Molecular definition of the 22q11 deletions in velo-cardio-facial syndrome

Bernice E. Morrow, R. Goldberg, C. Carlson, R. Das Gupta, H. Sirotkin, J. Collins, I. Dunham, H. O'Donnell, P. Scambler, R. Shprintzen, R. Kucherlapati

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Abstract

Velo-cardio-facial syndrome (VCFS) is a common genetic disorder among individuals with cleft palate and is associated with hemizygous deletions in human chromosome 22q11. Toward the molecular definition of the deletions, we constructed a physical map of 22q11 in the form of overlapping YACs. The physical map covers >9 cM of genetic distance, estimated to span 5 Mb of DNA, and contains a total of 64 markers. Eleven highly polymorphic short tandem- repeat polymorphic (STRP) markers were placed on the physical map, and 10 of these were unambiguously ordered. The 11 polymorphic markers were used to type the DNA from a total of 61 VCFS patients and 49 unaffected relatives. Comparison of levels of heterozygosity of these markers in VCFS patients and their unaffected relatives revealed that four of these markers are commonly hemizygous among VCFS patients. To confirm these results and to define further the breakpoints in VCFS patients, 15 VCFS individuals and their unaffected parents were genotyped for the 11 STRP markers. Haplotypes generated from this study revealed that 82% of the patients have deletions that can be defined by the STRP markers. The results revealed that all patients who have a deletion share a common proximal breakpoint, while there are two distinct distal breakpoints. Markers D22S941 and D22S944 appear to be consistently hemizygous in patients with deletions. Both of these markers are located on a single nonchimeric YAC that is 400 kb long. The results also show that the parental origin of the deleted chromosome does not have any effect on the phenotypic manifestation.

Original languageEnglish (US)
Pages (from-to)1391-1403
Number of pages13
JournalAmerican Journal of Human Genetics
Volume56
Issue number6
StatePublished - 1995

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DiGeorge Syndrome
Microsatellite Repeats
Inborn Genetic Diseases
DNA
Cleft Palate
Human Chromosomes
Haplotypes
Chromosomes
Parents

ASJC Scopus subject areas

  • Genetics

Cite this

Morrow, B. E., Goldberg, R., Carlson, C., Das Gupta, R., Sirotkin, H., Collins, J., ... Kucherlapati, R. (1995). Molecular definition of the 22q11 deletions in velo-cardio-facial syndrome. American Journal of Human Genetics, 56(6), 1391-1403.

Molecular definition of the 22q11 deletions in velo-cardio-facial syndrome. / Morrow, Bernice E.; Goldberg, R.; Carlson, C.; Das Gupta, R.; Sirotkin, H.; Collins, J.; Dunham, I.; O'Donnell, H.; Scambler, P.; Shprintzen, R.; Kucherlapati, R.

In: American Journal of Human Genetics, Vol. 56, No. 6, 1995, p. 1391-1403.

Research output: Contribution to journalArticle

Morrow, BE, Goldberg, R, Carlson, C, Das Gupta, R, Sirotkin, H, Collins, J, Dunham, I, O'Donnell, H, Scambler, P, Shprintzen, R & Kucherlapati, R 1995, 'Molecular definition of the 22q11 deletions in velo-cardio-facial syndrome', American Journal of Human Genetics, vol. 56, no. 6, pp. 1391-1403.
Morrow BE, Goldberg R, Carlson C, Das Gupta R, Sirotkin H, Collins J et al. Molecular definition of the 22q11 deletions in velo-cardio-facial syndrome. American Journal of Human Genetics. 1995;56(6):1391-1403.
Morrow, Bernice E. ; Goldberg, R. ; Carlson, C. ; Das Gupta, R. ; Sirotkin, H. ; Collins, J. ; Dunham, I. ; O'Donnell, H. ; Scambler, P. ; Shprintzen, R. ; Kucherlapati, R. / Molecular definition of the 22q11 deletions in velo-cardio-facial syndrome. In: American Journal of Human Genetics. 1995 ; Vol. 56, No. 6. pp. 1391-1403.
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abstract = "Velo-cardio-facial syndrome (VCFS) is a common genetic disorder among individuals with cleft palate and is associated with hemizygous deletions in human chromosome 22q11. Toward the molecular definition of the deletions, we constructed a physical map of 22q11 in the form of overlapping YACs. The physical map covers >9 cM of genetic distance, estimated to span 5 Mb of DNA, and contains a total of 64 markers. Eleven highly polymorphic short tandem- repeat polymorphic (STRP) markers were placed on the physical map, and 10 of these were unambiguously ordered. The 11 polymorphic markers were used to type the DNA from a total of 61 VCFS patients and 49 unaffected relatives. Comparison of levels of heterozygosity of these markers in VCFS patients and their unaffected relatives revealed that four of these markers are commonly hemizygous among VCFS patients. To confirm these results and to define further the breakpoints in VCFS patients, 15 VCFS individuals and their unaffected parents were genotyped for the 11 STRP markers. Haplotypes generated from this study revealed that 82{\%} of the patients have deletions that can be defined by the STRP markers. The results revealed that all patients who have a deletion share a common proximal breakpoint, while there are two distinct distal breakpoints. Markers D22S941 and D22S944 appear to be consistently hemizygous in patients with deletions. Both of these markers are located on a single nonchimeric YAC that is 400 kb long. The results also show that the parental origin of the deleted chromosome does not have any effect on the phenotypic manifestation.",
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AU - Collins, J.

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