Milestones in Drug Therapy MDT Series Editors Prof. Dr. Michael J. Parnham Prof. Dr. J. Bruinve1s PLIVA INFARM Research Institute Sweelincklaan 75 Prilaz baruna Filipovica 25 NL-3723 JC Bilthoven 10000 Zagreb The Netherlands Croatia Fluoroquinolone Antibiotics Edited by A.R. Ronald and D.E. Low Springer Basel AG Editors Alian R. Ronald Donald E. Low Faculty of Medicine Microbiology Laboratory The University of Manitoba, Room C5124 MI. Sinai Hospital, Room 1487 409 Tacho Avenue 600 University Avenue Winnipeg, Manitoba, R2H 2A6 Toronto, Ontario M5G IX5 Canada Canada Advisory Board J.c. Buckingham (Imperial College School of Medicine, London, UK) D. de Wied (Rudolf Magnus Institute for Neurosciences, Utrecht, The Netherlands) F.K. Goodwin (Center on Neuroscience, Washington, USA) G. Lambrecht (J.W. Goethe Universităt, Frankfurt, Germany) Library of Congress Cataloging-in-Publication Data Fluoroquinolone antibiotics / A.R. Ronald, D.E. Low (editors). p. cm Includes bibliographical references and index. ISBN 978-3-0348-9437-1 ISBN 978-3-0348-8103-6 (eBook) DOI 10.1007/978-3-0348-8103-6 1. Quinolone antibacterial agents. 1. Ronald, Alian R. II. Low, Don E. RM666.Q55 F577 2003 616.9'2061--{!c21 2002043611 Bibliographic information published by Die Deutsche Bibliothek Die Deutsche Bibliothek lists this publication in the Deutsche Nationalbibliografie; detailed biblio graphic data is available in the internet at http://dnb.ddb.de ISBN 978-3-0348-9437-1 The publisher and editor can give no guarantee for the information on drug dosage and administration contained in this publication. The respective user must check its accuracy by consulting other sources of reference in each individual case. The use of registered names, trademarks etc. in this publication, even if not identified as such, does not imply that thcy are exempt from the relevant protective laws and regulations or free for general use. This work is subject to copyright. AII rights are reserved, whether the whole or part of the material is concerned, specifically the rights of translation, reprinting, re-use of iIlustrations, recitation, broad casting, reproduction on microfilms or in other ways, and storage in data banks. For any kind of use, permission of the copyright owner must be obtained. © 2003 Springer Basel AG Originally published by Birkhl1user Verlag, Basel -Boston -Berlin in 2003 Softcover reprint of the hardcover 1s t edition 2003 Printed on acid-free paper produced from chlorine-free pulp. TFC ~ Cover iIlustration: Quinolone structure-side effect relationship (see. p. 7) ISBN 978-3-0348-9437-1 987654321 http://www.birkhauser-science.com v Contents List of contributors VII Preface IX Gerard Sheehan and Nicholas S. Y. Chew The history of quinolones 1 Lester A. Mitscher and Zhenkun Ma Structure-activity relationships of quinolones 11 c.c. Pak-Leung Ho and Vincent Cheng Epidemiology and mechanisms of resistance 49 Lionel A. Mandell Improved safety profile of newer fluoroquinolones 73 George G. Zhanel and Ayman M. Noreddin Pharmacokinetics and pharmacodynamics (PKJPD) of fluoro- quinolones: tools for combating bacteria and preventing resistance 87 James R. Johnson Fluoroquinolones in urinary tract infection 107 Sarah A. Wyllie and Geoffrey L. Ridgway The quinolones and sexually transmitted infections 121 Anthony W. Chow Gastrointestinal and intraabdominal infections 137 Eugene Leibovitz and Ron Dagan The quinolones in otitis media and upper respiratory infections 167 Thomas J. Marrie Quinolones in pneumonia 177 Donald E. Low Fluoroquinolones for the treatment of respiratory tract infections other than pneumonia ............................ 189 VI Contents John M. Embil Quinolones for the treatment of skin, soft tissue, bone and prosthetic joint infections . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . . .. 205 Helen Giamarellou and Anastasia Antoniadou The role of fluoroquinolones in the therapy and prophylaxis of neutropenic patients with cancer .......................... 219 Ziad A. Memish and Manuel W. Mah Less usual indications: Mycobacterial, Brucella, Yersinia, Francisella and other infections ............................. 239 Allan R. Ronald and Donald E. Low The quinolones: future prospects ............................ 251 Index ................................................. 255 VII List of contributors Anastasia Antoniadou, Athens University School of Medicine, 4th Department of Internal Medicine, Sismanoglio General Hospital, 1 Sismanogliou St., 15126 Maroussi, Athens, Greece; e-mail: [email protected] Vincent C.C. Cheng, Division of Infectious Diseases, Department of Microbio logy, Queen Mary Hospital, The University of Hong Kong, Pokfulam Road, Pokfulam, Hong Kong SAR, China; e-mail: [email protected] Nicholas S.Y. Chew, Department of Infectious Diseases, Mater Misericordiae Hospital, Eccles Street, Dublin 7, Ireland; e-mail: [email protected] Anthony W. Chow, Division of Infectious Diseases, Department of Medicine, University of British Columbia and Vancouver Hospital Health Sciences Centre, 2773 Heather Street, Vancouver, BC, Canada V5Z 3J5; e-mail: [email protected]. Present address: UCSD, 3717 Nobel Dr, Apt 1327, San Diego, CA 92122, USA Ron Dagan, Pediatric Infectious Disease Unit, Soroka University Medical Center, P.O. Box 151, Beer-Sheva 84101, Israel; e-mail: [email protected] John Embil, Infection Control Unit, Health Sciences Centre, MS 673-820 Sherbrook Street, Winnipeg, MB, R3A 1R9 Canada; e-mail: [email protected] Helen Giamarellou, Athens University School of Medicine, 4th Department of Internal Medicine, Sismanoglio General Hospital, 1 Sismanogliou St., 15126 Maroussi, Athens, Greece; e-mail: [email protected] Pak-Leung Ho, Division of Infectious Diseases, Department of Microbiology, Queen Mary Hospital, The University of Hong Kong, Pokfulam Road, Pokfulam, Hong Kong SAR, China; e-mail: [email protected] James R. Johnson, VA Medical Center and Department of Medicine, Uni versity of Minnesota, Minneapolis, MN, USA; e-mail: [email protected] Eugene Leibovitz, Pediatric Infectious Disease Unit, Soroka University Medical Center, P.O. Box 151, Beer-Sheva 84101, Israel; e-mail: [email protected] Donald E. Low, Department of Microbiology, Mount Sinai Hospital, 600 University Ave., Rm. 1487, Toronto, Ontario, Canada M5G 1X5; e-mail: [email protected] Zhenkun Ma, Medicinal Chemistry, Cumbre Inc., 1502 Viceroy Drive, Dallas, TX 75235-2304, USA; e-mail: [email protected] Manuel W. Mah, Infection Prevention and Control, Peter Lougheed Centre, 3500-26th Avenue NE, Calgary, AB, T1 Y 6J4 Canada; e-mail: [email protected] VIII List of contributors Lionel A. Mandell, McMaster University, Henderson Hospital, 5th floor, 40 Wing, 711 Concession St., Hamilton, Ontario L8V lC3, Canada Thomas J. Marrie, Department of Medicine, University of Alberta, 2F1.30 Walter C. Mackenzie Health Sciences Center, 6440 112th Street, Edmonton, Alberta, Canada T6H 2B7; e-mail: [email protected] Ziad A. Memish, Departments of Medicine and Infection Prevention and Control, King Fahad National Guard Hospital, P.O. Box 22490, Riyadh 11426, Saudi Arabia; e-mail: [email protected] Lester A. Mitscher, Medicinal Chemistry Department, Kansas University, 4010 Malott Hall, 1251 Wescoe Hall Drive, Lawrence, KS 66045-7582, USA; e-mail: [email protected] Ayman M. Noreddin, Microbiology, Health Sciences Centre, MS673-820 Sherbrook Street, Winnipeg, Manitoba R3A lR9, Canada Geoffrey L. Ridgway, Department of Clinical Microbiology, University College London Hospitals, Grafton Way, London WCIE 6DB, UK; e-mail: [email protected] Allan R. Ronald, Faculty of Medicine, The Unversity of Manitoba, Room C5124, 409 TachoAvenue, Winnipeg, Manitoba, R2H 2A6, Canada; e-mail: [email protected] Gerard Sheehan, Department of Infectious Diseases, Mater Misericordiae Hospital, Eccles Street, Dublin 7, Ireland Sarah A. Wyllie, Department of Clinical Microbiology, University College London Hospitals, Grafton Way, London WCIE 6DB, UK; e-mail: [email protected] George G. Zhanel, Microbiology, Health Sciences Centre, MS673-820 Sherbrook Street, Winnipeg, Manitoba R3A lR9, Canada; e-mail: [email protected] IX Preface Since the introduction of ciprofloxacin in 1987, fluoroquinolones have expanded far beyond their early role in the treatment of urinary tract infections. Clinical applications beyond genitourinary tract infections include upper and lower respiratory infections, gastrointestinal infections, gynecologic infec tions, sexually transmitted diseases, and some skin and soft tissue infections. Their ease of administration, favorable pharmacokinetic properties, excellent tolerability, and efficacy give them enormous potential for use and misuse alike. Quinolones have few common adverse effects, most notably nausea, headache and dizziness. Less frequent but more serious adverse events include prolongation of the corrected QT interval, phototoxicity, liver enzyme abnor malities, arthropathy, and cartilage and tendon abnormalities. While possess ing many of the favorable properties of intravenous agents, most fluoro quinolones offer the convenience of oral administration, thus contributing to decreased health-care costs through increased outpatient therapy and short ened hospital stays. With the recent introduction of agents such as gatifloxacin and moxifloxacin, the traditional Gram-negative coverage of fluoroquinolones has been expanded to include Gram-positive organisms, most importantly Streptococcus pneumoniae. Several issues have arisen over the last few years with the widespread acceptance and use of these agents: the emergence and dissemination of resist ance, the need for extensive clinical experience before we can feel confident about the safety of new agents, and the need for head-to-head clinical trials to define the optimal role of each agent. During the last decade we have seen the emergence and dissemination of resistance to the main pathogens for which these agents have been targeted, including Escherichia coli, Klebsiella spp., Pseudomonas aeruginosa, Neisseria gonorrhoeae, Salmonella enterica, and Streptococcus pneumoniae. If we had known what we know now regarding the pharmacokinetics and pharmacodynamics parameters of these antimicrobials when they were first introduced, we may have been able to prevent or slow the emergence of resistance by more appropriate use, especially with regards to agriculture. The approval of trovafloxacin by the Food and Drug Administration (FDA) in 1998 was met with great excitement by many clinicians based on its utility as monotherapy for numerous indications. In comparison with other available fluoroquinolones, trovafloxacin offered enhanced activity against anaerobic and Gram-positive organisms. In June, 1999 the FDA made a formal statement outlining recommendations for the cautious use of trovafloxacin in specific patient populations. Postmarketing experience revealed several cases of liver x Preface toxicity associated with the use of trovafloxacin, although similar findings had not been documented in earlier studies. The experience magnified the limita tions of information gained through clinical trials. Finally, we have seen the introduction of a number of new fluoroquinolones during the last 5 years. However, most of the clinical trials have been designed for equivalency and have included comparator agents in other classes. There are few studies which have been able to define the most optimal clinical indi cation for each of these agents. The new fluoroquinolones should currently rarely be prescribed as first-line agents and should always be employed judiciously. Inappropriate use of agents from this important class of antibiotics will likely worsen current problems with fluoroquinolone resistance. Allan R. Ronald Donald E. Low August 2002