La Jolla Bioengineering Institute

Improving Transcapillary Transport by Reducing Interstitial Fluid Pressure

NIH R03 EB006746

We have recently developed a minimally invasive, biosensor-based, diagnostic surgical procedure for measuring interstitial fluid pressure (IFP) in cancer. We propose to apply this new diagnostic technique to elucidate the role of contractile pericytes in IFP and transcapillary transport of nanoparticles in tumors. Similar to isometric contraction of skeletal muscle, neovascular pericytes generate contractile forces not only on the vessel walls but also on interstitial fluid entrapped within extracellular fibers, referred to as tissue gel. We will test whether interstitial fluid pressure in cancer can be reduced by interfering with pericytes to improve the convection of nanoparticle based anti-cancer drugs. We will test whether inhibition of pericytes results in a decrease in interstitial fluid pressure due to decreasing compressive contractile forces elicited by pericytes. We will test whether pericyte-NG2 proteoglycan inhibition lowers IFP and improves convection from the plasma to the interstitial space. We will quantify transcapillary transport by using nanoparticles as tracers. We anticipate finding a higher transcapillary convection of nanoparticles (simulating high molecular weight anti-cancer drugs) and lower interstitial fluid pressure in breast tumors when pericytes are inhibited. By combining skills and disciplines in bioengineering, clinical physiology and microvascular sciences this project will transform our biosensor-based diagnostic procedure into a tangible diagnostic tool for cancer patients. The use of ultraminiature transducer-tipped catheters as cancer interstitial fluid pressure biosensors is innovative in light of novel use of biosensors portfolio of National Institute of Biomedical Imaging and Bioengineering. The role of compressive forces generated by pericytes within breast cancer stroma has never been investigated; which makes this proposal innovative in shedding light on the etiology of interstitial hypertension, a significant clinical problem in breast cancer therapy in terms of drug delivery.

Funding

Principal Investigator: Leonardo Jose De Moura Carvalho, Ph.D.
Agency: NIH

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  • Improving Transcapillary Transport by Reducing Interstitial Fluid Pressure
  • Interstitial Fluid Flow in Bone Remodeling
  • Mechanosensitivity of Cell Membranes: Role of Lipid-Protein Interactions
  • Mechanosensory properties in the partially obstructed guinea pig small intestine
  • Multiplexed Analysis of Serum Antibodies to Influenza Virus
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  • Raman Flow Cytometry for Diagnostics and Drug Discovery
  • Shear Stress Activation of Endothelial Membrane Function
  • The Role of Dipole Potential in Mechanosensing
  • Using Simulated Microgravity to Enhance the Effectiveness of Nanodrug Chemotherapy in Breast Cancer
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  • John A. Frangos, PhD
  • John Nolan, PhD
  • Mirianas Chachisvilis, PhD
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