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Effect of CSL112 (apolipoprotein A‐I human) on cholesterol efflux capacity in Japanese subjects: Findings from a phase I study and a cross‐study comparison
by
Michael A. Tortorici
, Penelope Dalitz
, Serge Korjian
, John Roberts
, Shinya Goto
, John Feaster
, Regina Clementi
, Bo Zheng
, Jolanta Airey
, Danielle Duffy
, C. Michael Gibson
in
Acute coronary syndromes
/ Analysis
/ Apolipoprotein A
/ Apolipoprotein A-I
/ Apolipoprotein A-I - pharmacokinetics
/ Apolipoproteins
/ Biological Transport
/ Biomarkers
/ Cardiac patients
/ Cardiovascular diseases
/ Cholesterol
/ Clinical trials
/ Double-Blind Method
/ Drug dosages
/ Ethnicity
/ Heart attacks
/ Humans
/ Lipoproteins
/ Lipoproteins, HDL
/ Metabolism
/ Mortality
/ Myocardial infarction
/ Pharmacodynamics
/ Pharmacokinetics
/ Placebos
/ Plasma
/ Public aspects of medicine
/ RA1-1270
/ RM1-950
/ Therapeutics. Pharmacology
2022
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Effect of CSL112 (apolipoprotein A‐I human) on cholesterol efflux capacity in Japanese subjects: Findings from a phase I study and a cross‐study comparison
by
Michael A. Tortorici
, Penelope Dalitz
, Serge Korjian
, John Roberts
, Shinya Goto
, John Feaster
, Regina Clementi
, Bo Zheng
, Jolanta Airey
, Danielle Duffy
, C. Michael Gibson
in
Acute coronary syndromes
/ Analysis
/ Apolipoprotein A
/ Apolipoprotein A-I
/ Apolipoprotein A-I - pharmacokinetics
/ Apolipoproteins
/ Biological Transport
/ Biomarkers
/ Cardiac patients
/ Cardiovascular diseases
/ Cholesterol
/ Clinical trials
/ Double-Blind Method
/ Drug dosages
/ Ethnicity
/ Heart attacks
/ Humans
/ Lipoproteins
/ Lipoproteins, HDL
/ Metabolism
/ Mortality
/ Myocardial infarction
/ Pharmacodynamics
/ Pharmacokinetics
/ Placebos
/ Plasma
/ Public aspects of medicine
/ RA1-1270
/ RM1-950
/ Therapeutics. Pharmacology
2022
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Do you wish to request the book?
Effect of CSL112 (apolipoprotein A‐I human) on cholesterol efflux capacity in Japanese subjects: Findings from a phase I study and a cross‐study comparison
by
Michael A. Tortorici
, Penelope Dalitz
, Serge Korjian
, John Roberts
, Shinya Goto
, John Feaster
, Regina Clementi
, Bo Zheng
, Jolanta Airey
, Danielle Duffy
, C. Michael Gibson
in
Acute coronary syndromes
/ Analysis
/ Apolipoprotein A
/ Apolipoprotein A-I
/ Apolipoprotein A-I - pharmacokinetics
/ Apolipoproteins
/ Biological Transport
/ Biomarkers
/ Cardiac patients
/ Cardiovascular diseases
/ Cholesterol
/ Clinical trials
/ Double-Blind Method
/ Drug dosages
/ Ethnicity
/ Heart attacks
/ Humans
/ Lipoproteins
/ Lipoproteins, HDL
/ Metabolism
/ Mortality
/ Myocardial infarction
/ Pharmacodynamics
/ Pharmacokinetics
/ Placebos
/ Plasma
/ Public aspects of medicine
/ RA1-1270
/ RM1-950
/ Therapeutics. Pharmacology
2022
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Effect of CSL112 (apolipoprotein A‐I human) on cholesterol efflux capacity in Japanese subjects: Findings from a phase I study and a cross‐study comparison
Journal Article
Effect of CSL112 (apolipoprotein A‐I human) on cholesterol efflux capacity in Japanese subjects: Findings from a phase I study and a cross‐study comparison
2022
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Overview
CSL112 (apolipoprotein A‐I [apoA‐I, human]) is a novel drug in development to reduce the risk of recurrent cardiovascular events following acute myocardial infarction by increasing cholesterol efflux capacity (CEC). This phase I study aimed to compare the pharmacokinetics (PKs), pharmacodynamics (PDs), and safety of CSL112 in Japanese and White subjects. A total of 34 Japanese subjects were randomized to receive a single infusion of CSL112 (2, 4, or 6 g) or placebo and 18 White subjects were randomized to receive a single dose of 6 g CSL112 or placebo, followed by PK/PD assessment and adverse events monitoring. In addition, PK/PD parameters were compared across the CSL112 clinical development program. Plasma exposure of apoA‐I increased in a dose‐dependent but nonlinear manner in Japanese subjects receiving a single dose of CSL112. Mean baseline‐corrected area under the curve from 0 to 72 h (AUC0–72) increased from 840 to 6490 mg h/dl, in the 2 and 6 g cohorts, respectively, followed by dose‐dependent increase of CEC. The plasma PK profile of apoA‐I and increases in total and ATP binding cassette transporter A1 dependent CEC were comparable in Japanese and White subjects. The geometric mean ratio (Japanese:White) for plasma apoA‐I AUC0–72 and maximum plasma concentration (Cmax) was 1.08 and 0.945, respectively. Cross‐study comparison analysis demonstrated similar CSL112 exposure and CEC enhancement in Japanese and non‐Japanese subjects (including patients with cardiovascular disease) and further confirmed consistent PKs/PDs of CSL112. This study suggests CSL112 acutely enhances CEC and is well‐tolerated with no differences between Japanese and White subjects.
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