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Protocol for a pharmacogenomic study on individualised antipsychotic drug treatment for patients with schizophrenia

Published online by Cambridge University Press:  29 June 2021

Yi Su Open the ORCID record for Yi Su [Opens in a new window] ,
Hao Yu Open the ORCID record for Hao Yu [Opens in a new window] ,
Zhiren Wang ,
Sha Liu ,
Liansheng Zhao ,
Yingmei Fu ,
Yongfeng Yang ,
Bo Du ,
Fuquan Zhang  and
Xiangrong Zhang
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Yi Su
Affiliation:
Institute of Mental Health, The Sixth Hospital of Peking University, China; and Key Laboratory of Mental Health, Ministry of Health & National Clinical Research Center for Mental Disorders (Peking University), China
Hao Yu
Affiliation:
Institute of Mental Health, The Sixth Hospital of Peking University, China; Key Laboratory of Mental Health, Ministry of Health & National Clinical Research Center for Mental Disorders (Peking University), China; and Department of Psychiatry, Jining Medical University, China
Zhiren Wang
Affiliation:
Psychiatry Research Center, Beijing HuiLongGuan Hospital, Peking University, China
Sha Liu
Affiliation:
Department of Psychiatry, First Hospital/First Clinical Medical College of Shanxi Medical University, China
Liansheng Zhao
Affiliation:
Mental Health Center, West China Hospital, Sichuan University, China
Yingmei Fu
Affiliation:
Shanghai Mental Health Center, Shanghai Jiaotong University, China
Yongfeng Yang
Affiliation:
Henan Mental Hospital, The Second Affiliated Hospital of Xinxiang Medical University, China
Bo Du
Affiliation:
Hebei Mental Health Center, The Sixth People's Hospital of Hebei Province, China
Fuquan Zhang
Affiliation:
Wuxi Mental Health Center, Nanjing Medical University, China
Xiangrong Zhang
Affiliation:
Department of Geriatric Psychiatry, Nanjing Brain Hospital Affiliated to Nanjing Medical University, China
Manli Huang
Affiliation:
Department of Psychiatry, The First Affiliated Hospital, Zhejiang University School of Medicine, China; and The Key Laboratory of Mental Disorder's Management of Zhejiang Province, China
Cailan Hou
Affiliation:
Guangdong Mental Health Center, Guangdong Provincial People's Hospital, Guangdong Academy of Medical Sciences, Guangzhou, Guangdong province, China; and School of Medicine, South China University of Technology, Guangzhou, Guangdong province, China
Guoping Huang
Affiliation:
Department of Psychiatry, Mental Health Center of Sichuan Province, China
Zhonghua Su
Affiliation:
Department of Psychiatry, Jining Mental Hospital, China
Mao Peng
Affiliation:
Department of Neurology, Xuanwu Hospital, Capital Medical University, China
Ran Yan
Affiliation:
Department of Radiology, China-Japan Friendship Hospital Affiliated to the Ministry of Health of PRC, China
Yuyanan Zhang
Affiliation:
Institute of Mental Health, The Sixth Hospital of Peking University, China; and Key Laboratory of Mental Health, Ministry of Health & National Clinical Research Center for Mental Disorders (Peking University), China
Hao Yan
Affiliation:
Institute of Mental Health, The Sixth Hospital of Peking University, China; and Key Laboratory of Mental Health, Ministry of Health & National Clinical Research Center for Mental Disorders (Peking University), China
Lifang Wang
Affiliation:
Institute of Mental Health, The Sixth Hospital of Peking University, China; and Key Laboratory of Mental Health, Ministry of Health & National Clinical Research Center for Mental Disorders (Peking University), China
Tianlan Lu
Affiliation:
Institute of Mental Health, The Sixth Hospital of Peking University, China; and Key Laboratory of Mental Health, Ministry of Health & National Clinical Research Center for Mental Disorders (Peking University), China
Fujun Jia
Affiliation:
Guangdong Mental Health Center, Guangdong General Hospital, China; and School of Medicine, South China University of Technology, Guangzhou, Guangdong province, China
Keqing Li
Affiliation:
Hebei Mental Health Center, The Sixth People's Hospital of Hebei Province, China
Luxian Lv
Affiliation:
Henan Mental Hospital, The Second Affiliated Hospital of Xinxiang Medical University, China
Hongxing Wang
Affiliation:
Department of Neurology, Xuanwu Hospital, Capital Medical University, China
Shunying Yu
Affiliation:
Shanghai Mental Health Center, Shanghai Jiaotong University, China
Qiang Wang
Affiliation:
Mental Health Center, West China Hospital, Sichuan University, China
Yunlong Tan
Affiliation:
HuiLongGuan Clinical Medical School, Beijing HuiLongGuan Hospital, Peking University, China
Yong Xu
Affiliation:
Department of Psychiatry, First Hospital/First Clinical Medical College of Shanxi Medical University, China
Dai Zhang
Affiliation:
Institute of Mental Health, The Sixth Hospital of Peking University, China; Key Laboratory of Mental Health, Ministry of Health & National Clinical Research Center for Mental Disorders (Peking University), China; and Peking-Tsinghua Joint Center for Life Sciences, IDG/McGovern Institute for Brain Research, Peking University, China
Weihua Yue*
Affiliation:
Institute of Mental Health, The Sixth Hospital of Peking University, China; and Key Laboratory of Mental Health, Ministry of Health & National Clinical Research Center for Mental Disorders (Peking University), China
*
Correspondence: Weihua Yue. Email: [email protected].
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Abstract

Background

Schizophrenia is a severe and complex psychiatric disorder that needs treatment based on extensive experience. Antipsychotic drugs have already become the cornerstone of the treatment for schizophrenia; however, the therapeutic effect is of significant variability among patients, and only around a third of patients with schizophrenia show good efficacy. Meanwhile, drug-induced metabolic syndrome and other side-effects significantly affect treatment adherence and prognosis. Therefore, strategies for drug selection are desperately needed. In this study, we will perform pharmacogenomics research and set up an individualised preferred treatment prediction model.

Aims

We aim to create a standard clinical cohort, with multidimensional index assessment of antipsychotic treatment for patients with schizophrenia.

Method

This trial is designed as a randomised clinical trial comparing treatment with different kinds of antipsychotics. A total sample of 2000 patients with schizophrenia will be recruited from in-patient units from five clinical research centres. Using a computer-generated program, the participants will be randomly assigned to four treatment groups: aripiprazole, olanzapine, quetiapine and risperidone. The primary outcomes will be measured as changes in the Positive and Negative Syndrome Scale of schizophrenia, which reflects the efficacy. Secondary outcomes include the measure of side-effects, such as metabolic syndromes. The efficacy evaluation and side-effects assessment will be performed at baseline, 2 weeks, 6 weeks and 3 months.

Results

This trial will assess the efficacy and side effects of antipsychotics and create a standard clinical cohort with a multi-dimensional index assessment of antipsychotic treatment for schizophrenia patients.

Conclusion

This study aims to set up an individualized preferred treatment prediction model through the genetic analysis of patients using different kinds of antipsychotics.

Keywords

Antipsychoticsclinical trialschizophreniadrug interactions and side-effectsgenetics
Type
Papers
Information
BJPsych Open , Volume 7 , Issue 4 , July 2021 , e121
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Creative Commons
Creative Common License - CCCreative Common License - BY
This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted re-use, distribution, and reproduction in any medium, provided the original work is properly cited.
Copyright
Copyright © The Author(s), 2021. Published by Cambridge University Press on behalf of the Royal College of Psychiatrists

Schizophrenia is a severe psychiatric disorder with high heritability and multigenic inheritance, affecting approximately 1% of the world population.Reference Thaker and Carpenter1 Antipsychotic drugs are the mainstay of acute and long-term schizophrenia treatment, but the treatment response and tolerability are highly variable.Reference Huber, Naber and Lambert2 There are high rates of treatment discontinuation because of efficacy and tolerability issues.Reference Lieberman3 First-generation antipsychotics are often accompanied by significant side-effects, including extrapyramidal symptoms and tardive dyskinesia. Second-generation antipsychotics are associated with a variety of metabolic side-effects, such as dyslipidaemia, elevated glucose levels and weight gain, and may cause clinical exacerbation or psychotic relapse, often resulting in hospital stays and placing great burden on patients and their families. Antipsychotics represent a considerable fraction of healthcare costs in most developed countries.Reference Jones, Barnes, Davies, Dunn, Lloyd and Hayhurst4,Reference Ilyas and Moncrieff5 A modest improvement in outcomes may provide great benefits for society. Therefore, it is important to individualise drug treatment to obtain an adequate effect and minimise side-effects.

Several twin and family studies suggest that the response to antipsychotic treatment is a heritable trait. Studies on monozygotic twins observed a similar response to treatment with antipsychotics and similar levels of antipsychotic-induced weight gain.Reference Horáček, Libiger, Höschl, Borzova and Hendrychová6,Reference Wehmeier, Gebhardt, Schmidtke, Remschmidt, Hebebrand and Theisen7 Given that schizophrenia has a high heritability, it is likely that there is a substantial genetic component to individual differences in treatment response.Reference Lichtenstein, Yip, Bjork, Pawitan, Cannon and Sullivan8,Reference Malhotra and Kennedy9

Pharmacogenetics research has focused on the identification of genetic variants contributing to individual variability regarding several antipsychotic-related phenotypes. In past decades, research has succeeded in identifying genetic variants associated with variability in antipsychotic treatment.Reference Lencz, Robinson, Xu, Ekholm, Sevy and Gunduz-Bruce10Reference Consoli, Lastella, Ciapparelli, Dell'Osso, Ciofi and Guidotti17 These studies focused on encoding drug targets (pharmacodynamic candidates) or involvement in the metabolism of the drug itself (pharmacokinetic candidates). In contrast to candidate gene-based methods, genome-wide association studies (GWAS) could identify candidate variants without introducing prior hypothesis bias. Several groups have performed GWAS to identify candidate biomarkers for treatment response and side-effects of antipsychotics. Currently, research has mainly used the genotyping data from the original Clinical Antipsychotic Trials of Intervention Effectiveness (CATIE) study, and focused on various phenotypes.

However, the vast majority of common variants associated with treatment response and side-effects of antipsychotics were identified only in the samples of European ancestry.Reference Åberg, Adkins, Bukszár, Webb, Caroff and Miller18Reference McClay, Adkins, Åberg, Stroup, Perkins and Vladimirov22 The associated variants identified in populations of European ancestry might not be significant in other ancestry groups, because of underlying genetic heterogeneity. Therefore, there is a need for larger studies on the Chinese Han population, and independent samples to verify if there is any common genetic mechanism at the treatment response of the cross-ethnic population.

Study objectives

There are three primary objectives of this study. First, we aim to create a standard clinical cohort with multidimensional index assessment of antipsychotic treatment for patients with schizophrenia, which can be dynamically monitored. Second, we aim to perform the genetic association analysis with the standard clinical cohort, to identify the risk factors and biomarkers of drug efficacy and side-effects. Finally, we will conduct further research on different antipsychotics, to construct a multidimensional evaluation index system for treatment with antipsychotics and set up an individualised prediction model to help drug selection and improve treatment efficacy, thereby reducing side-effects and improving long-term prognosis.

Method

Design and setting

The study on individualised optimal treatment for antipsychotic drugs is a parallel, double-blind, randomised, controlled multicentre study, conducted from July 2016 to December 2020. Patients will be enrolled from five research centres (the Sixth Hospital of Peking University, the First Hospital of Shanxi Medical University, Shanghai Mental Health Centre, West China Hospital of Sichuan University and Beijing HuiLongGuan Hospital), containing 15 hospitals (Capital Peking University Sixth Hospital, the First Hospital of Shanxi Medical University, Shanghai Mental Health Centre, West China Hospital of Sichuan University, Beijing HuiLongGuan Hospital, Medical University Xuanwu Hospital, Henan Psychiatric Hospital, Nanjing Brain Hospital, The First Affiliated Hospital of Medical School of Zhejiang University, Guangdong Mental Health Center, Hebei Mental Health Center, Wuxi Mental Health Center, Sichuan Mental Health Center, Jining Psychiatric Hospital, China-Japan Friendship Hospital), across China. Considering the importance of coherence, we have conducted five pieces of training for 104 psychiatrists in 15 hospitals, respectively. The training included research protocols, standard diagnostic criteria and other scales for the assessment of symptoms and side-effects, as well as videos for standardised scale assessments and blood sample collections.

We will perform several assessments of baseline status at the start of the study. Then, patients who meet the criterion will be randomly assigned (1:1:1:1) to four groups (aripiprazole, olanzapine, quetiapine and risperidone). Group assignment will be determined by a Microsoft Excel (Excel 2016 for Windows) randomisation generator, without any stratification factors. The random allocation sequence will be generated by a trained research assistant, and will be concealed until after the baseline assessments. In detail, 200 cases were taken as a block group, and the research participants were randomly grouped according to the block randomisation method. We generated the random numbers with the Microsoft Excel formula (ROUNDUP (RAND ()*10 000,0)) as integers between 0 and 9999. A patient ID is a five-digit number generated from the centre number and random number.

All of the researchers administering baseline and follow-up assessments will be masked to the group assignments of each participant. All of the patients will be followed for up to 3 months or until the treatment was discontinued for any reason. Figure 1 shows a schematic diagram of the study design.

Fig. 1 Flowchart of this study. CGI, Clinical Global Impressions Scale; PANSS, Positive and Negative Syndrome Scale.

The trial is designed to use a standard clinical cohort to find out the risk factors and biomarkers of efficacy and side-effects of different drugs, which can help us establish individualised preferred treatment prediction model.

Participants

We will enrol a sample of 2000 Chinese Han descents aged 18–45 years, who currently meet or have met the DSM-IV diagnostic criteria for schizophrenia or schizophreniform disorder based on the Structured Clinical Interview for DSM-IV, a review of their clinical records and input from available informants. The consensus diagnoses will be made by at least two experienced psychiatrists. Inclusion and exclusion criteria are listed in Tables 1 and 2. Informed consent will be obtained at the outset of the study. All participants will be asked to appoint a family member or close friend who is involved with the informed consent discussion and assists the patient with decision-making. The power analysis was performed by G*Power (version 3.1 for Windows, Heinrich Heine University Düsseldorf, Germany; see http://www.gpower.hhu.de/), and this sample size has achieved a power of 0.9.

Table 1 Inclusion criteria

Table 2 Exclusion criteria

Pharmacological treatments

All patients will receive 6-week monotherapy of four kinds of randomly assigned antipsychotic drugs (aripiprazole, olanzapine, quetiapine and risperidone). Clinicians can prescribe the drugs based on individual patients, therapeutic response and side-effect burden (risperidone 2–6 mg/d, olanzapine 5–20 mg/d, quetiapine 400–750 mg/d and aripiprazole 10–30 mg/d). Withdrawal of the original medication and dosage titration to the lowest therapeutic dose will occur within 1 week. According to patients’ adverse reactions and drug efficacy, clinicians may continue to adjust the dose within the first 2 weeks, but the scope should be within the prescribed dosage. After the first 2 weeks, the dosage should not change during the study period.

Concomitant medications

All participants will be maintained on the same antipsychotic medication throughout the entire study period, as medically feasible, with no introduction of new chronic therapies. Data will not be analysed from participants who make changes to the type of treatment they are receiving during the 6-week study period. However, data from participants who change the dose of their medication, without changing the type, will be analysed.

Other psychotropic medications, including antidepressants, anxiolytics and mood stabilisers, are not allowed during the study period. Patients who receive electroconvulsive therapy should be excluded. For 2 weeks before enrolment and throughout the study period, patients should not take drugs that will induce or inhibit drug-metabolising enzymes, such as rifampin, carbamazepine, phenobarbital and phenytoin. During the study, clinicians should minimise the use of aspirin and non-steroidal anti-inflammatory drugs. Patients who receive systemic psychotherapy will also be excluded.

In the following cases, after clinicians have confirmed the specific conditions, patients may receive combination medications. Patients with serious somnipathy may receive an intermittent short-term oral sedative-hypnotics of non-benzodiazepine and benzodiazepine medications in the evening (to include clonazepam, estazolam, lorazepam and others), but the duration of treatment should not exceed 14 days. When patients present with extrapyramidal symptoms, they may receive trihexyphenidyl according to the dosage instructions. If patients present with acute dystonia, they may be treated with scopolamine 0.3 mg each time, administered by intramuscular injection. If patients present with akathisia and tachycardia, they would be treated with beta-adrenoceptor blocking agents (such as propranolol and metoprolol). Treatment for somatic diseases may continue to be taken during the study period, but the dosage should preferably remain constant. General physical disease that occurs during the study may receive symptomatic treatment. When patients present with excitement or agitation symptoms, they may receive clonazepam (1–3 mg) by intramuscular injection. The daily dose should not exceed 6 mg, and the duration should not exceed more than a week. They may also be treated with oral lorazepam (1–2 mg) or clonazepam (1–2 mg); the daily dose should not exceed 6 mg and the duration should not exceed more than a week. To avoid affecting the outcomes, within 2 hours before each assessment, clinicians should prohibit the use of sedative-hypnotics or anti-Parkinsonian drugs.

Discontinuation of participants

Participants might be discontinued from the study during the study period. We will record the reasons for their discontinuation as follows: (a) patients who violate the rules of the research project (e.g. patients who use banned drugs during the study, or patients who do not complete the study according to the protocol); (b) patients who have severe adverse effects or drug reactions; (c) patients who show poor adherence; (d) patients who withdraw their informed consent; (e) women who become pregnant during the study; (f) patients who fail to attend follow-up appointments; (g) according to the condition of patient, a psychiatrist will judge whether the patient should continue to participate in the study and can suspend those who are no longer suitable for the study because of reasons such as a lack of efficacy or intolerability; and (h) other reasons.

Measurements

The participants should follow the schedule to attend the study visits for clinical examinations and to participate in the assessments (Table 3). Outcome measures are obtained from a variety of sources, including patient self-report, clinician ratings and ratings by trained study personnel.

Table 3 Study visit schedule

PANSS, Positive and Negative Syndrome Scale; CGI-S, Clinical Global Impressions Scale–Severity of Illness; UKU, Udvalg for Kliniske Under-sogelser Side-Effect Rating Scale; ECG, electrocardiogram.

Baseline measures

At baseline, participants should complete a form assessing demographic factors (e.g. gender, age, ethnicity, income, inhabiting information and education), symptoms and medical history. Participants will then go through the Structured Clinical Interview for DSM-IV-TR.Reference First, Spitzer, Gibbon and Williams23 The clinicians will also perform body and nervous system examination and monitor vital signs for patients. The Positive and Negative Syndrome Scale (PANSS)Reference Kay, Flszbein and Opfer24 and the Clinical Global Impressions Scale–Severity of Illness (CGI-S)Reference Busner and Targum25 will be used to assess symptom severity in all participants. Then, a series of examinations will be performed, including laboratory examination, electrocardiogram, plasma concentration, concomitant medications monitoring and adverse events records. Finally, a blood sample will be obtained and stored for genotyping.

Efficacy evaluation

The efficacy of the antipsychotics will be evaluated with the PANSS (major index) or CGI-S (minor index) scales. The 30 items of the PANSS measure a broad range of symptoms typical for schizophrenia.Reference Kay, Flszbein and Opfer24 The PANSS scores are labelled as positive, negative and general psychopathology subscale scores, along with the total symptom scores, which is the sum of the 30 items. The CGI-S rates the severity of schizophrenia symptoms on a scale from one to seven, with higher scores indicating greater severity of illness.Reference Guy26 All of the participants will receive these assessments at baseline, weeks 2 and 6, and the end of the third month (Table 3).

Side-effects and other assessments

Side-effects are assessed with the Udvalg for Kliniske Under-sogelser Side-Effect Rating Scale.Reference Simpson and Angus27Reference Munetz and Benjamin29 In addition, to evaluate the effect of antipsychotic treatments on weight gain, glucose and lipid metabolism, each participant's pulse, blood pressure, fasting blood glucose level, haemoglobin, lipid profile (total cholesterol, high-density lipoprotein cholesterol and triglycerides) and weight will be assessed at baseline, weeks 2 and 6, and the end of the third month. Beyond that, complete blood count and serum prolactin level will be collected according to the schedule of events (Table 3).

Genotyping and sequencing

Genomic DNA samples will be extracted with the QIAamp DNA Mini Kit (QIAGEN). Genotyping of samples will be conducted using the Illumina Global Screening Array (Illumina, San Diego, CA), which was designed to include a core imputation backbone (approximately 660 000 markers) and thousands of other custom add-on markers of interest concerning Alzheimer's disease, drug metabolism, fertility, twinning and schizophrenia (approximately 40 000 markers). Normalised bead intensity data for each sample will be loaded into Illumina BeadStudio software (Illumina, Sand Diego, US; see https://www.illumina.com.cn/), which can convert fluorescence intensities into single-nucleotide polymorphism (SNP) genotypes. The quality control will be performed before conducting the association analysis. Samples will be excluded according to the following criteria: genotype call rate of <98%, gender discordance, samples with an inbreeding coefficient (F_HET) of <−0.2 or >0.2, and genetic outliers. SNPs will be excluded according to the following criteria: minor allele frequency of <0.01, genotype call rate of <95% (before sample removal), SNP missingness of <98% (after sample removal) and P-values in Hardy–Weinberg equilibrium of <1 × 10−6 in cases. Principal component analysis will be performed to identify genetic outliers, following the methodology of the EIGENSTRAT (Harvard University and The Broad Institute, US; see https://github.com/chrchang/eigensoft/tree/master/EIGENSTRAT) software.Reference Price, Patterson, Plenge, Weinblatt, Shadick and Reich30

Genotype imputation will be carried out for the discovery stage, using the pre-phasing/imputation stepwise approach.Reference Howie, Donnelly and Marchini31 Genotypes will be first phased with SHAPEIT (Linux (x86_64), version 2 http://mathgen.stats.ox.ac.uk/genetics_software/shapeit/shapeit.html),Reference Delaneau, Zagury and Marchini32 and imputation then performed over each 3-Mb interval centred on all index SNPs, using IMPUTE2 (Linux (x86_64) Static Executable, https://mathgen.stats.ox.ac.uk/impute/impute_v2.html) software.Reference Howie, Donnelly and Marchini31 Haplotypes derived from phase 1 of the 1000 Genomes Project (release v3, https://catalog.coriell.org/1/NHGRI/Collections/1000-Genomes-Collections/1000-Genomes-Project) will be used as reference data. We will use the same quality control, imputation and analysis pipeline for each GWAS in the discovery stage. We will exclude imputed SNPs with an imputation quality score below a set threshold (info <0.8), minor allele frequency of <0.01 and Hardy-Weinberg equilibrium P-value of  < 1 × 10−5. All genomic locations are given in National Center for Biotechnology (NCBI, https://www.ncbi.nlm.nih.gov/) Build 37 coordinates.

Analysis plan

Primary outcomes

PANSS reductive ratio

We will use short-term (at 6-week follow-up) changes in the PANSS reductive ratio to indicate treatment effects of antipsychotics. To avoid incorrect calculations, the theoretical minimum (30 for the total score) is subtracted from the baseline score, resulting in a score range that includes zero. Therefore, PANSS percentage change was defined as follows: the reduction rate of the total score of PANSS = (PANSS baseline score − PANSS end-point score)/(PANSS baseline score − 30) × 100%.

Secondary outcomes

Other effects of antipsychotics

We will assess short-term (at 6-week follow-up) changes in side-effects in both groups, using measures such as body mass index, blood pressure, fasting glucose, haemoglobin and waist and hip circumference. We will also assess short-term (at 6-week follow-up) changes in the Udvalg for Kliniske Under-sogelser Side-Effect Rating Scale.

Statistical analysis

Repeated measurements over time will be compared among the four groups, with the linear mixed model. The first analysis is an investigation into the relationship between the common variants and the efficacy of acute-stage treatment with different antipsychotics. We use the PANSS reductive ratio as the evaluation of acute-stage treatment response to different antipsychotic medications. We also use change in CGI-I score to assess the acute-stage treatment efficacy. Using PLINK version 1.07 (for Linux, https://www.cog-genomics.org/plink2),Reference Purcell, Neale, Todd-Brown, Thomas, Ferreira and Bender33 we will evaluate the association between allele dosages and the quantitative phenotype by the linear regression model. Gender, age, site of collection and the first four principal components of population structure will be used as covariates.

The second analysis of the secondary outcome consists of an investigation into the associations between the common variants and the side-effects of different antipsychotics. We will evaluate two kinds of phenotypes for side-effects of antipsychotics: dichotomous phenotype and continuous phenotype. The dichotomous phenotype will comprise patients with metabolic syndromes versus patients without metabolic syndromes. Metabolic syndrome diagnoses are based on the International Diabetes Federation Chinese criteria.Reference Alberti, Zimmet and Shaw34 Patients are identified as having a metabolic syndrome if they have central obesity (as assessed by waist circumference ≥85 cm in men and ≥80 cm in women), plus two of the following: elevated triglycerides level of ≥150 mg/dL (or use of a fibrate), high-density lipoprotein <40 mg/dL in men and <50 mg/dL in women (or use of a statin), fasting glucose ≥100 mg/dL (or use of an antidiabetic drug) and systolic arterial blood pressure ≥130 mmHg and/or diastolic arterial blood pressure ≥85 mmHg (or use of an antihypertensive drug). The continuous phenotype will comprise quantifying antipsychotic-induced change in the assessments as described above; for example, change in body mass index, blood lipids, glucose and haemoglobin. Using PLINK version 1.07,Reference Purcell, Neale, Todd-Brown, Thomas, Ferreira and Bender33 we will evaluate the association between allele dosages and the dichotomous phenotype by logistic regression, and perform the association between allele dosages and the quantitative phenotype by linear regression. The gender, age, site of collection and the first four principal components of population structure will be used as covariates.

The individualised preferred treatment prediction model will be set up based on the findings of different antipsychotics and the clinical data.

Ethics and dissemination

The study was reviewed and approved by the institutional ethical committee of each hospital. The study has been registered with Chinese Clinical Trial Registry, under registration number ChiCTR1800014755.

Discussion

There are several strengths to our study. The main strength is that it can provide a criterion to create a standard cohort, so that data can be well-preserved and used in later studies. A further strength is that this study is, to our knowledge, the first of its kind to be conducted on such a large scale among the Chinese Han population. Also, it considers both the efficacy and side-effects of antipsychotics. A limitation of this study is that it had a follow-up period of only 3 months.

In conclusion, this protocol describes the aims, hypotheses, design and procedures of the clinical trial, and its proposed method of identifying genetic determinants of response and side-effect to acute-stage antipsychotics treatment in patients with schizophrenia. This study may provide important evidence for translating the valuable findings from pharmacogenomics studies into clinical practice.

Data availability

The data that support the findings of this study are available from the corresponding author, W.Y., upon reasonable request.

Acknowledgements

We thank all of the patients and family members who participated in this study.

Author contributions

Y.S. and H.Y. are responsible for the writing of this manuscript, D.Z. and W.Y. are responsible for the study design. Z.W., S.L., L.Z., Y.F., Y.Y., B.D., F.Z., X.Z., M.H., C.H., G.H., Z.S., M.P., R.Y., Y.Z., H.Y., L.W., T.L., F.J., K.L., L.L., H.W., S.Y., Q.W., Y.T. and Y.X. contributed to the data acquisition and data analysis. Y.S., H.Y., D.Z. and W.Y. take responsibility for the collecting of information from the other authors, revising the manuscript, and submitting the manuscript.

Funding

This work is supported by a grant to Weihua Yue on behalf of the whole projectfrom the Chinese Ministry of Science and Technology (grant number 2016YFC1307000).

Declaration of interest

None.

References

Thaker, GK, Carpenter, WT Jr. Advances in schizophrenia. Nat Med 2001; 7(6): 667–71.CrossRefGoogle Scholar
Huber, CG, Naber, D, Lambert, M. Incomplete remission and treatment resistance in first-episode psychosis: definition, prevalence and predictors. Expert Opin Pharmacother 2008; 9(12): 2027–38.CrossRefGoogle ScholarPubMed
Lieberman, JA. Effectiveness of antipsychotic drugs in patients with chronic schizophrenia: efficacy, safety and cost outcomes of CATIE and other trials. J Clin Psychiatry 2007; 68(2): e04.CrossRefGoogle ScholarPubMed
Jones, PB, Barnes, TR, Davies, L, Dunn, G, Lloyd, H, Hayhurst, KP, et al. Randomized controlled trial of the effect on quality of life of second- vs first-generation antipsychotic drugs in schizophrenia: cost utility of the latest antipsychotic drugs in schizophrenia study (CUtLASS 1). Arch Gen Psychiatry 2006; 63(10): 1079–87.CrossRefGoogle Scholar
Ilyas, S, Moncrieff, J. Trends in prescriptions and costs of drugs for mental disorders in England, 1998–2010. Br J Psychiatry 2012; 200(5): 393–8.CrossRefGoogle Scholar
Horáček, J, Libiger, C, Höschl, K, Borzova, I, Hendrychová, J. Clozapine-induced concordant agranulocytosis in monozygotic twins. Int J Psychiatry Clin Pract 2001; 5(1): 71–3.CrossRefGoogle Scholar
Wehmeier, PM, Gebhardt, S, Schmidtke, J, Remschmidt, H, Hebebrand, J, Theisen, FM. Clozapine: weight gain in a pair of monozygotic twins concordant for schizophrenia and mild mental retardation. Psychiatry Res 2005; 133(2–3): 273–6.CrossRefGoogle Scholar
Lichtenstein, P, Yip, BH, Bjork, C, Pawitan, Y, Cannon, TD, Sullivan, PF, et al. Common genetic determinants of schizophrenia and bipolar disorder in Swedish families: a population-based study. Lancet 2009; 373(9659): 234–9.CrossRefGoogle ScholarPubMed
Malhotra, AK, Jr , MG, Kennedy, JL. Pharmacogenetics of psychotropic drug response. Am J Psychiatry 2004; 161(5): 780–96.CrossRefGoogle ScholarPubMed
Lencz, T, Robinson, DG, Xu, K, Ekholm, J, Sevy, S, Gunduz-Bruce, H, et al. DRD2 promoter region variation as a predictor of sustained response to antipsychotic medication in first-episode schizophrenia patients. Am J Psychiatry 2006; 163(3): 529–31.CrossRefGoogle ScholarPubMed
Zhang, J-P, Lencz, T, Malhotra, AK. D2 receptor genetic variation and clinical response to antipsychotic drug treatment: a meta-analysis. Am J Psychiatry 2010; 167(7): 763–72.CrossRefGoogle ScholarPubMed
Hwang, R, Zai, C, Tiwari, A, Müller, D, Arranz, M, Morris, A, et al. Effect of dopamine D3 receptor gene polymorphisms and clozapine treatment response: exploratory analysis of nine polymorphisms and meta-analysis of the Ser9Gly variant. Pharmacogenomics J 2010; 10(3): 200–18.CrossRefGoogle ScholarPubMed
Arranz, M, Collier, D, Sodhi, M, Ball, D, Roberts, G, Sham, P, et al. Association between clozapine response and allelic variation in 5-HT 2A receptor gene. Lancet 1995; 346(8970): 281–2.CrossRefGoogle Scholar
Reynolds, GP, Templeman, LA, Zhang, ZJ. The role of 5-HT2C receptor polymorphisms in the pharmacogenetics of antipsychotic drug treatment. Prog Neuro Psychopharmacol Biol Psychiatry 2005; 29(6): 1021–8.CrossRefGoogle ScholarPubMed
Ravyn, D, Ravyn, V, Lowney, R, Nasrallah, HA. CYP450 pharmacogenetic treatment strategies for antipsychotics: a review of the evidence. Schizophr Res 2013; 149(1–3): 114.CrossRefGoogle Scholar
Sirot, EJ, Knezevic, B, Morena, GP, Harenberg, S, Oneda, B, Crettol, S, et al. ABCB1 and cytochrome P450 polymorphisms: clinical pharmacogenetics of clozapine. J Clin Psychopharmacol 2009; 29(4): 319–26.CrossRefGoogle Scholar
Consoli, G, Lastella, M, Ciapparelli, A, Dell'Osso, MC, Ciofi, L, Guidotti, E, et al. ABCB1 polymorphisms are associated with clozapine plasma levels in psychotic patients. Pharmacogenomics 2009; 10(8): 1267–76.CrossRefGoogle ScholarPubMed
Åberg, K, Adkins, DE, Bukszár, J, Webb, BT, Caroff, SN, Miller, DD, et al. Genomewide association study of movement-related adverse antipsychotic effects. Biol Psychiatry 2010; 67(3): 279–82.CrossRefGoogle ScholarPubMed
Adkins, DE, Åberg, K, McClay, JL, Bukszár, J, Zhao, Z, Jia, P, et al. Genomewide pharmacogenomic study of metabolic side effects to antipsychotic drugs. Mol Psychiatry 2011; 16(3): 321–2.CrossRefGoogle ScholarPubMed
Clark, SL, Souza, RP, Adkins, DE, Åberg, K, Bukszár, J, McClay, JL, et al. Genome-wide association study of patient and clinician rated global impression severity during antipsychotic treatment. Pharmacogenet Genomics 2013; 23(2): 69.CrossRefGoogle ScholarPubMed
McClay, JL, Adkins, DE, Åberg, K, Bukszár, J, Khachane, AN, Keefe, RS, et al. Genome-wide pharmacogenomic study of neurocognition as an indicator of antipsychotic treatment response in schizophrenia. Neuropsychopharmacology 2011; 36(3): 616–26.CrossRefGoogle Scholar
McClay, JL, Adkins, DE, Åberg, K, Stroup, S, Perkins, DO, Vladimirov, VI, et al. Genome-wide pharmacogenomic analysis of response to treatment with antipsychotics. Mol Psychiatry 2011; 16(1): 7685.CrossRefGoogle ScholarPubMed
First, MB, Spitzer, RL, Gibbon, M, Williams, JB. User's Guide for the Structured Clinical Interview for DSM-IV Axis I Disorders SCID-I: Clinician Version. American Psychiatric Press, 1997.Google Scholar
Kay, SR, Flszbein, A, Opfer, LA. The Positive and Negative Syndrome Scale (PANSS) for schizophrenia. Schizophr Bull 1987; 13(2): 261.CrossRefGoogle Scholar
Busner, J, Targum, SD. The clinical global impressions scale: applying a research tool in clinical practice. Psychiatry (Edgmont) 2007; 4(7): 2837.Google ScholarPubMed
Guy, W. ECDEU Assessment Manual for Psychopharmacology. US Department of Health, Education, and Welfare, Public Health Service, Alcohol, Drug Abuse, and Mental Health Administration, National Institute of Mental Health, Psychopharmacology Research Branch, Division of Extramural Research Programs, 1976.Google Scholar
Simpson, G, Angus, J. A rating scale for extrapyramidal side effects. Acta Psychiatr Scand 1970; 45(S212): 11–9.CrossRefGoogle Scholar
Barnes, TR. A rating scale for drug-induced akathisia. Br J Psychiatry 1989; 154: 672–6.CrossRefGoogle ScholarPubMed
Munetz, MR, Benjamin, S. How to examine patients using the abnormal involuntary movement scale. Psychiatr Serv 1988; 39(11): 1172–7.CrossRefGoogle ScholarPubMed
Price, AL, Patterson, NJ, Plenge, RM, Weinblatt, ME, Shadick, NA, Reich, D. Principal components analysis corrects for stratification in genome-wide association studies. Nat Genet 2006; 38(8): 904–9.CrossRefGoogle ScholarPubMed
Howie, BN, Donnelly, P, Marchini, J. A flexible and accurate genotype imputation method for the next generation of genome-wide association studies. PLoS Genet 2009; 5(6): e1000529.CrossRefGoogle ScholarPubMed
Delaneau, O, Zagury, JF, Marchini, J. Improved whole-chromosome phasing for disease and population genetic studies. Nat Methods 2013; 10(1): 56.CrossRefGoogle ScholarPubMed
Purcell, S, Neale, B, Todd-Brown, K, Thomas, L, Ferreira, MA, Bender, D, et al. PLINK: a tool set for whole-genome association and population-based linkage analyses. Am J Hum Genet 2007; 81(3): 559–75.CrossRefGoogle ScholarPubMed
Alberti, KGMM, Zimmet, P, Shaw, J. Metabolic syndrome—a new world-wide definition. a consensus statement from the international diabetes federation. Diabet Med 2006; 23(5): 469–80.CrossRefGoogle ScholarPubMed
Figure 0

Fig. 1 Flowchart of this study. CGI, Clinical Global Impressions Scale; PANSS, Positive and Negative Syndrome Scale.

Figure 1

Table 1 Inclusion criteria

Figure 2

Table 2 Exclusion criteria

Figure 3

Table 3 Study visit schedule

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