Expandability of haemopoietic progenitors in first trimester fetal and maternal blood: implications for non-invasive prenatal diagnosis

• Published in: Prenatal diagnosis Vol. 22; no. 6; pp. 463 - 469
• Main Authors: Campagnoli, Cesare, Roberts, Irene A. G., Kumar, Sailesh, Choolani, Mahesh, Bennett, Phillip R., Letsky, Elizabeth, Fisk, Nicholas M.
• Format: Journal Article
• Language: English
• Published: Chichester, UK John Wiley & Sons, Ltd 01.06.2002; Wiley
• Subjects: amplification; Antigens, CD34 - analysis; Biological and medical sciences; blood; Cell Count; Cell Division; Cells, Cultured; Coculture Techniques; Colony-Forming Units Assay; Erythroid Precursor Cells - cytology; Female; Fetal Blood - cytology; first trimester; Gynecology. Andrology. Obstetrics; Hematopoietic Stem Cells - cytology; Hematopoietic Stem Cells - immunology; Hemoglobins - metabolism; Humans; In Situ Hybridization, Fluorescence; Management. Prenatal diagnosis; Medical sciences; Pregnancy; Pregnancy Trimester, First; Pregnancy. Fetus. Placenta; Prenatal Diagnosis - methods; progenitors; Human; Cell culture; Maternal origin; Venous blood; Cordocentesis; First trimester; Experimental study; Amplification; Pregnancy; Prenatal; Fetal cell; Non invasive method; Female; Isolation; Strategy; Diagnosis; Technique; Comparative study; Progenitor cell
• ISSN: 0197-3851; 1097-0223
• DOI: 10.1002/pd.350

Objectives Selective amplification of rare fetal cells in maternal blood is a potential strategy for non‐invasive prenatal diagnosis. We assessed the proliferative potential of first trimester fetal progenitors compared to maternal ones. Methods Fetal and maternal haemopoietic progenitors were cultured separately and in two model mixtures: (i) co‐cultures of male fetal nucleated cells mixed with maternal nucleated cells and (ii) co‐cultures of malefetal CD34+ cells with maternal CD34+ cells. Cell origin was detected by X‐Y fluorescence in situ hybridisation (FISH) Results The frequency of haemopoietic progenitors in first trimester fetal blood (predominantly CFU‐GEMM) differed from those in peripheral blood from pregnant women (predominantly BFU‐e). First trimester haemopoietic progenitors formed larger colonies (p=0.0001) and their haemoglobinisation was accelerated compared to those of maternal origin (p<0.001). CD34+ fetal haemopoietic progenitor cells could be expanded four times more than their maternal counterparts (median 235.8‐fold, range 174.0–968.0 vs 71.9‐fold, range 41.1–192.0; p=0.003). While selective expansion of fetal cells was not observed in the mononuclear cell model, the CD34+ cell rare event mixtures produced a 463.2‐fold (range 128.0–2915.0) expansion of fetal cells. Conclusion Selective expansion of first trimester fetal haemopoietic progenitors may be useful for amplifying fetal cells from maternal blood. Copyright © 2002 John Wiley & Sons, Ltd.