Association of Microsatellite Instability and Gene Expression Profile in Colorectal Carcinoma and Potential Implications for Therapy

Muhammad G Kibriya; Farzana Jasmine; Yuliia Khamkevych; Maruf Raza; Mohammed Kamal; Marc Bissonnette; Habibul Ahsan

doi:10.3390/medicina60030348

Association of Microsatellite Instability and Gene Expression Profile in Colorectal Carcinoma and Potential Implications for Therapy

Medicina (Kaunas). 2024 Feb 20;60(3):348. doi: 10.3390/medicina60030348.

Authors

Muhammad G Kibriya^{1

2}, Farzana Jasmine¹, Yuliia Khamkevych¹, Maruf Raza³, Mohammed Kamal⁴, Marc Bissonnette⁵, Habibul Ahsan^{1

2}

Affiliations

¹ Institute for Population and Precision Health, Biological Sciences Division, The University of Chicago, Chicago, IL 60637, USA.
² Department of Public Health Sciences, Biological Sciences Division, The University of Chicago, Chicago, IL 60637, USA.
³ Department of Pathology, Jahurul Islam Medical College, Kishoregonj 2336, Bangladesh.
⁴ Department of Pathology, The Laboratory, Dhaka 1205, Bangladesh.
⁵ Department of Medicine, The University of Chicago, Chicago, IL 60637, USA.

Abstract

Background and Objective: In sporadic colorectal carcinomas (CRC), microsatellite instability (MSI) pathways play important roles. Previously, we showed differences in DNA methylation patterns in microsatellite stable (MSS) colorectal carcinomas and MSI-CRC. In the current study, we explore the similarities and differences in gene expression profiles in MSS and MSI at the gene level and at the pathway level to better understand CRC pathogenesis and/or the potential for therapeutic opportunities. Material and Methods: Seventy-one CRC patients (MSI = 18, MSS = 53) were studied. Paired tumor and adjacent normal tissues were used for genome-wide gene expression assays. Result: At the gene level, we compared the list of differentially expressed genes (fold change (FC) ≥ 3 and FDR < 0.05) in tumor tissues compared to corresponding normal tissue in CRC patients with MSI tumors (190 genes) and MSS tumors (129 genes). Of these, 107 genes overlapped. The list of genes that were differentially expressed in MSI tumors only showed enrichment predominantly in two broad categories of pathways-(a) Inflammation-related pathways including the interleukin-17 (IL-17) signaling pathway, tumor necrosis factor (TNF) signaling pathway, chemokine signaling, nuclear factor kappa B (NFκB) signaling, and cytokine-cytokine interactions, and (b) metabolism-related pathways, including retinol metabolism, steroid hormone biosynthesis, drug metabolism, pentose and glucoronate interconversions, and ascorbate and aldarate metabolism. The genes in inflammation-related pathways were up-regulated whereas genes in metabolism-related pathways were down-regulated in MSI tumor tissue. Pathway-level analysis also revealed similar results confirming the gene enrichment findings. For example, the 150 genes involved in the IL-17 signaling pathway were on average up-regulated by 1.19 fold (CI 1.16-1.21) in MSI compared to 1.14 fold (CI 1.13-1.16) in MSS patients (interaction p = 0.0009). Conclusions: We document an association between MSI status and differential gene expression that broadens our understanding of CRC pathogenesis. Furthermore, targeting one or more of these dysregulated pathways could provide the basis for improved therapies for MSI and MSS CRC.

Keywords: IL-17 signaling; MMR deficiency; MSI; colorectal cancer; gene expression; immune check point inhibitors.

MeSH terms

Colorectal Neoplasms* / genetics
Colorectal Neoplasms* / pathology
Humans
Inflammation / genetics
Interleukin-17 / genetics
Microsatellite Instability*
Microsatellite Repeats
Transcriptome / genetics

Substances

Interleukin-17

Abstract

MeSH terms

Substances

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