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Use of collateral sensitivity networks to design drug cycling protocols that avoid resistance development

机译:使用附属敏感性网络设计避免耐药性发展的药物循环方案

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摘要

New drug deployment strategies are imperative to address the problem of drug resistance, which is limiting the management of infectious diseases and cancers. We evolved resistance in Escherichia coli toward 23 drugs used clinically for treating bacterial infections and mapped the resulting collateral sensitivity and resistance profiles, revealing a complex collateral sensitivity network. On the basis of these data, we propose a new treatment framework - collateral sensitivity cycling - in which drugs with compatible collateral sensitivity profiles are used sequentially to treat infection and select against drug resistance development. We identified hundreds of such drug sets and demonstrated that the antibiotics gentamicin and cefuroxime can be deployed cyclically such that the treatment regimen selected against resistance to either drug. We then validated our findings with related bacterial pathogens. These results provide proof of principle for collateral sensitivity cycling as a sustainable treatment paradigm that may be generally applicable to infectious diseases and cancer.
机译:必须采取新的药物部署策略来解决耐药性问题,该问题限制了传染病和癌症的管理。我们使大肠杆菌对临床上用于治疗细菌感染的23种药物的耐药性得到了发展,并绘制了由此产生的附带敏感性和耐药性图谱,揭示了复杂的附带敏感性网络。在这些数据的基础上,我们提出了一种新的治疗框架-侧支敏感性循环-在该框架中,具有兼容的侧支敏感性特征的药物被顺序用于治疗感染并选择抗药性发展。我们鉴定了数百种此类药物,并证明了抗生素庆大霉素和头孢呋辛可以循环使用,从而选择针对任一药物耐药性的治疗方案。然后,我们用相关细菌病原体验证了我们的发现。这些结果为侧支敏感性循环作为一种可持续的治疗范例提供了原则上的证明,该范例可能通常适用于传染病和癌症。

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