TY - JOUR
T1 - Clinical and genomic characterization of distal duplications and deletions of chromosome 4q
T2 - Study of two cases and review of the literature
AU - Rossi, Michael R.
AU - DiMaio, Miriam S.
AU - Xiang, Bixia
AU - Lu, Kangmo
AU - Kaymakcalan, Hande
AU - Seashore, Margretta
AU - Mahoney, Maurice J.
AU - Li, Peining
PY - 2009/12
Y1 - 2009/12
N2 - Variable clinical presentations of patients with chromosomally detected deletions in the distal long arm (q) of chromosome 4 have been reported. The lack ofmolecular characterization of the deletion sizes and deleted genes hinders further genotype-phenotype correlation. Using a validated oligonucleotide array comparative genomic hybridization (oaCGH) analysis, we examined two patients with apparent chromosomal deletions in the distal 4q region. In the first, oaCGH identified a 2.441 megabase (Mb) duplication and a 12.651Mb deletion at 4q34.1 in a pregnant female who transmitted this aberration to her son. This mother has only learning disabilities while her son had both renal and cardiac anomalies in the newborn period. Unrecognized paternal genetic factors may contribute to the variable expression. The second patient is a 17-year-old female with a history of Pierre Robin sequence, cardiac abnormalities and learning disabilities. She was diagnosed prenatally with a de novo 4q deletion, and oaCGH defined a 16.435Mb deletion of 4q34.1-4q35.2. Phenotypic comparisonand subtractive genomic mapping between these two cases suggested a 4Mb region possibly harboring a candidate gene for Pierre Robin sequence. Our cases and review of reported cases with genomic findings indicated the presence of familial variants with variable expressivity as well as de novo or inherited pathogenic simple deletion, duplication and complex deletion and duplication in the distal 4q region.
AB - Variable clinical presentations of patients with chromosomally detected deletions in the distal long arm (q) of chromosome 4 have been reported. The lack ofmolecular characterization of the deletion sizes and deleted genes hinders further genotype-phenotype correlation. Using a validated oligonucleotide array comparative genomic hybridization (oaCGH) analysis, we examined two patients with apparent chromosomal deletions in the distal 4q region. In the first, oaCGH identified a 2.441 megabase (Mb) duplication and a 12.651Mb deletion at 4q34.1 in a pregnant female who transmitted this aberration to her son. This mother has only learning disabilities while her son had both renal and cardiac anomalies in the newborn period. Unrecognized paternal genetic factors may contribute to the variable expression. The second patient is a 17-year-old female with a history of Pierre Robin sequence, cardiac abnormalities and learning disabilities. She was diagnosed prenatally with a de novo 4q deletion, and oaCGH defined a 16.435Mb deletion of 4q34.1-4q35.2. Phenotypic comparisonand subtractive genomic mapping between these two cases suggested a 4Mb region possibly harboring a candidate gene for Pierre Robin sequence. Our cases and review of reported cases with genomic findings indicated the presence of familial variants with variable expressivity as well as de novo or inherited pathogenic simple deletion, duplication and complex deletion and duplication in the distal 4q region.
KW - 4q distal duplications and deletions
KW - Array comparative genomic hybridization
KW - Pierre Robin sequence
UR - http://www.scopus.com/inward/record.url?scp=71949122225&partnerID=8YFLogxK
U2 - 10.1002/ajmg.a.33088
DO - 10.1002/ajmg.a.33088
M3 - Article
C2 - 19921640
AN - SCOPUS:71949122225
SN - 1552-4825
VL - 149
SP - 2788
EP - 2794
JO - American Journal of Medical Genetics, Part A
JF - American Journal of Medical Genetics, Part A
IS - 12
ER -