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染色体复制不足对大肠杆菌细胞分裂的影响。

Effects of chromosome underreplication on cell division in Escherichia coli.

作者信息

Botello E, Nordström K

机构信息

Department of Microbiology, Biomedical Center, Uppsala University, S-751 23 Uppsala, Sweden.

出版信息

J Bacteriol. 1998 Dec;180(23):6364-74. doi: 10.1128/JB.180.23.6364-6374.1998.

Abstract

The key processes of the bacterial cell cycle are controlled and coordinated to match cellular mass growth. We have studied the coordination between replication and cell division by using a temperature-controlled Escherichia coli intR1 strain. In this strain, the initiation time for chromosome replication can be displaced to later (underreplication) or earlier (overreplication) times in the cell cycle. We used underreplication conditions to study the response of cell division to a delayed initiation of replication. The bacteria were grown exponentially at 39 degreesC (normal DNA/mass ratio) and shifted to 38 and 37 degreesC. In the last two cases, new, stable, lower DNA/mass ratios were obtained. The rate of replication elongation was not affected under these conditions. At increasing degrees of underreplication, increasing proportions of the cells became elongated. Cell division took place in the middle in cells of normal size, whereas the longer cells divided at twice that size to produce one daughter cell of normal size and one three times as big. The elongated cells often produced one daughter cell lacking a chromosome; this was always the smallest daughter cells, and it was the size of a normal newborn cell. These results favor a model in which cell division takes place at only distinct cell sizes. Furthermore, the elongated cells had a lower probability of dividing than the cells of normal size, and they often contained more than two nucleoids. This suggests that for cell division to occur, not only must replication and nucleoid partitioning be completed, but also the DNA/mass ratio must be above a certain threshold value. Our data support the ideas that cell division has its own control system and that there is a checkpoint at which cell division may be abolished if previous key cell cycle processes have not run to completion.

摘要

细菌细胞周期的关键过程受到控制和协调,以匹配细胞质量的增长。我们通过使用温度可控的大肠杆菌intR1菌株研究了复制与细胞分裂之间的协调。在该菌株中,染色体复制的起始时间可以在细胞周期中被推迟到较晚(复制不足)或提前到较早(复制过度)的时间。我们利用复制不足的条件来研究细胞分裂对复制起始延迟的反应。细菌在39℃下呈指数生长(正常的DNA/质量比),然后转移到38℃和37℃。在后两种情况下,获得了新的、稳定的、较低的DNA/质量比。在这些条件下,复制延伸速率不受影响。随着复制不足程度的增加,越来越多比例的细胞变长。正常大小的细胞在中间进行细胞分裂,而较长的细胞在两倍于正常大小的时候进行分裂,产生一个正常大小的子细胞和一个三倍大的子细胞。拉长的细胞常常产生一个没有染色体的子细胞;这个子细胞总是最小的,其大小与正常新生细胞相同。这些结果支持了一种模型,即细胞分裂仅在特定的细胞大小下发生。此外,拉长的细胞比正常大小的细胞分裂的概率更低,并且它们常常含有不止两个类核。这表明,为了发生细胞分裂,不仅复制和类核分配必须完成,而且DNA/质量比必须高于某个阈值。我们的数据支持这样的观点,即细胞分裂有其自身的控制系统,并且存在一个检查点,如果之前的关键细胞周期过程没有完成,细胞分裂可能会被取消。

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