A familial chromosomal complex rearrangement confirms RUNX1T1 as a causative gene for intellectual disability and suggests that 1p22.1p21.3 duplication is likely benign

Fabrizia Restaldi; Viola Alesi; Angela Aquilani; Silvia Genovese; Serena Russo; Valentina Coletti; Daniele Pompili; Roberto Falasca; Bruno Dallapiccola; Rossella Capolino; Matteo Luciani; Antonio Novelli

doi:10.1186/s13039-019-0440-6

Molecular Cytogenetics (Jun 2019)

A familial chromosomal complex rearrangement confirms RUNX1T1 as a causative gene for intellectual disability and suggests that 1p22.1p21.3 duplication is likely benign

Fabrizia Restaldi,
Viola Alesi,
Angela Aquilani,
Silvia Genovese,
Serena Russo,
Valentina Coletti,
Daniele Pompili,
Roberto Falasca,
Bruno Dallapiccola,
Rossella Capolino,
Matteo Luciani,
Antonio Novelli

Affiliations

Fabrizia Restaldi: Bambino Gesù Children’s Hospital
Viola Alesi: Bambino Gesù Children’s Hospital
Angela Aquilani: Bambino Gesù Children’s Hospital
Silvia Genovese: Bambino Gesù Children’s Hospital
Serena Russo: Bambino Gesù Children’s Hospital
Valentina Coletti: Bambino Gesù Children’s Hospital
Daniele Pompili: Bambino Gesù Children’s Hospital
Roberto Falasca: Bambino Gesù Children’s Hospital
Bruno Dallapiccola: Bambino Gesù Children’s Hospital
Rossella Capolino: Bambino Gesù Children’s Hospital
Matteo Luciani: Bambino Gesù Children’s Hospital
Antonio Novelli: Bambino Gesù Children’s Hospital

DOI: https://doi.org/10.1186/s13039-019-0440-6
Journal volume & issue: Vol. 12, no. 1
pp. 1 – 5

Abstract

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Abstract Background Complex chromosomal rearrangements are constitutive structural aberrations involving three or more breaks. They can be balanced or unbalanced and result in different outcomes, depending on deletion/duplication of genomic material, gene disruption, or position effects. Case presentation We report on a patient presenting with severe anemia, splenomegaly, mild intellectual disability and facial dysmorphisms harboring a 4.3 Mb duplication at 1p22.1p21.3 and a 2.1 Mb deletion at 8q21.3q22.1, involving RUNX1T1 gene. The healthy brother presented the same duplication of chromosome 1p as at 1p22.1p21.3. Conclusions The rearrangement found both these siblings resulted from malsegregation in the proband and recombination in her healthy brother of a balanced paternal complex chromosomal rearrangement. These results confirm RUNX1T1 as a causative gene for intellectual disability and suggest the 1p22.1p21.3 duplication is likely benign.

Published in Molecular Cytogenetics

ISSN: 1755-8166 (Online)
Publisher: BMC
Country of publisher: United Kingdom
LCC subjects: Science: Biology (General): Genetics
Website: https://molecularcytogenetics.biomedcentral.com/

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