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顶复门寄生虫微小隐孢子虫的生活史进展和性发育。

Life cycle progression and sexual development of the apicomplexan parasite Cryptosporidium parvum.

机构信息

Department of Pathobiology, School of Veterinary Medicine, University of Pennsylvania, Philadelphia, PA, USA.

Franklin College of Arts and Science, University of Georgia, Athens, GA, USA.

出版信息

Nat Microbiol. 2019 Dec;4(12):2226-2236. doi: 10.1038/s41564-019-0539-x. Epub 2019 Sep 2.

DOI:10.1038/s41564-019-0539-x
PMID:31477896
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6877471/
Abstract

The apicomplexan parasite Cryptosporidium is a leading global cause of severe diarrhoeal disease and an important contributor to early childhood mortality. Currently, there are no fully effective treatments or vaccines available. Parasite transmission occurs through ingestion of oocysts, through either direct contact or consumption of contaminated water or food. Oocysts are meiotic spores and the product of parasite sex. Cryptosporidium has a single-host life cycle in which both asexual and sexual processes occur in the intestine of infected hosts. Here, we genetically engineered strains of Cryptosporidium to make life cycle progression and parasite sex tractable. We derive reporter strains to follow parasite development in culture and in infected mice and define the genes that orchestrate sex and oocyst formation through mRNA sequencing of sorted cells. After 2 d, parasites in cell culture show pronounced sexualization, but productive fertilization does not occur and infection falters. By contrast, in infected mice, male gametes successfully fertilize female parasites, which leads to meiotic division and sporulation. To rigorously test for fertilization, we devised a two-component genetic-crossing assay using a reporter that is activated by Cre recombinase. Our findings suggest obligate developmental progression towards sex in Cryptosporidium, which has important implications for the treatment and prevention of the infection.

摘要

顶复门寄生虫隐孢子虫是全球严重腹泻病的主要病因之一,也是导致儿童早期死亡的重要因素。目前,尚无完全有效的治疗方法或疫苗。寄生虫通过摄入卵囊传播,通过直接接触或食用受污染的水或食物传播。卵囊是减数分裂孢子,是寄生虫有性生殖的产物。隐孢子虫的单宿主生活史中,感染宿主的肠道内同时发生无性和有性过程。在这里,我们通过基因工程改造隐孢子虫菌株,使其生活史能够进行并追踪其有性生殖过程。我们构建了报告菌株,以在培养物和感染的小鼠中追踪寄生虫的发育,并通过对分选细胞进行 mRNA 测序来定义协调有性生殖和卵囊形成的基因。在细胞培养中,寄生虫在 2 天后表现出明显的性化,但不会发生有性生殖,感染也会停滞。相比之下,在感染的小鼠中,雄性配子成功地使雌性寄生虫受精,这导致减数分裂和孢子形成。为了严格测试受精,我们设计了一种使用 Cre 重组酶激活的报告基因的两部分遗传杂交测定法。我们的发现表明隐孢子虫的发育必然会向有性生殖方向发展,这对感染的治疗和预防具有重要意义。

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