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年龄对恒河猴(猕猴)CD34+细胞及造血祖细胞的频率、细胞周期和谱系成熟的影响。

Effect of age on the frequency, cell cycle, and lineage maturation of rhesus monkey (Macaca mulatta) CD34+ and hematopoietic progenitor cells.

作者信息

Lee C Chang I, Fletcher Misty D, Tarantal Alice F

机构信息

California National Primate Research Center, University of California, Davis, Davis, California 95616, USA.

出版信息

Pediatr Res. 2005 Aug;58(2):315-22. doi: 10.1203/01.PDR.0000169975.30339.32. Epub 2005 Jul 8.

Abstract

The effects of maturation and aging on hematopoietic progenitor cells, blood and bone marrow from second- and third-trimester fetal, newborn, infant, adult, and aged rhesus monkeys (Macaca mulatta) were analyzed. CD34(+) cells were immunoselected and stained with propidium iodide for cell cycle analysis. Blood and bone marrow mononuclear cells were plated in methylcellulose, and erythroid and myeloid progenitors were grown and counted. A higher frequency of circulating CD34(+)CD38(-) and CD34(+)DR(-) cells was observed in second-trimester fetuses compared with the other age groups. The frequency of bone marrow CD34(+)CD38(-) and CD34(+)DR(-) cells declined in adult and aged animals when compared with the younger age groups. Cell-cycle analysis showed 4.5% second-trimester fetal bone marrow CD34(+) cells entering the G(2)/M phase, compared with 1.7% CD34(+) cells in aged animals. More than 95% of circulating CD34(+) cells remained quiescent for most age groups, except for second-trimester fetuses. Adult marrow myeloid progenitors were found in a lower quantity when compared with third-trimester fetuses, whereas erythroid progenitors were greatest in early-gestation fetuses and adults. The results of these studies suggest that 1) the greatest quantity of CD34(+)CD38(-) and CD34(+)DR(-) cells was found in fetal and infant bone marrow, 2) the frequency of cycling CD34(+) cells declines with maturation and aging, and 3) an age-dependent difference in lineage commitment occurs.

摘要

分析了成熟和衰老对妊娠中期和晚期胎儿、新生儿、婴儿、成年和老年恒河猴(猕猴)的造血祖细胞、血液和骨髓的影响。对CD34(+)细胞进行免疫分选并用碘化丙啶染色以进行细胞周期分析。将血液和骨髓单核细胞接种于甲基纤维素中,培养并计数红系和髓系祖细胞。与其他年龄组相比,妊娠中期胎儿循环中CD34(+)CD38(-)和CD34(+)DR(-)细胞的频率更高。与较年轻年龄组相比,成年和老年动物骨髓中CD34(+)CD38(-)和CD34(+)DR(-)细胞的频率下降。细胞周期分析显示,妊娠中期胎儿骨髓CD34(+)细胞进入G(2)/M期的比例为4.5%,而老年动物中CD34(+)细胞的这一比例为1.7%。除妊娠中期胎儿外,大多数年龄组中超过95%的循环CD34(+)细胞处于静止状态。与妊娠晚期胎儿相比,成年骨髓中的髓系祖细胞数量较少,而红系祖细胞在妊娠早期胎儿和成年动物中最多。这些研究结果表明:1)胎儿和婴儿骨髓中CD34(+)CD38(-)和CD34(+)DR(-)细胞数量最多;2)循环中CD34(+)细胞的增殖频率随成熟和衰老而下降;3)谱系定向存在年龄依赖性差异。

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