Maheen Imran, Muhammad Hassan Nasir, S. A. Attique, A. Baig, Q. Ain, Muhammad Usman, Muzna Munir, H. Rathore
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Several studies illustrated RA as an inherent immune response and triggered due to the “shared epitope.” Therefore, the involvement of all these receptors (IL-6, HLA-DR, and CD20) leads to the neurological, ocular, respiratory, cardiac, skin, and hematological manifestations that have been considered a potential therapeutic target for drug design. Various herbal, natural, and synthetic source inhibitors of interleukin-6 (IL-6), human leukocyte (HLA-DR), and CD20 were studied and reported previously. Reported inhibitors are compared to elucidate the best inhibitor for clinical trials, leading to the orally active drug. In this study, a computer-aided drug designing approach disclosed the potential inhibitors for all receptors based on their distinct binding affinity. Moreover, drug suitability was carried out using Lipinski’s rule by considering the adsorption, distribution, metabolism, and excretion (ADME) of ligands. Results elucidated “calycosin 7-O-glucoside” and “angeliferulate” as putative ligands for IL-6 and HLA-DR, respectively. However, the pharmacokinetic properties (ADMET) revealed angeliferulate as an effete ligand for the biological system compared to calycosin 7-O-glucoside. Based on docking, drug toxicity profiling or pharmacokinetics, and MD simulation stability, this study highlights orally active therapeutic inhibitors to inhibit the activity of pivotal receptors (IL6, HLA-DR, and CD20) of RA in humans. 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引用次数: 1
摘要
类风湿性关节炎(RA)是一种全身性炎症性疾病,可导致破坏性关节疾病、严重残疾和死亡率增加。类风湿性关节炎是所有慢性炎症性关节疾病中最常见的,其在巴基斯坦的流行频率为每千人1.6。不同的细胞因子和受体参与RA的触发,包括白细胞介素-6 (ILR-6)、主要组织相容性复合体(MHC)抗原人白细胞(HLA-DR)受体和CD20。几项研究表明,RA是一种固有的免疫反应,由“共享表位”引发。因此,所有这些受体(IL-6、HLA-DR和CD20)的参与导致神经系统、眼部、呼吸、心脏、皮肤和血液系统的表现,这些表现被认为是药物设计的潜在治疗靶点。各种草药、天然和合成的白细胞介素-6 (IL-6)、人白细胞(HLA-DR)和CD20源抑制剂已经被研究和报道过。将报道的抑制剂进行比较,以阐明临床试验的最佳抑制剂,从而获得口服活性药物。在这项研究中,计算机辅助药物设计方法揭示了基于不同结合亲和力的所有受体的潜在抑制剂。结合配体的吸附、分布、代谢和排泄(ADME),采用Lipinski法则进行药物适宜性评价。结果表明“毛蕊异黄酮- 7- o -葡萄糖苷”和“白芷”分别是IL-6和HLA-DR的可能配体。然而,药代动力学特性(ADMET)显示,与毛蕊异黄酮7- o -葡萄糖苷相比,白花是生物系统的有效配体。基于对接,药物毒性分析或药代动力学,以及MD模拟稳定性,本研究强调了口服活性治疗抑制剂抑制人类RA关键受体(IL6, HLA-DR和CD20)的活性。经过临床试验,所得抑制剂可能成为抗类风湿性关节炎药物开发的潜在治疗药物。
Molecular Modeling Guided Drug Designing for the Therapeutic Treatment of Rheumatoid Arthritis
Rheumatoid arthritis (RA) is a systemic inflammatory disorder that can cause destructive joint disease, significant disability, and increased mortality. RA is the most frequent of all chronic inflammatory joint diseases, and its prevalence frequency in Pakistan is 1.6 per thousand people. Different cytokines and receptors were involved in the triggering of RA, including interleukin-6 (ILR-6), major histocompatibility complex (MHC) antigen human leukocyte (HLA-DR) receptor, and CD20. Several studies illustrated RA as an inherent immune response and triggered due to the “shared epitope.” Therefore, the involvement of all these receptors (IL-6, HLA-DR, and CD20) leads to the neurological, ocular, respiratory, cardiac, skin, and hematological manifestations that have been considered a potential therapeutic target for drug design. Various herbal, natural, and synthetic source inhibitors of interleukin-6 (IL-6), human leukocyte (HLA-DR), and CD20 were studied and reported previously. Reported inhibitors are compared to elucidate the best inhibitor for clinical trials, leading to the orally active drug. In this study, a computer-aided drug designing approach disclosed the potential inhibitors for all receptors based on their distinct binding affinity. Moreover, drug suitability was carried out using Lipinski’s rule by considering the adsorption, distribution, metabolism, and excretion (ADME) of ligands. Results elucidated “calycosin 7-O-glucoside” and “angeliferulate” as putative ligands for IL-6 and HLA-DR, respectively. However, the pharmacokinetic properties (ADMET) revealed angeliferulate as an effete ligand for the biological system compared to calycosin 7-O-glucoside. Based on docking, drug toxicity profiling or pharmacokinetics, and MD simulation stability, this study highlights orally active therapeutic inhibitors to inhibit the activity of pivotal receptors (IL6, HLA-DR, and CD20) of RA in humans. After clinical trials, the resultant inhibitors could be potential therapeutic agents in the drug development against RA.
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