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小鼠中的疟疾-丝虫共感染会使疟疾病情更加严重,除非丝虫感染达到成虫期。

Malaria-filaria coinfection in mice makes malarial disease more severe unless filarial infection achieves patency.

作者信息

Graham Andrea L, Lamb Tracey J, Read Andrew F, Allen Judith E

机构信息

Institutes of Evolution, Immunology and Infection Research, School of Biological Sciences, University of Edinburgh, Edinburgh, Scotland.

出版信息

J Infect Dis. 2005 Feb 1;191(3):410-21. doi: 10.1086/426871. Epub 2004 Dec 21.

Abstract

Coinfections are common in natural populations, and the literature suggests that helminth coinfection readily affects how the immune system manages malaria. For example, type 1-dependent control of malaria parasitemia might be impaired by the type 2 milieu of preexisting helminth infection. Alternatively, immunomodulatory effects of helminths might affect the likelihood of malarial immunopathology. Using rodent models of lymphatic filariasis (Litomosoides sigmodontis) and noncerebral malaria (clone AS Plasmodium chabaudi chabaudi), we quantified disease severity, parasitemia, and polyclonal splenic immune responses in BALB/c mice. We found that coinfected mice, particularly those that did not have microfilaremia (Mf(-)), had more severe anemia and loss of body mass than did mice with malaria alone. Even when controlling for parasitemia, malaria was most severe in Mf(-) coinfected mice, and this was associated with increased interferon- gamma responsiveness. Thus, in Mf(-) mice, filariasis upset a delicate immunological balance in malaria infection and exacerbated malaria-induced immunopathology.

摘要

共感染在自然种群中很常见,并且文献表明蠕虫共感染很容易影响免疫系统对疟疾的控制方式。例如,预先存在的蠕虫感染的2型环境可能会损害1型依赖性对疟原虫血症的控制。或者,蠕虫的免疫调节作用可能会影响疟疾免疫病理学的可能性。使用淋巴丝虫病(Sigmodontis Litomosoides)和非脑型疟疾(克隆AS疟原虫chabaudi chabaudi)的啮齿动物模型,我们量化了BALB/c小鼠的疾病严重程度、疟原虫血症和多克隆脾脏免疫反应。我们发现,共感染的小鼠,特别是那些没有微丝蚴血症(Mf(-))的小鼠,比单独感染疟疾的小鼠有更严重的贫血和体重减轻。即使在控制疟原虫血症的情况下,疟疾在Mf(-)共感染小鼠中最为严重,这与干扰素-γ反应性增加有关。因此,在Mf(-)小鼠中,丝虫病扰乱了疟疾感染中微妙的免疫平衡,并加剧了疟疾诱导的免疫病理学。

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