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The human placenta is a hematopoietic organ during the embryonic and fetal periods of development.

Authors :
Bárcena A
Kapidzic M
Muench MO
Gormley M
Scott MA
Weier JF
Ferlatte C
Fisher SJ
Source :
Developmental biology [Dev Biol] 2009 Mar 01; Vol. 327 (1), pp. 24-33. Date of Electronic Publication: 2008 Dec 03.
Publication Year :
2009

Abstract

We studied the potential role of the human placenta as a hematopoietic organ during embryonic and fetal development. Placental samples contained two cell populations-CD34(++)CD45(low) and CD34(+)CD45(low)-that were found in chorionic villi and in the chorioamniotic membrane. CD34(++)CD45(low) cells express many cell surface antigens found on multipotent primitive hematopoietic progenitors and hematopoietic stem cells. CD34(++)CD45(low) cells contained colony-forming units culture (CFU-C) with myeloid and erythroid potential in clonogenic in vitro assays, and they generated CD56(+) natural killer cells and CD19(+)CD20(+)sIgM(+) B cells in polyclonal liquid cultures. CD34(+)CD45(low) cells mostly comprised erythroid- and myeloid-committed progenitors, while CD34(-) cells lacked CFU-C. The placenta-derived precursors were fetal in origin, as demonstrated by FISH using repeat-sequence chromosome-specific probes for X and Y. The number of CD34(++)CD45(low) cells increased with gestational age, but their density (cells per gram of tissue) peaked at 5-8 wk, decreasing more than sevenfold at the onset of the fetal phase (9 wk of gestation). In addition to multipotent progenitors, the placenta contained myeloid- and erythroid-committed progenitors indicative of active in situ hematopoiesis. These data suggest that the human placenta is an important hematopoietic organ, raising the possibility of banking placental hematopoietic stem cells along with cord blood for transplantation.

Details

Language :
English
ISSN :
1095-564X
Volume :
327
Issue :
1
Database :
MEDLINE
Journal :
Developmental biology
Publication Type :
Academic Journal
Accession number :
19073167
Full Text :
https://doi.org/10.1016/j.ydbio.2008.11.017