Volatile profiling of Cinnamomum heyneanum and Cinnamomum Palghatensis and in vitro and in silico antidiabetic activity of essential oil nanoemulsions

Venkatraman Sriramavaratharajan , Ilamathi M-Thirusenthilarasan , Ramadas Nirupama , Vellingiri Vadivel , Vppalayam Shanmugam Pragadheesh , Velusamy Sundaresan , Ramar Murugan
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Abstract

Essential oil nanoemulsions (EONs) of two wild cinnamons, Cinnamomum heyneanum (CH) and Cinnamomum Palghatensis (CP), were formulated, characterized and investigated for their antidiabetic activity. Leaf essential oils (EOs) were extracted and characterized by GC-MS and GC-FID. Two sets of EONs were formulated and characterized by zeta analyzer, viscometer and TEM. Antioxidant activity was studied using DPPH, ABTS, superoxide, hydroxyl and hydrogen peroxide assays. Antidiabetic activity was evaluated by α-amylase inhibition, α-glucosidase inhibition, glucose uptake and glucose-stimulated insulin secretion assays. In silico studies were performed to support the efficacy. Methyl eugenol (60.3 %), safrole (27.8 %) in CH EO and bicyclogermacrene (19.5 %), (E)-caryophyllene (14 %) in CP EO were major components. Of two sets of EONs, 1:2 ratio showed better hydrodynamic average diameter [CH 42.9±0.78 nm & CP 27.9±1.70 nm] and better zeta potential [CH −38.4±0.85 mV & CP −38.4±0.45 mV (1st day)]. TEM observation showed that 1:2 ratio EONs were spherical with an average diameter of 85 nm (CH) and 8.98 nm (CP). Both CH and CP showed remarkable antioxidant activity. CP showed better α-glucosidase inhibition (IC50 0.599±0.008 mg/mL), enhanced glucose uptake (0.53±0.08 fold vs. control) and insulin secretion (1.40±0.06 fold vs. control). In silico analysis reveals that all major components of CH and CP interact with key residues of the protein targets associated with diabetes, α-amylase, α-glucosidase, insulin receptor, Glugagon like peptide1 Receptor and Glut 4. In vitro and in silico studies revealed that EON of CH and CP have pharmacological properties due to the presence of various compounds against diabetes mellitus.

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Cinnamomum heyneanum 和 Cinnamomum Palghatensis 的挥发性分析以及精油纳米乳剂的体外和硅学抗糖尿病活性
对两种野生肉桂(Cinnamomum heyneanum (CH) 和 Cinnamomum Palghatensis (CP))的精油纳米乳剂(EONs)进行了配制、表征和抗糖尿病活性研究。通过 GC-MS 和 GC-FID 对叶片精油(EOs)进行提取和表征。配制了两组 EONs,并通过 zeta 分析仪、粘度计和 TEM 进行了表征。使用 DPPH、ABTS、超氧化物、羟基和过氧化氢检测法研究了抗氧化活性。通过α-淀粉酶抑制、α-葡萄糖苷酶抑制、葡萄糖摄取和葡萄糖刺激胰岛素分泌试验评估了抗糖尿病活性。为证实其功效,还进行了硅学研究。CH 环氧乙烷中的主要成分是甲基丁香酚(60.3%)和黄樟素(27.8%),而 CP 环氧乙烷中的主要成分是双环己二烯(19.5%)和(E)-石竹烯(14%)。在两组环氧乙烷中,1:2 的比例显示出更好的流体力学平均直径[CH 42.9±0.78 nm & CP 27.9±1.70 nm]和更好的 zeta 电位[CH -38.4±0.85 mV & CP -38.4±0.45 mV(第一天)]。TEM观察显示,1:2比例的EON呈球形,平均直径为85 nm(CH)和8.98 nm(CP)。CH和CP都显示出显著的抗氧化活性。CP 对α-葡萄糖苷酶有更好的抑制作用(IC50 0.599±0.008 mg/mL),葡萄糖摄取量(比对照组高 0.53±0.08 倍)和胰岛素分泌量(比对照组高 1.40±0.06 倍)均有所提高。硅学分析表明,CH 和 CP 的所有主要成分都能与α-淀粉酶、α-葡萄糖苷酶、胰岛素受体、胰高血糖素样肽 1 受体和 Glut 4 等与糖尿病相关的蛋白质靶点的关键残基相互作用。 体外和硅学研究表明,CH 和 CP 的 EON 具有药理特性,因为其中含有多种防治糖尿病的化合物。
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