Revealing curcumin therapeutic targets on SRC, PPARG, MAPK8 and HSP90 as liver cirrhosis therapy based on comprehensive bioinformatic study

Khalish Arsy Al Khairy Siregar; Putri Hawa Syaifie; Muhammad Miftah Jauhar; Adzani Gaisani Arda; Nurul Taufiqu Rochman; Paula Mariana Kustiawan; Etik Mardliyati

doi:10.1080/07391102.2023.2301534

Revealing curcumin therapeutic targets on SRC, PPARG, MAPK8 and HSP90 as liver cirrhosis therapy based on comprehensive bioinformatic study

J Biomol Struct Dyn. 2024 Jan 12:1-18. doi: 10.1080/07391102.2023.2301534. Online ahead of print.

Authors

Khalish Arsy Al Khairy Siregar^{1

2}, Putri Hawa Syaifie², Muhammad Miftah Jauhar², Adzani Gaisani Arda², Nurul Taufiqu Rochman^{2

3}, Paula Mariana Kustiawan¹, Etik Mardliyati^{2

4}

Affiliations

¹ Faculty of Pharmacy, Universitas Muhammadiyah Kalimantan Timur, Samarinda, Indonesia.
² Center of Excellence Life Sciences, Nano Center Indonesia, South Tangerang, Indonesia.
³ Research Center for Advanced Material, National Research and Innovation Agency (BRIN), South Tangerang, Indonesia.
⁴ Research Center for Vaccine and Drug, National Research and Innovation Agency (BRIN), Bogor, Indonesia.

PMID: 38217310
DOI: 10.1080/07391102.2023.2301534

Abstract

Cirrhosis naturally progresses through three stages: compensated, decompensated, and late decompensated, which carry an elevated risk of death. Although curcumin's anti-cirrhosis effects have been studied, underlying mechanism in preventing cirrhosis progression and the correlation between curcumin's action with upregulated genes remains insufficiently explored. In this study, we employed network pharmacology approach to construct a drug-target-disease network through bioinformatics and validate the findings with molecular docking and dynamic simulation. The curcumin-targeted liver cirrhosis network encompassed 54 nodes with 282 edges in protein-protein interactions (PPI) network. By utilizing network centrality analysis, we identified eight crucial genes. KEGG enrichment pathway revealed that these crucial genes are involved in pathway of cancer, endocrine resistance, estrogen signaling, chemical carcinogenesis-receptor activation, lipid metabolism, and atherosclerosis. Notably, these eight genes predominantly participate in cancer-related pathways. Further investigation revealed upregulation of four genes and downregulation of four others in hepatocellular carcinoma patients. These upregulated genes-MAPK8, SRC, PPARG, and HSP90AA1-strongly correlated with reduced survival probability in liver hepatocellular carcinoma patients with survival times approximately under 4000 days (∼11 years). Molecular docking and molecular dynamic results exhibited curcumin's superior binding affinities and stability compared to native ligands of MAPK8, SRC, PPARG, and HSP90AA1 within 50 ns simulations. Moreover, MM-GBSA analysis showed stronger binding energy of curcumin to MAPK8, SRC, and HSP90AA1 than native ligand. In conclusion, this study provides valuable insights into curcumin's potential mechanisms in preventing liver cirrhosis progression, specifically in HCC. These findings offer a theoretical basis for further pharmacological research into anti-HCC effect of curcumin.Communicated by Ramaswamy H. Sarma.

Keywords: Liver cirrhosis; curcumin; molecular docking; molecular dynamic; network pharmacology.