靶向肺炎链球菌udp -葡萄糖焦磷酸化酶(UGPase):一种推定抑制剂的体外验证。

IF 2 Q3 PHARMACOLOGY & PHARMACY Drug Target Insights Pub Date : 2020-10-07 eCollection Date: 2020-01-01 DOI:10.33393/dti.2020.2103
Monica Sharma, Swati Sharma, Pallab Ray, Anuradha Chakraborti
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引用次数: 3

摘要

背景:肺炎链球菌的基因组可塑性是各种抗生素和荚膜多糖疫苗疗效降低的原因。因此,寻求独立于荚膜类型的靶点来控制肺炎球菌的致病性。udp -葡萄糖焦磷酸化酶(UGPase)就是其中一种需要的候选物,它负责合成udp -葡萄糖,这是包膜生物合成和代谢Leloir途径中的糖前体。作为肺炎球菌病理生物学的关键,我们在体外评估了UGPase抑制对毒力的影响。方法:研究一种推定的抑制剂尿苷二磷酸(UDP)对肺炎链球菌和A549细胞的有效抑制浓度、疗效和毒性。在人呼吸上皮(A549和HEp-2)和巨噬细胞(THP1和J774.A.1)细胞系中分别测定了UDP对粘附和吞噬的影响。结果:UDP在肺炎链球菌和A549细胞中对UGPase的有效抑制浓度不同,分别为5µM和100µM。UDP治疗降低了肺炎球菌感染单层细胞的细胞毒性百分比,并且对存活率没有不利影响。UDP治疗显著降低了肺炎链球菌对宿主细胞的粘附性。UDP诱导白细胞介素(IL)-1β、肿瘤坏死因子(TNF)-α、IL-6和IL-8的分泌,增加肺炎球菌的吞噬能力。结论:我们的研究显示UDP介导的肺炎链球菌毒力下降,并证明UDP是肺炎球菌UGPase的有效抑制剂。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

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Targeting Streptococcus pneumoniae UDP-glucose pyrophosphorylase (UGPase): in vitro validation of a putative inhibitor.

Background: Genome plasticity of Streptococcus pneumoniae is responsible for the reduced efficacy of various antibiotics and capsular polysaccharide-based vaccines. Therefore, targets independent of capsular types are sought to control the pneumococcal pathogenicity. UDP-glucose pyrophosphorylase (UGPase) is one such desired candidate being responsible for the synthesis of UDP-glucose, a sugar precursor in capsular biosynthesis and metabolic Leloir pathway. Being crucial to pneumococcal pathobiology, the effect of UGPase inhibition on virulence was evaluated in vitro.

Methods: A putative inhibitor, uridine diphosphate (UDP), was evaluated for effective inhibitory concentration in S. pneumoniae and A549 cells, its efficacy and toxicity. The effect of UDP on adherence and phagocytosis was measured in human respiratory epithelial (A549 and HEp-2) and macrophage (THP1 and J774.A.1) cell lines respectively.

Results: A differential effective inhibitory concentration of UDP for UGPase inhibition was observed in S. pneumoniae and A549 cells, that is, 5 and 100 µM respectively. UDP treatments lowered percent cytotoxicity in pneumococcal-infected monolayers and didn't exert adverse effects on viabilities. S. pneumoniae adherence to host cells decreased significantly with UDP treatments. UDP induced the secretion of interleukin (IL)-1β, tumor necrosis factor (TNF)-α, IL-6, and IL-8 and increased pneumococcal phagocytosis.

Conclusion: Our study shows UDP-mediated decrease in the virulence of S. pneumoniae and demonstrates UDP as an effective inhibitor of pneumococcal UGPase.

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来源期刊
Drug Target Insights
Drug Target Insights PHARMACOLOGY & PHARMACY-
CiteScore
2.70
自引率
0.00%
发文量
5
审稿时长
8 weeks
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