Pathogenic Variants in CEP85L Cause Sporadic and Familial Posterior Predominant Lissencephaly

doi:10.1016/j.neuron.2020.01.027

Title:	Pathogenic Variants in CEP85L Cause Sporadic and Familial Posterior Predominant Lissencephaly
Authors:	Tsai, Meng-Han Muir, Alison M. Wang, Won-Jing Kang, Yi-Ning Yang, Kun-Chuan Chao, Nian-Hsin Wu, Mei-Feng Chang, Ying-Chao Porter, Brenda E. Jansen, Laura A. Sebire, Guillaume Deconinck, Nicolas Fan, Wen-Lang Su, Shih-Chi Chung, Wen-Hung Fuerte, Edith P. Almanza Mehaffey, Michele G. Ng, Ching-Ching Chan, Chung-Kin Lim, Kheng-Seang Leventer, Richard J. Lockhart, Paul J. Riney, Kate Damiano, John A. Hildebrand, Michael S. Mirzaa, Ghayda M. Dobyns, William B. Berkovic, Samuel F. Scheffer, Ingrid E. Tsai, Jin-Wu Mefford, Heather C. 生物科技學系 Department of Biological Science and Technology
Issue Date:	22-Apr-2020
Abstract:	Lissencephaly (LIS), denoting a "smooth brain," is characterized by the absence of normal cerebral convolutions with abnormalities of cortical thickness. Pathogenic variants in over 20 genes are associated with LIS. The majority of posterior predominant LIS is caused by pathogenic variants in LIS1 (also known as PAFAH1B1), although a significant fraction remains without a known genetic etiology. We now implicate CEP85L as an important cause of posterior predominant LIS, identifying 13 individuals with rare, heterozygous CEP85L variants, including 2 families with autosomal dominant inheritance. We show that CEP85L is a centrosome protein localizing to the pericentriolar material, and knockdown of Cep85l causes a neuronal migration defect in mice. LIS1 also localizes to the centrosome, suggesting that this organelle is key to the mechanism of posterior predominant LIS.
URI:	http://dx.doi.org/10.1016/j.neuron.2020.01.027 http://hdl.handle.net/11536/154423
ISSN:	0896-6273
DOI:	10.1016/j.neuron.2020.01.027
Journal:	NEURON
Volume:	106
Issue:	2
Begin Page:	237
End Page:	0
Appears in Collections:	Articles