Tetrasomy 3q26.32-q29 due to a supernumerary marker chromosome in a child with pigmentary mosaicism of Ito

Pigmentary mosaicism of Ito (PMI) is a skin abnormality often characterized by hypopigmentation of skin, following, in most cases, the Blaschko lines, usually associated with extracutaneous abnormalities, especially abnormalities of the central nervous system (CNS). It is suggested that this pattern...

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Published inGenetics and molecular biology Vol. 39; no. 1; pp. 35 - 39
Main Authors Cunha, Karina S, Simioni, Milena, Vieira, Tarsis P, Gil-da-Silva-Lopes, Vera L, Puzzi, Maria B, Steiner, Carlos E
Format Journal Article
LanguageEnglish
Portuguese
Published Brazil Sociedade Brasileira de Genética 01.03.2016
Subjects
array genomic hybridization
BIOCHEMISTRY & MOLECULAR BIOLOGY
GENETICS & HEREDITY
Human and Medical Genetics
Pigmentary mosaicism of Ito
supernumerary marker chromosome
tetrasomy
supernumerary marker chromosome
array genomic hybridization
tetrasomy
Pigmentary mosaicism of Ito
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Summary:Pigmentary mosaicism of Ito (PMI) is a skin abnormality often characterized by hypopigmentation of skin, following, in most cases, the Blaschko lines, usually associated with extracutaneous abnormalities, especially abnormalities of the central nervous system (CNS). It is suggested that this pattern arises from the presence and migration of two cell lineages in the ectoderm layer during the embryonic period and embryonic cell migration, with different gene expression profiles associated with pigmentation. Several types of chromosomal aberrations, with or without mosaicism, have been associated with this disorder. This study comprised clinical description and cytogenetic analysis of a child with PMI. The G-banded karyotype analysis revealed a supernumerary marker chromosome in 76% of the analyzed metaphases from peripheral blood lymphocytes. Array genomic hybridization analysis showed a copy number gain between 3q26.32-3q29, of approximately 20.5 Mb. Karyotype was defined as 47,XX,+mar[38]/46,XX[12].arr 3q26.32-3q29(177,682,859- 198,043,720)x4 dn. Genes mapped in the overlapping region among this patient and three other cases described prior to this study were listed and their possible involvement on PMI pathogenesis is discussed.
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ISSN:1415-4757
1678-4685
1415-4757
1678-4685
DOI:10.1590/1678-4685-GMB-2015-0033