PSMA Expression in Glioblastoma as a Basis for Theranostic Approaches: A Retrospective, Correlational Panel Study Including Immunohistochemistry, Clinical Parameters and PET Imaging

Adrien Holzgreve,Nathalie L Albert,Viktoria C Ruf,Peter Bartenstein,Lena Mittlmeier,Jörg-Christian Tonn,Jürgen Schlegel,Annamaria Biczok,Marcus Unterrainer,Friederike Liesche-Starnecker,Bogdana Suchorska,Maximilian A Kirchner,Jochen Herms,Katja Steiger

doi:10.3389/fonc.2021.646387

Abstract

AimThe aim of the current study was to enlighten the evolution of prostate-specific membrane antigen (PSMA) expression in glioblastoma between initial diagnosis and recurrence in order to provide preliminary insight for further clinical investigations into innovative PSMA-directed treatment concepts in neuro-oncology.MethodsPatients who underwent resection for de-novo glioblastoma (GBM) and had a re-resection in case of a recurrent tumor following radiochemotherapy and subsequent chemotherapy were included (n = 16). Histological and immunohistochemical stainings were performed at initial diagnosis and at recurrence (n = 96 tissue specimens). Levels of PSMA expression both in endothelial and non-endothelial cells as well as vascular density (CD34) were quantified via immunohistochemistry and changes between initial diagnosis and recurrence were determined. Immunohistochemical findings were correlated with survival and established clinical parameters.ResultsPSMA expression was found to be present in all GBM tissue samples at initial diagnosis as well as in all but one case of recurrent tumor samples. The level of PSMA expression in glioblastoma varied inter-individually both in endothelial and non-endothelial cells. Likewise, the temporal evolution of PSMA expression highly varied in between patients. The level of vascular PSMA expression at recurrence and its change between initial diagnosis and recurrence was associated with post recurrence survival time: Patients with high vascular PSMA expression at recurrence as well as patients with increasing PSMA expression throughout the disease course survived shorter than patients with low vascular PSMA expression or decreasing vascular PSMA expression. There was no significant correlation of PSMA expression with MGMT promoter methylation status or Ki-67 labelling index.ConclusionPSMA is expressed in glioblastoma both at initial diagnosis and at recurrence. High vascular PSMA expression at recurrence seems to be a negative prognostic marker. Thus, PSMA expression in GBM might present a promising target for theranostic approaches in recurrent glioblastoma. Especially PSMA PET imaging and PSMA-directed radioligand therapy warrant further studies in brain tumor patients.

Highlights

Prostate-specific membrane antigen (PSMA) is a well characterized and validated marker for prostate cancer
We demonstrate in a homogeneously treated glioblastoma patient cohort that PSMA
PSMA is a promising target for theranostic approaches in glioblastoma

Summary

Introduction

Prostate-specific membrane antigen (PSMA) is a well characterized and validated marker for prostate cancer. Its naming is misleading, since PSMA expression is restricted to carcinomas of the prostate alone: Early reports have already shown that some tissues such as salivary glands have a physiological expression of PSMA and that monoclonal antibodies to the extracellular domain of PSMA strongly react with the tumor vasculature in a variety of other cancers including lung, breast and colon carcinoma [8,9,10]. Malignant central nervous system tumors have not been studied in those early investigations on PSMA expression in non-prostatic cancers – at first, only a single case of a glioblastoma patient had been analyzed and the tumor was found to express. Several immunohistopathological studies confirmed PSMA expression in the tumoral vessels of high grade gliomas [12,13,14,15,16]

Objectives

Methods

Results

Discussion

Conclusion