Molecular characterization of HDAC8 deletions in individuals with atypical Cornelia de Lange syndrome

Maria Helgeson; Jennifer Keller-Ramey; Amy Knight Johnson; Jennifer A. Lee; Daniel B. Magner; Brett Deml; Jacea Deml; Ying Ying Hu; Zejuan Li; Kirsten Donato; Soma Das; Rachel Laframboise; Sandra Tremblay; Ian Krantz; Sarah Noon; George Hoganson; Jennifer Burton; Christian P. Schaaf; Daniela Del Gaudio

doi:10.1038/s10038-017-0387-6

Molecular characterization of HDAC8 deletions in individuals with atypical Cornelia de Lange syndrome

Maria Helgeson, Jennifer Keller-Ramey, Amy Knight Johnson, Jennifer A. Lee, Daniel B. Magner, Brett Deml, Jacea Deml, Ying Ying Hu, Zejuan Li, Kirsten Donato, Soma Das, Rachel Laframboise, Sandra Tremblay, Ian Krantz, Sarah Noon, George Hoganson, Jennifer Burton, Christian P. Schaaf, Daniela Del Gaudio

Research output: Contribution to journal › Article › peer-review

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Abstract

Cornelia de Lange syndrome (CdLS) is a rare neurodevelopmental syndrome for which mutations in five causative genes that encode (SMC1A, SMC3, RAD21) or regulate (NIPBL, HDAC8) the cohesin complex, account for ~70% of cases. Herein we report on four female Subjects who were found to carry novel intragenic deletions in HDAC8. In one case, the deletion was found in mosaic state and it was determined to be present in ~38% of blood lymphocytes and in nearly all cells of a buccal sample. All deletions, for which parental blood samples were available, were shown to have arisen de novo. X-chromosome inactivation studies demonstrated marked skewing, suggesting strong selection against the mutated HDAC8 allele. Based on an investigation of the deletion breakpoints, we hypothesize that microhomology-mediated replicative mechanisms may be implicated in the formation of some of these rearrangements. This study broadens the mutational spectrum of HDAC8, provides the first description of a causative HDAC8 somatic mutation and increases the knowledge on possible mutational mechanisms underlying copy number variations in HDAC8. Moreover our findings highlight the clinical utility of considering copy number analysis in HDAC8 as well as the analysis on DNA from more than one tissue as an indispensable part of the routine molecular diagnosis of individuals with CdLS or CdLS-overlapping features.

Original language	English (US)
Pages (from-to)	349-356
Number of pages	8
Journal	Journal of Human Genetics
Volume	63
Issue number	3
DOIs	https://doi.org/10.1038/s10038-017-0387-6
State	Published - Mar 1 2018

ASJC Scopus subject areas

Genetics
Genetics(clinical)

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Helgeson, M., Keller-Ramey, J., Knight Johnson, A., Lee, J. A., Magner, D. B., Deml, B., Deml, J., Hu, Y. Y., Li, Z., Donato, K., Das, S., Laframboise, R., Tremblay, S., Krantz, I., Noon, S., Hoganson, G., Burton, J., Schaaf, C. P., & Del Gaudio, D. (2018). Molecular characterization of HDAC8 deletions in individuals with atypical Cornelia de Lange syndrome. Journal of Human Genetics, 63(3), 349-356. https://doi.org/10.1038/s10038-017-0387-6

Helgeson, M, Keller-Ramey, J, Knight Johnson, A, Lee, JA, Magner, DB, Deml, B, Deml, J, Hu, YY, Li, Z, Donato, K, Das, S, Laframboise, R, Tremblay, S, Krantz, I, Noon, S, Hoganson, G, Burton, J, Schaaf, CP & Del Gaudio, D 2018, 'Molecular characterization of HDAC8 deletions in individuals with atypical Cornelia de Lange syndrome', Journal of Human Genetics, vol. 63, no. 3, pp. 349-356. https://doi.org/10.1038/s10038-017-0387-6

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title = "Molecular characterization of HDAC8 deletions in individuals with atypical Cornelia de Lange syndrome",

abstract = "Cornelia de Lange syndrome (CdLS) is a rare neurodevelopmental syndrome for which mutations in five causative genes that encode (SMC1A, SMC3, RAD21) or regulate (NIPBL, HDAC8) the cohesin complex, account for ~70% of cases. Herein we report on four female Subjects who were found to carry novel intragenic deletions in HDAC8. In one case, the deletion was found in mosaic state and it was determined to be present in ~38% of blood lymphocytes and in nearly all cells of a buccal sample. All deletions, for which parental blood samples were available, were shown to have arisen de novo. X-chromosome inactivation studies demonstrated marked skewing, suggesting strong selection against the mutated HDAC8 allele. Based on an investigation of the deletion breakpoints, we hypothesize that microhomology-mediated replicative mechanisms may be implicated in the formation of some of these rearrangements. This study broadens the mutational spectrum of HDAC8, provides the first description of a causative HDAC8 somatic mutation and increases the knowledge on possible mutational mechanisms underlying copy number variations in HDAC8. Moreover our findings highlight the clinical utility of considering copy number analysis in HDAC8 as well as the analysis on DNA from more than one tissue as an indispensable part of the routine molecular diagnosis of individuals with CdLS or CdLS-overlapping features.",

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AU - Helgeson, Maria

AU - Keller-Ramey, Jennifer

AU - Knight Johnson, Amy

AU - Lee, Jennifer A.

AU - Magner, Daniel B.

AU - Deml, Brett

AU - Deml, Jacea

AU - Hu, Ying Ying

AU - Li, Zejuan

AU - Donato, Kirsten

AU - Das, Soma

AU - Laframboise, Rachel

AU - Tremblay, Sandra

AU - Krantz, Ian

AU - Noon, Sarah

AU - Hoganson, George

AU - Burton, Jennifer

AU - Schaaf, Christian P.

AU - Del Gaudio, Daniela

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N2 - Cornelia de Lange syndrome (CdLS) is a rare neurodevelopmental syndrome for which mutations in five causative genes that encode (SMC1A, SMC3, RAD21) or regulate (NIPBL, HDAC8) the cohesin complex, account for ~70% of cases. Herein we report on four female Subjects who were found to carry novel intragenic deletions in HDAC8. In one case, the deletion was found in mosaic state and it was determined to be present in ~38% of blood lymphocytes and in nearly all cells of a buccal sample. All deletions, for which parental blood samples were available, were shown to have arisen de novo. X-chromosome inactivation studies demonstrated marked skewing, suggesting strong selection against the mutated HDAC8 allele. Based on an investigation of the deletion breakpoints, we hypothesize that microhomology-mediated replicative mechanisms may be implicated in the formation of some of these rearrangements. This study broadens the mutational spectrum of HDAC8, provides the first description of a causative HDAC8 somatic mutation and increases the knowledge on possible mutational mechanisms underlying copy number variations in HDAC8. Moreover our findings highlight the clinical utility of considering copy number analysis in HDAC8 as well as the analysis on DNA from more than one tissue as an indispensable part of the routine molecular diagnosis of individuals with CdLS or CdLS-overlapping features.

AB - Cornelia de Lange syndrome (CdLS) is a rare neurodevelopmental syndrome for which mutations in five causative genes that encode (SMC1A, SMC3, RAD21) or regulate (NIPBL, HDAC8) the cohesin complex, account for ~70% of cases. Herein we report on four female Subjects who were found to carry novel intragenic deletions in HDAC8. In one case, the deletion was found in mosaic state and it was determined to be present in ~38% of blood lymphocytes and in nearly all cells of a buccal sample. All deletions, for which parental blood samples were available, were shown to have arisen de novo. X-chromosome inactivation studies demonstrated marked skewing, suggesting strong selection against the mutated HDAC8 allele. Based on an investigation of the deletion breakpoints, we hypothesize that microhomology-mediated replicative mechanisms may be implicated in the formation of some of these rearrangements. This study broadens the mutational spectrum of HDAC8, provides the first description of a causative HDAC8 somatic mutation and increases the knowledge on possible mutational mechanisms underlying copy number variations in HDAC8. Moreover our findings highlight the clinical utility of considering copy number analysis in HDAC8 as well as the analysis on DNA from more than one tissue as an indispensable part of the routine molecular diagnosis of individuals with CdLS or CdLS-overlapping features.

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Molecular characterization of HDAC8 deletions in individuals with atypical Cornelia de Lange syndrome

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