Insilico Validation of Selected Natural Products as Multi-regulator of EZH2-PPAR Therapeutic Targets; A Hallmark for Prospective Restoration of Pancreatic Insulin Production and Cancer dysregulation

Author:

Olowosoke Christopher Busayo1ORCID,Gbemisola Otitoola Shobi2,Alaba Adebola Abosede1,Adepoju Oluwadamilola Hope3,Okorie Benson1,Odjegba Peace Ifeoma1,Ogunsanmi Ayomide Oluwaseyi4,Oke Grace Ayomide1,Akinlolu Oluwatoyin1,Olubena Tomiwa Lois1,Bello Ridwan Opeyemi1,Adegboyega Benjamin Babatunde1

Affiliation:

1. Federal University of Technology Akure

2. University of Ibadan College of Medicine

3. Federal University of Agriculture Abeokuta

4. Kwara State University

Abstract

Abstract The prevalence of cancer and diabetes has been a major global threat that has led to the continuous investigation of numerous biomarker that can serve in novel therapeutic targets for their treatment. Recently, epigenetic regulatory function of EZH2-PPAR was discovered to influence the metabolic and signaling pathway causing this disease. Hence, the synergistic combination of inhibitors like GSK126 and Bezafibrate was reported have promising outcome for these disease treatment, but without clear understanding of other biomarker association and side effect detriment. The disease association and protein interaction networks between EZH2-PPARs and other biomarkers regulating pancreatic cancer and diabetes pathology were identified, with obesity, and hypertensive disease being the closest vast connection. Natural compounds employed in the molecular docking, adme/toxicity and reactivity screening for candidate inhibitor of versatile capacity against the target identify nine compounds as lead hits. Overall, Phytocassane A exhibit the most recognizable insilico validation for drug likeness profiles better than the standards, and all nine compounds were conclusively proposed for further experimental screening to compliment this finding on their benefit in drug development for diabetes and cancer therapy.

Publisher

Research Square Platform LLC

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