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在年轻的Cyp2c70小鼠中,血浆胆汁酸升高与心脏应激和炎症同时出现。

Elevated plasma bile acids coincide with cardiac stress and inflammation in young Cyp2c70 mice.

作者信息

de Vries Hilde D, Eijgenraam Tim R, Bloks Vincent W, Mulder Niels L, van Zutphen Tim, Silljé Herman H W, Kuipers Folkert, de Boer Jan Freark

机构信息

Department of Laboratory Medicine, University of Groningen, University Medical Center Groningen, Groningen, The Netherlands.

Faculty Campus Fryslân, University of Groningen, Leeuwarden, The Netherlands.

出版信息

Pediatr Res. 2024 Oct 2. doi: 10.1038/s41390-024-03596-4.

Abstract

BACKGROUND

High plasma bile acids (BAs), for instance due to intrahepatic cholestasis of pregnancy or neonatal cholestasis, are associated with cardiac abnormalities. Here, we exploited the variability in plasma BA levels in Cyp2c70 mice with a human-like BA composition to investigate the acute effects of elevated circulating BAs on the heart.

METHODS

RNA sequencing was performed on hearts of 3-week-old Cyp2c70 mice lacking mouse-specific BA species that show features of neonatal cholestasis. Cardiac transcriptomes were compared between wild-type pups, Cyp2c70 pups with low or high plasma BAs, and Cyp2c70 pups from dams that were perinatally treated with ursodeoxycholic acid (UDCA).

RESULTS

We identified 1355 genes that were differentially expressed in hearts of Cyp2c70 mice with high versus low plasma BAs with enrichment of inflammatory processes. Strikingly, expression of 1053 (78%) of those genes was normalized in hearts of pups of UDCA-treated dams. Moreover, 645 cardiac genes strongly correlated to plasma BAs, of which 172 genes were associated with cardiovascular disease.

CONCLUSIONS

Elevated plasma BAs alter gene expression profiles of hearts of mice with a human-like BA profile, revealing cardiac stress and inflammation. Our findings support the notion that high plasma BAs induce cardiac complications in early life.

IMPACT

Cyp2c70 mice with a human-like bile acid composition show features of neonatal cholestasis but the extrahepatic consequences hereof have so far hardly been addressed Elevated plasma bile acids in Cyp2c70 pups coincide with cardiac stress and inflammation Perinatal treatment with UDCA prevents dysregulated cardiac gene expression patterns in Cyp2c70 pups.

摘要

背景

高血浆胆汁酸(BAs),例如由于妊娠肝内胆汁淤积或新生儿胆汁淤积,与心脏异常有关。在此,我们利用具有类人胆汁酸组成的Cyp2c70小鼠血浆BA水平的变异性,来研究循环胆汁酸升高对心脏的急性影响。

方法

对缺乏显示新生儿胆汁淤积特征的小鼠特异性胆汁酸种类的3周龄Cyp2c70小鼠的心脏进行RNA测序。比较野生型幼崽、血浆BA水平低或高的Cyp2c70幼崽以及在围产期接受熊去氧胆酸(UDCA)治疗的母鼠所生的Cyp2c70幼崽的心脏转录组。

结果

我们鉴定出1355个在血浆BA水平高与低的Cyp2c70小鼠心脏中差异表达的基因,这些基因富集于炎症过程。引人注目的是,其中1053个(78%)基因的表达在接受UDCA治疗的母鼠所生幼崽的心脏中恢复正常。此外,645个心脏基因与血浆BA密切相关,其中172个基因与心血管疾病有关。

结论

血浆BA升高会改变具有类人胆汁酸谱的小鼠心脏的基因表达谱,揭示心脏应激和炎症。我们的研究结果支持高血浆BA在生命早期诱发心脏并发症的观点。

影响

具有类人胆汁酸组成的Cyp2c70小鼠表现出新生儿胆汁淤积的特征,但迄今为止几乎未涉及由此产生的肝外后果。Cyp2c70幼崽血浆胆汁酸升高与心脏应激和炎症同时出现。围产期用UDCA治疗可防止Cyp2c70幼崽心脏基因表达模式失调。

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