DOCSLIB.ORG

Food and Drug Administration, HHS § 201.323

Total Page:16

File Type:pdf, Size:1020Kb

Download full-text PDF Read full-text
Food and Drug Administration, HHS § 201.323 Food and Drug Administration, HHS § 201.323 liver damage or gastrointestinal bleed- calcium, choline salicylate, magnesium ing). OTC drug products containing in- salicylate, or sodium salicylate] or ternal analgesic/antipyretic active in- other pain relievers/fever reducers. [Ac- gredients may cause similar adverse ef- etaminophen and (insert one nonste- fects. FDA concludes that the labeling roidal anti-inflammatory analgesic/ of OTC drug products containing inter- antipyretic ingredient—including, but nal analgesic/antipyretic active ingre- not limited to aspirin, carbaspirin cal- dients should advise consumers with a cium, choline salicylate, magnesium history of heavy alcohol use to consult salicylate, or sodium salicylate] may a physician. Accordingly, any OTC cause liver damage and stomach bleed- drug product, labeled for adult use, ing.’’ containing any internal analgesic/anti- (b) Requirements to supplement ap- pyretic active ingredients (including, proved application. Holders of approved but not limited to, acetaminophen, as- applications for OTC drug products pirin, carbaspirin calcium, choline sa- that contain internal analgesic/anti- licylate, ibuprofen, ketoprofen, magne- pyretic active ingredients that are sub- sium salicylate, naproxen sodium, and ject to the requirements of paragraph sodium salicylate) alone or in combina- (a) of this section must submit supple- tion shall bear an alcohol warning ments under § 314.70(c) of this chapter statement in its labeling as follows: to include the required warning in the (1) Acetaminophen. ‘‘Alcohol Warn- product’s labeling. Such labeling may ing’’ [heading in boldface type]: ‘‘If you be put into use without advance ap- consume 3 or more alcoholic drinks proval of FDA provided it includes the every day, ask your doctor whether exact information included in para- you should take acetaminophen or graph (a) of this section. other pain relievers/fever reducers. Ac- (c) Any drug product subject to this etaminophen may cause liver damage.’’ section that is not labeled as required (2) Nonsteroidal anti-inflammatory an- and that is initially introduced or ini- algesic/antipyretic active ingredients—in- tially delivered for introduction into cluding but not limited to aspirin, interstate commerce after April 23, carbaspirin calcium, choline salicylate, 1999, is misbranded under section 502 of ibuprofen, ketoprofen, magnesium salicy- the Federal Food, Drug, and Cosmetic late, naproxen sodium, and sodium salicy- Act (21 U.S.C. 352) and is subject to reg- late. ‘‘Alcohol Warning’’ [heading in ulatory action. boldface type]: ‘‘If you consume 3 or more alcoholic drinks every day, ask [63 FR 56801, Oct. 23, 1998] your doctor whether you should take [insert one nonsteroidal anti-inflam- § 201.323 Aluminum in large and small matory analgesic/antipyretic active in- volume parenterals used in total parenteral nutrition. gredient] or other pain relievers/fever reducers. [Insert one nonsteroidal anti- (a) The aluminum content of large inflammatory analgesic/antipyretic ac- volume parenteral (LVP) drug products tive ingredient] may cause stomach used in total parenteral nutrition bleeding.’’ (TPN) therapy must not exceed 25 (3) Combinations of acetaminophen with micrograms per liter (µg/L). nonsteroidal anti-inflammatory analgesic/ (b) The package insert of LVP’s used antipyretic active ingredients—including in TPN therapy must state that the but not limited to aspirin, carbaspirin cal- drug product contains no more than 25 cium, choline salicylate, ibuprofen, µg/L of aluminum. This information ketoprofen, magnesium salicylate, must be contained in the ‘‘Pre- naproxen sodium, and sodium salicylate. cautions’’ section of the labeling of all ‘‘Alcohol Warning’’ [heading in bold- large volume parenterals used in TPN face type]: ‘‘If you consume 3 or more therapy. alcoholic drinks every day, ask your (c) Except as provided in paragraph doctor whether you should take [insert (d) of this section, the maximum level acetaminophen and one nonsteroidal of aluminum present at expiry must be anti-inflammatory analgesic/anti- stated on the immediate container pyretic active ingredient—including, label of all small volume parenteral but not limited to aspirin, carbaspirin (SVP) drug products and pharmacy 73 VerDate Aug<04>2004 12:59 Apr 25, 2005 Jkt 205068 PO 00000 Frm 00083 Fmt 8010 Sfmt 8010 Y:\SGML\205068.XXX 205068 Pt. 201, App. A 21 CFR Ch. I (4–1–05 Edition) bulk packages (PBPs) used in the prep- (f) Applicants and manufacturers aration of TPN solutions. The alu- must use validated assay methods to minum content must be stated as fol- determine the aluminum content in lows: ‘‘Contains no more than ll µg/L parenteral drug products. The assay of aluminum.’’ The immediate con- methods must comply with current tainer label of all SVP’s and PBP’s good manufacturing practice require- that are lyophilized powders used in ments. Applicants must submit to the the preparation of TPN solutions must Food and Drug Administration valida- contain the following statement: tion of the method used and release ‘‘When reconstituted in accordance data for several batches. Manufactur- with the package insert instructions, ers of parenteral drug products not the concentration of aluminum will be subject to an approved application no more than ll µg/L.’’ This max- must make assay methodology avail- imum level of aluminum must be stat- able to FDA during inspections. Hold- ed as the highest of: ers of pending applications must sub- (1) The highest level for the batches mit an amendment under § 314.60 or produced during the last 3 years; § 314.96 of this chapter. (2) The highest level for the latest [65 FR 4110, Jan. 26, 2000, as amended at 67 five batches, or FR 70691, Nov. 26, 2002; 68 FR 32981, June 3, (3) The maximum historical level, 2003] but only until completion of produc- APPENDIX A TO PART 201—EXAMPLES OF tion of the first five batches after July GRAPHIC ENHANCEMENTS USED BY FDA 26, 2004. (d) If the maximum level of alu- I. SECTION 201.66 STANDARD LABELING FORMAT µ minum is 25 g/L or less, instead of A. Overall stating the exact amount of aluminum as required in paragraph (c) of this sec- 1. The ‘‘Drug Facts’’ labeling is set off in a tion, the immediate container label box or similar enclosure by the use of a barline with all black type printed on a may state: ‘‘Contains no more than 25 white, color contrasting background. µg/L of aluminum.’’ If the SVP or PBP is a lyophilized powder, the immediate B. Typeface and size container label may state: ‘‘When re- 1. ‘‘Drug Facts’’ is set in 14 point Helvetica constituted in accordance with the Bold Italic, left justified. package insert instructions, the con- 2. ‘‘Drug Facts (continued)’’ is set in 8 centration of aluminum will be no point Helvetica Bold Italic for the words more than 25 µg/L’’. ‘‘Drug Facts’’ and 8 point Helvetica Regular for the word ‘‘(continued)’’ and is left justi- (e) The package insert for all LVP’s, fied. all SVP’s, and PBP’s used in TPN must 3. The headings (e.g., ‘‘Directions’’) are set contain a warning statement. This in 8 point Helvetica Bold Italic, left justified. warning must be contained in the 4. The subheadings (e.g., ‘‘Ask a doctor or ‘‘Warnings’’ section of the labeling. pharmacist before use if you are’’) are set in The warning must state: 6 point Helvetica Bold, left justified. 5. The information is set in 6 point WARNING: This product contains alu- Helvetica Regular with 6.5 point leading, left minum that may be toxic. Aluminum may justified. reach toxic levels with prolonged parenteral 6. The heading ‘‘Purpose’’ is right justified. administration if kidney function is im- 7. The bullet is a 5-point solid square. paired. Premature neonates are particularly 8. Two em spacing separates bullets when at risk because their kidneys are immature, more than one bullet is on the same line. and they require large amounts of calcium 9. A table format is used for 3 or more dos- and phosphate solutions, which contain alu- age directions. minum. 10. A graphic appears at the bottom of the Research indicates that patients with im- first panel leading the reader to the next paired kidney function, including premature panel. neonates, who receive parenteral levels of C. Barlines and hairlines aluminum at greater than 4 to 5 µg/kg/day accumulate aluminum at levels associated 1. A 2.5-point horizontal barline extends to with central nervous system and bone tox- each end of the ‘‘Drug Facts’’ box (or similar icity. Tissue loading may occur at even enclosure), providing separation between lower rates of administration. each of the headings. 74 VerDate Aug<04>2004 12:59 Apr 25, 2005 Jkt 205068 PO 00000 Frm 00084 Fmt 8010 Sfmt 8002 Y:\SGML\205068.XXX 205068.
Load more

Recommended publications
  • Pharmacokinetics of Salicylic Acid Following Intravenous and Oral Administration of Sodium Salicylate in Sheep
    animals Article Pharmacokinetics of Salicylic Acid Following Intravenous and Oral Administration of Sodium Salicylate in Sheep Shashwati Mathurkar 1,*, Preet Singh 2 ID , Kavitha Kongara 2 and Paul Chambers 2 1 1B, He Awa Crescent, Waikanae 5036, New Zealand 2 School of Veterinary Sciences, College of Sciences, Massey University, Palmerston North 4474, New Zealand; [email protected] (P.S.); [email protected] (K.K.); [email protected] (P.C.) * Correspondence: [email protected]; Tel.: +64-221-678-035 Received: 13 June 2018; Accepted: 16 July 2018; Published: 18 July 2018 Simple Summary: Scarcity of non-steroidal anti-inflammatory drugs (NSAID) to minimise the pain in sheep instigated the current study. The aim of this study was to know the pharmacokinetic parameters of salicylic acid in New Zealand sheep after administration of multiple intravenous and oral doses of sodium salicylate (sodium salt of salicylic acid). Results of the study suggest that the half-life of the drug was shorter and clearance was faster after intravenous administration as compared to that of the oral administration. The minimum effective concentration required to produce analgesia in humans (16.8 µL) was achieved in sheep for about 0.17 h in the current study after intravenous administration of 100 and 200 mg/kg body weight of sodium salicylate. However, oral administration of these doses failed to achieve the minimum effective concentration as mentioned above. This study is of significance as it adds valuable information on pharmacokinetics and its variation due to breed, species, age, gender and environmental conditions.
    [Show full text]
  • KETOFEN ® (Ketoprofen)
    See other side for instructions for use in cattle. KETOFEN® (ketoprofen) Injectable Solution, 100 mg/mL For intravenous use in horses. PHARMACOLOGY KETOFEN is a non-narcotic, non-steroidal anti-inflammatory agent CAUTION with analgesic and antipyretic properties. Federal law restricts this drug to use by or on the order of a In horses, intravenous dosages of ketoprofen ranging from licensed veterinarian. 0.5 to 1.5 mg/lb resulted in dosage dependent anti-inflammatory effects in the chronic adjuvant carpitis model as depicted in the DESCRIPTION following graph. Ketoprofen is a non-steroidal anti-inflammatory agent of the propionic acid class that includes ibuprofen, naproxen and fenoprofen. Active Ingredient: Each mL contains 100 mg ketoprofen/mL of aqueous solution. Inactive Ingredients: 70 mg L-Arginine/mL; citric acid (to adjust pH); benzyl alcohol, 0.025 g (as preservative). It is packaged in a multiple dose bottle. INDICATION KETOFEN® (ketoprofen) is recommended for the alleviation of inflammation and pain associated with musculoskeletal disorders in the horse. DOSAGE AND ADMINISTRATION The recommended dosage is 1 mg/lb (1 mL/100 lbs) of body weight administered intravenously once daily. Treatment may be repeated for up to five days. Onset of activity is within two hours with peak response by 12 hours. Use contents within 4 months of first vial puncture. CONTRAINDICATIONS Additional studies using the same model in horses have There are no known contraindications to this drug when used as shown that the effects of ketoprofen are maximal by 12 hours directed. and still measurable at 24 hours after each dosage as depicted in Intra-arterial injection should be avoided.
    [Show full text]
  • Sodium-Salicylate-European-Public-Mrl-Assessment-Report-Epmar-Committee-Veterinary
    27 October 2010 EMA/CVMP/562066/2007 Veterinary Medicines and Product Data Management Committee for Medicinal Products for Veterinary Use European public MRL assessment report (EPMAR) Sodium salicylate (turkeys) On 12 October 2010 the European Commission adopted a Regulation1 establishing provisional maximum residue limits for sodium salicylate in turkeys, valid throughout the European Union. These provisional maximum residue limits were based on the favourable opinion and the assessment report adopted by the Committee for Medicinal Products for Veterinary Use. In turkeys, sodium salicylate is intended for use orally as an antipyretic in the treatment of acute respiratory diseases. Sodium salicylate was previously assessed for the purpose of establishing maximum residue limits and was entered in Annex II of Regulation (EEC) No 2377/902 (no MRL required) for topical use in all food producing species except fish and for oral use in bovine and porcine species. Chevita Tierarzneimittel GmbH submitted to the European Medicines Agency on 4 January 2007 an application for the extension of existing entry in Annex II of Regulation (EEC) No 2377/90 for sodium salicylates to turkeys. On 12 December 2007 the Committee for Medicinal Products for Veterinary Use adopted an opinion recommending the amendment of the entry in Annex II of Regulation (EEC) No 2377/90 to include sodium salicylate for oral use in turkeys. The European Commission subsequently returned the opinion to the Committee to consider whether its opinion should be reviewed to take into account issues raised during the Commission’s inter service consultation and in particular to consider whether establishment of maximum residue limits for sodium salicylate in turkeys should be established.
    [Show full text]
  • Nsaids: Dare to Compare 1997
    NSAIDs TheRxFiles DARE TO COMPARE Produced by the Community Drug Utilization Program, a Saskatoon District Health/St. Paul's Hospital program July 1997 funded by Saskatchewan Health. For more information check v our website www.sdh.sk.ca/RxFiles or, contact Loren Regier C/O Pharmacy Department, Saskatoon City Hospital, 701 Queen St. Saskatoon, SK S7K 0M7, Ph (306)655-8506, Fax (306)655-8804; Email [email protected] We have come a long way from the days of willow Highlights bark. Today salicylates and non-steroidal anti- • All NSAIDs have similar efficacy and side inflammatory drugs (NSAIDs) comprise one of the effect profiles largest and most commonly prescribed groups of • In low risk patients, Ibuprofen and naproxen drugs worldwide.1 In Saskatchewan, over 20 may be first choice agents because they are different agents are available, accounting for more effective, well tolerated and inexpensive than 300,000 prescriptions and over $7 million in • Acetaminophen is the recommended first line sales each year (Saskatchewan Health-Drug Plan agent for osteoarthritis data 1996). Despite the wide selection, NSAIDs • are more alike than different. Although they do Misoprostol is the only approved agent for differ in chemical structure, pharmacokinetics, and prophylaxis of NSAID-induced ulcers and is to some degree pharmacodynamics, they share recommended in high risk patients if NSAIDS similar mechanisms of action, efficacy, and adverse cannot be avoided. effects. week or more to become established. For this EFFICACY reason, an adequate trial of 1-2 weeks should be NSAIDs work by inhibiting cyclooxygenase (COX) allowed before increasing the dose or changing to and subsequent prostaglandin synthesis as well as another NSAID.
    [Show full text]
  • New Zealand Data Sheet 1
    New Zealand Data Sheet 1. PRODUCT NAME NAXEN® 250 mg tablets 2. QUALITATIVE AND QUANTITATIVE COMPOSITION Each NAXEN 250 mg tablet contains 250 mg of Naproxen For the full list of excipients, see section 6.1. 3. PHARMACEUTICAL FORM NAXEN 250 mg tablets are yellow, biconvex, round tablet of 11 mm diameter with one face engraved NX250 and having a bisecting score. The score line is only to facilitate breaking for ease of swallowing and not to divide into equal doses. 4. CLINICAL PARTICULARS 4.1. Therapeutic indications NAXEN is indicated in adults for the relief of symptoms associated with rheumatoid arthritis, osteoarthritis, ankylosing spondylitis, tendonitis and bursitis, acute gout and primary dysmenorrhoea. NAXEN is indicated in children for juvenile arthritis. 4.2. Dose and method of administration After assessing the risk/benefit ratio in each individual patient, the lowest effective dose for the shortest possible duration should be used (see Section 4.4). During long-term administration the dose of naproxen may be adjusted up or down depending on the clinical response of the patient. A lower daily dose may suffice for long-term administration. In patients who tolerate lower doses well, the dose may be increased to 1000 mg per day when a higher level of anti-inflammatory/analgesic 1 | P a g e activity is required. When treating patients with naproxen 1000 mg/day, the physician should observe sufficient increased clinical benefit to offset the potential increased risk. Dose Adults For rheumatoid arthritis, osteoarthritis and ankylosing spondylitis Initial therapy: The usual dose is 500-1000 mg per day taken in two doses at 12 hour intervals.
    [Show full text]
  • Colonoscopy Instructions
    Colonoscopy Checklist Five days before your colonoscopy: Stop any medications that thin the blood (see list below) Discuss the discontinuation of these medications with your primary care physician to ensure that it is safe to stop them Three days before your colonoscopy: Stop eating high fiber foods including nuts, corn, popcorn, raw fruits, vegetables, and bran Stop fiber supplements The day before your colonoscopy: Have a normal breakfast If your colonoscopy is scheduled before noon the following day, do not have any lunch If your colonoscopy is scheduled after noon, have a light lunch Have clear liquids for the rest of the day (see below) Start prep as instructed by your physician Do not have anything to eat or drink after midnight The day of your colonoscopy: Take your blood pressure medications with a sip of water Make sure you bring your driver’s license or photo ID and leave valuables and jewelry at home Clear Liquid Diet Water Any kind of soft drink (ginger ale, cola, tonic, etc) Gatorade Apple Juice Orange Juice without pulp Lemonade Tea/Coffee (without milk) Dietary supplements (Ensure, Boost, Enlive, etc) Clear broth (vegetable, chicken, or beef) Jell‐O (stay away from red, blue, or purple colors) Ice pops without milk or fruit bits Honey or sugar NO DAIRY PRODUCTS Medications to stop prior to colonoscopy Below is a list of many medications (but not all) that fall into these categories. It is important to remember that there are hundreds of over‐the‐counter medications that contain NSAIDs or aspirin, so it is important to carefully read the label of any medication that you are taking (prescription or over‐the‐counter).
    [Show full text]
  • Salicylate, Diflunisal and Their Metabolites Inhibit CBP/P300 and Exhibit Anticancer Activity
    RESEARCH ARTICLE Salicylate, diflunisal and their metabolites inhibit CBP/p300 and exhibit anticancer activity Kotaro Shirakawa1,2,3,4, Lan Wang5,6, Na Man5,6, Jasna Maksimoska7,8, Alexander W Sorum9, Hyung W Lim1,2, Intelly S Lee1,2, Tadahiro Shimazu1,2, John C Newman1,2, Sebastian Schro¨ der1,2, Melanie Ott1,2, Ronen Marmorstein7,8, Jordan Meier9, Stephen Nimer5,6, Eric Verdin1,2* 1Gladstone Institutes, University of California, San Francisco, United States; 2Department of Medicine, University of California, San Francisco, United States; 3Department of Hematology and Oncology, Kyoto University, Kyoto, Japan; 4Graduate School of Medicine, Kyoto University, Kyoto, Japan; 5University of Miami, Gables, United States; 6Sylvester Comprehensive Cancer Center, Miami, United States; 7Perelman School of Medicine, University of Pennsylvania, Philadelphia, United States; 8Department of Biochemistry and Biophysics, Abramson Family Cancer Research Institute, Philadelphia, United States; 9Chemical Biology Laboratory, National Cancer Institute, Frederick, United States Abstract Salicylate and acetylsalicylic acid are potent and widely used anti-inflammatory drugs. They are thought to exert their therapeutic effects through multiple mechanisms, including the inhibition of cyclo-oxygenases, modulation of NF-kB activity, and direct activation of AMPK. However, the full spectrum of their activities is incompletely understood. Here we show that salicylate specifically inhibits CBP and p300 lysine acetyltransferase activity in vitro by direct *For correspondence: everdin@ competition with acetyl-Coenzyme A at the catalytic site. We used a chemical structure-similarity gladstone.ucsf.edu search to identify another anti-inflammatory drug, diflunisal, that inhibits p300 more potently than salicylate. At concentrations attainable in human plasma after oral administration, both salicylate Competing interests: The and diflunisal blocked the acetylation of lysine residues on histone and non-histone proteins in cells.
    [Show full text]
  • (Ketorolac Tromethamine Tablets) Rx Only WARNING TORADOL
    TORADOL ORAL (ketorolac tromethamine tablets) Rx only WARNING TORADOLORAL (ketorolac tromethamine), a nonsteroidal anti-inflammatory drug (NSAID), is indicated for the short-term (up to 5 days in adults), management of moderately severe acute pain that requires analgesia at the opioid level and only as continuation treatment following IV or IM dosing of ketorolac tromethamine, if necessary. The total combined duration of use of TORADOLORAL and ketorolac tromethamine should not exceed 5 days. TORADOLORAL is not indicated for use in pediatric patients and it is NOT indicated for minor or chronic painful conditions. Increasing the dose of TORADOLORAL beyond a daily maximum of 40 mg in adults will not provide better efficacy but will increase the risk of developing serious adverse events. GASTROINTESTINAL RISK Ketorolac tromethamine, including TORADOL can cause peptic ulcers, gastrointestinal bleeding and/or perforation of the stomach or intestines, which can be fatal. These events can occur at any time during use and without warning symptoms. Therefore, TORADOL is CONTRAINDICATED in patients with active peptic ulcer disease, in patients with recent gastrointestinal bleeding or perforation, and in patients with a history of peptic ulcer disease or gastrointestinal bleeding. Elderly patients are at greater risk for serious gastrointestinal events (see WARNINGS). CARDIOVASCULAR RISK NSAIDs may cause an increased risk of serious cardiovascular thrombotic events, myocardial infarction, and stroke, which can be fatal. This risk may increase with duration of use. Patients with cardiovascular disease or risk factors for cardiovascular disease may be at greater risk (see WARNINGS and CLINICAL STUDIES). TORADOL is CONTRAINDICATED for the treatment of peri-operative pain in the setting of coronary artery bypass graft (CABG) surgery (see WARNINGS).
    [Show full text]
  • Flufenamic Acid Prevents Behavioral Manifestations of Salicylate-Induced Tinnitus in the Rat
    Experimental research Flufenamic acid prevents behavioral manifestations of salicylate-induced tinnitus in the rat Ramazan Bal1, Yasemin Ustundag2, Funda Bulut3, Caner Feyzi Demir4, Ali Bal5 1Department of Physiology, Faculty of Medicine, Gaziantep University, Gaziantep, Corresponding author: Turkey Prof. Dr. Ramazan Bal 2Department of Anatomy, Faculty of Veterinary, Firat University, Elazig, Turkey Department of Physiology 3Department of Medical Biology, Faculty of Medicine, Kirikkale University, Kirikkale, Faculty of Medicine Turkey Gaziantep University 4Department of Neurology, Faculty of Medicine, Firat University, Elazig, Turkey 27310 Gaziantep, Turkey 5Department of Plastic-Reconstructive and Esthetic Surgery, Faculty of Medicine, Phone: +90 342 Firat University, Elazig, Turkey 3606060/77732 Fax: +90 342 360 16 17 Submitted: 7 March 2014 E-mail: [email protected], Accepted: 21 May 2014 [email protected] Arch Med Sci 2016; 12, 1: 208–215 DOI: 10.5114/aoms.2016.57597 Copyright © 2016 Termedia & Banach Abstract Introduction: Tinnitus is defined as a phantom auditory sensation, the per- ception of sound in the absence of external acoustic stimulation. Given that flufenamic acid (FFA) blocks TRPM2 cation channels, resulting in reduced neuronal excitability, we aimed to investigate whether FFA suppresses the behavioral manifestation of sodium salicylate (SSA)-induced tinnitus in rats. Material and methods: Tinnitus was evaluated using a conditioned lick sup- pression model of behavioral testing. Thirty-one Wistar rats, randomly di- vided into four treatment groups, were trained and tested in the behavioral experiment: (1) control group: DMSO + saline (n = 6), (2) SSA group: DMSO + SSA (n = 6), (3) FFA group: FFA (66 mg/kg bw) + saline (n = 9), (4) FFA + SSA group: FFA (66 mg/kg bw) + SSA (400 mg/kg bw) (n = 10).
    [Show full text]
  • Efficacy of Ketoprofen Vs. Ibuprofen and Diclofenac: a Systematic Review of the Literature and Meta-Analysis P
    Efficacy of ketoprofen vs. ibuprofen and diclofenac: a systematic review of the literature and meta-analysis P. Sarzi-Puttini1, F. Atzeni1, L. Lanata2, M. Bagnasco2 1Rheumatology Unit, L. Sacco University Hospital, Milan, Italy; 2Medical Department, Dompé SpA, Milan, Italy. Abstract Objective The aim of this systematic review of the literature and meta-analysis of randomised controlled trials (RCTs) was to compare the efficacy of orally administered ketoprofen with that of ibuprofen and/or diclofenac. Methods The literature was systematically reviewed in accordance with the Cochrane Collaboration guidelines. The search was restricted to randomised clinical trials published in the Medline and Embase databases up to June 2011, and comparing the efficacy of oral ketoprofen (50–200 mg/day) with ibuprofen (600-1800 mg/day) or diclofenac (75–150 mg/day). Results A total of 13 RCTs involving 898 patients met the inclusion criteria: eight comparing ketoprofen with ibuprofen, and five comparing ketoprofen with diclofenac. The results of the meta-analysis showed a statistically significant difference in efficacy in favour of ketoprofen. The difference between ketoprofen and the pooled ibuprofen/diclofenac data was also statistically significant (0.459, 95% CI 0.33-0.58; p=0.00) at all point-estimates of the mean weighted size effect. Ketoprofen was significantly superior to both diclofenac (mean = 0.422; 95% CI 0.19-0.65; p=0.0007) and ibuprofen (mean = 0.475; 95% CI 0.32-0.62; p=0.0000) at all point-estimates. Heterogeneity for the analysed efficacy outcome was not statisically significant in any of the meta-analyses. Conclusion The efficacy of orally administered ketoprofen in relieving moderate-severe pain and improving functional status and general condition was significantly better than that of ibuprofen and/or diclofenac.
    [Show full text]
  • Medication Guide for Non-Steroidal Anti-Inflammatory Drugs (Nsaids)
    Medication Guide for Non-Steroidal Anti-Inflammatory Drugs (NSAIDs) (See the end of this Medication Guide for a list of prescription NSAID medicines.) What is the most important information I should know about medicines called Non-Steroidal Anti- Inflammatory Drugs (NSAIDs)? NSAID medicines may increase the chance of a heart attack or stroke that can lead to death. This chance increases: • with longer use of NSAID medicines • in people who have heart disease NSAID medicines should never be used right before or after a heart surgery called a “coronary artery bypass graft (CABG).” NSAID medicines can cause ulcers and bleeding in the stomach and intestines at any time during treatment. Ulcers and bleeding: can happen without warning symptoms may cause death The chance of a person getting an ulcer or bleeding increases with: ▪ taking medicines called "corticosteroids” and “anticoagulants” ▪ longer use ▪ smoking ▪ drinking alcohol ▪ older age ▪ having poor health NSAID medicines should only be used: • exactly as prescribed • at the lowest dose possible for your treatment • for the shortest time needed What are Non-Steroidal Anti-Inflammatory Drugs (NSAIDs)? NSAID medicines are used to treat pain and redness, swelling, and heat (inflammation) from medical conditions such as: different types of arthritis menstrual cramps and other types of short-term pain Who should not take a Non-Steroidal Anti-Inflammatory Drug (NSAID)? Do not take an NSAID medicine: • if you had an asthma attack, hives, or other allergic reaction with aspirin or any other NSAID medicine • for pain right before or after heart bypass surgery Tell your healthcare provider: • about all of your medical conditions.
    [Show full text]
  • Central Nervous System Toxicity of Mefenamic Acid
    Central Nervous System toxicity of mefenamic acid overdose compared to other NSAIDs: an analysis of cases reported to the United Kingdom National Poisons Information Service. Running header: CNS toxicity of mefenamic acid A Kamour1, S Crichton2, G Cooper3, DJ Lupton4, M Eddleston4,5, JA Vale6, JP Thompson 3, SHL Thomas1,7 1National Poisons Information Service, Newcastle Unit, Newcastle upon Tyne Hospitals NHS Foundation Trust, Wolfson Unit, Claremont Place, Newcastle upon Tyne, NE2 4HH. 2Department of Primary Care and Public Health, King's College London, Capital House, London, SE1 3QD 3National Poisons Information Service, Cardiff Unit, University Hospital Llandough, Penlan Road, Penarth, Vale of Glamorgan CF64 2XX. 4National Poisons Information Service, Edinburgh Unit, Royal Infirmary of Edinburgh, 51 Little France Crescent, Old Dalkeith Road, Edinburgh EH16 4SA. 5Pharmacology, Toxicology and Therapeutics, University/BHF Centre for Cardiovascular Science, University of Edinburgh, Edinburgh, UK. 6National Poisons Information Service, Birmingham Unit, City Hospital, Dudley Road, Birmingham B18 7QH. 7Medical Toxicology Centre, Institute of Cellular Medicine, Wolfson Building, Newcastle University, Newcastle NE2 4HH. Address for correspondence: Dr Ashraf Kamour, Acute Medical Unit, North Manchester General Hospital Delaunays Road, Crumpsall, Manchester, M8 5RB, UK. Tel: +44 (0)161 918 4673 This article has been accepted for publication and undergone full peer review but has not been through the copyediting, typesetting, pagination and proofreading process which may lead to differences between this version and the Version of Record. Please cite this article as doi: 10.1111/bcp.13169 This article is protected by copyright. All rights reserved. Fax: +44 (0)161 604 5323 Email: [email protected] Keywords: Mefenamic acid, non-steroidal anti-inflammatory drug, overdose, poisoning, CNS toxicity, convulsions.
    [Show full text]