Deletions and microdeletions of 22q11.2 in velo-cardio-facial syndrome

D. A. Driscoll; N. B. Spinner; M. L. Budarf; D. M. McDonald-McGinn; E. H. Zackai; R. B. Goldberg; R. J. Shprintzen; H. M. Saal; J. Zonana; M. C. Jones; J. T. Mascarello; B. S. Emanuel

doi:10.1002/ajmg.1320440237

Deletions and microdeletions of 22q11.2 in velo-cardio-facial syndrome

D. A. Driscoll, N. B. Spinner, M. L. Budarf, D. M. McDonald-McGinn, E. H. Zackai, R. B. Goldberg, R. J. Shprintzen, H. M. Saal, J. Zonana, M. C. Jones, J. T. Mascarello, B. S. Emanuel

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349 Scopus citations

Abstract

Velo-cardio-facial syndrome (VCFS), an autosomal dominant disorder, is characterized by cleft palate, cardiac defects, learning disabilities and a typical facial appearance. Less frequently, VCFS patients have manifestations of the DiGeorge complex (DGC) including hypocalcemia, hypoplastic or absent lymphoid tissue and T-cell deficiency suggesting that these 2 conditions share a common pathogenesis. Here, we report the results of cytogenetic and molecular studies of 15 VCFS patients. High - resolution banding techniques detected an interstitial deletion of 22q11.21-q11.23 in 3 patients. The remaining 12 patients had apparently normal chromosomes. Molecular analysis with probes from the DiGeorge Chromosome Region (DGCR) within 22q11 detected DNA deletions in 14 of 15 patients. In 2 families, deletions were detected in the affected parent as well as the propositus suggesting that the autosomal dominant transmission of VCFS is due to segregation of a deletion. Deletions of the same loci previously shown to be deleted in patients with DGC explains the overlapping phenotype of VCFS and the DGC and supports the hypothesis that the cause of these two disorders is the same.

Original language	English (US)
Pages (from-to)	261-268
Number of pages	8
Journal	American Journal of Medical Genetics
Volume	44
Issue number	2
DOIs	https://doi.org/10.1002/ajmg.1320440237
State	Published - 1992
Externally published	Yes

Keywords

22q11 microdeletions
chromosome 22q11 interstitial deletions
segmentally aneusomic disorder

ASJC Scopus subject areas

Genetics(clinical)

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10.1002/ajmg.1320440237

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Driscoll, D. A., Spinner, N. B., Budarf, M. L., McDonald-McGinn, D. M., Zackai, E. H., Goldberg, R. B., Shprintzen, R. J., Saal, H. M., Zonana, J., Jones, M. C., Mascarello, J. T., & Emanuel, B. S. (1992). Deletions and microdeletions of 22q11.2 in velo-cardio-facial syndrome. American Journal of Medical Genetics, 44(2), 261-268. https://doi.org/10.1002/ajmg.1320440237

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abstract = "Velo-cardio-facial syndrome (VCFS), an autosomal dominant disorder, is characterized by cleft palate, cardiac defects, learning disabilities and a typical facial appearance. Less frequently, VCFS patients have manifestations of the DiGeorge complex (DGC) including hypocalcemia, hypoplastic or absent lymphoid tissue and T-cell deficiency suggesting that these 2 conditions share a common pathogenesis. Here, we report the results of cytogenetic and molecular studies of 15 VCFS patients. High - resolution banding techniques detected an interstitial deletion of 22q11.21-q11.23 in 3 patients. The remaining 12 patients had apparently normal chromosomes. Molecular analysis with probes from the DiGeorge Chromosome Region (DGCR) within 22q11 detected DNA deletions in 14 of 15 patients. In 2 families, deletions were detected in the affected parent as well as the propositus suggesting that the autosomal dominant transmission of VCFS is due to segregation of a deletion. Deletions of the same loci previously shown to be deleted in patients with DGC explains the overlapping phenotype of VCFS and the DGC and supports the hypothesis that the cause of these two disorders is the same.",

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author = "Driscoll, {D. A.} and Spinner, {N. B.} and Budarf, {M. L.} and McDonald-McGinn, {D. M.} and Zackai, {E. H.} and Goldberg, {R. B.} and Shprintzen, {R. J.} and Saal, {H. M.} and J. Zonana and Jones, {M. C.} and Mascarello, {J. T.} and Emanuel, {B. S.}",

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AU - McDonald-McGinn, D. M.

AU - Zackai, E. H.

AU - Goldberg, R. B.

AU - Shprintzen, R. J.

AU - Saal, H. M.

AU - Zonana, J.

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AU - Mascarello, J. T.

AU - Emanuel, B. S.

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AB - Velo-cardio-facial syndrome (VCFS), an autosomal dominant disorder, is characterized by cleft palate, cardiac defects, learning disabilities and a typical facial appearance. Less frequently, VCFS patients have manifestations of the DiGeorge complex (DGC) including hypocalcemia, hypoplastic or absent lymphoid tissue and T-cell deficiency suggesting that these 2 conditions share a common pathogenesis. Here, we report the results of cytogenetic and molecular studies of 15 VCFS patients. High - resolution banding techniques detected an interstitial deletion of 22q11.21-q11.23 in 3 patients. The remaining 12 patients had apparently normal chromosomes. Molecular analysis with probes from the DiGeorge Chromosome Region (DGCR) within 22q11 detected DNA deletions in 14 of 15 patients. In 2 families, deletions were detected in the affected parent as well as the propositus suggesting that the autosomal dominant transmission of VCFS is due to segregation of a deletion. Deletions of the same loci previously shown to be deleted in patients with DGC explains the overlapping phenotype of VCFS and the DGC and supports the hypothesis that the cause of these two disorders is the same.

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Deletions and microdeletions of 22q11.2 in velo-cardio-facial syndrome

Abstract

Keywords

ASJC Scopus subject areas

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