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The Journal of Pediatrics | 1990

CORTISOL PRODUCTION RATE IN CHILDHOOD AND ADOLESCENCE

Barbara Linder; Nora V. Esteban; Alfred L. Yergey; Jorg Winterer; D. Lynn Loriaux; Fernando Cassorla

We studied the daily cortisol production rate in 33 normal children and adolescents, using a stable isotope-dilution technique employing high-performance liquid chromatography-mass spectrometry. Two indwelling intravenous catheters were inserted and tracer 9,12,12-2H3-cortisol (deuterated cortisol) was infused continuously for 30 hours. After 6 hours of tracer infusion to allow for equilibration, blood was obtained every 20 minutes for 24 hours. The mean (+/- SD) cortisol production rate was 9.5 +/- 2.5 mg/day (6.8 +/- 1.9 mg/m2/day). Cortisol production rate did not vary with sex or pubertal stage. These results suggest that the cortisol production rate in children and adolescents is significantly lower than previously estimated.


Journal of Pediatric Gastroenterology and Nutrition | 1991

Stable Isotopic Measurement of Endogenous Fecal Calcium Excretion in Children

Steven A. Abrams; James B. Sidbury; Joseph Muenzer; Nora V. Esteban; Nancy E. Vieira; Alfred L. Yergey

Using a stable isotopic technique in which 42Ca was administered via a bolus injection, we measured endogenous fecal calcium excretion, Vf, in five healthy children, aged 3-14 years. The Vf averaged 1.4 +/- 0.4 mg/kg/day, and was lower than urinary Ca excretion (Vu) in four of the five children. These results for Vf are consistent with previously reported results for Vf in healthy adults and much lower than those reported in premature infants. These results may be useful in understanding developmental changes in Ca metabolism and in interpreting dual tracer Ca isotope studies in children.


Steroids | 1990

Cortisol production rates measured by liquid chromatography/mass spectrometry

Nora V. Esteban; Alfred L. Yergey

Cortisol production rates (FPRs) in physiologic and pathologic states in humans have been investigated over the past 30 years. However, there has been conflicting evidence concerning the validity of the currently accepted value of FPRs in humans (12 to 15 mg/m2/d) as determined by radiotracer methodology. The present study reviews previous methods proposed for the measurement of FPRs in humans and discusses the applications of the first method for the direct determination of 24-hour plasma FPRs during continuous administration of a stable isotope, using a thermospray high-pressure liquid chromatography-mass spectrometry technique. The technique is fast, sensitive, and, unlike gas chromatography-mass spectrometry methods, does not require derivatization, allowing on-line detection and quantification of plasma cortisol after a simple extraction procedure. The results of determination of plasma FPRs by stable tracer/mass spectrometry are directly in units of mass/time and, unlike radiotracer methods, are independent of any determination of volume of distribution or cortisol concentration. Our methodology offers distinct advantages over radiotracer techniques in simplicity and reliability since only single measurements of isotope ratios are required. The technique was validated in adrenalectomized patients. Circadian variations in daily FRPs were observed in normal volunteers, and, to date, results suggest a lower FRP in normal children and adults than previously believed.


Steroids | 1995

Direct determination of human urinary cortisol metabolites by HPLC/CRIMS.

Alfred L. Yergey; Yohannes Teffera; Nora V. Esteban; Fred P. Abramson

Feasibility of using high performance liquid chromatographic input to the chemical reaction interface mass spectrometry system was assessed by measuring the profile of hydrolyzed urinary metabolites of [9,12,12-2H3] cortisol in six human subjects with no preparation other than hydrolysis and solid phase extraction. Relative amounts of tetrahydrocortisol, tetrahydrocortisone, and cortolones (as the sum of alpha- and beta-) were 0.417 +/- 0.047, 0.523 +/- 0.036 and 0.059 +/- 0.019, respectively. The constant reproducibility of the measurements coupled with a profile consistent with that observed by other workers shows that the technique represents an important tool in the determination of metabolites of endogenous molecules.


The Journal of Clinical Endocrinology and Metabolism | 1991

Daily Cortisol Production Rate in Man Determined by Stable Isotope Dilution/Mass Spectrometry

Nora V. Esteban; Thérèse Loughlin; Alfred L. Yergey; Joanna K. Zawadzki; John D. Booth; Jorg C. Winterer; D. Lynn Loriaux


Journal of Bone and Mineral Research | 1992

Developmental changes in calcium kinetics in children assessed using stable isotopes

Steven A. Abrams; Nora V. Esteban; Nancy E. Vieira; James B. Sidbury; Bonny Specker; Alfred L. Yergey


Journal of Mass Spectrometry | 1988

Stable isotope dilution method using thermospray liquid chromatography/mass spectrometry for quantification of daily cortisol production in humans

Nora V. Esteban; Alfred L. Yergey; Daniel J. Liberato; T. Loughlin; D. L. Loriaux


Analytical Chemistry | 1987

Stable isotope dilution thermospray liquid chromatography/mass spectrometry method for determination of sugars and sugar alcohols in humans

Nora V. Esteban; Daniel J. Liberato; James B. Sidbury; Alfred L. Yergey


Journal of Mass Spectrometry | 1987

Metabolic kinetics and quantitative analysis by isotope dilution thermospray LC/MS

Alfred L. Yergey; Nora V. Esteban; Daniel J. Liberato


Journal of Adolescent Health | 1992

Decreased calcium (Ca) absorption in adolescents with anorexia nervosa is associated with decreased bone Ca flow and increased urinary Ca excretion

Steven A. Abrams; Tomas J. Silber; Nora V. Esteban; Nancy E. Vieira; Robin Meyers; Norman H. Bell; Judith Shary; Alfred Yerqey

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Alfred L. Yergey

National Institutes of Health

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Nancy E. Vieira

National Institutes of Health

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Steven A. Abrams

University of Texas at Austin

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Daniel J. Liberato

National Institutes of Health

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James B. Sidbury

National Institutes of Health

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Fernando Cassorla

National Institutes of Health

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Jorg Winterer

National Institutes of Health

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Tomas J. Silber

George Washington University

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