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The near future: improving the activity of rifamycins and pyrazinamide.

机译:不久的将来:提高利福霉素和吡嗪酰胺的活性。

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摘要

While we wait for improved new anti-tuberculosis drugs, the main aim for improving current treatment should be to optimize the use of the two current drugs, rifampicin and the pro-drug pyrazinamide, which are responsible to a similar extent for the entire sterilizing activity of current therapy. The rifamycin activity could be improved by increasing the dose size of rifampicin or by daily dosing with long acting rifapentine. Increasing the dose size of pyrazinamide is limited by toxicity but an alternative approach is to use inhalation with pyrazinoic acid, as an adjunct to standard oral therapy. This would acidify pulmonary lesions, thus increasing the bactericidal activity of the orally administered pyrazinamide. Because pyrazinoic acid is the active moiety, it should also increase overall pyrazinamide activity and, because most resistance arises in the pncA gene that converts pyrazinamide to pyrazinoic acid, it should act on most pyrazinamide resistant strains. Inhalation technology allows delivery of drug to lesions rapidly and without first pass toxicity. The properties of drug containing microparticles and nanoparticles during inhalation and storage are reviewed. Spray-dried larger Trojan particles in which the smaller encapsulated particles can reside should be able to improve localisation within alveoli and avoid some storage problems.
机译:在等待改进的抗结核新药的过程中,改善当前治疗的主要目标应该是优化两种当前药物的使用:利福平和前药吡嗪酰胺,它们对整个杀菌活性的影响程度相似。目前的治疗方法。利福霉素的活性可以通过增加利福平的剂量大小或每天服用长效利福喷丁来提高。吡嗪酰胺的剂量增加受到毒性的限制,但是另一种方法是使用吡嗪酸吸入作为标准口服疗法的辅助手段。这将酸化肺部病变,从而增加口服吡嗪酰胺的杀菌活性。因为吡嗪酸是活性部分,所以它也应该增加吡嗪酰胺的整体活性,并且由于大多数将pazA基因转化为吡嗪酰胺为吡嗪酸的耐药性,因此它应作用于大多数对吡嗪酰胺耐药的菌株。吸入技术可将药物快速递送至病变部位,而无首过毒性。综述了吸入和储存过程中含药物的微粒和纳米颗粒的特性。喷雾干燥的较大Trojan颗粒(其中可以包含较小的封装颗粒)应该能够改善肺泡内的定位并避免某些存储问题。

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