Practical guidelines for interpreting copy number gains detected by high-resolution array in routine diagnostics

Nicolien M. Hanemaaijer; Birgit Sikkema-Raddatz; Gerben van der Vries; Trijnie Dijkhuizen; Roel Hordijk; Anthonie J. van Essen; Hermine E. Veenstra-Knol; Wilhelmina S. Kerstjens-Frederikse; Johanna C. Herkert; Erica H. Gerkes; Lamberta K. Leegte; Klaas Kok; Richard J. Sinke; Conny M. A. van Ravenswaaij-Arts

doi:10.1038/ejhg.2011.174

Practical guidelines for interpreting copy number gains detected by high-resolution array in routine diagnostics

Nicolien M. Hanemaaijer, Birgit Sikkema-Raddatz, Gerben van der Vries, Trijnie Dijkhuizen, Roel Hordijk, Anthonie J. van Essen, Hermine E. Veenstra-Knol, Wilhelmina S. Kerstjens-Frederikse, Johanna C. Herkert, Erica H. Gerkes, Lamberta K. Leegte, Klaas Kok, Richard J. Sinke, Conny M. A. van Ravenswaaij-Arts^*

^*Corresponding author voor dit werk

Onderzoeksoutput › Academic › peer review

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The correct interpretation of copy number gains in patients with developmental delay and multiple congenital anomalies is hampered by the large number of copy number variations (CNVs) encountered in healthy individuals. The variable phenotype associated with copy number gains makes interpretation even more difficult. Literature shows that inheritence, size and presence in healthy individuals are commonly used to decide whether a certain copy number gain is pathogenic, but no general consensus has been established. We aimed to develop guidelines for interpreting gains detected by array analysis using array CGH data of 300 patients analysed with the 105K Agilent oligo array in a diagnostic setting. We evaluated the guidelines in a second, independent, cohort of 300 patients. In the first 300 patients 797 gains of four or more adjacent oligonucleotides were observed. Of these, 45.4% were de novo and 54.6% were familial. In total, 94.8% of all de novo gains and 87.1% of all familial gains were concluded to be benign CNVs. Clinically relevant gains ranged from 288 to 7912 kb in size, and were significantly larger than benign gains and gains of unknown clinical relevance (P

Originele taal-2	English
Pagina's (van-tot)	161-165
Aantal pagina's	5
Tijdschrift	European Journal of Human Genetics
Volume	20
Nummer van het tijdschrift	2
DOI's	https://doi.org/10.1038/ejhg.2011.174
Status	Published - feb.-2012

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Hanemaaijer, N. M., Sikkema-Raddatz, B., van der Vries, G., Dijkhuizen, T., Hordijk, R., van Essen, A. J., Veenstra-Knol, H. E., Kerstjens-Frederikse, W. S., Herkert, J. C., Gerkes, E. H., Leegte, L. K., Kok, K., Sinke, R. J., & van Ravenswaaij-Arts, C. M. A. (2012). Practical guidelines for interpreting copy number gains detected by high-resolution array in routine diagnostics. European Journal of Human Genetics, 20(2), 161-165. https://doi.org/10.1038/ejhg.2011.174

@article{dfe3c79c558a4bbba55ecbfefe59c391,

title = "Practical guidelines for interpreting copy number gains detected by high-resolution array in routine diagnostics",

abstract = "The correct interpretation of copy number gains in patients with developmental delay and multiple congenital anomalies is hampered by the large number of copy number variations (CNVs) encountered in healthy individuals. The variable phenotype associated with copy number gains makes interpretation even more difficult. Literature shows that inheritence, size and presence in healthy individuals are commonly used to decide whether a certain copy number gain is pathogenic, but no general consensus has been established. We aimed to develop guidelines for interpreting gains detected by array analysis using array CGH data of 300 patients analysed with the 105K Agilent oligo array in a diagnostic setting. We evaluated the guidelines in a second, independent, cohort of 300 patients. In the first 300 patients 797 gains of four or more adjacent oligonucleotides were observed. Of these, 45.4% were de novo and 54.6% were familial. In total, 94.8% of all de novo gains and 87.1% of all familial gains were concluded to be benign CNVs. Clinically relevant gains ranged from 288 to 7912 kb in size, and were significantly larger than benign gains and gains of unknown clinical relevance (P",

keywords = "genome-wide array analysis, copy number gain, microduplication, guideline, MENTAL-RETARDATION, DEVELOPMENTAL DELAY, CLINICAL-PRACTICE, HUMAN GENOME, MICRODUPLICATIONS, ABNORMALITIES, DUPLICATION, CHALLENGES, PHENOTYPES, WORKFLOW",

author = "Hanemaaijer, {Nicolien M.} and Birgit Sikkema-Raddatz and {van der Vries}, Gerben and Trijnie Dijkhuizen and Roel Hordijk and {van Essen}, {Anthonie J.} and Veenstra-Knol, {Hermine E.} and Kerstjens-Frederikse, {Wilhelmina S.} and Herkert, {Johanna C.} and Gerkes, {Erica H.} and Leegte, {Lamberta K.} and Klaas Kok and Sinke, {Richard J.} and {van Ravenswaaij-Arts}, {Conny M. A.}",

year = "2012",

month = feb,

doi = "10.1038/ejhg.2011.174",

language = "English",

volume = "20",

pages = "161--165",

journal = "European Journal of Human Genetics",

issn = "1018-4813",

publisher = "Nature Publishing Group",

number = "2",

}

Hanemaaijer, NM, Sikkema-Raddatz, B , van der Vries, G , Dijkhuizen, T, Hordijk, R, van Essen, AJ, Veenstra-Knol, HE , Kerstjens-Frederikse, WS , Herkert, JC , Gerkes, EH, Leegte, LK, Kok, K, Sinke, RJ & van Ravenswaaij-Arts, CMA 2012, 'Practical guidelines for interpreting copy number gains detected by high-resolution array in routine diagnostics', European Journal of Human Genetics, vol. 20, nr. 2, blz. 161-165. https://doi.org/10.1038/ejhg.2011.174

TY - JOUR

T1 - Practical guidelines for interpreting copy number gains detected by high-resolution array in routine diagnostics

AU - Hanemaaijer, Nicolien M.

AU - Sikkema-Raddatz, Birgit

AU - van der Vries, Gerben

AU - Dijkhuizen, Trijnie

AU - Hordijk, Roel

AU - van Essen, Anthonie J.

AU - Veenstra-Knol, Hermine E.

AU - Kerstjens-Frederikse, Wilhelmina S.

AU - Herkert, Johanna C.

AU - Gerkes, Erica H.

AU - Leegte, Lamberta K.

AU - Kok, Klaas

AU - Sinke, Richard J.

AU - van Ravenswaaij-Arts, Conny M. A.

PY - 2012/2

Y1 - 2012/2

N2 - The correct interpretation of copy number gains in patients with developmental delay and multiple congenital anomalies is hampered by the large number of copy number variations (CNVs) encountered in healthy individuals. The variable phenotype associated with copy number gains makes interpretation even more difficult. Literature shows that inheritence, size and presence in healthy individuals are commonly used to decide whether a certain copy number gain is pathogenic, but no general consensus has been established. We aimed to develop guidelines for interpreting gains detected by array analysis using array CGH data of 300 patients analysed with the 105K Agilent oligo array in a diagnostic setting. We evaluated the guidelines in a second, independent, cohort of 300 patients. In the first 300 patients 797 gains of four or more adjacent oligonucleotides were observed. Of these, 45.4% were de novo and 54.6% were familial. In total, 94.8% of all de novo gains and 87.1% of all familial gains were concluded to be benign CNVs. Clinically relevant gains ranged from 288 to 7912 kb in size, and were significantly larger than benign gains and gains of unknown clinical relevance (P

AB - The correct interpretation of copy number gains in patients with developmental delay and multiple congenital anomalies is hampered by the large number of copy number variations (CNVs) encountered in healthy individuals. The variable phenotype associated with copy number gains makes interpretation even more difficult. Literature shows that inheritence, size and presence in healthy individuals are commonly used to decide whether a certain copy number gain is pathogenic, but no general consensus has been established. We aimed to develop guidelines for interpreting gains detected by array analysis using array CGH data of 300 patients analysed with the 105K Agilent oligo array in a diagnostic setting. We evaluated the guidelines in a second, independent, cohort of 300 patients. In the first 300 patients 797 gains of four or more adjacent oligonucleotides were observed. Of these, 45.4% were de novo and 54.6% were familial. In total, 94.8% of all de novo gains and 87.1% of all familial gains were concluded to be benign CNVs. Clinically relevant gains ranged from 288 to 7912 kb in size, and were significantly larger than benign gains and gains of unknown clinical relevance (P

KW - genome-wide array analysis

KW - copy number gain

KW - microduplication

KW - guideline

KW - MENTAL-RETARDATION

KW - DEVELOPMENTAL DELAY

KW - CLINICAL-PRACTICE

KW - HUMAN GENOME

KW - MICRODUPLICATIONS

KW - ABNORMALITIES

KW - DUPLICATION

KW - CHALLENGES

KW - PHENOTYPES

KW - WORKFLOW

U2 - 10.1038/ejhg.2011.174

DO - 10.1038/ejhg.2011.174

M3 - Article

SN - 1018-4813

VL - 20

SP - 161

EP - 165

JO - European Journal of Human Genetics

JF - European Journal of Human Genetics

IS - 2

ER -

Practical guidelines for interpreting copy number gains detected by high-resolution array in routine diagnostics

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