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大鼠足部皮肤的修复、细胞再填充及细胞周期再分布

Repair, repopulation and cell cycle redistribution in rat foot skin.

作者信息

Rezvani M, Hopewell J W, Morris G M, Wilding D, Whitehouse E, Robbins M E, Cortina-Borja M J

机构信息

Research Institute, University of Oxford, Churchill Hospital, UK.

出版信息

Radiother Oncol. 1998 Feb;46(2):193-9. doi: 10.1016/s0167-8140(97)00114-x.

Abstract

The influence of the phenomena of the repair of sublethal damage, repopulation and the role of the reassortment of surviving clonogenic target cells within the cell cycle have been examined in the foot skin of rats using a series of split dose experiments. The dose-related incidence of moist desquamation was used as an end-point. Initially the iso-effect dose for moist desquamation (ED50) increased with an increasing time interval (1-22 h) between two equal fractions. This effect was attributed to the well established phenomenon of the repair of sublethal damage. This appeared to be maximal with a 22 h gap between fractions. A further increase in the time interval, from 2-7 days, between two equal fractions resulted in a decrease in the ED50 value for moist desquamation. The phenomenon is most likely to be explained by a shortening of the cell cycle time in surviving epithelial target cells as repopulation first initiated. With intervals between two fractions of greater than 10 days the ED50 for moist desquamation again increased. This is likely to represent an increase in the number of epidermal target cells (repopulation). Further evidence for the effect of a reassortment of cells in the cell cycle has come from another study in which a half-tolerance priming dose of 16.8 Gy was followed by three daily fractions starting 48 or 125 h after the priming dose. The ED50 for moist desquamation based on the total fractionated dose (three fractions) was significantly lower (P < 0.05) after the longer time interval, i.e. fractions given on days 5, 6 and 7 after the primary dose. These findings were supported by the results of a cell proliferation kinetic study and jointly question the validity of a frequently made assumption of equal biological effect per fraction in a prolonged fractionated irradiation schedule.

摘要

利用一系列分割剂量实验,在大鼠足部皮肤中研究了亚致死损伤修复、再增殖现象以及存活的克隆形成靶细胞在细胞周期内重新排列的作用。将与剂量相关的湿性脱屑发生率用作终点指标。最初,湿性脱屑的等效效应剂量(ED50)随着两个相等剂量部分之间时间间隔(1 - 22小时)的增加而增加。这种效应归因于已充分确立的亚致死损伤修复现象。当剂量部分之间间隔22小时时,这种效应似乎达到最大。两个相等剂量部分之间的时间间隔进一步增加至2 - 7天,导致湿性脱屑的ED50值降低。这种现象很可能是由于再增殖开始时,存活的上皮靶细胞的细胞周期时间缩短所致。当两个剂量部分之间的间隔大于10天时,湿性脱屑的ED50再次增加。这可能代表表皮靶细胞数量的增加(再增殖)。细胞周期中细胞重新排列效应的进一步证据来自另一项研究,其中先给予16.8 Gy的半耐受预照射剂量,然后在预照射剂量后48或125小时开始每天给予三个剂量部分。基于总分割剂量(三个剂量部分)的湿性脱屑ED50在较长时间间隔后显著降低(P < 0.05),即主要剂量后第5、6和7天给予的剂量部分。这些发现得到了细胞增殖动力学研究结果的支持,并共同质疑了在延长的分割照射方案中经常做出的每个剂量部分具有相等生物学效应这一假设的有效性。

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