Abstract

The intent of this research is to develop an imaging approach with positron emission tomography to quantitatively characterize the adrenergic innervation of the heart. Despite the physiological importance of norepinephrine (NE) as an adrenergic transmitter, no radiopharmaceutical exists that can quantitatively and non- invasively assess catecholamine accumulation and turnover in peripheral tissue. The work proposed for the next 5 years will focus on the radiosynthesis of true and false neurotransmitters and the use of these tracers to map cardiac neurophysiology in experimental and clinical studies. NE and a select number of false transmitters will be F-18-labeled and tested for their ability to serve as anatomical and functional neuronal mapping agents. False transmitters to be studied include: p-hydroxynorephedrine, octopamine, m-octopamine, and m-hydroxyamphetamine. Factors that will affect tracer choice are: 1) ease of synthesis; 2) specific activity requirements mandated by pharmacological potency; 3) metabolic fate; 4) informational content. The tracers will be validated first in animal experiments. In vivo tissue distribution, pretreatment studies with the uptake 1 blocker desmethylimipramine and chemical sympathectomy studies with 6-hydroxydopamine will determine the global accumulation in and selectivity for adrenergic nerves. Radio-HPLC analysis of blood and heart following i.v. tracer injection will be used to determine extent of metabolism and arterial input function. Correlation of tracer accumulation with tissue norepinephrine distribution in normal and regionally denervated heart will be performed in the dog. Based on first pass kinetics of myocardial uptake and turnover, a tracer kinetic model will be derived to quantitate regional sympathetic function. Applications will include determining the dependence of F-18-tracer depletion on time period and severity of ischemia, the time course of restoration of tracer following ischemic insult, and correlation of regional depletion of tracer with electrophysiological parameters such as conduction velocity and inducible arrhythmias. Clinical applications will include mapping the normal distribution of the heart adrenergic system, its reproducibility, and its relationship to age and cardiac work. The study of patients with cardiac transplants, diabetic neuropathy, acute infarction, unstable angina and congestive heart failure will be pursued.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Heart, Lung, and Blood Institute (NHLBI)
Type
Research Project (R01)
Project #
5R01HL027555-08
Application #
3339220
Study Section
Diagnostic Radiology Study Section (RNM)
Project Start
1981-08-01
Project End
1991-03-31
Budget Start
1989-04-01
Budget End
1990-03-31
Support Year
8
Fiscal Year
1989
Total Cost
Indirect Cost

  Institution

Name
University of Michigan Ann Arbor
Department
Type
Schools of Medicine
DUNS #
791277940
City
Ann Arbor
State
MI
Country
United States
Zip Code
48109

  Publications

Van Dort, M E (1999) Direct chromatographic resolution and isolation of the four stereoisomers of meta-hydroxyphenylpropanolamine. Chirality 11:684-8
Raffel, D M; Corbett, J R; del Rosario, R B et al. (1999) Sensitivity of [11C]phenylephrine kinetics to monoamine oxidase activity in normal human heart. J Nucl Med 40:232-8
Raffel, D M; Wieland, D M (1999) Influence of vesicular storage and monoamine oxidase activity on [11C]phenylephrine kinetics: studies in isolated rat heart. J Nucl Med 40:323-30
Romanenko, V G; Gebara, R; Miller, K M et al. (1998) Determination of transport parameters of permeant substrates of the vesicular amine transporter. Anal Biochem 257:127-33
Van Dort, M E; Kim, J H; Tluczek, L et al. (1997) Synthesis of 11C-labeled desipramine and its metabolite 2-hydroxydesipramine: potential radiotracers for PET studies of the norepinephrine transporter. Nucl Med Biol 24:707-11
Nguyen, N T; DeGrado, T R; Chakraborty, P et al. (1997) Myocardial kinetics of carbon-11-epinephrine in the isolated working rat heart. J Nucl Med 38:780-5
Raffel, D M; Corbett, J R; del Rosario, R B et al. (1996) Clinical evaluation of carbon-11-phenylephrine: MAO-sensitive marker of cardiac sympathetic neurons. J Nucl Med 37:1923-31
Gildersleeve, D L; Van Dort, M E; Johnson, J W et al. (1996) Synthesis and evaluation of [123I]-iodo-PK11195 for mapping peripheral-type benzodiazepine receptors (omega 3) in heart. Nucl Med Biol 23:23-8
Del Rosario, R B; Jung, Y W; Caraher, J et al. (1996) Synthesis and preliminary evaluation of [11C]-(-)-phenylephrine as a functional heart neuronal PET agent. Nucl Med Biol 23:611-6
Van Dort, M E; Jung, Y W; Sherman, P S et al. (1995) Fluorine for hydroxy substitution in biogenic amines: asymmetric synthesis and biological evaluation of fluorine-18-labeled beta-fluorophenylalkylamines as model systems. J Med Chem 38:810-5

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