Human intratumoral therapy: Linking drug properties and tumor transport of drugs in clinical trials.

J Control Release

Department of Pharmaceutical Chemistry, University of Kansas, Lawrence, KS, USA; Department of Chemical and Petroleum Engineering, University of Kansas, Lawrence, KS, USA; Bioengineering Graduate Program, University of Kansas, Lawrence, KS, USA. Electronic address:

Published: October 2020

AI Article Synopsis

  • Cancer therapies target tumor cells directly or boost the immune system, utilizing methods like checkpoint inhibitors and oncolytic viruses, but can cause unwanted side effects.
  • Intratumoral drug delivery minimizes systemic exposure by administering small amounts of therapy directly into tumors, which helps avoid off-target toxicities.
  • The effectiveness of intratumoral therapies is influenced by factors in the tumor microenvironment and the physical properties of the drugs, with ongoing exploration of new strategies to enhance drug retention in tumors.

Article Abstract

Cancer therapies aim to kill tumor cells directly or engage the immune system to fight malignancy. Checkpoint inhibitors, oncolytic viruses, cell-based immunotherapies, cytokines, and adjuvants have been applied to prompt the immune system to recognize and attack cancer cells. However, systemic exposure of cancer therapies can induce unwanted adverse events. Intratumoral administration of potent therapies utilizes small amounts of drugs, in an effort to minimize systemic exposure and off-target toxicities. Here, we discuss the properties of the tumor microenvironment and transport considerations for intratumoral drug delivery. Specifically, we consider various tumor tissue factors and physicochemical factors that can affect tumor retention after intratumoral injection. We also review approved and clinical-stage intratumoral therapies and consider how the molecular and biophysical properties (e.g. size and charge) of these therapies influences intratumoral transport (e.g. tumor retention and cellular uptake). Finally, we offer a critical review and highlight several emerging approaches to promote tumor retention and limit systemic exposure of potent intratumoral therapies.

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http://dx.doi.org/10.1016/j.jconrel.2020.06.029DOI Listing

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