Postnatal Fetal and Adult Hemoglobin Synthesis in D1 Trisomy Syndrome

Author:

Bard Harry12

Affiliation:

1. Division of Perinatal Medicine, University of Colorado Medical Center, Denver, Colo., and the Neonatal Service, Hôpital Sainte-Justine, Department of Pediatrics, University of Montreal, Montreal, Canada.

2. University of Montreal, Montreal, Canada.

Abstract

Abstract Studies were carried out during the neonatal period in three infants with D1 trisomy syndrome to measure the proportion of fetal and adult hemoglobin being synthesized. These values were compared on the one hand to those previously reported from samples obtained from cord blood of normal newborn infants ranging from 25 to 43 wk gestation, and on the other hand to those values determined in critically ill infants of the same postconceptional age. Blood samples were incubated in an amino acid mixture containing 14C-leucine followed by column chromatography on DEAE Sephadex for separation of fetal and adult hemoglobin fractions. Liquid scintillation counting was carried out on the hemoglobin fractions. In infants with the D1 trisomy, the delay in transition to adult hemoglobin synthesis was 7-8 wk behind that expected for their postconceptional ages, and there was no accelerated transition to adult hemoglobin synthesis in the one case studied beyond the early neonatal period. Unlike the D1 trisomy infants, the critically ill controls showed no retardation in their transition toward adult hemoglobin synthesis. The duplication of the genes in one of the 13-15 chromosome groups is a factor that delays the developmental synchrony of hemoglobin synthesis.

Publisher

American Society of Hematology

Subject

Cell Biology,Hematology,Immunology,Biochemistry

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