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An analysis of sexual dimorphism in the tumor microenvironment of colorectal cancer. | LitMetric

AI Article Synopsis

  • * The study found higher proportions of CD4+ T cells in women’s tumor and lymph node samples, while CD8+ T cells were more prevalent in their uninvolved colon compared to men.
  • * Differential gene expression related to immune functions was observed in women, suggesting that these immune system disparities may explain the survival advantages seen in female CRC patients.

Article Abstract

Women with colorectal cancer (CRC) have survival advantages over men, yet the underlying mechanisms are unclear. T cell infiltration within the CRC tumor microenvironment (TME) correlates strongly with survival. We hypothesized that women with CRC have increased T cell infiltration and differential gene expression in the TME compared to men. Tissue microarrays comprising primary tumor, tumor infiltrated lymph nodes, and uninvolved colon were created from CRC patients. Proportions of CD4 positive (CD4+) and CD8 positive (CD8+) T cells were identified using immunohistochemistry. TME immune- and cancer-related genetic expression from primary and metastatic CRC tumor were also evaluated the NanoStringIO360 panel and The Cancer Genome Atlas Project database. CD4+ was higher in tumor samples from women compared to men (22.04% vs. 10.26%, p=0.002) and also in lymph node samples (39.54% vs. 8.56%, p=0.001). CD8+ was increased in uninvolved colon from women compared to men (59.40% vs. 43.61%, p=0.015), and in stage I/II tumors compared to III/IV in all patients (37.01% vs. 23.91%, p=0.009). Top CD8+ tertile patients survived longer compared to the bottom (43.9 months vs. 25.3 months, p=0.007). Differential gene expression was observed in pathways related to Treg function, T cell activity, and T cell exhaustion, amongst several others, in women compared to men. Thus, significant sexual dimorphism exists in the TME that could contribute to survival advantages observed in female patients with CRC.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC9651089PMC
http://dx.doi.org/10.3389/fonc.2022.986103DOI Listing

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