Mild Whole-Body Hyperthermia-Induced Interstitial Fluid Pressure Reduction and Enhanced Nanoparticle Delivery to PC3 Tumors: In Vivo Studies and Micro-Computed Tomography Analyses-Reference-Cited by-同舟云学术

Mild Whole-Body Hyperthermia-Induced Interstitial Fluid Pressure Reduction and Enhanced Nanoparticle Delivery to PC3 Tumors: In Vivo Studies and Micro-Computed Tomography Analyses

Published:2020-06-16 Issue:6 Volume:12 Page:
ISSN:1948-5085
Container-title:Journal of Thermal Science and Engineering Applications
language:en
Short-container-title:

Author:

Gu Qimei¹,Liu Shuaishuai²,Saha Ray Arunendra³,Florinas Stelios⁴,Christie Ronald James⁴,Daniel Marie-Christine³,Bieberich Charles²,Ma Ronghui¹,Zhu Liang¹

Affiliation:

1. Department of Mechanical Engineering, University of Maryland Baltimore County, Baltimore, MD 21250

2. Department of Biology, University of Maryland Baltimore County, Baltimore, MD 21250

3. Department of Chemistry and Biochemistry, University of Maryland Baltimore County, Baltimore, MD 21250

4. Department of Antibody Discovery and Protein Engineering, AstraZeneca R&D, Gaithersburg, MD 20878

Abstract

Abstract In this study, we performed in vivo experiments on mice to evaluate whether whole-body hyperthermia enhances nanoparticle delivery to PC3 (prostatic cancer) tumors. PC3 xenograft tumors in immunodeficient mice were used in this study. The mice in the experimental group were subjected to whole-body hyperthermia by maintaining their body temperatures at 39–40 °C for 1 h. Interstitial fluid pressures (IFPs) in tumors were measured before heating, immediately after, and at 2 and 24 h postheating in both the experimental group and in a control group (without heating). A total of 0.2 ml of a newly developed nanofluid containing gold nanoparticles (AuNPs) was delivered via the tail vein in both groups. The micro-computed tomography (microCT) scanned images of the resected tumors were analyzed to visualize the nanoparticle distribution in the tumors and to quantify the total amount of nanoparticles delivered to the tumors. Statistically significant IFP reductions of 45% right after heating, 47% 2 h after heating, and 52% 24 h after heating were observed in the experimental group. Analyses of microCT scans of the resected tumors illustrated that nanoparticles were more concentrated near the tumor periphery rather than at the tumor center. The 1-h whole-body hyperthermia treatment resulted in more nanoparticles present in the tumor central region than that in the control group. The mass index calculated from the microCT scans suggested overall 42% more nanoparticle delivery in the experimental group than that in the control group. We conclude that 1-h mild whole-body hyperthermia leads to sustained reduction in tumoral IFPs and significantly increases the total amount of targeted gold nanoparticle deposition in PC3 tumors. The present study suggests that mild whole-body hyperthermia is a promising approach for enhancing targeted drug delivery to tumors.

Funder

National Science Foundation

Publisher

ASME International

Subject

Fluid Flow and Transfer Processes,General Engineering,Condensed Matter Physics,General Materials Science

Link

http://asmedigitalcollection.asme.org/thermalscienceapplication/article-pdf/doi/10.1115/1.4046520/6599025/tsea_12_6_061001.pdf

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