Literature DB >> 1657448

First-pass entry of nonionic contrast agent into the myocardial extravascular space. Effects on radiographic estimates of transit time and blood volume.

J M Canty1, R M Judd, A S Brody, F J Klocke.   

Abstract

BACKGROUND: Almost all x-ray-based techniques intended to assess regional myocardial perfusion from myocardial concentration-time curves following the administration of soluble contrast agents assume that these agents behave as intravascular indicators and can therefore provide measurements of intravascular transit time and intramyocardial blood volume. METHODS AND
RESULTS: We tested this assumption by comparing a conventional nonionic contrast agent (ioversol) to a particulate emulsion (ethiodol) that remained in the vascular space in closed-chest dogs during pharmacological vasodilation. Using fast computed tomography (CT), pairs of myocardial CT intensity-time curves were obtained following sequential bolus aortic administration of the two contrast agents. The emulsion (particle size less than 3 microns) was almost completely washed out of the myocardial region of interest within a few seconds, as would be anticipated for a vascular indicator. At the onset of recirculation, CT intensity for ethiodol fell to 5 +/- 1% (SEM) of peak values in normally perfused areas and to 10 +/- 4% of peak values in an area in which flow had been reduced by 50% by a chronically implanted coronary artery occluder (p = NS). In comparison, the diffusible nonionic contrast agent ioversol showed substantial intramyocardial retention at the onset of recirculation. At the time of recirculation, CT intensities for ioversol averaged 36 +/- 2% of peak values in normally perfused nonstenotic areas and 54 +/- 4% of peak values in stenotic areas (p less than 0.01). Using residue function analysis for a diffusible indicator, first-pass extractions of the conventional nonionic agent averaged 33 +/- 2% in normally perfused areas and 50 +/- 3% in stenotic areas (p less than 0.01). Because of the significant first-pass myocardial retention of ioversol, both mean myocardial appearance time and intramyocardial blood volume were consistently overestimated.
CONCLUSIONS: Soluble radiographic contrast agents, like other small molecules, enter the interstitial space to a degree, which is important because it affects estimates of myocardial perfusion based on transit time and intramyocardial blood volume. Indicator dilution models intended to quantify myocardial perfusion with conventional radiographic contrast agents need to account for this extravascular exchange.

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Year:  1991        PMID: 1657448     DOI: 10.1161/01.cir.84.5.2071

Source DB:  PubMed          Journal:  Circulation        ISSN: 0009-7322            Impact factor:   29.690


  22 in total

1.  3D assessment of myocardial perfusion parameter combined with 3D reconstructed coronary artery tree from digital coronary angiograms.

Authors:  T H Schindler; N Magosaki; M Jeserich; E Nitzsche; U Oser; T Abdollahnia; M Nageleisen; M Zehender; H Just; U Solzbach
Journal:  Int J Card Imaging       Date:  2000-02

2.  Changes in myocardial blood volume over a wide range of coronary driving pressures: role of capillaries beyond the autoregulatory range.

Authors:  D E Le; A R Jayaweera; K Wei; M P Coggins; J R Lindner; S Kaul
Journal:  Heart       Date:  2004-10       Impact factor: 5.994

Review 3.  Assessment of coronary blood flow with computed tomography and magnetic resonance imaging.

Authors:  Karl H Schuleri; Richard T George; Albert C Lardo
Journal:  J Nucl Cardiol       Date:  2010-08       Impact factor: 5.952

Review 4.  Applications of cardiac multidetector CT beyond coronary angiography.

Authors:  Karl H Schuleri; Richard T George; Albert C Lardo
Journal:  Nat Rev Cardiol       Date:  2009-11       Impact factor: 32.419

Review 5.  Insights into the assessment of myocardial perfusion offered by different cardiac imaging modalities.

Authors:  J R Lindner; S Kaul
Journal:  J Nucl Cardiol       Date:  1995 Sep-Oct       Impact factor: 5.952

6.  Modeling regional myocardial flows from residue functions of an intravascular indicator.

Authors:  K Kroll; N Wilke; M Jerosch-Herold; Y Wang; Y Zhang; R J Bache; J B Bassingthwaighte
Journal:  Am J Physiol       Date:  1996-10

Review 7.  Nanoparticles for Cardiovascular Imaging and Therapeutic Delivery, Part 2: Radiolabeled Probes.

Authors:  John C Stendahl; Albert J Sinusas
Journal:  J Nucl Med       Date:  2015-08-20       Impact factor: 10.057

8.  Comparison of coronary flow reserve estimated by dynamic radionuclide SPECT and multi-detector x-ray CT.

Authors:  Cecilia Marini; Sara Seitun; Camilla Zawaideh; Matteo Bauckneht; Margherita Castiglione Morelli; Pietro Ameri; Giulia Ferrarazzo; Irilda Budaj; Manrico Balbi; Francesco Fiz; Sara Boccalini; Athena Galletto Pregliasco; Ambra Buschiazzo; Alice Saracco; Maria Claudia Bagnara; Paolo Bruzzi; Claudio Brunelli; Carlo Ferro; Gian Paolo Bezante; Gianmario Sambuceti
Journal:  J Nucl Cardiol       Date:  2016-05-05       Impact factor: 5.952

Review 9.  Assessment of myocardial perfusion using contrast-enhanced MR imaging: current status and future developments.

Authors:  A Mühler
Journal:  MAGMA       Date:  1995-03       Impact factor: 2.310

10.  Permanent coronary artery occlusion: cardiovascular MR imaging is platform for percutaneous transendocardial delivery and assessment of gene therapy in canine model.

Authors:  Maythem Saeed; Alastair Martin; Alexis Jacquier; Matthew Bucknor; David Saloner; Loi Do; Philip Ursell; Hua Su; Yuet W Kan; Charles B Higgins
Journal:  Radiology       Date:  2008-09-09       Impact factor: 11.105

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