C. Winkler scite author profile

The uptake and turnover of omega(p 123I iodophenyl-)pentadecanoic acid (I-PPA), a radioiodinated free-fatty-acid analog, was examined in the heart, lung, liver, kidneys, spleen, and skeletal muscle of rats. At 2 min post injection, a high cardiac uptake of 4.4% dose per gram had already been achieved; this was followed by a rapid, two-component, tracer clearance. The kinetics of tissue concentrations of labeled hydrophilic catabolites indicated a rapid oxidation of I-PPA and the subsequent washout of I-PPA catabolites from heart-muscle tissue. The fractional distribution of the labeled cardiac lipids compared favorably with previously reported values for 3H-oleic- or 14C-palmitic-acid-labeled myocardial lipids. Typical patterns of I-PPA metabolism were observed in tissues depending on primary fatty-acid oxidation, lipid metabolism regulation, or I-PPA-catabolite excretion. The tissue concentrations and kinetics of I-PPA and its metabolites in the heart muscle indicated that general pathways of cardiac-lipid metabolism are traced by this new gamma-emitting isotope-labeled radiopharmaceutical.

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COMPTEL measurements of the gamma-ray burst GRB 930131

Ryan¹,

Bennett²,

Collmar³

et al. 1994

ApJ

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Captopril mediated decrease of aortic regurgitation.

Reske¹,

Heck²,

Kropp³

et al. 1985

Heart

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The effect of captopril mediated afterload reduction on aortic regurgitation was investigated in 10 patients. Regurgitation was quantitated by means of the regurgitation fraction and the relation of regurgitant volume to end diastolic volume. These variables were derived from gated radionuclide ventriculography. After captopril treatment the blood concentration of angiotensin I rose whereas that of angiotensin II fell significantly. The conversion of angiotensin I to II was reduced to about 50% of the control value. Whereas blood pressure and heart rate did not change significantly, the regurgitation fraction and the regurgitant volume, normalised to end diastolic volume, were significantly reduced by captopril treatment. The ejection fraction remained essentially unchanged. These findings suggest that captopril reduces aortic regurgitation by reducing afterload.

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[sup 44]Ti gamma-ray line emission from Cas A and RXJ0852-4622/GROJ0852-4642

Schönfelder¹,

Bloemen²,

Collmar³

et al. 2000

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C. Winkler

Instrument description and performance of the Imaging Gamma-Ray Telescope COMPTEL aboard the Compton Gamma-Ray Observatory

Metabolism of 15 (p123I iodophenyl-)pentadecanoic acid in heart muscle and noncardiac tissues

COMPTEL measurements of the gamma-ray burst GRB 930131

Captopril mediated decrease of aortic regurgitation.

[sup 44]Ti gamma-ray line emission from Cas A and RXJ0852-4622/GROJ0852-4642

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