Microduplications of 22q11.2 are frequently inherited and are associated with variable phenotypes

Ou, Zhishuo; Berg, Jonathan S.; Yonath, Hagith; Enciso, Victoria B.; Miller, David T.; Picker, Jonathan; Lenzi, Tiffanee; Keegan, Catherine E.; Sutton, V. Reid; Belmont, John W.; Chinault, A. Craig; Lupski, James R.; Cheung, Sau Wai; Roeder, Elizabeth; Patel, Ankita

doi:10.1097/gim.0b013e31816b64c2

Cited by 170 publications

(188 citation statements)

References 54 publications

(55 reference statements)

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“…However, caution should be taken not to automatically regard an inherited CNV as benign [Buysse et al, 2009]. There are numerous reports of inherited pathogenic deletions/duplications that display reduced penetrance and/or variable expression [Cooper et al, 2011;Fernandez et al, 2009;Kaminsky et al, 2011;Ou et al, 2008]. In addition, a deletion inherited from an apparently normal parent may in fact reveal a recessive disorder in the proband due to a mutation on the remaining allele that is not detectable by the array.…”

Section: Inheritance Status/familial Studiesmentioning

confidence: 99%

Genome-wide arrays: Quality criteria and platforms to be used in routine diagnostics

et al. 2012

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Whole-genome analysis using genome-wide arrays, also called "genomic arrays," "microarrays," or "arrays," has become the first-tier diagnostic test for patients with developmental abnormalities and/or intellectual disabilities. In addition to constitutional anomalies, genomic arrays are also used to diagnose acquired disorders. Despite the rapid implementation of these technologies in diagnostic laboratories, external quality control schemes (such as CEQA, EMQN, UK NEQAS, and the USA QA scheme CAP) and interlaboratory comparisons show that there are huge differences in quality, interpretation, and reporting among laboratories. We offer guidance to laboratories to help assure the quality of array experiments and to standardize minimum detection resolution, and we also provide guidelines to standardize interpretation and reporting.

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Section: Inheritance Status/familial Studiesmentioning

confidence: 99%

Genome-wide arrays: Quality criteria and platforms to be used in routine diagnostics

et al. 2012

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“…In theory, these events should occur with equal frequency. However, reports of the 22q11.2 duplication syndrome have been quite rare in comparison with the del22q11 syndrome [4][5][6] .…”

Section: Tof -Tetralogy Of Fallot; Lhh -Left Heart Hypoplasia; Tga -Tmentioning

confidence: 99%

“…With an estimated prevalence of 1:2,000-6,000 live births, this syndrome currently represents one of the main known causes of congenital cardiopathy 1 . It is known that the region q11.2 of chromosome 22 presents a non-usual rearrangement, with regions of low-copy number repeats which, during meiosis, predispose to a pairing error between the chromosomes and, consequently, to an unequal crossing-over, which can lead to a deletion (del22q11) or a duplication of the q11.2 rgion [2][3][4] . The latter condition was recently identified and has been characterized by an extremely variable phenotypic spectrum, which includes the presence, among many abnormalities, of congenital cardiac defects [4][5][6] .…”

Section: Introductionmentioning

confidence: 99%

“…It is known that the region q11.2 of chromosome 22 presents a non-usual rearrangement, with regions of low-copy number repeats which, during meiosis, predispose to a pairing error between the chromosomes and, consequently, to an unequal crossing-over, which can lead to a deletion (del22q11) or a duplication of the q11.2 rgion [2][3][4] . The latter condition was recently identified and has been characterized by an extremely variable phenotypic spectrum, which includes the presence, among many abnormalities, of congenital cardiac defects [4][5][6] . However, the actual frequency of these malformations is still unknown in individuals with the 22q11.2 duplication, as well as the frequency of this duplication in patients with congenital cardiopathy 3 …”

Section: Introductionmentioning

confidence: 99%

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Duplicação 22q11.2 e defeitos cardíacos congênitos

Rosa¹,

Zen²,

Ricachinevsky³

et al. 2009

Arq. Bras. Cardiol.

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“…Microduplication syndromes show a highly variable penetrance between generations and they are often found to be inherited from an asymptomatic or very mildly affected parent. 19,20 If we exclude the known microduplication syndromes, still 7 of the 14 remaining clinically relevant gains with known segregation were inherited. None of these were located in a region that is known to be parentally imprinted.…”

Section: Do Not Exclude a Clinical Relevance For Gains Inherited Frommentioning

confidence: 99%

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

et al. 2011

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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 (Po0.001). Our study showed that a threshold of 200 kb is acceptable in a clinical setting, whereas heritability does not exclude a pathogenic nature of a gain. Evaluation of the guidelines in the second cohort of 300 patients revealed that the interpretation guidelines were clear, easy to follow and efficient.

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Microduplications of 22q11.2 are frequently inherited and are associated with variable phenotypes

Cited by 170 publications

References 54 publications

Genome-wide arrays: Quality criteria and platforms to be used in routine diagnostics

Genome-wide arrays: Quality criteria and platforms to be used in routine diagnostics

Duplicação 22q11.2 e defeitos cardíacos congênitos

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

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