Author
Listed:
- Sangmin You
(University of Rhode Island)
- Ai-Min Cui
(Nantong University)
- Syed F. Hashmi
(University of Rhode Island)
- Xinmu Zhang
(University of Rhode Island)
- Christina Nadolny
(University of Rhode Island)
- Yuan Chen
(University of Rhode Island)
- Qiwen Chen
(University of Rhode Island)
- Xin Bush
(University of Rhode Island)
- Zachary Hurd
(University of Rhode Island)
- Winifer Ali
(University of Rhode Island)
- Gang Qin
(Nantong University)
- Ruitang Deng
(University of Rhode Island)
Abstract
Preterm birth (PTB) is the leading cause of perinatal mortality and newborn complications. Bile acids are recognized as signaling molecules regulating a myriad of cellular and metabolic activities but have not been etiologically linked to PTB. In this study, a hospital-based cohort study with 36,755 pregnant women is conducted. We find that serum total bile acid levels directly correlate with the PTB rates regardless of the characteristics of the subjects and etiologies of liver disorders. Consistent with the findings from pregnant women, PTB is successfully reproduced in mice with liver injuries and dysregulated bile acids. More importantly, bile acids dose-dependently induce PTB with minimal hepatotoxicity. Furthermore, restoring bile acid homeostasis by farnesoid X receptor activation markedly reduces PTB and dramatically improves newborn survival rates. The findings thus establish an etiologic link between bile acids and PTB, and open an avenue for developing etiology-based therapies to prevent or delay PTB.
Suggested Citation
Sangmin You & Ai-Min Cui & Syed F. Hashmi & Xinmu Zhang & Christina Nadolny & Yuan Chen & Qiwen Chen & Xin Bush & Zachary Hurd & Winifer Ali & Gang Qin & Ruitang Deng, 2020.
"Dysregulation of bile acids increases the risk for preterm birth in pregnant women,"
Nature Communications, Nature, vol. 11(1), pages 1-15, December.
Handle:
RePEc:nat:natcom:v:11:y:2020:i:1:d:10.1038_s41467-020-15923-4
DOI: 10.1038/s41467-020-15923-4
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