Planar cell polarity genes, Celsr1-3, in neural development

Feng, Jia; Han, Qi; Zhou, Libing

doi:10.1007/s12264-012-1232-8

Cited by 36 publications

(25 citation statements)

References 49 publications

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“…These data suggest that LSD1 and HDACs might associate with REST and other factors to create a repressive chromatin environment in untreated cells and that Corin blocks the removal of activating chromatin marks by LSD1 and HDACs at these regions. This hypothesis is exemplified by increased H3K27ac and H3K4me1 near predicted REST-binding sites at the CELSR1 locus ( Figure 2F), which encodes a regulator of neuronal differentiation and brain development (Boucherie et al, 2018;Feng et al, 2012), and a Corin-dependent increase in H3K27ac and H3K4me1 at REST sites on a global scale ( Figure S5D). In contrast, motifs bound by MAFG and NR3C family nuclear receptors are enriched in regions where Corin induces H3K27me3 ( Figure 2D).…”

Section: Chip-seq Reveals Global Alterations In H3k4me1- H3k27me3- mentioning

confidence: 86%

Re-programing Chromatin with a Bifunctional LSD1/HDAC Inhibitor Induces Therapeutic Differentiation in DIPG

et al. 2019

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Section: Chip-seq Reveals Global Alterations In H3k4me1- H3k27me3- mentioning

confidence: 86%

Re-programing Chromatin with a Bifunctional LSD1/HDAC Inhibitor Induces Therapeutic Differentiation in DIPG

et al. 2019

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“…CELSR3 belongs to the flamingo subfamily of non-classic cadherins, which are defined by non-interaction with catenins and seven transmembrane domains (Feng et al, 2012). The protein encoded by this gene may be involved in the regulation of contact-dependent neurite outgrowth (Chai et al, 2015).…”

Section: Discussionmentioning

confidence: 99%

De Novo Coding Variants Are Strongly Associated with Tourette Disorder

Willsey

Fernandez

et al. 2017

Neuron

154

187

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SUMMARY Whole-exome sequencing (WES) and de novo variant detection have proven a powerful approach to gene discovery in complex neurodevelopmental disorders. We have completed WES of 325 Tourette disorder trios from the Tourette International Collaborative Genetics cohort and a replication sample of 186 trios from the Tourette Syndrome Association International Consortium on Genetics (511 total). We observe strong and consistent evidence for the contribution of de novo likely gene-disrupting (LGD) variants (rate ratio [RR] 2.32, p = 0.002). Additionally, de novo damaging variants (LGD and probably damaging missense) are overrepresented in probands (RR 1.37, p = 0.003). We identify four likely risk genes with multiple de novo damaging variants in unrelated probands: WWC1 (WW and C2 domain containing 1), CELSR3 (Cadherin EGF LAG seven-pass G-type receptor 3), NIPBL (Nipped-B-like), and FN1 (fibronectin 1). Overall, we estimate that de novo damaging variants in approximately 400 genes contribute risk in 12% of clinical cases.

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“…CELSR1 is a developmentally regulated, neural‐specific gene involved in early embryogenesis. Recent work has shown that Celsr1 play important roles in neural development, such as in axon guidance and neuronal migration (Feng, Han, & Zhou, ). From a clinical point of view, coding mutations of CELSR1 were associated to neural tube defect both in mouse (Curtin et al, ) than in men (De Marco et al, ).…”

Section: Discussionmentioning

confidence: 99%

Clinical and molecular characterization of an emerging chromosome 22q13.31 microdeletion syndrome

Palumbo

Accadia

Leone

et al. 2017

American J of Med Genetics Pt A

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Microdeletion of chromosome 22q13.31 is a very rare condition. Fourteen patients have been annotated in public databases but, to date, a clinical comparison has not been done and, consequently, a specific phenotype has not been delineated yet. We describe a patient showing neurodevelopmental disorders, dysmorphic features, and multiple congenital anomalies in which SNP array analysis revealed an interstitial 3.15 Mb de novo microdeletion in the 22q13.31 region encompassing 21 RefSeq genes and seven non-coding microRNAs. To perform an accurate phenotype characterization, clinical features observed in previously reported cases of 22q13.31 microdeletions were reviewed and compared to those observed in our patient. To the best of our knowledge, this is the first time that a comparison between patients carrying overlapping 22q13.31 deletions has been done. This comparison allowed us to identify a distinct spectrum of clinical manifestations suggesting that patients with a de novo interstitial microdeletion involving 22q13.31 have an emerging syndrome characterized by developmental delay/intellectual disability, speech delay/language disorders, behavioral problems, hypotonia, urogenital, and hands/feet anomalies. The microdeletion identified in our patient is the smallest reported so far and, for this reason, useful to perform a detailed genotype-phenotype correlation. In particular, we propose the CELSR1, ATXN10, FBLN1, and UPK3A as candidate genes in the onset of the main clinical features of this contiguous gene syndrome. Thus, the patient reported here broadens our knowledge of the phenotypic consequences of 22q13.31 microdeletions facilitating genotype-phenotype correlations. Additional cases are needed to corroborate our hypothesis and confirm genotype-phenotype correlations of this emerging syndrome.

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Planar cell polarity genes, Celsr1-3, in neural development

Cited by 36 publications

References 49 publications

Re-programing Chromatin with a Bifunctional LSD1/HDAC Inhibitor Induces Therapeutic Differentiation in DIPG

Re-programing Chromatin with a Bifunctional LSD1/HDAC Inhibitor Induces Therapeutic Differentiation in DIPG

De Novo Coding Variants Are Strongly Associated with Tourette Disorder

Clinical and molecular characterization of an emerging chromosome 22q13.31 microdeletion syndrome

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