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Application of structured statistical analyses to identify a biomarker predictive of enhanced tralokinumab efficacy in phase III clinical trials for severe, uncontrolled asthma
by
Huhn, Monika
, Lipkovich, Ilya
, Bowen, Karin
, Colice, Gene
, Gottlow, Mattis
, Svensson, David J.
, Wessman, Peter
in
Adolescent
/ Adult
/ Aged
/ Algorithms
/ Anti-Asthmatic Agents - therapeutic use
/ Antibodies
/ Antibodies, Monoclonal - therapeutic use
/ Asthma
/ Asthma - drug therapy
/ Asthma and allergic disorders
/ Biological markers
/ Biomarkers - analysis
/ Cell Adhesion Molecules - blood
/ Child
/ Clinical trials
/ Critical Care Medicine
/ Disease Progression
/ Double-Blind Method
/ Drug therapy
/ Eosinophils - cytology
/ Exhalation
/ Female
/ Health aspects
/ Humans
/ Identification and classification
/ IL-13
/ Immunoglobulin E
/ Immunoglobulin E - blood
/ Immunoglobulins
/ Intensive
/ Interleukins
/ Internal Medicine
/ Male
/ Medicine
/ Medicine & Public Health
/ Methods
/ Middle Aged
/ Monoclonal antibodies
/ Nitric oxide
/ Nitric Oxide - analysis
/ Nitrogen oxides
/ Pharmacological research
/ Physiological aspects
/ Pneumology/Respiratory System
/ Predictive biomarker
/ Predictive Value of Tests
/ Severity of Illness Index
/ SIDES (subgroup identification based on differential effect search)
/ Statistics (Mathematics)
/ STRATOS 1
/ STRATOS 2
/ Technical Advance
/ Testing
/ Treatment Outcome
/ Young Adult
2019
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Application of structured statistical analyses to identify a biomarker predictive of enhanced tralokinumab efficacy in phase III clinical trials for severe, uncontrolled asthma
by
Huhn, Monika
, Lipkovich, Ilya
, Bowen, Karin
, Colice, Gene
, Gottlow, Mattis
, Svensson, David J.
, Wessman, Peter
in
Adolescent
/ Adult
/ Aged
/ Algorithms
/ Anti-Asthmatic Agents - therapeutic use
/ Antibodies
/ Antibodies, Monoclonal - therapeutic use
/ Asthma
/ Asthma - drug therapy
/ Asthma and allergic disorders
/ Biological markers
/ Biomarkers - analysis
/ Cell Adhesion Molecules - blood
/ Child
/ Clinical trials
/ Critical Care Medicine
/ Disease Progression
/ Double-Blind Method
/ Drug therapy
/ Eosinophils - cytology
/ Exhalation
/ Female
/ Health aspects
/ Humans
/ Identification and classification
/ IL-13
/ Immunoglobulin E
/ Immunoglobulin E - blood
/ Immunoglobulins
/ Intensive
/ Interleukins
/ Internal Medicine
/ Male
/ Medicine
/ Medicine & Public Health
/ Methods
/ Middle Aged
/ Monoclonal antibodies
/ Nitric oxide
/ Nitric Oxide - analysis
/ Nitrogen oxides
/ Pharmacological research
/ Physiological aspects
/ Pneumology/Respiratory System
/ Predictive biomarker
/ Predictive Value of Tests
/ Severity of Illness Index
/ SIDES (subgroup identification based on differential effect search)
/ Statistics (Mathematics)
/ STRATOS 1
/ STRATOS 2
/ Technical Advance
/ Testing
/ Treatment Outcome
/ Young Adult
2019
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Application of structured statistical analyses to identify a biomarker predictive of enhanced tralokinumab efficacy in phase III clinical trials for severe, uncontrolled asthma
by
Huhn, Monika
, Lipkovich, Ilya
, Bowen, Karin
, Colice, Gene
, Gottlow, Mattis
, Svensson, David J.
, Wessman, Peter
in
Adolescent
/ Adult
/ Aged
/ Algorithms
/ Anti-Asthmatic Agents - therapeutic use
/ Antibodies
/ Antibodies, Monoclonal - therapeutic use
/ Asthma
/ Asthma - drug therapy
/ Asthma and allergic disorders
/ Biological markers
/ Biomarkers - analysis
/ Cell Adhesion Molecules - blood
/ Child
/ Clinical trials
/ Critical Care Medicine
/ Disease Progression
/ Double-Blind Method
/ Drug therapy
/ Eosinophils - cytology
/ Exhalation
/ Female
/ Health aspects
/ Humans
/ Identification and classification
/ IL-13
/ Immunoglobulin E
/ Immunoglobulin E - blood
/ Immunoglobulins
/ Intensive
/ Interleukins
/ Internal Medicine
/ Male
/ Medicine
/ Medicine & Public Health
/ Methods
/ Middle Aged
/ Monoclonal antibodies
/ Nitric oxide
/ Nitric Oxide - analysis
/ Nitrogen oxides
/ Pharmacological research
/ Physiological aspects
/ Pneumology/Respiratory System
/ Predictive biomarker
/ Predictive Value of Tests
/ Severity of Illness Index
/ SIDES (subgroup identification based on differential effect search)
/ Statistics (Mathematics)
/ STRATOS 1
/ STRATOS 2
/ Technical Advance
/ Testing
/ Treatment Outcome
/ Young Adult
2019
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Application of structured statistical analyses to identify a biomarker predictive of enhanced tralokinumab efficacy in phase III clinical trials for severe, uncontrolled asthma
Journal Article
Application of structured statistical analyses to identify a biomarker predictive of enhanced tralokinumab efficacy in phase III clinical trials for severe, uncontrolled asthma
2019
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Overview
Background
Tralokinumab is an anti–interleukin (IL)-13 monoclonal antibody investigated for the treatment of severe, uncontrolled asthma in two Phase III clinical trials, STRATOS 1 and 2. The STRATOS 1 biomarker analysis plan was developed to identify biomarker(s) indicative of IL-13 activation likely to predict tralokinumab efficacy and define a population in which there was an enhanced treatment effect; this defined population was then tested in STRATOS 2.
Methods
The biomarkers considered were blood eosinophil counts, fractional exhaled nitric oxide (FeNO), serum dipeptidyl peptidase-4, serum periostin and total serum immunoglobulin E. Tralokinumab efficacy was measured as the reduction in annualised asthma exacerbation rate (AAER) compared with placebo (primary endpoint measure of STRATOS 1 and 2). The biomarker analysis plan included negative binomial and generalised additive models, and the Subgroup Identification based on Differential Effect Search (SIDES) algorithm, supported by robustness and sensitivity checks. Effects on the key secondary endpoints of STRATOS 1 and 2, which included changes from baseline in standard measures of asthma outcomes, were also investigated. Prior to the STRATOS 1 read-out, numerous simulations of the methodology were performed with hypothetical data.
Results
FeNO and periostin were identified as the only biomarkers potentially predictive of treatment effect, with cut-offs chosen by the SIDES algorithm of > 32.3 ppb and > 27.4 ng/ml, respectively. The FeNO > 32.3 ppb subgroup was associated with greater AAER reductions and improvements in key secondary endpoints compared with the periostin > 27.4 ng/ml subgroup. Upon further evaluation of AAER reductions at different FeNO cut-offs, ≥37 ppb was chosen as the best cut-off for predicting tralokinumab efficacy.
Discussion
A rigorous statistical approach incorporating multiple methods was used to investigate the predictive properties of five potential biomarkers and to identify a participant subgroup that demonstrated an enhanced tralokinumab treatment effect. Using STRATOS 1 data, our analyses identified FeNO at a cut-off of ≥37 ppb as the best assessed biomarker for predicting enhanced treatment effect to be tested in STRATOS 2. Our findings were inconclusive, which reflects the complexity of subgroup identification in the severe asthma population.
Trial registration
STRATOS 1 and 2 are registered on ClinicalTrials.gov (
NCT02161757
registered on June 12, 2014, and
NCT02194699
registered on July 18, 2014).
Publisher
BioMed Central,BioMed Central Ltd,BMC
Subject
/ Adult
/ Aged
/ Anti-Asthmatic Agents - therapeutic use
/ Antibodies, Monoclonal - therapeutic use
/ Asthma
/ Asthma and allergic disorders
/ Cell Adhesion Molecules - blood
/ Child
/ Female
/ Humans
/ Identification and classification
/ IL-13
/ Male
/ Medicine
/ Methods
/ Pneumology/Respiratory System
/ SIDES (subgroup identification based on differential effect search)
/ Testing
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