Telavancin versus vancomycin for hospital-acquired pneumonia due to gram-positive pathogens

Ethan Rubinstein; Tahaniyat Lalani; G. Ralph Corey; Zeina A. Kanafani; Esteban C. Nannini; Marcelo G. Rocha; Galia Rahav; Michael S. Niederman; Marin H. Kollef; Andrew F. Shorr; Patrick C. Lee; Arnold L. Lentnek; Carlos M. Luna; Jean Yves Fagon; Antoni Torres; Michael M. Kitt; Fredric C. Genter; Steven L. Barriere; H. David Friedland; Martin E. Stryjewski

doi:10.1093/cid/ciq031

Telavancin versus vancomycin for hospital-acquired pneumonia due to gram-positive pathogens

Ethan Rubinstein
, Tahaniyat Lalani
, G. Ralph Corey
, Zeina A. Kanafani
, Esteban C. Nannini
, Marcelo G. Rocha
, Galia Rahav
, Michael S. Niederman
, Marin H. Kollef
, Andrew F. Shorr
, Patrick C. Lee
, Arnold L. Lentnek
, Carlos M. Luna
, Jean Yves Fagon
, Antoni Torres
, Michael M. Kitt
, Fredric C. Genter
, Steven L. Barriere
, H. David Friedland
, Martin E. Stryjewski

نتاج البحث: نشر في مجلة › مقالة › مراجعة النظراء

241 اقتباسات (Scopus)

ملخص

Background: Telavancin is a lipoglycopeptide bactericidal against gram-positive pathogens. Methods: Two methodologically identical, double-blind studies (0015 and 0019) were conducted involving patients with hospital-acquired pneumonia (HAP) due to gram-positive pathogens, particularly methicillin-resistant Staphylococcus aureus (MRSA). Patients were randomized 1:1 to telavancin (10 mg/kg every 24 h) or vancomycin (1 g every 12 h) for 7-21 days. The primary end point was clinical response at follow-up/test-of-cure visit. Results: A total of 1503 patients were randomized and received study medication (the all-treated population). In the pooled alltreated population, cure rates with telavancin versus vancomycin were 58.9% versus 59.5% (95% confidence interval [CI] for the difference, -5.6% to 4.3%). In the pooled clinically evaluable population (n = 654), cure rates were 82.4% with telavancin and 80.7% with vancomycin (95% CI for the difference, -4.3% to 7.7%). Treatment with telavancin achieved higher cure rates in patients with monomicrobial S. aureus infection and comparable cure rates in patients with MRSA infection; in patients with mixed gram-positive/gram-negative infections, cure rates were higher in the vancomycin group. Incidence and types of adverse events were comparable between the treatment groups. Mortality rates for telavancin-treated versus vancomycin-treated patients were 21.5% versus 16.6% (95% CI for the difference, -0.7% to 10.6%) for study 0015 and 18.5% versus 20.6% (95% CI for the difference, -7.8% to 3.5%) for study 0019. Increases in serum creatinine level were more common in the telavancin group (16% vs 10%). Conclusions: The primary end point of the studies was met, indicating that telavancin is noninferior to vancomycin on the basis of clinical response in the treatment of HAP due to gram-positive pathogens.

اللغة الأصلية	الإنجليزيّة
الصفحات (من إلى)	31-40
عدد الصفحات	10
دورية	Clinical Infectious Diseases
مستوى الصوت	52
رقم الإصدار	1
المعرِّفات الرقمية للأشياء	https://doi.org/10.1093/cid/ciq031
حالة النشر	نُشِر - 1 يناير 2011
منشور خارجيًا	نعم

الوصول إلى المستند

10.1093/cid/ciq031

الملفات والروابط الأخرى

Link to publication in Scopus

قم بذكر هذا

Rubinstein, E., Lalani, T., Corey, G. R., Kanafani, Z. A., Nannini, E. C., Rocha, M. G., Rahav, G., Niederman, M. S., Kollef, M. H., Shorr, A. F., Lee, P. C., Lentnek, A. L., Luna, C. M., Fagon, J. Y., Torres, A., Kitt, M. M., Genter, F. C., Barriere, S. L., Friedland, H. D., & Stryjewski, M. E. (2011). Telavancin versus vancomycin for hospital-acquired pneumonia due to gram-positive pathogens. Clinical Infectious Diseases, 52(1), 31-40. https://doi.org/10.1093/cid/ciq031

@article{07fbdf1e3f0b4ce7a60e101b2486e804,

title = "Telavancin versus vancomycin for hospital-acquired pneumonia due to gram-positive pathogens",

abstract = "Background: Telavancin is a lipoglycopeptide bactericidal against gram-positive pathogens. Methods: Two methodologically identical, double-blind studies (0015 and 0019) were conducted involving patients with hospital-acquired pneumonia (HAP) due to gram-positive pathogens, particularly methicillin-resistant Staphylococcus aureus (MRSA). Patients were randomized 1:1 to telavancin (10 mg/kg every 24 h) or vancomycin (1 g every 12 h) for 7-21 days. The primary end point was clinical response at follow-up/test-of-cure visit. Results: A total of 1503 patients were randomized and received study medication (the all-treated population). In the pooled alltreated population, cure rates with telavancin versus vancomycin were 58.9\% versus 59.5\% (95\% confidence interval [CI] for the difference, -5.6\% to 4.3\%). In the pooled clinically evaluable population (n = 654), cure rates were 82.4\% with telavancin and 80.7\% with vancomycin (95\% CI for the difference, -4.3\% to 7.7\%). Treatment with telavancin achieved higher cure rates in patients with monomicrobial S. aureus infection and comparable cure rates in patients with MRSA infection; in patients with mixed gram-positive/gram-negative infections, cure rates were higher in the vancomycin group. Incidence and types of adverse events were comparable between the treatment groups. Mortality rates for telavancin-treated versus vancomycin-treated patients were 21.5\% versus 16.6\% (95\% CI for the difference, -0.7\% to 10.6\%) for study 0015 and 18.5\% versus 20.6\% (95\% CI for the difference, -7.8\% to 3.5\%) for study 0019. Increases in serum creatinine level were more common in the telavancin group (16\% vs 10\%). Conclusions: The primary end point of the studies was met, indicating that telavancin is noninferior to vancomycin on the basis of clinical response in the treatment of HAP due to gram-positive pathogens.",

author = "Ethan Rubinstein and Tahaniyat Lalani and Corey, \{G. Ralph\} and Kanafani, \{Zeina A.\} and Nannini, \{Esteban C.\} and Rocha, \{Marcelo G.\} and Galia Rahav and Niederman, \{Michael S.\} and Kollef, \{Marin H.\} and Shorr, \{Andrew F.\} and Lee, \{Patrick C.\} and Lentnek, \{Arnold L.\} and Luna, \{Carlos M.\} and Fagon, \{Jean Yves\} and Antoni Torres and Kitt, \{Michael M.\} and Genter, \{Fredric C.\} and Barriere, \{Steven L.\} and Friedland, \{H. David\} and Stryjewski, \{Martin E.\}",

note = "Funding Information: Manuscript preparation. Theravance, Inc. (South San Francisco) provided assistance with statistical analyses. Medical writing and editorial support was provided by Ivo Stoilov and Zeena Nackerdien, Envision Scientific Solutions, funded by Astellas Pharma Global Development, Inc. Funding Information: Potential conflicts of interest. E.R. has served as a consultant for Theravance, Inc., Astellas, Pfizer, Bayer, Wyeth, Merck, Atox, Ortho-Mc-Neill, and sanofi-aventis. G.R.C. has served as a consultant for Theravance, Inc.; has received support from Cubist Pharmaceuticals and Theravance, Inc.; and serves as a consultant for Cerexa, Merck, Pfizer, Cempra, and Astellas. E.C.N. received honoraria from Theravance, Inc. and research support from Astellas and Johnson \& Johnson. M.G.R. has received research support from Theravance, Inc., Hospira, Novartis, and Chiron for conducting clinical trials. G.R. has received a research grant from Pfizer. M.S.N. has served as a consultant and received honoraria from Pfizer, Merck, Astra-Zeneca, Johnson \& Johnson, Theravance, Inc., Schering-Plough, and Nektar and had received research support from Nektar and Pfizer. M.H.K. has received research support from Merck, Pfizer, and As-tellas. A.F.S. has either served as a consultant or investigator or has delivered promotional lectures for Astellas, Theravance, Inc., Pfizer, Merck, Johnson \& Johnson, Boehringer Ingelheim, GSK, sanofi-aventis, Canyon and Medicine Comp. P.L. has served as a consultant for Smiths Medical and received honoraria from Wyeth, King Pharmaceutical, and Adolor Corporation. A.L.L. has received research support from Ortho-McNeill, Cer-exa, Targanta, Optimer, and Theravance, Inc. and has received honoraria from Cubist Pharmaceuticals. C.M.L. has served as a consultant and received honoraria from Pfizer, Merck, Astra-Zeneca, and Bayer and has received independent research support from Pfizer. A.T. has served as a speaker for Astellas, Novartis, and Bayer and has research support from Pfizer. M.M.K. is a former employee of Theravance, Inc. F.C.G. is an employee of Theravance, Inc. S.L.B. is an employee of Theravance, Inc. H.D.F. is a former employee of Theravance, Inc. M.E.S. has served as a consultant for Theravance, Inc. and Trius Therapeutics, has received honoraria from Astellas, and received research support from Theravance, Inc.",

year = "2011",

month = jan,

day = "1",

doi = "10.1093/cid/ciq031",

language = "אנגלית",

volume = "52",

pages = "31--40",

number = "1",

}

Rubinstein, E, Lalani, T, Corey, GR, Kanafani, ZA, Nannini, EC, Rocha, MG, Rahav, G, Niederman, MS, Kollef, MH, Shorr, AF, Lee, PC, Lentnek, AL, Luna, CM, Fagon, JY, Torres, A, Kitt, MM, Genter, FC, Barriere, SL, Friedland, HD & Stryjewski, ME 2011, 'Telavancin versus vancomycin for hospital-acquired pneumonia due to gram-positive pathogens', Clinical Infectious Diseases, المجلد 52, رقم 1, الصفحات 31-40. https://doi.org/10.1093/cid/ciq031

TY - JOUR

T1 - Telavancin versus vancomycin for hospital-acquired pneumonia due to gram-positive pathogens

AU - Rubinstein, Ethan

AU - Lalani, Tahaniyat

AU - Corey, G. Ralph

AU - Kanafani, Zeina A.

AU - Nannini, Esteban C.

AU - Rocha, Marcelo G.

AU - Rahav, Galia

AU - Niederman, Michael S.

AU - Kollef, Marin H.

AU - Shorr, Andrew F.

AU - Lee, Patrick C.

AU - Lentnek, Arnold L.

AU - Luna, Carlos M.

AU - Fagon, Jean Yves

AU - Torres, Antoni

AU - Kitt, Michael M.

AU - Genter, Fredric C.

AU - Barriere, Steven L.

AU - Friedland, H. David

AU - Stryjewski, Martin E.

N1 - Funding Information: Manuscript preparation. Theravance, Inc. (South San Francisco) provided assistance with statistical analyses. Medical writing and editorial support was provided by Ivo Stoilov and Zeena Nackerdien, Envision Scientific Solutions, funded by Astellas Pharma Global Development, Inc. Funding Information: Potential conflicts of interest. E.R. has served as a consultant for Theravance, Inc., Astellas, Pfizer, Bayer, Wyeth, Merck, Atox, Ortho-Mc-Neill, and sanofi-aventis. G.R.C. has served as a consultant for Theravance, Inc.; has received support from Cubist Pharmaceuticals and Theravance, Inc.; and serves as a consultant for Cerexa, Merck, Pfizer, Cempra, and Astellas. E.C.N. received honoraria from Theravance, Inc. and research support from Astellas and Johnson & Johnson. M.G.R. has received research support from Theravance, Inc., Hospira, Novartis, and Chiron for conducting clinical trials. G.R. has received a research grant from Pfizer. M.S.N. has served as a consultant and received honoraria from Pfizer, Merck, Astra-Zeneca, Johnson & Johnson, Theravance, Inc., Schering-Plough, and Nektar and had received research support from Nektar and Pfizer. M.H.K. has received research support from Merck, Pfizer, and As-tellas. A.F.S. has either served as a consultant or investigator or has delivered promotional lectures for Astellas, Theravance, Inc., Pfizer, Merck, Johnson & Johnson, Boehringer Ingelheim, GSK, sanofi-aventis, Canyon and Medicine Comp. P.L. has served as a consultant for Smiths Medical and received honoraria from Wyeth, King Pharmaceutical, and Adolor Corporation. A.L.L. has received research support from Ortho-McNeill, Cer-exa, Targanta, Optimer, and Theravance, Inc. and has received honoraria from Cubist Pharmaceuticals. C.M.L. has served as a consultant and received honoraria from Pfizer, Merck, Astra-Zeneca, and Bayer and has received independent research support from Pfizer. A.T. has served as a speaker for Astellas, Novartis, and Bayer and has research support from Pfizer. M.M.K. is a former employee of Theravance, Inc. F.C.G. is an employee of Theravance, Inc. S.L.B. is an employee of Theravance, Inc. H.D.F. is a former employee of Theravance, Inc. M.E.S. has served as a consultant for Theravance, Inc. and Trius Therapeutics, has received honoraria from Astellas, and received research support from Theravance, Inc.

PY - 2011/1/1

Y1 - 2011/1/1

N2 - Background: Telavancin is a lipoglycopeptide bactericidal against gram-positive pathogens. Methods: Two methodologically identical, double-blind studies (0015 and 0019) were conducted involving patients with hospital-acquired pneumonia (HAP) due to gram-positive pathogens, particularly methicillin-resistant Staphylococcus aureus (MRSA). Patients were randomized 1:1 to telavancin (10 mg/kg every 24 h) or vancomycin (1 g every 12 h) for 7-21 days. The primary end point was clinical response at follow-up/test-of-cure visit. Results: A total of 1503 patients were randomized and received study medication (the all-treated population). In the pooled alltreated population, cure rates with telavancin versus vancomycin were 58.9% versus 59.5% (95% confidence interval [CI] for the difference, -5.6% to 4.3%). In the pooled clinically evaluable population (n = 654), cure rates were 82.4% with telavancin and 80.7% with vancomycin (95% CI for the difference, -4.3% to 7.7%). Treatment with telavancin achieved higher cure rates in patients with monomicrobial S. aureus infection and comparable cure rates in patients with MRSA infection; in patients with mixed gram-positive/gram-negative infections, cure rates were higher in the vancomycin group. Incidence and types of adverse events were comparable between the treatment groups. Mortality rates for telavancin-treated versus vancomycin-treated patients were 21.5% versus 16.6% (95% CI for the difference, -0.7% to 10.6%) for study 0015 and 18.5% versus 20.6% (95% CI for the difference, -7.8% to 3.5%) for study 0019. Increases in serum creatinine level were more common in the telavancin group (16% vs 10%). Conclusions: The primary end point of the studies was met, indicating that telavancin is noninferior to vancomycin on the basis of clinical response in the treatment of HAP due to gram-positive pathogens.

AB - Background: Telavancin is a lipoglycopeptide bactericidal against gram-positive pathogens. Methods: Two methodologically identical, double-blind studies (0015 and 0019) were conducted involving patients with hospital-acquired pneumonia (HAP) due to gram-positive pathogens, particularly methicillin-resistant Staphylococcus aureus (MRSA). Patients were randomized 1:1 to telavancin (10 mg/kg every 24 h) or vancomycin (1 g every 12 h) for 7-21 days. The primary end point was clinical response at follow-up/test-of-cure visit. Results: A total of 1503 patients were randomized and received study medication (the all-treated population). In the pooled alltreated population, cure rates with telavancin versus vancomycin were 58.9% versus 59.5% (95% confidence interval [CI] for the difference, -5.6% to 4.3%). In the pooled clinically evaluable population (n = 654), cure rates were 82.4% with telavancin and 80.7% with vancomycin (95% CI for the difference, -4.3% to 7.7%). Treatment with telavancin achieved higher cure rates in patients with monomicrobial S. aureus infection and comparable cure rates in patients with MRSA infection; in patients with mixed gram-positive/gram-negative infections, cure rates were higher in the vancomycin group. Incidence and types of adverse events were comparable between the treatment groups. Mortality rates for telavancin-treated versus vancomycin-treated patients were 21.5% versus 16.6% (95% CI for the difference, -0.7% to 10.6%) for study 0015 and 18.5% versus 20.6% (95% CI for the difference, -7.8% to 3.5%) for study 0019. Increases in serum creatinine level were more common in the telavancin group (16% vs 10%). Conclusions: The primary end point of the studies was met, indicating that telavancin is noninferior to vancomycin on the basis of clinical response in the treatment of HAP due to gram-positive pathogens.

UR - https://www.scopus.com/pages/publications/79951656334

U2 - 10.1093/cid/ciq031

DO - 10.1093/cid/ciq031

M3 - ???researchoutput.researchoutputtypes.contributiontojournal.article???

C2 - 21148517

AN - SCOPUS:79951656334

SN - 1058-4838

VL - 52

SP - 31

EP - 40

JO - Clinical Infectious Diseases

JF - Clinical Infectious Diseases

IS - 1

ER -

Telavancin versus vancomycin for hospital-acquired pneumonia due to gram-positive pathogens

ملخص

الوصول إلى المستند

الملفات والروابط الأخرى

بصمة

قم بذكر هذا