Potential mechanistic profiling of an OTC analgesic as a cytotoxic agent in the treatment of hepatocellular carcinoma
ACTA Pharmaceutica Sciencia • 2018
معلومات البحث
المؤلفون
Marwa E. Sayour , Ibrahim Basheer, Rania Abd El Salam, Mohamed El Yamany, Amr Badr, Ahmed Farouk Al-Sadek, Raafat El-Awady
الكلمات المفتاحية
Paracetamol; Cyclooxygenase 1; Cyclin Dependent kinase 2; Breast Cancer Type 2 Susceptibility Protein; Molecular Docking
المجلة العلمية
ACTA Pharmaceutica Sciencia
الناشر
Not Available
المجلد
56
العدد
1
الصفحات
Not Available
publication.type
International
رابط البحث
Open Link
المواد المرفقة
Not Available
الملخص
While being a safe over the counter drug, paracetamol has also proved to be a cytotoxic agent for cultured hepatocellular carcinoma cells (HepG2). In order to understand the biochemical mechanisms underlying its cytotoxic ability, molecular docking of paracetamol with cyclin dependent kinase 2 protein (CDK2) and breast cancer type 2 susceptibility protein (BRCA2) plus cyclooxygenase 1 (COX1) enzyme protein was undergone. Computational simulation was performed using Schrödinger software to describe the details of binding between atoms of the active sites and paracetamol. All COX1, CDK2 and BRCA2 proteins showed binding scores with paracetamol. Their G-scores were -5.32, -5.61 and -6.08 respectively leading to selective inhibition of these proteins and loss of their cell cycle related activity. The binding strength of COX1 and CDK2 with paracetamol was mainly dependent on the hydrophobic residues, while that of BRCA2 was contributed to charged residues. Binding is responsible for the subsequent loss of activity of these cell cycle related proteins and eventual cancer cell death via apoptosis.
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