Association of C-reactive protein and metabolic risk with cognitive effects of lurasidone in patients with schizophrenia

Brian J. Miller; Andrei Pikalov; Cynthia O. Siu; Michael Tocco; Joyce Tsai; Philip D. Harvey; John W. Newcomer; Antony Loebel

Comprehensive Psychiatry (Oct 2020)

Association of C-reactive protein and metabolic risk with cognitive effects of lurasidone in patients with schizophrenia

Brian J. Miller,
Andrei Pikalov,
Cynthia O. Siu,
Michael Tocco,
Joyce Tsai,
Philip D. Harvey,
John W. Newcomer,
Antony Loebel

Affiliations

Brian J. Miller: Department of Psychiatry and Health Behavior, Augusta University, Augusta, GA, United States of America; Corresponding author at: Augusta University, Department of Psychiatry, 997 St. Sebastian Way, Augusta, GA 30912, United States of America.
Andrei Pikalov: Sunovion Pharmaceuticals Inc., Marlborough, MA and Fort Lee, NJ, United States of America
Cynthia O. Siu: COS and Associates Ltd., Central, Hong Kong
Michael Tocco: Sunovion Pharmaceuticals Inc., Marlborough, MA and Fort Lee, NJ, United States of America
Joyce Tsai: Sunovion Pharmaceuticals Inc., Marlborough, MA and Fort Lee, NJ, United States of America
Philip D. Harvey: University of Miami Miller School of Medicine, Miami, FL, United States of America
John W. Newcomer: Thriving Mind South Florida, Miami, FL, United States of America; Washington University School of Medicine, St. Louis, MO, United States of America
Antony Loebel: Sunovion Pharmaceuticals Inc., Marlborough, MA and Fort Lee, NJ, United States of America

Journal volume & issue: Vol. 102
p. 152195

Abstract

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Background: Accumulating evidence has implicated insulin resistance and inflammation in the pathophysiology of cognitive impairments associated with neuropsychiatric disorders. This post-hoc analysis based on a placebo-controlled trial investigated the effect of inflammation (indexed by CRP) and metabolic risk factors on cognitive performance in patients with schizophrenia treated with lurasidone. Methods: Acutely exacerbated patients with schizophrenia were randomized to lurasidone (80 or 160 mg/day), quetiapine XR 600 mg/day, or placebo. A wide range CRP test and a cognitive assessment using the CogState computerized battery were performed at baseline and week 6 study endpoint. Associations between log-transformed CRP, high density lipoprotein (HDL), homeostatic model assessment of insulin resistance (HOMA-IR) and treatment response were evaluated. Results: CRP combined with HDL, triglyceride-to-HDL (TG/HDL) ratio, or HOMA-IR at study baseline were significant moderators of the improvement in cognitive performance associated with lurasidone 160 mg/day (vs. placebo) treatment (p < .05). Greater placebo-corrected treatment effect size on the CogState composite score was observed for patients in the lurasidone 160 mg/day treatment group who had either low CRP and high HDL (d = 0.43), or low CRP and low HOMA-IR (d = 0.46). Interactive relationships between CRP, HDL, TG/HDL, HOMA-IR and the antipsychotic efficacy of lurasidone or quetiapine XR were not significant. There were no significant associations between antipsychotic treatment and changes in CRP level at study endpoint. Conclusions: Findings of this post-hoc analysis based on a placebo-controlled trial in patients with schizophrenia suggest that baseline CRP level combined with measures of metabolic risk significantly moderated the improvement in cognitive performance associated with lurasidone 160 mg/day (vs. placebo) treatment. Our findings underscore the importance of maintaining a low metabolic risk profile in patients with schizophrenia.

Published in Comprehensive Psychiatry

ISSN: 0010-440X (Print); 1532-8384 (Online)
Publisher: Elsevier
Country of publisher: United States
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry: Neurology. Diseases of the nervous system: Psychiatry
Website: https://www.journals.elsevier.com/comprehensive-psychiatry

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