Abstract

The long-term objective of this research is to quantify transport in tumor microcirulation. The specific anim of this renewal application are to investigate the detailed fluid flow profile within the interstitial space of living tissues and to determine the contribution of convective transport to the overall transport of macromolecules in norman and cancerous tissues. The expermental phase of this research will involve the determination of the diffusion coefficient, D, and the convective velocity field, v, for the transport of various macromoles in normal (mature granulation) as well as neoplastic (VX2 carcinoma) tissues in the rabbit ear chamber preparation. The measured transport characteristics will be correlated to the properties of the macromolecule (size, charge, configuration) and the tissue (norman versus tumor). Fluorescence recovery after photobleaching (FRAP) will be used to discriminate between convection and diffusion. This technique involves laser irradiation of a select region of the fluorescence-bathed interstitium to create a well- defined area of low fluorescence intensity. The fluorophore concentration within this bleached region is monitored as a funciton of space and time, and is analyzed to determine the intersitial convective velocity and the interstitial diffusion coefficient. Investigation into the heterogeneity of the convective velocity will also provide information on the detailed flow profile within the intersitial space tissues. The theoretical phase of the research will involve mathematical nodeling of the fluorescence recovery after photobleaching for arbitrary intersitial flow fields to determine accurately a convective velocity profile and a diffusion coefficient frrom analysis of the obtained data. The fluid flow in the interstitum will also be modeled in order to investigate the Starling mechanism of fluid exhange between a microvessel and the surrounding interstitial space. The significant tissue characteristics governing the velocity profile will be determined. The fiver- matrix model for intersitial transport will be improved, incorporating convection and viscous/hydrodynamic hindrance in the analysis, leading to a more accurate description of transport in vivo. The proposed investigation will provide the first measure of the magnitude and direction of convective velocity in the interstitium. The results obtained will be of value to physiologists in developing a better understanding of Starling's hypothesis of transcapillary exchange, and in characterizing interstitial transport in tissues; and to cancer researchers and oncologist in improving current methods of cancer detection and treatment.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
7R01CA036902-08
Application #
3174538
Study Section
Cardiovascular and Renal Study Section (CVB)
Project Start
1984-12-01
Project End
1992-11-30
Budget Start
1991-09-15
Budget End
1991-11-30
Support Year
8
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

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

  Publications

Yuan, F; Leunig, M; Berk, D A et al. (1993) Microvascular permeability of albumin, vascular surface area, and vascular volume measured in human adenocarcinoma LS174T using dorsal chamber in SCID mice. Microvasc Res 45:269-89
Boucher, Y; Jain, R K (1992) Microvascular pressure is the principal driving force for interstitial hypertension in solid tumors: implications for vascular collapse. Cancer Res 52:5110-4
Leunig, M; Yuan, F; Menger, M D et al. (1992) Angiogenesis, microvascular architecture, microhemodynamics, and interstitial fluid pressure during early growth of human adenocarcinoma LS174T in SCID mice. Cancer Res 52:6553-60
Kaufman, E N; Jain, R K (1992) In vitro measurement and screening of monoclonal antibody affinity using fluorescence photobleaching. J Immunol Methods 155:1-17
Baxter, L T; Yuan, F; Jain, R K (1992) Pharmacokinetic analysis of the perivascular distribution of bifunctional antibodies and haptens: comparison with experimental data. Cancer Res 52:5838-44
Kaufman, E N; Jain, R K (1992) Effect of bivalent interaction upon apparent antibody affinity: experimental confirmation of theory using fluorescence photobleaching and implications for antibody binding assays. Cancer Res 52:4157-67
Kaufman, E N; Jain, R K (1991) Measurement of mass transport and reaction parameters in bulk solution using photobleaching. Reaction limited binding regime. Biophys J 60:596-610
Yuan, F; Baxter, L T; Jain, R K (1991) Pharmacokinetic analysis of two-step approaches using bifunctional and enzyme-conjugated antibodies. Cancer Res 51:3119-30
Baxter, L T; Jain, R K (1991) Transport of fluid and macromolecules in tumors. IV. A microscopic model of the perivascular distribution. Microvasc Res 41:252-72
Clauss, M A; Jain, R K (1990) Interstitial transport of rabbit and sheep antibodies in normal and neoplastic tissues. Cancer Res 50:3487-92

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