Participants

This meta-analysis will include male and female individuals aged 16–65 years with a diagnosis of schizophrenia or other psychotic disorder (schizophrenia, schizophreniform, schizoaffective disorder, delusional disorder, brief psychotic disorder, recent-onset psychosis, ultra-high risk for psychosis) irrespective of the diagnostic criteria used, following the strategy of the Cochrane Schizophrenia Group. The Cochrane Schizophrenia Group suggests that specific diagnostic criteria – such as those of ICD-11 or DSM-5 – are not accurately used in routine clinical practice. Therefore, including studies that do not use these systems should increase generalisability and representativeness.^{Reference Adams, Coutinho, Davis, Duggan, Leucht and Li11} Moreover, our purpose is to examine the duality male/female as determined by sex chromosomes, but we cannot control the use of ‘gender’ and ‘sex’ in the studies we are including in the review.

Studies with participants with non-psychotic disorders will be included only if individuals with a diagnosis of a psychotic disorder represent more than 80% of the sample.

We will exclude studies in which all participants, by study inclusion criteria, (a) are acutely ill, (b) have a comorbid pathology or psychosis secondary to another psychiatric or medical diagnosis (e.g. dual pathology, bipolar disorder with psychotic symptoms, psychotic depression, obsessive–compulsive disorder comorbid with psychosis), (c) have a concomitant medical illness or (d) have dementia or intellectual disability (premorbid IQ < 70).

For the purposes of the review we define recent-onset psychosis as a first diagnosis of schizophrenia or other psychotic disorder within the preceding 5 years, according to research done in our group^{Reference Ochoa, López-Carrilero, Barrigón, Pousa, Barajas and Lorente-Rovira12} and established operational definitions.^{Reference Breitborde, Srihari and Woods13}

Studies

We will include both cross-sectional and longitudinal observational studies. To be included, we require that a study presents data about outcomes separately for males and females. For the case of longitudinal studies or clinical trials, we will only include their baseline data.

To reduce the risk of ‘language bias’,^{Reference Egger, Zellweger-Zähner, Schneider, Junker, Lengeler and Antes14} the included languages will be English, Spanish, Italian, German and Chinese. We will consider studies irrespective of setting (in-patients and out-patients), nationality and ethnicity. Grey literature will be included where identified.

Outcomes

As primary outcomes, we will consider data on positive, negative, depressive and disorganised symptomatology and general psychopathology measured using published and validated scales such as the Positive and Negative Syndrome Scale (PANSS), Brief Psychiatric Rating Scale (BPRS), Scale for the Assessment of Positive Symptoms (SAPS), Scale for the Assessment of Negative Symptoms (SANS), Beck Depression Inventory (BDI) and Calgary Depression Inventory (CDI).

As secondary outcomes, we will consider data on other symptoms of interest in the study of psychosis (e.g. mania, anxiety). As with primary outcomes, we will include secondary outcomes measured using rating scales published in peer-reviewed journals, such as the Beck Anxiety Inventory (BAI) and the Young Mania Rating Scale (YMRS).

Electronic searches

The PsychInfo, PubMed, Web of Science, Scopus and Dialnet databases were searched in August 2021 without restrictions for publication period. The final search strategy for PubMed appears in the Appendix. The full search strategies for the different databases are shown the supplementary material available at https://dx.doi.org/10.1192/bjo.2022.596. The date of the last search update will be provided in the final publication.

Reference lists and other sources

We will inspect (a) previous narrative reviews concerning sex differences in psychotic disorders in a broad array of outcomes and (b) the reference lists of our included studies, to check for additional studies that could meet our inclusion criteria not found by the electronic search.

Identification and selection of studies

Studies identified using electronic and manual searches will be exported and listed in the Picoportal software;^{Reference Agai15} duplicates will be excluded. Determining eligibility for the inclusion will comprise the following two stages.

1. (1) Screening: two authors (M.F.-Q. and M.E.S.) will independently check titles and abstracts identified in the literature searches. Records that do not meet inclusion criteria will be excluded. Disagreement will be resolved by discussion. If there is remaining doubt, we will obtain the full article for further inspection.

2. (2) Eligibility: in the inspection of full articles, the same two authors (M.F.-Q. and M.E.S.) will independently assess them for eligibility. Disagreements will be resolved with a third author (H.G.-M.) or, when this is not possible, by contacting the study authors.

Characteristics of the included studies

We will generate descriptive statistics and study sample characteristics across all eligible studies, describing clinical and methodological variables such as sample distribution (number of males and females), age, diagnoses, duration of the disorder, country, setting and scales used to measure symptoms.

Pairwise meta-analysis: data synthesis

As we expect most studies to report means and standard deviations, we will calculate standardised mean differences (s.m.d.) with 95% confidence intervals for each outcome.^{Reference Sedgwick and Marston20} If an asset-based outcome has negative valence, we will recode the means (multiplied by −1) so that the valences coincide. For studies with more than one scale in the same outcome group, we will convert mean values for each of these measures to a single mean value for the intervention and control groups respectively. We will compute the variance of the mean between scales within the same outcome grouping using Borenstein et al's method.^{Reference Borenstein, Hedges, Higgins and Rothstein21} If means or standard deviations are not available to calculate effect size and associated standard error we will estimate it/them from other reported statistics (e.g. t, f) or contact study authors for this information. If we find studies in which symptomatology is treated as a binary variable, odds ratios (OR) will be calculated as an index of effect size.

We will perform series of pairwise meta-analyses by separating studies according to the stage of the disorder (ultra-high risk for psychosis, recent-onset psychosis and established psychosis) and separated by symptom domain. If there are not enough studies available for meta-analysis in a particular symptom domain for one of the stages of the disorder, these studies will be presented narratively in the form of systematic review. As heterogeneity is likely, we will use a random-effects model.

Assessment of heterogeneity

Statistical heterogeneity will be assessed using Cochran's Q, I² and τ². Cochran's Q is a chi-squared distributed measure of weighted squared deviations. It can be converted into a P-value and is the usual heterogeneity test statistic. The principal advantage of the I² statistic, the proportion of the observed variance reflecting real differences in effect size, is that it can be calculated and compared across meta-analyses of different sizes, of different types of study and using different types of outcome data.^{Reference Higgins, Thompson, Deeks and Altman22} Finally, τ² is the random-effects variance of the true effect sizes.

Investigation of heterogeneity: meta-regression and sensitivity analysis

As we expect some degree of heterogeneity in our outcomes, we will explore the following potential effect modifiers of our symptomatology outcomes by meta-regression (for continuous variables) and subgroup analyses (for dichotomous variables) if there are ten or more studies that include these factors:

1. (a) year of publication of the study

2. (b) country of the study: high-income versus low- and middle-income countries

3. (c) setting: in-patients versus out-patients (on enrolment in the study)

4. (d) sample size

5. (e) diagnostic system, for example manualised diagnostic criteria (such as DSM or ICD) versus clinical diagnosis (where no diagnostic manual is referred to)

6. (f) relevant sociodemographic characteristics that might affect symptom presentation. Given that sex differences in outcomes in people with psychosis vary depending on the individual's age,^{Reference Seeman23} one of the main characteristics that will be controlled for will be the age of the participants in the studies. Other characteristics to be controlled for may include age at onset, duration of illness, duration of untreated psychosis, premorbid adjustment, substance misuse, marital status, work status and dose of antipsychotic medication.

We will perform two types of sensitivity analysis if there are enough studies:

1. (a) exclusion of studies characterised as being of poor methodological quality (as assessed using the NHLBI assessment tool)

2. (b) exclusion of studies where the median or mean age of the participants is over 45 years.

Publication bias

To assess small study effects and publication bias, we will use contour-enhanced funnel plots and Begg & Mazumdar^{Reference Begg and Mazumdar24} tests by outcome valence if ten or more studies are included.

Statistical software

All analyses will be done using the R package ‘meta’.^{25,Reference Schwarzer, Carpenter and Rücker26} The procedures described here follow steps similar to those used in previous meta-analyses done by the corresponding author (H.G.-M.).^{Reference Eiroa-Orosa and García-Mieres27}