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Large-scale normal cell death in the developing rat kidney and its reduction by epidermal growth factor.发育中大鼠肾脏的大规模正常细胞死亡及其被表皮生长因子的减少。
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A longitudinal study of the growth of the black-hooded rat: methods of measurement and rates of growth for skull, limbs, pelvis, nose-rump and tail lengths.黑帽大鼠生长的纵向研究:颅骨、四肢、骨盆、鼻臀长度和尾巴长度的测量方法及生长速率
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负责限制小鼠体细胞生长的细胞周期动力学变化。

Changes in cell-cycle kinetics responsible for limiting somatic growth in mice.

作者信息

Chang Maria, Parker Elizabeth A, Muller Tessa J M, Haenen Caroline, Mistry Maanasi, Finkielstain Gabriela P, Murphy-Ryan Maureen, Barnes Kevin M, Sundaram Rajeshwari, Baron Jeffrey

机构信息

Section on Growth and Development, National Institutes of Health, Bethesda, MD 20892, USA.

出版信息

Pediatr Res. 2008 Sep;64(3):240-5. doi: 10.1203/PDR.0b013e318180e47a.

DOI:10.1203/PDR.0b013e318180e47a
PMID:18535488
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2729112/
Abstract

In mammals, the rate of somatic growth is rapid in early postnatal life but then slows with age, approaching zero as the animal approaches adult body size. To investigate the underlying changes in cell-cycle kinetics, [methyl-H]thymidine and 5'-bromo-2'deoxyuridine were used to double-label proliferating cells in 1-, 2-, and 3-wk-old mice for four weeks. Proliferation of renal tubular epithelial cells and hepatocytes decreased with age. The average cell-cycle time did not increase in liver and increased only 1.7 fold in kidney. The fraction of cells in S-phase that will divide again declined approximately 10 fold with age. Concurrently, average cell area increased approximately 2 fold. The findings suggest that somatic growth deceleration primarily results not from an increase in cell-cycle time but from a decrease in growth fraction (fraction of cells that continue to proliferate). During the deceleration phase, cells appear to reach a proliferative limit and undergo their final cell divisions, staggered over time. Concomitantly, cells enlarge to a greater volume, perhaps because they are relieved of the size constraint imposed by cell division. In conclusion, a decline in growth fraction with age causes somatic growth deceleration and thus sets a fundamental limit on adult body size.

摘要

在哺乳动物中,出生后早期体细胞生长速率很快,但随后会随着年龄增长而减缓,当动物接近成年体型时,生长速率趋近于零。为了研究细胞周期动力学的潜在变化,使用[甲基 - H]胸苷和5'-溴 - 2'-脱氧尿苷对1周龄、2周龄和3周龄小鼠的增殖细胞进行了为期四周的双重标记。肾小管上皮细胞和肝细胞的增殖随年龄增长而下降。肝脏中的平均细胞周期时间没有增加,肾脏中的平均细胞周期时间仅增加了1.7倍。随着年龄增长,处于S期且会再次分裂的细胞比例下降了约10倍。同时,平均细胞面积增加了约2倍。这些发现表明,体细胞生长减速主要不是由于细胞周期时间的增加,而是由于生长分数(继续增殖的细胞比例)的下降。在减速阶段期间,细胞似乎达到了增殖极限并进行其最后的细胞分裂,这些分裂随时间交错进行。同时,细胞体积增大,这可能是因为它们摆脱了细胞分裂所施加的大小限制。总之,随着年龄增长生长分数下降导致体细胞生长减速,从而为成年体型设定了一个基本限制。