Title
Investigating Immune Profiles in Differentiated Thyroid Cancer by Multiplex Immunofluorescence
Files
Download Full Text (801 KB)
Presentation date
8-12-2021
College, Institute, or Department
Internal Medicine
Faculty Mentor
Anupam Kotwal MBBS
Research Mentor
Krysten Vance
Abstract
BACKGROUND: As the most common endocrine malignancy in the United States (U.S.), differentiated thyroid cancer (DTC) accounts for 3.8% of all cancers in the U.S., with roughly 10% of cases progressing to distant metastatic DTC, which is associated with a poor five year survival outcome despite conventional management, including surgery and radioactive iodine ablation. Recently, novel immunotherapies have garnered attention as a viable therapeutic resource for patients with advanced DTC. However, the response to therapy has been variable and unpredictable, which may be associated with an immune suppressive circulating phenotype. Nonetheless, the intra-tumoral immune infiltrate remains to be elucidated, demonstrating a critical need to address the gap in understanding in order to better prognosticate the disease.
OBJECTIVE: To identify and compare tumor-infiltrating immune markers with those present in the adjacent normal thyroid tissue, and collate these immune infiltrates with tumor characteristics.
METHODS: Twenty-nine adult tissue samples containing tumor and stromal regions were collected from patients with DTC. The samples were analyzed using multiplex immunofluorescence (MxIF) with antibodies against cell-surface molecules CD56, PD-1, PD-L1, FOXP3, CD3, CD8, CD4, CD45, CD68, CD163, INOS, HLA-DR, CD33, and CD19. 17 of the specimens were analyzed using HALO and a positive threshold was assigned based on review by a trained researcher.
RESULTS: In evaluating the immune profiles, important differences in the immune infiltrates between different stages of the cancer were observed. Generally, PD-1 and PD-L1 were highly expressed within the tumor, despite variability in lymphocyte infiltration, indicating the importance of PD-1 and PD-L1 as potential predictive biomarkers for the aggressiveness of thyroid cancer. Tumor from patients with distant metastases demonstrated higher T cell infiltration, T regulatory cells, macrophages and PD-L1 positive cells as compared to localized tumor.
CONCLUSION: Immune profiling demonstrated significant differences between tumor and adjacent healthy regions, particularly in terms of PD-1 and PD-L1 expression and lymphocyte infiltration, indicating that higher intratumor infiltration of T regulatory cells, macrophages and PD-1/PD-L1 positive cells may be associated with advanced thyroid cancer. Therefore, the data demonstrates the efficacy of MxIF in gathering valuable information regarding the tumor microenvironment, which will have major implications in guiding the selection of patients for immunotherapy.
Keywords
Differentiated thyroid cancer (DTC), multiplex immunofluorescence (MxIF), immunotherapy
Recommended Citation
Hajric, Kemal; Vance, Krysten BS; Martinez-Duarte, Ernesto MD; Yuil-Valdes, Ana MD; Hollingsworth, Michael PhD; Holzapfel, Melissa BS; Elhag, Salma; Fitch, Madelyn; Shats, Oleg; Goldner, Whitney MD; Ganti, Apar MD; Band, Hamid MD, PhD; Swanson, Benjamin MD, PhD; and Kotwal, Anupam MBBS, "Investigating Immune Profiles in Differentiated Thyroid Cancer by Multiplex Immunofluorescence" (2021). Posters: 2021 Summer Undergraduate Research Program. 38.
https://digitalcommons.unmc.edu/surp2021/38