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二价阳离子化合物对克氏锥虫体外细胞内生长的抑制作用。

Inhibition of in vitro intracellular growth of Trypanosoma cruzi by dicationic compounds.

作者信息

Rowland Edwin C, Moore-Lai Deborah, Seed John R, Stephens Chad E, Boykin David W

机构信息

Biomedical Sciences Department, College of Osteopathic Medicine, Ohio University, Athens, Ohio 45701, USA.

出版信息

J Parasitol. 2003 Oct;89(5):1078-80. doi: 10.1645/GE-53R.

Abstract

Dicationic compounds, which are derivatives of pentamidine, are being developed for use as antiprotozoal drugs. These compounds bind to the minor groove of DNA and are thought to inhibit DNA-dependent enzymes and thereby prevent cellular replication by protozoans. The objective of this study was to test the ability of a group of these compounds to inhibit the intracellular and extracellular reproduction of Trypanosoma cruzi in vitro. At present, there are few drugs in use capable of inhibiting the intracellular stages of this parasite, and therefore compounds with this ability would be of value. Cultures of mouse fibroblasts were infected and treated with doses of dicationic compounds, and the numbers of parasites released at the end of the 5- to 7-day growth cycle were determined. Five of the compounds tested were found to be effective at inhibiting T. cruzi growth at doses that were not toxic to the host cells. The compound found most effective (DB709) inhibited parasite release at the low concentration of 0.8 ng/ ml, justifying further study. These results suggest that dicationic compounds may have potential as chemotherapy against T. cruzi infection.

摘要

作为戊烷脒衍生物的双阳离子化合物正在被开发用作抗原生动物药物。这些化合物与DNA的小沟结合,被认为可抑制依赖DNA的酶,从而阻止原生动物进行细胞复制。本研究的目的是测试一组此类化合物在体外抑制克氏锥虫细胞内和细胞外繁殖的能力。目前,能够抑制该寄生虫细胞内阶段的药物很少,因此具有这种能力的化合物将很有价值。用双阳离子化合物剂量感染并处理小鼠成纤维细胞培养物,并确定在5至7天生长周期结束时释放的寄生虫数量。测试的化合物中有五种被发现在对宿主细胞无毒的剂量下能有效抑制克氏锥虫生长。发现最有效的化合物(DB709)在0.8 ng/ml的低浓度下就能抑制寄生虫释放,这值得进一步研究。这些结果表明,双阳离子化合物可能具有作为抗克氏锥虫感染化疗药物的潜力。

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