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卡氏棘口吸虫感染小鼠中约氏疟原虫疟疾的加重及通过驱虫治疗的减轻

Exacerbation of Plasmodium yoelii malaria in Echinostoma caproni infected mice and abatement through anthelmintic treatment.

作者信息

Noland Gregory S, Graczyk Thaddeus K, Fried Bernard, Fitzgerald Erik J, Kumar Nirbhay

机构信息

Johns Hopkins Malaria Research Institute, Department of Molecular Microbiology and Immunology, Bloomberg School of Public Health, Johns Hopkins University, Baltimore, Maryland 21205, USA.

出版信息

J Parasitol. 2005 Aug;91(4):944-8. doi: 10.1645/GE-456R.1.

Abstract

The effect of chronic intestinal trematode infection on malaria was examined in a murine model of co-infection using Echinostoma caproni and Plasmodium yoelii. BALB/c mice (n = 32) infected with a low dose of E. caproni (approximately 10 cysts) 25-35 days before malaria infection displayed significantly increased malaria parasitemia (P = 0.01), extended patency of malaria (P = 0.03), and increased fatality (47%; P < 0.001) compared to mice infected only with P. yoelii (17X nonlethal strain) (n = 18). Further analysis revealed that differences in malaria parasitemia between fatal co-infections and infections with P. yoelii only were highly significant (P < 0.0001), whereas nonfatal co-infections were not statistically different. Exacerbation of malaria was demonstrated to be reversible through clearance of E. caproni worms by praziquantel treatment administered 10 days before malaria infection. No deaths were observed during malaria infection in mice cleared of their E. caproni infection (n = 10), and parasitemia was significantly reduced from that of untreated co-infected mice (P = 0.03) and was not different from that of mice infected with P. yoelii only. Further studies examining parasite-parasite interactions and host immune response in the echinostome model are warranted to understand the mechanisms affecting the course and outcome of malaria infection during concomitant helminth infection.

摘要

在使用卡氏棘口吸虫和约氏疟原虫的共感染小鼠模型中,研究了慢性肠道吸虫感染对疟疾的影响。在疟疾感染前25 - 35天感染低剂量卡氏棘口吸虫(约10个囊蚴)的BALB/c小鼠(n = 32),与仅感染约氏疟原虫(17X非致死株)的小鼠(n = 18)相比,疟疾寄生虫血症显著增加(P = 0.01),疟疾持续时间延长(P = 0.03),死亡率增加(47%;P < 0.001)。进一步分析表明,致命共感染与仅感染约氏疟原虫之间的疟疾寄生虫血症差异非常显著(P < 0.0001),而非致命共感染在统计学上无差异。通过在疟疾感染前10天给予吡喹酮清除卡氏棘口吸虫,证明疟疾的恶化是可逆的。清除卡氏棘口吸虫感染的小鼠(n = 10)在疟疾感染期间未观察到死亡,其寄生虫血症与未治疗的共感染小鼠相比显著降低(P = 0.03),且与仅感染约氏疟原虫的小鼠无差异。有必要在棘口吸虫模型中进一步研究寄生虫 - 寄生虫相互作用和宿主免疫反应,以了解在合并蠕虫感染期间影响疟疾感染进程和结果的机制。

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