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Filarial Nematode Parasites Secrete a Homologue of the Human Cytokine Macrophage Migration Inhibitory Factor

巨噬细胞移动抑制因子 生物 马来丝虫 卷盘尾丝虫 班克罗夫提乌切列氏菌 多形螺旋线虫 丝虫总科 免疫学 巨噬细胞 细胞因子 分泌物 微生物学 免疫系统 丝虫病 蠕虫 盘尾丝虫病 体外 生物化学
作者
Diana V. Pastrana,Nithyakalyani Raghavan,Peter Fitzgerald,Stephen W. Eisinger,Christine N. Metz,Richard Bucala,Robert P. Schleimer,Carol A. Bickel,Alan L. Scott
出处
期刊:Infection and Immunity [American Society for Microbiology]
卷期号:66 (12): 5955-5963 被引量:196
标识
DOI:10.1128/iai.66.12.5955-5963.1998
摘要

ABSTRACT Filarial nematode parasites establish long-term chronic infections in the context of an antiparasite immunity that is strongly biased toward a Th2 response. The mechanisms that lead to this Th2 bias toward filarial antigens are not clear, but one possibility is that the parasites produce molecules that have the capacity to proactively modify their immunological environment. Here we report that filarial parasites of humans secrete a homologue of the human proinflammatory cytokine macrophage migration inhibitory factor (MIF) that has the capability of modifying the activity of human monocytes/macrophages. A cDNA clone isolated from a Brugia malayi infective-stage larva expression library encoded a 12.5-kDa protein product ( Bm -MIF) with 42% identity to human and murine MIF. MIF homologues were also found to be expressed in the related filarial species Wuchereria bancrofti and Onchocerca volvulus . Bm-mif was transcribed by adult and larval parasites, and the protein product was found in somatic extracts and in the parasite’s excretory-secretory products. Immunohistocytochemistry revealed that Bm -MIF was localized to cells of the hypodermis/lateral chord, the uterine wall, and larvae developing in utero. Unexpectedly, the activities of recombinant Bm- MIF and human MIF on human monocytes/macrophages were found to be similar. When placed with monocytes/macrophages in a cell migration assay, Bm -MIF inhibited random migration. When placed away from cells, Bm -MIF induced an increase in monocyte/macrophage migration that was specifically inhibited by neutralizing anti- Bm -MIF antibodies. Bm -MIF is the first demonstration that helminth parasites produce cytokine homologues that have the potential to modify host immune responses to promote parasite survival.
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