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胎儿生长受限对海马神经发育和功能的轨迹产生不利影响。

Fetal growth restriction adversely impacts trajectory of hippocampal neurodevelopment and function.

作者信息

Dudink Ingrid, Sutherland Amy E, Castillo-Melendez Margie, Ahmadzadeh Elham, White Tegan A, Malhotra Atul, Coleman Harold A, Parkington Helena C, Dean Justin M, Pham Yen, Yawno Tamara, Sepehrizadeh Tara, Jenkin Graham, Camm Emily J, Allison Beth J, Miller Suzanne L

机构信息

The Ritchie Centre, Hudson Institute of Medical Research, Translational Research Facility, Clayton, VIC, Australia.

Department of Obstetrics and Gynaecology, Monash University, Clayton, VIC, Australia.

出版信息

Brain Pathol. 2025 Jul;35(4):e13330. doi: 10.1111/bpa.13330. Epub 2025 Jan 8.

Abstract

The last pregnancy trimester is critical for fetal brain development but is a vulnerable period if the pregnancy is compromised by fetal growth restriction (FGR). The impact of FGR on the maturational development of neuronal morphology is not known, however, studies in fetal sheep allow longitudinal analysis in a long gestation species. Here we compared hippocampal neuron dendritogenesis in FGR and control fetal sheep at three timepoints equivalent to the third trimester of pregnancy, complemented by magnetic resonance image for brain volume, and electrophysiology for synaptic function. We hypothesized that the trajectory of hippocampal neuronal dendrite outgrowth would be decreased in the growth-restricted fetus, with implications for hippocampal volume, connectivity, and function. In control animals, total dendrite length increased with advancing gestation, but not in FGR, resulting in a significantly reduced trajectory of dendrite outgrowth in FGR fetuses for total length, branching, and complexity. Ex vivo electrophysiology analysis shows that paired-pulse facilitation was reduced in FGR compared to controls for cornu ammonis 1 hippocampal outputs, reflecting synaptic dysfunction. Hippocampal brain-derived neurotrophic factor density decreased over late gestation in FGR fetuses but not in controls. This study reveals that FGR is associated with a significant deviation in the trajectory of dendrite outgrowth of hippocampal neurons. Where dendrite length significantly increased over the third trimester of pregnancy in control brains, there was no corresponding increase over time in FGR brains, and the trajectory of dendrite outgrowth in FGR offspring was significantly reduced compared to controls. Reduced hippocampal dendritogenesis in FGR offspring has severe implications for the development of hippocampal connectivity and long-term function.

摘要

妊娠晚期对胎儿大脑发育至关重要,但如果妊娠因胎儿生长受限(FGR)而受到影响,这一时期则很脆弱。然而,FGR对神经元形态成熟发育的影响尚不清楚,不过,对胎羊的研究能够在一个妊娠期较长的物种中进行纵向分析。在此,我们比较了FGR胎羊和对照胎羊在相当于妊娠晚期的三个时间点的海马神经元树突发生情况,并辅以脑容量磁共振成像和突触功能电生理学检测。我们假设,生长受限胎儿海马神经元树突生长轨迹会减少,这会对海马体积、连通性和功能产生影响。在对照动物中,总树突长度随妊娠进展而增加,但在FGR胎羊中并非如此,导致FGR胎羊总长度树突生长轨迹、分支和复杂性显著降低。离体电生理学分析表明,与对照组相比,FGR胎羊海马1区输出的配对脉冲易化作用降低,反映出突触功能障碍。FGR胎羊海马脑源性神经营养因子密度在妊娠晚期降低,而对照胎羊则未降低。本研究表明,FGR与海马神经元树突生长轨迹的显著偏差有关。在对照大脑中,树突长度在妊娠晚期显著增加,而在FGR大脑中则没有随时间相应增加,并且与对照组相比,FGR后代的树突生长轨迹显著降低。FGR后代海马树突发生减少对海马连通性和长期功能的发育具有严重影响。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/aee3/12145903/51b9d8b40cd4/BPA-35-e13330-g003.jpg

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