜在治疗靶点:二噻吩乙烯配体作为有效的抗寄生虫药物。

DNA G-quadruplexes in the genome of Trypanosoma cruzi as potential therapeutic targets for Chagas disease: Dithienylethene ligands as effective antiparasitic agents.

机构信息

Departamento de Biología Molecular, Instituto de Parasitología y Biomedicina López Neyra, CSIC, PTS Granada, Avenida Del Conocimiento, 17, Armilla, 18016 Granada, Spain.

School of Chemistry, University of Bristol, Bristol BS8 1TS, United Kingdom.

出版信息

Eur J Med Chem. 2024 Oct 5;276:116641. doi: 10.1016/j.ejmech.2024.116641. Epub 2024 Jul 1.

Abstract

Chagas disease is caused by the parasite Trypanosoma cruzi and affects over 7 million people worldwide. The two actual treatments, Benznidazole (Bzn) and Nifurtimox, cause serious side effects due to their high toxicity leading to treatment abandonment by the patients. In this work, we propose DNA G-quadruplexes (G4) as potential therapeutic targets for this infectious disease. We have found 174 PQS per 100,000 nucleotides in the genome of T. cruzi and confirmed G4 formation of three frequent motifs. We synthesized a family of 14 quadruplex ligands based in the dithienylethene (DTE) scaffold and demonstrated their binding to these identified G4 sequences. Several DTE derivatives exhibited micromolar activity against epimastigotes of four different strains of T. cruzi, in the same concentration range as Bzn. Compounds L3 and L4 presented remarkable activity against trypomastigotes, the active form in blood, of T. cruzi SOL strain (IC = 1.5-3.3 μM, SI = 25-40.9), being around 40 times more active than Bzn and displaying much better selectivity indexes.

摘要

恰加斯病是由寄生虫克氏锥虫引起的,影响着全球超过 700 万人。现有的两种实际治疗方法,苯并咪唑(Bzn)和硝呋替莫,由于其高毒性导致患者放弃治疗,会引起严重的副作用。在这项工作中,我们提出 DNA 四链体(G4)作为治疗这种传染病的潜在靶点。我们在克氏锥虫的基因组中发现了每 10 万个核苷酸中有 174 个 PQS,并证实了三个常见基序的 G4 形成。我们合成了一系列基于二噻吩乙烯(DTE)支架的 14 个四链体配体,并证明它们与这些已识别的 G4 序列结合。几种 DTE 衍生物对四种不同株系的克氏锥虫的滋养体表现出微摩尔活性,与 Bzn 的浓度范围相同。化合物 L3 和 L4 对克氏锥虫 SOL 株的血内活动形式——锥虫(IC = 1.5-3.3 μM,SI = 25-40.9)具有显著的活性,比 Bzn 活性高约 40 倍,且具有更好的选择性指数。

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