Overcoming limitations in nanoparticle drug delivery: Triggered, intravascular release to improve drug penetration into tumors

Ashley A. Manzoor; Lars H. Lindner; Chelsea D. Landon; Ji Young Park; Andrew J. Simnick; Matthew R. Dreher; Shiva Das; Gabi Hanna; Won Park; Ashutosh Chilkoti; Gerben A. Koning; Timo L.M. Ten Hagen; David Needham; Mark W. Dewhirst

doi:10.1158/0008-5472.CAN-12-1683

Overcoming limitations in nanoparticle drug delivery: Triggered, intravascular release to improve drug penetration into tumors

Ashley A. Manzoor
, Lars H. Lindner
, Chelsea D. Landon
, Ji Young Park
, Andrew J. Simnick
, Matthew R. Dreher
, Shiva Das
, Gabi Hanna
, Won Park
, Ashutosh Chilkoti
, Gerben A. Koning
, Timo L.M. Ten Hagen
, David Needham
, Mark W. Dewhirst

Medical Physics Program
Duke University
Erasmus University Rotterdam
Ludwig Maximilian University of Munich
Helmholtz Zentrum München - German Research Center for Environmental Health
National Institutes of Health

Research output: Contribution to journal › Article › peer-review

434 Scopus citations

Abstract

Traditionally, the goal of nanoparticle-based chemotherapy has been to decrease normal tissue toxicity by improving drug specificity to tumors. The enhanced permeability and retention effect can permit passive accumulation into tumor interstitium. However, suboptimal delivery is achieved with most nanoparticles because of heterogeneities of vascular permeability, which limits nanoparticle penetration. Furthermore, slow drug release limits bioavailability. We developed a fast drug-releasing liposome triggered by local heat that has already shown substantial antitumor efficacy and is in human trials. Here, we show that thermally sensitive liposomes (Dox-TSL) release doxorubicin inside the tumor vasculature. Real-time confocal imaging of doxorubicin delivery to murine tumors in window chambers and histologic analysis of flank tumors illustrates that intravascular drug release increases free drug in the interstitial space. This increases both the time that tumor cells are exposed to maximum drug levels and the drug penetration distance, compared with free drug or traditional pegylated liposomes. These improvements in drug bioavailability establish a new paradigm in drug delivery: rapidly triggered drug release in the tumor bloodstream.

Original language	English
Pages (from-to)	5566-5575
Number of pages	10
Journal	Cancer Research
Volume	72
Issue number	21
DOIs	https://doi.org/10.1158/0008-5472.CAN-12-1683
State	Published - 1 Nov 2012
Externally published	Yes

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SDG 3 Good Health and Well-being

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10.1158/0008-5472.CAN-12-1683

Cite this

Manzoor, A. A., Lindner, L. H., Landon, C. D., Park, J. Y., Simnick, A. J., Dreher, M. R., Das, S., Hanna, G., Park, W., Chilkoti, A., Koning, G. A., Ten Hagen, T. L. M., Needham, D., & Dewhirst, M. W. (2012). Overcoming limitations in nanoparticle drug delivery: Triggered, intravascular release to improve drug penetration into tumors. Cancer Research, 72(21), 5566-5575. https://doi.org/10.1158/0008-5472.CAN-12-1683

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title = "Overcoming limitations in nanoparticle drug delivery: Triggered, intravascular release to improve drug penetration into tumors",

abstract = "Traditionally, the goal of nanoparticle-based chemotherapy has been to decrease normal tissue toxicity by improving drug specificity to tumors. The enhanced permeability and retention effect can permit passive accumulation into tumor interstitium. However, suboptimal delivery is achieved with most nanoparticles because of heterogeneities of vascular permeability, which limits nanoparticle penetration. Furthermore, slow drug release limits bioavailability. We developed a fast drug-releasing liposome triggered by local heat that has already shown substantial antitumor efficacy and is in human trials. Here, we show that thermally sensitive liposomes (Dox-TSL) release doxorubicin inside the tumor vasculature. Real-time confocal imaging of doxorubicin delivery to murine tumors in window chambers and histologic analysis of flank tumors illustrates that intravascular drug release increases free drug in the interstitial space. This increases both the time that tumor cells are exposed to maximum drug levels and the drug penetration distance, compared with free drug or traditional pegylated liposomes. These improvements in drug bioavailability establish a new paradigm in drug delivery: rapidly triggered drug release in the tumor bloodstream.",

author = "Manzoor, \{Ashley A.\} and Lindner, \{Lars H.\} and Landon, \{Chelsea D.\} and Park, \{Ji Young\} and Simnick, \{Andrew J.\} and Dreher, \{Matthew R.\} and Shiva Das and Gabi Hanna and Won Park and Ashutosh Chilkoti and Koning, \{Gerben A.\} and \{Ten Hagen\}, \{Timo L.M.\} and David Needham and Dewhirst, \{Mark W.\}",

year = "2012",

month = nov,

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doi = "10.1158/0008-5472.CAN-12-1683",

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Manzoor, AA, Lindner, LH, Landon, CD, Park, JY, Simnick, AJ, Dreher, MR, Das, S, Hanna, G, Park, W, Chilkoti, A, Koning, GA, Ten Hagen, TLM, Needham, D & Dewhirst, MW 2012, 'Overcoming limitations in nanoparticle drug delivery: Triggered, intravascular release to improve drug penetration into tumors', Cancer Research, vol. 72, no. 21, pp. 5566-5575. https://doi.org/10.1158/0008-5472.CAN-12-1683

TY - JOUR

T1 - Overcoming limitations in nanoparticle drug delivery

T2 - Triggered, intravascular release to improve drug penetration into tumors

AU - Manzoor, Ashley A.

AU - Lindner, Lars H.

AU - Landon, Chelsea D.

AU - Park, Ji Young

AU - Simnick, Andrew J.

AU - Dreher, Matthew R.

AU - Das, Shiva

AU - Hanna, Gabi

AU - Park, Won

AU - Chilkoti, Ashutosh

AU - Koning, Gerben A.

AU - Ten Hagen, Timo L.M.

AU - Needham, David

AU - Dewhirst, Mark W.

PY - 2012/11/1

Y1 - 2012/11/1

N2 - Traditionally, the goal of nanoparticle-based chemotherapy has been to decrease normal tissue toxicity by improving drug specificity to tumors. The enhanced permeability and retention effect can permit passive accumulation into tumor interstitium. However, suboptimal delivery is achieved with most nanoparticles because of heterogeneities of vascular permeability, which limits nanoparticle penetration. Furthermore, slow drug release limits bioavailability. We developed a fast drug-releasing liposome triggered by local heat that has already shown substantial antitumor efficacy and is in human trials. Here, we show that thermally sensitive liposomes (Dox-TSL) release doxorubicin inside the tumor vasculature. Real-time confocal imaging of doxorubicin delivery to murine tumors in window chambers and histologic analysis of flank tumors illustrates that intravascular drug release increases free drug in the interstitial space. This increases both the time that tumor cells are exposed to maximum drug levels and the drug penetration distance, compared with free drug or traditional pegylated liposomes. These improvements in drug bioavailability establish a new paradigm in drug delivery: rapidly triggered drug release in the tumor bloodstream.

AB - Traditionally, the goal of nanoparticle-based chemotherapy has been to decrease normal tissue toxicity by improving drug specificity to tumors. The enhanced permeability and retention effect can permit passive accumulation into tumor interstitium. However, suboptimal delivery is achieved with most nanoparticles because of heterogeneities of vascular permeability, which limits nanoparticle penetration. Furthermore, slow drug release limits bioavailability. We developed a fast drug-releasing liposome triggered by local heat that has already shown substantial antitumor efficacy and is in human trials. Here, we show that thermally sensitive liposomes (Dox-TSL) release doxorubicin inside the tumor vasculature. Real-time confocal imaging of doxorubicin delivery to murine tumors in window chambers and histologic analysis of flank tumors illustrates that intravascular drug release increases free drug in the interstitial space. This increases both the time that tumor cells are exposed to maximum drug levels and the drug penetration distance, compared with free drug or traditional pegylated liposomes. These improvements in drug bioavailability establish a new paradigm in drug delivery: rapidly triggered drug release in the tumor bloodstream.

UR - https://www.scopus.com/pages/publications/84868256944

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JO - Cancer Research

JF - Cancer Research

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ER -

Overcoming limitations in nanoparticle drug delivery: Triggered, intravascular release to improve drug penetration into tumors

Abstract

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