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Manipulation of fungal development as source of novel secondary metabolites for biotechnology

机译:操纵真菌发育作为生物技术新的次生代谢产物的来源

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摘要

Fungal genomics revealed a large potential of yet-unexplored secondary metabolites, which are not produced during vegetative growth. The discovery of novel bioactive compounds is increasingly gaining importance. The high number of resistances against established antibiotics requires novel drugs to counteract increasing human and animal mortality rates. In addition, growth of plant pathogens has to be controlled to minimize harvest losses. An additional critical issue is the post-harvest production of deleterious mycotoxins. Fungal development and secondary metabolite production are linked processes. Therefore, molecular regulators of development might be suitable to discover new bioactive fungal molecules or to serve as targets to control fungal growth, development, or secondary metabolite production. The fungal impact is relevant as well for our healthcare systems as for agriculture. We propose here to use the knowledge about mutant strains discovered in fungal model systems for a broader application to detect and explore new fungal drugs or toxins. As examples, mutant strains impaired in two conserved eukaryotic regulatory complexes are discussed. The COP9 signalosome (CSN) and the velvet complex act at the interface between development and secondary metabolism. The CSN is a multi-protein complex of up to eight subunits and controls the activation of CULLIN-RING E3 ubiquitin ligases, which mark substrates with ubiquitin chains for protein degradation by the proteasome. The nuclear velvet complex consists of the velvet-domain proteins VeA and VelB and the putative methyltransferase LaeA acting as a global regulator for secondary metabolism. Defects in both complexes disturb fungal development, light perception, and the control of secondary metabolism. The potential biotechnological relevance of these developmental fungal mutant strains for drug discovery, agriculture, food safety, and human healthcare is discussed.
机译:真菌基因组学揭示了尚未开发的次生代谢产物的巨大潜力,其在营养生长过程中并未产生。新型生物活性化合物的发现越来越重要。对既定抗生素的大量耐药性需要新药来抵消人类和动物死亡率的上升。另外,必须控制植物病原体的生长以最小化收获损失。另一个关键问题是有害真菌毒素的收获后生产。真菌的发育和次级代谢产物的产生是相互联系的过程。因此,发育的分子调节剂可能适合发现新的生物活性真菌分子或用作控制真菌生长,发育或次级代谢产物生产的靶标。真菌的影响对我们的医疗体系和农业同样重要。我们建议在这里使用在真菌模型系统中发现的有关突变菌株的知识,以更广泛的应用来检测和探索新的真菌药物或毒素。作为例子,讨论了在两个保守的真核调节复合物中受损的突变株。 COP9信号小体(CSN)和天鹅绒复合物在发育和次级代谢之间的界面起作用。 CSN是由八个亚基组成的多蛋白复合物,可控制CULLIN-RING E3泛素连接酶的激活,该酶标记具有泛素链的底物,可被蛋白酶体降解。核天鹅绒复合物由天鹅绒结构域蛋白VeA和VelB以及假定的甲基转移酶LaeA充当次级代谢的全局调节剂组成。两种复合物中的缺陷都会干扰真菌的发育,光线的感知以及对次级代谢的控制。讨论了这些发育性真菌突变菌株对药物发现,农业,食品安全和人类保健的潜在生物技术意义。

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