Deciphering the coordinated roles of the host genome, duodenal mucosal genes, and microbiota in regulating complex traits in chickens.

IF 13.8 1区 生物学 Q1 MICROBIOLOGY
Fangren Lan, Xiqiong Wang, Qianqian Zhou, Xiaochang Li, Jiaming Jin, Wenxin Zhang, Chaoliang Wen, Guiqin Wu, Guangqi Li, Yiyuan Yan, Ning Yang, Congjiao Sun
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引用次数: 0

Abstract

Background: The complex interactions between host genetics and the gut microbiome are well documented. However, the specific impacts of gene expression patterns and microbial composition on each other remain to be further explored.

Results: Here, we investigated this complex interplay in a sizable population of 705 hens, employing integrative analyses to examine the relationships among the host genome, mucosal gene expression, and gut microbiota. Specific microbial taxa, such as the cecal family Christensenellaceae, which showed a heritability of 0.365, were strongly correlated with host genomic variants. We proposed a novel concept of regulatability ( r b 2 ), which was derived from h2, to quantify the cumulative effects of gene expression on the given phenotypes. The duodenal mucosal transcriptome emerged as a potent influencer of duodenal microbial taxa, with much higher r b 2 values (0.17 ± 0.01, mean ± SE) than h2 values (0.02 ± 0.00). A comparative analysis of chickens and humans revealed similar average microbiability values of genes (0.18 vs. 0.20) and significant differences in average r b 2 values of microbes (0.17 vs. 0.04). Besides, cis ( h cis 2 ) and trans heritability ( h trans 2 ) were estimated to assess the effects of genetic variations inside and outside the cis window of the gene on its expression. Higher h trans 2 values than h cis 2 values and a greater prevalence of trans-regulated genes than cis-regulated genes underscored the significant role of loci outside the cis window in shaping gene expression levels. Furthermore, our exploration of the regulatory effects of duodenal mucosal genes and the microbiota on 18 complex traits enhanced our understanding of the regulatory mechanisms, in which the CHST14 gene and its regulatory relationships with Lactobacillus salivarius jointly facilitated the deposition of abdominal fat by modulating the concentration of bile salt hydrolase, and further triglycerides, total cholesterol, and free fatty acids absorption and metabolism.

Conclusions: Our findings highlighted a novel concept of r b 2 to quantify the phenotypic variance attributed to gene expression and emphasize the superior role of intestinal mucosal gene expressions over host genomic variations in elucidating host‒microbe interactions for complex traits. This understanding could assist in devising strategies to modulate host-microbe interactions, ultimately improving economic traits in chickens.

破译宿主基因组、十二指肠粘膜基因和微生物群在调节鸡复杂性状中的协调作用。
背景:宿主遗传和肠道微生物群之间复杂的相互作用已被充分记录。然而,基因表达模式和微生物组成对彼此的具体影响仍有待进一步探索。结果:在这里,我们在705只鸡中研究了这种复杂的相互作用,采用综合分析来检查宿主基因组、粘膜基因表达和肠道微生物群之间的关系。特定的微生物类群,如盲肠科Christensenellaceae,其遗传力为0.365,与宿主基因组变异密切相关。我们提出了一个新的可调节性概念(r b2),它来源于h2,以量化基因表达对给定表型的累积效应。十二指肠黏膜转录组是影响十二指肠微生物分类群的重要因素,rb2值(0.17±0.01,平均±SE)远高于h2值(0.02±0.00)。对比分析显示,鸡和人基因的平均微生物率值相似(0.18 vs. 0.20),微生物的平均r b 2值差异显著(0.17 vs. 0.04)。此外,估计顺式(h cis 2)和反式遗传力(h trans 2)来评估基因顺式窗口内外的遗传变异对其表达的影响。htrans - 2值比hcis - 2值高,反式调控基因比顺式调控基因更普遍,这强调了顺式窗口外的位点在塑造基因表达水平方面的重要作用。此外,我们对十二指肠粘膜基因和微生物群对18个复杂性状的调控作用的探索,增强了我们对其调控机制的理解,其中CHST14基因及其与唾液乳杆菌的调控关系,通过调节胆汁盐水解酶的浓度,促进腹部脂肪的沉积,进而调节甘油三酯、总胆固醇和游离脂肪酸的吸收和代谢。结论:我们的研究结果强调了rb2的新概念,可以量化归因于基因表达的表型差异,并强调了肠黏膜基因表达在阐明复杂性状的宿主-微生物相互作用方面比宿主基因组变异的优越作用。这一认识有助于设计调节宿主-微生物相互作用的策略,最终改善鸡的经济性状。
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来源期刊
Microbiome
Microbiome MICROBIOLOGY-
CiteScore
21.90
自引率
2.60%
发文量
198
审稿时长
4 weeks
期刊介绍: Microbiome is a journal that focuses on studies of microbiomes in humans, animals, plants, and the environment. It covers both natural and manipulated microbiomes, such as those in agriculture. The journal is interested in research that uses meta-omics approaches or novel bioinformatics tools and emphasizes the community/host interaction and structure-function relationship within the microbiome. Studies that go beyond descriptive omics surveys and include experimental or theoretical approaches will be considered for publication. The journal also encourages research that establishes cause and effect relationships and supports proposed microbiome functions. However, studies of individual microbial isolates/species without exploring their impact on the host or the complex microbiome structures and functions will not be considered for publication. Microbiome is indexed in BIOSIS, Current Contents, DOAJ, Embase, MEDLINE, PubMed, PubMed Central, and Science Citations Index Expanded.
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