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精原干细胞增殖的调控

Regulation of the proliferation of spermatogonial stem cells.

作者信息

De Rooij D G

机构信息

Department of Cell Biology, State University of Utrecht, Medical School, The Netherlands.

出版信息

J Cell Sci Suppl. 1988;10:181-94. doi: 10.1242/jcs.1988.supplement_10.14.

Abstract

The proliferating cells in the seminiferous epithelium can be subdivided into the (morphologically) undifferentiated and the differentiating spermatogonia. In turn the undifferentiated spermatogonia can be subdivided according to their topographical arrangement into clones consisting of one cell, the A-single (As) spermatogonia, two cells, the A-paired (Apr) spermatogonia or groups of 4, 8 or 16 cells, the A-aligned (Aal) spermatogonia. Most likely the As spermatogonia are the stem cells of spermatogesis. When these cells divide their daughter cells can either migrate away from each other and become two new stem cells or stay together as Apr spermatogonia. The Apr spermatogonia can divide further to form Aal spermatogonia. Although suggestions have been made for the existence of a class of long-cycling stem cells with a higher probability for self-renewal, all cell kinetic data are still compatible with a homogeneous population of stem cells, the proliferative activity of which varies during the cycle of the seminiferous epithelium. Radiobiological studies have revealed that the radiosensitivity of the stem cells varies with their proliferative activity and that there is no particular class of radioresistant stem cells. In both rat and Chinese hamster the cell cycle time of the undifferentiated spermatogonia appeared to be much longer than that of the differentiating spermatogonia. All types of undifferentiated spermatogonia have the same minimum cell cycle time. However, the As spermatogonia, the stem cells, generally divide after longer intervals. The proliferative activity of the undifferentiated spermatogonia varies during the cycle of the seminiferous epithelium. At a certain moment during the epithelial cycle the undifferentiated spermatogonia, including the stem cells, are stimulated to proliferate. After a period of active proliferation the Apr and Aal spermatogonia are arrested in G1 phase possibly by the production of a chalone by the differentiating spermatogonia. In both rat and Chinese hamster the As spermatogonia are less sensitive towards this inhibition and continue to proliferate for some time longer. In the normal epithelium the probability of self-renewal of the stem cells varies with their proliferative activity in such a way that is low during active proliferation. In the normal epithelium there appeared to be no regulatory mechanism to ensure an even density of the stem cells. A large variation in stem cell density was found between areas. However, after heavy cell loss, for example after irradiation, the probability of self-renewal was found to be close to 100%. In primates the undifferentiated spermatogonia are composed of the so-called Ap and Ad spermatogonia.(ABSTRACT TRUNCATED AT 400 WORDS)

摘要

生精上皮中的增殖细胞可细分为(形态学上)未分化的精原细胞和正在分化的精原细胞。未分化的精原细胞又可根据其拓扑排列细分为由一个细胞组成的克隆,即A单倍体(As)精原细胞;由两个细胞组成的克隆,即A双联体(Apr)精原细胞;或由4、8或16个细胞组成的群体,即A排列体(Aal)精原细胞。As精原细胞很可能是精子发生的干细胞。当这些细胞分裂时,它们的子细胞要么彼此分离并成为两个新的干细胞,要么作为Apr精原细胞聚集在一起。Apr精原细胞可进一步分裂形成Aal精原细胞。尽管有人提出存在一类具有更高自我更新概率的长周期干细胞,但所有细胞动力学数据仍与一类均匀的干细胞群体相符,其增殖活性在生精上皮周期中有所变化。放射生物学研究表明,干细胞的放射敏感性随其增殖活性而变化,不存在特殊的抗辐射干细胞类别。在大鼠和中国仓鼠中,未分化精原细胞的细胞周期时间似乎比正在分化的精原细胞长得多。所有类型的未分化精原细胞具有相同的最短细胞周期时间。然而,作为干细胞的As精原细胞通常间隔更长时间才分裂。未分化精原细胞的增殖活性在生精上皮周期中有所变化。在上皮周期的某个时刻,包括干细胞在内的未分化精原细胞受到刺激而增殖。经过一段时间的活跃增殖后,Apr和Aal精原细胞可能因正在分化的精原细胞产生的抑素而停滞在G1期。在大鼠和中国仓鼠中,As精原细胞对这种抑制的敏感性较低,并会继续增殖一段时间。在正常上皮中,干细胞自我更新的概率随其增殖活性而变化,在活跃增殖期间较低。在正常上皮中,似乎不存在确保干细胞密度均匀的调节机制。不同区域的干细胞密度差异很大。然而,在大量细胞损失后,例如照射后,发现自我更新的概率接近100%。在灵长类动物中,未分化的精原细胞由所谓的Ap和Ad精原细胞组成。(摘要截于400字)

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