Interstitial Microduplication at 2p11.2 in a Patient with Syndromic Intellectual Disability: 30-year Follow-up

Overview

Journal Mol Cytogenet

Publisher Biomed Central

Specialty Biochemistry

Date 2014 Oct 9

PMID 25295072

Citations 5

Authors

Kyung Ran Jun

Reinhard Ullmann

Saadullah Khan

Lawrence C Layman

Hyung-Goo Kim

Affiliations

Soon will be listed here.

Abstract

Background: Copy number variations at 2p11.2 have been rare and to our knowledge, no abnormal phenotype with an interstitial 2p11.2 duplication has yet been reported. Here we report the first case with syndromic intellectual disability associated with microduplication at 2p11.2.

Results: We revisited a white female subject with a chromosome translocation, t(8;10)(p23;q23)mat and a 10q telomeric deletion suspected by G-banding 30 years ago. This female with severe intellectual disability, no speech, facial dysmorphism, intractable epilepsy, recurrent infection, and skeletal abnormalities has been observed from the birth until her death. The karyotype analysis reconfirmed the previously reported chromosome translocation with a revision as 46,XX,t(8;10)(p23.3;q23.2)mat by adding more detail in chromosomal sub-bands. The array comparative genomic hybridization, however, did not detect the 10q terminal deletion originally reported, but instead, revealed a 390 kb duplication at 2p11.2; 46,XX,t(8;10)(p23.3;q23.2)mat.arr[hg 19] 2p11.2(85469151x2,85474356-85864257x3,85868355x2). This duplication region was confirmed by real-time quantitative PCR and real-time reverse transcriptase quantitative PCR.

Conclusions: We suggest three positional candidate genes for intellectual disability and recurrent infection based upon gene function and data from real-time reverse transcriptase quantitative PCR-VAMP8 and RNF181 for intellectual disability and CAPG for recurrent infection.

Citing Articles

A cryptic microdeletion del(12)(p11.21p11.23) within an unbalanced translocation t(7;12)(q21.13;q23.1) implicates new candidate loci for intellectual disability and Kallmann syndrome.

Ben-Mahmoud A, Kishikawa S, Gupta V, Leach N, Shen Y, Moldovan O Sci Rep. 2023; 13(1):12984.

PMID: 37563198 PMC: 10415337. DOI: 10.1038/s41598-023-40037-4.

Copy number variations on chromosome 2: impact on human phenotype, a cross-sectional study.

Sousa B, Grangeia A, Pinto J, Santos H, Doria S Porto Biomed J. 2023; 8(1):e198.

PMID: 37213247 PMC: 10194716. DOI: 10.1097/j.pbj.0000000000000198.

A microdeletion del(12)(p11.21p11.23) with a cryptic unbalanced translocation t(7;12)(q21.13;q23.1) implicates new candidate loci for intellectual disability and Kallmann syndrome.

Ben-Mahmoud A, Kishikawa S, Gupta V, Leach N, Shen Y, Moldovan O Res Sq. 2023; .

PMID: 37034680 PMC: 10081357. DOI: 10.21203/rs.3.rs-2572736/v1.

Comparative Genomic Mapping Implicates LRRK2 for Intellectual Disability and Autism at 12q12, and HDHD1, as Well as PNPLA4, for X-Linked Intellectual Disability at Xp22.31.

Labonne J, Driessen T, Harris M, Kong I, Brakta S, Theisen J J Clin Med. 2020; 9(1).

PMID: 31963867 PMC: 7019335. DOI: 10.3390/jcm9010274.

Comparative deletion mapping at 1p31.3-p32.2 implies NFIA responsible for intellectual disability coupled with macrocephaly and the presence of several other genes for syndromic intellectual disability.

Labonne J, Shen Y, Kong I, Diamond M, Layman L, Kim H Mol Cytogenet. 2016; 9:24.

PMID: 26997977 PMC: 4797196. DOI: 10.1186/s13039-016-0234-z.

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