ROLE OF COX-2 IN ORAL CANCER AND IN-SILICO DOCKING OF NATURAL FRAGMENTED AND DRUG BASED LIGANDS OF COX-2 FOR INHIBITION OF PROGRESSION OF ORAL CANCER

Arpita Maitra, S. Das, R.R Paul, Mousumi Pal
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Abstract

Oral cancer is known for its devastating effects which need to be addressed at the molecular level to achieve the best possible outcomes. An upsurge in the COX-2 levels amongst premalignant & malignant tissues may be attributed to increased transcription along with enhanced mRNA stability. Compelling research evidence is being shown with respect to complexes which have dual COX-2/COX-1 inhibitors are beneficial in chemotherapeutic procedures of cancer.Amongst 15 compounds, we found the highest binding capacity to be -10.9 in rutaecarpine as per the ADV webserver and -11.2 in VX-809 (Lumacaftor) as per the ProdigY webserver. Highest hydrophobicity was seen in OSR, LMR & ECG weighing 389.33, 452.41 & 458.37 with the most common amino acids being Leu (338), Ser (339), Val (509), Val (335). In respect to the molar refractivity, OSR & LMR presented with 92.01 & 113.98 values, whereas the lipophilisity was found to be 2.46 & 3.08 respectively with toxicity score (assessed by toxi M score & ProTox), being 0.929 & 0.944 by ToxiM score & 4 in both compounds by ProTox class.Characteristic properties such as the hydrophobicity, hydrophilicity, molecular weight, number of H-bond acceptors, Num of H-bond donors, molar refractivity, lipophilisity (ilogP), drug likeliness and toxicity score play an important role in understanding drug-drug interactions at the molecular level which helps in determining the pharmacological actions and its application in humans. Therefore, further research in the field is recommended to comprehend the drug reactions & their outcome.
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COX-2 在口腔癌中的作用以及 COX-2 的天然片段和药物配体在抑制口腔癌进展方面的硅对接研究
众所周知,口腔癌具有破坏性影响,需要在分子水平上加以解决,以达到最佳治疗效果。癌前病变和恶性肿瘤组织中 COX-2 水平的飙升可能是由于转录增加和 mRNA 稳定性增强所致。有令人信服的研究证据表明,具有 COX-2/COX-1 双重抑制剂的复合物有利于癌症的化疗过程。在 15 种化合物中,我们发现芦他卡品的结合能力最高,为 ADV 网络服务器的-10.9;VX-809(Lumacaftor)的结合能力最高,为 ProdigY 网络服务器的-11.2。OSR、LMR 和 ECG 的疏水性最高,分别为 389.33、452.41 和 458.37,最常见的氨基酸为亮氨酸(338)、丝氨酸(339)、缬氨酸(509)和缬氨酸(335)。在摩尔折射率方面,OSR 和 LMR 的值分别为 92.01 和 113.98,而亲脂性分别为 2.46 和 3.08,毒性评分(通过 Toxi M 评分和 ProTox 评估)分别为 0.929 和 0.944(通过 Toxi M 评分和 ProTox 评估)和 4(通过 ProTox 评估)。疏水性、亲水性、分子量、H 键受体数、H 键供体数、摩尔折射率、亲油性(ilogP)、药物相容性和毒性评分等特征特性在理解药物与药物之间的分子水平相互作用方面发挥着重要作用,有助于确定药理作用及其在人体中的应用。因此,建议在该领域开展进一步研究,以了解药物反应及其结果。
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