2011
DOI: 10.1016/j.ajhg.2011.09.011
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Assessment of 2q23.1 Microdeletion Syndrome Implicates MBD5 as a Single Causal Locus of Intellectual Disability, Epilepsy, and Autism Spectrum Disorder

Abstract: Persons with neurodevelopmental disorders or autism spectrum disorder (ASD) often harbor chromosomal microdeletions, yet the individual genetic contributors within these regions have not been systematically evaluated. We established a consortium of clinical diagnostic and research laboratories to accumulate a large cohort with genetic alterations of chromosomal region 2q23.1 and acquired 65 subjects with microdeletion or translocation. We sequenced translocation breakpoints; aligned microdeletions to determine… Show more

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Cited by 199 publications
(247 citation statements)
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“…One such example is the 2q23.1 deletion syndrome, which has been associated with intellectual disability, seizures, microcephaly, and speech delay. Recently, the minimal region has been fine mapped via deletions as small as 37 kbp to a single gene-MBD5 [1, [52][53][54][55]. This gene has also been discovered to contain both a rare mutation and common variants as well as translocation breakpoints by sequencing studies of ID, epilepsy, and ASD (Figure 2) [52,53].…”
Section: Size Spectrum Of Copy Number Variationmentioning
confidence: 99%
“…One such example is the 2q23.1 deletion syndrome, which has been associated with intellectual disability, seizures, microcephaly, and speech delay. Recently, the minimal region has been fine mapped via deletions as small as 37 kbp to a single gene-MBD5 [1, [52][53][54][55]. This gene has also been discovered to contain both a rare mutation and common variants as well as translocation breakpoints by sequencing studies of ID, epilepsy, and ASD (Figure 2) [52,53].…”
Section: Size Spectrum Of Copy Number Variationmentioning
confidence: 99%
“…4 Further, these NDDs share many overlapping features, including a high prevalence of sleep disturbance. Understanding the molecular alterations in NDDs individually and collectively and the subsequent overlapping pathways affected that lead to the sleep disturbance could possibly lead to behavioral and pharmaceutical therapies.…”
Section: Introductionmentioning
confidence: 99%
“…4 Genomic disruptions of MBD5 lead to the primary clinical phenotypes present in the disorder, including ID, epilepsy, speech impairment, unusual behaviors, ASD, and broad-based ataxic gate. 4 Sleep disturbance have been previously reported in a few cases.…”
Section: Introductionmentioning
confidence: 99%
“…Interestingly, both NRXN1 and the postsynaptic binding partners NLGN1-4 have been strongly implicated in autism and reviewed elsewhere [106,[167][168][169][170]. MBD5, a methylCpG-binding domain gene, has been identified as the causal gene in the 2q23.1 locus, which is characterized by ASD and ID [171,172]. Deletions encompassing the C-terminus of AUTS2 are associated with autistic features and developmental delay [173].…”
Section: Other Recurrent Cnvs In Asd and Cnvs That Identify Individuamentioning
confidence: 99%