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三重突变体揭示了黄色粘球菌社会运动所需的三个新基因。

Triple mutants uncover three new genes required for social motility in Myxococcus xanthus.

作者信息

Youderian Philip, Hartzell Patricia L

机构信息

Department of Biology, Texas A&M University, College Station, Texas 83843-3052, USA.

出版信息

Genetics. 2007 Sep;177(1):557-66. doi: 10.1534/genetics.107.076182. Epub 2007 Jul 29.

Abstract

The bacterium Myxococcus xanthus glides over surfaces using two different locomotive mechanisms, called S (social) and A (adventurous) motility that enable cells to move both as groups and as individuals. Neither mechanism involves flagella. The functions of these two motors are coordinated by the activity of a small Ras-like protein, encoded by the mglA gene. The results of previous studies of a second-site suppressor of the mglA-8 missense mutation masK-815 indicate that MglA interacts with a protein tyrosine kinase, MasK, to control social motility. Sequence analysis of the sites of 12 independent insertions of the transposon magellan-4 that result in the loss of motility in an M. xanthus mglA-8 masK-815 double mutant shows that nine of these 12 insertions are in genes known to be required for S gliding motility. This result confirms that the masK-815 suppressor restores S but not A motility. Three of the 12 insertions define three new genes required for S motility and show that the attachment of heptose to the lipopolysaccharide inner core, an ortholog of the CheR methyltransferase, and a large protein with YD repeat motifs, are required for S motility. When these three insertions are backcrossed into an otherwise wild-type genetic background, their recombinants are found to have defects in S, but not, A motility. The spectrum of magellan-4 insertions that lead to the loss of S motility in the mglA-8 masK-815 double mutant background is different than that resulting from a previous mutant hunt starting with a different (A mutant) genetic background, suggesting that the number of genes required for S motility in M. xanthus is quite large.

摘要

黄色粘球菌利用两种不同的运动机制在表面滑行,这两种机制分别称为S(社会性)运动和A(冒险性)运动,使细胞既能群体移动,也能单独移动。这两种机制都不涉及鞭毛。这两种运动机制的功能由一种由mglA基因编码的小Ras样蛋白的活性协调。先前对mglA - 8错义突变的第二位点抑制子masK - 815的研究结果表明,MglA与一种蛋白酪氨酸激酶MasK相互作用,以控制社会性运动。对转座子麦哲伦 - 4的12个独立插入位点进行序列分析,这些插入导致黄色粘球菌mglA - 8 masK - 815双突变体失去运动能力,结果显示这12个插入中有9个位于已知S型滑行运动所需的基因中。这一结果证实masK - 815抑制子恢复了S型运动,但没有恢复A 型运动。12个插入中有3个确定了S型运动所需的3个新基因,并表明庚糖与脂多糖内核的连接、CheR甲基转移酶的一个直系同源物以及一个具有YD重复基序的大蛋白是S型运动所必需的。当将这3个插入回交至其他方面为野生型的遗传背景中时,发现它们的重组体在S型运动方面有缺陷,但在A 型运动方面没有缺陷。在mglA - 8 masK - 815双突变体背景下导致S型运动丧失的麦哲伦 - 4插入谱与先前从不同(A突变体)遗传背景开始的突变筛选所得到的结果不同,这表明黄色粘球菌中S型运动所需的基因数量相当多。

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