Genetic and clinical characterization of 73 Pigmentary Mosaicism patients: revealing the genetic basis of clinical manifestations

BACKGROUND: Pigmentary mosaicism constitutes a heterogeneous group of skin pigmentation alterations associated with multisystem involvement. The aim of this study was to establish a complete cytogenetic and molecular characterization of PM patients, emphasizing on searching for possible low chromoso...

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Autores principales: Salas-Labadía, C., Gómez-Carmona, S., Cruz-Alcívar, R., Martínez-Anaya, D., Del Castillo-Ruiz, V., Durán-McKinster, C., Ulloa-Avilés, V., Yokoyama-Rebollar, E., Ruiz-Herrera, A., Navarrete-Meneses, P., Lieberman-Hernández, E., González-Del Angel, A., Cervantes-Barragán, D., Villarroel-Cortés, C., Reyes-León, A., Suárez-Pérez, D., Pedraza-Meléndez, A., González-Orsuna, A., Pérez-Vera, P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2019
Materias:
Research
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6858688/
https://www.ncbi.nlm.nih.gov/pubmed/31730496
http://dx.doi.org/10.1186/s13023-019-1208-0
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author Salas-Labadía, C.
Gómez-Carmona, S.
Cruz-Alcívar, R.
Martínez-Anaya, D.
Del Castillo-Ruiz, V.
Durán-McKinster, C.
Ulloa-Avilés, V.
Yokoyama-Rebollar, E.
Ruiz-Herrera, A.
Navarrete-Meneses, P.
Lieberman-Hernández, E.
González-Del Angel, A.
Cervantes-Barragán, D.
Villarroel-Cortés, C.
Reyes-León, A.
Suárez-Pérez, D.
Pedraza-Meléndez, A.
González-Orsuna, A.
Pérez-Vera, P.
author_facet Salas-Labadía, C.
Gómez-Carmona, S.
Cruz-Alcívar, R.
Martínez-Anaya, D.
Del Castillo-Ruiz, V.
Durán-McKinster, C.
Ulloa-Avilés, V.
Yokoyama-Rebollar, E.
Ruiz-Herrera, A.
Navarrete-Meneses, P.
Lieberman-Hernández, E.
González-Del Angel, A.
Cervantes-Barragán, D.
Villarroel-Cortés, C.
Reyes-León, A.
Suárez-Pérez, D.
Pedraza-Meléndez, A.
González-Orsuna, A.
Pérez-Vera, P.
author_sort Salas-Labadía, C.
collection PubMed
description BACKGROUND: Pigmentary mosaicism constitutes a heterogeneous group of skin pigmentation alterations associated with multisystem involvement. The aim of this study was to establish a complete cytogenetic and molecular characterization of PM patients, emphasizing on searching for possible low chromosomal mosaicism and on establishing an accurate genotype-phenotype correlation. RESULTS: A total of 73 patients were included (3 months to 18 years of age), 52% male and 48% female. Observed in 69 (95%) patients, the most frequent pattern of pigmentation was fine and whorled BL, which was associated with disseminated skin extent in 41 (59%) patients. Central nervous system (84%) alterations were the most frequent observed in the group of patients, followed by the musculoskeletal (53%) and ophthalmologic (27%) alterations. Considering the pattern of pigmentation, no significant differences in association with skin extent or extracutaneous manifestations were detected. Following a strict cytogenetic analysis strategy, screening metaphases from three different tissues (peripheral blood, hyperpigmented and hypopigmented skin) we found that 23/73 patients had chromosomal abnormalities classified as follows: 1) Mosaic with 2 or more different cell lines with structural alterations n = 19; 2) Polyploidy (mosaic) n = 1 and 3) Alterations in all cells in three different tissues n = 3. SNP array, array CGH and FISH were useful for the complete characterization of the chromosomal aberrations, for the detection of microdeletions in patients with normal karyotype but with strong clinical suspicious of chromosomal alteration, and for a better establishment of genotype-phenotype correlation. In 2 patients we found genes associated with some of the extracutaneous manifestations (SHH, MNX1, PPP2R2C). CONCLUSIONS: This group of 73 patients finely described is the largest series of patients with pigmentary mosaicism reported worldwide. As we showed in this study, the followed analysis strategy allowed the detection of cytogenetic and molecular abnormalities, and made possible the establishment of genotype-phenotype associations in some patients. An important limitation of our study was the analysis of fibroblasts cultures instead of melanocytes and keratinocytes. In some cases the direct molecular DNA analysis of skin biopsy could be another choice.
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spelling pubmed-68586882019-11-29 Genetic and clinical characterization of 73 Pigmentary Mosaicism patients: revealing the genetic basis of clinical manifestations Salas-Labadía, C. Gómez-Carmona, S. Cruz-Alcívar, R. Martínez-Anaya, D. Del Castillo-Ruiz, V. Durán-McKinster, C. Ulloa-Avilés, V. Yokoyama-Rebollar, E. Ruiz-Herrera, A. Navarrete-Meneses, P. Lieberman-Hernández, E. González-Del Angel, A. Cervantes-Barragán, D. Villarroel-Cortés, C. Reyes-León, A. Suárez-Pérez, D. Pedraza-Meléndez, A. González-Orsuna, A. Pérez-Vera, P. Orphanet J Rare Dis Research BACKGROUND: Pigmentary mosaicism constitutes a heterogeneous group of skin pigmentation alterations associated with multisystem involvement. The aim of this study was to establish a complete cytogenetic and molecular characterization of PM patients, emphasizing on searching for possible low chromosomal mosaicism and on establishing an accurate genotype-phenotype correlation. RESULTS: A total of 73 patients were included (3 months to 18 years of age), 52% male and 48% female. Observed in 69 (95%) patients, the most frequent pattern of pigmentation was fine and whorled BL, which was associated with disseminated skin extent in 41 (59%) patients. Central nervous system (84%) alterations were the most frequent observed in the group of patients, followed by the musculoskeletal (53%) and ophthalmologic (27%) alterations. Considering the pattern of pigmentation, no significant differences in association with skin extent or extracutaneous manifestations were detected. Following a strict cytogenetic analysis strategy, screening metaphases from three different tissues (peripheral blood, hyperpigmented and hypopigmented skin) we found that 23/73 patients had chromosomal abnormalities classified as follows: 1) Mosaic with 2 or more different cell lines with structural alterations n = 19; 2) Polyploidy (mosaic) n = 1 and 3) Alterations in all cells in three different tissues n = 3. SNP array, array CGH and FISH were useful for the complete characterization of the chromosomal aberrations, for the detection of microdeletions in patients with normal karyotype but with strong clinical suspicious of chromosomal alteration, and for a better establishment of genotype-phenotype correlation. In 2 patients we found genes associated with some of the extracutaneous manifestations (SHH, MNX1, PPP2R2C). CONCLUSIONS: This group of 73 patients finely described is the largest series of patients with pigmentary mosaicism reported worldwide. As we showed in this study, the followed analysis strategy allowed the detection of cytogenetic and molecular abnormalities, and made possible the establishment of genotype-phenotype associations in some patients. An important limitation of our study was the analysis of fibroblasts cultures instead of melanocytes and keratinocytes. In some cases the direct molecular DNA analysis of skin biopsy could be another choice. BioMed Central 2019-11-15 /pmc/articles/PMC6858688/ /pubmed/31730496 http://dx.doi.org/10.1186/s13023-019-1208-0 Text en © The Author(s). 2019 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research
Salas-Labadía, C.
Gómez-Carmona, S.
Cruz-Alcívar, R.
Martínez-Anaya, D.
Del Castillo-Ruiz, V.
Durán-McKinster, C.
Ulloa-Avilés, V.
Yokoyama-Rebollar, E.
Ruiz-Herrera, A.
Navarrete-Meneses, P.
Lieberman-Hernández, E.
González-Del Angel, A.
Cervantes-Barragán, D.
Villarroel-Cortés, C.
Reyes-León, A.
Suárez-Pérez, D.
Pedraza-Meléndez, A.
González-Orsuna, A.
Pérez-Vera, P.
Genetic and clinical characterization of 73 Pigmentary Mosaicism patients: revealing the genetic basis of clinical manifestations
title Genetic and clinical characterization of 73 Pigmentary Mosaicism patients: revealing the genetic basis of clinical manifestations
title_full Genetic and clinical characterization of 73 Pigmentary Mosaicism patients: revealing the genetic basis of clinical manifestations
title_fullStr Genetic and clinical characterization of 73 Pigmentary Mosaicism patients: revealing the genetic basis of clinical manifestations
title_full_unstemmed Genetic and clinical characterization of 73 Pigmentary Mosaicism patients: revealing the genetic basis of clinical manifestations
title_short Genetic and clinical characterization of 73 Pigmentary Mosaicism patients: revealing the genetic basis of clinical manifestations
title_sort genetic and clinical characterization of 73 pigmentary mosaicism patients: revealing the genetic basis of clinical manifestations
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6858688/
https://www.ncbi.nlm.nih.gov/pubmed/31730496
http://dx.doi.org/10.1186/s13023-019-1208-0
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