ライフサイエンスコーパス: lissencephaly

1 y contribute to the cell-sparse pathology of lissencephaly.

2 ed with a human cortical malformation termed lissencephaly.

3 ell migration diseases including Cobblestone lissencephaly.

4 eterotopia, subcortical band heterotopia and lissencephaly.

5 ene cause the smooth brain disease classical lissencephaly.

6 ion defects resembling cobblestone (type II) lissencephaly.

7 causing the severe human brain malformation lissencephaly.

8 raphically distinguishable recessive form of lissencephaly.

9 entical neuronal migration defects, known as lissencephaly.

10 pling may contribute to migration defects in lissencephaly.

11 nized genetic anomaly associated with type I lissencephaly.

12 new insights into the pathogenesis of type I lissencephaly.

13 in the neuronal migration disorder X-linked lissencephaly.

14 vere developmental brain abnormality, type I lissencephaly.

15 d to a very similar phenotype, termed type 1 lissencephaly.

16 neuronal basis for seizures associated with lissencephaly.

17 s a malformation of the human brain known as lissencephaly.

18 spared him from the more severe phenotype of lissencephaly.

19 Lis1, a mouse model of human 17p13.3-linked lissencephaly.

20 le epilepsy, and bilateral temporo-occipital lissencephaly.

21 eterotopia) and affected males show X-linked lissencephaly.

22 mutations in the same exons have had diffuse lissencephaly.

23 migration defects observed in Miller-Dieker lissencephaly.

24 an neuronal migration disorder Miller-Dieker lissencephaly.

25 patients with the neurodevelopmental disease lissencephaly.

26 psy or cognitive impairments associated with lissencephaly.

27 ll the basis of TMTC3-associated Cobblestone lissencephaly.

28 fficiency in the neurodevelopmental disorder lissencephaly.

29 PTEN-related macrocephaly and Miller-Dieker lissencephaly.

30 lopment and is associated with human type II lissencephaly.

31 doublecortin, is the main cause of classical lissencephaly.

32 structural homology with LIS1, which causes lissencephaly.

33 s, DCX is a major genetic locus for X-linked lissencephaly.

34 e molecular and cellular bases of DCX-linked lissencephaly.

35 otypes that frequently accompany cobblestone lissencephaly.

36 the human neurodevelopmental disorder Type I Lissencephaly.

37 ration and a smooth brain phenotype known as lissencephaly.

38 iventricular and subcortical heterotopia and lissencephaly.

39 cerebral cortex malformation in cobblestone lissencephaly.

40 was demonstrated in a mouse model of type I lissencephaly.

41 neocortex and hippocampus known as classical lissencephaly.

42 involved in the pathogenesis of cobblestone lissencephalies.

43 rms of human brain malformation than classic lissencephalies.

44 as to the broad clinical spectrum of type II lissencephalies.

45 n E-like (Nudel or Ndel1) interact with both lissencephaly 1 (Lis1) and dynein.

46 letions on chromosome 17p13.3, including the lissencephaly 1 (LIS1) gene.

47 The microtubule-associated protein lissencephaly 1 (Lis1) is a key regulator of cell divisi

48 verlapping localization patterns of ASUN and lissencephaly 1 (LIS1), a dynein adaptor, suggest that A

49 lear distribution factor E-homolog 1 (NDE1), Lissencephaly 1 (LIS1), and NDE-like 1 (NDEL1) together

50 2, and a third subunit, the dynein regulator lissencephaly 1 (LIS1), mediates the structure and funct

51 olding protein 4.1B and the dynein regulator lissencephaly 1 (Lis1).

52 We conclude that the NDE1/Lissencephaly 1 and dynactin complexes separately mediat

53 The lissencephaly 1 gene, LIS1, is mutated in patients with

54 tor acetylhydrolase, isoform Ib, PAFAH1B1 or lissencephaly 1 protein (LIS1) and nuclear distribution

55 The lissencephaly 1 protein, LIS1, is mutated in type-1 liss

56 e dynactin complex, cargo adapters and LIS1 (Lissencephaly 1).

57 and in Lis1, the Drosophila homolog of human lissencephaly 1, reinforcing the role of the dynein comp

58 The main causative gene of this disease - lissencephaly-1 (LIS1) - has been a focus of intense scr

59 We identified the protein Lissencephaly-1 (Lis1) and found that minus-end travel d

60 of dynactin, end-binding protein-1 (EB1) and Lissencephaly-1 (LIS1) in the interaction of end trackin

61 Lissencephaly-1 (LIS1) is a highly conserved dynein-regu

62 Lissencephaly-1 (Lis1) is a key cofactor for dynein-medi

63 and the role of critical regulators such as lissencephaly-1 (LIS1) protein (LIS1) remain unclear.

64 Here we show that Lissencephaly-1 (Lis1) regulates BMP signaling and E-cad

65 ogether with dynein's cofactors dynactin and Lissencephaly-1 (Lis1).

66 -D2 (BicD2) or the multifunctional regulator Lissencephaly-1 (Lis1).

67 The CTLH (C-terminal to lissencephaly-1 homology motif) complex is a multisubuni

68 on of muskelin with RanBP9, and its atypical lissencephaly-1 homology motif, which has a nuclear loca

69 ase IB subunit alpha (Pafah1b1), also called Lissencephaly-1, can cause classical lissencephaly, a se

70 Deficiency of the LIS1 protein causes lissencephaly, a brain developmental disorder.

71 Mutations in Lis1 cause classical lissencephaly, a developmental brain abnormality charact

72 Mutation of human LIS1 causes lissencephaly, a developmental brain disorder.

73 nalysis of infant human neocortex exhibiting lissencephaly, a developmental malformation thought to b

74 ked to LIS-1, the disease gene for a form of lissencephaly, a disorder of cortical development.

75 Haploinsufficiency of LIS1 results in lissencephaly, a human neuronal migration disorder.

76 ng reelin) or PAFAH1B1 (encoding LIS1) cause lissencephaly, a human neuronal migration disorder.

77 e of two major genetic loci underlying human lissencephaly, a neurodevelopmental disorder with defect

78 ales with loss of the X-linked DCX result in lissencephaly, a neuronal migration defect.

79 Type I lissencephaly, a neuronal migration disorder characteriz

80 utations in the human LIS1 gene cause type I lissencephaly, a severe brain developmental disease invo

81 Lissencephaly, a severe cortical malformation caused by

82 as LIS1) in humans is associated with type I lissencephaly, a severe developmental brain disorder tho

83 ng mutations of the Lis1 gene display type I lissencephaly, a severe form of cortical dysplasia hypot

84 called Lissencephaly-1, can cause classical lissencephaly, a severe malformation of cortical develop

85 Twenty-two genes are associated with lissencephaly, accounting for approximately 80% of disea

86 pically includes severe brain malformations (lissencephaly, agenesis of the corpus callosum, and midb

87 , which comprises the less severe end of the lissencephaly (agyria-pachygyria-band) spectrum of malfo

88 type of TUBA1A and TUBG1 tubulinopathies are lissencephalies and microlissencephalies, whereas TUBB2B

89 ent progress made in understanding the human lissencephalies and related disorders.

90 X-linked lissencephaly and "double cortex" are allelic human diso

91 ormation syndrome characterized by classical lissencephaly and a characteristic facies.

92 ammalian brain, and its misregulation causes lissencephaly and behavioral and cognitive defects.

93 cloned following the study of children with lissencephaly and cytogenetic abnormalities involving ch

94 ulated the thickened cortex typical of human lissencephaly and demonstrated dysregulation of protein

95 Classical lissencephaly and double cortex are genetic neuronal mig

96 ephaly 1 protein, LIS1, is mutated in type-1 lissencephaly and is a key regulator of cytoplasmic dyne

97 results in the severe developmental disorder lissencephaly and is associated with neurological diseas

98 Cobblestone (type II) lissencephaly and mental retardation are characteristic

99 ) are frequently associated with cobblestone lissencephaly and mental retardation.

100 a-tubulin genes have been identified in both lissencephaly and polymicrogyria, usually associated wit

101 ties agree with the classical pathologies of lissencephaly and polymicrogyria.

102 r gradient similar to PAFAH1B1(LIS1)-related lissencephaly and severe hypoplasia or absence of the co

103 ngenital muscular dystrophy with cobblestone lissencephaly and structural eye defects to a mild form

104 c putative signaling protein, cause X-linked lissencephaly and subcortical band heterotopia.

105 CX (Xq22.3), a gene associated with X-linked lissencephaly and subcortical band heterotopia.

106 ronal migration abnormalities (often type II lissencephaly) and ocular or retinal defects.

107 restriction, ventriculomegaly, microcephaly, lissencephaly, and extensive degenerative changes of the

108 oprosencephaly, periventricular heterotopia, lissencephaly, and Joubert syndrome.

109 nhibitory input may underlie the epilepsy in lissencephaly, and suggest potential therapeutic strateg

110 The lissencephalies are usually single-gene disorders affect

111 Polymicrogyria and lissencephaly are causally heterogeneous disorders of co

112 These data suggest that SBH and X-linked lissencephaly are caused by mutation of a single gene, X

113 Among the clinical consequences of lissencephaly are mental retardation and intractable epi

114 Signaling pathways that help maintain lissencephaly are still poorly understood.

115 orders in humans, including microcephaly and lissencephaly, are often associated with impaired gyrifi

116 lso occurred, similar to type II cobblestone lissencephaly as seen in congenital muscular dystrophy.

117 issencephaly, similar to PAFAH1B1-associated lissencephaly, as well as co-occurrence of subcortical h

118 Megalencephaly and lissencephaly associated with defective programmed cell

119 experimental paradigm in understanding human lissencephaly, but clear limitations exist in these stud

120 llelic variants have moderate frontotemporal lissencephaly, but with normal cerebellar structure and

121 ns of TMTCs provide insight into cobblestone lissencephaly caused by deficiency in TMTC3.

122 Cobblestone lissencephaly (COB) is a severe brain malformation in wh

123 Much of our knowledge about DCX-associated lissencephaly comes from post-mortem analyses of patient

124 Lissencephaly comprises a spectrum of brain malformation

125 Lissencephaly comprises a spectrum of malformations of c

126 MDS and ILS deletion patients, localizes the lissencephaly critical region within the LIS1 gene.

127 d epilepsy, including double cortex/X-linked lissencephaly (DC/XLIS), have been localized to Xq21.3-q

128 ince discovery of the first genetic cause of lissencephaly, deletions of chromosome 17p13.3 in Miller

129 Deletion of the lissencephaly disease gene LIS-1 in humans causes an ext

130 interactions more accurately, and map type-1 lissencephaly disease mutations, as well as mutations in

131 the product of the gene mutated in X-linked lissencephaly/double cortex syndrome, a severe developme

132 otopia, polymicrogyria, band heterotopia and lissencephaly, dysembryoplastic neuroepithelial tumours,

133 changes suggests shared function with other lissencephaly-encoded cytoskeletal proteins such as alph

134 distinct phenotypes including frontotemporal lissencephaly, epilepsy, autism and probably schizophren

135 Secondary lissencephaly evolved in mice due to effects on neurogen

136 Four double cortex/X-linked lissencephaly families and three sporadic double cortex

137 TMTC3 mutations associated with Cobblestone lissencephaly found that three of the variants exhibit r

138 to dissociate the epileptic consequences of lissencephaly from the more phenotypically overt cortica

139 ion factor FOXO1 that represses the X-linked lissencephaly gene encoding doublecortin (DCX).

140 RNA interference (RNAi) of the lissencephaly gene LIS1 (also known as PAFAH1b1) inhibit

141 Two identified lissencephaly genes do not account for all known cases,

142 atients with missense mutations had a milder lissencephaly grade compared with those with mutations l

143 lon delineates patients with the most severe lissencephaly grade.

144 euronal disorganization resulting from Lis1 (lissencephaly) haploinsufficiency contributes to cogniti

145 rved motif within the amino-terminal domain, lissencephaly homology motif (LisH) and C-terminal to Li

146 topias resembling those found in cobblestone lissencephalies in which neuroepithelial cells migrate i

147 expression explains the frontal-predominant lissencephaly in an individual with a homozygous stop-ga

148 cellular infiltrations, calcifications, and lissencephaly in fetal brains.

149 ein, whose gene (DCX) has been implicated in lissencephaly in humans.

150 c facial features and a more severe grade of lissencephaly in MDS.

151 s on neocortical gyrification and shows that lissencephaly in mice is actively maintained via redunda

152 o maintain normal levels of neurogenesis and lissencephaly in mice.

153 s together sustain neurogenic continuity and lissencephaly in rodent cortices.

154 rom two males with mutated DCX and classical lissencephaly including smooth brain and abnormal cortic

155 five genes that cause or contribute to human lissencephaly, including LIS1, 14-3-3 epsilon, DCX, RELN

156 Type I lissencephaly is a central nervous system (CNS) malforma

157 Lissencephaly is a cortical malformation secondary to im

158 Classical lissencephaly is a genetic neurological disorder associa

159 Lissencephaly is a human developmental brain abnormality

160 Classical lissencephaly is a human developmental brain disorder ch

161 Lissencephaly is a malformation of cortical development

162 Type I lissencephaly is a neuronal migration disorder caused by

163 Lissencephaly is a severe brain malformation caused by i

164 Lissencephaly is a severe brain malformation in which fa

165 Lissencephaly is a severe congenital brain malformation

166 The pathogenesis of type I lissencephaly is believed to be a defect in radial neuro

167 For example, lissencephaly is caused by mutations in the dynein-assoc

168 Classical lissencephaly is characterized by smooth cerebral surfac

169 An autosomal recessive form of lissencephaly (LCH) associated with severe abnormalities

170 pic similarity with existing mouse models of lissencephaly led us to screen a cohort of patients with

171 n in meningeal fibroblasts and a cobblestone lissencephaly-like phenotype in the developing cortex.

172 lectively facilitates phosphorylation of the lissencephaly-linked doublecortin (DCX) by cdk5/p35, but

173 ively facilitates the phosphorylation of the lissencephaly-linked protein doublecortin (DCX) by cdk5/

174 Classical lissencephaly (LIS) is a neuronal migration disorder res

175 ortical band heterotopia (SBH) and classical lissencephaly (LIS) result from deficient neuronal migra

176 Lissencephaly (LIS), denoting a "smooth brain," is chara

177 Subcortical band heterotopia (SBH) and lissencephaly (LIS), two distinct neuronal migration dis

178 s PAF and is composed of three subunits [the lissencephaly (LIS1) protein and alpha1 and alpha2 subun

179 devastating human brain malformation, type I lissencephaly (Lis1).

180 tion of cortical development that results in lissencephaly (meaning smooth brain).

181 romes: (i) microlissencephaly (n = 12); (ii) lissencephaly (n = 19); (iii) central pachygyria and pol

182 a relationship between the specific type of lissencephaly observed and deficiency of specific modes

183 of polymicrogyria and five with an atypical lissencephaly on neuroimaging.

184 ene cause gross neocortical disorganization (lissencephaly or "smooth brain") in hemizygous males, wh

185 s resembling defects in type 2 (cobblestone) lissencephaly or congenital muscular dystrophies but app

186 or doublecortin can lead to either classical lissencephaly or double cortex, but because LIS1 is auto

187 versed cellular and molecular defects in the lissencephaly organoids.

188 The agyria (lissencephaly)/pachygyria phenotypes are catastrophic de

189 racteristic cerebellar dysplasia but without lissencephaly, pachygyria and polymicrogyria typically a

190 ons of cortical development (MCD), typically lissencephaly, pachygyria and polymicrogyria; however, s

191 Such "tubulinopathies" include lissencephaly/pachygyria, polymicrogyria-like malformati

192 ual disability, short stature, microcephaly, lissencephaly, periventricular heterotopia, polymicrogyr

193 remains the strongest candidate gene for the lissencephaly phenotype in ILS and MDS.

194 Given the similarities between the lissencephaly phenotypes that result from aberrations in

195 n array of neurological disorders, including lissencephaly, polymicrogyria and microcephaly.

196 Human cortical malformations, including lissencephaly, polymicrogyria and other diseases of neur

197 ter segment proteins were reduced, but LIS1 (lissencephaly protein 1), a well-characterized dynein co

198 The lissencephaly protein Lis1 has been reported to regulate

199 f the PAFAH1B complex and, particularly, the lissencephaly protein Lis1 in spermatogenesis.

200 that Pac1, the yeast homologue of the human lissencephaly protein LIS1, plays a key role in this pro

201 Mutations of doublecortin causing lissencephaly (R59H, D62N, and G253D) abolished binding

202 Moreover, we find that the Lissencephaly-related protein, LIS1 (Pac1 in yeast), pla

203 However, the basis of the epilepsy in lissencephaly remains unclear.

204 A, identified in patients with pachygyria or lissencephaly, respectively.

205 idence of additional abnormalities including lissencephaly, schizencephaly, polymicrogyria and, in on

206 S1 may contribute to the more severe form of lissencephaly seen only in patients with MDS.

207 human neuronal migration disorders isolated lissencephaly sequence (ILS) and the more severe Miller-

208 ith Miller-Dieker syndrome (MDS) or isolated lissencephaly sequence (ILS) have a hemizygous deletion

209 Approximately 65% of patients with isolated lissencephaly sequence (ILS) show intragenic mutations o

210 owever, the phenotype can vary from isolated lissencephaly sequence (ILS) to Miller-Dieker syndrome (

211 been observed and is referred to as isolated lissencephaly sequence (ILS).

212 Isolated lissencephaly sequence and Miller-Dieker syndrome are re

213 two related neurological disorders: isolated lissencephaly sequence and Miller-Dieker syndrome.

214 encoding LIS1) in 17p13.3 result in isolated lissencephaly sequence, and extended deletions including

215 Our results suggest that the lissencephaly severity in ILS caused by LIS1 mutations m

216 phenotypes and hypothesize that the greater lissencephaly severity seen in Miller-Dieker syndrome ma

217 demonstrate extensive posterior predominant lissencephaly, similar to PAFAH1B1-associated lissenceph

218 rons to arrest in the cortex lead to type II lissencephaly (smooth brain with clusters of neurons alo

219 quired for neuroblast migration cause type I lissencephaly (smooth brain) and subcortical band hetero

220 nsufficiency of human LIS1 results in type I lissencephaly (smooth brain) with severely reduced surfa

221 LIS1, the product of a causal gene for human lissencephaly (smooth brain), has also been implicated i

222 Mutations of the LIS1 gene result in human lissencephaly (smooth brain), which features misplaced c

223 n major brain malformations, including human lissencephaly (smooth brain).

224 Lissencephaly ("smooth brain," from "lissos," meaning sm

225 Lissencephaly ('smooth brain') is a severe brain disease

226 Lissencephaly ('smooth brain') spectrum disorders compri

227 a clinically relevant molecular mechanism in lissencephaly spectrum disorders.

228 nism contributes to two genetically distinct lissencephaly spectrum disorders.

229 account for nearly a quarter of all cases of lissencephaly-spectrum brain malformations(2)(,)(3) that

230 p.Cys539Arg and p.Arg3207Cys associated with lissencephaly suggesting a dominant-negative effect.

231 p13.3 microdeletion leading to Miller-Dieker lissencephaly syndrome (MDLS).

232 -epicanthus inversus syndrome, Miller-Dieker lissencephaly syndrome, and Williams-Beuren syndrome--in

233 account for all known cases, and additional lissencephaly syndromes have been described.

234 ule-binding domain resulted in a more severe lissencephaly than later truncation/deletion mutations (

235 a more important role in the development of lissencephaly than previously suspected.

236 In classical lissencephaly, the six-layered cortex is replaced by a f

237 port on 12 individuals with a unique form of lissencephaly; these individuals come from eight unrelat

238 Here we describe a "thin" lissencephaly (TLIS) variant characterized by megalencep

239 e products of genes mutated in Miller-Dieker lissencephaly, Treacher Collins, oral-facial-digital typ

240 ith dramatic neuroanatomical defects such as lissencephaly type II or cobblestone brain.

241 n RELN have been associated with a recessive lissencephaly variant with cerebellar hypoplasia, which

242 N and frontotemporal or temporal-predominant lissencephaly variant.

243 established Drosophila model for cobblestone lissencephaly was used to understand how Dg is regulated

244 tin (Dcx) is the causative gene for X-linked lissencephaly, which encodes a microtubule-binding prote

245 e associated with the anatomical abnormality lissencephaly, which is believed to reflect failure of n

246 h humans and mice that resembles cobblestone lissencephaly, which is characterized by overmigration o

247 LIS1 gene, result in the brain malformation lissencephaly, which is characterized by reduced gyratio

248 d from individuals with genetically distinct lissencephalies with a recessive mutation in p53-induced

249 a highly recognizable combination of classic lissencephaly with a posterior more severe than anterior

250 est that truncating mutations cause X-linked lissencephaly with abnormal genitalia, and insertion/mis

251 ive spectrum of tubulinopathies and X-linked lissencephaly with abnormal genitalia, but neurodevelopm

252 X mutations have also been found in X-linked lissencephaly with abnormal genitalia, which typically i

253 gene, only 11 individuals with RELN-related lissencephaly with cerebellar hypoplasia from six famili

254 r' phenotype in mice and autosomal recessive lissencephaly with cerebellar hypoplasia in man.

255 Homozygous RELN mutations are known to cause lissencephaly with cerebellar hypoplasia.

256 me, ventriculomegaly, cerebellar hypoplasia, lissencephaly with hydrocephalus, and fetal akinesia def

257 y have severe brain abnormalities resembling lissencephaly, with abnormal layering of neurons in the

258 Lissencephaly without facial dysmorphism has also been o

259 sociated protein that is mutated in X-linked lissencephaly (X-LIS), a neuronal migration disorder ass

260 ex" syndrome (DC) in females and to X-linked lissencephaly (XLIS) in males.