Inhibition of calpain increases LIS1(PAFAH1B1) and partially rescues in vivo phenotypes in a mouse model of lissencephaly

Lissencephaly is a devastating neurological disorder due to defective neuronal migration. LIS1 (or PAFAH1B1) was identified as the gene mutated in lissencephaly patients, and was found to regulate cytoplasmic dynein function and localization. Here, we show that more than half of LIS1 is degraded via...

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Autores principales: Yamada, Masami, Yoshida, Yuko, Mori, Daisuke, Takitoh, Takako, Kengaku, Mineko, Umeshima, Hiroki, Takao, Keizo, Miyakawa, Tsuyoshi, Sato, Makoto, Sorimachi, Hiroyuki, Wynshaw-Boris, Anthony, Hirotsune, Shinji
Formato: Texto
Lenguaje:English
Publicado: 2009
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Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2759411/
https://www.ncbi.nlm.nih.gov/pubmed/19734909
http://dx.doi.org/10.1038/nm.2023
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author Yamada, Masami
Yoshida, Yuko
Mori, Daisuke
Takitoh, Takako
Kengaku, Mineko
Umeshima, Hiroki
Takao, Keizo
Miyakawa, Tsuyoshi
Sato, Makoto
Sorimachi, Hiroyuki
Wynshaw-Boris, Anthony
Hirotsune, Shinji
author_facet Yamada, Masami
Yoshida, Yuko
Mori, Daisuke
Takitoh, Takako
Kengaku, Mineko
Umeshima, Hiroki
Takao, Keizo
Miyakawa, Tsuyoshi
Sato, Makoto
Sorimachi, Hiroyuki
Wynshaw-Boris, Anthony
Hirotsune, Shinji
author_sort Yamada, Masami
collection PubMed
description Lissencephaly is a devastating neurological disorder due to defective neuronal migration. LIS1 (or PAFAH1B1) was identified as the gene mutated in lissencephaly patients, and was found to regulate cytoplasmic dynein function and localization. Here, we show that more than half of LIS1 is degraded via calpain-dependent proteolysis, and that inhibition or knockdown of calpains protects LIS1 from proteolysis, resulting in the augmentation of LIS1 levels in Lis1+/− mouse embryonic fibroblast (MEF) cells, which leads to rescue of the aberrant distribution of cytoplasmic dynein, mitochondria and β-COP positive vesicles. We also show that calpain inhibitors improve neuronal migration of Lis1+/− cerebellar granular neurons. Intra-peritoneal injection of ALLN to pregnant Lis1+/− dams rescued apoptotic neuronal cell death and neuronal migration defects in Lis1+/− offspring. Furthermore, in utero knockdown of calpain by shRNA rescued defective cortical layering in Lis1+/− mice. Thus, the inhibition of calpain is a potential therapeutic intervention for lissencephaly.
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spelling pubmed-27594112010-04-01 Inhibition of calpain increases LIS1(PAFAH1B1) and partially rescues in vivo phenotypes in a mouse model of lissencephaly Yamada, Masami Yoshida, Yuko Mori, Daisuke Takitoh, Takako Kengaku, Mineko Umeshima, Hiroki Takao, Keizo Miyakawa, Tsuyoshi Sato, Makoto Sorimachi, Hiroyuki Wynshaw-Boris, Anthony Hirotsune, Shinji Nat Med Article Lissencephaly is a devastating neurological disorder due to defective neuronal migration. LIS1 (or PAFAH1B1) was identified as the gene mutated in lissencephaly patients, and was found to regulate cytoplasmic dynein function and localization. Here, we show that more than half of LIS1 is degraded via calpain-dependent proteolysis, and that inhibition or knockdown of calpains protects LIS1 from proteolysis, resulting in the augmentation of LIS1 levels in Lis1+/− mouse embryonic fibroblast (MEF) cells, which leads to rescue of the aberrant distribution of cytoplasmic dynein, mitochondria and β-COP positive vesicles. We also show that calpain inhibitors improve neuronal migration of Lis1+/− cerebellar granular neurons. Intra-peritoneal injection of ALLN to pregnant Lis1+/− dams rescued apoptotic neuronal cell death and neuronal migration defects in Lis1+/− offspring. Furthermore, in utero knockdown of calpain by shRNA rescued defective cortical layering in Lis1+/− mice. Thus, the inhibition of calpain is a potential therapeutic intervention for lissencephaly. 2009-09-06 2009-10 /pmc/articles/PMC2759411/ /pubmed/19734909 http://dx.doi.org/10.1038/nm.2023 Text en Users may view, print, copy, download and text and data- mine the content in such documents, for the purposes of academic research, subject always to the full Conditions of use: http://www.nature.com/authors/editorial_policies/license.html#terms
spellingShingle Article
Yamada, Masami
Yoshida, Yuko
Mori, Daisuke
Takitoh, Takako
Kengaku, Mineko
Umeshima, Hiroki
Takao, Keizo
Miyakawa, Tsuyoshi
Sato, Makoto
Sorimachi, Hiroyuki
Wynshaw-Boris, Anthony
Hirotsune, Shinji
Inhibition of calpain increases LIS1(PAFAH1B1) and partially rescues in vivo phenotypes in a mouse model of lissencephaly
title Inhibition of calpain increases LIS1(PAFAH1B1) and partially rescues in vivo phenotypes in a mouse model of lissencephaly
title_full Inhibition of calpain increases LIS1(PAFAH1B1) and partially rescues in vivo phenotypes in a mouse model of lissencephaly
title_fullStr Inhibition of calpain increases LIS1(PAFAH1B1) and partially rescues in vivo phenotypes in a mouse model of lissencephaly
title_full_unstemmed Inhibition of calpain increases LIS1(PAFAH1B1) and partially rescues in vivo phenotypes in a mouse model of lissencephaly
title_short Inhibition of calpain increases LIS1(PAFAH1B1) and partially rescues in vivo phenotypes in a mouse model of lissencephaly
title_sort inhibition of calpain increases lis1(pafah1b1) and partially rescues in vivo phenotypes in a mouse model of lissencephaly
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2759411/
https://www.ncbi.nlm.nih.gov/pubmed/19734909
http://dx.doi.org/10.1038/nm.2023
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