Pathogenic Variants in CEP85L Cause Sporadic and Familial Posterior Predominant Lissencephaly

University of Washington Center for Mendelian Genomics

doi:10.1016/j.neuron.2020.01.027

Pathogenic Variants in CEP85L Cause Sporadic and Familial Posterior Predominant Lissencephaly

University of Washington Center for Mendelian Genomics

研究成果: Article › 同行評審

11 引文斯高帕斯（Scopus）

摘要

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.

原文	English
頁（從 - 到）	237-245.e8
期刊	Neuron
卷	106
發行號	2
DOIs	https://doi.org/10.1016/j.neuron.2020.01.027
出版狀態	Published - 22 4月 2020

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10.1016/j.neuron.2020.01.027

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@article{f1a7a0b1250144538b946e34c4dd92d8,

title = "Pathogenic Variants in CEP85L Cause Sporadic and Familial Posterior Predominant Lissencephaly",

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.",

keywords = "centrosome, CEP85L, lissencephaly, pachygyria, posterior predominant, subcortical band heterotopia",

author = "{University of Washington Center for Mendelian Genomics} and Tsai, {Meng Han} and Muir, {Alison M.} and Wang, {Won Jing} and Kang, {Yi Ning} and Yang, {Kun Chuan} and Chao, {Nian Hsin} and Wu, {Mei Feng} and Chang, {Ying Chao} and Porter, {Brenda E.} and Jansen, {Laura A.} and Guillaume Sebire and Nicolas Deconinck and Fan, {Wen Lang} and Su, {Shih Chi} and Chung, {Wen Hung} and {Almanza Fuerte}, {Edith P.} and Mehaffey, {Michele G.} and Ng, {Ching Ching} and Chan, {Chung Kin} and Lim, {Kheng Seang} and Leventer, {Richard J.} and Lockhart, {Paul J.} and Kate Riney and Damiano, {John A.} and Hildebrand, {Michael S.} and Mirzaa, {Ghayda M.} and Dobyns, {William B.} and Berkovic, {Samuel F.} and Scheffer, {Ingrid E.} and Tsai, {Jin Wu} and Mefford, {Heather C.}",

note = "Publisher Copyright: {\textcopyright} 2020 Elsevier Inc.",

year = "2020",

month = apr,

day = "22",

doi = "10.1016/j.neuron.2020.01.027",

language = "English",

volume = "106",

pages = "237--245.e8",

journal = "Neuron",

issn = "0896-6273",

publisher = "Cell Press",

number = "2",

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TY - JOUR

T1 - Pathogenic Variants in CEP85L Cause Sporadic and Familial Posterior Predominant Lissencephaly

AU - University of Washington Center for Mendelian Genomics

AU - Tsai, Meng Han

AU - Muir, Alison M.

AU - Wang, Won Jing

AU - Kang, Yi Ning

AU - Yang, Kun Chuan

AU - Chao, Nian Hsin

AU - Wu, Mei Feng

AU - Chang, Ying Chao

AU - Porter, Brenda E.

AU - Jansen, Laura A.

AU - Sebire, Guillaume

AU - Deconinck, Nicolas

AU - Fan, Wen Lang

AU - Su, Shih Chi

AU - Chung, Wen Hung

AU - Almanza Fuerte, Edith P.

AU - Mehaffey, Michele G.

AU - Ng, Ching Ching

AU - Chan, Chung Kin

AU - Lim, Kheng Seang

AU - Leventer, Richard J.

AU - Lockhart, Paul J.

AU - Riney, Kate

AU - Damiano, John A.

AU - Hildebrand, Michael S.

AU - Mirzaa, Ghayda M.

AU - Dobyns, William B.

AU - Berkovic, Samuel F.

AU - Scheffer, Ingrid E.

AU - Tsai, Jin Wu

AU - Mefford, Heather C.

PY - 2020/4/22

Y1 - 2020/4/22

N2 - 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.

AB - 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.

KW - centrosome

KW - CEP85L

KW - lissencephaly

KW - pachygyria

KW - posterior predominant

KW - subcortical band heterotopia

UR - http://www.scopus.com/inward/record.url?scp=85083323136&partnerID=8YFLogxK

U2 - 10.1016/j.neuron.2020.01.027

DO - 10.1016/j.neuron.2020.01.027

M3 - Article

C2 - 32097630

AN - SCOPUS:85083323136

SN - 0896-6273

VL - 106

SP - 237-245.e8

JO - Neuron

JF - Neuron

IS - 2

ER -

Pathogenic Variants in CEP85L Cause Sporadic and Familial Posterior Predominant Lissencephaly

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