In-depth analysis reveals complex molecular aetiology in a cohort of idiopathic cerebral palsy

Cerebral palsy is the most prevalent physical disability in children; however, its inherent molecular mechanisms remain unclear. In the present study, we performed in-depth clinical and molecular analysis on 120 idiopathic cerebral palsy families, and identified underlying detrimental genetic varian...

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Autores principales: Li, Na, Zhou, Pei, Tang, Hongmei, He, Lu, Fang, Xiang, Zhao, Jinxiang, Wang, Xin, Qi, Yifei, Sun, Chuanbo, Lin, Yunting, Qin, Fengying, Yang, Miaomiao, Zhang, Zhan, Liao, Caihua, Zheng, Shuxin, Peng, Xiaofang, Xue, Ting, Zhu, Qianying, Li, Hong, Li, Yan, Liu, Liru, Huang, Jingyu, Liu, Li, Peng, Changgeng, Kaindl, Angela M, Gecz, Jozef, Han, Dingding, Liu, Dong, Xu, Kaishou, Hu, Hao
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Oxford University Press 2021
Materias:
Original Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8967106/
https://www.ncbi.nlm.nih.gov/pubmed/34077496
http://dx.doi.org/10.1093/brain/awab209
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author Li, Na
Zhou, Pei
Tang, Hongmei
He, Lu
Fang, Xiang
Zhao, Jinxiang
Wang, Xin
Qi, Yifei
Sun, Chuanbo
Lin, Yunting
Qin, Fengying
Yang, Miaomiao
Zhang, Zhan
Liao, Caihua
Zheng, Shuxin
Peng, Xiaofang
Xue, Ting
Zhu, Qianying
Li, Hong
Li, Yan
Liu, Liru
Huang, Jingyu
Liu, Li
Peng, Changgeng
Kaindl, Angela M
Gecz, Jozef
Han, Dingding
Liu, Dong
Xu, Kaishou
Hu, Hao
author_facet Li, Na
Zhou, Pei
Tang, Hongmei
He, Lu
Fang, Xiang
Zhao, Jinxiang
Wang, Xin
Qi, Yifei
Sun, Chuanbo
Lin, Yunting
Qin, Fengying
Yang, Miaomiao
Zhang, Zhan
Liao, Caihua
Zheng, Shuxin
Peng, Xiaofang
Xue, Ting
Zhu, Qianying
Li, Hong
Li, Yan
Liu, Liru
Huang, Jingyu
Liu, Li
Peng, Changgeng
Kaindl, Angela M
Gecz, Jozef
Han, Dingding
Liu, Dong
Xu, Kaishou
Hu, Hao
author_sort Li, Na
collection PubMed
description Cerebral palsy is the most prevalent physical disability in children; however, its inherent molecular mechanisms remain unclear. In the present study, we performed in-depth clinical and molecular analysis on 120 idiopathic cerebral palsy families, and identified underlying detrimental genetic variants in 45% of these patients. In addition to germline variants, we found disease-related postzygotic mutations in ∼6.7% of cerebral palsy patients. We found that patients with more severe motor impairments or a comorbidity of intellectual disability had a significantly higher chance of harbouring disease-related variants. By a compilation of 114 known cerebral-palsy-related genes, we identified characteristic features in terms of inheritance and function, from which we proposed a dichotomous classification system according to the expression patterns of these genes and associated cognitive impairments. In two patients with both cerebral palsy and intellectual disability, we revealed that the defective TYW1, a tRNA hypermodification enzyme, caused primary microcephaly and problems in motion and cognition by hindering neuronal proliferation and migration. Furthermore, we developed an algorithm and demonstrated in mouse brains that this malfunctioning hypermodification specifically perturbed the translation of a subset of proteins involved in cell cycling. This finding provided a novel and interesting mechanism for congenital microcephaly. In another cerebral palsy patient with normal intelligence, we identified a mitochondrial enzyme GPAM, the hypomorphic form of which led to hypomyelination of the corticospinal tract in both human and mouse models. In addition, we confirmed that the aberrant Gpam in mice perturbed the lipid metabolism in astrocytes, resulting in suppressed astrocytic proliferation and a shortage of lipid contents supplied for oligodendrocytic myelination. Taken together, our findings elucidate novel aspects of the aetiology of cerebral palsy and provide insights for future therapeutic strategies.
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spelling pubmed-89671062022-03-31 In-depth analysis reveals complex molecular aetiology in a cohort of idiopathic cerebral palsy Li, Na Zhou, Pei Tang, Hongmei He, Lu Fang, Xiang Zhao, Jinxiang Wang, Xin Qi, Yifei Sun, Chuanbo Lin, Yunting Qin, Fengying Yang, Miaomiao Zhang, Zhan Liao, Caihua Zheng, Shuxin Peng, Xiaofang Xue, Ting Zhu, Qianying Li, Hong Li, Yan Liu, Liru Huang, Jingyu Liu, Li Peng, Changgeng Kaindl, Angela M Gecz, Jozef Han, Dingding Liu, Dong Xu, Kaishou Hu, Hao Brain Original Article Cerebral palsy is the most prevalent physical disability in children; however, its inherent molecular mechanisms remain unclear. In the present study, we performed in-depth clinical and molecular analysis on 120 idiopathic cerebral palsy families, and identified underlying detrimental genetic variants in 45% of these patients. In addition to germline variants, we found disease-related postzygotic mutations in ∼6.7% of cerebral palsy patients. We found that patients with more severe motor impairments or a comorbidity of intellectual disability had a significantly higher chance of harbouring disease-related variants. By a compilation of 114 known cerebral-palsy-related genes, we identified characteristic features in terms of inheritance and function, from which we proposed a dichotomous classification system according to the expression patterns of these genes and associated cognitive impairments. In two patients with both cerebral palsy and intellectual disability, we revealed that the defective TYW1, a tRNA hypermodification enzyme, caused primary microcephaly and problems in motion and cognition by hindering neuronal proliferation and migration. Furthermore, we developed an algorithm and demonstrated in mouse brains that this malfunctioning hypermodification specifically perturbed the translation of a subset of proteins involved in cell cycling. This finding provided a novel and interesting mechanism for congenital microcephaly. In another cerebral palsy patient with normal intelligence, we identified a mitochondrial enzyme GPAM, the hypomorphic form of which led to hypomyelination of the corticospinal tract in both human and mouse models. In addition, we confirmed that the aberrant Gpam in mice perturbed the lipid metabolism in astrocytes, resulting in suppressed astrocytic proliferation and a shortage of lipid contents supplied for oligodendrocytic myelination. Taken together, our findings elucidate novel aspects of the aetiology of cerebral palsy and provide insights for future therapeutic strategies. Oxford University Press 2021-06-02 /pmc/articles/PMC8967106/ /pubmed/34077496 http://dx.doi.org/10.1093/brain/awab209 Text en © The Author(s) (2021). Published by Oxford University Press on behalf of the Guarantors of Brain. https://creativecommons.org/licenses/by-nc/4.0/This is an Open Access article distributed under the terms of the Creative Commons Attribution-NonCommercial License (https://creativecommons.org/licenses/by-nc/4.0/), which permits non-commercial re-use, distribution, and reproduction in any medium, provided the original work is properly cited. For commercial re-use, please contact journals.permissions@oup.com
spellingShingle Original Article
Li, Na
Zhou, Pei
Tang, Hongmei
He, Lu
Fang, Xiang
Zhao, Jinxiang
Wang, Xin
Qi, Yifei
Sun, Chuanbo
Lin, Yunting
Qin, Fengying
Yang, Miaomiao
Zhang, Zhan
Liao, Caihua
Zheng, Shuxin
Peng, Xiaofang
Xue, Ting
Zhu, Qianying
Li, Hong
Li, Yan
Liu, Liru
Huang, Jingyu
Liu, Li
Peng, Changgeng
Kaindl, Angela M
Gecz, Jozef
Han, Dingding
Liu, Dong
Xu, Kaishou
Hu, Hao
In-depth analysis reveals complex molecular aetiology in a cohort of idiopathic cerebral palsy
title In-depth analysis reveals complex molecular aetiology in a cohort of idiopathic cerebral palsy
title_full In-depth analysis reveals complex molecular aetiology in a cohort of idiopathic cerebral palsy
title_fullStr In-depth analysis reveals complex molecular aetiology in a cohort of idiopathic cerebral palsy
title_full_unstemmed In-depth analysis reveals complex molecular aetiology in a cohort of idiopathic cerebral palsy
title_short In-depth analysis reveals complex molecular aetiology in a cohort of idiopathic cerebral palsy
title_sort in-depth analysis reveals complex molecular aetiology in a cohort of idiopathic cerebral palsy
topic Original Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8967106/
https://www.ncbi.nlm.nih.gov/pubmed/34077496
http://dx.doi.org/10.1093/brain/awab209
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