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繁殖期间母体肠道的生长。

Growth of the maternal intestine during reproduction.

作者信息

Ameku Tomotsune, Laddach Anna, Beckwith Hannah, Milona Alexandra, Rogers Loranzie S, Schwayer Cornelia, Nye Emma, Tough Iain R, Thoumas Jean-Louis, Gautam Umesh Kumar, Wang Yi-Fang, Jha Shreya, Castano-Medina Alvaro, Amourda Christopher, Vaelli Patric M, Gevers Sira, Irvine Elaine E, Meyer Leah, Andrew Ivan, Choi Ka Lok, Patel Bhavik, Francis Alice J, Studd Chris, Game Laurence, Young George, Murphy Kevin G, Owen Bryn, Withers Dominic J, Rodriguez-Colman Maria, Cox Helen M, Liberali Prisca, Schwarzer Martin, Leulier François, Pachnis Vassilis, Bellono Nicholas W, Miguel-Aliaga Irene

机构信息

The Francis Crick Institute, 1 Midland Road, London NW1 1AT, UK; MRC Laboratory of Medical Sciences, Hammersmith Hospital Campus, Du Cane Road, London W12 0NN, UK; Institute of Clinical Sciences, Faculty of Medicine, Imperial College London, Du Cane Road, London W12 0NN, UK.

The Francis Crick Institute, 1 Midland Road, London NW1 1AT, UK.

出版信息

Cell. 2025 May 15;188(10):2738-2756.e22. doi: 10.1016/j.cell.2025.02.015. Epub 2025 Mar 19.

Abstract

The organs of many female animals are remodeled by reproduction. Using the mouse intestine, a striking and tractable model of organ resizing, we find that reproductive remodeling is anticipatory and distinct from diet- or microbiota-induced resizing. Reproductive remodeling involves partially irreversible elongation of the small intestine and fully reversible growth of its epithelial villi, associated with an expansion of isthmus progenitors and accelerated enterocyte migration. We identify induction of the SGLT3a transporter in a subset of enterocytes as an early reproductive hallmark. Electrophysiological and genetic interrogations indicate that SGLT3a does not sustain digestive functions or enterocyte health; rather, it detects protons and sodium to extrinsically support the expansion of adjacent Fgfbp1-positive isthmus progenitors, promoting villus growth. Our findings reveal unanticipated specificity to physiological organ remodeling. We suggest that organ- and state-specific growth programs could be leveraged to improve pregnancy outcomes or prevent maladaptive consequences of such growth.

摘要

许多雌性动物的器官会因繁殖而重塑。利用小鼠肠道这一显著且易于处理的器官大小调整模型,我们发现生殖重塑具有前瞻性,且与饮食或微生物群诱导的大小调整不同。生殖重塑涉及小肠部分不可逆的伸长及其上皮绒毛的完全可逆生长,这与峡部祖细胞的扩增和肠上皮细胞迁移加速有关。我们确定在一部分肠上皮细胞中诱导SGLT3a转运蛋白是早期生殖标志。电生理和基因研究表明,SGLT3a并不维持消化功能或肠上皮细胞健康;相反,它检测质子和钠以从外部支持相邻Fgfbp1阳性峡部祖细胞的扩增,促进绒毛生长。我们的研究结果揭示了生理器官重塑中意想不到的特异性。我们建议,可以利用器官和状态特异性生长程序来改善妊娠结局或预防这种生长的不良后果。

相似文献

1
Growth of the maternal intestine during reproduction.繁殖期间母体肠道的生长。
Cell. 2025 May 15;188(10):2738-2756.e22. doi: 10.1016/j.cell.2025.02.015. Epub 2025 Mar 19.

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