An Alternative Pipeline for Glioblastoma Therapeutics: A Systematic Review of Drug Repurposing in Glioblastoma.

Seán B Lyne,Bakhtiar Yamini

doi:10.3390/cancers13081953

Abstract

Simple SummaryGlioblastoma is a devastating malignancy that has continued to prove resistant to a variety of therapeutics. No new systemic therapy has been approved for use against glioblastoma in almost two decades. This observation is particularly disturbing given the amount of money invested in identifying novel therapies for this disease. A relatively rapid and economical pipeline for identification of novel agents is drug repurposing. Here, a comprehensive review detailing the state of drug repurposing in glioblastoma is provided. We reveal details on studies that have examined agents in vitro, in animal models and in patients. While most agents have not progressed beyond the initial stages, several drugs, from a variety of classes, have demonstrated promising results in early phase clinical trials.The treatment of glioblastoma (GBM) remains a significant challenge, with outcome for most pa-tients remaining poor. Although novel therapies have been developed, several obstacles restrict the incentive of drug developers to continue these efforts including the exorbitant cost, high failure rate and relatively small patient population. Repositioning drugs that have well-characterized mechanistic and safety profiles is an attractive alternative for drug development in GBM. In ad-dition, the relative ease with which repurposed agents can be transitioned to the clinic further supports their potential for examination in patients. Here, a systematic analysis of the literature and clinical trials provides a comprehensive review of primary articles and unpublished trials that use repurposed drugs for the treatment of GBM. The findings demonstrate that numerous drug classes that have a range of initial indications have efficacy against preclinical GBM models and that certain agents have shown significant potential for clinical benefit. With examination in randomized, placebo-controlled trials and the targeting of particular GBM subgroups, it is pos-sible that repurposing can be a cost-effective approach to identify agents for use in multimodal anti-GBM strategies.

Highlights

Glioblastoma (GBM) is the most common primary malignant brain tumor worldwide and is the most lethal, with a median survival of approximately 15 months after diagnosis [1]
Repurposed drugs have a quicker approval time for an additional indication, and have over 50% cost reduction in comparison to novel drug development [6], observations that are exemplified by the success of prior spontaneous and planned repurposing discoveries [7]
The trial began in 2018 with plans to enroll 30 patients with a primary outcome of intratumoral ketoconazole and/or posaconazole concentration. Clioquinol is another topical antifungal being investigated in GBM [92,95]. These results suggest that there is some preclinical evidence for the potential use of azoles and clioquinol for GBM, their clinical safety and efficacy remain to be determined

Summary

Introduction

Glioblastoma (GBM) is the most common primary malignant brain tumor worldwide and is the most lethal, with a median survival of approximately 15 months after diagnosis [1]. The adjunctive use of tumor-treating field (TTF) technology has shown some survival benefit [3]. Despite this multimodal approach, overall survival (OS) and quality of life remain poor for patients with GBM [4,5]. Repurposed drugs are attractive as they already have well-established safety profiles and often require smaller cohorts for therapeutic efficacy analysis [6]. These factors help to streamline the passage of repurposed agents through the stringent FDA requirements for approval of novel agents. Repurposed drugs have a quicker approval time for an additional indication, and have over 50% cost reduction in comparison to novel drug development [6], observations that are exemplified by the success of prior spontaneous and planned repurposing discoveries [7]

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