Implantable polymers for tirapazamine treatments of experimental intracranial malignant glioma

Yuan, Xuan; Tabassi, Kevin; Williams, Jeffery A.

doi:10.1002/(sici)1520-6823(1999)7:4<218::aid-roi3>3.0.co;2-c

Cited by 13 publications

(4 citation statements)

References 43 publications

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“…For various reasons, the surge of research in PCPP:SA wafer technology for delivering antitumor drugs abated when the TMZ standard-of-care model emerged, perhaps because of growing interest in other local delivery systems such as convection-enhanced delivery of drugs and gene transfer. Before 2008, antitumor agents that were incorporated into PCPP:SA wafers and studied in rodent glioma models included paclitaxel, 46 camptothecin, 47,48 hydroperoxycyclophosphamide, 49 tirapazamine, 50 and 5-iodo-2V deoxyuridine. 51,52 It was even found by Brem et al that local delivery of TMZ by means of PCPP:SA wafers in a rodent glioma model was superior to oral TMZ in terms of median survival.…”

Section: Introduction and Rationalementioning

confidence: 99%

Polymeric drug delivery for the treatment of glioblastoma

et al. 2015

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Section: Introduction and Rationalementioning

confidence: 99%

Polymeric drug delivery for the treatment of glioblastoma

et al. 2015

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“…These PLGA wafers used a pre-encapsulation process and reported 25% long-term survivors (survived >120 days compared to median survival of 28 days) in the F344 rat model [ 141 ]. Other chemotherapeutic agents that have been explored for sustained local delivery via polymeric implants include taxol, camptothecin, minocycline, doxorubicin, and others [ 142 , 143 , 144 , 145 , 146 , 147 , 148 , 149 , 150 , 151 , 152 , 153 , 154 , 155 , 156 ]. Novel polymeric implants and microchips can be used to deliver several drugs locally at varying time points in a controlled manner, and various formulations such as nanoparticles, liposomes, and microparticles can also be delivered via these implants.…”

Section: Invasive Technologiesmentioning

confidence: 99%

Addressing BBB Heterogeneity: A New Paradigm for Drug Delivery to Brain Tumors

et al. 2020

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Effective treatments for brain tumors remain one of the most urgent and unmet needs in modern oncology. This is due not only to the presence of the neurovascular unit/blood–brain barrier (NVU/BBB) but also to the heterogeneity of barrier alteration in the case of brain tumors, which results in what is referred to as the blood–tumor barrier (BTB). Herein, we discuss this heterogeneity, how it contributes to the failure of novel pharmaceutical treatment strategies, and why a “whole brain” approach to the treatment of brain tumors might be beneficial. We discuss various methods by which these obstacles might be overcome and assess how these strategies are progressing in the clinic. We believe that by approaching brain tumor treatment from this perspective, a new paradigm for drug delivery to brain tumors might be established.

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“…For example, when inulin, a large molecule that has less potential to cross the blood–brain barrier, is administered by wafer technology, the inulin persists in the brain for a longer period of time and diffuses a larger distance from the brain/polymer interface. The feasibility of polifeprosan 20 polymer as a slow release delivery technology for alternative therapeutic agents has been demonstrated in preclinical models using paclitaxel,60 IUDR,61,62 temozolomide,63 taxotere64 camptothecin,65,66 tiripazamine,67 and other agents. When more effective agents are identified, this may be considered again.…”

Section: Wafer Technology: Possible Renewed Interest In the Future?mentioning

confidence: 99%

Polifeprosan 20, 3.85% carmustine slow release wafer in malignant glioma: patient selection and perspectives on a low-burden therapy

Kleinberg¹

2016

PPA

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Polifeprosan 20 with carmustine (GLIADEL®) polymer implant wafer is a biodegradable compound containing 3.85% carmustine (BCNU, bischloroethylnitrosourea) implanted in the brain at the time of planned tumor surgery, which then slowly degrades to release the BCNU chemotherapy directly into the brain thereby bypassing the blood–brain barrier. Carmustine implant wafers were demonstrated to improve survival in randomized placebo-controlled trials in patients undergoing a near total resection of newly diagnosed or recurrent malignant glioma. Based on these trials and other supporting data, carmustine wafer therapy was approved for use for newly diagnosed and recurrent malignant glioma in the United States and the European Union. Adverse events are uncommon, and as this therapy is placed at the time of surgery, it does not add to patient treatment burden. Nevertheless, this therapy appears to be underutilized. This article reviews the evidence for a favorable therapeutic ratio for the patient and the potential barriers. Consideration of these issues is important for optimal use of this therapeutic approach and may be important as this technology and other local therapies are further developed in the future.

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Implantable polymers for tirapazamine treatments of experimental intracranial malignant glioma

Cited by 13 publications

References 43 publications

Polymeric drug delivery for the treatment of glioblastoma

Polymeric drug delivery for the treatment of glioblastoma

Addressing BBB Heterogeneity: A New Paradigm for Drug Delivery to Brain Tumors

Polifeprosan 20, 3.85% carmustine slow release wafer in malignant glioma: patient selection and perspectives on a low-burden therapy

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