Single-cell image analysis reveals over-expression of organic anion transporting polypeptides (OATPs) in human glioblastoma tissue

Author:

Cooper Elizabeth1234,Woolf Zoe12,Swanson Molly E V5,Correia Jason26,Schweder Patrick26,Mee Edward26ORCID,Heppner Peter6ORCID,Turner Clinton27ORCID,Faull Richard L M2,Scotter Emma L5,Denny William A3,Choi Peter J3,Dragunow Mike124ORCID,Jose Jiney3,Park Thomas I-H124ORCID

Affiliation:

1. Department of Pharmacology, University of Auckland , Auckland , New Zealand

2. Neurosurgical Research Unit, The Centre for Brain Research, University of Auckland , Auckland , New Zealand

3. Auckland Cancer Society Research Centre, University of Auckland , Auckland , New Zealand

4. The Hugh Green Biobank, University of Auckland , Auckland , New Zealand

5. Department of Biological Sciences, University of Auckland , Auckland , New Zealand

6. Department of Neurosurgery, Auckland City Hospital , Auckland , New Zealand

7. Department of Anatomical Pathology, LabPlus, Auckland City Hospital , Auckland , New Zealand

Abstract

Abstract Background Glioblastoma (GBM) is the most common and aggressive primary brain tumor in adults. Whilst the role of the efflux transporters are well established in GBM, the expression and function of uptake transporters, such as the organic anion transporting polypeptide (OATP) family, are not well understood. OATPs possess broad substrate specificity that includes anti-cancer agents; therefore, we sought to investigate the expression of four OATP isoforms in human GBM cell types using patient tumor tissue. Methods We used fluorescent immunohistochemical labeling of paraffin-embedded surgically resected tissues and single-cell image analysis methods to explore the expression of the OATP isoforms in different tumor cell types through co-labeling with cell-type specific markers, such as IBA1 (pan-myeloid), GFAP (tumor cell), PDGFRβ (stromal cell), and UEA-1-lectin (endothelial). Results We found significant over-expression of all the OATP isoforms (OATP1A2, 2B1, 1C1 and 4A1) in GBM tumor sections when compared to non-neoplastic brain. A single-cell image analysis revealed that OATPs were significantly upregulated throughout the tumor parenchyma, with significantly higher expression found on lectin-positive blood vessels and IBA1-positive myeloid cells in GBM compared to non-tumor brain tissue. Qualitative analysis of the four OATP isoforms demonstrated greater expression of OATP4A1 in peri-necrotic regions of GBM tissue, which correlated with hypoxia-related markers within the Ivy GAP RNAseq dataset. Conclusion Here, we demonstrate, for the first time, the protein expression of four OATPs in human GBM tissue, including upregulation within the tumor microenvironment by myeloid cells and tumor vasculature, and isoform-specific upregulation within hypoxic niches.

Publisher

Oxford University Press (OUP)

Subject

Electrical and Electronic Engineering,Building and Construction

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