A randomized placebo-controlled phase II study of a Pseudomonas vaccine in ventilated ICU patients

Jordi Rello; Claus-Georg Krenn; Gottfried Locker; Ernst Pilger; Christian Madl; Laura Balica; Thierry Dugernier; Pierre-François Laterre; Herbert Spapen; Pieter Depuydt; Jean-Louis Vincent; Lajos Bogár; Zsuzsanna Szabó; Barbara Völgyes; Rafael Máñez; Nahit Çakar; Atilla Ramazanoglu; Arzu Topeli; Maria A. Mastruzzo; Abel Jasovich; Christian G. Remolif; Liliana del Carmen Soria; Max A. Andresen Hernandez; Carolina Ruiz Balart; Ildikó Krémer; Zsolt Molnár; Frank von Sonnenburg; Arthur Lyons; Michael Joannidis; Heinz Burgmann; Tobias Welte; Anton Klingler; Romana Hochreiter; Kerstin Westritschnig

doi:10.1186/s13054-017-1601-9

A randomized placebo-controlled phase II study of a Pseudomonas vaccine in ventilated ICU patients

Jordi Rello, Claus-Georg Krenn, Gottfried Locker, Ernst Pilger, Christian Madl, Laura Balica, Thierry Dugernier, Pierre-François Laterre, Herbert Spapen, Pieter Depuydt, Jean-Louis Vincent, Lajos Bogár, Zsuzsanna Szabó, Barbara Völgyes, Rafael Máñez, Nahit Çakar, Atilla Ramazanoglu, Arzu Topeli, Maria A. Mastruzzo, Abel JasovichChristian G. Remolif, Liliana del Carmen Soria, Max A. Andresen Hernandez, Carolina Ruiz Balart, Ildikó Krémer, Zsolt Molnár, Frank von Sonnenburg, Arthur Lyons, Michael Joannidis, Heinz Burgmann, Tobias Welte, Anton Klingler, Romana Hochreiter, Kerstin Westritschnig

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Resum

Currently, no vaccine against Pseudomonas is available. IC43 is a new, recombinant, protein (OprF/I)-based vaccine against the opportunistic pathogen, Pseudomonas aeruginosa, a major cause of serious hospital-acquired infections. IC43 has proven immunogenicity and tolerability in healthy volunteers, patients with burns, and patients with chronic lung diseases. In order to assess the immunogenicity and safety of IC43 in patients who are most at risk of acquiring Pseudomonas infections, it was evaluated in mechanically ventilated ICU patients. We conducted a randomized, placebo-controlled, partially blinded study in mechanically ventilated ICU patients. The immunogenicity of IC43 at day 14 was determined as the primary endpoint, and safety, efficacy against P. aeruginosa infections, and all-cause mortality were evaluated as secondary endpoints. Vaccinations (100 μg or 200 μg IC43 with adjuvant, or 100 μg IC43 without adjuvant, or placebo) were given twice in a 7-day interval and patients were followed up for 90 days. Higher OprF/I IgG antibody titers were seen at day 14 for all IC43 groups versus placebo (P < 0.0001). Seroconversion (≥4-fold increase in OprF/I IgG titer from days 0 to 14) was highest with 100 μg IC43 without adjuvant (80.6%). There were no significant differences in P. aeruginosa infection rates, with a low rate of invasive infections (pneumonia or bacteremia) in the IC43 groups (11.2-14.0%). Serious adverse events (SAEs) considered possibly related to therapy were reported by 2 patients (1.9%) in the group of 100 µg IC43 with adjuvant. Both SAEs resolved and no deaths were related to study treatment. Local tolerability symptoms were mild and rare (<5% of patients), a low rate of treatment-related treatment-emergent adverse events (3.1-10.6%) was observed in the IC43 groups. This phase II study has shown that IC43 vaccination of ventilated ICU patients produced a significant immunogenic effect. P. aeruginosa infection rates did not differ significantly between groups. In the absence of any difference in immune response following administration of 100 μg IC43 without adjuvant compared with 200 μg IC43 with adjuvant, the 100 μg dose without adjuvant was considered for further testing of its possible benefit of improved outcomes. There were no safety or mortality concerns. ClinicalTrials.gov, . Registered on 3 April 2009. The online version of this article (doi:10.1186/s13054-017-1601-9) contains supplementary material, which is available to authorized users.

Idioma original	Anglès
Revista	Critical Care
Volum	21
DOIs	https://doi.org/10.1186/s13054-017-1601-9
Estat de la publicació	Publicada - 2017

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10.1186/s13054-017-1601-9

https://ddd.uab.cat/record/186143

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https://www.scopus.com/pages/publications/85011385249

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Rello, J., Krenn, C.-G., Locker, G., Pilger, E., Madl, C., Balica, L., Dugernier, T., Laterre, P.-F., Spapen, H., Depuydt, P., Vincent, J.-L., Bogár, L., Szabó, Z., Völgyes, B., Máñez, R., Çakar, N., Ramazanoglu, A., Topeli, A., Mastruzzo, M. A., ... Westritschnig, K. (2017). A randomized placebo-controlled phase II study of a Pseudomonas vaccine in ventilated ICU patients. Critical Care, 21. https://doi.org/10.1186/s13054-017-1601-9

@article{e7d2108eb9c64de99e9f277c422ab680,

title = "A randomized placebo-controlled phase II study of a Pseudomonas vaccine in ventilated ICU patients",

abstract = "Currently, no vaccine against Pseudomonas is available. IC43 is a new, recombinant, protein (OprF/I)-based vaccine against the opportunistic pathogen, Pseudomonas aeruginosa, a major cause of serious hospital-acquired infections. IC43 has proven immunogenicity and tolerability in healthy volunteers, patients with burns, and patients with chronic lung diseases. In order to assess the immunogenicity and safety of IC43 in patients who are most at risk of acquiring Pseudomonas infections, it was evaluated in mechanically ventilated ICU patients. We conducted a randomized, placebo-controlled, partially blinded study in mechanically ventilated ICU patients. The immunogenicity of IC43 at day 14 was determined as the primary endpoint, and safety, efficacy against P. aeruginosa infections, and all-cause mortality were evaluated as secondary endpoints. Vaccinations (100 μg or 200 μg IC43 with adjuvant, or 100 μg IC43 without adjuvant, or placebo) were given twice in a 7-day interval and patients were followed up for 90 days. Higher OprF/I IgG antibody titers were seen at day 14 for all IC43 groups versus placebo (P < 0.0001). Seroconversion (≥4-fold increase in OprF/I IgG titer from days 0 to 14) was highest with 100 μg IC43 without adjuvant (80.6\%). There were no significant differences in P. aeruginosa infection rates, with a low rate of invasive infections (pneumonia or bacteremia) in the IC43 groups (11.2-14.0\%). Serious adverse events (SAEs) considered possibly related to therapy were reported by 2 patients (1.9\%) in the group of 100 µg IC43 with adjuvant. Both SAEs resolved and no deaths were related to study treatment. Local tolerability symptoms were mild and rare (<5\% of patients), a low rate of treatment-related treatment-emergent adverse events (3.1-10.6\%) was observed in the IC43 groups. This phase II study has shown that IC43 vaccination of ventilated ICU patients produced a significant immunogenic effect. P. aeruginosa infection rates did not differ significantly between groups. In the absence of any difference in immune response following administration of 100 μg IC43 without adjuvant compared with 200 μg IC43 with adjuvant, the 100 μg dose without adjuvant was considered for further testing of its possible benefit of improved outcomes. There were no safety or mortality concerns. ClinicalTrials.gov, . Registered on 3 April 2009. The online version of this article (doi:10.1186/s13054-017-1601-9) contains supplementary material, which is available to authorized users.",

keywords = "Pseudomonas aeruginosa, Vaccination, Immunity, Immunocompromised host, Bacterial infections, Mortality",

author = "Jordi Rello and Claus-Georg Krenn and Gottfried Locker and Ernst Pilger and Christian Madl and Laura Balica and Thierry Dugernier and Pierre-Fran{\c c}ois Laterre and Herbert Spapen and Pieter Depuydt and Jean-Louis Vincent and Lajos Bog{\'a}r and Zsuzsanna Szab{\'o} and Barbara V{\"o}lgyes and Rafael M{\'a}{\~n}ez and Nahit {\c C}akar and Atilla Ramazanoglu and Arzu Topeli and Mastruzzo, \{Maria A.\} and Abel Jasovich and Remolif, \{Christian G.\} and \{del Carmen Soria\}, Liliana and \{Andresen Hernandez\}, \{Max A.\} and \{Ruiz Balart\}, Carolina and Ildik{\'o} Kr{\'e}mer and Zsolt Moln{\'a}r and \{von Sonnenburg\}, Frank and Arthur Lyons and Michael Joannidis and Heinz Burgmann and Tobias Welte and Anton Klingler and Romana Hochreiter and Kerstin Westritschnig",

year = "2017",

doi = "10.1186/s13054-017-1601-9",

language = "English",

volume = "21",

}

Rello, J, Krenn, C-G, Locker, G, Pilger, E, Madl, C, Balica, L, Dugernier, T, Laterre, P-F, Spapen, H, Depuydt, P, Vincent, J-L, Bogár, L, Szabó, Z, Völgyes, B, Máñez, R, Çakar, N, Ramazanoglu, A, Topeli, A, Mastruzzo, MA, Jasovich, A, Remolif, CG, del Carmen Soria, L, Andresen Hernandez, MA, Ruiz Balart, C, Krémer, I, Molnár, Z, von Sonnenburg, F, Lyons, A, Joannidis, M, Burgmann, H, Welte, T, Klingler, A, Hochreiter, R & Westritschnig, K 2017, 'A randomized placebo-controlled phase II study of a Pseudomonas vaccine in ventilated ICU patients', Critical Care, vol. 21. https://doi.org/10.1186/s13054-017-1601-9

TY - JOUR

T1 - A randomized placebo-controlled phase II study of a Pseudomonas vaccine in ventilated ICU patients

AU - Rello, Jordi

AU - Krenn, Claus-Georg

AU - Locker, Gottfried

AU - Pilger, Ernst

AU - Madl, Christian

AU - Balica, Laura

AU - Dugernier, Thierry

AU - Laterre, Pierre-François

AU - Spapen, Herbert

AU - Depuydt, Pieter

AU - Vincent, Jean-Louis

AU - Bogár, Lajos

AU - Szabó, Zsuzsanna

AU - Völgyes, Barbara

AU - Máñez, Rafael

AU - Çakar, Nahit

AU - Ramazanoglu, Atilla

AU - Topeli, Arzu

AU - Mastruzzo, Maria A.

AU - Jasovich, Abel

AU - Remolif, Christian G.

AU - del Carmen Soria, Liliana

AU - Andresen Hernandez, Max A.

AU - Ruiz Balart, Carolina

AU - Krémer, Ildikó

AU - Molnár, Zsolt

AU - von Sonnenburg, Frank

AU - Lyons, Arthur

AU - Joannidis, Michael

AU - Burgmann, Heinz

AU - Welte, Tobias

AU - Klingler, Anton

AU - Hochreiter, Romana

AU - Westritschnig, Kerstin

PY - 2017

Y1 - 2017

N2 - Currently, no vaccine against Pseudomonas is available. IC43 is a new, recombinant, protein (OprF/I)-based vaccine against the opportunistic pathogen, Pseudomonas aeruginosa, a major cause of serious hospital-acquired infections. IC43 has proven immunogenicity and tolerability in healthy volunteers, patients with burns, and patients with chronic lung diseases. In order to assess the immunogenicity and safety of IC43 in patients who are most at risk of acquiring Pseudomonas infections, it was evaluated in mechanically ventilated ICU patients. We conducted a randomized, placebo-controlled, partially blinded study in mechanically ventilated ICU patients. The immunogenicity of IC43 at day 14 was determined as the primary endpoint, and safety, efficacy against P. aeruginosa infections, and all-cause mortality were evaluated as secondary endpoints. Vaccinations (100 μg or 200 μg IC43 with adjuvant, or 100 μg IC43 without adjuvant, or placebo) were given twice in a 7-day interval and patients were followed up for 90 days. Higher OprF/I IgG antibody titers were seen at day 14 for all IC43 groups versus placebo (P < 0.0001). Seroconversion (≥4-fold increase in OprF/I IgG titer from days 0 to 14) was highest with 100 μg IC43 without adjuvant (80.6%). There were no significant differences in P. aeruginosa infection rates, with a low rate of invasive infections (pneumonia or bacteremia) in the IC43 groups (11.2-14.0%). Serious adverse events (SAEs) considered possibly related to therapy were reported by 2 patients (1.9%) in the group of 100 µg IC43 with adjuvant. Both SAEs resolved and no deaths were related to study treatment. Local tolerability symptoms were mild and rare (<5% of patients), a low rate of treatment-related treatment-emergent adverse events (3.1-10.6%) was observed in the IC43 groups. This phase II study has shown that IC43 vaccination of ventilated ICU patients produced a significant immunogenic effect. P. aeruginosa infection rates did not differ significantly between groups. In the absence of any difference in immune response following administration of 100 μg IC43 without adjuvant compared with 200 μg IC43 with adjuvant, the 100 μg dose without adjuvant was considered for further testing of its possible benefit of improved outcomes. There were no safety or mortality concerns. ClinicalTrials.gov, . Registered on 3 April 2009. The online version of this article (doi:10.1186/s13054-017-1601-9) contains supplementary material, which is available to authorized users.

AB - Currently, no vaccine against Pseudomonas is available. IC43 is a new, recombinant, protein (OprF/I)-based vaccine against the opportunistic pathogen, Pseudomonas aeruginosa, a major cause of serious hospital-acquired infections. IC43 has proven immunogenicity and tolerability in healthy volunteers, patients with burns, and patients with chronic lung diseases. In order to assess the immunogenicity and safety of IC43 in patients who are most at risk of acquiring Pseudomonas infections, it was evaluated in mechanically ventilated ICU patients. We conducted a randomized, placebo-controlled, partially blinded study in mechanically ventilated ICU patients. The immunogenicity of IC43 at day 14 was determined as the primary endpoint, and safety, efficacy against P. aeruginosa infections, and all-cause mortality were evaluated as secondary endpoints. Vaccinations (100 μg or 200 μg IC43 with adjuvant, or 100 μg IC43 without adjuvant, or placebo) were given twice in a 7-day interval and patients were followed up for 90 days. Higher OprF/I IgG antibody titers were seen at day 14 for all IC43 groups versus placebo (P < 0.0001). Seroconversion (≥4-fold increase in OprF/I IgG titer from days 0 to 14) was highest with 100 μg IC43 without adjuvant (80.6%). There were no significant differences in P. aeruginosa infection rates, with a low rate of invasive infections (pneumonia or bacteremia) in the IC43 groups (11.2-14.0%). Serious adverse events (SAEs) considered possibly related to therapy were reported by 2 patients (1.9%) in the group of 100 µg IC43 with adjuvant. Both SAEs resolved and no deaths were related to study treatment. Local tolerability symptoms were mild and rare (<5% of patients), a low rate of treatment-related treatment-emergent adverse events (3.1-10.6%) was observed in the IC43 groups. This phase II study has shown that IC43 vaccination of ventilated ICU patients produced a significant immunogenic effect. P. aeruginosa infection rates did not differ significantly between groups. In the absence of any difference in immune response following administration of 100 μg IC43 without adjuvant compared with 200 μg IC43 with adjuvant, the 100 μg dose without adjuvant was considered for further testing of its possible benefit of improved outcomes. There were no safety or mortality concerns. ClinicalTrials.gov, . Registered on 3 April 2009. The online version of this article (doi:10.1186/s13054-017-1601-9) contains supplementary material, which is available to authorized users.

KW - Pseudomonas aeruginosa

KW - Vaccination

KW - Immunity

KW - Immunocompromised host

KW - Bacterial infections

KW - Mortality

UR - https://www.scopus.com/pages/publications/85011385249

U2 - 10.1186/s13054-017-1601-9

DO - 10.1186/s13054-017-1601-9

M3 - Article

C2 - 28159015

SN - 1466-609X

VL - 21

JO - Critical Care

JF - Critical Care

ER -

A randomized placebo-controlled phase II study of a Pseudomonas vaccine in ventilated ICU patients

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