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J.J. Tomasik (Jakub), E. Schwarz (Emanuel), S.G. Lago (Santiago G.), M. Rothermundt (Matthias), F.M. Leweke (Marcus), N.J.M. van Beveren (Nico), P.C. Guest (Paul), H. Rahmoune (Hassan), J. Steiner (Johann) and S. Bahn (Sabine)

2016-02-01

Pretreatment levels of the fatty acid handling proteins H-FABP and CD36 predict response to olanzapine in recent-onset schizophrenia patients

Publication

Publication

Brain, Behavior, and Immunity , Volume 52 p. 178- 186

Traditional schizophrenia pharmacotherapy remains a subjective trial and error process involving administration, titration and switching of drugs multiple times until an adequate response is achieved. Despite this time-consuming and costly process, not all patients show an adequate response to treatment. As a consequence, relapse is a common occurrence and early intervention is hampered. Here, we have attempted to identify candidate blood biomarkers associated with drug response in 121 initially antipsychotic-free recent-onset schizophrenia patients treated with widely-used antipsychotics, namely olanzapine (. n=. 40), quetiapine (. n=. 23), risperidone (. n=. 30) and a mixture of these drugs (. n=. 28). Patients were recruited and investigated as two separate cohorts to allow biomarker validation. Data analysis showed the most significant relationship between pre-treatment levels of heart-type fatty acid binding protein (H-FABP) and response to olanzapine (. p=. 0.008, F=. 8.6, β=. 70.4 in the discovery cohort and p=. 0.003, F=. 15.2, β=. 24.4 in the validation cohort, adjusted for relevant confounding variables). In a functional follow-up analysis of this finding, we tested an independent cohort of 10 patients treated with olanzapine and found that baseline levels of plasma H-FABP and expression of the binding partner for H-FABP, fatty acid translocase (CD36), on monocytes predicted the reduction of psychotic symptoms (. p=. 0.040, F=. 6.0, β=. 116.3 and p=. 0.012, F=. 11.9, β=. -0.0054, respectively). We also identified a set of serum molecules changed after treatment with antipsychotic medication, in particular olanzapine. These molecules are predominantly involved in cellular development and metabolism. Taken together, our findings suggest an association between biomarkers involved in fatty acid metabolism and response to olanzapine, while other proteins may serve as surrogate markers associated with drug efficacy and side effects.

Additional Metadata
Keywords Biomarker, CD36, FABP3, Olanzapine, Personalised medicine, Schizophrenia
Persistent URL doi.org/10.1016/j.bbi.2015.10.019, hdl.handle.net/1765/90965
Journal Brain, Behavior, and Immunity
Grant This work was funded by the European Commission 7th Framework Programme; grant id fp7/223427 - Developing minimally invasive, tools and technologies for high throughput, low cost molecular assays for the early diagnosis of schizophrenia and other psychiatric disorders (SCHIZDX), This work was funded by the European Commission 7th Framework Programme; grant id fp7/286334 - Advanced Immuno-neuro-endocrine Diagnostics in Psychiatry (PSYCH-AID)
Organisation Department of Neuroscience
Citation
Tomasik, J., Schwarz, E., Lago, S. G., Rothermundt, M., Leweke, M., van Beveren, N., … Bahn, S. (2016). Pretreatment levels of the fatty acid handling proteins H-FABP and CD36 predict response to olanzapine in recent-onset schizophrenia patients. Brain, Behavior, and Immunity, 52, 178–186. doi:10.1016/j.bbi.2015.10.019
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