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宿主和病原体基因组的配对分析确定了人类结核病的决定因素。

Paired analysis of host and pathogen genomes identifies determinants of human tuberculosis.

机构信息

Center for Data Sciences, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, USA.

Division of Rheumatology, Inflammation and Immunity, Brigham and Women's Hospital, Harvard Medical School, Boston, MA, USA.

出版信息

Nat Commun. 2024 Nov 29;15(1):10393. doi: 10.1038/s41467-024-54741-w.

Abstract

Infectious disease is the result of interactions between host and pathogen and can depend on genetic variations in both. We conduct a genome-to-genome study of paired human and Mycobacterium tuberculosis genomes from a cohort of 1556 tuberculosis patients in Lima, Peru. We identify an association between a human intronic variant (rs3130660, OR = 10.06, 95%CI: 4.87 - 20.77, P = 7.92 × 10) in the FLOT1 gene and a subclavaluee of Mtb Lineage 2. In a human macrophage infection model, we observe hosts with the rs3130660-A allele exhibited stronger interferon gene signatures. The interacting strains have altered redox states due to a thioredoxin reductase mutation. We investigate this association in a 2020 cohort of 699 patients recruited during the COVID-19 pandemic. While the prevalence of the interacting strain almost doubled between 2010 and 2020, its infection is not associated with rs3130660 in this recent cohort. These findings suggest a complex interplay among host, pathogen, and environmental factors in tuberculosis dynamics.

摘要

传染病是宿主和病原体相互作用的结果,并且可能取决于两者的遗传变异。我们对来自秘鲁利马的 1556 名结核病患者队列中的人类和结核分枝杆菌基因组进行了基因组对基因组研究。我们在 FLOT1 基因中的一个人类内含子变体(rs3130660,OR=10.06,95%CI:4.87-20.77,P=7.92×10)中发现了与结核分枝杆菌 2 谱系的一个亚谱系值之间的关联。在人类巨噬细胞感染模型中,我们观察到携带 rs3130660-A 等位基因的宿主表现出更强的干扰素基因特征。由于硫氧还蛋白还原酶突变,相互作用的菌株具有改变的氧化还原状态。我们在 2020 年 COVID-19 大流行期间招募的 699 名患者的 2020 年队列中研究了这种关联。虽然在 2010 年至 2020 年期间,相互作用的菌株的流行率几乎翻了一番,但在最近的队列中,其感染与 rs3130660 无关。这些发现表明在结核病动态中宿主、病原体和环境因素之间存在复杂的相互作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bfdb/11607449/78b60eb4b13c/41467_2024_54741_Fig1_HTML.jpg

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