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新生小鼠对不同十二指肠贾第鞭毛虫菌株的免疫和病理生理反应。

Immune and pathophysiological responses to different strains of Giardia duodenalis in neonatal mice.

作者信息

Williamson A L, O'Donoghue P J, Upcroft J A, Upcroft P

机构信息

Department of Microbiology and Parasitology, The University of Queensland, Qld 4072, Australia.

出版信息

Int J Parasitol. 2000 Feb;30(2):129-36. doi: 10.1016/s0020-7519(99)00181-2.

DOI:10.1016/s0020-7519(99)00181-2
PMID:10704595
Abstract

Numerous studies have demonstrated various strain differences between Giardia isolates, but little is known about the immunology and pathogenesis of infections. This study aimed to compare host responses to strains of Giardi duodenalis differing in levels of virulence and pathogenicity and, by doing so, elucidate the mechanisms via which pathogenic strains establish infections. Marked differences were found in the infection dynamics, histopathological responses and serum antibody responses of neonatal mice infected with either G. duodenalis strain BRIS/83/HEPU/106 (isolated from a human) or BRIS/95/HEPU/2041 (isolated from a sulphur-crested cockatoo, Cacatua galerita). Infections with the bird strain were more intense (6.7-times greater) and persisted longer (by 14days) than infections with the human strain. The bird strain was more pathogenic and caused greater pathophysiological alteration to the gut mucosa, including increased villous atrophy, hyperplasia of goblet cells and vacuolated epithelial cells. Mice infected with the bird strain produced less serum anti-Giardia IgA and IgM, but more total (non-specific) serum IgA than those infected with the human strain of Giardia. This suggests that avian G. duodenalis strains are infective for mammalian hosts and may contribute to zoonotic infections. Furthermore, infection of mice with BRIS/95/HEPU/2041 serves as a good experimental model to provide further insight into the mechanisms via which G. duodenalis causes disease.

摘要

众多研究已证实贾第虫分离株之间存在各种菌株差异,但对于感染的免疫学和发病机制却知之甚少。本研究旨在比较宿主对不同毒力和致病性水平的十二指肠贾第虫菌株的反应,并借此阐明致病菌株建立感染的机制。在感染了十二指肠贾第虫菌株BRIS/83/HEPU/106(从人类分离)或BRIS/95/HEPU/2041(从硫冠凤头鹦鹉,白凤头鹦鹉分离)的新生小鼠的感染动态、组织病理学反应和血清抗体反应中发现了显著差异。与人类菌株感染相比,鸟类菌株感染更强烈(高6.7倍)且持续时间更长(长14天)。鸟类菌株致病性更强,对肠道黏膜造成更大的病理生理改变,包括绒毛萎缩增加、杯状细胞增生和空泡化上皮细胞。感染鸟类菌株的小鼠产生的血清抗贾第虫IgA和IgM较少,但总(非特异性)血清IgA比感染人类贾第虫菌株的小鼠更多。这表明鸟类十二指肠贾第虫菌株对哺乳动物宿主具有感染性,可能导致人畜共患感染。此外,用BRIS/95/HEPU/2041感染小鼠可作为一个良好的实验模型,以进一步深入了解十二指肠贾第虫致病的机制。

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