FOCUS 1: A randomized, double-blinded, multicentre, phase III trial of the efficacy and safety of ceftaroline fosamil versus ceftriaxone in community-acquired pneumonia

File T.M.; Low D.E.; Eckburg P.B.; Talbot G.H.; Friedland H.D.; Lee J.; Llorens L.; Critchley I.A.; Thye D.A.; Pullman J.; Giordano P.; Welker J.; Manos P.; Mehra P.; De Santo J.; Venkateswaralu B.; Gerald Schrock C.; Tillis W.; Winetz J.A.; Gonzalez J.M.; Ramage A.; Eisenhower D.D.; Koegelenberg C.; Engelbrecht I.; Jurgens J.; Mitha I.; Breedt J.; Gani M.; Roos J.; Basson M.; Van Zyl L.; Meeding R.; Fulat M.; Le Roux M.; Bonvehi P.E.; Ganaha M.C.; Gurini A.L.; Daniel Lopardo G.; Cristina L.; Edwardo Prieto S.; Rodiguez C.G.; Augusto Teijeiro R.; Carmen Pallone E.; Pryluka D.H.; da Cunha C.A.; da Silva N.B.; de Faria Freire A.T.; Ferreira Starling C.E.; Costa Fiterman J.; Góngora Rubio F.; Carlos Losso L.; Patelli M.; Souza Lima J.; Zimermann Teixeira P.J.; Carmo Moreira M.A.; Abreu de Oliveira J.C.; Roudas V.; Gamal E.A.; Leschenko I.; Rudnov V.A.; Yevdokimova A.G.; Vertkin A.L.; Ambalov Y.M.; Dvoryashina I.V.; Zilber E.; Khamitov R.F.; Galustyan A.N.; Reshetko O.V.; Senior V.A.; Grosan M.F.; Jimborean G.; Lupse M.; Aron G.; Olteanu D.; Puschita M.; Gavris C.; Tudorache V.M.; Youroukova V.; Petkova M.; Troshanova E.; Dzhabalyan M.; Kavtaradze G.; Makhviladze M.; Tabukashvili R.; PONS CASELLAS, MARIA JESÚS; Garbino J.; Genne D.; Rothen M.; de Saracho J.O.; Capelastegui A.; Menendez R.; Torres A.; Shum C.; Falco V.; Bouza E.; Bru J.P.; Misset B.; Megarbane B.; Sollet J.P.; Molina J.M.

Title

Date Issued

01 April 2011

Access level

open access

Resource Type

journal article

Author(s)

File T.M.

Low D.E.

Eckburg P.B.

Talbot G.H.

Friedland H.D.

Lee J.

Llorens L.

Critchley I.A.

Thye D.A.

Pullman J.

Giordano P.

Welker J.

Manos P.

Mehra P.

De Santo J.

Venkateswaralu B.

Gerald Schrock C.

Tillis W.

Winetz J.A.

Gonzalez J.M.

Ramage A.

Eisenhower D.D.

Koegelenberg C.

Engelbrecht I.

Jurgens J.

Mitha I.

Breedt J.

Gani M.

Roos J.

Basson M.

Van Zyl L.

Meeding R.

Fulat M.

Le Roux M.

Bonvehi P.E.

Ganaha M.C.

Gurini A.L.

Daniel Lopardo G.

Cristina L.

Edwardo Prieto S.

Rodiguez C.G.

Augusto Teijeiro R.

Carmen Pallone E.

Pryluka D.H.

da Cunha C.A.

da Silva N.B.

de Faria Freire A.T.

Ferreira Starling C.E.

Costa Fiterman J.

Góngora Rubio F.

Carlos Losso L.

Patelli M.

Souza Lima J.

Zimermann Teixeira P.J.

Carmo Moreira M.A.

Abreu de Oliveira J.C.

Roudas V.

Gamal E.A.

Leschenko I.

Rudnov V.A.

Yevdokimova A.G.

Vertkin A.L.

Ambalov Y.M.

Dvoryashina I.V.

Zilber E.

Khamitov R.F.

Galustyan A.N.

Reshetko O.V.

Senior V.A.

Grosan M.F.

Jimborean G.

Lupse M.

Aron G.

Olteanu D.

Puschita M.

Gavris C.

Tudorache V.M.

Youroukova V.

Petkova M.

Troshanova E.

Dzhabalyan M.

Kavtaradze G.

Makhviladze M.

Tabukashvili R.

PONS CASELLAS, MARIA JESÚS

Garbino J.

Genne D.

Rothen M.

de Saracho J.O.

Capelastegui A.

Menendez R.

Torres A.

Shum C.

Falco V.

Bouza E.

Bru J.P.

Misset B.

Megarbane B.

Sollet J.P.

Molina J.M.

Publisher(s)

Oxford University Press

Abstract

Objectives: Ceftaroline, the active form of the prodrug ceftaroline fosamil, is a novel cephalosporin with bactericidal activity against important pathogens associated with community-acquired pneumonia (CAP), including Streptococcus pneumoniae and common Gram-negative pathogens. FOCUS 1 is a randomized, double-blinded, Phase III study that was conducted to evaluate the efficacy and safety of ceftaroline fosamil in treating patients with CAP. The primary objective was to determine non-inferiority [lower limit of 95% confidence interval (CI) ≥ -10%] in clinical cure rates achieved with ceftaroline fosamil compared with those achieved with ceftriaxone in the clinically evaluable (CE) and modified intent-to-treat efficacy (MITTE) populations. Methods: Patients hospitalized in a non-intensive care unit setting with CAP of Pneumonia Outcomes Research Team (PORT) risk class III or IV requiring intravenous (iv) therapy were randomized (1:1) to receive 600 mg of ceftaroline fosamil iv every 12 h or 1 g of ceftriaxone iv every 24 h. Patients also received two 500 mg doses of oral clarithromycin every 12 h administered on day 1. Clinical cure, microbiological response, adverse events (AEs) and laboratory tests were assessed. FOCUS 1 registration number NCT00621504 (http://clinicaltrials.gov/ct2/show/NCT00621504). Results: Of 613 enrolled patients, 298 received ceftaroline fosamil and 308 received ceftriaxone. Baseline characteristics between treatment groups were comparable. Clinical cure rates were as follows: CE population, 86.6% (194/224) for ceftaroline fosamil and 78.2% (183/234) for ceftriaxone [difference (95% CI), 8.4% (1.4, 15.4)]; and MITTE population, 83.8% (244/291) for ceftaroline fosamil and 77.7% (233/300) for ceftriaxone [difference (95% CI), 6.2% (-0.2, 12.6)]. Clinical cure rates for CAP caused by S. pneumoniae in the microbiological MITTE population were 88.9% (24/27) and 66.7% (20/30) for ceftaroline fosamil and ceftriaxone, respectively. Both agents were well tolerated, with similar rates of AEs, serious AEs, deaths and discontinuations because of an AE. The most common AEs for ceftaroline fosamil-treated patients were diarrhoea, headache, insomnia and nausea, and the most common AEs for ceftriaxone-treated patients were hypokalaemia, hypertension, nausea and diarrhoea. Conclusions: Ceftaroline fosamil demonstrated high clinical cure and microbiological response rates in hospitalized patients with CAP of PORT risk class III or IV. Ceftaroline fosamil was well tolerated, with a safety profile similar to that of ceftriaxone and consistent with the cephalosporin class. In this study, ceftaroline fosamil was an effective and well-tolerated treatment option for CAP. © The Author 2011. Published by Oxford University Press on behalf of the British Society for Antimicrobial Chemotherapy. All rights reserved.

Volume

66

Issue

SUPPL.3

Language

English

Subjects

DOI

10.1093/jac/dkr096

Scopus EID

2-s2.0-79954622500

PubMed ID

21482566

Source

Journal of Antimicrobial Chemotherapy

ISSN of the container

03057453

Sponsor(s)

Funding for the study was provided by Forest Laboratories, Inc. T. M. F. received recent research funding from Cerexa, Inc. (a wholly owned subsidiary of Forest Laboratories, Inc.), Ortho-McNeil, Pfizer, Boehringer-Ingelheim, Gilead and Tibotec. He is also a consultant for Bayer, Cerexa, Inc., GlaxoSmithKline, Ortho-McNeil, Protez/Novartis, Merck, Nabriva, Pfizer and Tetraphase. T. M. F. did not receive payment for work on the manuscript. D. E. L. serves as a speaker for Forest Laboratories, Inc. and did not receive payment for work on the manuscript. G. H. T. was an employee of Cerexa, Inc. at the time the work was performed; his company Talbot Advisors LLC is currently a consultant to Cerexa, Inc., but it was not paid for the time G. H. T. spent on manuscript preparation. G. H. T. has an equity interest in Cerexa, Inc. P. B. E., H. D. F., J. L., L. L. and I. A. C. are employees of Cerexa, Inc. D. A. T. was an employee of Cerexa, Inc. at the time the work and analyses were performed. P. B. E., H. D. F., J. L., L. L., I. A. C. and D. A. T. hold stock/stock options in Cerexa, Inc. Pfizer Forest Laboratories Ortho-McNeil Gilead and Tibotec

Sources of information: Directorio de Producción Científica Scopus

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