Age-associated reduction of the count and functional activity of stromal precursor cells can be caused by both true reduction

The study was carried out on CBA mice using the method of heterotopic transplantation. A fragment of the femoral bone marrow (1/2) or spleen (1/5 of the organ) was transplanted under the renal capsule of a recipient. The following donor-recipient cross-transplantation variants were studied: young[ri...

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Published inBulletin of experimental biology and medicine Vol. 151; no. 2; p. 210
Main Authors Danilova, T.A, Gorskaya, Yu. F, Nesterenko, V.G
Format Journal Article
LanguageEnglish
Published Springer 01.06.2011
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Summary:The study was carried out on CBA mice using the method of heterotopic transplantation. A fragment of the femoral bone marrow (1/2) or spleen (1/5 of the organ) was transplanted under the renal capsule of a recipient. The following donor-recipient cross-transplantation variants were studied: young[right arrow]young (Y[right arrow]Y), young[right arrow]old (Y[right arrow]O), old[right arrow]old (O[right arrow]O), and old[right arrow]young (O[right arrow]Y). Cell suspensions were prepared from 2-month transplants inoculated in monolayer cultures and the cloning efficiency (ECF-F) of stromal precursor cells (CFC-F) was evaluated. The bone marrow transplant ECF-F and the count of CFC-F in the O[right arrow]O group were 8-fold lower than in the Y[right arrow]Y group. In the O[right arrow]Y group, ECF-F was 3-fold higher than in the O[right arrow]O group, but by 2.5 times lower than in the Y[right arrow]Y group. ECF-F in Y[right arrow]O group was 2-fold lower than in Y[right arrow]Y group. The ECF-F and CFC-F count in spleen transplants in the O[right arrow]O group were 4- and 6-fold lower, respectively, than in Y[right arrow]Y group. However, in O[right arrow]Y group ECF-F was 7-fold higher than in O[right arrow]O group and higher than even in Y[right arrow]Y group. The weight of induced ectopic bone tissue after transplantation of the osteoinductor (fragments of the allogenic urinary bladder mucosa) was 2-fold lower in the O[right arrow]O vs. Y[right arrow]Y group. However, comparison of the ectopic bone tissue weights in different experimental groups showed that osteoinductor activity of the bladder epithelium did not decrease, but increased 3-fold with age (O[right arrow]Y:Y[right arrow]Y). A 5-fold reduction of this proportion in groups where the osteoinductor was transplanted from old donors to old and young recipients (O[right arrow]Y:O[right arrow]O) could be attributed to age-specific reduction of the count of inducible osteogenic precursor cells (IOPC). The data in general suggest that age-specific reduction of the stromal precursor count and functional activity could be caused by the true reduction (exhaustion) of cell pool (bone marrow CFC-F; presumably, IOPC) and by the regulatory effects of the organism (bone marrow and splenic CFC-F, IOPC). These data seem to be significant for understanding of the role of osteogenic stromal precursor cells in the development of age-associated bone tissue defects, for example, senile osteoporosis. Key Words: stromal cells; age-associated changes
ISSN:0007-4888