DOCSLIB.ORG

Page Numbers in Bold Type Relate to Monograph Titles Index A771

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text
Page Numbers in Bold Type Relate to Monograph Titles Index A771 page numbers in bold type relate to monograph titles Index A771 Index Page numbers in bold type relate to monograph titles. Pages – Vol I: i – xxviii, (Preliminaries and Introduction) 1 – 1126, (General Notices and Monographs) Pages – Vol II: xxix – xxxvi, (Preliminaries) 1127 – 2184, (General Notices and Monographs) Pages – Vol III: xxxvii – xliv, (Preliminaries) 2185 – 3612, (General Notices and Monographs) Pages – Vol IV: xlv – lii, (Preliminaries) 3613 – 3644, (General Notices) S1 – S132, (Spectra) A1 – A770, (Appendices; Supplementary Chapters) page numbers in bold type relate to monograph titles Index A773 Acetate Buffer Solution pH 6.0, see Aciclovir Eye Ointment, 2268 A Acetate Buffer pH 6.0 Aciclovir Intravenous Infusion, 2269 Abbreviated, A520 Acetate Buffer Solution pH 4.5, A139 Aciclovir Oral Suspension, 2270 Adjectives, A520 Acetate Buffer Solution pH 4.7, A139 Aciclovir Sodium for Intravenous Anions, A520 Acetate Buffer Solution pH 5.0, A139 Infusion, 2269 Cations, A520 Acetate–Edetate Buffer Solution pH 5.5, Aciclovir Tablets, 2270 Preparations, A520 A139 Aciclovir Tablets, Dispersible, 2271 Titles of Monographs, A520 Acetates, Reactions of, A232 Acicular, A453 Abbreviated Titles, Status of, 7, 1133, Acetazolamide, 50,S5 Acid Blue 92, A19 2191, 3619 Acetazolamide Tablets, 2266 Acid Blue 92 Solution, A19 Abnormal Toxicity, Test for, A347 Acetic Acid, A17 Acid Blue 83, A19 About, definition of, 5, 1131, 2189, Acetic Acid (6 per cent), 51 Acid Blue 93 Solution, A19 3617 Acetic Acid (33 per cent), 52 Acid Blue 90, A19 Absence of Aristolochic Acids I and II in Acetic Acid, Anhydrous, A18 Acid Gentian Mixture, 2624 Herbal Drugs, A287 Acetic Acid, Deuterated, A46 Acid Gentian Oral Solution, 2624 Absolute Alcohol, see Ethanol Acetic Acid, Dilute, A18 Acid Potassium Iodobismuthate Absolute Ethanol, A56 Acetic Acid, Dilute, see Acetic Acid Solution, A100 Absolute Ethanol R1, A56 (6 per cent) Acid Value, A268 Absolute viscometers, A221-222 Acetic Acid, Glacial, 51, A18 Acid/base Indicators, A766 Absorbable Braided Sutures, Sterile Acetic Acid in Synthetic Peptides, Acid-base titrations, A765 Synthetic, 3311 Determination of, A260 Acidified Chloroform, A38 Absorbable Monofilament Sutures, Acetic Acid VS, A129 Acidified Dichloromethane, A48 Sterile Synthetic, 3312 Acetic Acid, see Acetic Acid (33 per cent) Acidified Methanol, A78 Absorbance, Control of, A539 Acetic Anhydride, A18 Acidified Methylene Chloride, see Absorbance, Determination of, A538 Acetic Anhydride Solution R1, A18 Acidified Dichloromethane Absorbent Cotton, 3307 Acetic Anhydride–Dioxan Solution, A18 Acid-insoluble Ash, Determination of, Absorbent Viscose Wadding, 3308 Acetic Anhydride–Sulphuric Acid A284 Absorption spectrophotometry, infrared, Solution, A18 Acid-washed Diatomaceous Support, A147 Acetic Bromine Solution, A32 A47 Absorption Spectrophotometry, Acetone, 52, A18 Acitretin, 63 Ultraviolet and Visible, A153 Acetone, Deuterated, A46 Acknowledgements, xxiii Acacia, 37, A17 Acetone Solution, Buffered, A139 Acriflavinium Chloride, xxvi Acacia Solution, A17 Acetone-dried Ox Brain, A90 Acrylamide, A19 Acacia, Spray-dried, 38 Acetonitrile, A18 Acrylamide/bisacrylamide (29:1) Acamprosate Calcium, 39 Acetonitrile for Chromatography, A18 Solution, 30 per cent, A19 Acarbose, 40 Acetonitrile R1, A18 Acrylamide/bisacrylamide (36.5:1) Acarbose, Chromatogram, A645 Acetoxyvalerenic Acid, A18 Solution, 30 per cent, A19 Accuracy, A587 Acetyl Chloride, A18 Acrylic Acid, A19 Acebutolol Capsules, 2265 Acetyl groups (O-Acetyl) in Acteoside, A19 Acebutolol Hydrochloride, 42, S4, A17 Polysaccharide Vaccines, A391 Action and Use Statement, Status of, 16, Acebutolol Tablets, 2265 Acetyl Groups, Reactions of, A232 1142, 2200, 3628 Aceclofenac, 44 Acetyl Value, Determination of, A268- Activated Acid Aluminium Oxide, A21 Acemetacin, 46 280 Activated Attapulgite, 192 Acenocoumarol, 48,S5 Acetylacetamide, A18 Activated Charcoal, 437, A37 Acenocoumarol Tablets, 2266 Acetylacetone, A18 Activated coagulation factors, A358 Acesulfame Potassium, 48 Acetylacetone Reagent R1, A18 Activated protein C chromogenic Acetal, A17 4-Acetylbiphenyl, A18 substrate, A363 Acetaldehyde, A17 N-Acetyl-e-caprolactam, A18 Activated Zinc, A128 Acetaldehyde Ammonia Trimer Acetylcholine Chloride, 53, A18 Active Moiety, A564 Trihydrate, A17 Acetylcysteine, 55,S6 Active Substances, 35, 1161, see also Acetaldehyde Standard Solution Acetylcysteine Injection, 2267 Substances for Pharmaceutical Use (100 ppm C2H4O), A135 Acetyldigoxin, 56 Additions, List of, xxiii Acetaldehyde Standard Solution b-Acetyldigoxin, Chromatogram, A646 Additions, List of Monographs, xix (100 ppm C2H4O) R1, A135 b-Acetyldigoxin, see Acetyldigoxin Additives, Plastic, A514 Acetamide, A17 Acetyleugenol, A18 Adenine, 64 Acetaminophen, see Paracetamol N-Acetylglucosamine, A18 Adenosine, 65, A19 Acetate Buffer pH 2.8, A139 Acetyl-11-keto-b-boswellic Acid, A18 Adenovirus Vectors for Human Use, Acetate Buffer pH 2.45, A139 N-Acetyl-L-cysteine, A18 A750 Acetate Buffer pH 3.4, A139 N-Acetylneuraminic Acid, A19 Adipic Acid, 67, A19 Acetate Buffer pH 3.5, A139 Acetylsalicylic Acid Tablets, see Aspirin Adjustment of chromatographic Acetate Buffer pH 3.7, A139 Tablets conditions, A172 Acetate Buffer pH 4.4, A139 Acetylsalicylic Acid, see Aspirin Adrenaline, 68, A19 Acetate Buffer pH 4.6, A139 N-Acetyltryptophan, 58, A19 Adrenaline Acid Tartrate, 70, A19 Acetate Buffer pH 5.0, A139 N-Acetyltryptophan, see Acetyltryptophan Adrenaline and Cocaine Intranasal Acetate Buffer pH 6.0, A139 Acetyltyrosine, 60 Solution, 2274 Acetate Buffer Solution pH 4.4, see Acetyltyrosine Ethyl Ester, A19 Adrenaline (Epinephrine), S6 Acetate Buffer pH 4.4 Acetyltyrosine Ethyl Ester, 0.2M, A19 Adrenaline Eye Drops, Acetate buffer solution pH 4.6, see N-Acetyltyrosine, see Acetyltyrosine Neutral/Epinephrine Eye Drops, Acetate Buffer pH 4.6 Aciclovir, 61 Neutral, 2271 Aciclovir Cream, 2268 A774 Index Adrenaline Eye Drops/Epinephrine Eye Aescin, A19 Aldehyde-free alcohol, see Ethanol (96%), Drops, 2271 Aflatoxin B1 in Herbal Drugs, Aldehyde-free Adrenaline Injection, Bupivacaine and, Determination of, A288 Aldehyde-free Ethanol (96%), A57 2352 Aflatoxin B1, A20 Aldehyde-free Methanol, A78 Adrenaline Injection, Dilute (1 in Agar, 71, A19 Aldehydes, Determination of, A272 10,000), 2273 Agarose for Chromatography, A20 Aldrin, A20 Adrenaline Injection, Lidocaine and, Agarose for Chromatography, Cross- Aleuritic Acid, A20 2725 linked, A20 Alexandrian Senna Fruit, 3552 Adrenaline Injection/Epinephrine Agarose for Chromatography R1, Cross- Alexandrian Senna Pods, see Alexandrian Injection, 2272 linked, A20 Senna Fruit Adrenaline Solution/Epinephrine Agarose for Electrophoresis, A20 Alfacalcidol, 79 Solution, 2274 Agarose/Cross-linked Polyacrylamide, Alfadex, 81 Adrenaline Tartrate A20 Alfentanil Hydrochloride, 82 Injection/Epinephrine Tartrate Agarose-DEAE for Ion Exchange Alfuzosin Hydrochloride, 84 Injection, 2272 Chromatography, A20 Alginate Antacid Oral Suspension, Adrenaline Tartrate Agglomerate, A453 Compound, 2276 Solution/Epinephrine Tartrate Aggregate, A453 Alginate Oral Suspension, Raft-forming, Solution, 2274 Agnus Castus Fruit, 3326 2277 Adrenaline Tartrate, see Adrenaline Acid Agrimony, 3327 Alginate Raft-forming Oral Suspension, Tartrate Air, Medical, 72 2277 Adrenalone Hydrochloride, A19 Air Permeability, Specific Surface Area Alginic Acid, 85 Adsorbed Diphtheria and Tetanus by, A435 Alimemazine, S7 Vaccine for Adults and Adolescents, Air, Synthetic, 75 Alimemazine Oral Solution, Paediatric, see Diphtheria and Tetanus Vaccine Air, Synthetic Medicinal, see Synthetic Air 2277 (Adsorbed, Reduced Antigen(s) Content) Airtight Container, A472 Alimemazine Tablets, 2278 Adsorbed Diphtheria and Tetanus Airtight container, Definition of, 26, Alimemazine Tartrate, 86 Vaccine, see Diptheria and Tetanus 1152, 2210, 3638 Alizarin S, A20 Vaccine, Adsorbed Alanine, 76, A20 Alizarin S Solution, A20 Adsorbed Diphtheria, Tetanus and ß-Alanine, see 3-Aminopropionic Acid Alkaline Corallin Solution, A43 Pertussis (Acellular Component) Albendazole, 77 Alkaline Eye Drops, see Hypromellose Eye Vaccine, see Diphtheria, Tetanus and Albumin, Bovine, A20 Drops Pertussis (Acellular Component) Vaccine, Albumin, Human, A20 Alkaline Gentian Mixture, 2624 Adsorbed Albumin Injection, Iodinated [125I], 3242 Alkaline Gentian Oral Solution, 2624 Adsorbed Diphtheria, Tetanus and Albumin Solution, 3067 Alkaline Hydroxylamine Solution, A68 Pertussis Vaccine, 3127 Albumin Solution, Human, A20 Alkaline Hydroxylamine Solution R1, Adsorbed Diphtheria, Tetanus, Pertussis Albumin Solution R1, Human, A20 A68 (Acellular Component) and Albumin, see Albumin Solution Alkaline Impurities, Fixed Oils, A273 Haemophilus Type b Conjugate Alchemilla, 3328 Alkaline Potassium Mercuri-iodide Vaccine, see Diphtheria, Tetanus, Alcohol (20 per cent), 797 Solution, A100 Pertussis (Acellular Component) and Alcohol (25 per cent), 797 Alkaline Potassium Tetraiodomercurate Haemophilus Type b Conjugate Vaccine, Alcohol (45 per cent), 797 Solution, A101 Adsorbed Alcohol (50 per cent), 797 Alkaline Pyrogallol Solution, A102 Adsorbed Diphtheria, Tetanus, Pertussis Alcohol (60 per cent), 797 Alkaline Sodium Picrate Solution, A113 (Acellular Component) and Hepatitis Alcohol (70 per cent), 797 Alkaline Tetrazolium Blue Solution, B (rDNA) Vaccine, see Diphtheria, Alcohol (80 per cent), 797 A120 Tetanus, Pertussis (Acellular Component) Alcohol (90 per cent), 797 Alkali-washed Diatomaceous Support, and Hepatitis B (rDNA) Vaccine, Alcohol, Aldehyde-free,
Load more

Recommended publications
  • (12) Patent Application Publication (10) Pub. No.: US 2011/0263526 A1 SATYAM (43) Pub
    US 20110263526A1 (19) United States (12) Patent Application Publication (10) Pub. No.: US 2011/0263526 A1 SATYAM (43) Pub. Date: Oct. 27, 2011 (54) NITRICOXIDE RELEASING PRODRUGS OF CD7C 69/96 (2006.01) THERAPEUTICAGENTS C07C 319/22 (2006.01) CD7C 68/02 (2006.01) (75) Inventor: Apparao SATYAM, Mumbai (IN) A6IP 29/00 (2006.01) A6IP 9/00 (2006.01) (73) Assignee: PIRAMAL LIFE SCIENCES A6IP37/08 (2006.01) LIMITED, Mumbai (IN) A6IP35/00 (2006.01) A6IP 25/24 2006.O1 (21) Appl. No.: 13/092.245 A6IP 25/08 308: A6IP3L/04 2006.O1 (22) Filed: Apr. 22, 2011 A6IP3L/2 308: Related U.S. Application Data 39t. O 308: (60) Provisional application No. 61/327,175, filed on Apr. A6IP3/10 (2006.01) 23, 2010. A6IPL/04 (2006.01) A6IP39/06 (2006.01) Publication Classification A6IP3/02 (2006.01) (51) Int. Cl. A6IP 9/06 (2006.01) A 6LX 3L/7072 (2006.01) 39t. W 308: A6 IK3I/58 (2006.01) A6IP II/08 (2006.015 A6 IK3I/55 (2006.01) A63/62 (2006.015 A6 IK 3/495 (2006.01) A6 IK 3/4439 (2006.01) (52) U.S. Cl. ........... 514/50: 514/166; 514/172: 514/217; A6 IK 3L/455 (2006.01) 514/255.04: 514/338; 514/356; 514/412; A6 IK 3/403 (2006.01) 514/420; 514/423: 514/510,536/28.53:540/67; A6 IK 3/404 (2006.01) 540/591; 544/396; 546/273.7: 546/318: 548/452: A6 IK 3/40 (2006.01) 548/500: 548/537; 549/464; 558/275 A6 IK3I/265 (2006.01) C7H 9/06 (2006.01) (57) ABSTRACT CO7I 71/00 (2006.01) CO7D 22.3/26 (2006.01) The present invention relates to nitric oxide releasing pro C07D 295/14 (2006.01) drugs of known drugs or therapeutic agents which are repre CO7D 40/12 (2006.01) sented herein as compounds of formula (I) wherein the drugs CO7D 213/80 (2006.01) or therapeutic agents contain one or more functional groups C07D 209/52 (2006.01) independently selected from a carboxylic acid, an amino, a CO7D 209/26 (2006.01) hydroxyl and a sulfhydryl group.
    [Show full text]
  • F1y3x CHAPTER 29 ORGANIC CHEMICALS VI 29-1 Notes 1
    )&f1y3X CHAPTER 29 ORGANIC CHEMICALS VI 29-1 Notes 1. Except where the context otherwise requires, the headings of this chapter apply only to: (a) Separate chemically defined organic compounds, whether or not containing impurities; (b) Mixtures of two or more isomers of the same organic compound (whether or not containing impurities), except mixtures of acyclic hydrocarbon isomers (other than stereoisomers), whether or not saturated (chapter 27); (c) The products of headings 2936 to 2939 or the sugar ethers and sugar esters, and their salts, of heading 2940, or the products of heading 2941, whether or not chemically defined; (d) Products mentioned in (a), (b) or (c) above dissolved in water; (e) Products mentioned in (a), (b) or (c) above dissolved in other solvents provided that the solution constitutes a normal and necessary method of putting up these products adopted solely for reasons of safety or for transport and that the solvent does not render the product particularly suitable for specific use rather than for general use; (f) The products mentioned in (a), (b), (c), (d) or (e) above with an added stabilizer necessary for their preservation or transport; (g) The products mentioned in (a), (b), (c), (d), (e) or (f) above with an added antidusting agent or a coloring or odoriferous substance added to facilitate their identification or for safety reasons, provided that the additions do not render the product particularly suitable for specific use rather than for general use; (h) The following products, diluted to standard strengths, for the production of azo dyes: diazonium salts, couplers used for these salts and diazotizable amines and their salts.
    [Show full text]
  • Page Numbers in Bold Type Relate to Monograph Titles Index V-A797
    page numbers in bold type relate to monograph titles Index V-A797 Index Page numbers in bold type relate to monograph titles. Pages – Vol I: i – xxxii, (Preliminaries and Introduction) 1 – 1280, (General Notices and Monographs) Pages – Vol II: i – viii, (Preliminaries) 1 – 1220, (General Notices and Monographs) Pages – Vol III: i – viii, (Preliminaries) 1 – 1238, (General Notices and Monographs) Pages – Vol IV: i – viii, (Preliminaries) 1 – 754, (General Notices and Monographs) Pages – Vol V: i – viii, (Preliminaries) 1 – 34, (General Notices) S1 – S144, (Spectra) A1 – A796, (Appendices; Supplementary Chapters) page numbers in bold type relate to monograph titles Index V-A799 Acetate Buffer Solution pH 6.0, see N-Acetyltryptophan see Acetyltryptophan A Acetate Buffer pH 6.0 Acetyltryptophan, I-63 Abacavir, V-S4 Acetate Buffer Solution pH 4.4, V-A152 Acetyltyrosine, I-65 Abacavir Oral Solution, III-85 Acetate Buffer Solution pH 4.5, V-A152 N-Acetyltyrosine see Acetyltyrosine Abacavir Sulfate, I-39 Acetate Buffer Solution pH 4.7, V-A152 Acetyltyrosine Ethyl Ester, V-A21 Abacavir Tablets, III-86 Acetate Buffer Solution pH 5.0, V-A153 Acetyltyrosine Ethyl Ester, 0.2M, V-A21 Abbreviated, V-598 Acetate Buffer Solution pH 6.0, V-A153 Aciclovir, I-67 Adjectives, V-598 Acetate–edetate Buffer Solution pH 5.5, Aciclovir Cream, III-93 Anions, V-598 V-A153 Aciclovir Eye Ointment, III-94 Cations, V-598 Acetates, Reactions of, V-266 Aciclovir Infusion, III-95 Preparations, V-598 Acetazolamide, I-54, V-S5 Aciclovir Intravenous Infusion, see Titles of
    [Show full text]
  • (12) Patent Application Publication (10) Pub. No.: US 2011/0159073 A1 De Juan Et Al
    US 20110159073A1 (19) United States (12) Patent Application Publication (10) Pub. No.: US 2011/0159073 A1 de Juan et al. (43) Pub. Date: Jun. 30, 2011 (54) METHODS AND DEVICES FOR THE Publication Classification TREATMENT OF OCULAR CONDITIONS (51) Int. Cl. (76) Inventors: Eugene de Juan, LaCanada, CA A6F 2/00 (2006.01) (US); Signe E. Varner, Los (52) U.S. Cl. ........................................................ 424/427 Angeles, CA (US); Laurie R. Lawin, New Brighton, MN (US) (57) ABSTRACT Featured is a method for instilling one or more bioactive (21) Appl. No.: 12/981,038 agents into ocular tissue within an eye of a patient for the treatment of an ocular condition, the method comprising con (22) Filed: Dec. 29, 2010 currently using at least two of the following bioactive agent delivery methods (A)-(C): (A) implanting a Sustained release Related U.S. Application Data delivery device comprising one or more bioactive agents in a (63) Continuation of application No. 1 1/175,850, filed on posterior region of the eye so that it delivers the one or more Jul. 5, 2005, now abandoned. bioactive agents into the vitreous humor of the eye; (B) instill ing (e.g., injecting or implanting) one or more bioactive (60) Provisional application No. 60/585,236, filed on Jul. 2, agents Subretinally; and (C) instilling (e.g., injecting or deliv 2004, provisional application No. 60/669,701, filed on ering by ocular iontophoresis) one or more bioactive agents Apr. 8, 2005. into the vitreous humor of the eye. Patent Application Publication Jun. 30, 2011 Sheet 1 of 22 US 2011/O159073 A1 Patent Application Publication Jun.
    [Show full text]
  • (12) United States Patent (10) Patent No.: US 8,623,419 B2 Malakhov Et Al
    USOO8623419B2 (12) United States Patent (10) Patent No.: US 8,623,419 B2 Malakhov et al. (45) Date of Patent: Jan. 7, 2014 (54) TECHNOLOGY FOR PREPARATION OF WO 2004/047735 6, 2004 MACROMOLECULAR MICROSPHERES WO WO2005/035088 4/2005 WO 2006/031291 3, 2006 (75) Inventors: Michael P. Malakhov, San Francisco, CA (US); Fang Fang, Rancho Santa Fe, OTHER PUBLICATIONS CA (US) US 5,849,884, 11/09/99, Woiszwillo et al (withdrawn). Agrawal et al., “Basis of rise in intracellular sodium in airway hyper (73) Assignee: Ansun Biopharma, Inc., San Diego, CA responsiveness and asthma.” Lung, 183:375-387. (2005). (US) Alcock, R., et al., “Modifying the release of leuprolide from spray dried OED microparticles,” Journal of Control Release, 82(2-3):429 (*) Notice: Subject to any disclaimer, the term of this 440, (2002). patent is extended or adjusted under 35 Barbey-Morel, C.L., et al., “Role of respiratory tract proteases in U.S.C. 154(b) by 0 days. infectivity of influenza A virus,” Journal of Infectious Diseases, 155:667-672, (1987). (21) Appl. No.: 13/289,644 Bot A.I. et al., “Novel lipid-based hollow-porous microparticles as a platform for immunoglobulin delivery to the respiratory tract.” Phar (22) Filed: Nov. 4, 2011 maceutical Research, 17(3):275-283, (2000). (65) Prior Publication Data Cryan S.A., "Carrier-based strategies for targeting protein and peptide drugs to the lungs.” American Association of Pharmaceutical US 2012/O116062 A1 May 10, 2012 Scientists PharmSci AAPS electronic resource), 7(1): E20-E41, (2005). Edwards D.A. et al., "Large porous particles for pulmonary drug Related U.S.
    [Show full text]
  • Pharmacology Cito
    Pharmacology Cito 5 Read: it is important! Dear future physicians and pharmaceutists! The scientific and pedagogical staff of the Pharmacology department of the National University of Pharmacy (Kharkiv) presents a new textbook "Pharmacology – Cito!" to you. We want to change the myth that it is impossible to learn pharmacology quickly and qualitatively. The textbook "Pharmacology – Cito!" is published for those, who have decided to connect his or her profession with medicines, but think that a great amount of the information in pharmacology is hard to learn. Taking this fact into account we have decided to help those, who wish to master pharmacology in logical, fast - "Cito!"- version. Not be afraid of pharmacology! The 40-year experience of teaching pharmacology testifies that for the last 10-15 years a tendency of reducing the amount of classroom hours in pharmacology because of increasing the amount of the individual work is being observed. However, because of the lack of time and the constant increasing volume of information in pharmacology, everyone has not enough time to master it soundly and qualitatively. This textbook trains future pharmaceutists and physicians in the pharmacological logic, i.e. knowing the mechanisms of drug action one can understand their pharmacodynamics, naturally, on the basis of pharmacodynamics one can find logically the indications to their application and from their side effects the contraindications can be seen. The information about the peculiarities of medicines has been generalized and given as a pharmacological ―face‖ in tables. The volume of this textbook in pharmacology is sufficient for acquiring the confidence in the opportunity of the further improving of knowledge in this discipline, which is important for a physician and a pharmaceutist.
    [Show full text]
  • Pharmacology
    STATE ESTABLISHMENT «DNIPROPETROVSK MEDICAL ACADEMY OF HEALTH MINISTRY OF UKRAINE» V.I. MAMCHUR, V.I. OPRYSHKO, А.А. NEFEDOV, A.E. LIEVYKH, E.V.KHOMIAK PHARMACOLOGY WORKBOOK FOR PRACTICAL CLASSES FOR FOREIGN STUDENTS STOMATOLOGY DEPARTMENT DNEPROPETROVSK - 2016 2 UDC: 378.180.6:61:615(075.5) Pharmacology. Workbook for practical classes for foreign stomatology students / V.Y. Mamchur, V.I. Opryshko, A.A. Nefedov. - Dnepropetrovsk, 2016. – 186 p. Reviewed by: N.I. Voloshchuk - MD, Professor of Pharmacology "Vinnitsa N.I. Pirogov National Medical University.‖ L.V. Savchenkova – Doctor of Medicine, Professor, Head of the Department of Clinical Pharmacology, State Establishment ―Lugansk state medical university‖ E.A. Podpletnyaya – Doctor of Pharmacy, Professor, Head of the Department of General and Clinical Pharmacy, State Establishment ―Dnipropetrovsk medical academy of Health Ministry of Ukraine‖ Approved and recommended for publication by the CMC of State Establishment ―Dnipropetrovsk medical academy of Health Ministry of Ukraine‖ (protocol №3 from 25.12.2012). The educational tutorial contains materials for practical classes and final module control on Pharmacology. The tutorial was prepared to improve self-learning of Pharmacology and optimization of practical classes. It contains questions for self-study for practical classes and final module control, prescription tasks, pharmacological terms that students must know in a particular topic, medical forms of main drugs, multiple choice questions (tests) for self- control, basic and additional references. This tutorial is also a student workbook that provides the entire scope of student’s work during Pharmacology course according to the credit-modular system. The tutorial was drawn up in accordance with the working program on Pharmacology approved by CMC of SE ―Dnipropetrovsk medical academy of Health Ministry of Ukraine‖ on the basis of the standard program on Pharmacology for stomatology students of III - IV levels of accreditation in the specialties Stomatology – 7.110105, Kiev 2011.
    [Show full text]
  • Annex 8 Proposal to Waive in Vivo Bioequivalence Requirements for WHO Model List of Essential Medicines Immediate-Release, Solid Oral Dosage Forms
    © World Health Organization WHO Technical Report Series, No. 937, 2006 Annex 8 Proposal to waive in vivo bioequivalence requirements for WHO Model List of Essential Medicines immediate-release, solid oral dosage forms Introduction 1. Background 2. WHO revisions to the criteria for Biopharmaceutics Classifi cation System classifi cation 3. WHO extensions to the scope of application of the biowaiver 4. WHO additional criteria for application of the biowaiver procedure 5. Explanation of the tables 6. Biowaiver testing procedure according to WHO Introduction This proposal is closely linked to the Multisource (generic) pharmaceutical products: guidelines on registration requirements to establish interchange- ability (WHO Technical Report Series, No. 937, Annex 7). It aims to give national authorities suffi cient background information on the various orally administered active pharmaceutical ingredients (APIs) on the WHO Model List of Essential Medicines (EML), also taking into account local usage of the API, to enable them to make an informed decision as to whether generic formulations should be subjected to in vivo bioequivalence (BE) studies or whether a biowaiver can be granted. In light of scientifi c work and dis- cussion in the last decade, some of the criteria used to evaluate the API in terms of potential for a biowaiver have been revised to allow a broadened scope of application. The result is that many APIs on the EML can now be considered for the biowaiver procedure, subject to the usage and risks in the national setting. 1. Background 1.1 Initiatives to allow biowaivers based on the Biopharmaceutics Classifi cation System In 1995 the American Department of Health and Human Services, US Food and Drug Administration (HHS-FDA) instigated the Biopharmaceutics 391 TSR2006_Annexs6-9.indd 391 4.5.2006 15:48:56 Classifi cation System (BCS), with the aim of granting so-called biowaiv- ers for scale-up and post-approval changes (SUPAC) (www.fda.gov/cder/ guidance/cmc5.pdf).
    [Show full text]
  • Page Numbers in Bold Type Relate to Monograph Titles Index A769
    page numbers in bold type relate to monograph titles Index A769 Index Page numbers in bold type relate to monograph titles. Pages – Vol I: i – xxviii, (Preliminaries and Introduction) 1 – 1172, (General Notices and Monographs) Pages – Vol II: xxix – xxxvi, (Preliminaries) 1173 – 2252, (General Notices and Monographs) Pages – Vol III: xxxvii – xliv, (Preliminaries) 2253 – 3794, (General Notices and Monographs) Pages – Vol IV: xlv – lii, (Preliminaries) 3795 – 3828, (General Notices) S1 – S134, (Spectra) A1 – A768, (Appendices; Supplementary Chapters) page numbers in bold type relate to monograph titles Index A771 Acetate–edetate Buffer Solution pH 5.5, Aciclovir Tablets, 2341 A A141 Aciclovir Tablets, Dispersible, 2341 Abbreviated, A519 Acetates, Reactions of, A239 Acicular, A449 Adjectives, A519 Acetazolamide, 52,S5 Acid Blue 92, A19 Anions, A519 Acetazolamide Tablets, 2336 Acid Blue 92 Solution, A19 Cations, A519 Acetic Acid, A17 Acid Blue 83, A19 Preparations, A519 Acetic Acid (6 per cent), 54 Acid Blue 93 Solution, A19 Titles of Monographs, A519 Acetic Acid (33 per cent), 55 Acid Blue 90, A19 Abbreviated Titles, Status of, 7, 1179, Acetic Acid, Anhydrous, A18 Acid Gentian Mixture, 3585 2259, 3801 Acetic Acid, Deuterated, A46 Acid Gentian Oral Solution, 3585 Abnormal Toxicity, Test for, A354 Acetic Acid, Dilute, A18 Acid Potassium Iodobismuthate About, definition of, 5, 1177, 2257, Acetic Acid, Dilute, see Acetic Acid Solution, A100 3799 (6 per cent) Acid Value, A275 Absolute Alcohol, see Ethanol Acetic Acid, Glacial, 54, A18 Acid/base
    [Show full text]
  • Botulinum Toxin
    Botulinum toxin From Wikipedia, the free encyclopedia Jump to: navigation, search Botulinum toxin Clinical data Pregnancy ? cat. Legal status Rx-Only (US) Routes IM (approved),SC, intradermal, into glands Identifiers CAS number 93384-43-1 = ATC code M03AX01 PubChem CID 5485225 DrugBank DB00042 Chemical data Formula C6760H10447N1743O2010S32 Mol. mass 149.322,3223 kDa (what is this?) (verify) Bontoxilysin Identifiers EC number 3.4.24.69 Databases IntEnz IntEnz view BRENDA BRENDA entry ExPASy NiceZyme view KEGG KEGG entry MetaCyc metabolic pathway PRIAM profile PDB structures RCSB PDB PDBe PDBsum Gene Ontology AmiGO / EGO [show]Search Botulinum toxin is a protein and neurotoxin produced by the bacterium Clostridium botulinum. Botulinum toxin can cause botulism, a serious and life-threatening illness in humans and animals.[1][2] When introduced intravenously in monkeys, type A (Botox Cosmetic) of the toxin [citation exhibits an LD50 of 40–56 ng, type C1 around 32 ng, type D 3200 ng, and type E 88 ng needed]; these are some of the most potent neurotoxins known.[3] Popularly known by one of its trade names, Botox, it is used for various cosmetic and medical procedures. Botulinum can be absorbed from eyes, mucous membranes, respiratory tract or non-intact skin.[4] Contents [show] [edit] History Justinus Kerner described botulinum toxin as a "sausage poison" and "fatty poison",[5] because the bacterium that produces the toxin often caused poisoning by growing in improperly handled or prepared meat products. It was Kerner, a physician, who first conceived a possible therapeutic use of botulinum toxin and coined the name botulism (from Latin botulus meaning "sausage").
    [Show full text]
  • SERATEC® Drug Screen
    SERATEC ® Gesellschaft für Biotechnologie mbH Ernst-Ruhstrat-Str. 5 D -37079 Göttingen Phone: +49 (0)551/504 800 • Fax: +49 (0)551/504 80 80 • e-mail: [email protected], web: www.seratec.com SERATEC Drug Screen BZO REF DSC-BZO A visual one-step immunoassay for the qualitative detection of benzodiazepines in human urine. For professional In Vitro diagnostic use only. INTENDED USE A control band with a different antigen/antibody reaction is also added The SERATEC Drug Screen BZO is a lateral flow, one-step immu- to the immunochromatographic membrane strip at the control region noassay for the qualitative detection of benzodiazepines in human (C) to indicate that the test has performed properly. This control line urine at a cut-off of 300 ng/ml (Oxazepam). This product is used to should always appear, regardless of the presence of drug and me- obtain a visual, qualitative result and is intended for professional use. tabolite. This means that negative urine will produce two colored The assay should not be used without proper supervision and is not bands, and positive urine will produce only one band. The presence intended for over the counter sale to lay persons. of this colored band in the control region also serves as 1) verification This assay provides only a preliminary analytical test result. A more that sufficient volume has been added, and 2) that proper flow was specific alternative chemical method must be used in order to obtain obtained. a confirmed analytical result. Gas chromatography/mass spectrome- STORAGE AND STABILITY try (GC/ MS) has been established as the preferred confirmatory The test kit is to be stored refrigerated or at room temperature +4-+30 method by the National Institute of Drug Abuse (NIDA).
    [Show full text]
  • 14 Informe 40.Pdf
    WHO Technical Report Series 937 SPECIFICATIONS This report presents the recommendations of an international WHO EXPERT COMMITTEE group of experts convened by the World Health Organization to consider matters concerning the quality assurance of ON SPECIFICATIONS FOR pharmaceuticals and specifi cations for drug substances and dosage forms. PHARMACEUTICAL PREPARATIONS FOR The report is complemented by a number of annexes. These include: a list of available International Chemical Reference PHARMACEUTICAL Substances and International Infrared Spectra; supplementary guidelines on good manufacturing practices for heating, ventilation and air-conditioning systems for non-sterile pharmaceutical dosage forms; updated supplementary guidelines on good manufacturing practices for the manufacture of herbal medicines; supplementary guidelines on Fortieth Report good manufacturing practices for validation; good distribution practices for pharmaceutical products; a model quality assurance PREPARATIONS system for procurement agencies (recommendations for quality assurance systems focusing on prequalifi cation of products and manufacturers, purchasing, storage and distribution of pharmaceutical products); multisource (generic) pharmaceutical products: guidelines on registration requirements to establish interchangeability; a proposal to waive in vivo bioequivalence requirements for WHO Model List of Essential Medicines immediate-release, solid oral WHO dosage forms; and additional guidance for organizations Technical performing in vivo bioequivalence studies.
    [Show full text]