Rat renal epinephrine synthesis.

Kennedy, Brian P.; Elayan, Hamzeh

doi:10.1172/jci114276

Cited by 22 publications

(11 citation statements)

References 15 publications

(14 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…This synthesis was abolished when the kidney was denervated, suggesting that the renal nerves were the main sites of the (urinary) norepinephrine synthesis" 148 • "Several recent studies have demonstrated that dopamine can be generated from L-dopa in the isolated perfused rat kidney, and those findings led to the conclusion that most of the urinary dopamine could be derived from circulating L-dopa (in the kidneys)" 148 • "Recent studies from our laboratory have suggested that urinary NE (norepinephrine) may be derived, in part, from intrarenal sources in man" 149 • "We have previously reported that in standing humans a significant portion of urinary norepinephrine is derived from processes other than glomerular filtration" 149 • "Net production was observed for NE (norepinephrine), DA (dopamine), and NM (normetanephrine) in the renal metabolic compartment, suggesting that a portion of these compounds excreted in the urine may result from intrarenal synthesis or metabolism of these materials" 149 • "… urinary epinephrine may not simply be filtered from the bloodstream" and "urinary epinephrine was derived from the kidney" 150 • "We conclude that appreciable portions of renal and urinary epinephrine are synthesized in the kidney by an enzyme distinct from PNMT". 151 In reviewing the validity of the "spot baseline urinary neurotransmitter testing marketing model" it is important to determine what is being assayed and where it came from. The first assertion of the model claims that it is urinary neurotransmitters that are being assayed.…”

Section: Source Of Urinary Monoaminesmentioning

confidence: 99%

Validity of urinary monoamine assay sales under the “spot baseline urinary neurotransmitter testing marketing model”

Hinz¹,

Stein²,

Uncini³

2011

IJNRD

View full text Add to dashboard Cite

Spot baseline urinary monoamine assays have been used in medicine for over 50 years as a screening test for monoamine-secreting tumors, such as pheochromocytoma and carcinoid syndrome. In these disease states, when the result of a spot baseline monoamine assay is above the specific value set by the laboratory, it is an indication to obtain a 24-hour urine sample to make a definitive diagnosis. There are no defined applications where spot baseline urinary monoamine assays can be used to diagnose disease or other states directly. No peer-reviewed published original research exists which demonstrates that these assays are valid in the treatment of individual patients in the clinical setting. Since 2001, urinary monoamine assay sales have been promoted for numerous applications under the “spot baseline urinary neurotransmitter testing marketing model”. There is no published peer-reviewed original research that defines the scientific foundation upon which the claims for these assays are made. On the contrary, several articles have been published that discredit various aspects of the model. To fill the void, this manuscript is a comprehensive review of the scientific foundation and claims put forth by laboratories selling urinary monoamine assays under the spot baseline urinary neurotransmitter testing marketing model.

show abstract

Section: Source Of Urinary Monoaminesmentioning

confidence: 99%

Validity of urinary monoamine assay sales under the “spot baseline urinary neurotransmitter testing marketing model”

Hinz¹,

Stein²,

Uncini³

2011

IJNRD

View full text Add to dashboard Cite

show abstract

“…Most evidence suggests that plasma NE is a more reliable index. More than half of urine NE is apparently derived from the sympathetic nerves that innervate the kidney, 86,87 whereas plasma NE generally has a smaller contribution from local nerves. In addition, urine NE levels are influenced by more metabolic processes than are plasma NE levels, as is illustrated by the fact that only about 10% of plasma NE is excreted unchanged into urine in humans.…”

Section: Sympathetic Activitymentioning

confidence: 99%

Contributions of the sympathetic nervous system, glutathione, body mass and gender to blood pressure increase with normal aging: influence of heredity

Kennedy

Rao

Botiglieri³

et al. 2005

J Hum Hypertens

Self Cite

View full text Add to dashboard Cite

Body mass and sympathetic activity increase with aging and might underlie blood pressure (BP) elevation. Increased body mass index (BMI) may elevate BP by increasing sympathetic activity. Glutathione (GSH) can decrease BP, and declines with aging. We measured systolic (SBP) and diastolic BP, BMI, plasma (NE pl ) and urine norepinephrine (NE u ), and plasma GSH in n ¼ 204 twins across the age spectrum. BP correlated directly with BMI, NE pl , and NE u , but inversely with GSH. Age correlated with BP, BMI, NE pl , and NE u . BP, BMI, NE pl , and NE u were higher in older subjects than younger subjects, whereas GSH was lower with aging. In older subjects with high (above median) NE pl , SBP was 8 mmHg higher than in those of comparable age with low NE. In younger subjects with high GSH, BP was significantly lower than in younger subjects having low GSH. NE u was significantly reduced in young high-BMI subjects vs young low-BMI subjects. The heritability (h 2 ) of NE pl, NE u , and GSH ranged from B50 to B70%, and these biochemical quantities were considerably more heritable than BP. We conclude that increases in sympathetic activity contribute to aging-induced SBP elevations, especially in older females. GSH reductions apparently participate in aging-induced BP elevations, most strongly in males. BMI increases contribute to BP elevations, particularly in younger subjects. BMI elevations apparently raise BP mainly by peripheral mechanisms, with generally little sympathetic activation. Substantial h 2 for plasma GSH, NE, and urine NE suggests that such traits may be useful 'intermediate phenotypes' in the search for genetic determinants of BP.

show abstract

“…Rat kidney synthesizes E in vivo (10) and lung, heart, and several other peripheral tissues can synthesize E from norepinephrine in vitro (11)(12)(13). Recent studies in adrenalectomized rats demonstrate that extraadrenal E synthesis can play an important regulatory role in animal models of hypertension, diabetes, and glucocorticoid toxicity (14,15).…”

Section: Introductionmentioning

confidence: 99%

Nonadrenal epinephrine-forming enzymes in humans. Characteristics, distribution, regulation, and relationship to epinephrine levels.

Kennedy

Bigby²,

Ziegler³

1995

J. Clin. Invest.

Self Cite

View full text Add to dashboard Cite

Animal studies indicate that nonadrenal tissues may synthesize epinephrine (E). Here we demonstrate phenylethanolamine N-methyltransferase (PNMT) and/or nonspecific Nmethyltransferase (NMT) enzymatic activity in human lung, kidney, heart, liver, spleen, and pancreas. There was a significant overall correlation (r = 0.34) between tissue PNMT and E. PNMT and NMT in human tissues differed in substrate and inhibitor specificity, thermal stability, and antigenicity. By these criteria, PNMT in human lung and in human bronchial epithelial cells were indistinguishable from adrenal PNMT. PNMT and/or NMT activity were present in red blood cells (RBCs), and cancer cell lines. Human kidney, lung, and pancreas showed immunohistochemical staining with an antibody to adrenal PNMT. RBC PNMT activity was lower in males than females and was increased in hyperthyroidism and decreased in hypothyroidism. PNMT activity in a human bronchial epithelial cell line was dramatically increased by incubation with dexamethasone. E and 3H-E levels in plasma and urine during an intravenous infusion of 3H-E into humans indicated that kidney may synthesize half of urinary E. We conclude that PNMT and NMT are widely distributed in human tissues, that they may synthesize E in vivo and are influenced by glucocorticoid and thyroid hormones. (J. Clin. Invest. 1995Invest. . 95:2896Invest. -2902

show abstract

Rat renal epinephrine synthesis.

Cited by 22 publications

References 15 publications

Validity of urinary monoamine assay sales under the “spot baseline urinary neurotransmitter testing marketing model”

Validity of urinary monoamine assay sales under the “spot baseline urinary neurotransmitter testing marketing model”

Contributions of the sympathetic nervous system, glutathione, body mass and gender to blood pressure increase with normal aging: influence of heredity

Nonadrenal epinephrine-forming enzymes in humans. Characteristics, distribution, regulation, and relationship to epinephrine levels.

Contact Info

Product

Resources

About

Rat renal epinephrine synthesis.

Cited by 22 publications

References 15 publications

Validity of urinary monoamine assay sales under the &ldquo;spot baseline urinary neurotransmitter testing marketing model&rdquo;

Validity of urinary monoamine assay sales under the &ldquo;spot baseline urinary neurotransmitter testing marketing model&rdquo;

Contributions of the sympathetic nervous system, glutathione, body mass and gender to blood pressure increase with normal aging: influence of heredity

Nonadrenal epinephrine-forming enzymes in humans. Characteristics, distribution, regulation, and relationship to epinephrine levels.

Contact Info

Product

Resources

About

Validity of urinary monoamine assay sales under the “spot baseline urinary neurotransmitter testing marketing model”

Validity of urinary monoamine assay sales under the “spot baseline urinary neurotransmitter testing marketing model”