Zhejiang Key Laboratory of Organ Development and Regeneration, College of Life and Environmental Sciences, Hangzhou Normal University, Hangzhou 311121, China.
The Children's Hospital, National Clinical Research Center for Child Health, Zhejiang University School of Medicine, Hangzhou 310052, China.
J Zhejiang Univ Sci B. 2024 Oct 2;25(10):878-889. doi: 10.1631/jzus.B2300712.
Cockayne syndrome (CS) group B (CSB), which results from mutations in the excision repair cross-complementation group 6 () genes, which produce CSB protein, is an autosomal recessive disease characterized by multiple progressive disorders including growth failure, microcephaly, skin photosensitivity, and premature aging. Clinical data show that brain atrophy, demyelination, and calcification are the main neurological manifestations of CS, which progress with time. Neuronal loss and calcification occur in various brain areas, particularly the cerebellum and basal ganglia, resulting in dyskinesia, ataxia, and limb tremors in CSB patients. However, the understanding of neurodevelopmental defects in CS has been constrained by the lack of significant neurodevelopmental and functional abnormalities observed in CSB-deficient mice. In this review, we focus on elucidating the protein structure and distribution of CSB and delve into the impact of CSB mutations on the development and function of the nervous system. In addition, we provide an overview of research models that have been instrumental in exploring CS disorders, with a forward-looking perspective on the substantial contributions that brain organoids are poised to further advance this field.
科凯恩综合征(CS)B 组(CSB)是由切除修复交叉互补基因组 6(ERCC6)基因突变引起的,该基因产生 CSB 蛋白,是一种常染色体隐性疾病,其特征是多种进行性疾病,包括生长发育迟缓、小头畸形、皮肤光敏感性和早衰。临床数据表明,脑萎缩、脱髓鞘和钙化是 CS 的主要神经表现,随着时间的推移而进展。神经元丢失和钙化发生在各个脑区,特别是小脑和基底节,导致 CSB 患者出现运动障碍、共济失调和肢体震颤。然而,由于在 CSB 缺陷型小鼠中观察到的神经发育和功能异常并不显著,因此对 CS 中的神经发育缺陷的理解一直受到限制。在这篇综述中,我们重点阐明 CSB 的蛋白结构和分布,并深入探讨 CSB 突变对神经系统发育和功能的影响。此外,我们还概述了在探索 CS 疾病方面发挥重要作用的研究模型,并前瞻性地展望了脑类器官将如何进一步推动这一领域的发展。
