Abstract

In its journey from blood vessels to cancer cells a therapeutic agent must overcome the transport barrier posed by the interstitial matrix. In contrast to our understanding of blood vessels, our understanding of the formation and function of the tumor interstitial matrix is still in its infancy. To make progress toward the goal of normalizing interstitial transport, we need to (i) identify the matrix components that contribute to the barrier function of the interstitium, (ii) image these components in vivo, (iii) measure interstitial transport parameters with high sensitivity, and (iv) modify the matrix without harming the host. In the past 5 years we have made significant progress toward these goals. We discovered that collagen is the key determinant of the interstitial barrier (Cancer Research 2000), established the use of second harmonic generation for in vivo imaging of the collagen matrix in tumors (Nature Medicine 2003), adapted multi-photon fluorescence correlation spectroscopy in vivo and revealed the two phase nature of interstitial transport in tumors (Nature Medicine 2004a), and used an endogenous molecule, the hormone relaxin, to modify the collagen matrix and make it more penetrable (Nature Medicine 2003). Finally, we demonstrated that the xenograft models can be used to estimate diffusion in human tumors. This project builds upon these exciting technical developments and scientific findings. Our new goal is to reveal the molecular underpinnings of matrix modification and to identify additional, novel matrix modifiers that can be used clinically. TGF-fJl and PDGF can stimulate production of collagen by stromal cells in tumors;therefore, we will determine if modulating these molecules or their downstream signaling pathways improves interstitial transport (Aim1). Since MMP-1, -8, and -13 degrade fibrillar collagen, we will express these.MMPs in cancer cells or stromal cells, or deliver them with a replication-defective virus, and measure transport (Aim 2). Finally, we will determine the mechanism and extent to which relaxin and halofuginone - two agents proven to be safe in humans - increase the delivery and efficacy of clinically approved therapeutics (Aim 3). We will carry out these studies in orthotopically-growing human mammary carcinoma and melanoma xenografts as well as in a spontaneous tumor model using IgG, IgM, AAV, HSV-1 and Herceptin as models of macromolecular therapeutic agents. We have the necessary technology, molecular reagents and animal models from Cores A, B and C (Nature Reviews Cancer 2002) as well as from our collaborators. We also have clinicalcollaborators in place to initiate a clinical trial based on our findings, similar to our ongoing trial using a VEGF-specific antibody (Nature Medicine 2004b).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
5P01CA080124-09
Application #
7874641
Study Section
Subcommittee G - Education (NCI)
Project Start
Project End
Budget Start
2009-05-01
Budget End
2010-04-30
Support Year
9
Fiscal Year
2009
Total Cost
$304,190
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
073130411
City
Boston
State
MA
Country
United States
Zip Code
02199

  Publications

Khandekar, Melin J; Jain, Rakesh (2018) Smooth sailing for immunotherapy for unresectable stage III non-small cell lung cancer: the PACIFIC study. Transl Cancer Res 7:S16-S20
Stylianopoulos, Triantafyllos; Munn, Lance L; Jain, Rakesh K (2018) Reengineering the Tumor Vasculature: Improving Drug Delivery and Efficacy. Trends Cancer 4:258-259
Grassberger, Clemens; Hong, Theodore S; Hato, Tai et al. (2018) Differential Association Between Circulating Lymphocyte Populations With Outcome After Radiation Therapy in Subtypes of Liver Cancer. Int J Radiat Oncol Biol Phys 101:1222-1225
Zhang, Na; Chen, Jie; Ferraro, Gino B et al. (2018) Anti-VEGF treatment improves neurological function in tumors of the nervous system. Exp Neurol 299:326-333
Aoki, Shuichi; Cobbold, Mark; Zhu, Andrew X et al. (2018) Can smart nanomedicine deliver effective targeted cytotoxic treatments to hepatocellular carcinomas while reducing the liver damage? Hepatology 67:826-828
Li, Wende; Liu, Yujiao; Yang, Weining et al. (2018) MicroRNA-378 enhances radiation response in ectopic and orthotopic implantation models of glioblastoma. J Neurooncol 136:63-71
Griveau, Amelie; Seano, Giorgio; Shelton, Samuel J et al. (2018) A Glial Signature and Wnt7 Signaling Regulate Glioma-Vascular Interactions and Tumor Microenvironment. Cancer Cell 33:874-889.e7
Stylianopoulos, Triantafyllos; Munn, Lance L; Jain, Rakesh K (2018) Reengineering the Physical Microenvironment of Tumors to Improve Drug Delivery and Efficacy: From Mathematical Modeling to Bench to Bedside. Trends Cancer 4:292-319
Incio, Joao; Ligibel, Jennifer A; McManus, Daniel T et al. (2018) Obesity promotes resistance to anti-VEGF therapy in breast cancer by up-regulating IL-6 and potentially FGF-2. Sci Transl Med 10:
Sung, Yun-Chieh; Liu, Ya-Chi; Chao, Po-Han et al. (2018) Combined delivery of sorafenib and a MEK inhibitor using CXCR4-targeted nanoparticles reduces hepatic fibrosis and prevents tumor development. Theranostics 8:894-905

Showing the most recent 10 out of 320 publications