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Published in: Annals of Intensive Care 1/2018

Open Access 01-12-2018 | Research

Pharmacogenomic biomarkers do not predict response to drotrecogin alfa in patients with severe sepsis

Authors: Djillali Annane, Jean-Paul Mira, Lorraine B. Ware, Anthony C. Gordon, Charles J. Hinds, David C. Christiani, Jonathan Sevransky, Kathleen Barnes, Timothy G. Buchman, Patrick J. Heagerty, Robert Balshaw, Nadia Lesnikova, Karen de Nobrega, Hugh F. Wellman, Mauricio Neira, Alexandra D. J. Mancini, Keith R. Walley, James A. Russell

Published in: Annals of Intensive Care | Issue 1/2018

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Abstract

Purpose

To explore potential design for pharmacogenomics trials in sepsis, we investigate the interaction between pharmacogenomic biomarkers and response to drotrecogin alfa (activated) (DrotAA). This trial was designed to validate whether previously identified improved response polymorphisms (IRPs A and B) were associated with an improved response to DrotAA in severe sepsis.

Methods

Patients with severe sepsis at high risk of death, who received DrotAA or not, with DNA available were included and matched to controls adjusting for age, APACHE II or SAPS II, organ dysfunction, ventilation, medical/surgical status, infection site, and propensity score (probability that a patient would have received DrotAA given their baseline characteristics). Independent genotyping and two-phase data transfer mitigated bias. The primary analysis compared the effect of DrotAA in IRP+ and IRP− groups on in-hospital 28-day mortality. Secondary endpoints included time to death in hospital; intensive care unit (ICU)-, hospital-, and ventilator-free days; and overall DrotAA treatment effect on mortality.

Results

Six hundred and ninety-two patients treated with DrotAA were successfully matched to 1935 patients not treated with DrotAA. Genotyping was successful for 639 (DrotAA) and 1684 (nonDrotAA) matched patients. The primary hypothesis of a genotype-by-treatment interaction (assessed by conditional logistic regression analysis) was not significant (P = 0.30 IRP A; P = 0.78 IRP B), and there was no significant genotype by treatment interaction for any secondary endpoint.

Conclusions

Neither IRP A nor IRP B predicted differential response to DrotAA on in-hospital 28-day mortality.
ClinicalTrials.gov registration NCT01486524
Appendix
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Metadata
Title
Pharmacogenomic biomarkers do not predict response to drotrecogin alfa in patients with severe sepsis
Authors
Djillali Annane
Jean-Paul Mira
Lorraine B. Ware
Anthony C. Gordon
Charles J. Hinds
David C. Christiani
Jonathan Sevransky
Kathleen Barnes
Timothy G. Buchman
Patrick J. Heagerty
Robert Balshaw
Nadia Lesnikova
Karen de Nobrega
Hugh F. Wellman
Mauricio Neira
Alexandra D. J. Mancini
Keith R. Walley
James A. Russell
Publication date
01-12-2018
Publisher
Springer International Publishing
Published in
Annals of Intensive Care / Issue 1/2018
Electronic ISSN: 2110-5820
DOI
https://doi.org/10.1186/s13613-018-0353-2

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