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从人类病原体微小巴贝斯虫中测序最小的顶复门基因组。

Sequencing of the smallest Apicomplexan genome from the human pathogen Babesia microti.

机构信息

Laboratoire de Biologie Cellulaire et Moléculaire (LBCM-EA4558), UFR Pharmacie, Université Montpellier 1, 15, av. Charles Flahault, 34093 Montpellier cedex 5, France.

出版信息

Nucleic Acids Res. 2012 Oct;40(18):9102-14. doi: 10.1093/nar/gks700. Epub 2012 Jul 24.

Abstract

We have sequenced the genome of the emerging human pathogen Babesia microti and compared it with that of other protozoa. B. microti has the smallest nuclear genome among all Apicomplexan parasites sequenced to date with three chromosomes encoding ∼3500 polypeptides, several of which are species specific. Genome-wide phylogenetic analyses indicate that B. microti is significantly distant from all species of Babesidae and Theileridae and defines a new clade in the phylum Apicomplexa. Furthermore, unlike all other Apicomplexa, its mitochondrial genome is circular. Genome-scale reconstruction of functional networks revealed that B. microti has the minimal metabolic requirement for intraerythrocytic protozoan parasitism. B. microti multigene families differ from those of other protozoa in both the copy number and organization. Two lateral transfer events with significant metabolic implications occurred during the evolution of this parasite. The genomic sequencing of B. microti identified several targets suitable for the development of diagnostic assays and novel therapies for human babesiosis.

摘要

我们已经对新兴的人类病原体微小巴贝斯虫的基因组进行了测序,并将其与其他原生动物进行了比较。微小巴贝斯虫具有迄今为止所有已测序的顶复门寄生虫中最小的核基因组,其中三个染色体编码约 3500 种多肽,其中几种是种特异性的。全基因组系统发育分析表明,微小巴贝斯虫与巴贝斯科和泰勒科的所有种都有很大的距离,并在顶复门中定义了一个新的进化枝。此外,与所有其他顶复门不同,其线粒体基因组是环状的。功能网络的基因组规模重建表明,微小巴贝斯虫具有最低限度的红细胞内原生动物寄生代谢需求。微小巴贝斯虫的多基因家族在数量和组织上都与其他原生动物不同。在寄生虫的进化过程中发生了两次具有重要代谢意义的侧向转移事件。微小巴贝斯虫的基因组测序确定了几个适合开发人类巴贝斯虫病诊断检测和新疗法的靶标。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/94b1/3467087/719c3d99d7a4/gks700f1.jpg

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