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大肠杆菌中一种新型的腐胺输出蛋白SapBCDF

A Novel Putrescine Exporter SapBCDF of Escherichia coli.

作者信息

Sugiyama Yuta, Nakamura Atsuo, Matsumoto Mitsuharu, Kanbe Ayaka, Sakanaka Mikiyasu, Higashi Kyohei, Igarashi Kazuei, Katayama Takane, Suzuki Hideyuki, Kurihara Shin

机构信息

From the Division of Applied Life Science, Graduate School of Bioresources and Environmental Sciences, Ishikawa Prefectural University, Nonoichi, Ishikawa 921-8836.

the Dairy Science and Technology Institute, Kyodo Milk Industry Co. Ltd., Tokyo 190-0182.

出版信息

J Biol Chem. 2016 Dec 16;291(51):26343-26351. doi: 10.1074/jbc.M116.762450. Epub 2016 Nov 1.

Abstract

Recent research has suggested that polyamines (putrescine, spermidine, and spermine) in the intestinal tract impact the health of animals either negatively or positively. The concentration of polyamines in the intestinal tract results from the balance of uptake and export of the intestinal bacteria. However, the mechanism of polyamine export from bacterial cells to the intestinal lumen is still unclear. In Escherichia coli, PotE was previously identified as a transporter responsible for putrescine excretion in an acidic growth environment. We observed putrescine concentration in the culture supernatant was increased from 0 to 50 μm during growth of E. coli under neutral conditions. Screening for the unidentified putrescine exporter was performed using a gene knock-out collection of E. coli, and deletion of sapBCDF significantly decreased putrescine levels in the culture supernatant. Complementation of the deletion mutant with the sapBCDF genes restored putrescine levels in the culture supernatant. Additionally, the ΔsapBCDF strain did not facilitate uptake of putrescine from the culture supernatant. Quantification of stable isotope-labeled putrescine derived from stable isotope-labeled arginine supplemented in the medium revealed that SapBCDF exported putrescine from E. coli cells to the culture supernatant. It was previously reported that SapABCDF of Salmonella enterica sv. typhimurium and Haemophilus influenzae conferred resistance toantimicrobial peptides; however, the E. coli ΔsapBCDF strain did not affect resistance to antimicrobial peptide LL-37. These results strongly suggest that the natural function of the SapBCDF proteins is the export of putrescine.

摘要

最近的研究表明,肠道中的多胺(腐胺、亚精胺和精胺)对动物健康有正面或负面影响。肠道中多胺的浓度取决于肠道细菌摄取和排出的平衡。然而,多胺从细菌细胞输出到肠腔的机制仍不清楚。在大肠杆菌中,PotE先前被确定为在酸性生长环境中负责腐胺排泄的转运蛋白。我们观察到,在中性条件下大肠杆菌生长期间,培养上清液中腐胺浓度从0增加到50μm。使用大肠杆菌基因敲除文库对未鉴定的腐胺输出蛋白进行筛选,sapBCDF缺失显著降低了培养上清液中腐胺水平。用sapBCDF基因对缺失突变体进行互补恢复了培养上清液中腐胺水平。此外,ΔsapBCDF菌株不促进从培养上清液中摄取腐胺。对培养基中添加的稳定同位素标记精氨酸衍生的稳定同位素标记腐胺进行定量分析表明,SapBCDF将腐胺从大肠杆菌细胞输出到培养上清液中。先前有报道称,鼠伤寒沙门氏菌和流感嗜血杆菌的SapABCDF赋予对抗菌肽的抗性;然而,大肠杆菌ΔsapBCDF菌株不影响对抗菌肽LL-37的抗性。这些结果强烈表明,SapBCDF蛋白的天然功能是腐胺输出。

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