FETAL TO ADULT HEMOGLOBIN SWITCH IN CULTURES OF EARLY ERYTHROID PRECURSORS FROM HUMAN FETUSES AND NEONATES

Erythroid burst colonies derived from the cord blood of nine neonates and from the blood and liver of three fetuses aborted after 20 weeks of gestation were grown in plasma clot culture. Their quantitative study revealed a higher proportion of burst‐forming units (BFU‐Es) in cord blood than in cord blood of normal adults. In addition, colony‐forming units (CFU‐Es) were present in cord blood but absent from adult blood. Study of haemoglobin synthesis in 14‐day cultures of cord blood BFU‐Es showed a significantly higher degree of Hb A synthesis than was found in reticulocytes from fresh cord blood; this proportion was, however, similar to that expected in vivo about three weeks after birth. These data suggest that the hemoglobin switch is already programmed in most of the early erythroid precursors present in cord blood of full‐term neonates and indicate that the differentiation time is probably of the same order of magnitude in vivo and in vitro. The proportion of Hb A and F synthesis in erythroid bursts was not influenced by the concentration of erythropoietin in the range studied – ie, from 0.5 to 12 international units. Low but identical proportions of Hb A synthesis were found both in erythroid cells from liver after two hours of incubation with [3H]‐leucine, and in 14‐day liver bursts from fetuses aborted at 20 weeks of gestation. Copyright © 1979 Wiley‐Liss, Inc., A Wiley Company