Literature DB >> 10484446

Cardiac endothelial transport and metabolism of adenosine and inosine.

L M Schwartz1, T R Bukowski, J H Revkin, J B Bassingthwaighte.   

Abstract

The influence of transmembrane flux limitations on cellular metabolism of purine nucleosides was assessed in whole organ studies. Transcapillary transport of the purine nucleosides adenosine (Ado) and inosine (Ino) via paracellular diffusion through interendothelial clefts in parallel with carrier-mediated transendothelial fluxes was studied in isolated, Krebs-Henseleit-perfused rabbit and guinea pig hearts. After injection into coronary inflow, multiple-indicator dilution curves were obtained from coronary outflow for 90 s for 131I-labeled albumin (intravascular reference tracer), [3H]arabinofuranosyl hypoxanthine (AraH; extracellular reference tracer and nonreactive adenosine analog), and either [14C]Ado or [14C]Ino. Ado or Ino was separated from their degradative products, hypoxanthine, xanthine, and uric acid, in each outflow sample by HPLC and radioisotope counting. Ado and Ino, but not AraH, permeate the luminal membrane of endothelial cells via a saturable transporter with permeability-surface area product PS(ecl) and also diffuse passively through interendothelial clefts with the same conductance (PSg) as AraH. These parallel conductances were estimated via fitting with an axially distributed, multi-pathway, four-region blood-tissue exchange model. PSg for AraH were approximately 4 and 2.5 ml. g(-1). min(-1) in rabbits and guinea pigs, respectively. In contrast, transplasmalemmal conductances (endothelial PS(ecl)) were approximately 0.2 ml. g(-1). min(-1) for both Ado and Ino in rabbit hearts but approximately 2 ml. g(-1). min(-1) in guinea pig hearts, an order of magnitude different. Purine nucleoside metabolism also differs between guinea pig and rabbit cardiac endothelium. In guinea pig heart, 50% of the tracer Ado bolus was retained, 35% was washed out as Ado, and 15% was lost as effluent metabolites; 25% of Ino was retained, 50% washed out, and 25% was lost as metabolites. In rabbit heart, 45% of Ado was retained and 5% lost as metabolites, and 7% of Ino was retained and 3% lost as metabolites. We conclude that endothelial transport of Ado and Ino is a prime determinant of their metabolic fates: where transport rates are high, metabolic transformation is high.

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Year:  1999        PMID: 10484446      PMCID: PMC3483093          DOI: 10.1152/ajpheart.1999.277.3.H1241

Source DB:  PubMed          Journal:  Am J Physiol        ISSN: 0002-9513


  46 in total

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7.  Hypoxanthine production by ischemic heart demonstrated by high pressure liquid chromatography of blood purine nucleosides and oxypurines.

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Journal:  Clin Chim Acta       Date:  1981       Impact factor: 3.786

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Journal:  J Physiol       Date:  1982-03       Impact factor: 5.182

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Journal:  Circ Res       Date:  1979-10       Impact factor: 17.367

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2.  Transient transcapillary exchange of water driven by osmotic forces in the heart.

Authors:  Michael R Kellen; James B Bassingthwaighte
Journal:  Am J Physiol Heart Circ Physiol       Date:  2003-05-08       Impact factor: 4.733

3.  Strategies and Tactics in Multiscale Modeling of Cell-to-Organ Systems.

Authors:  James B Bassingthwaighte; Howard Jay Chizeck; Les E Atlas
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Review 4.  Theoretical models for coronary vascular biomechanics: progress & challenges.

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Review 5.  Multiscale modeling of cardiac cellular energetics.

Authors:  James B Bassingthwaighte; Howard J Chizeck; Les E Atlas; Hong Qian
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6.  GENTEX, a general multiscale model for in vivo tissue exchanges and intraorgan metabolism.

Authors:  James B Bassingthwaighte; Gary M Raymond; James D Ploger; Lisa M Schwartz; Thomas R Bukowski
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7.  Linking cellular energetics to local flow regulation in the heart.

Authors:  James B Bassingthwaighte
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Review 9.  Microcirculation and the physiome projects.

Authors:  James B Bassingthwaighte
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Review 10.  Modeling to link regional myocardial work, metabolism and blood flows.

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