DOCSLIB.ORG

View More About EXTENSO Platform.Pdf

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text
View More About EXTENSO Platform.Pdf HOW TO USE 30°C 13 min. No sample preparation. REVOLUTIONARY Just mix milk and reagents, MILK ANALYSIS PLATFORM then incubate with the EXTENSO BIOSTICK and read. 1. Mix milk and reagents 2. Incubate for 13 minutes into the Extenso Incubator DUO FROM RISK ANALYSIS TO DAILY SCREENING 3. Insert the BIOSTICK in the drawer 4. Tap to start the reading of the DEVICE RESULTS ON THE EXTENSO DEVICE EXTENSO is the all-in-one multiplex, fast, easy and automated solution the dairy industry needs to detect the widest range of contaminants in milk. All in the shortest possible time and ANALYSIS THROUGH The EXTENSO Data Manager providing a simple data-processing interface. allows you to store, track and YOUR DATA MANAGER manage your data in your PREVENT ANTIBIOTICS FROM ENDING UP IN THE FOOD CHAIN centralized environment, in the START FROM MONITORING AND... cloud or on premise. Residues of antibiotics in raw milk alters the efficiency of DETERMINE THE ANTIBIOTIC RISK PROFILE industrial processing of cheese or other fermented dairy products preparation. THEN ADOPT A SPECIFIC SCREENING PLAN Moreover, the extensive use of antibiotics is linked to the emergence of multi-resistant bacteria raising a big challenge CHOOSE YOUR CUSTOM CONFIGURATION for both animal and human health. CHANNELS BENEFITS AFLA COLI QUINO X TETRA X AZINE X ERYTHRO X SDX TYLO MULTIPLE BETA X GENTA SPIRA Detect more than 100 antibiotic residues and CAP LINCO STREPTO PRODUCT REFERENCES toxins in milk in one single test. CEFA NEO SULFA X EXTENSO ASSAY APP075 APP027 Define your own surveillance plan: check and pay only for the channels EXTENSO DEVICE EXTENSO INCUBATOR DUO corresponding to the contaminants you wish to detect in your sample. • 6 CHANNELS FLEXIBLE • 12 CHANNELS Whether for monitoring or for a release plan, • 17 CHANNELS choose any combination of contaminants to test amongst 131071 possibilities. EXTENSO IS VALIDATED AND CERTIFIED RAPID Only 13 minutes to get your results. EXTENSO helps you to take immediate action. Reseller Liège Science Park EXT 39/01-10/2018 CONNECTED Rue Louis Plescia, 8 ALTERNATIVE ANALYTICAL METHODS B-4102 Seraing (Ougrée) Remote access, multiple data export options, FOR AGRIBUSINESS BELGIUM full traceability and automated actions. http://nf-validation.afnor.org/en unisensor.be Phone +32 4 252 66 02 [email protected] MKT152-2019-11-29 SENSITIVITY TEST DETECTION EU-MRL/MRPL in ng/ml - ppb TEST DETECTION EU-MRL/MRPL in ng/ml - ppb FAMILY NAME OF FAMILY NAME OF CHANNEL ID COMPOUNDS DETECTED (ng/mL ; ppb) (codex) CHANNEL ID COMPOUNDS DETECTED (ng/mL ; ppb) (codex) THE COMPOUNDS THE COMPOUNDS [Not validated by ILVO] [US safe level] [Not validated by ILVO] [US safe level] Aflatoxin-M1 0,4 0,05 [0,5] Difloxacin 16 / AFLA MYCOTOXINS Aflatoxin-B1 [0,2-0,5] / Enofloxacin [<20] / Melamine 30 1000-2500 Lomefloxacin [<30] / MELAMINE Ammeline 600 / Flumequine 25 50 AZINE Baquiloprim 250 30 Norfloxacin 20 / PYRIMIDINE DERIVATIVES Trimethoprim 200 50 Pefloxacin [<20] / Amoxicillin 3 4 (4) Orbilfloxacin [>100] / Ampicillin 4 4 Oxolonic acid 125 / Benzylpenicillin (Pen G) 2 4 (4) Nalidixic acid 150 / Phenoxymethylpenicillin (Pen V) 4 / Sarafloxacin 16 n.f.u. Cloxacillin 12 30 Cinoxacin [<1000] / Nafcillin 350 30 Fleroxacin [<50] / BETALACTAMS - Dicloxacillin 8 30 Pipemidic acid Not detected / PENICILLINS Oxacillin 16 30 Piromidic acid Not detected / Penethamate [55] 4 Levofloxacin tbd / Piperacillin [0,5-1] / SDX SULFONAMIDES Sulfadoxine 70 100*** Ticarcillin [10-15] / Spiramycin 80 SPIRA MACROLIDES 200** (200) Aspoxicillin [1-2] / Neospiramycin 90 Sulbactam [100-1000] / Dihydrostreptomycin 150 200 (200) STREPTO AMINOGLYCOSIDES BETA Tazobactam [1000] / Streptomycin 175 200 (200) BETALACTAMASE INHIBITORS Clavunalic acid Not detected 200 Sulfadiazine 3 Cefalonium 3 20 Sulfamerazin 1 Cefazolin 9 50 Sulfadimethoxine 5 Cefoperazone 3 50 Sulfamethazine (SMTZ) 1 Cefquinome 14 20 Sulfamethoxazol 100 Ceftiofur 8 Sulfaquinoxaline 4 100** (100) BETALACTAMS - Desfuroylceftiofur 60 Sulfamonomethoxin 2 CEPHALOSPORINS Cephapirin 4 Sulfamethoxypyridazin 1 60** Desacetylcephapirin 16 Sulfaethoxypyridazin tbd Cefacetrile 9 125 Sulfazalasin [115] 100*** SULFONAMIDES Ceftizoxime 200 / SULFA Sulfapyridin 1 (25 for SMTZ) Cefuroxime 90 50 Sulfacetamide Not detected Ceftriaxone 6 / Sulfachloropyridazin 8 Chloramphenicol 0,6 n.f.u. (0,3) Sulfaguanidin 7 Chloramphenicol succinate [0,6] / Sulfathiazol 3 CAP PHENICOLS Thiamphenicol [5000] 50 Sulfisoxazol tbd Florphenicol(amine) [5000] n.f.u. Sulphatroxozole Not detected BETALACTAMS - Cefalexin 4 100 Sulfamethizole 150 CEFA CEPHALOSPORINS Cefadroxil 4 / Sulfameter 2 COLI POLYMYXINS Colistin 30 50 (50) Sulfamoxol 1 Erythromycin 30 40 DAPSONE Dapsone Not detected n.f.u. Gamithromycin Not detected n.f.u. Tetracycline (TC) 70 ERYTHRO MACROLIDES 100* (100) Oleandomycin Not detected / 4-epimer of TC Not detected Roxithromycin 700 / Chlortetracycline (CTC) 25 100* (100) Gentamicin (C1, C1a, C2, C2a) 60 100 (200) 4-epimer of CTC 1000 Kanamycin A Not detected 150 Oxytetracycline (OTC) 40 GENTA AMINOGLYCOSIDES 100* (100) Spectinomycin Not detected 200 4-epimer of OTC 1000 Sisomycin 175 / TETRA TETRACYCLINES Doxycycline 10 n.f.u. Lincomycin 80 150 (150) Mynocycline [<50] / LINCO LINCOSAMIDES Clindamycin 40 / Demeclocycline [<50] / Pirlimycin Not detected 100 (100) Sancycline [<50] / Neomycin 1000 1500 (1500) Amicycline [<50] / NEO AMINOGLYCOSIDES Paramomycin [4000-20000] n.f.u. Meclocycline [<50] / Apramycin 125 n.f.u. Methacycline [<50] / Danofloxacin 14 30 Tylosin A 30 50 (100) Enrofloxacin 14 Desmycosin 30 50 100** QUINO QUINOLONES Ciprofloxacin 16 TYLO MACROLIDES Tilmicosin Not detected 50 Marbofloxacin 14 75 Tulathromycin equivalents Not detected n.f.u. Ofloxacin [<20] / Tildipirosine Not detected n.f.u. EXTENSO LODs can be adapted to local regulations upon request | RUSSIA: Decision of the Board of the Eurasian Economic Commission dated February 13, 2018 N 28 | CHINA: Annex No. 235 of the Ministry of Agriculture and Rural Affairs of the People’s Republic of China - Maximum Residue Limits of Veterinary Drugs in Animal Foods | USA: Tolerance And/Or Target Testing Levels Of Animal Drug Residues In Milk (M-I-18-9 February 12, 2018) | tbd : to be determined / n.f.u : not for use in product for human consumption - not permissible taking into consideration the limit of the reference method / * : sum of the single compound and its epimer form / ** : sum of the single compound and its metabolites / *** : sum of all compounds of the family.
Load more

Recommended publications
  • Review Electrochemical Immunosensors for Antibiotics
    Review Electrochemical Immunosensors for Antibiotic Detection Aleksandra Pollap and Jolanta Kochana * Department of Analytical Chemistry, Faculty of Chemistry, Jagiellonian University, Gronostajowa 2, 30-387 Kraków, Poland; [email protected] * Correspondence: [email protected]; Tel.: +48-12-6862-416 Received: 27 March 2019; Accepted: 25 April 2019; Published: 1 May 2019 Abstract: Antibiotics are an important class of drugs destined for treatment of bacterial diseases. Misuses and overuses of antibiotics observed over the last decade have led to global problems of bacterial resistance against antibiotics (ABR). One of the crucial actions taken towards limiting the spread of antibiotics and controlling this dangerous phenomenon is the sensitive and accurate determination of antibiotics residues in body fluids, food products, and animals, as well as monitoring their presence in the environment. Immunosensors, a group of biosensors, can be considered an attractive tool because of their simplicity, rapid action, low-cost analysis, and especially, the unique selectivity arising from harnessing the antigen–antibody interaction that is the basis of immunosensor functioning. Herein, we present the recent achievements in the field of electrochemical immunosensors designed to determination of antibiotics. Keywords: antibiotic; immunosensor; antibody; electrochemical; immunoassay; antibacterial resistance 1. Introduction In recent years, a rapid development of analytical methods employing biosensors has been observed. A biosensor is a small analytical device that consists of a bioreceptor and a transducer. The role of a bioreceptor is the recognition of the target analyte, while a transducer converts the biological signal, produced by the bioreceptor and depending on the concentration of analyte molecules, into a measured signal, e.g., electrical, thermal, or optical [1].
    [Show full text]
  • Antibiotic Use and Abuse: a Threat to Mitochondria and Chloroplasts with Impact on Research, Health, and Environment
    Insights & Perspectives Think again Antibiotic use and abuse: A threat to mitochondria and chloroplasts with impact on research, health, and environment Xu Wang1)†, Dongryeol Ryu1)†, Riekelt H. Houtkooper2)* and Johan Auwerx1)* Recently, several studies have demonstrated that tetracyclines, the antibiotics Introduction most intensively used in livestock and that are also widely applied in biomedical research, interrupt mitochondrial proteostasis and physiology in animals Mitochondria and chloroplasts are ranging from round worms, fruit flies, and mice to human cell lines. Importantly, unique and subcellular organelles that a plant chloroplasts, like their mitochondria, are also under certain conditions have evolved from endosymbiotic - proteobacteria and cyanobacteria-like vulnerable to these and other antibiotics that are leached into our environment. prokaryotes, respectively (Fig. 1A) [1, 2]. Together these endosymbiotic organelles are not only essential for cellular and This endosymbiotic origin also makes organismal homeostasis stricto sensu, but also have an important role to play in theseorganellesvulnerabletoantibiotics. the sustainability of our ecosystem as they maintain the delicate balance Mitochondria and chloroplasts retained between autotrophs and heterotrophs, which fix and utilize energy, respec- multiple copies of their own circular DNA (mtDNA and cpDNA), a vestige of the tively. Therefore, stricter policies on antibiotic usage are absolutely required as bacterial DNA, which encodes for only a their use in research confounds experimental outcomes, and their uncontrolled few polypeptides, tRNAs and rRNAs [1, 3, applications in medicine and agriculture pose a significant threat to a balanced 4]. Furthermore, both mitochondria and ecosystem and the well-being of these endosymbionts that are essential to chloroplasts have bacterial-type ribo- sustain health.
    [Show full text]
  • STUDY GUIDE the TETRACYCLINE ANTIBIOTICS 1. Identify the Tetracyclines (Tcs) As First Or Second Generation Agents and by Duratio
    STUDY GUIDE THE TETRACYCLINE ANTIBIOTICS 1. Identify the tetracyclines (TCs) as first or second generation agents and by duration of action (short, intermediate and long). 2. Be able to identify the TC rings (A, B, C and D) and number the entire ring system. 3. Which organisms biosynthesize TCs? What are the biochemical precursors? 4. Identify the TWO acidic functionalities of the TC ring system and explain why they are acidic. Identify the basic functionality of the TCs. 5. Why are the TSs compounds zwitterionic at physiological pH? Which salts (of the base) are used and why these salts? 6. Understand the epimerization reaction; where it occurs and what is its significance. 7. Explain the tetracycline elimination reaction involving substituents in Ring C. When and why does this occur? What electronic factor drives this reaction to completion? 8. Why is the elimination reaction less likely to occur with demeclocycline than tetracycline? Why is it less likely with minocycline than demeclocycline? 9. What are the elimination products generally called? Explain why methacycline and meclocycline may also undergo an "elimination- type" reaction like those TCs with a 6-OH group? 10. Identify all of the TCs as acid unstable, intermediate acid stability and acid-stable and know why! Why is this reaction important? 11. What is an epianhydrotetracycline? How does it form and why is it's formation important? 12. How do isotetracyclines form? What is the key functional group in this reaction? Why is this reaction important? 13. What is the chelation reaction, when does it occur and why is it significant? 14.
    [Show full text]
  • WO 2007/147133 Al
    (12) INTERNATIONAL APPLICATION PUBLISHED UNDER THE PATENT COOPERATION TREATY (PCT) (19) World Intellectual Property Organization International Bureau (43) International Publication Date PCT (10) International Publication Number 21 December 2007 (21.12.2007) WO 2007/147133 Al (51) International Patent Classification: (74) Agent: SARUSSI, Steven, J.; Mcdonnel Boehnen HuI- A61K9/20 (2006.01) A61K 31/65 (2006.01) bert & Berghoff LIp, 300 South Wacker Drive, Suite 3200, A61K9/00 (2006.01) A61P 31/00 (2006.01) Chicago, IL 60606 (US). (81) Designated States (unless otherwise indicated, for every (21) International Application Number: kind of national protection available): AE, AG, AL, AM, PCT/US2007/071369 AT,AU, AZ, BA, BB, BG, BH, BR, BW, BY, BZ, CA, CH, CN, CO, CR, CU, CZ, DE, DK, DM, DO, DZ, EC, EE, EG, (22) International Filing Date: 15 June 2007 (15.06.2007) ES, FI, GB, GD, GE, GH, GM, GT, HN, HR, HU, ID, IL, IN, IS, JP, KE, KG, KM, KN, KP, KR, KZ, LA, LC, LK, (25) Filing Language: English LR, LS, LT, LU, LY, MA, MD, ME, MG, MK, MN, MW, MX, MY, MZ, NA, NG, NI, NO, NZ, OM, PG, PH, PL, (26) Publication Language: English PT, RO, RS, RU, SC, SD, SE, SG, SK, SL, SM, SV, SY, TJ, TM, TN, TR, TT, TZ, UA, UG, US, UZ, VC, VN, ZA, (30) Priority Data: ZM, ZW 60/813,925 15 June 2006 (15.06.2006) US 60/814,255 16 June 2006 (16.06.2006) US (84) Designated States (unless otherwise indicated, for every kind of regional protection available): ARIPO (BW, GH, (71) Applicant (for all designated States except US): GM, KE, LS, MW, MZ, NA, SD, SL, SZ, TZ, UG, ZM, SERENEX, INC.
    [Show full text]
  • Effect of Chloramphenicol on a Bioassay Response for the Detection of Tetracycline Residues in Milk
    36 Journal of Food and Drug Analysis, Vol. 17, No. 1, 2009, Pages 36-42 藥物食品分析 第十七卷 第一期 Effect of Chloramphenicol on a Bioassay Response for the Detection of Tetracycline Residues in Milk ORLANDO NAGEL1, MARÍA DE LA LUZ ZAPATA2, JUAN CARLOS BASÍLICO2, JORGE BERTERO1, MARÍA PILAR MOLINA3 AND RAFAEL ALTHAUS1* 1. Cátedra de Biofísica, Departamento de Ciencias Básicas, Universidad Nacional del Litoral, R.P.L. Kreder 2805, 3080 Esperanza, República Argentina. 2. Cátedra de Microbiología, Facultad de Ingeniería Química, Universidad Nacional del Litoral, Santiago del Estero 2826, 3000 Santa Fe, República Argentina. 3. Departamento de Ciencia Animal, Universidad Politécnica de Valencia, Camino de Vera, Valencia, España. (Received: Febuary 4, 2008; Accepted: October 9, 2008) ABSTRACT The tetracyclines are commonly used in veterinary medicine, and yet the residues are not always detected by microbiological inhibitor tests using Geobacillus stearothermophilus subsp. calidolactis C-953 at their Maximum Residue Limit levels. In order to improve the sensitivity of these methods, a bioassay was evaluated to study the effect produced by the incorporation of different chloramphenicol (CAP) concentrations in the culture medium. The specificity and detection limits of six tetracyclines in milk were determined. As the levels of CAP increased, a decrease in specificity, from 97.9% (for 0, 50, 200 and 400 µg/kg of CAP) to 88.0% (for 600 µg/kg of CAP) was observed. The logistic regression model indicates a significant effect of the CAP concentra- tion. However, the tetracycline-CAP interaction was not significant, and thus, a synergetic effect can not be considered between the two antimicrobials, with only a simple sum of their antimicrobial effects.
    [Show full text]
  • Using Saccharomyces Cerevisiae for the Biosynthesis of Tetracycline Antibiotics
    Using Saccharomyces cerevisiae for the Biosynthesis of Tetracycline Antibiotics Ehud Herbst Submitted in partial fulfillment of the requirements for the degree of Doctor of Philosophy in the Graduate School of Arts and Sciences COLUMBIA UNIVERSITY 2019 © 2019 Ehud Herbst All rights reserved ABSTRACT Using Saccharomyces cerevisiae for the biosynthesis of tetracycline antibiotics Ehud Herbst Developing treatments for antibiotic resistant bacterial infections is among the most urgent public health challenges worldwide. Tetracyclines are one of the most important classes of antibiotics, but like other antibiotics classes, have fallen prey to antibiotic resistance. Key small changes in the tetracycline structure can lead to major and distinct pharmaceutically essential improvements. Thus, the development of new synthetic capabilities has repeatedly been the enabling tool for powerful new tetracyclines that combatted tetracycline-resistance. Traditionally, tetracycline antibiotics were accessed through bacterial natural products or semisynthetic analogs derived from these products or their intermediates. More recently, total synthesis provided an additional route as well. Importantly however, key promising antibiotic candidates remained inaccessible through existing synthetic approaches. Heterologous biosynthesis is tackling the production of medicinally important and structurally intriguing natural products and their unnatural analogs in tractable hosts such as Saccharomyces cerevisiae. Recently, the heterologous biosynthesis of several tetracyclines was achieved in Streptomyces lividans through the expression of their respective biosynthetic pathways. In addition, the heterologous biosynthesis of fungal anhydrotetracyclines was shown in S. cerevisiae. This dissertation describes the use of Saccharomyces cerevisiae towards the biosynthesis of target tetracyclines that have promising prospects as antibiotics based on the established structure- activity relationship of tetracyclines but have been previously synthetically inaccessible.
    [Show full text]
  • DALACIN V Vaginal Cream (Clindamycin Phosphate)
    Dalacin-V/LPD/PK-06 DALACIN V Vaginal Cream (Clindamycin Phosphate) 1. NAME OF THE MEDICINAL PRODUCT DALACIN V Vaginal Cream 2. QUALITATIVE AND QUANTITATIVE COMPOSITION Clindamycin phosphate is a water-soluble ester of the semisynthetic antibiotic produced by a 7(S)-chloro-substitution of the 7(R)-hydroxyl group of the parent antibiotic lincomycin. Clindamycin vaginal cream 2%, is a semi-solid, white cream, which contains 2% clindamycin phosphate, USP, at a concentration equivalent to 20 mg clindamycin per gram. Each applicatorful of 5 grams of vaginal cream contains approximately 100 mg of clindamycin phosphate. 3. PHARMACEUTICAL FORM Vaginal cream. 4. CLINICAL PARTICULARS 4.1. THERAPEUTIC INDICATIONS DALACIN V Vaginal Cream 2%1-9 is indicated in the treatment of bacterial vaginosis (formerly referred to as Haemophilus vaginitis, Gardnerella vaginitis, non-specific vaginitis, Corynebacterium vaginitis, or anaerobic vaginosis). DALACIN V Vaginal Cream can be used to treat non-pregnant women and pregnant women during their second and third trimesters.13,14 4.2. POSOLOGY AND METHOD OF ADMINISTRATION DALACIN V Vaginal Cream: The recommended dose is one applicatorful of clindamycin vaginal cream 2% intravaginally, preferably at bedtime, for three or seven consecutive days.3-9 4.3. CONTRAINDICATIONS Clindamycin vaginal cream is contraindicated in patients with a history of hypersensitivity to clindamycin, lincomycin or any of the components of these products. Clindamycin vaginal cream25 is also contraindicated in individuals with a history of antibiotic-associated colitis.34,35 4.4. SPECIAL WARNINGS AND PRECAUTIONS FOR USE The use of clindamycin vaginal products3-12 may result in the overgrowth of non-susceptible organisms, particularly yeasts.
    [Show full text]
  • Stembook 2018.Pdf
    The use of stems in the selection of International Nonproprietary Names (INN) for pharmaceutical substances FORMER DOCUMENT NUMBER: WHO/PHARM S/NOM 15 WHO/EMP/RHT/TSN/2018.1 © World Health Organization 2018 Some rights reserved. This work is available under the Creative Commons Attribution-NonCommercial-ShareAlike 3.0 IGO licence (CC BY-NC-SA 3.0 IGO; https://creativecommons.org/licenses/by-nc-sa/3.0/igo). Under the terms of this licence, you may copy, redistribute and adapt the work for non-commercial purposes, provided the work is appropriately cited, as indicated below. In any use of this work, there should be no suggestion that WHO endorses any specific organization, products or services. The use of the WHO logo is not permitted. If you adapt the work, then you must license your work under the same or equivalent Creative Commons licence. If you create a translation of this work, you should add the following disclaimer along with the suggested citation: “This translation was not created by the World Health Organization (WHO). WHO is not responsible for the content or accuracy of this translation. The original English edition shall be the binding and authentic edition”. Any mediation relating to disputes arising under the licence shall be conducted in accordance with the mediation rules of the World Intellectual Property Organization. Suggested citation. The use of stems in the selection of International Nonproprietary Names (INN) for pharmaceutical substances. Geneva: World Health Organization; 2018 (WHO/EMP/RHT/TSN/2018.1). Licence: CC BY-NC-SA 3.0 IGO. Cataloguing-in-Publication (CIP) data.
    [Show full text]
  • Advance Data from Vital and Health Statistics; No
    From VKal and Health Statwtics of the National Center for Health Statrs.tics Number 106 . April 10, 1985 Use of Topical Antimicrobial Drugs in Office-Based Practice: United States, 1980-81 by Gloria J. Gardocki, Ph. D., Division of Health Care Statistics This report examines the use of topical antimicrobial 1980 and 1981 then were screened for these ingredients. The , medications in the office-based patient care setting. The infor­ resulting list of antimicrobial drugs was divided into two sets: mation used was obtained by combining the 1980 and 1981 those known to be used only topically and all others. The topical results of the National Ambulato~ Medical Care Survey, a drugs, and the patient visits associated with them, are discussed sample survey of care provided by office-based physicians. in this repofi, the other antimicrobial drugs will be presented in Conducted annually by the National Center for Health Sta­ an additional report scheduled for publication in 1985. istics from 1973 through 1981, the survey is being carried out Thirty-six specific antimicrobial generic ingredients ap again in 1985. peared in the topical drug mentions recorded in the 1980 and m Because of the nature of the data collected by means of the 1981 surveys. For the purposes of this analysis, they can be National Ambulatory Medical Care Survey (NAMCS), the classified in the following eight categories: investigation of the use of antimicrobial medications is limited to an inspection of the patterns in physicians’ ordering or pro­ Amphenicols (chlorarnphenicol). viding them to patients. It is not possible to assess the extent to Macrolide antibiotics (erythromycin).
    [Show full text]
  • 761 Part 446—Tetracycline Antibiotic Drugs
    Food and Drug Administration, HHS Pt. 446 (c) The batch for neomycin content, PART 446ÐTETRACYCLINE polymyxin B content, pH, and sterility. ANTIBIOTIC DRUGS (ii) Samples required: (a) The neomycin sulfate used in Subpart AÐBulk Drugs making the batch: Ten packages, each containing approximately 300 milli- Sec. grams. 446.10 Chlortetracycline hydrochloride. (b) The polymyxin B sulfate used in 446.10a Sterile chlortetracycline hydro- making the batch: Ten packages, each chloride. 446.15 Demeclocycline. containing approximately 300 milli- 446.16 Demeclocycline hydrochloride. grams 446.20 Doxycycline hyclate. (c) The batch: 446.20a Sterile doxycycline hyclate. (1) For all tests except sterility: A 446.21 Doxycycline monohydrate. minimum of six immediate containers. 446.42 Meclocycline sulfosalicylate. (2) For sterility testing: Twenty im- 446.50 Methacycline hydrochloride. mediate containers, collected at regu- 446.60 Minocycline hydrochloride. lar intervals throughout each filling 446.65 Oxytetracycline. operation. 446.65a Sterile oxytetracycline. 446.66 Oxytetracycline calcium. (b) Tests and methods of assayÐ(1) Po- 446.67 Oxytetracycline hydrochloride. tencyÐ(i) Neomycin content. Proceed as 446.67a Sterile oxytetracycline hydro- directed in § 444.42a(b)(1), except pre- chloride. pare the sample as follows: Remove an 446.75a Sterile rolitetracycline. accurately measured portion and dilute 446.76a Sterile rolitetracycline nitrate. with 0.1M potassium phosphate buffer, 446.80 Tetracycline. pH 8.0, to the proper prescribed ref- 446.81 Tetracycline hydrochloride. erence concentration. The neomycin 446.81a Sterile tetracycline hydrochloride. 446.82 Tetracycline phosphate complex. content is satisfactory if it is not less than 90 percent nor more than 130 per- Subpart BÐOral Dosage Forms cent of the number of milligrams of ne- omycin that it is represented to con- 446.110 Chlortetracycline hydrochloride cap- tain.
    [Show full text]
  • Classification of Anti‐Bacterial Agents and Their Functions
    Chapter 1 Classification of Anti‐Bacterial Agents and Their Functions Hamid Ullah and Saqib Ali Additional information is available at the end of the chapter http://dx.doi.org/10.5772/intechopen.68695 Abstract Bacteria that cause bacterial infections and disease are called pathogenic bacteria. They cause diseases and infections when they get into the body and begin to reproduce and crowd out healthy bacteria or to grow into tissues that are normally sterile. To cure infec‐ tious diseases, researchers discovered antibacterial agents, which are considered to be the most promising chemotherapeutic agents. Keeping in mind the resistance phenomenon developing against antibacterial agents, new drugs are frequently entering into the mar‐ ket along with the existing drugs. In this chapter, we discussed a revised classification and function of the antibacterial agent based on a literature survey. The antibacterial agents can be classified into five major groups, i.e. type of action, source, spectrum of activity, chemical structure, and function. Keywords: anti‐bacterial agents, classification, functions 1. Introduction Bacteria are simple one‐celled organism, which were first identified in the 1670s by van Leeuwenhoek. Latter in the nineteenth century, concepts have been developed that there is the strongest correlation between bacteria and diseases. Such considerations attracted interest of the researchers not only to answer some mysterious questions about infectious diseases, but also to find a substance that could kill, inhibit, or at least slow down the growth of such disease‐causing bacteria. These efforts led to the revolutionary discovery of the antibacterial agent “penicillin” in 1928 fromPenicillium notatum by Sir Alexander Fleming.
    [Show full text]
  • PF 44(2) Table of Contents Publish Date: April 30, 2018
    PF 44(2) Table of Contents Publish date: April 30, 2018 PROPOSED IRA: Proposed Interim Revision Announcements USP MONOGRAPHS IN-PROCESS REVISION: In-Process Revision GENERAL CHAPTERS <2> ORAL DRUG PRODUCTS-PRODUCT QUALITY TESTS (USP42-NF37 1S) <41> BALANCES (USP42-NF37 1S) <701> DISINTEGRATION (USP42-NF37 1S) <729> GLOBULE SIZE DISTRIBUTION IN LIPID INJECTABLE EMULSIONS (USP42-NF37 1S) REAGENTS, INDICATORS, AND SOLUTIONS Reagent Specifications Octylamine [NEW] (USP42-NF37 1S) Poly(dimethylsiloxane-co-methylphenylsiloxane) [NEW] (USP42-NF37 1S) Silica Gel, Precoated Plates, with Fluorescence Indicator F254 [NEW] (USP42-NF37 1S) Sodium 1-Heptanesulfonate Monohydrate (USP42-NF37 1S) Tryptamine Hydrochloride [NEW] (USP42-NF37 1S) Test Solutions 1 M Phosphoric Acid TS [NEW] (USP42-NF37 1S) Volumetric Solutions 0.1 N Potassium Arsenite VS (USP42-NF37 1S) 0.1 N Sodium Hydroxide VS (USP42-NF37 1S) Chromatographic Columns G50 [NEW] (USP42-NF37 1S) L87 (USP42-NF37 1S) L117 [NEW] (USP42-NF37 1S) REFERENCE TABLES Container Specifications Container Specifications [NEW] (USP42-NF37) Description and Solubility PF 43(4) Table of Contents 1 | P a g e Description and Relative Solubility of USP and NF Articles (USP42-NF37 1S) Description and Solubility - A Description and Solubility - C Description and Solubility - F Description and Solubility - N Description and Solubility - S USP MONOGRAPHS Allopurinol Compounded Oral Suspension (USP42-NF37 1S) Aminoglutethimide (USP42-NF37 1S) Aminoglutethimide Tablets (USP42-NF37 1S) Aminosalicylate Sodium (USP42-NF37
    [Show full text]