Mesalamine may be a plausible therapeutic agent for the management of diabetic wounds: A computational approach

Letters in Drug Design & Discovery Pub Date : 2023-04-27 DOI:10.2174/1570180820666230427145116

Vidyasrilekha. Yele, Bharat Kumar Reddy Sanapalli, Jayrajsinh Jadeja, Priya. Kakasaniya, Jaydip. Asodariya

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Abstract

Validation of mesalamine (MS) as a potential therapeutic agent in treating diabetic wound (DW) healing using in silico approach. Diabetic wound (DW) is a serious consequence of diabetes that frequently results in the amputation of the affected organ. Maggot therapy, pressure off-loading, surgical intervention, glucose control, hyperbaric oxygen therapy, wound debridement, and other treatments are currently available for DW. However, the majority of people do not meet all DW requirements due to significant pathology and the high expense of the solutions. To address the issues with current conventional therapy, we reasoned that repurposing existing medication (MS) to a target receptor that plays a significant role in the progression of DW might be advantageous. Mesalamine (MS), also known as Mesalazine or 5- Aminosalicylic acid, is an aminosalicylate anti-inflammatory used to treat inflammatory bowel disease (IBD), ulcerative colitis (UC), inflamed anus or rectum. The complicated pathophysiology of DW, which includes prolonged inflammation, increased infection, decreased cell proliferation, and migration, is a serious issue. As a result, we chose the MMP-9, TNF-α, MurC, ParE, and GSK-3β receptors as a universal target for treating the complex pathogenesis of DW. The use of MS as a therapeutic modulator on MMP-9, TNF-α, MurC, ParE, and GSK-3β receptors was studied in the current hypothetical investigation. Computational studies such as molecular docking and MMGBSA were performed by using the Schrödinger suite. Computational investigations, such as molecular docking and MMGBSA were used to test our theory. It is clear from the in silico methods that MS has a higher binding affinity for the designated receptors. Hence, it is predicted that MS may be a good therapeutic agent to use in the treatment of DW. As a result of our findings, MS appears to be a unique therapeutic drug for the treatment of DW. However, further studies are highly required to take MS into clinical use.

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美沙拉明可能是一种合理的治疗药物管理糖尿病伤口:计算方法

美沙拉胺(MS)作为一种潜在的治疗药物在糖尿病创面(DW)愈合中的应用。糖尿病性伤口是糖尿病的一个严重后果，经常导致受影响器官的截肢。目前，蛆疗法、减压、手术干预、血糖控制、高压氧治疗、伤口清创和其他治疗方法可用于DW。然而，由于严重的病理和解决方案的高费用，大多数人不能满足所有的DW要求。为了解决当前常规治疗的问题，我们认为将现有药物(MS)重新用于在DW进展中起重要作用的靶受体可能是有利的。美沙拉明(MS)，也被称为美沙拉嗪或5-氨基水杨酸，是一种氨基水杨酸类抗炎药，用于治疗炎症性肠病(IBD)、溃疡性结肠炎(UC)、肛门或直肠发炎。DW复杂的病理生理，包括炎症延长、感染增加、细胞增殖减少和迁移，是一个严重的问题。因此，我们选择了MMP-9、TNF-α、MurC、ParE和GSK-3β受体作为治疗DW复杂发病机制的通用靶点。在目前的假设研究中，研究了MS作为MMP-9、TNF-α、MurC、ParE和GSK-3β受体的治疗调节剂的使用。使用Schrödinger套件进行分子对接和MMGBSA等计算研究。计算研究，如分子对接和MMGBSA被用来验证我们的理论。从计算机方法中可以清楚地看出，MS对指定受体具有更高的结合亲和力。因此，预测MS可能是一种很好的治疗DW的药物。由于我们的发现，MS似乎是治疗DW的一种独特的治疗药物。然而，将MS应用于临床还需要进一步的研究。

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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Letters in Drug Design & Discovery

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