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Convection-enhanced delivery of Ls-TPT enables an effective, continuous, low-dose chemotherapy against malignant glioma xenograft model. | LitMetric

AI Article Synopsis

  • Treatment of malignant gliomas is challenging, with current methods yielding less than one year median survival; a new technique, convection-enhanced delivery (CED), using a nanoparticle liposome with topotecan shows promise.
  • CED of liposomal topotecan allows for prolonged retention in brain tissue (1.5 days) and effective accumulation around blood vessels, enhancing its antiangiogenic effects and topoisomerase I inhibition.
  • In rat models, CED with liposomal topotecan significantly improved survival rates and treatment efficacy compared to free topotecan, suggesting that this method could be effective for treating brain tumors.

Article Abstract

Treatment of malignant gliomas represents one of the most formidable challenges in oncology. The combination of surgery, radiation, and chemotherapy yields median survivals of less than one year. Here we demonstrate the use of a minimally invasive surgical technique, convection-enhanced delivery (CED), for local administration of a novel nanoparticle liposome containing topotecan. CED of this liposomal topotecan (Ls-TPT) resulted in extended brain tissue retention (t1/2 = 1.5 days), whereas free topotecan was rapidly cleared (t1/2 = 0.1 days) after CED. The favorable pharmacokinetic profile of extended topotecan release for about seven days, along with biodistribution featuring perivascular accumulation of the nanoparticles, provided, in addition to the known topoisomerase I inhibition, an effective antiangiogenic therapy. In the rat intracranial U87MG tumor model, vascular targeting of Ls-TPT with CED was associated with reductions in laminin expression and vascular density compared to free topotecan or control treatments. A single CED treatment on day 7 showed that free topotecan conferred no survival benefit versus control. However, Ls-TPT produced a significant (P = 0.0002) survival benefit, with six of seven complete cures. Larger U87MG tumors, where CED of Ls-TPT on day 12 resulted in one of six cures, indicated the necessity to cover the entire tumor with the infused therapeutic agent. CED of Ls-TPT was also efficacious in the intracranial U251MG tumor model (P = 0.0005 versus control). We conclude that the combination of a novel nanoparticle Ls-TPT and CED administration was very effective in treating experimental brain tumors.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC1871954PMC
http://dx.doi.org/10.1215/15228517-2006-001DOI Listing

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