DOCSLIB.ORG

Pharmacopoeial Reference Standards and Their Current Lot Numbers EP, EPISA, ICRS, USP, BP December 2016

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text
Pharmacopoeial Reference Standards and Their Current Lot Numbers EP, EPISA, ICRS, USP, BP December 2016 Pharmacopoeial reference standards and their current lot numbers EP, EPISA, ICRS, USP, BP December 2016 New: LGCon Standards LinkedIn Pharma Dear user, This catalogue includes all pharmacopoeial reference materials from EP, EPISA, ICRS, USP and BP available at LGC, as well as their current lot numbers. We update the catalogue on a monthly basis so that you can use the lot numbers to easily track the expiry dates of your stocked reference materials. We took the lot information from actual data from the Pharmacopoeias and correct at the time of production. We retained all spelling and information as provided by the Pharmacopoeias. The list was compiled with caution, however errors in this list may be possible, and LGC is not responsible for any consequences as a result of these errors, may it be errors in the original Pharmacopoeia data, or from LGC during compilation of this list. For any questions or orders please contact your local LGC office. You will find all contact details on the last page of this list. Alternatively, you can browse and buy pharmaceutical reference materials online at www.lgcstandards.com. Stay connected via LinkedIn (LGC Standards Pharma) or Twitter @LGCStdsPharma Kind regards Your LGC Standards Team LGC, Queens Road, Teddington, Middlesex, TW11 0LY, United Kingdom Tel.: +44 (0)20 8943 8480, Fax: +44 (0)20 8943 7554 E-Mail: [email protected] European Pharmacopoeia (EP) Available Current Unit Cat. No. Name What is new? since Batch No. Quantity 24.10.2016 EPY0001912 Erythromycin A 4 250 mg New batch! EPY0001561 Abacavir sulfate 1 20 mg EPY0001552 Abacavir for peak identification 1 10 mg EPY0001551 Abacavir for system suitability 1 10 mg EPY0000055 Acamprosate calcium - reference spectrum 1 n/a EPY0000116 Acamprosate impurity A 2 110 mg EPY0000500 Acarbose 3 100 mg EPY0000354 Acarbose for identification 1 10 mg EPY0000427 Acarbose for peak identification 3 20 mg EPA0040000 Acebutolol hydrochloride 1 50 mg EPY0000359 Acebutolol impurity B 2 10 mg EPY0000127 Acebutolol impurity C 1 20 mg EPY0000128 Acebutolol impurity I 2 0.004 mg EPY0000056 Aceclofenac - reference spectrum 1 n/a EPY0000085 Aceclofenac impurity F 2 15 mg EPY0000086 Aceclofenac impurity H 1 10 mg EPY0001094 Aceclofenac for peak identification 1 10 mg EPY0000810 Acemetacin 1 100 mg EPY0000811 Acemetacin impurity A 1 10 mg EPY0000842 Acemetacin impurity mixture 1 0.06 mg EPA0070000 Acesulfame potassium 2 50 mg EPA0070020 Acesulfame potassium impurity B 4 15 mg EPA0100000 Acetazolamide 1 100 mg EPY0001084 Acetazolamide for system suitability 2 0.0068 mg EPY0000002 Acetylcholine chloride 1 50 mg EPA0150000 Acetylcysteine 3 50 mg EPA0152000 Acetylcysteine impurity C 11 10 mg EPA0153000 Acetylcysteine impurity D 6 10 mg EPY0000565 ß-Acetyldigoxin 2 50 mg EPY0000642 ß-Acetyldigoxin for peak identification 1 10 mg EPA0200000 Acetylsalicylic acid 5 10 mg Follow LGC Standards Pharma on LinkedIn and December 2016 Twitter @LGCStdsPharma Pharmaceutical Lot List - NL European Pharmacopoeia (EP) Available Current Unit Cat. No. Name What is new? since Batch No. Quantity EPY0001460 Acetylsalicylic acid for peak identification 3 10.3 mg EPY0001462 Acetylsulfadiazine 1 0.002 mg EPA0208000 N-Acetyltryptophan 2 125 mg EPA0202000 N-Acetyltyrosine 1 200 mg EPY0000693 Acholeplasma laidlawii BRP 1 1 ml EPA0220000 Aciclovir 3 75 mg EPY0001271 Aciclovir for peak identification 1 4 0.3 mg EPY0001269 Aciclovir for peak identification 2 4 0.004 mg EPY0001264 Aciclovir for system suitability 1 10 mg EPA0225000 Acitretin 2 100 mg EPY0001463 Actaea racemosa HRS 1 1200 mg EPY0001543 Actaea racemosa for assay CRS 1 300 mg EPY0001464 Actaea racemosa dry extract for system suitability HRS 1 1200 mg EPY0001121 Adapalene 1 100 mg EPY0001120 Adapalene impurity C 3 6 mg EPY0001119 Adapalene for peak identification 2 2.02 mg EPA0230000 Adenine 2 50 mg EPA0230200 Adenosine 1 50 mg EPY0000110 Adipic acid 1 50 mg EPY0000882 Adrenaline 1 5 mg EPY0000740 Adrenaline impurity mixture 3 0.005 mg EPY0000883 Adrenaline with impurity F 1 10 mg EPA0300000 Adrenaline tartrate 6 100 mg EPY0000707 Adrenaline tartrate with impurity A 1 15 mg EPY0001527 Aescin for LC assay HRS 1 150 mg EPY0001724 Agnus castus fruit dry extract 1 350 mg EPA0325000 Alanine 3 60 mg EPA0325100 Albendazole 2 50 mg EPA0325200 Alcuronium chloride 2 50 mg EPA0325450 Alfacalcidol 9 5 mg EPY0001601 Alfacalcidol for system suitability 1 2.5 mg Follow LGC Standards Pharma on LinkedIn and December 2016 Twitter @LGCStdsPharma Pharmaceutical Lot List - NL European Pharmacopoeia (EP) Available Current Unit Cat. No. Name What is new? since Batch No. Quantity EPA0325451 Alfacalcidol - reference spectrum 1 n/a EPA1225000 Alfadex 3 150 mg EPA0325500 Alfentanil hydrochloride - reference spectrum 1 n/a EPY0000832 Alfuzosin for system suitability 1 10 mg EPA0325800 Alfuzosin hydrochloride 2 10 mg EPY0001583 Alimemazine hemitartrate 1 15 mg EPY0001581 Alimemazine for system suitability 1 5 mg EPA0349000 Allantoin 1 60 mg EPA0350000 Allopurinol 3 100 mg EPA0350010 Allopurinol impurity A 2 10 mg EPA0350020 Allopurinol impurity B 3 10 mg EPA0350030 Allopurinol impurity C 3 10 mg EPA0350040 Allopurinol impurity D 4 15 mg EPA0350050 Allopurinol impurity E 1 20 mg EPA0351000 Allylstrychnine bromide 1 10 mg EPY0000235 Almagate 2 50 mg EPY0000255 Almagate - reference spectrum 1 n/a EPA0357000 Alprazolam - * psy 2 100 mg EPA0360000 Alprenolol hydrochloride 1 100 mg EPY0000054 Alprostadil 3 25 mg EPY0000606 Altizide 2 150 mg EPY0000843 Altizide impurity B 1 15 mg EPY0000687 Alverine citrate 1 5 mg 04.11.2016 EPY0001819 Alverine impurity C 2 40 mg New batch! EPY0000607 Alverine impurity D 1 10 mg EPA0363000 Amantadine hydrochloride 1 100 mg EPA0363700 Ambroxol hydrochloride 3 125 mg EPA0900000 Amfetamine sulfate - reference spectrum 1 n/a EPA0365000 Amidotrizoic acid dihydrate 1 100 mg EPY0001461 Amidotrizoic acid for system suitability 1 0.08 mg EPA0368000 Amikacin 3 200 mg Follow LGC Standards Pharma on LinkedIn and December 2016 Twitter @LGCStdsPharma Pharmaceutical Lot List - NL European Pharmacopoeia (EP) Available Current Unit Cat. No. Name What is new? since Batch No. Quantity EPY0001467 Amikacin impurity I 1 20 mg EPY0001117 Amikacin for system suitability 3 10 mg EPA0365900 Amikacin sulfate 3 200 mg EPA0370000 Amiloride hydrochloride 2 100 mg EPY0000020 Amiloride impurity A 3 20 mg EPY0000173 4-Aminobenzoic acid 2 60 mg EPA0420000 Aminocaproic acid 1 50 mg EPA0460000 7-Aminodesacetoxycephalosporanic acid 2 20 mg EPA0496000 Aminoglutethimide 1 125 mg EPA0496005 Aminoglutethimide impurity A 1 20 mg EPA0496020 Aminoglutethimide impurity D 1 10 mg EPA0575000 Amiodarone hydrochloride 3 100 mg EPY0000129 Amiodarone impurity D 3 20 mg EPY0000130 Amiodarone impurity E 3 20 mg EPA0590000 Amisulpride 2 10 mg EPY0001534 Amisulpride for system suitability 1 1.0015 mg EPY0000563 Amitriptyline hydrochloride 1 10 mg EPY0000049 Amlodipine besilate 4 150 mg EPY0001068 Amlodipine impurity A 3 15 mg EPY0001069 Amlodipine impurity B 3 15 mg EPY0001070 Amlodipine impurity G 3 10 mg EPY0001067 Amlodipine for peak identification 3 15 mg EPY0000302 Ammonio methacrylate copolymer(type A) - reference spectrum 1 n/a EPY0000303 Ammonio methacrylate copolymer(type B) - reference spectrum 1 n/a EPA0650000 Amobarbital - * psy 1 500 mg EPA0700000 Amobarbital sodium - * psy 1 500 mg EPY0001794 Amorolfine Hydrochloride 1 10 mg EPY0001795 Amorolfine for system suitability 1 10 mg EPA0800000 Amoxicillin trihydrate 5 200 mg 07.11.2016 EPY0001521 Amoxicillin trihydrate for performance verification 2 5000 mg New batch! EPY0000005 Amphotericin B 5 100 mg Follow LGC Standards Pharma on LinkedIn and December 2016 Twitter @LGCStdsPharma Pharmaceutical Lot List - NL European Pharmacopoeia (EP) Available Current Unit Cat. No. Name What is new? since Batch No. Quantity EPY0001361 Amphotericin B for microbiological assay 1 100 mg EPY0001014 Amphotericin B for peak identification 2 10 mg EPA1000000 Ampicillin (anhydrous) 5 220 mg EPA1100000 Ampicillin trihydrate 2 150 mg EPY0001244 Amylmetacresol 1 285 mg EPY0001245 Amylmetacresol for peak identification 1 10 mg EPY0001522 Anastrozole 1 100 mg EPY0001531 Anastrozole impurity E 1 10 mg 04.11.2016 EPY0001870 Andrographis herb HRS 1 2050 mg New compound! 04.11.2016 EPY0001866 Andrographolide 1 15 mg New compound! EPY0001753 Anemarrhena rhizome for system suitability HRS 1 150 mg EPY0001386 Angelica dahurica root HRS 1 160 mg EPY0001385 Angelica pubescens root 1 500 mg EPA1200000 Anhydrotetracycline hydrochloride 5 25 mg EPY0001466 Anhydrous Docetaxel 1 15 mg EPA1210000 Antazoline hydrochloride 1 50 mg EPY0001777 Apigenin 7-glucoside 1 25 mg EPY0001465 Apomorphine hydrochloride hemihydrate 1 15 mg EPY0001471 Apomorphine impurity B (morphine sulfate) * - narc 1 40 mg EPA1220000 Alpha-apo-oxytetracycline 5 20 mg EPA1230000 Beta-apo-oxytetracycline 5 20 mg EPY0001825 Aprepitant 1 150 mg EPY0001826 Aprepitant for system suitability 1 15 mg EPY0001154 Aprotinin for system suitability 1 2.7 mg EPA1250000 Aprotinin solution BRP 4 0.5 mL EPA1269000 L-Arabinitol 2 10 mg EPY0000806 Arbutin 2 110 mg EPA1270000 Arginine 4 60 mg EPY0000304 Arginine aspartate 1 20 mg EPA1271000 Arginine hydrochloride 3 60 mg EPY0001649 Aripiprazole 2 170 mg Follow LGC Standards Pharma on LinkedIn and December 2016 Twitter @LGCStdsPharma Pharmaceutical Lot List - NL European Pharmacopoeia (EP) Available Current Unit Cat. No. Name What is new? since Batch No. Quantity EPY0001650 Aripiprazole impurity F 2 15 mg EPY0001323 Aristolochia 1 140 mg EPY0001185 Aristolochic
Load more

Recommended publications
  • Individual Patient & Medication Factors That Invalidate Morphine
    Individual Patient & Medication Factors that Invalidate Morphine Milligram Equivalents Presented on June 7-8, 2021 at FDA Collaborative with various Federal Government Agency Stakeholders Jeffrey Fudin, PharmD, FCCP, FASHP, FFSMB Clinical Pharmacy Specialist & PGY2 Pain Residency Director Stratton VAMC, Albany NY Adjunct Associate Professor Albany College of Pharmacy & Health Sciences, Albany NY Western New England University College of Pharmacy, Springfield MA President, Remitigate Therapeutics, Delmar NY Disclosures Affiliation Role/Activities Abbott Laboratories Speaking, non-speakers bureau AcelRx Pharmaceuticals Acute perioperative pain (speakers bureau, consulting, advisory boards) BioDelivery Sciences International Collaborative publications, consulting, advisory boards Firstox Laboratories Micro serum testing for substances of abuse (consulting) GlaxoSmithKline (GSK) Collaborative non-paid poster presentations) Hisamitsu America Inc Advisory Board Hikma Pharmaceuticals Advisory Board Scilex Pharmaceuticals Collaborative non-paid publications Salix Pharmaceuticals Speakers bureau, consultant, advisory boards Torrent Pharmaceuticals Lecture, non-speakers bureau Learning Objectives At the completion of this activity, participants will be able to: 1. Explain opioid conversion and calculation strategies when developing a care plan for patients with chronic pain. 2. Assess patient-specific factors that warrant adjustment to an opioid regimen. 3. Identify important drug interactions that can affect opioid serum levels. 4. Describe how pharmacogenetic differences can affect opioid efficacy, toxicity, and tolerability. Not All Opioids are Created Equally Issues with MEDD & Opioid Conversion1-4 › Pharmacogenetic variability › Drug interactions › Lack of universal morphine equivalence › Specific opioids that should never have an MEDD – Methadone, Buprenorphine, Tapentadol, Tramadol 1. Fudin J, Marcoux MD, Fudin JA. Mathematical Model For Methadone Conversion Examined. Practical Pain Management. Sept. 2012. 46-51. 2. Donner B, et al.
    [Show full text]
  • Analysis of Oxycodone and Its Metabolites-Noroxycodone, Oxymorphone, and Noroxymorphone in Plasma by LC/MS with an Agilent ZORBAX Stablebond SB -C18 LC Column
    Analysis of Oxycodone and Its Metabolites-Noroxycodone, Oxymorphone, and Noroxymorphone in Plasma by LC/MS with an Agilent ZORBAX StableBond SB -C18 LC Column Application Note Pharmaceutical Authors Abstract Linda L. Risler Oxycodone and its oxidative metabolites (noroxycodone, oxymorphone, and Fred Hutchinson Cancer Research noroxymorphone) were analyzed by high performance liquid chromatography/mass Center, spectrometry (HPLC/MS), coupled with chromatographic separation by an Agilent Seattle, WA 98109 ZORBAX Rapid Resolution High Throughput (RRHT) StableBond SB-C18 column. The method used an ammonium acetate/acetonitrile gradient with detection by a mass Anne E. Mack spectrometer in electrospray mode with positive polarity. Spiked human plasma Agilent Technologies, Inc. samples underwent solid phase extraction (SPE) prior to LC/MS analysis. This method provided good linearity (R 2 > 0.9900) and reproducibility (< 10% difference between duplicates) for all compounds, while increasing productivity with a fast, efficient analysis and minimal solvent usage. Introduction Experimental Oxycodone was developed in 1916 as an opioid analgesic An Agilent 1100 Series LC/MS was used for this work: medication intended to replace the far too addictive analgesic at the time, heroin. Today, oxycodone is a Schedule II drug in • Agilent G1312A Binary Pump. Mobile phase A: 20 mM the US, which means, while it has proven medical uses, it is ammonium acetate, pH 4.0 and B: acetonitrile. Flow rate still considered highly addictive with the possibility of both was 0.300 mL/min. Hold 5% B for 2.33 minutes, then physical and psychological dependencies. Figure 1 shows increase B from 5% to 20% from 2.33 to 4.33 minutes, stop oxycodone and its metabolic scheme, yielding noroxycodone, time is 6 minutes, and post time is 4 minutes.
    [Show full text]
  • Presentation Slides (PDF)
    Urine toxicology testing to support pain management and treatment for substance use disorder Yifei Yang, PhD, DABCC Medical Director, Toxicology, ARUP Laboratories Assistant Professor, University of Utah Learning Objectives and Presentation Outline • Describe the general analytical workflow of urine drug testing • Understand the testing approaches for medication compliance in pain management and treatment for substance use disorder (SUD) settings • Recognize the utilities and limitations of qualitative and quantitative test results • Discuss case-based unexpected urine drug testing results and considerations for results interpretation Urine toxicology testing to support controlled substance prescription and monitoring • Pain management and SUD treatment • Long-term prescription of controlled substances • Various opiates: hydrocodone, oxycodone, etc. at various doses • Buprenorphine, with naloxone (Suboxone) • Co-medication with benzodiazepines, heroin, and other opiates can increase risk for over-dose • Urine toxicology testing is recommended: • Baseline testing prior to prescription • Annual monitoring (minimal), interval up to clinician discretion • Detect undisclosed medication use • Confirm expected medication use CDC Guideline for Prescribing Opioids for Chronic Pain. (2016) Centers for Disease Control and Prevention. Urine toxicology testing is used to confirm the presence of prescribed medications • Drug presence prevalence: • High positivity rate • Patients are mostly taking medications • Appropriate positive cutoffs are needed
    [Show full text]
  • Drug Plasma Half-Life and Urine Detection Window | January 2019
    500 Chipeta Way | Salt Lake City, UT 84108-1221 Phone: (800) 522-2787 | Fax: (801) 583-2712 www.aruplab.com | www.arupconsult.com DRUG PLASMA HALF-LIFE AND URINE DETECTION WINDOW | JANUARY 2019 URINE- PLASMA DRUG, DRUG METABOLITE(S)* COMMON TRADE AND STREET NAMES, NOTES DETECTION HALF-LIFEt WINDOWt STIMULANTS Benzedrine, dexedrine, Adderall, Vyvanse, speed; could be methamphetamine Amphetamine 7–34 hours 1–5 days metabolite; if so, typically < 30 percent of parent Cocaine Coke, crack; parent drug rarely observed due to short half-life 0.7–1.5 hours < 1 day Benzoylecgonine Cocaine metabolite 5.5–7.5 hours 1–2 days Desoxyn, methedrine, Vicks inhaler (D- and L-isomers not resolved; low concentrations Methamphetamine expected if the source is Vicks); selegeline (Atapryl, Carbex, Eldepryl, Zelapar) 6–17 hours 1–5 days metabolite Methylenedioxyamphetamine (MDA) MDA 11–17 hours 1–3 days Methylenedioxyethylamphetamine (MDEA) MDEA, MDE, Eve 6–11 hours 1–3 days Methylenedioxymethamphetamine (MDMA) MDMA, XTC, ecstasy, Molly 6–10 hours 1–3 days Methylphenidate Ritalin, Concerta, Focalin, Metadate, Methylin 1.4–4.2 hours < 1 day Ritalinic acid Methylphenidate metabolite 1.8–2.5 hours < 1 day Phentermine Adipex-P, Lomaira, Qsymia 19–24 hours 1–5 days OPIOIDS Buprenorphine Belbuca, Buprenex, Butrans, Suboxone, Subutex, Sublocade, Zubsolv 26–42 hours 1–7 days Norbuprenorphine, Glucuronides Buprenorphine metabolites 15–150 hours 1–14 days Included in many preparations; morphine metabolite; may be a contaminant if < 2 Codeine 1.9–3.9 hours 1–3 days percent of morphine Fentanyl Actiq, Duragesic, Fentora, Lazanda, Sublimaze, Subsys, Ionsys 3–12 hours 1–3 days Norfentanyl Fentanyl metabolite 9–10 hours 1–3 days Heroin Diacetylmorphine, dope, smack, dust; parent drug not detected.
    [Show full text]
  • NIDA Drug Supply Program Catalog, 25Th Edition
    RESEARCH RESOURCES DRUG SUPPLY PROGRAM CATALOG 25TH EDITION MAY 2016 CHEMISTRY AND PHARMACEUTICS BRANCH DIVISION OF THERAPEUTICS AND MEDICAL CONSEQUENCES NATIONAL INSTITUTE ON DRUG ABUSE NATIONAL INSTITUTES OF HEALTH DEPARTMENT OF HEALTH AND HUMAN SERVICES 6001 EXECUTIVE BOULEVARD ROCKVILLE, MARYLAND 20852 160524 On the cover: CPK rendering of nalfurafine. TABLE OF CONTENTS A. Introduction ................................................................................................1 B. NIDA Drug Supply Program (DSP) Ordering Guidelines ..........................3 C. Drug Request Checklist .............................................................................8 D. Sample DEA Order Form 222 ....................................................................9 E. Supply & Analysis of Standard Solutions of Δ9-THC ..............................10 F. Alternate Sources for Peptides ...............................................................11 G. Instructions for Analytical Services .........................................................12 H. X-Ray Diffraction Analysis of Compounds .............................................13 I. Nicotine Research Cigarettes Drug Supply Program .............................16 J. Ordering Guidelines for Nicotine Research Cigarettes (NRCs)..............18 K. Ordering Guidelines for Marijuana and Marijuana Cigarettes ................21 L. Important Addresses, Telephone & Fax Numbers ..................................24 M. Available Drugs, Compounds, and Dosage Forms ..............................25
    [Show full text]
  • Prediction of Drug Interactions with Methadone, Buprenorphine and Oxycodone from in Vitro Inhibition of Metabolism
    The author(s) shown below used Federal funds provided by the U.S. Department of Justice and prepared the following final report: Document Title: Prediction of Drug Interactions with Methadone, Buprenorphine and Oxycodone from In Vitro Inhibition of Metabolism Author(s): David E. Moody, Ph.D. Document No.: 250127 Date Received: July 2016 Award Number: 2011-DN-BX-K532 This report has not been published by the U.S. Department of Justice. To provide better customer service, NCJRS has made this federally funded grant report available electronically. Opinions or points of view expressed are those of the author(s) and do not necessarily reflect the official position or policies of the U.S. Department of Justice. February 2016 Research and Development in Forensic Toxicology Prediction of drug interactions with methadone, buprenorphine and oxycodone from in vitro inhibition of metabolism Final Technical Report Submitted electronically to: U.S. Department of Justice Office of Justice Programs National Institute of Justice Prepared by: David E. Moody. Ph.D. Director of the Center for Human Toxicology, and Research Professor of Pharmacology and Toxicology [email protected] / 801-581-5117 NIJ Award Number: 2011-DN-BX-K532 Reporting Period: January 1, 2012 to December 31, 2015 Recipient Organization: University of Utah 75 South 2000 East, Room 222 Salt Lake City, UT 84112-8930 Organizational DUNS: 0090953650000 EIN: 876000525 This document is a research report submitted to the U.S. Department of Justice. This report has not been published by the Department. Opinions or points of view expressed are those of the author(s) and do not necessarily reflect the official position or policies of the U.S.
    [Show full text]
  • Interpretation of Drug Testing Results in Medication Assisted Treatment
    Interpretation of Drug Testing Results in Medication Assisted Treatment By: Paul L. Cary Independent Forensic Toxicology Consultant What Does This Result Mean? Two-Step Testing Approach ■ screening test – designed to separate negative samples from samples that are “presumptively” positive ■ confirmation test – follow-up procedure designed to validate positive test results ■ why can’t you adjudicate based on the screening test results? ■ FALSE POSITIVES Drug tests & cross reactivity: ■ screening tests can and do react to “non-target” compounds ◆ amphetamines ◆ benzodiazepines ■ obtain list of interfering compounds from lab or on-site test vendor ■ study results have demonstrated accuracy rates for initial screening tests as low as 70% ■ confirm positive results Typical Cutoff Levels screening & confirmation ■ amphetamines * 500 ng/mL 250 ng/mL ■ benzodiazepines 300 ng/mL variable ■ cannabinoids * 20 & 50 ng/mL 15 ng/mL ■ cocaine (crack)* 150 ng/mL 100 ng/mL ■ opiates (heroin) * 300/2000 ng/mL variable ■ phencyclidine (PCP) * 25 ng/mL 25 ng/mL ■ alcohol 20 mg/dL 10 mg/dL ◆ * SAMHSA (formerly NIDA) drugs What is a “cutoff” level ? ■ cutoffs are not designed to frustrate CJ professionals ■ a drug concentration, administratively established for a drug test that allows the test to distinguish between negative and positive sample - “threshold” ■ cutoffs provide important safeguards: ◆ scientific purposes (detection accuracy) ◆ legal protections (evidentiary admissibility) ■ measured in ng/mL = ppb Cutoffs and False Positives as you lower you
    [Show full text]
  • Review Memorandum
    510(k) SUBSTANTIAL EQUIVALENCE DETERMINATION DECISION SUMMARY ASSAY AND INSTRUMENT COMBINATION TEMPLATE A. 510(k) Number: K130082 B. Purpose for Submission: New Device C. Measurand: Amphetamine, Barbiturates, Cocaine, Marijuana, Methadone, Methamphetamine, Morphine, Oxycodone, Phencyclidine D. Type of Test: Qualitative immunochromatographic tests for drugs of abuse in urine E. Applicant: GenPrime Inc. F. Proprietary and Established Names: The GenPrime Drugs of Abuse (DOA) Reader System G. Regulatory Information: 1. Regulation section: 21 CFR §862.3100, Amphetamine Test System 21 CFR §862.3150, Barbiturate Test System 21 CFR §862.3250, Cocaine and cocaine metabolite Test System 21 CFR §862.3870, Cannabinoid Test System 21 CFR §862.3620, Methadone Test System 21 CFR §862.3610, Methamphetamine Test System 21 CFR §862.3640, Morphine test system 21 CFR §862.3650, Opiate Test System Phencyclidine, Unclassified 21 CFR §862.2400, Densitometer/Scanner (integrating, reflectance, TLC, or radiochromatogram) for clinical use 2. Classification: Class II – for all except Phencyclidine and the Densitometer/Scanner Phencyclidine – Unclassified Densitometer/Scanner – Class I 3. Product code: DKZ, DIS, DIO, LDJ, DJR, DJC, DJG, LCM, DNK, JQT 4. Panel: Clinical Toxicology (91) and Clinical Chemistry (75) H. Intended Use: 1. Intended use(s): See Indications for Use below. 2. Indication(s) for use: The GenPrime Drugs of Abuse (DOA) Reader System consists of the GenPrime DOA Reader, GenPrime DOA Windows®-compatible Software and compatible qualitative immunochromatographic, OS Cup and Split Key Cup (SK Cup) test devices. The GenPrime DOA Reader System is for in vitro diagnostic use and is intended for prescription use in laboratories, point-of-care, and workplaces by trained users.
    [Show full text]
  • Number: K040257 B. Analyte: THC An
    510(k) SUBSTANTIAL EQUIVALENCE DETERMINATION DECISION SUMMARY DEVICE ONLY TEMPLATE A. 510(k) Number: k040257 B. Analyte: THC and carboxy-THC C. Type of Test: Qualitative screening test: immunoassay Quantitative confirmatory test: GC-MS-MS D. Applicant: Quest Diagnostics, Inc. E. Proprietary and Established Names: Quest Diagnostics Haircheck-DT (THC) F. Regulatory Information: 1. Regulation section: 21 CFR § 862.3870 2. Classification: II 3. Product Code: LDJ 4. Panel: Toxicology (91) G. Intended Use: 1. Intended use(s): Refer to Indications for use. 2. Indication(s) for use: The Quest Diagnostics HairCheck-DT (THC-COOH) is a bipartite device employing enzyme-linked immunosorbent assay (ELISA) for qualitative screening at 1.0 pg/mg hair of THC-COOH and Gas Chromatography – Mass Spectroscopy – Mass Spectroscopy (GC-MS-MS) for confirmation and the final quantitative reporting of THC-COOH in human hair samples for the purpose of identifying chronic marijuana use. This process has not been evaluated with hair specimens other than head. This process is intended exclusively for in-house professional use only. The process is not intended for sale to anyone. Clinical consideration and professional judgement should be applied to any drug of abuse test result. Page 2 of 16 The device is for in vitro diagnostic use. The device is for prescription use only. 3. Special condition for use statement(s): The Quest Diagnostics HairCheck-DT (THC-COOH) combines a screening method (immunoassay) with a confirmation method (GC-MS-MS) in one test system. A negative screening result is reported as negative. A presumptive positive screening result is not reported until it has been confirmed by GC- MS-MS.
    [Show full text]
  • Federal Register/Vol. 85, No. 230/Monday, November 30, 2020
    76604 Federal Register / Vol. 85, No. 230 / Monday, November 30, 2020 / Notices notifications disclosing all changes in Act on September 18, 2020 (85 FR DEPARTMENT OF JUSTICE membership. 58390). Drug Enforcement Administration On September 10, 2018, CONFERS Suzanne Morris, [Docket No. DEA–688E] filed its original notification pursuant to Chief, Premerger and Division Statistics, Section 6(a) of the Act. The Department Antitrust Division. Established Aggregate Production of Justice published a notice in the [FR Doc. 2020–26362 Filed 11–27–20; 8:45 am] Federal Register pursuant to Section Quotas for Schedule I and II Controlled BILLING CODE P Substances and Assessment of 6(b) of the Act on October 19, 2018 (83 Annual Needs for the List I Chemicals FR 53106). Ephedrine, Pseudoephedrine, and The last notification was filed with DEPARTMENT OF JUSTICE Phenylpropanolamine for 2021 the Department on May 1, 2020. A notice was published in the Federal Antitrust Division AGENCY: Drug Enforcement Register pursuant to Section 6(b) of the Administration, Department of Justice. Act on May 28, 2020 (85 FR 32049). Notice Pursuant to the National ACTION: Final order. Cooperative Research and Production Suzanne Morris, Act of 1993—Cooperative Research SUMMARY: This final order establishes Chief, Premerger and Division Statistics, Group on AC2AT–II the initial 2021 aggregate production Antitrust Division. quotas for controlled substances in [FR Doc. 2020–26358 Filed 11–27–20; 8:45 am] Notice is hereby given that, on schedules I and II of the Controlled Substances Act and the assessment of BILLING CODE 4410–11–P November 19, 2020, pursuant to Section 6(a) of the National Cooperative annual needs for the list I chemicals Research and Production Act of 1993, ephedrine, pseudoephedrine, and DEPARTMENT OF JUSTICE 15 U.S.C.
    [Show full text]
  • Patient and Billing Information (Please Use Name Printed on Insurance Card) Last Name First Name M.I
    Schedule Adherence Specialist Suggestion: 1. New/Initial Evaluation/Return Magnolia Medical Group | CLIA # 06D2121590 | NPI# 1043769862 after 2 months. th 2. Stabilizing/Weekly/Possible Laboratory Address: 10515 E 40 Ave, STE 115 Denver, CO 80239 th missed appts./Relapsed Office Address: 10515 E 40 Ave, STE 115 Denver, CO80239 3. Maintenance/Monthly/2x Phone: (303) 209-5115| Fax: (720) 638-5562| Email: [email protected] | Website: www.magnoliamed.com monthly/ No missed appts. Patient and Billing Information (Please use name printed on insurance card) Last Name First Name M.I. S.S.N. / Patient ID D.O.B. Street Address City State Zip Phone Gender Insurance Provider Policy # Group # Billing (Select One) Private Insurance Client Bill Write in ICD-10 Diagnosis Codes Medicare Medicaid Self-Pay Workers Comp Patient Release and Consent (Please attach copy of patient demographics and front and back of insurance card) Consent / Insurance Release: I voluntarily consent to the collection and testing of my specimen and certify that the specimen identified on this form is my own; it is fresh and has not been adulterated in any manner. I certify that the information provided on this form and on the specimen container is accurate. I authorize my insurance benefits to be paid directly to Magnolia Medical Group, for service I receive. I acknowledge that the lab may be an out-of-network facility within my insurance. I am also aware that in some circumstances my insurance will send the payment directly to me for the service provided. If this occurs, I agree to endorse the insurance check and forward it to the lab within 30 days of receipt.
    [Show full text]
  • Preparation of Noroxymorphone from Morphine
    Europaisches Patentamt European Patent Office © Publication number: 0 158 476 Office europeen des brevets A1 © EUROPEAN PATENT APPLICATION © Application number: 85302103.8 © int ci ": C 07 D 489/08 C 07 D 489/02 © Date of filing: 26.03.85 //A61K3 1/485 © Priority: 27.03.84 US 593744 © Applicant: MALUNCKRODT, INC. 20.03.85 US 713932 675 McDonnell Boulevard P.O. Box 5840 St. Louis Missouri 63134(US) 2) Date of publication of application: © Inventor: Wallace, Rebecca A. 16.10.85 Bulletin 85/42 1444 Sunnytree Lane Manchester Missouri 6301 1 (US) , §) Designated Contracting States: AT BE CH DE FR GB IT LI LU NL SE © Representative: Eyles, Christopher Thomas et al, BATCHELLOR. KIRK & EYLES 2 Pear Tree Court Farringdon Road London, ECIRODS(GB) © Preparation of noroxymorphone from morphine. 3-O,N-(diethoxycarbonyl) normorphine, which may be prepared by reaction of morphine with ethyl chloroformate, is converted to 3-0,n-(diethoxycarbonyl) normorphinone, a novel compound, by oxidation. The novel normorphinone derivative is converted to 3-0,N-(diethoxycarbonyl) normor- phinone dienol acetate, a second novel compound, by es- terification with acetic anhydride or acetyl halide. A 14-hydroxy group is introduced into the novel dienol ester by oxidation with peroxy-acid. The resultant 3-0,N-(die- thoxycarbonyl)-14-hydroxy-normorphinone, a third novel compound, may be catalytically hydrogenated to produce 3- O,N-(diethoxycarbonyl)noroxymorphone. The latter inter- mediate may be converted to noroxymorphone by hydroly- sis. <* oo ID 0. LU This invention relates to a method for preparing 14-hydroxy-3-0,N-(diethoxycarbonyl) normorphinone from 3-0,N-(diethoxycarbonyl) normorphinone dienol acetate and to a process for preparing noroxymorphone from morphine in high yield.
    [Show full text]