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Antibiotic Discovery: Where Have We Come from, Where Do We Go?

机译:抗生素发现:我们来自哪里,我们去哪里?

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Given the increase in antibiotic-resistant bacteria, alongside the alarmingly low rate of newly approved antibiotics for clinical usage, we are on the verge of not having effective treatments for many common infectious diseases. Historically, antibiotic discovery has been crucial in outpacing resistance and success is closely related to systematic procedures—platforms—that have catalyzed the antibiotic golden age, namely the Waksman platform, followed by the platforms of semi-synthesis and fully synthetic antibiotics. Said platforms resulted in the major antibiotic classes: aminoglycosides, amphenicols, ansamycins, beta-lactams, lipopeptides, diaminopyrimidines, fosfomycins, imidazoles, macrolides, oxazolidinones, streptogramins, polymyxins, sulphonamides, glycopeptides, quinolones and tetracyclines. During the genomics era came the target-based platform, mostly considered a failure due to limitations in translating drugs to the clinic. Therefore, cell-based platforms were re-instituted, and are still of the utmost importance in the fight against infectious diseases. Although the antibiotic pipeline is still lackluster, especially of new classes and novel mechanisms of action, in the post-genomic era, there is an increasingly large set of information available on microbial metabolism. The translation of such knowledge into novel platforms will hopefully result in the discovery of new and better therapeutics, which can sway the war on infectious diseases back in our favor.
机译:鉴于耐药性细菌的增加,以及新批准的临床使用抗生素的比率惊人地低,我们濒临对许多常见传染病没有有效治疗的边缘。从历史上看,抗生素的发现对于超越耐药性至关重要,而成功与催化抗生素黄金时代的系统程序平台密切相关,平台即Waksman平台,其次是半合成和完全合成抗生素平台。所述平台产生了主要的抗生素类别:氨基糖苷类,苯甲酚类,安沙霉素类,β-内酰胺类,脂肽类,二氨基嘧啶类,磷霉素类,咪唑类,大环内酯类,恶唑烷酮类,链霉菌素类,多粘菌素,磺酰胺类,糖肽类,喹诺酮类和四环素类。在基因组学时代出现了基于靶标的平台,该平台大多被认为是失败的,原因是药物在临床上的应用受到限制。因此,重新建立了基于细胞的平台,并且在对抗传染病方面仍然至关重要。尽管抗生素的销售渠道仍然乏善可陈,特别是对于新类别和新颖的作用机制,但在后基因组时代,关于微生物代谢的信息越来越多。将这些知识转化为新颖的平台将有望导致发现新的更好的治疗方法,从而使对传染病的战争重新回到我们的角度。

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