地衣芽孢杆菌中螯铁环二肽 pulcherriminic 酸的合成和分泌调控。
Regulation of the Synthesis and Secretion of the Iron Chelator Cyclodipeptide Pulcherriminic Acid in Bacillus licheniformis.
机构信息
State Key Laboratory of Agricultural Microbiology, College of Life Science and Technology, Huazhong Agricultural University, Wuhan, People's Republic of China.
Environmental Microbial Technology Center of Hubei Province, Hubei Collaborative Innovation Center for Green Transformation of Bio-Resources, College of Life Sciences, Hubei University, Wuhan, People's Republic of China.
出版信息
Appl Environ Microbiol. 2018 Jun 18;84(13). doi: 10.1128/AEM.00262-18. Print 2018 Jul 1.
The cyclodipeptide pulcherriminic acid synthesized by is an iron chelator that antagonizes certain pathogens by removing iron from the environment. But since the insoluble iron-pulcherriminic acid complex cannot act as an iron carrier as siderophores do, excessive synthesized pulcherriminic acid causes iron starvation for the producer cells. At present, the regulation of pulcherriminic acid synthesis and the mechanism by which strikes a balance between biocontrol and self-protection from excessive iron removal remain unclear. This study provides insights into the regulatory network and explains the mechanism of pulcherriminic acid biosynthesis. The synthetic gene cluster was directly negatively regulated by three regulators: AbrB, YvnA, and YvmB. Within the regulatory network, YvnA expression was repressed not only by AbrB but also by iron-limiting environments, while YvmB expression was repressed by YvnA. The transporter gene is repressed by YvmB and is required for pulcherriminic acid secretion. The biosynthesis window is determined by the combined concentration of the three regulators in an iron-rich environment. Under iron-limiting conditions, cells close the pulcherriminic acid synthesis pathway by downregulating YvnA expression. The cyclodipeptides are widespread in nature and exhibit a broad variety of biological and pharmacological activities. The cyclodipeptide scaffold is synthesized by nonribosomal peptide synthetases (NRPSs) and cyclodipeptide synthases (CDPSs). At present, it is clear that CDPSs use aminoacyl tRNAs as substrates to synthesize the two peptide bonds, and the pulcherriminic acid synthase YvmC is a member of the eight identified CDPSs. However, little is known about the regulation of cyclodipeptide synthesis and secretion. In this study, we show that AbrB, which is considered to be the main regulator of NRPS-dependent pathways, is also involved in the regulation of CDPS genes. However, AbrB is not the decisive factor for pulcherriminic acid synthesis, as the expression of YvnA determines the fate of pulcherriminic acid synthesis. With this information on how CDPS gene transcription is regulated, a clearer understanding of cyclodipeptide synthesis can be developed for Similar approaches may be used to augment our knowledge on CDPSs in other bacteria.
由 合成的环二肽 pulcherriminic 酸是一种铁螯合剂,通过从环境中去除铁来拮抗某些病原体。但是,由于不溶性的铁-pulcherriminic 酸复合物不能像铁载体那样作为铁载体,因此过量合成的 pulcherriminic 酸会导致产生细胞缺铁。目前,pulcherriminic 酸合成的调节以及 如何在生物防治和自身免受过度铁去除之间取得平衡的机制尚不清楚。本研究提供了对调控网络的深入了解,并解释了 pulcherriminic 酸生物合成的机制。 合成基因簇直接受到三个调节剂的负调控:AbrB、YvnA 和 YvmB。在调控网络中,YvnA 的表达不仅受到 AbrB 的抑制,还受到缺铁环境的抑制,而 YvmB 的表达受到 YvnA 的抑制。转运基因 受到 YvmB 的抑制,是 pulcherriminic 酸分泌所必需的。生物合成窗口由铁丰富环境中三种调节剂的组合浓度决定。在缺铁条件下,细胞通过下调 YvnA 的表达关闭 pulcherriminic 酸合成途径。环二肽在自然界中广泛存在,具有广泛的生物学和药理学活性。环二肽支架由非核糖体肽合成酶(NRPSs)和环二肽合成酶(CDPSs)合成。目前,已经清楚 CDPSs 使用氨酰-tRNA 作为底物合成两个肽键,而 pulcherriminic 酸合成酶 YvmC 是已鉴定的 8 个 CDPSs 之一。然而,关于环二肽合成和分泌的调节知之甚少。在这项研究中,我们表明,被认为是 NRPS 依赖性途径的主要调节剂的 AbrB 也参与了 CDPS 基因的调节。然而,AbrB 不是 pulcherriminic 酸合成的决定性因素,因为 YvnA 的表达决定了 pulcherriminic 酸合成的命运。有了关于 CDPS 基因转录如何调节的信息,就可以更清楚地了解环二肽的合成, 类似的方法可能用于增强我们对其他细菌中 CDPSs 的了解。
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