Exploring Spatial Heterogeneity of Immune Cells in Nasopharyngeal Cancer

Aastha Sobti; Christina Sakellariou; Johan S Nilsson; David Askmyr; Lennart Greiff; Malin Lindstedt

doi:10.3390/cancers15072165

Exploring Spatial Heterogeneity of Immune Cells in Nasopharyngeal Cancer

Cancers (Basel). 2023 Apr 5;15(7):2165. doi: 10.3390/cancers15072165.

Authors

Aastha Sobti¹, Christina Sakellariou¹, Johan S Nilsson^{2

3}, David Askmyr^{2

3}, Lennart Greiff^{2

3}, Malin Lindstedt¹

Affiliations

¹ Department of Immunotechnology, Lund University, 223 81 Lund, Sweden.
² Department of ORL, Head & Neck Surgery, Skåne University Hospital, 221 85 Lund, Sweden.
³ Department Clinical Sciences, Lund University, 221 00 Lund, Sweden.

Abstract

Nasopharyngeal cancer (NPC) is a malignant tumor. In a recent publication, we described the presence and distribution of CD8⁺ T cells in NPC and used the information to identify 'inflamed', 'immune-excluded', and 'desert' immune phenotypes, where 'inflamed' and 'immune-excluded' NPCs were correlated with CD8 T cell infiltration and survival. Arguably, more detailed and, in particular, spatially resolved data are required for patient stratification and for the identification of new treatment targets. In this study, we investigate the phenotype of CD45⁺ leukocytes in the previously analyzed NPC samples by applying multiplexed tissue analysis to assess the spatial distribution of cell types and to quantify selected biomarkers. A total of 47 specified regions-of-interest (ROIs) were generated based on CD45, CD8, and PanCK morphological staining. Using the GeoMx^® Digital Spatial Profiler (DSP), 49 target proteins were digitally quantified from the selected ROIs of a tissue microarray consisting of 30 unique NPC biopsies. Protein targets associated with B cells (CD20), NK cells (CD56), macrophages (CD68), and regulatory T cells (PD-1, FOXP3) were most differentially expressed in CD45⁺ segments within 'immune-rich cancer cell islet' regions of the tumor (cf. 'surrounding stromal leukocyte' regions). In contrast, markers associated with suppressive populations of myeloid cells (CD163, B7-H3, VISTA) and T cells (CD4, LAG3, Tim-3) were expressed at a higher level in CD45⁺ segments in the 'surrounding stromal leukocyte' regions (cf. 'immune-rich cancer cell islet' regions). When comparing the three phenotypes, the 'inflamed' profile (cf. 'immune-excluded' and 'desert') exhibited higher expression of markers associated with B cells, NK cells, macrophages, and myeloid cells. Myeloid markers were highly expressed in the 'immune-excluded' phenotype. Granulocyte markers and immune-regulatory markers were higher in the 'desert' profile (cf. 'inflamed' and 'immune-excluded'). In conclusion, this study describes the spatial heterogeneity of the immune microenvironment in NPC and highlights immune-related biomarkers in immune phenotypes, which may aid in the stratification of patients for therapeutic purposes.

Keywords: biomarker discovery; digital spatial profiling; immune cells; immune phenotypes; nasopharyngeal cancer; spatial omics.

Abstract

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