Microdeletion of pseudogene chr14.232.a affects LRFN5 expression in cells of a patient with autism spectrum disorder

Cappuccio, Gerarda; Attanasio, Sergio; Alagia, Marianna; Mutarelli, Margherita; Borzone, Roberta; Karali, Marianthi; Genesio, Rita; Mormile, Angela; Nitsch, Lucio; Imperati, Floriana; Esposito, Annalisa; Banfi, Sandro; Giudice, Ennio Del; Brunetti‐Pierri, Nicola

doi:10.1038/s41431-019-0430-5

Cited by 16 publications

(13 citation statements)

References 25 publications

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“…Slitrk1 is a Tourette’s disorder candidate gene (Abelson et al 2005; O’Roak et al 2010) and Slitrk5 mouse mutants have OCD like phenotypes (Shmelkov et al 2010). Lrfn5 , encoding another leucine-rich repeat extracellular protein implicated in NDDs (Cappuccio et al 2019), was down-regulated in Pogz −/− as well.…”

Section: Resultsmentioning

confidence: 99%

Autism risk gene POGZ promotes chromatin accessibility and expression of clustered synaptic genes

Markenscoff-Papadimitriou

Binyameen

Whalen

et al. 2021

Preprint

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De novo mutations in POGZ, which encodes the chromatin regulator Pogo Transposable Element with ZNF Domain protein, are strongly associated with autism spectrum disorder (ASD). Here we find that in the developing mouse and human brain POGZ binds predominantly euchromatic loci and these are enriched for human neurodevelopmental disorder genes and transposable elements. We profile chromatin accessibility and gene expression in Pogz-/- mice and find that POGZ promotes chromatin accessibility of candidate regulatory elements (REs) and the expression of clustered synaptic genes. We further demonstrate that POGZ forms a nuclear complex and co-occupies loci with HP1gamma and ADNP, another high-confidence ASD risk gene. In Pogz+/- mice, Adnp expression is reduced. We postulate that reduced POGZ dosage disrupts cortical function through alterations in the POGZ-ADNP balance which modifies neuronal gene expression.

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Section: Resultsmentioning

confidence: 99%

Autism risk gene POGZ promotes chromatin accessibility and expression of clustered synaptic genes

Markenscoff-Papadimitriou

Binyameen

Whalen

et al. 2021

Preprint

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“…iPSC-derived neurons of patients with PTCHD1-AS deletions showed decreased excitatory synaptic activity, although PTCHD1 expression does not appear to be affected. This in contrast to lncLRFN5-10, which does appear to regulate expression of its nearby gene LRFN5 and was also found to be affected by a microdeletion in an ASD patient 80 . Translocations and deletions disrupting LINC00299 have been identified in patients with DD and ID 81,82 .…”

Section: Review Articlementioning

confidence: 79%

Interpreting the impact of noncoding structural variation in neurodevelopmental disorders

D’haene

Vergult

2021

Genetics in Medicine

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The emergence of novel sequencing technologies has greatly improved the identification of structural variation, revealing that a human genome harbors tens of thousands of structural variants (SVs). Since these SVs primarily impact noncoding DNA sequences, the next challenge is one of interpretation, not least to improve our understanding of human disease etiology. However, this task is severely complicated by the intricacy of the gene regulatory landscapes embedded within these noncoding regions, their incomplete annotation, as well as their dependence on the three-dimensional (3D) conformation of the genome. Also in the context of neurodevelopmental disorders (NDDs), reports of putatively causal, noncoding SVs are accumulating and understanding their impact on transcriptional regulation is presenting itself as the next step toward improved genetic diagnosis.

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“…Previous investigation demonstrates that RGS4 [83], CXCL11 [84], EGR1 [85], CALB1 [86], BDNF (brain derived neurotrophic factor) [87], TERT (telomerase reverse transcriptase) [88], NEFL (neurofilament light) [89], SNAP25 [90], RPH3A [91], NRN1 [92], SYT1 [93], GRIN2B [94], AVP (arginine vasopressin) [95], VSNL1 [96], HTR2A [97], PAK3 [98], STXBP5L [99], HCRTR2 [100], SYP (synaptophysin) [101], SYT10 [102], PRKCE (protein kinase C epsilon) [103], NRG1 [104], KISS1 [105], NRXN3 [106], RAB3A [107], IGF1 [108], PLK2 [109], CBLN4 [110], CAP2 [111], SV2B [112], CAMK4 [113], INA (internexin neuronal intermediate filament protein alpha) [114], GAP43 [115], TTR (transthyretin) [116], CXCR2 [117], IL1R2 [118], CXCR4 [119], CCR2 [120], MYOCD (myocardin) [121], S100A12 [122], CXCR3 [123], PROK2 [124], CXCL8 [125], RGS1 [126], NOTCH3 [127], P2RX7 [128], NGFR (nerve growth factor receptor) [129], GDF15 [130], CR1 [131], ADORA2A [132], GPER1 [133], FCGR2B [134], MMP9 [135], CNN2 [136], C5AR1 [137], CCL15 [138], RBPMS (RNA binding protein, mRNA processing factor) [139], TBX2 [140], FPR2 [141], PCK1 [142], ADH1B [143], TLR5 [144], C7 [145] and CD163 [146] are thought to contribute to AD development and it has been reported to act as a potential biomarkers for AD treatment. IL1RAPL2 [147], GAD1 [148], EPHA5 [149], HTR1A [150], CADPS (calcium dependent secretion activator) [151], GABRG3 [152], LRFN5 [153] a...…”

Section: Discussionmentioning

confidence: 99%

Bioinformatics analyses of significant genes, related pathways and candidate prognostic biomarkers in Alzheimer’s disease

Bm¹,

Cm²

2021

Preprint

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Alzheimers disease (AD) is one of the most common causes of dementia and frailty. This study aimed to use bioinformatics analysis to identify differentially expressed genes (DEGs) in AD. The Expression profiling by high throughput sequencing dataset GSE125583 was downloaded from the Gene Expression Omnibus (GEO) database and DEGs were identified. After assessment of Gene Ontology (GO) terms and pathway enrichment for DEGs, a protein protein interaction (PPI) network, module analysis, miRNA hub gene regulatory network construction and TF hub gene regulatory network were conducted via comprehensive target prediction and network analyses. Finally, we validated hub genes by receiver operating characteristic curve (ROC) and RT-PCR. In total, 956 DEGs were identified in the AD samples, including 479 up regulated genes and 477 down regulated genes. Functional enrichment analysis showed that these DEGs are mainly involved in the neuronal system, GPCR ligand binding, regulation of biological quality and cell communication. The hub genes of PAK1, ELAVL2, NSF, HTR2C, TERT, UBD, MKI67, HSPB1, PYHIN1 and TES might be associated with AD. The diagnostic value and expression levels of these hub genes in AD were further confirmed by ROC analysis and RT-PCR. In conclusion, we identified pathways and crucial candidate genes that affect the outcomes of patients with AD, and these genes might serve as potential therapeutic targets.

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Microdeletion of pseudogene chr14.232.a affects LRFN5 expression in cells of a patient with autism spectrum disorder

Cited by 16 publications

References 25 publications

Autism risk gene POGZ promotes chromatin accessibility and expression of clustered synaptic genes

Autism risk gene POGZ promotes chromatin accessibility and expression of clustered synaptic genes

Interpreting the impact of noncoding structural variation in neurodevelopmental disorders

Bioinformatics analyses of significant genes, related pathways and candidate prognostic biomarkers in Alzheimer’s disease

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