DOCSLIB.ORG

Discover Essential Insights Oids Omatase TIC S ,20 Desmolase Ro with Specialized Hormone Testing

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text
Discover Essential Insights Oids Omatase TIC S ,20 Desmolase Ro with Specialized Hormone Testing TM with specialized hormone testing Discover Essential Insights the GDX-7-144 Cholesterol Steroidogenic Pathways © 2018 Genova Diagnostics Pregnenolone 17-OH-Pregnenolone DHEAAndrostenediol Essence_trifold_030718 Pregnanediol Pregnanetriol Progesterone 17-OH-Progesterone Androstenedione Testosterone Etiocholanolone 11-Deoxycortisol DHT Corticosterone THS 11β-OH-Androstenedione Androsterone Androstanediol Mineralocorticoids Cortisol Cortisone 11-OH-Androsterone Estrone (E1) Estradiol (E2) Aldosterone* a-THFTHF THE 11-OH-Etiocholanolone Adrenosterone 2-OH (E1+E2) 2-MeO (E1+E2) 17-Hydroxysteroids 800.522.4762 • www.gdx.net 16a-OH(E1) Estriol (E3) ENZYMATIC STEPS: 11-Keto-Androsterone 11-Keto-Etiocholanolone 3βHSD = 3beta-Hydroxysteroid dehydrogenase 4-OH (E1+E2) 5α = 5alpha-Reductase 17-Ketosteroids 4-MeO (E1+E2) 5β = 5beta-Reductase CYP11b1 = 11beta-Hydroxylase Hormones measurable 11βHSD = 11beta-Hydroxysteroid dehydrogenase Estrogen Metabolites 17βHSD = 17beta-Hydroxysteroid dehydrogenase by Genova Diagnostics: 17,20 Lyase = 17,20 Desmolase CYPc17 = 17alpha-Hydroxylase Measurable in Urine CYP19 = Aromatase CYP21 = 21-Hydroxylase ESTROGEN METABOLISM: Measurable in Blood 1A1 = Cytochrome p450 1A1 (CYP1A1) 3A4 = Cytochrome p450 3A4 (CYP3A4) 1B1 = Cytochrome p450 1B1 (CYP1B1) Measurable in Saliva COMT = Catechol-O-Methyl-transferase © 2016 Genova Diagnostics • e,po,steropath,031016 *Serum Testosterone Melatonin (x3) Progesterone (x3) Estrogens (x3) (E1, E2, E3) Testosterone Progesterone Melatonin (x3) Peri/Menopausal Females Estrogens (E1, E2, E3) *Serum Saliva Profiles Testosterone Melatonin (x3) Estradiol (x11) Progesterone (x11) for Cycling Females *Saliva www.gdx.net Cortisol Metabolites Genetic SNPs (add-on) 24 Hour or FMV Urine Profiles HORMONE TESTING COMPREHENSIVE-TO-SPECIFIC TESTING HORMONE Not sure where to start? Androgens & Metabolites Progesterone Metabolites Additional Tests additional product information. Please visit SALIVARY HORMONES URINARY HORMONES SERUM HORMONES Adrenocortex Estrogen Male Hormonal Estrogen Comprehensive Cortisol Awakening Adrenocortex Stress Profile with Menopause Check One Day Hormone Male Hormones Comprehensive Complete Essential Estrogens™ BIOMARKERS Menopause™ * Menopause Plus™ * Rhythm Plus™ * Rhythm™ * Cortisol, Salivary Metabolism Estronex® Profile * Hormonal Health™ Health™ * Metabolism Thyroid Response Stress Profile Cortisol Awakening Plus™ Check™ * Plus™ Melatonin Profile * Hormones™ * FMV/24Hr What sample type should I use? Response Assessment Assessment Assessment ‡ 11-Hydroxy-androsterone 11-Hydroxy-etiocholanolone 11-Keto-androsterone 11-Keto-etiocholanolone 2-Hydroxyestrone + 2-Hydroxyestradiol [2-OH(E1+E2)] also reported separately 16α-Hydroxyestrone (16α-OH E1) 4-Hydroxyestrone + 4-Hydroxyestradiol [4-OH(E1+E2)] 4-OHE1 only 2-Methoxyestrone + 2-Methoxyestradiol [2MeO(E1+E2) 2-MeOE1 only Serum 4-Methoxyestrone + 4-Methoxyestradiol [4MeO(E1+E2)] 4-MeOE1 only • Measures bound circulating hormones Anabolic/Catabolic Balance • In-office collection E/A: 5β/5α Ratio • Useful to evaluate baseline primary sex hormone levels 2-OH (E1+E2) / 16α-OHE1 • Useful to monitor bioidentical hormone therapy (oral, pellets, injectables) 2-OH (E1+E2) / 2-MeO (E1+E2) 2-OHE1 / 2-MeOE1 Anti-TG Anti-TPO Saliva Androstanediol Androsterone • Measures unbound, bioavailable hormones Cortisol x4 x4 x6 + • At-home collection Creatinine • Optimal choice to evaluate diurnal cortisol and melatonin levels Dihydrotestosterone (DHT) • Useful to evaluate baseline primary sex hormone levels • Useful to monitor bioidentical hormone therapy (oral, topical) DHEA Estradiol (E2) Estriol (E3) Estrone (E1) Urine Estrone Sulfate • Measures unbound, bioavailable hormones Etiocholanolone • Evaluates hormone metabolites Free T3 + • At-home collection Free T4 • 24-hour collection for patients on hormone therapy or First Morning Void (FMV) Insulin-Like Growth Factor 1 (IGF-1) for non-supplemented patients Melatonin Progesterone Patients with hormonal imbalance may present with: Pregnanediol • Fatigue Pregnanetriol • Weight loss or gain Prostate Specific Antigen (PSA) • Menstrual irregularities Reverse T3* • GI complaints INDIVIDUAL COMPONENTS INDIVIDUAL Sex Hormone Binding Globulin (SHBG) • Memory decline Testosterone • Low libido Tetrahydrocortisol, THF • Insomnia Tetrahydrocortisone, THE • Change in hair and skin Tetrahydrodeoxycortisol • Hot flashes allo-Tetrahydrocortisol, a-THF Using hormone testing, clinicians can customize hormone TSH and/or nutritional therapies. Add-On Androstenedione Add-on Bone Resorption Add-On Follicle Stimulating Hormone Add-On Luteinizing Hormone Add-On Prolactin Add-On Vitamin D * NOT AVAILABLE IN NEW YORK + Add-On for this test only.
Load more

Recommended publications
  • Hormone Testing Summary
    Accession # 00280399 Female Sample Report 123 A Street Sometown , CA 90266 Last Menstrual Period: Ordering Physician: DOB: 1953-10-10 Collection Times: Precision Analytical Age: 63 2016-10-02 06:00AM 2016-10-02 08:00AM Gender: Female 2016-10-01 06:00PM 2016-10-01 10:00PM 2016-10-02 02:00AM Hormone Testing Summary Key (how to read the results): Sex Hormones See Pages 2 and 3 for a thorough breakdown of sex hormone metabolites opausa n l R e a m n e g 1.8 4.5 6.0 2.3 14.0 r 5.1 2.8 1.5 P e patient low limit high limit 20.0 result 0.2-0.7 0.3-2.0 Postmenopausal range Estradiol(E2) Progesterone Testosterone (Serum Equivalent, ng/mL) Progesterone Serum Equivalent is a calculated value based on urine pregnanediol. Adrenal Hormones See pages 4 and 5 for a more complete breakdown of adrenal hormones Total DHEA Production 300 500 3000 Age Range 2516 Daily Free Cortisol Pattern 20-39 1300-3000 240 40-60 750-2000 (ng/mg) >60 500-1200 Total DHEA Production (DHEAS + Etiocholanolone + Androsterone) 180 High Range Limit 120Cortisol 80 52 2750 5930 60 230 6500 Patient Values Low Range Limit 24hr Free Cortisol cortisol Metabolized Cortisol (THF+THE) 0 (A+B+C+D) metabolism (Total Cortisol Production) Waking (A) Morning (B) Afternoon (C) Night (D) Free cortisol best reflects tissue levels. Metabolized cortisol best reflects total cortisol production. The following videos (which can also be found on the website under the listed names along with others) may aid your understanding: DUTCH Complete Overview Estrogen Tutorial Female Androgen Tutorial Cortisol Tutorial PLEASE BE SURE TO READ BELOW FOR A NY SPECIFIC LA B COMMENTS.
    [Show full text]
  • Evaluation of Deficiency of 21 -Hydroxylation in Patients with Congenital Adrenal Hyperplasia 0
    Arch Dis Child: first published as 10.1136/adc.43.230.410 on 1 August 1968. Downloaded from Arch. Dis. Childh., 1968, 43, 410. Evaluation of Deficiency of 21 -hydroxylation in Patients with Congenital Adrenal Hyperplasia 0. M. GALAL, B. T. RUDD, and N. M. DRAYER From the Institute of Child Health, University of Birmingham Congenital adrenal hyperplasia can manifest therapy in these 13 children started within the first 3 itself in a variety of clinical and biochemical weeks of life. abnormalities (Bongiovanni and Root, 1963). The In addition to the 18 patients with congenital adrenal salt-losing tendency in some of these patients can hyperplasia, 3 children with shortness of stature and 3 with early signs of puberty were given ACTH to be due to the absence of specific enzymes: dehydro- investigate their adrenal function. None of these genases or hydroxylases (Bongiovanni and Root, patients had received steroids and all had normal free 1963; Ulick et al., 1964; Visser and Cost, 1964). cortisol and 17-hydroxycorticosteroid urinary excretion In addition to the impaired production of certain rates. The age and sex of the patients in the 3 groups steroids, antagonism by steroids or other compounds and details of the steroid therapy are listed in Table I. could, theoretically, account for the salt-losing tendency (Neher, Meystre, and Wettstein, 1959; ACTH test. Twenty-four hour urine collections Jacobs et al., 1961). were obtained before and during ACTH stimulation. The purpose ofthis study was to discover whether, ACTH gel (Organon) was given intramuscularly at a copyright. despite the continuation of steroid therapy, stimula- dose of 20 I.U.
    [Show full text]
  • The Steroid Metabolome in Men with Mood and Anxiety Disorders
    Physiol. Res. 64 (Suppl. 2): S275-S282, 2015 https://doi.org/10.33549/physiolres.933067 The Steroid Metabolome in Men With Mood and Anxiety Disorders M. DUŠKOVÁ1, M. HILL1, M. BIČÍKOVÁ1, M. ŠRÁMKOVÁ1, D. ŘÍPOVÁ2, P. MOHR2, L. STÁRKA1 1Institute of Endocrinology, Prague, Czech Republic, 2National Institute of Mental Health, Klecany, Czech Republic Received May 5, 2015 Accepted May 20, 2015 Summary many other hormones and various factors have been The mood and behavior of individuals result from an orchestra of identified as modulators of mood and behavior in such many factors. Among them steroids play an important role; disorders. Recent studies have described the role of brain- however, only several common hormones have been investigated derived neurotrophic factor (BDNF) (Pluchino et al. in this respect. It has been demonstrated that some steroid 2013, Numakawa et al. 2014), thyroid hormones (Duntas metabolites long considered merely the products of steroid and Mails 2013), inflammation (Halaris 2013), immunity hormone metabolism in fact possess considerable activity in the (Pitychoutis and Papadopoulou-Daifoti 2010), melatonin CNS. For this reason we studied the steroid metabolome (Boyce and Hopwood 2013), oxytocin and vasopressin including 50 analytes in 20 men with depression, 20 men with (Scantamburlo et al. 2009, Matsuzaki et al. 2012), the anxiety and 30 healthy controls. Significant differences were renin-angiotensin-aldosterone system (Franklin et al. found not only between controls and men with either depression 2012, Murck et al. 2012), the cannabinoid system or anxiety, but also between men with depression and anxiety. (Martykánová 2010, Gorzalka and Hill 2011, Smaga et Particularly striking were those steroids until now not generally al.
    [Show full text]
  • Increased and Mistimed Sex Hormone Production in Night Shift Workers
    Published OnlineFirst March 3, 2015; DOI: 10.1158/1055-9965.EPI-14-1271 Research Article Cancer Epidemiology, Biomarkers Increased and Mistimed Sex Hormone Production & Prevention in Night Shift Workers Kyriaki Papantoniou1,2,3,4, Oscar J. Pozo2, Ana Espinosa1,2,3,4, Josep Marcos2,3, Gemma Castano-Vinyals~ 1,2,3,4, Xavier Basagana~ 1,2,3,4, Elena Juanola Pages 5, Joan Mirabent6,7, Jordi Martín8, Patricia Such Faro9, Amparo Gasco Aparici10, Benita Middleton11, Debra J. Skene11, and Manolis Kogevinas1,2,3,4,12 Abstract Background: Night shift work has been associated with Results: Night workers had higher levels of total progestagens an increased risk for breast and prostate cancer. The effect [geometric mean ratio (GMR) 1.65; 95% confidence intervals of circadian disruption on sex steroid production is a pos- (CI), 1.17–2.32] and androgens (GMR: 1.44; 95% CI, 1.03–2.00), sible underlying mechanism, underinvestigated in hum- compared with day workers, after adjusting for potential con- ans. We have assessed daily rhythms of sex hormones founders. The increased sex hormone levels among night and melatonin in night and day shift workers of both shift workers were not related to the observed suppression of sexes. 6-sulfatoxymelatonin. Peak time of androgens was significantly Methods: We recruited 75 night and 42 day workers, ages later among night workers, compared with day workers (testos- 22 to 64 years, in different working settings. Participants terone: 12:14 hours; 10:06-14:48 vs. 08:35 hours; 06:52-10:46). collected urine samples from all voids over 24 hours on a Conclusions: We found increased levels of progestagens and working day.
    [Show full text]
  • Endocrinology Test List Endocrinology Test List
    For Endocrinologists Endocrinology Test List Endocrinology Test List Extensive Capabilities Managing patients with endocrine disorders is complex. Having access to the right test for the right patient is key. With a legacy of expertise in endocrine laboratory diagnostics, Quest Diagnostics offers an extensive menu of laboratory tests across the spectrum of endocrine disorders. This test list highlights the extensive menu of laboratory diagnostic tests we offer, including highly specialized tests and those performed using highly specific and sensitive mass spectrometry detection. It is conveniently organized by glandular function or common endocrine disorder, making it easy for you to identify the tests you need to care for the patients you treat. Comprehensive Care Quest Diagnostics Nichols Institute has been pioneering state-of-the-art endocrine testing for over four decades. Our commitment to innovative diagnostics and our dedication to quality and service means we deliver solutions that enable you to make informed clinical decisions for comprehensive patient management. We strive to remain at the forefront of innovation in endocrine testing so you can deliver the highest level of patient care. Abbreviations and Footnotes NDM, neonatal diabetes mellitus; MODY, maturity-onset diabetes of the young; CH, congenital hyperinsulinism; MSUD, maple syrup urine disease; IHH, idiopathic hypogonadotropic hypogonadism; BBS, Bardet-Biedl syndrome; OI, osteogenesis imperfecta; PKD, polycystic kidney disease; OPPG, osteoporosis-pseudoglioma syndrome; CPHD, combined pituitary hormone deficiency; GHD, growth hormone deficiency. The tests highlighted in green are performed using highly specific and sensitive mass spectrometry detection. Panels that include a test(s) performed using mass spectrometry are highlighted in yellow. For tests highlighted in blue, refer to the Athena Diagnostics website (athenadiagnostics.com/content/test-catalog) for test information.
    [Show full text]
  • Comprehensive Urinary Hormone Assessments
    ENDOCRINOLOGY Complete Hormones – Analytes Comprehensive Urinary Hormone Assessments Urinary Pregesterones Urinary Glucocorticoids Urinary Androgens Urinary Estrogens Pregnanediol Cortisol, Free Testosterone Estrone Pregnanetriol Total 17-Hydroxy-corticosteroids Dehydroepiandrosterone (DHEA) Estradiol allo-Tetrahydrocortisol, a-THF Total 17-Ketosteroids Estriol Tetrahydrodeoxycortisol Androsterone 2-Hydroxyestrone Tetrahydrocortisol, THF Etiocholanolone 2-Methoxyestrone Tetrahydrocortisone, THE 11-Keto-androsterone 4-Hydroxyestrone 17-Hydroxysteriods, Total 11-Keto-etiocholanolone 4-Methoxyestrone Pregnanetriol 11-Hydroxy-androsterone 16α-Hydroxyestrone 11-Hydroxy-etiocholanolone 2-Hydroxy-estrone:16α-Hydroxyestrone ratio 2-Methoxyestrone:2-Hydroxyestrone ratio CLINICIAN INFORMATION 4-Methoxyestrone:4-Hydroxyestrone ratio ADVANCING THE CLINICAL UTILITY OF URINARY HORMONE ASSESSMENT Specimen Requirements Complete Hormones™ is Genova’s most comprehensive • 120 ml aliquot, refrigerated until shipped, urinary hormone profile, and is designed to assist with the from either First Morning Urine or 24-Hour clinical management of hormone-related symptoms. This profile Collection Why Use Complete Hormones? assesses parent hormones and their metabolites as well as key metabolic pathways, and provides insight into the contribution Hormone testing is an effective tool for assessing Related Profiles: that sex hormones may have in patients presenting with and managing patients with hormone- related symptoms. This profile supports: • Male Hormonal Health™
    [Show full text]
  • Studies on Steroid Fever II. Pyrogenic and Anti-Pyrogenic Activity in Vitro of Some Endogenous Steroids of Man
    Studies on steroid fever II. Pyrogenic and anti-pyrogenic activity in vitro of some endogenous steroids of man G. M. Dillard, Phyllis Bodel J Clin Invest. 1970;49(12):2418-2426. https://doi.org/10.1172/JCI106461. Research Article The pyrogenic properties of some C-19 and C-21 steroids were examined by in vitro incubation of human blood leukocytes with serum-buffer solutions of the steroids and injection of the 18-hr supernatants into rabbits. In previous studies this method demonstrated release of leukocyte endogenous pyrogen by etiocholanolone. With two exceptions, steroids known to cause fever in man, such as 11β-OH etiocholanolone and 3α-hydroxy-5β-pregnane-20-one were also pyrogenic in vitro. All steroids tested which are nonpyrogenic in man, such as androsterone, 3β-OH etiocholanolone, and 3α, 17α-dihydroxy-5β-pregnan-20-one were also nonpyrogenic in vitro. Solubility in aqueous solution did not correlate with pyrogenic capacity. Inhibition of pyrogen release from human leukocytes in vitro by hydrocortisone and estradiol was demonstrated. Hydrocortisone-treated leukocytes released less pyrogen than did normal leukocytes when stimulated either by etiocholanolone or by phagocytosis of heat-killed staphylococci. On the other hand, estradiol-treated blood leukocytes and mononuclear cells showed significant suppression of pyrogen release when phagocytosis, but not etiocholanolone, was used as the stimulus. When blood cells were incubated with progesterone, greater than normal amounts of pyrogen were released following phagocytosis, and the inhibiting effect of estradiol could be partially reversed. Neither estradiol nor hydrocortisone appeared to act on rabbit leukocytes. These studies indicate that a variety of naturally-occurring steroids may alter pyrogen release from leukocytes.
    [Show full text]
  • The Metabolism of Anabolic Agents in the Racing Greyhound
    The Metabolism of Anabolic Agents In the Racing Greyhound A thesis submitted in partial fulfilment of the requirements for the Degree of Doctor of Philosophy by Mr. Keith Robert Williams, B.Sc. July 1999 Department of Forensic Medicine & Science University of Glasgow Copyright © 1999 by Keith R. Williams. All rights reserved. No part o f this thesis may be reproduced in any forms or by any means without the written permission o f the author. I ProQuest Number: 13833925 All rights reserved INFORMATION TO ALL USERS The quality of this reproduction is dependent upon the quality of the copy submitted. In the unlikely event that the author did not send a com plete manuscript and there are missing pages, these will be noted. Also, if material had to be removed, a note will indicate the deletion. uest ProQuest 13833925 Published by ProQuest LLC(2019). Copyright of the Dissertation is held by the Author. All rights reserved. This work is protected against unauthorized copying under Title 17, United States C ode Microform Edition © ProQuest LLC. ProQuest LLC. 789 East Eisenhower Parkway P.O. Box 1346 Ann Arbor, Ml 48106- 1346 GLASGOW UNIVERSITY LIBRARY 111-X (coK To my parents for all their help, support and encouragement i Table of Contents i List of Figures V List of Tables VIII Summary IX Chapter 1: Drugs in Sport ...............................................................................................................................1 Introduction .................................................................................................................................................
    [Show full text]
  • AOD Biennial Review
    Introduction The Drug-Free Schools and Communities Act and Part 86 of the Education Department General Administrative Regulations (EDGAR) require each institution of higher education participating in Title IV student financial assistance to certify that it has developed and implemented a program to prevent the unlawful possession, use, and distribution of drugs and alcohol on campus and at institution-recognized events and activities. Annually, the institution must distribute to current students and employees written information about its drug and alcohol abuse prevention program, including information about related sanctions. The distribution plan must include provisions for sharing this information with new students and employees who join the institution at later points in the year as well. In addition, on a biennial basis, the institution must conduct a review to determine the effectiveness of its programs and prepare a report of the review’s findings. The report must be retained and made available to the US Department of Education upon request. Notre Dame of Maryland University (“NDMU” or “the University”) acknowledges these responsibilities, including the timely review of and reporting on the effectiveness of its prevention programs. NDMU is a private, Catholic university established in 1895 with the mission to educate leaders to transform the world. NDMU is a comprehensive university that is home to Maryland's only women's college and offers a wide variety of full and part-time undergraduate, graduate, doctoral, and certificate programs to women and men. The University enrolls approximately 2300 students and has Schools of Arts, Sciences, and Business; Education; Nursing; and Pharmacy. Additionally, the University offers programs for adult students fully online and at several locations throughout the State.
    [Show full text]
  • Alteration of the Steroidogenesis in Boys with Autism Spectrum Disorders
    Janšáková et al. Translational Psychiatry (2020) 10:340 https://doi.org/10.1038/s41398-020-01017-8 Translational Psychiatry ARTICLE Open Access Alteration of the steroidogenesis in boys with autism spectrum disorders Katarína Janšáková 1, Martin Hill 2,DianaČelárová1,HanaCelušáková1,GabrielaRepiská1,MarieBičíková2, Ludmila Máčová2 and Daniela Ostatníková1 Abstract The etiology of autism spectrum disorders (ASD) remains unknown, but associations between prenatal hormonal changes and ASD risk were found. The consequences of these changes on the steroidogenesis during a postnatal development are not yet well known. The aim of this study was to analyze the steroid metabolic pathway in prepubertal ASD and neurotypical boys. Plasma samples were collected from 62 prepubertal ASD boys and 24 age and sex-matched controls (CTRL). Eighty-two biomarkers of steroidogenesis were detected using gas-chromatography tandem-mass spectrometry. We observed changes across the whole alternative backdoor pathway of androgens synthesis toward lower level in ASD group. Our data indicate suppressed production of pregnenolone sulfate at augmented activities of CYP17A1 and SULT2A1 and reduced HSD3B2 activity in ASD group which is partly consistent with the results reported in older children, in whom the adrenal zona reticularis significantly influences the steroid levels. Furthermore, we detected the suppressed activity of CYP7B1 enzyme readily metabolizing the precursors of sex hormones on one hand but increased anti-glucocorticoid effect of 7α-hydroxy-DHEA via competition with cortisone for HSD11B1 on the other. The multivariate model found significant correlations between behavioral indices and circulating steroids. From dependent variables, the best correlation was found for the social interaction (28.5%). Observed changes give a space for their utilization as biomarkers while reveal the etiopathogenesis of ASD.
    [Show full text]
  • Endocrinology Assessments
    2013 Edition Endocrinology Assessments PRODUCT LINE GUIDE THE GENOVA DIAGNOSTICS Advantage Our comprehensive line of assessments for personalized treatment & prevention of chronic disease: • Provides Fully Licensed and Certified Laboratory Services • Saves Practitioner Time with Easy-to-Read Test Results • Features Rapid Turnaround • Includes Support for Practitioner and Patient • Offers Patient and Practitioner Billing Options Visit us anytime on the web at www.GDX.net or call 800-522-4762 Monday through Friday, 8:30 am to 6:30 pm (Eastern Time) to order tests or more information about our services. ACCREDITATION Genova Diagnostics is fully licensed federally under Clinical Laboratory Improvement Amendments (CLIA) and certified by Medicare (all states), and by New York State. TABLE OF CONTENTS Endocrinology Product Line Guide for Genova Diagnostics 2-5 Steroidogenic Pathways Chart __________________________________18 Essence Hormone Tests ____________ First Morning Void vs. 24-Hour Collection __________________________19 Specimen Selection Salivary Assessments A Guide to Choosing Sample Types ________________________________2 Menopause Plus ______________________________________________20 Complete Testing Line Rhythm ____________________________________________________22 Individual Components Breakdown Chart __________________________4 Male Hormones Plus __________________________________________24 One Day Hormone Check ______________________________________26 Therapeutic Ranges for Menopause Profile ________________________28 Profiles
    [Show full text]
  • Investigation About the Effects and the Detection of Finasteride, a Substance Which Can Be Misused As Masking Agent in Doping Control” W
    PROJECT SUMMARY “Investigation about the effects and the detection of finasteride, a substance which can be misused as masking agent in doping control” W. Schanzer, H. Geyer (German Sport University, Cologne, Germany) Finasteride is an inhibitor of 5-alpha reductase, the enzyme responsible for conversion of testosterone to dihydrotestosterone. It is administered orally in a dose of 5 mg daily for the treatment of benign prostatic hypertrophy. Since 1999 it is also admitted in several countries for the treatment of men with hair loss (androgenetic alopecia) and it seems to become a so called ,,life style drug”. The recommended dose for the treatment of hair loss is 1 mglday. Recent studies with finasteride have shown, that this substance can be misused as a potential masking agent. The application of finasteride may prevent the detection of misuse of anabolic-androgenic steroids like nandrolone, norandrostendione, norandrostenediols, dihydrotestosterone and testosterone. These preliminary results should be confirmed by more extensive studies with several volunteers. If the preliminary results can be confirmed, it should be discussed, if finasteride is added to the prohibited class of masking agents. The second aim of the study is to develop and validate a sensitive and specific method for the detection of finasteride misuse. Investigation about the effects and the detection of finasteride, a substance which can be misused as masking agent in doping control Results and conclusions Finasteride is an inhibitor of 5-alpha reductase and used for the treatment of benign prostatic hypertrophy and androgenetic alopecia. Investigations with finsteride with only one volunteer have shown, that the use of finasteride complicates the detection of the misuse of several anabolic steroids in doping control.
    [Show full text]