脑白嘌呤和番茄碱作为新型LpxC和TLR4抑制剂减轻帕金森病肠道介导炎症的潜力：通过分子对接和动态模拟的高通量研究

IF 2.9 4区生物学 Q3 BIOTECHNOLOGY & APPLIED MICROBIOLOGY

3 Biotech Pub Date : 2025-07-01 Epub Date: 2025-06-16 DOI:10.1007/s13205-025-04386-3

Rubina Roy, Indira Gahatraj, Anupama Sharma, Vishal Kumar, Rajib Paul, Diwakar Kumar, Pallab Bhattacharya, Anupom Borah

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引用次数: 0

摘要

肠道生态失调与帕金森病（PD）的发病密切相关，其中细菌内毒素脂多糖（LPS）和人类toll样受体4 （TLR4）之间的相互作用起着至关重要的作用。抑制lps -合成酶LpxC和LPS-TLR4相互作用将减少细菌负荷和肠-脑炎症。与目前研究的合成抑制剂相关的副作用迫切需要有效的替代品。本研究旨在从植物生物碱中鉴定LpxC和TLR4抑制剂，这是一类众所周知的治疗能力。数据库检索得到505种生物碱，其中314种生物碱具有肠血和血脑屏障渗透性，且具有良好的药物相似性。314种生物碱的位点特异性对接，分别为LpxC和TLR4获得了29个和88个命中配体。随后，分子相互作用分析显示，头孢酞氨酸是最有潜力的LpxC和TLR4双抑制剂，其次是番茄碱。在分子动力学模拟中观察到更强的亲和力、强度和稳定性，进一步增强了头孢酞素和番茄碱对LpxC和TLR4的抑制作用，头孢酞素是更有潜力的TLR4抑制剂，番茄碱是更好的LpxC抑制剂。药代动力学评价表明番茄碱具有良好的吸收、分布、代谢和消除作用，而头孢酞素用于治疗蛇咬伤、白细胞减少和脱发的临床应用表明其毒性很小。该研究提出了头孢酞氨酸和番茄碱作为LpxC和TLR4的双重抑制剂，为对抗肠道生态失调和PD提供了一种合理的多靶点单药或联合药物治疗策略。然而，临床前和临床研究以及改进的头孢蒽醌和番茄碱的药代动力学有必要验证我们的计算机研究结果。

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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Potentials of cepharanthine and tomatidine as novel LpxC and TLR4 inhibitors to mitigate gut-mediated inflammation in Parkinson's disease: a high-throughput investigation through molecular docking and dynamic simulation.

Gut dysbiosis is strongly implicated in the pathogenesis of Parkinson's disease (PD), where the interaction between bacterial endotoxin lipopolysaccharide (LPS) and human toll-like receptor 4 (TLR4) plays a crucial role. Inhibiting LPS-synthesizing enzyme LpxC and LPS-TLR4 interaction will reduce bacterial load and gut-brain inflammation. Side effects associated with the currently investigated synthetic inhibitors urge the need for effective alternatives. The present study was conducted to identify LpxC and TLR4 inhibitors from phyto-alkaloids, a class well-known for its therapeutic abilities. 505 alkaloids were yielded from the database search, amongst which 314 alkaloids showed gut-blood and blood-brain barrier permeability, and favorable drug-likeness. Site-specific docking of 314 alkaloids yielded 29 and 88 hit ligands for LpxC and TLR4 respectively. Subsequently, the molecular interaction analysis revealed cepharanthine as the most potential dual inhibitor of LpxC and TLR4, followed by tomatidine. Greater affinity, strength, and stability observed in molecular dynamic simulation further strengthened the LpxC and TLR4 inhibition by cepharanthine and tomatidine, with cepharanthine being a more potential TLR4 inhibitor and tomatidine a better LpxC inhibitor. Pharmacokinetic property assessment suggested favorable absorption, distribution, metabolism, and elimination of tomatidine, while the clinical application of cepharanthine for snake bite, leukopenia, and alopecia supports its minimal toxicity. Presenting cepharanthine and tomatidine as dual inhibitors of LpxC and TLR4, the study suggests a plausible multitarget single or combinatorial drug therapy strategy for countering gut dysbiosis and PD. However, preclinical and clinical investigations and improved pharmacokinetics of cepharanthine and tomatidine are warranted to validate our in silico findings.

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来源期刊

3 Biotech Agricultural and Biological Sciences-Agricultural and Biological Sciences (miscellaneous)

CiteScore

6.00

自引率

0.00%

发文量

314

期刊介绍： 3 Biotech publishes the results of the latest research related to the study and application of biotechnology to: - Medicine and Biomedical Sciences - Agriculture - The Environment The focus on these three technology sectors recognizes that complete Biotechnology applications often require a combination of techniques. 3 Biotech not only presents the latest developments in biotechnology but also addresses the problems and benefits of integrating a variety of techniques for a particular application. 3 Biotech will appeal to scientists and engineers in both academia and industry focused on the safe and efficient application of Biotechnology to Medicine, Agriculture and the Environment.