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犬的肠道微生物群与胃扩张-扭转的高风险和免疫系统的高风险遗传变异有关。

The canine gut microbiome is associated with higher risk of gastric dilatation-volvulus and high risk genetic variants of the immune system.

机构信息

Public Health Sciences Division, Fred Hutchinson Cancer Research Center, Seattle, Washington, United States of America.

Department of Transplantation Biology, Clinical Research Division, Fred Hutchinson Cancer Research Center, Seattle, Washington, United States of America.

出版信息

PLoS One. 2018 Jun 11;13(6):e0197686. doi: 10.1371/journal.pone.0197686. eCollection 2018.

Abstract

BACKGROUND

Large and giant dog breeds have a high risk for gastric dilatation-volvulus (GDV) which is an acute, life-threatening condition. Previous work by our group identified a strong risk of GDV linked to specific alleles in innate and adaptive immune genes. We hypothesize that variation in the genes of the immune system act through modulation of the gut microbiome, or through autoimmune mechanisms, or both, to predispose dogs to this condition. Here, we investigate whether differences in the canine fecal microbiome are associated with GDV and are linked to previously identified risk alleles.

METHODOLOGY/PRINCIPLE FINDINGS: Fecal samples from healthy Great Danes (n = 38), and dogs with at least one occurrence of GDV (n = 37) were collected and analyzed by paired-end sequencing of the 16S rRNA gene. Dietary intake and temperament were estimated from a study-specific dietary and temperament questionnaire. Dogs with GDV had significantly more diverse fecal microbiomes than healthy control dogs. Alpha diversity was significantly increased in dogs with GDV, as well as dogs with at least one risk allele for DRB1 and TRL5. We found no significant association of dietary intake and GDV. Dogs with GDV showed a significant expansion of the rare lineage Actinobacteria (p = 0.004), as well as a significantly greater abundance of Firmicutes (p = 0.004) and a significantly lower abundance of Bacteroidetes (p<0.004). There was a significant difference in the abundance of 10 genera but after correction for multiple comparisons, none were significant. Bacterial phyla were significantly different between controls and dogs with GDV and at least one risk allele for DRB1 and TRL5. Actinobacteria were significantly higher in dogs with GDV and with one risk allele for DRB1 and TLR5 but not DLA88 genes. Furthermore, Collinsella was significantly increased in dogs with at least one risk allele for DRB1 and TLR5. Logistic regression showed that a model which included Actinobacteria, at least one risk allele,and temperament, explained 29% of the variation in risk of GDV in Great Danes.

CONCLUSIONS

The microbiome in GDV was altered by an expansion of a minor lineage and was associated with specific alleles of both innate and adaptive immunity genes. These associations are consistent with our hypothesis that immune genes may play a role in predisposition to GDV by altering the gut microbiome. Further research will be required to directly test the causal relationships of immune genes, the gut microbiome and GDV.

摘要

背景

大型犬和巨型犬患胃扩张-扭转(GDV)的风险较高,GDV 是一种急性、危及生命的疾病。我们小组之前的工作发现,特定的先天和适应性免疫基因中的特定等位基因与 GDV 有很强的关联。我们假设免疫系统基因的变异通过调节肠道微生物组,或通过自身免疫机制,或两者兼而有之,使狗易患这种疾病。在这里,我们研究了犬粪便微生物组的差异是否与 GDV 相关,并与之前确定的风险等位基因相关。

方法/主要发现:收集了 38 只健康大丹犬和 37 只至少发生过一次 GDV 的犬的粪便样本,并通过 16S rRNA 基因的配对末端测序进行分析。通过专门的饮食和气质问卷来估计饮食摄入和气质。GDV 犬的粪便微生物组多样性明显高于健康对照组。GDV 犬和至少有一个 DRB1 和 TRL5 风险等位基因的犬的 alpha 多样性显著增加。我们没有发现饮食摄入与 GDV 的显著关联。GDV 犬的放线菌(Actinobacteria)稀有谱系显著扩张(p = 0.004),厚壁菌门(Firmicutes)丰度显著增加(p = 0.004),拟杆菌门(Bacteroidetes)丰度显著降低(p<0.004)。有 10 个属的丰度有显著差异,但在进行多次比较校正后,没有一个属有显著差异。对照组和 GDV 犬以及至少有一个 DRB1 和 TRL5 风险等位基因的犬之间的细菌门有显著差异。在 GDV 犬和至少有一个 DRB1 和 TLR5 风险等位基因的犬中,放线菌显著升高。柯林斯菌(Collinsella)在至少有一个 DRB1 和 TLR5 风险等位基因的犬中显著增加。逻辑回归显示,一个包含放线菌、至少一个风险等位基因和气质的模型,解释了大丹犬 GDV 风险的 29%的变异。

结论

GDV 的微生物组被一个小谱系的扩张所改变,并与先天和适应性免疫基因的特定等位基因相关。这些关联与我们的假设一致,即免疫基因可能通过改变肠道微生物组,在易患 GDV 方面发挥作用。需要进一步研究来直接测试免疫基因、肠道微生物组和 GDV 的因果关系。

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