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疟原虫的药物敏感性是否取决于其毒力?

Does the drug sensitivity of malaria parasites depend on their virulence?

作者信息

Schneider Petra, Chan Brian Hk, Reece Sarah E, Read Andrew F

机构信息

Institutes of Evolution, Immunology and Infection Research, University of Edinburgh, EH9 3JT, UK.

出版信息

Malar J. 2008 Dec 16;7:257. doi: 10.1186/1475-2875-7-257.

Abstract

BACKGROUND

Chemotherapy can prompt the evolution of classical drug resistance, but selection can also favour other parasite traits that confer a survival advantage in the presence of drugs. The experiments reported here test the hypothesis that sub-optimal drug treatment of malaria parasites might generate survival and transmission advantages for virulent parasites.

METHODS

Two Plasmodium chabaudi lines, one derived from the other by serial passage, were used to establish avirulent and virulent infections in mice. After five days, infections were treated with various doses of pyrimethamine administered over 1 or 4 days. Virulence measures (weight and anaemia), parasite and gametocyte dynamics were followed until day 21.

RESULTS

All treatment regimes reduced parasite and gametocyte densities, but infections with the virulent line always produced more parasites and more gametocytes than infections with the avirulent line. Consistent with our hypothesis, drug treatment was disproportionately effective against the less virulent parasites. Treatment did not affect the relative transmission advantage of the virulent line. Neither of the lines contained known mutations conferring classical drug resistance.

CONCLUSION

Drug-sensitivity of malaria parasites can be virulence-dependent, with virulent parasites more likely to survive sub-optimal treatment. If this proves to be general for a variety of drugs and parasite species, selection imposed by sub-optimal drug treatment could result in the evolution of more aggressive malaria parasites.

摘要

背景

化疗可促使经典耐药性的演变,但选择也可能有利于其他寄生虫特征,这些特征在有药物存在的情况下赋予生存优势。本文报道的实验检验了以下假设:对疟原虫进行次优药物治疗可能会为毒性较强的寄生虫带来生存和传播优势。

方法

使用两个来自查巴迪疟原虫品系,其中一个是通过连续传代从另一个衍生而来,在小鼠中建立无毒和有毒感染。五天后,用不同剂量的乙胺嘧啶在1天或4天内对感染进行治疗。跟踪毒性指标(体重和贫血)、寄生虫和配子体动态直至第21天。

结果

所有治疗方案均降低了寄生虫和配子体密度,但与无毒品系感染相比,有毒品系感染总是产生更多的寄生虫和更多的配子体。与我们的假设一致,药物治疗对毒性较小的寄生虫效果尤为显著。治疗并未影响有毒品系的相对传播优势。两个品系均未包含已知的赋予经典耐药性的突变。

结论

疟原虫的药物敏感性可能取决于毒性,毒性较强的寄生虫在次优治疗下更有可能存活。如果这被证明对多种药物和寄生虫物种普遍适用,次优药物治疗所施加的选择可能会导致更具侵袭性的疟原虫的进化。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/df62/2636820/24ae7f5d0730/1475-2875-7-257-1.jpg

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