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Article Abstract
Objectives: The prevalence of microsatellite instability (MSI) subtype among all colon cancers in India is about 30 %, approximately two times more than that of western population suggesting different molecular pathogeneses.
Methods: A analysis-based Pan cancer differential expression (DE) profile was determined in a primary cohort of early-stage CRC (tumor=10, normal=7), and correlated against MSI status. Using RT-PCR, tumor-specific genes were validated in another cohort of MSI-high CRC (n=15).
Results: Among the most differentially expressed genes, , and were tumor cell-specific signals, while a set of genes including , , , , , , and others were immune cell-specific signals, that had a differential expression between MSI and MSS groups. When overlapped with The Cancer Genome Atlas (TCGA) studies using the Tumor immune estimation resource tool (TIMER), and protein-protein interaction analysis by STRING.db, these genes were segregated to representative tumor cells and immune cells. On validation, the tumor-specific gene signals were inversely associated with expression.
Conclusions: The differential expression distribution of , , and among tumor and immune cells, suggests more than one pathological subset in the MSI-H subgroup of early-stage CRC in the Indian population.
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| http://dx.doi.org/10.1515/dmpt-2024-0033 | DOI Listing |
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