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利用类器官模拟人类大脑中的性别差异。

Using Organoids to Model Sex Differences in the Human Brain.

作者信息

Pavlinek Adam, Adhya Dwaipayan, Tsompanidis Alex, Warrier Varun, Vernon Anthony C, Lancaster Madeline, Mill Jonathan, Srivastava Deepak P, Baron-Cohen Simon

机构信息

Department of Basic and Clinical Neuroscience, Institute of Psychiatry, Psychology and Neuroscience, King's College London, London, United Kingdom.

MRC Centre for Neurodevelopmental Disorders, King's College London, London, United Kingdom.

出版信息

Biol Psychiatry Glob Open Sci. 2024 Jun 4;4(5):100343. doi: 10.1016/j.bpsgos.2024.100343. eCollection 2024 Sep.

Abstract

Sex differences are widespread during neurodevelopment and play a role in neuropsychiatric conditions such as autism, which is more prevalent in males than females. In humans, males have been shown to have larger brain volumes than females with development of the hippocampus and amygdala showing prominent sex differences. Mechanistically, sex steroids and sex chromosomes drive these differences in brain development, which seem to peak during prenatal and pubertal stages. Animal models have played a crucial role in understanding sex differences, but the study of human sex differences requires an experimental model that can recapitulate complex genetic traits. To fill this gap, human induced pluripotent stem cell-derived brain organoids are now being used to study how complex genetic traits influence prenatal brain development. For example, brain organoids from individuals with autism and individuals with X chromosome-linked Rett syndrome and fragile X syndrome have revealed prenatal differences in cell proliferation, a measure of brain volume differences, and excitatory-inhibitory imbalances. Brain organoids have also revealed increased neurogenesis of excitatory neurons due to androgens. However, despite growing interest in using brain organoids, several key challenges remain that affect its validity as a model system. In this review, we discuss how sex steroids and the sex chromosomes each contribute to sex differences in brain development. Then, we examine the role of X chromosome inactivation as a factor that drives sex differences. Finally, we discuss the combined challenges of modeling X chromosome inactivation and limitations of brain organoids that need to be taken into consideration when studying sex differences.

摘要

性别差异在神经发育过程中广泛存在,并在自闭症等神经精神疾病中发挥作用,自闭症在男性中比女性更普遍。在人类中,已显示男性的脑容量比女性大,海马体和杏仁核的发育存在显著的性别差异。从机制上讲,性类固醇和性染色体驱动大脑发育中的这些差异,这些差异似乎在产前和青春期阶段达到峰值。动物模型在理解性别差异方面发挥了关键作用,但对人类性别差异的研究需要一个能够重现复杂遗传特征的实验模型。为了填补这一空白,人类诱导多能干细胞衍生的脑类器官现在正被用于研究复杂遗传特征如何影响产前大脑发育。例如,来自自闭症患者以及患有X染色体连锁的瑞特综合征和脆性X综合征患者的脑类器官揭示了细胞增殖方面的产前差异,细胞增殖是脑容量差异的一个指标,以及兴奋性-抑制性失衡。脑类器官还揭示了雄激素导致兴奋性神经元的神经发生增加。然而,尽管对使用脑类器官的兴趣日益浓厚,但仍存在几个关键挑战,这些挑战影响其作为模型系统的有效性。在这篇综述中,我们讨论了性类固醇和性染色体如何各自促成大脑发育中的性别差异。然后,我们研究了X染色体失活作为驱动性别差异的一个因素的作用。最后,我们讨论了模拟X染色体失活的综合挑战以及在研究性别差异时需要考虑的脑类器官的局限性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0e01/11292257/3dcd0aa3d3d6/gr1.jpg

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