Abstract

Reduction of intracellular pH (pHi) by acute reduction of extracellular pH (pHe) leads to hyperthermia sensitization and reduced thermotolerance development. However, cells adapt to chronic exposures to low pHe by re-establishing a near-normal pHi, and are no longer hyperthermia sensitive. We and others have shown that much of the tumor population is below normal pHe (mean of 7.2 vs. 7.4) and that hyperglycemia can acutely and specifically reduce tumor pHe by another 0.2 pH units in both American and Chinese patients. The overall objectives of this program are to test the general hypothesis that the response of tumors to hyperthermia can be enhanced by reducing pHi. If manipulation of pH is to lead to an improvement of the therapeutic ratio by trimodality therapy, strategies must be developed based on fundamental principles which can lead to a rational basis for the design of clinical trials. Five interactive projects are proposed. Project #1 tests the hypothesis that the increased capability for cellular proton expulsion can largely be accounted for by increased activity of one or both of the two proton translocating mechanisms which are thought to be the principal systems active in mammalian cells: a) the amiloride-sensitive sodium-proton (Na+/H+) exchange, and b) the sodium-sensitive chloride-bicarbonate (HCO3-/Cl-) exchange. Project #2 tests the hypothesis that inhibition of the Na+/H+ antiport system, inhibition of the H+/lactate symport or inhibition of HCO3-/Cl- exchange in cells adapted to low pHe will reduce pHi and will sensitize to hyperthermia. Whether the hyperthermia response is enhanced primarily by means of sensitization or primarily by inhibition of thermotolerance development will be evaluated. In addition, the hypothesis that the synthesis of certain heat shock proteins is tightly coupled with thermotolerance development will be tested. Project #3 tests the hypothesis that reduction of pHi will enhance heat-induced potentially lethal damage to cellular structural systems, thereby leading to increased killing. Project #4 tests the hypothesis that regions of chronic acidosis brought about by substrate limitation exist in normal bone marrow, and therefore marrow stem cells and committed precursors may also be sensitized to thermochemotherapy by inhibition of the Na+/H+ antiport or inhibition of lactate transport. The effect of hyperthermia on blood flow in human tumors during hyperthermia, and the correlation between blood flow and interstitial pH are documented in Project #5. Alterations in tumor blood flow result in concomitant alterations in the accessibility of metabolites, the accumulation of lactic acid and other metabolic by-products, and the dissipation of temperature by convective processes. There is a Core component which provides administrative, statistical and technical support (e.g., intracellular pH measurement) for all projects.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Program Projects (P01)
Project #
1P01CA056690-01A1
Application #
3094613
Study Section
Special Emphasis Panel (SRC (O1))
Project Start
1993-04-23
Project End
1997-03-31
Budget Start
1993-04-23
Budget End
1994-03-31
Support Year
1
Fiscal Year
1993
Total Cost
Indirect Cost

  Institution

Name
Thomas Jefferson University
Department
Type
Schools of Medicine
DUNS #
061197161
City
Philadelphia
State
PA
Country
United States
Zip Code
19107

  Publications

Coss, Ronald Allen; Storck, Christopher W; Wells, Tiffany C et al. (2014) Thermal sensitisation by lonidamine of human melanoma cells grown at low extracellular pH. Int J Hyperthermia 30:75-8
Li, Lin Z; Zhou, Rong; Leeper, Dennis B et al. (2011) ³¹P-MRS studies of melanoma xenografts with different metastatic potential. Adv Exp Med Biol 701:69-73
Xu, He N; Zhou, Rong; Nioka, Shoko et al. (2009) Histological basis of MR/optical imaging of human melanoma mouse xenografts spanning a range of metastatic potentials. Adv Exp Med Biol 645:247-53
Li, Lin Z; Zhou, Rong; Xu, He N et al. (2009) Quantitative magnetic resonance and optical imaging biomarkers of melanoma metastatic potential. Proc Natl Acad Sci U S A 106:6608-13
Sonveaux, Pierre; Vegran, Frederique; Schroeder, Thies et al. (2008) Targeting lactate-fueled respiration selectively kills hypoxic tumor cells in mice. J Clin Invest 118:3930-42
Li, Lin Z J; Zhou, Rong; Zhong, Tuoxiu et al. (2007) Predicting melanoma metastatic potential by optical and magnetic resonance imaging. Adv Exp Med Biol 599:67-78
Chi, Sulene L; Wahl, Miriam L; Mowery, Yvonne M et al. (2007) Angiostatin-like activity of a monoclonal antibody to the catalytic subunit of F1F0 ATP synthase. Cancer Res 67:4716-24
Fang, Jun; Quinones, Quintin J; Holman, Trevor L et al. (2006) The H+-linked monocarboxylate transporter (MCT1/SLC16A1): a potential therapeutic target for high-risk neuroblastoma. Mol Pharmacol 70:2108-15
Adams, David J; Wahl, Miriam L; Flowers, James L et al. (2006) Camptothecin analogs with enhanced activity against human breast cancer cells. II. Impact of the tumor pH gradient. Cancer Chemother Pharmacol 57:145-54
Coss, Ronald A (2005) Inhibiting induction of heat shock proteins as a strategy to enhance cancer therapy. Int J Hyperthermia 21:695-701

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