Camptothecin Encapsulated in β-Cyclodextrin-EDTA-Fe3O4 Nanoparticles Induce Metabolic Reprogramming Repair in HT29 Cancer Cells through Epigenetic Modulation: A Bioinformatics Approach

Aisha Farhana; Avin Ee-Hwan Koh; Pooi Ling Mok; Abdullah Alsrhani; Yusuf Saleem Khan; Suresh Kumar Subbiah

doi:10.3390/nano11123163

Camptothecin Encapsulated in β-Cyclodextrin-EDTA-Fe₃O₄ Nanoparticles Induce Metabolic Reprogramming Repair in HT29 Cancer Cells through Epigenetic Modulation: A Bioinformatics Approach

Nanomaterials (Basel). 2021 Nov 23;11(12):3163. doi: 10.3390/nano11123163.

Authors

Aisha Farhana¹, Avin Ee-Hwan Koh², Pooi Ling Mok^{1

2}, Abdullah Alsrhani¹, Yusuf Saleem Khan³, Suresh Kumar Subbiah^{4

5

6}

Affiliations

¹ Department of Clinical Laboratory Sciences, College of Applied Medical Sciences, Jouf University, Sakaka 72388, Saudi Arabia.
² Department of Biomedical Science, Faculty of Medicine and Health Sciences, Universiti Putra Malaysia (UPM), Serdang 43400, Malaysia.
³ Department of Anatomy, College of Medicine, Jouf University, Sakaka 72388, Saudi Arabia.
⁴ Department of Medical Microbiology and Parasitology, Universiti Putra Malaysia (UPM), Serdang 43400, Malaysia.
⁵ Centre for Materials Engineering and Regenerative Medicine, Bharath Institute of Higher Education and Research, Bharath University, Selaiyur, Chennai 600073, India.
⁶ Institute of Bioscience, Universiti Putra Malaysia (UPM), Serdang 43400, Malaysia.

Abstract

Cancer progresses through a distinctive reprogramming of metabolic pathways directed by genetic and epigenetic modifications. The hardwired changes induced by genetic mutations are resilient, while epigenetic modifications are softwired and more vulnerable to therapeutic intervention. Colon cancer is no different. This gives us the need to explore the mechanism as an attractive therapeutic target to combat colon cancer cells. We have previously established the enhanced therapeutic efficacy of a newly formulated camptothecin encapsulated in β-cyclodextrin-EDTA-Fe₃O₄ nanoparticles (CPT-CEF) in colon cancer cells. We furthered this study by carrying out RNA sequencing (RNA-seq) to underscore specific regulatory signatures in the CPT-CEF treated versus untreated HT29 cells. In the study, we identified 95 upregulated and 146 downregulated genes spanning cellular components and molecular and metabolic functions. We carried out extensive bioinformatics analysis to harness genes potentially involved in epigenetic modulation as either the cause or effect of metabolic rewiring exerted by CPT-CEF. Significant downregulation of 13 genes involved in the epigenetic modulation and 40 genes from core metabolism was identified. Three genes, namely, DNMT-1, POLE3, and PKM-2, were identified as the regulatory overlap between epigenetic drivers and metabolic reprogramming in HT29 cells. Based on our results, we propose a possible mechanism that intercepts the two functional axes, namely epigenetic control, and metabolic modulation via CPT-CEF in colon cancer cells, which could skew cancer-induced metabolic deregulation towards metabolic repair. Thus, the study provides avenues for further validation of transcriptomic changes affected by these deregulated genes at epigenetic level, and ultimately may be harnessed as targets for regenerating normal metabolism in colon cancer with better treatment potential, thereby providing new avenues for colon cancer therapy.

Keywords: colon cancer; epigenetic modulation; metabolic reprogramming; nanoparticles; transcriptome analysis.

Grants and funding

375213500/Deputyship for Research and Innovation, Ministry of Education in Saudi Arabia