Concurrent occurrence of an inherited 16p13.11 microduplication and a de novo 19p13.3 microdeletion involving MAP2K2 in a patient with developmental delay, distinctive facial features, and lambdoid synostosis

AbstractWe report a patient with developmental delay, extremely short stature, small hands, dysmorphic facial features, hearing loss, and epilepsy carrying a de novo 2.76-Mb deletion of 2q36.3q37.1, including TRIP12 and NPPC. TRIP12 haploinsufficiency causes developmental delay with isolated dysmorphic facial features, whereas NPPC haploinsufficiency causes short stature and small hands. This is the first report of a unique phenotype, which is secondary to a microdeletion encompassing TRIP12 and NPPC.

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A Rare de novo Interstitial Duplication at 4p15.2 in a Boy with Severe Congenital Heart Defects, Limb Anomalies, Hypogonadism, and Global Developmental Delay

Cytogenetic and Genome Research ◽

10.1159/000454698 ◽

2016 ◽

Vol 150 (2) ◽

pp. 112-117 ◽

Cited By ~ 4

Author(s):

Liyang Liang ◽

Yingjun Xie ◽

Yiping Shen ◽

Qibin Yin ◽

Haiming Yuan

Keyword(s):

Developmental Delay ◽

Congenital Heart Defects ◽

Congenital Heart ◽

De Novo ◽

Heart Defects ◽

Deletion Syndrome ◽

Facial Features ◽

Chromosomal Microarray Analysis ◽

Limb Anomalies ◽

Interstitial Duplication

Proximal 4p deletion syndrome is a relatively rare genetic condition characterized by dysmorphic facial features, limb anomalies, minor congenital heart defects, hypogonadism, cafe-au-lait spots, developmental delay, tall and thin habitus, and intellectual disability. At present, over 20 cases of this syndrome have been published. However, duplication of the same region in proximal 4p has never been reported. Here, we describe a 2-year-5-month-old boy with severe congenital heart defects, limb anomalies, hypogonadism, distinctive facial features, pre- and postnatal developmental delay, and mild cognitive impairments. A de novo 4.5-Mb interstitial duplication at 4p15.2p15.1 was detected by chromosomal microarray analysis. Next-generation sequencing was employed and confirmed the duplication, but revealed no additional pathogenic variants. Several candidate genes in this interval responsible for the complex clinical phenotype were identified, such as RBPJ, STIM2, CCKAR, and LGI2. The results suggest a novel contiguous gene duplication syndrome.

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De novo chromosome 7q36.1q36.2 triplication in a child with developmental delay, growth failure, distinctive facial features, and multiple congenital anomalies: a case report

BMC Medical Genetics ◽

10.1186/s12881-017-0482-8 ◽

2017 ◽

Vol 18 (1) ◽

Cited By ~ 2

Author(s):

Muna A. Al Dhaibani ◽

Diane Allingham-Hawkins ◽

Ayman W. El-Hattab

Keyword(s):

Case Report ◽

Developmental Delay ◽

Congenital Anomalies ◽

De Novo ◽

Growth Failure ◽

Facial Features ◽

Multiple Congenital Anomalies

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Gene discovery for Mendelian conditions via social networking: de novo variants in KDM1A cause developmental delay and distinctive facial features

10.1101/028241 ◽

2015 ◽

Cited By ~ 2

Author(s):

Jessica X. Chong ◽

Joon-Ho Yu ◽

Peter Lorentzen ◽

Karen M. Park ◽

Seema M. Jamal ◽

...

Keyword(s):

Social Networking ◽

Developmental Delay ◽

De Novo ◽

Gene Discovery ◽

Pathogenic Variant ◽

Facial Features ◽

Variants Of Unknown Significance ◽

Mendelian Gene ◽

Unknown Significance ◽

Share Data

ABSTRACTPurpose:The pace of Mendelian gene discovery is slowed by the “n-of-1 problem” – the difficulty of establishing causality of a putatively pathogenic variant in a single person or family. Identification of an unrelated person with an overlapping phenotype and suspected pathogenic variant in the same gene can overcome this barrier but is often impeded by lack of a convenient or widely-available way to share data on candidate variants / genes among families, clinicians and researchers.Methods:Social networking among families, clinicians and researchers was used to identify three children with variants of unknown significance in KDM1A and similar phenotypes.Results:De novo variants in KDM1A underlie a new syndrome characterized by developmental delay and distinctive facial features.Conclusion:Social networking is a potentially powerful strategy to discover genes for rare Mendelian conditions, particularly those with non-specific phenotypic features. To facilitate the efforts of families to share phenotypic and genomic information with each other, clinicians, and researchers, we developed the Repository for Mendelian Genomics Family Portal (RMD-FP). Design and development of a web-based tool, MyGene2, that enables families, clinicians and researchers to search for gene matches based on analysis of phenotype and exome data deposited into the RMD-FP is underway.

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Recurrent de novo pathogenic variant of WASF1 in a Japanese patient with neurodevelopmental disorder with absent language and variable seizures

Human Genome Variation ◽

10.1038/s41439-021-00176-4 ◽

2021 ◽

Vol 8 (1) ◽

Author(s):

Keiko Shimojima Yamamoto ◽

Tomoe Yanagishita ◽

Hisako Yamamoto ◽

Yusaku Miyamoto ◽

Miho Nagata ◽

...

Keyword(s):

Developmental Delay ◽

Neurodevelopmental Disorders ◽

Japanese Patient ◽

De Novo ◽

Neurodevelopmental Disorder ◽

Pathogenic Variant ◽

Adult Patients ◽

Facial Features ◽

Initial Report

AbstractA recurrent de novo pathogenic variant of WASF1, NM_003931:c.1516C>T [p.Arg506*], was identified in a 6-year-old female Japanese patient with severe developmental delay, hypotonia, hyperkinetic behavior, and distinctive facial features. The initial report of five adult patients with WASF1 variants was the only previous report regarding variants of this gene; this is the second such report, reaffirming that rare but recurrent truncating variants of WASF1 are associated with severe neurodevelopmental disorders.

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