Jung Hyeim, Liang Junwei, Jung Yuna, Lim Dongbin
School of Systems Biomedical Science, Soongsil University, Seoul, 06978, Republic of Korea.
J Microbiol. 2015 Dec;53(12):820-8. doi: 10.1007/s12275-015-5304-0. Epub 2015 Dec 2.
Exonuclease VII (ExoVII) of Escherichia coli is a single strandspecific DNA nuclease composed of two different subunits: the large subunit, XseA, and the small subunit, XseB. In this study, we found that multicopy single-stranded DNAs (msDNAs), Ec83 and Ec78, are the in vivo substrates of ExoVII; the enzyme cuts the phosphodiester bond between the fourth and fifth nucleotides from the 5'end. We used this msDNA cleavage to assess ExoVII activity in vivo. Both subunits were required for enzyme activity. Expression of XseA without XseB caused cell death, even though no ExoVII activity was detected. The lethality caused by XseA was rescued by surplus XseB. In XseA-induced death, cells were elongated and multinucleated, and their chromosomes were fragmented and condensed; these are the morphological hallmarks of apoptotic cell death in bacteria. A putative caspase recognition sequence (FVAD) was found in XseA, and its hypothetical caspase product with 257 amino acids was as active as the intact protein in inducing cell death. We propose that under ordinary conditions, XseA protects chromosome as a component of the ExoVII enzyme, but in some conditions, the protein causes cell death; the destruction of cell is probably carried out by the amino terminal fragment derived from the cleavage of XseA by caspase-like enzyme.
大肠杆菌的核酸外切酶VII(ExoVII)是一种单链特异性DNA核酸酶,由两个不同的亚基组成:大亚基XseA和小亚基XseB。在本研究中,我们发现多拷贝单链DNA(msDNA),即Ec83和Ec78,是ExoVII在体内的底物;该酶切割5'端第四和第五个核苷酸之间的磷酸二酯键。我们利用这种msDNA切割来评估ExoVII在体内的活性。酶活性需要两个亚基。即使未检测到ExoVII活性,单独表达XseA也会导致细胞死亡。过量的XseB可挽救由XseA引起的致死性。在由XseA诱导的死亡中,细胞伸长且多核,其染色体断裂并浓缩;这些是细菌中凋亡细胞死亡的形态学特征。在XseA中发现了一个假定的半胱天冬酶识别序列(FVAD),其具有257个氨基酸的假定半胱天冬酶产物在诱导细胞死亡方面与完整蛋白一样活跃。我们提出,在正常条件下,XseA作为ExoVII酶的一个组分保护染色体,但在某些条件下,该蛋白会导致细胞死亡;细胞的破坏可能是由类似半胱天冬酶的酶切割XseA产生的氨基末端片段进行的。
