1. Interstitial deletion of chromosome 1 [del(1)(q25q32)] in an infant with prune belly sequence
- Author
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Sara C. Finley, Wayne H. Finley, P R Scarbrough, R. William Quinlan, Andrew J. Carroll, and Beatrice Files
- Subjects
Male ,Pathology ,medicine.medical_specialty ,Microcephaly ,Clinodactyly ,Biology ,Pathogenesis ,Pregnancy ,Prune belly ,medicine ,Humans ,Prune Belly Syndrome ,Fetal Death ,Genetics (clinical) ,Sequence (medicine) ,medicine.diagnostic_test ,Cesarean Section ,Breakpoint ,Infant, Newborn ,Obstetrics and Gynecology ,Chromosome ,Anatomy ,medicine.disease ,Chromosomes, Human, Pair 1 ,Amniocentesis ,Female ,Chromosome Deletion ,medicine.symptom - Abstract
Relatively few cases of deletion 1q have been reported. These cases have been divided into three groups according to assigned breakpoints. They include proximal interstitial, intermediate interstitial, and terminal deletions. We present a male infant with an interstitial deletion of 1q with breakpoints determined by GTG banding as q25 and q32. Comparison with similar case reports suggests common physical features which include microcephaly, growth retardation, developmental delay, clinodactyly, and genital anomalies in affected males. However, no characteristic phenotypic appearance is definable. The infant also presented with prune belly sequence (PBS) with Potter facies. Fetal ascites, as noted in this case on prenatal ultrasound, appears to be an early factor in the pathogenesis of PBS. Therefore, detection of fetal ascites should suggest the presence of the PBS association and the need for more extensive prenatal evaluation.
- Published
- 1988
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