A theoretical approach on ADMET properties of an azo-ester based fluorophore (AEF), and it's energetics, binding stability and molecular interactions with select globular proteins

Q1 Social Sciences South African Journal of Chemical Engineering Pub Date : 2024-07-01 DOI:10.1016/j.sajce.2024.06.003

Arumugam Gopalakrishnan , Ravichandran Keerthiga , Murugan Sreedevi Sangeetha , Seba Merin Vinod , Perumal Tamizhdurai , V.L. Mangesh , Rajaraman Vasanthi , Vaidyanathan Rajagopalan , Rajendran Kumaran , Mahalingam Vanjinathan

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Abstract

Molecular docking (Mol.Doc) approach of an azo-ester based fluorophore (AEF) with widely studied proteins like Human serum Albumin (HSA), Bovine serum Albumin (BSA), Beta lactoglobin (βLG) and Ovalbumin (OVA) were carried out. The binding affinity and strength of AEF-HSA complex is due to hydrogen-bonding (h-bonding) and hydrophobic interactions (predominantly attributed to pi-alkyl). AEF and HSA acts as h-bonding acceptor as well as donor. The energetically favored conformers of AEF-HSA complex are governed and stabilized by polar as well as non-polar amino acids. On the contrary, the pattern observed in all the conformers of AEF-BSA, AEF- βLG and AEF-OVA are energetically least favored (+ve ∆G) compared to that of HSA. The least binding affinity of AEF is towards OVA (Binding energy (BE) +581.15 Kcalmol⁻¹ followed by βLG (+55.11) and BSA (+12.12) . Though BSA and HSA are structurally similar to each other, they vary in the binding stability with AEF. This is attributed to several unfavorable interactions that destabilize AEF-BSA complex which was not resulted in the complex existing between AEF-HSA. The energetically least stable complexes (AEF-BSA, AEF-βLG and AEF-OVA) are predominantly governed by hydrophobic interactions. However, several h-bonding interactions along with pi-sigma/pi-pi/pi-alkyl interactions result in destabilization of the above complexes. Interestingly, AEF-HSA complex stability is attributed to fewer number of hydrophobic interactions along with h-bonding interactions. The h-bonding interaction governs the stability of the complex which is the driving force. Docking studies illustrates that the binding of amino acids (AAs) in various subdomains play a significant role on the binding nature. The stability of AEF-HSA over other protein complexes in terms of BE is emphasized in the study. The energetically stable sites and sub-domains of AEF with HSA and BSA establish the site selective and site-specific nature of AEF with proteins. In silico studies provide an excellent and easier approach in establishing the molecular interactions existing between AEF with globular proteins. ADMET parameters of the guest molecule calculated exemplifies that AEF compound is less toxic and possesses high oral bioavailability. Based on the binding efficiency of AEF with albumins, the ADMET properties and drug likeliness approach of AEF provides an information on the application towards proteins in the concept of medicine and chemistry.

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基于偶氮酯的荧光团 (AEF) 的 ADMET 特性及其与特定球蛋白的能量、结合稳定性和分子相互作用的理论方法

研究人员采用分子对接（Mol.Doc）方法，将偶氮酯类荧光团（AEF）与人血清白蛋白（HSA）、牛血清白蛋白（BSA）、β-乳红蛋白（βLG）和卵清蛋白（OVA）等广泛研究的蛋白质进行了对接。AEF-HSA 复合物的结合亲和力和强度是由于氢键（h-bonding）和疏水相互作用（主要归因于 pi-alkyl ）。AEF 和 HSA 既是氢键受体，也是氢键供体。AEF-HSA 复合物的能量优势构象受极性和非极性氨基酸的支配和稳定。相反，与 HSA 相比，在 AEF-BSA、AEF- βLG 和 AEF-OVA 的所有构象中观察到的模式在能量上都是最不利的（+ve ∆G）。AEF 与 OVA 的结合亲和力最小（结合能（BE）+581.15 Kcalmol-1），其次是 βLG（+55.11）和 BSA（+12.12）。虽然 BSA 和 HSA 结构相似，但它们与 AEF 的结合稳定性却各不相同。这是由于一些不利的相互作用破坏了 AEF-BSA 复合物的稳定性，而 AEF-HSA 之间的复合物却没有发生这种作用。能量上最不稳定的复合物（AEF-BSA、AEF-βLG 和 AEF-OVA）主要受疏水相互作用的影响。然而，一些 h 键相互作用以及 pi-sigma/pi-pi/pi-alkyl 相互作用导致上述复合物不稳定。有趣的是，AEF-HSA 复合物的稳定性归因于较少的疏水相互作用和 h 键相互作用。h 键相互作用决定了复合物的稳定性，而这种作用是复合物的驱动力。对接研究表明，氨基酸（AA）在不同子域中的结合对结合性质起着重要作用。与其他蛋白质复合物相比，AEF-HSA 在 BE 方面的稳定性在研究中得到了强调。AEF 与 HSA 和 BSA 的能量稳定位点和亚域确定了 AEF 与蛋白质结合的位点选择性和位点特异性。硅学研究为确定 AEF 与球蛋白之间存在的分子相互作用提供了一种极好且更简便的方法。计算出的客体分子 ADMET 参数表明，AEF 复合物毒性较低，口服生物利用度高。基于 AEF 与白蛋白的结合效率，AEF 的 ADMET 特性和药物相容性方法为蛋白质在医学和化学概念中的应用提供了信息。

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来源期刊

South African Journal of Chemical Engineering Social Sciences-Education

CiteScore

8.40

自引率

0.00%

发文量

100

审稿时长

33 weeks

期刊介绍： The journal has a particular interest in publishing papers on the unique issues facing chemical engineering taking place in countries that are rich in resources but face specific technical and societal challenges, which require detailed knowledge of local conditions to address. Core topic areas are: Environmental process engineering • treatment and handling of waste and pollutants • the abatement of pollution, environmental process control • cleaner technologies • waste minimization • environmental chemical engineering • water treatment Reaction Engineering • modelling and simulation of reactors • transport phenomena within reacting systems • fluidization technology • reactor design Separation technologies • classic separations • novel separations Process and materials synthesis • novel synthesis of materials or processes, including but not limited to nanotechnology, ceramics, etc. Metallurgical process engineering and coal technology • novel developments related to the minerals beneficiation industry • coal technology Chemical engineering education • guides to good practice • novel approaches to learning • education beyond university.