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Multiparameter flow cytometry characterization of MHC class I negative mouse bone marrow cells.

Authors :
Quarta M
Stroka D
Keogh A
Sidler D
Avital I
Gloor B
Muraca M
Candinas D
Inderbitzin D
Source :
Medical science monitor : international medical journal of experimental and clinical research [Med Sci Monit] 2008 Dec; Vol. 14 (12), pp. BR286-93.
Publication Year :
2008

Abstract

Background: MHC-I down-regulation was described in foetal liver progenitors, and two different subsets of adult bone marrow derived stem cells. These cells, namely, MHC-I-/Thy1+ bone marrow derived liver stem cells (BMDLSC) and the multipotent adult progenitors (MAPC) differentiated into functioning hepatocytes. The aim of this paper was to characterize the MHC-I negative bone marrow compartment as it pertains to BMDLSC and MAPC.<br />Material/methods: We performed multiparameter flow-cytometry analyses of the MHC-I negative compartment using hematopoietic (CD45, Ter119), and stem cell markers (Thy1.2, c-Kit, IL-3R, CD34) in adult mice.<br />Results: When analysing CD45 and Ter119 expression, the MHC-I negative bone marrow compartment divides into four sub-populations: 1. CD45-/Ter119+: 86.0+/-4.4%; 2. CD45+/Ter119+: 0.2+/-0.1%; 3. CD45+/Ter119-: 11.6+/-3.0%; 4. CD45-/Ter119-: 2.0+/-2.1%. Stem cells markers were only expressed on MHC-I negative/ CD45+/Ter119- cells. In vivo, MAPC (Ter119-/CD45- cells) are composed of MHC-I negative (24%) and MHC-I positive cells and do not express any of the stem cell markers tested.<br />Conclusions: In conclusion, mouse BMDLSC and MAPC are two distinct stem cell populations. Down-regulation of MHC-I was the only common characteristic found between BMDLSC and MAPC suggesting that selection of MHC-I negative cells might represent an efficient strategy to enrich for bone marrow stem cells with liver developmental potential.

Details

Language :
English
ISSN :
1643-3750
Volume :
14
Issue :
12
Database :
MEDLINE
Journal :
Medical science monitor : international medical journal of experimental and clinical research
Publication Type :
Academic Journal
Accession number :
19043363