The incidence of psychotic disorders in the Republic of Ireland: a systematic review

R. P. Jacinto; T. Ding; J. Stafford; G. Baio; J. B. Kirkbride

doi:10.1017/ipm.2023.35

The incidence of psychotic disorders in the Republic of Ireland: a systematic review

Published online by Cambridge University Press: 31 July 2023

T. Ding ,

G. Baio and

R. P. Jacinto: Affiliation:
Division of Psychiatry, UCL, London, UK
T. Ding: Affiliation:
Department of Statistical Sciences, UCL, London, UK
J. Stafford: Affiliation:
Division of Psychiatry, UCL, London, UK MRC Unit for Lifelong Health and Ageing, UCL, London, UK
G. Baio: Affiliation:
Department of Statistical Sciences, UCL, London, UK
J. B. Kirkbride*: Affiliation:
Division of Psychiatry, UCL, London, UK
*: Corresponding author: James B. Kirkbride; Email: j.kirkbride@ucl.ac.uk

Article contents

Abstract
Objectives:
Methods:
Results:
Conclusions:
Introduction
Methods
Results
Discussion
Conclusion
Supplementary material
Competing interests
Ethical standard
Financial support
Preprint information
References

Rights & Permissions

Abstract

Objectives:

Despite a substantial epidemiological literature on the incidence of psychotic disorders in Ireland, no systematic review has previously been undertaken. Such evidence can help inform understanding of need for psychosis care.

Methods:

We conducted a prospectively registered systematic review (PROSPERO: CRD42021245891) following PRISMA guidelines. We searched four databases (Medline, PsycInfo, Web of Science, Embase) for papers containing incidence data on non-organic psychotic disorders, in people 16–64 years, published between 1950 and 2021 in the general adult population. We conducted duplicate screening, risk of bias assessments, and extracted data to a standardised template. We undertook a narrative synthesis for each major diagnostic outcome. Random effects meta-analyses were conducted for comparisons with ≥5 incidence rates.

Results:

Our search yielded 1975 non-duplicate citations, of which 23 met inclusion criteria, containing incidence data ascertained between 1974 and 2016 (median study quality: 5/8; interquartile range: 4–6). Incidence of all psychotic disorders (N = 4 studies) varied from 22.0 (95%CI: 17.3–28.0) in Dublin to 34.1 per 100,000 person-years (95%CI: 31.0–37.5) in Cavan and Monaghan. The pooled incidence of schizophrenia (N = 6 studies, N = 8 settings) was 20.0 per 100,000 person-years, though with imprecision around this estimate (95%CI: 10.6–37.5; I2: 97.6%). Higher rates of most outcomes were observed in men. There was consistent evidence of raised rates in more deprived and fragmented social environments, but no clear pattern by rural-urban status.

Conclusions:

Patterns of incidence of psychotic disorders in Ireland are broadly consistent with the wider literature from the Global North. Findings could help identify populations at higher risk of psychosis in Ireland.

Keywords

Systematic review incidence epidemiology psychotic disorders Ireland

Type: Review Article
Information: Irish Journal of Psychological Medicine , First View , pp. 1 - 13

DOI: https://doi.org/10.1017/ipm.2023.35 [Opens in a new window]
Creative Commons: This is an Open Access article, distributed under the terms of the Creative Commons Attribution licence (https://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: © The Author(s), 2023. Published by Cambridge University Press on behalf of The College of Psychiatrists of Ireland

Introduction

Psychotic disorders are associated with substantial psychiatric and physical morbidity (Firth et al., Reference Firth, Siddiqi, Koyanagi, Siskind, Rosenbaum and Galletly2019), negative social outcomes and premature mortality (Hjorthøj et al., 2019; Laursen Reference Laursen2011), and require early intervention to reduce the risk of these deleterious outcomes. A substantial body of evidence suggests that the longer people go without treatment for psychosis (so-called ‘duration of untreated psychosis’ [DUP]) the worse these outcomes become (Csillag et al., Reference Csillag, Nordentoft, Mizuno, McDaid, Arango, Smith, Lora, Verma, Di Fiandra and Jones2018; Marshall et al., Reference Marshall, Lewis, Lockwood, Drake, Jones and Croudace2005). This has led to the development of Early Intervention in Psychosis [EIP] services (McGorry et al., Reference McGorry, Edwards, Mihalopoulos, Harrigan and Jackson1996), which provide early, multidisciplinary care for people experiencing psychosis for the first time, founded upon evidence-based treatments (Csillag et al., Reference Csillag, Nordentoft, Mizuno, McDaid, Arango, Smith, Lora, Verma, Di Fiandra and Jones2018). Treatments offered in EIP services often include pharmacological intervention, cognitive behavioural therapy, physical health monitoring and physical health interventions, supported education/employment programmes, family therapy and carer support.

Randomised controlled trials [RCTs] have demonstrated that EIP care over treatment as usual results in beneficial functional and social outcomes for people with psychosis (Kane et al., Reference Kane, Robinson, Schooler, Mueser, Penn and Rosenheck2016; Nordentoft et al., Reference Nordentoft, Rasmussen, Melau, Hjorthoj and Thorup2014). EIP services have become a dominant model of care provision for young people experiencing psychosis in many countries including England, Australia, Denmark, Canada and the US (Csillag et al., Reference Csillag, Nordentoft, Mizuno, McDaid, Arango, Smith, Lora, Verma, Di Fiandra and Jones2018). In Ireland, EIP services have also recently been established in some areas, including Dublin (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021), Cork, Sligo, and Cavan and Monaghan (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021). A recent health economic evaluation of EIP services in Ireland has suggested that they are associated with substantial potential incremental net benefits over the first year of treatment, in terms of both health sector and societal economic benefits (Behan et al., Reference Behan, Kennelly, Roche, Renwick, Masterson, Lyne, O’Donoghue, Waddington, McDonough, McCrone and Clarke2020). This economic impact is particularly important, given the high total economic cost of schizophrenia in Ireland, which was estimated to be €460.6 million as far back as 2006 (Behan et al., Reference Behan, Kennelly and O’Callaghan2008), made up of substantial direct costs (€117.5 million) and indirect costs (€343 million) due to lost productivity faced by both patients and their informal caregivers.

The timely provision of evidence-based psychosis care must be predicated on an understanding of predicted local need to allocate resources in a just and proportional way to optimise service delivery. The incidence of psychotic disorders follows highly replicable and precisely delineated demographic and social distributions (Jongsma et al., Reference Jongsma, Turner, Kirkbride and Jones2019; Kirkbride et al., Reference Kirkbride, Errazuriz, Croudace, Morgan, Jackson, Boydell, Murray and Jones2012; Kirkbride et al., Reference Kirkbride, Hameed, Ioannidis, Ankireddypalli, Crane and Nasir2017), which has been used in other jurisdictions, most notably England, to develop models to predict future need for services based on a local understanding of the determinants of psychosis risk in different populations (McDonald et al., Reference McDonald, Ding, Ker, Dliwayo, Osborn, Wohland, Coid, French, Jones, Baio and Kirkbride2021). Thus, in planning psychosis care in the Irish context, it is crucial to understand the epidemiological landscape through which the incidence of psychotic disorders manifests in the population. Although several reviews have investigated the incidence of psychotic disorders in the UK (Kirkbride et al., Reference Kirkbride, Errazuriz, Croudace, Morgan, Jackson, Boydell, Murray and Jones2012) and worldwide (Jongsma et al., Reference Jongsma, Turner, Kirkbride and Jones2019; McGrath et al., Reference McGrath, Saha, Welham, El Saadi, MacCauley and Chant2004), a dedicated synthesis of the evidence base for the incidence of psychotic disorders in the Republic of Ireland has not previously been conducted, despite a long history of methodologically robust studies in this space (see, for example, publications from the CAMFEPS study in Cavan and Monaghan (Scully et al., Reference Scully, Quinn, Morgan, Kinsella, O’Callaghan, Owens and Waddington2002; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021), and publications from recent data from the DETECT Early Intervention in Psychosis [EIP] service in South Dublin and Wicklow (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016).

The aim of this systematic review is to summarise and assess the current evidence on the incidence of psychotic disorders in the Republic of Ireland, and examine how this varied by sociodemographic variables (age, sex, ethnicity, religion, etc.) and neighbourhood characteristics (social deprivation, social fragmentation, population density, etc.).

Methods

In this systematic review, we sought to synthesise evidence on the incidence of psychotic disorders in the Republic of Ireland from the published literature between 1950 and 2021, and investigate how rates varied by reported sociodemographic and socioenvironmental factors. Our review was prospectively registered on the PROSPERO systematic review protocol database: CRD42021245891. We followed guidelines for the conduct and reporting of systematic reviews from the Preferred Reporting Items for Systematic Reviews and Meta-Analyses [PRISMA] statement (Supplemental Table 1) (Moher et al., Reference Moher, Liberati, Tetzlaff and Altman2009).

Eligibility criteria

We sought to identify all studies:

Published between 1 January 1950 and 31 August 2021
Reporting the incidence of psychotic disorders in any study, wholly or partially conducted in Ireland, or which provided sufficient information to derive incidence rates
Including participants from the general adult population aged 16–64 years old
Including any non-organic psychotic disorder according to a validated classification system (i.e. Diagnostic and Statistical Manual [DSM] (American Psychiatric Association 2013) or International Statistical Classification of Diseases and Related Health Problems [ICD] (World Health Organization 2004).)
Published in English

Studies were excluded if they focused solely on:

Organic psychotic disorders, or those with clear evidence of an intellectual disability
Non-population-based samples or specialist groups (e.g. perinatal mental health, prison, military or other specialist populations)

Information sources and search strategy

We searched four electronic databases: OVID Medline, Embase, PsycInfo and Web of Science. We also screened citation lists of included publications, and contacted authors of relevant papers to identify potentially missed studies or omitted data relevant to our review.

We developed our search strategy (see Supplemental Methods) in conjunction with a UCL librarian, adapted from a previously validated search strategy for incidence studies (Jongsma et al., Reference Jongsma, Turner, Kirkbride and Jones2019). Our search strategy included terms for (i) psychotic disorders, (ii) incidence / first episode psychosis [FEP], and (iii) a location-based term for studies restricted to the Republic of Ireland. Our initial search was conducted between March 2021 and August 2021 by one researcher (RPJ).

Study selection

After excluding duplicates, citation titles were screened independently by two authors (RPJ, JBK). Citations were rated as either excluded, insufficient information or included; discrepancies were resolved by consensus, with only citations flagged as included or as insufficient information progressing to abstract review. The same process was repeated at abstract review stage. One author (RPJ) reviewed the full text of remaining citations for eligibility, with uncertainties resolved by consensus with the senior author (JBK).

Data extraction

Data extraction was conducted by a single author (RPJ) into a prespecified spreadsheet, with uncertainties discussed and resolved with the senior author (JBK), who also reviewed the spreadsheet for accuracy. We extracted citation-level (e.g. setting, publication year, diagnostic outcomes, study quality), rate-level (e.g. number of cases, denominator data, rates and standard errors), individual-level (e.g. age, sex, ethnicity or socioeconomic status) and area-level (e.g. deprivation) data, as provided in each citation (see Supplemental Methods; Supplemental Table 2). Data were extracted from each citation according to the original metric reported in each study (i.e. the age groups reported in each study, or quintiles of deprivation).

Diagnostic outcomes

We extracted rate-level data from all identified citations according to the diagnostic codes used in each original citation. We then used algorithms previously developed for use in other national and international systematic reviews of psychotic disorders (Jongsma et al., Reference Jongsma, Turner, Kirkbride and Jones2019; Kirkbride et al., Reference Kirkbride, Errazuriz, Croudace, Morgan, Jackson, Boydell, Murray and Jones2012) to create broad diagnostic outcomes of interest (Supplemental Table 3) following the International Classification of Diseases, 10^th edition [ICD-10]. We included the following outcomes: all psychotic disorders (ICD-10 F10-33), non-affective psychotic disorders (F20-29), schizophrenia (F20), affective psychotic disorders (F30.2, 31.2, 32.3, 33.3), bipolar disorder (F30.2, 31.2), depression with psychotic features (F32.3, 33.3) and substance-induced psychoses (F1x.5). We did not distinguish between different types of rates in our study (i.e. ‘first contact’, ‘first episode’, ‘first admission’ etc) because they typically estimate a similar latent construct of ‘treated’ incidence, with nomenclature reflecting the mode of care delivery at the time (for example, studies of ‘first admission’ tend to be older, based on case ascertainment when treatment was almost exclusively based on inpatient care). Exceptions exist, including the CAMFEPS epidemiological study, which employed population-based case finding, such that rates may be closer to the true incidence in the population, which we captured as part of our assessment of methodological quality.

Methodological quality and risk of bias of included studies

To assess risk of bias, we identified seven relevant epidemiological criteria (Supplemental Table 4, a–g) indicative of study quality for estimating incidence rates in psychiatric epidemiology, based on previous reviews (Jongsma et al., Reference Jongsma, Turner, Kirkbride and Jones2019; Kirkbride et al., Reference Kirkbride, Errazuriz, Croudace, Morgan, Jackson, Boydell, Murray and Jones2012). These items included reporting of a defined catchment area, accurate denominator estimation, population-based case finding, standardised research diagnoses, defined inclusion criteria, and conduct of a ‘leakage’ study to identify cases potentially missed during the initial ascertainment period (see Supplemental Table 4 for more details). We also included two additional criteria (h–i) regarding the reporting of sufficient data to derive both incidence rates and associated statistical uncertainty (h), and whether crude and standardised rates were reported (i). In a small deviation from our protocol, we retrospectively dropped criterion (e) because our review did not identify any study that reported incidence by ethnicity or country-of-birth, the primary purpose for which this criterion has been used previously (Kirkbride et al., Reference Kirkbride, Fearon, Morgan, Dazzan, Morgan, Tarrant, Lloyd, Holloway, Hutchinson, Leff, Mallett, Harrison, Murray and Jones2006). Thus, each citation was scored on our risk of bias assessment from 0 to 8 (‘a–i’, except ‘e’).

Data synthesis

We adopted a narrative synthesis to describe variance in incidence of psychotic disorders in Ireland for each diagnostic group (see ‘Diagnostic outcomes’, above), where possible assessing variance by sociodemographic and socioenvironmental characteristics. In instances where several citations provided overlapping data from the same setting (for example, for a series of studies in the Cavan-Monaghan region), we reported data from the most relevant (i.e. principal) citation(s) for a given outcome. Incidence rates were reported per 100,000 person-years as our measure of effect.

Where at least five incidence rates (with corresponding standard errors) were available for a given analysis, we also conducted a random effects meta-analysis to formally pool the data, and estimated between-study heterogeneity in reported rates. Heterogeneity was estimated using the Q-test, and quantified using the I²-statistic (Higgins and Thompson Reference Higgins and Thompson2002). Where possible, we also conducted meta-regression to inspect whether reported rates varied by risk of bias (study quality). We also assessed identified citations for the presence of small study effects, the most common of which is publication bias, via visual inspection of funnel plots and a formal Egger’s test of publication bias where we had sufficient data to pool estimates. All analyses were conducted in Stata, version 17.

Results

Study selection

After removing duplicate records, our initial search identified 1,975 citations (Fig. 1) of which 21 met our inclusion criteria (Scully et al., Reference Scully, Quinn, Morgan, Kinsella, O’Callaghan, Owens and Waddington2002; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Keatinge Reference Keatinge1986; Baldwin et al., Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O’Callaghan and Waddington2005; Morgan et al., Reference Morgan, Scully, Quinn, Kinsella, Owens and Waddington2001; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2012; Keatinge Reference Keatinge1987; Daly et al., Reference Daly, Webb and Kaliszer1995; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella and O’Callaghan2002; Waddington et al., Reference Waddington, Baldwin, Morgan, Quinn, Scully and Kinsella2004; Kingston et al., Reference Kingston, Owoeye, Kinsella, Russell, O’Callaghan, Waddington and Ritsner2011; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella, Owens, O’Callaghan and Waddington2003; Owoeye et al., Reference Owoeye, Kingston, Scully, Baldwin, Browne, Kinsella, Russell, O’Callaghan and Waddington2013; Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014; Keatinge Reference Keatinge1988; Browne et al., Reference Browne, Scully, Quinn, Morgan, Baldwin, Kinsella, Owens, O’Callaghan and Waddington2005; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987; Kelly et al., Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014). Via author contacting, we identified a further two citations which met inclusion criteria (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021). Of the 23 citations included in this review (Table 1), only six unique citations contained poolable incidence rate data for meta-analyses (see below) as the remainder of citations did not provide a corresponding estimate of standard error alongside reported rates.

Figure 1. PRISMA flow diagram of search strategy.

Table 1. Overview of included citations on the incidence of psychotic disorders in Ireland

Legend: N: number of cases; NR: Not reported; ∼derived; Pop.: population.

Location: C-M: Cavan-Monaghan; DSC: Dublin South Central; D: Dublin; C&W: Clare & Wexford; M&W: Monaghan & Waterford; SD&C-M: South Dublin & Cavan-Monaghan, SD&W: South Dublin & Wicklow; CWR: Carlow, Westmeath, Roscommon.

Study: CAMFEPS: Cavan-Monaghan First Episode Psychosis Study; COPE: Carepath for Overcoming Psychosis Early; WHO: World Health Organization 10-country / DOSMED study; K-T: Keatinge thesis; K-O: Keatinge other; DETECT: Dublin East Treatment and Early Care Team; 3CS: Three-county Study.

Diagnostic confirmation method: SCID: Structured Clinical Interview for DSM Disorders; Clinical: Clinical diagnosis; PSE: Present State Examination; PPHS: Personal & Psychiatric History Schedule; SCL: Syndrome Check List; AS: Aetiology Schedule.

Diagnostic outcomes included: FEP: All first episode psychotic disorders; NAP: Non-affective psychosis; AP: Affective psychosis; SZ: Schizophrenia; BD/M: Bipolar disorder/Mania; PD: Psychotic Depression; SIP: Substance-induced psychotic disorders; O: Other psychotic disorders.

# Conference abstract.

* likely, but not reported. Based on other citations from same group/setting, or other deduction.

Study characteristics

Citations were published between 1986 (Keatinge Reference Keatinge1986) and 2021 (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021) and contained incidence data on psychotic disorders collected between 1974 (Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987) and 2016 (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021). Sample sizes ranged from just 30 new cases of bipolar disorder or mania with psychotic features in Dublin South Central (Daly et al., Reference Daly, Webb and Kaliszer1995) between 1975 and 1981, to 593 new cases of any FEP in the Dublin East Treatment and Early Care Team [DETECT] EIP service in South Dublin and Wicklow between 2006 and 2014 (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021).

Twelve citations (52.2%) reported incidence rates of psychotic disorders in the Cavan-Monaghan First Episode Psychosis Study [CAMFEPS] (Scully et al., Reference Scully, Quinn, Morgan, Kinsella, O’Callaghan, Owens and Waddington2002; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Baldwin et al., Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O’Callaghan and Waddington2005; Morgan et al., Reference Morgan, Scully, Quinn, Kinsella, Owens and Waddington2001; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2012; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella and O’Callaghan2002; Waddington et al., Reference Waddington, Baldwin, Morgan, Quinn, Scully and Kinsella2004; Kingston et al., Reference Kingston, Owoeye, Kinsella, Russell, O’Callaghan, Waddington and Ritsner2011; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella, Owens, O’Callaghan and Waddington2003; Owoeye et al., Reference Owoeye, Kingston, Scully, Baldwin, Browne, Kinsella, Russell, O’Callaghan and Waddington2013; Browne et al., Reference Browne, Scully, Quinn, Morgan, Baldwin, Kinsella, Owens, O’Callaghan and Waddington2005; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014), with a further citation reporting inception rates of FEP in the COPE EIP service in the same catchment area following the end of the CAMFEPS study in 2011 (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021). Six citations provided incidence data from studies partially set in Dublin (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Daly et al., Reference Daly, Webb and Kaliszer1995; Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014; Kelly et al., Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992), including the World Health Organization [WHO] Ten-country study (Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992) and three citations from the DETECT EIP service (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014). Other locations included Clare and Wexford (O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Keatinge Reference Keatinge1986; Keatinge Reference Keatinge1987; Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014), Waterford (Keatinge Reference Keatinge1988) and Carlow, Westmeath and Roscommon (Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987), as part of the ‘The Three-County Study’.

All included citations used either DSM-IV (n = 17; 73.9%) or ICD criteria (n = 6; 26.1%). The most common method of diagnostic assessment reported was the Structured Clinical Interview for DSM Disorders [SCID] (n = 10; 43.5%). The most common diagnostic outcomes were ‘all FEP disorders’ (n = 18; 77.3%) and ‘affective psychotic disorders’ (n = 18; 78.3%), followed by ‘non-affective psychotic disorders’ (n = 12; 52.2%) and ‘bipolar disorder with psychotic features’ (n = 12; 52.2%) (Table 1; Supplemental Figure 1). Most citations included in this review adopted an age range from 15 years and older (Table 1) with no upper cut-off (Scully et al., Reference Scully, Quinn, Morgan, Kinsella, O’Callaghan, Owens and Waddington2002; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Keatinge Reference Keatinge1986; Baldwin et al., Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O’Callaghan and Waddington2005; Morgan et al., Reference Morgan, Scully, Quinn, Kinsella, Owens and Waddington2001; Keatinge Reference Keatinge1987; Daly et al., Reference Daly, Webb and Kaliszer1995; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella and O’Callaghan2002; Waddington et al., Reference Waddington, Baldwin, Morgan, Quinn, Scully and Kinsella2004; Kingston et al., Reference Kingston, Owoeye, Kinsella, Russell, O’Callaghan, Waddington and Ritsner2011; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella, Owens, O’Callaghan and Waddington2003; Owoeye et al., Reference Owoeye, Kingston, Scully, Baldwin, Browne, Kinsella, Russell, O’Callaghan and Waddington2013; Keatinge1988; Browne et al., Reference Browne, Scully, Quinn, Morgan, Baldwin, Kinsella, Owens, O’Callaghan and Waddington2005; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014). Four citations (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987) specified an upper cut-off of 64 or 65 years old, while the WHO 10-Country study was restricted to 15–54 years (Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992). One citation did not report an age range (Kelly et al., Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010).

Risk of bias within studies

Study quality varied from one (Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella, Owens, O’Callaghan and Waddington2003) to seven (Scully et al., Reference Scully, Quinn, Morgan, Kinsella, O’Callaghan, Owens and Waddington2002; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Baldwin et al., Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O’Callaghan and Waddington2005; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992) out of eight, with a median of five (interquartile range [IQR]: 4–6; see Supplemental Table 5). Only one criterion was met by all studies: ‘a. Defined catchment area’, while the criterion met least often (N = 6; 26.1%) was ‘i. reporting crude and standardised rates’.

Variation in incidence rates by individual characteristics

All first episode psychotic disorders

Figure 2. Crude incidence rate per 100,000 person-years of selected psychotic outcomes in the Republic of Ireland, overall and by sex. Legend: 100 kpy: 100,000 person-years. (A) All psychotic disorders; (B) All psychotic disorders, by sex; (C) Non-affective psychotic disorders; (D) Non-affective psychotic disorders, by sex.

Five principal citations (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Kelly et al., Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992) provided FEP incidence data separately for men and women, with evidence of higher rates for men than women (Fig. 2b). For example, Nkire et al. (Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021) reported the incidence rate ratio [IRR] for all clinically relevant psychotic disorders to be 1.3 times higher in men than women (95%CI: 1.1–1.6), while Fayyaz et al. (Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021) reported a greater crude IRR of 2.1 (95%CI: 1.4–3.1). Study quality was high (at least 6 out of 8; Table 1).

We failed to identify any citation which had published incidence rates by age group, although Omer et al. (Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014) reported incidence rate ratios by age group in Cavan and Monaghan, with highest rates for men aged 15–34, although no statistically significantly differences by age for women were observed. Further data on median age-at-onset in these studies is given in the Supplemental Results section.

One citation reported FEP incidence rates by migrant status and region-of-birth (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021), from the DETECT EIP service in South Dublin and Wicklow. Although no overall difference in FEP incidence was observed between migrant and Irish-born groups (IRR: 1.02; 95%CI: 0.83–1.24), subgroup analyses found rates were 1.83 (95%CI: 1.11–3.02) times higher for people born in Africa than Ireland.

Non-affective psychotic disorders

Eleven citations provided data on the overall incidence of non-affective psychotic disorders in Ireland (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; Scully et al., Reference Scully, Quinn, Morgan, Kinsella, O’Callaghan, Owens and Waddington2002; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Baldwin et al., Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O’Callaghan and Waddington2005; Morgan et al., Reference Morgan, Scully, Quinn, Kinsella, Owens and Waddington2001; Waddington et al., Reference Waddington, Baldwin, Morgan, Quinn, Scully and Kinsella2004; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella, Owens, O’Callaghan and Waddington2003; Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014; Browne et al., Reference Browne, Scully, Quinn, Morgan, Baldwin, Kinsella, Owens, O’Callaghan and Waddington2005; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014), of which four principal citations provided the most relevant data (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014). These studies were conducted in Dublin (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992), Wicklow (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021), Cavan and Monaghan (Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014) and Carlow, Westmeath and Roscommon (Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987). We observed heterogeneity in rates (Fig. 2c), from around 10–11 new cases per 100,000 person-years in two good quality studies (6 (Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021) or 7 (Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992) out of 8) in Dublin (N = 35 cases, 15–54 years (Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992)) and Cavan-Monaghan (N = 132 cases, 15+ years) (Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021) to 36.6 per 100,000 person-years in the 3-county study (quality: 4 of 7, N = 34 cases, 15–64 years) (Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987). Finally, in the most recent and largest (N = 443) study identified, we derived the incidence of non-affective psychotic disorders from the DETECT EIP service in South Dublin and Wicklow (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021) as 19.2 (95%CI: 17.4–21.1) per 100,000 person-years (quality: 6 of 8, 16–64 years).

Three principal citations (Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014) reported higher point estimates of rates in men than women (Fig. 2d), albeit with overlapping confidence intervals, where provided (Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014). Only one citation (Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987) (the Three-County study) reported rates by age, finding no evidence of differences in this small study (Supplemental Figure 2a).

One citation provided rates by migrant status and region-of-birth (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021). As described above, no overall differences by migrant status were observed, but rates were higher for migrants born in Africa compared with Ireland (IRR: 1.78; 95%CI: 1.00–3.18; p = 0.049).

Schizophrenia

We identified 16 citations (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Scully et al., Reference Scully, Quinn, Morgan, Kinsella, O’Callaghan, Owens and Waddington2002; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Keatinge Reference Keatinge1986; Baldwin et al., Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O’Callaghan and Waddington2005; Morgan et al., Reference Morgan, Scully, Quinn, Kinsella, Owens and Waddington2001; Keatinge Reference Keatinge1987; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella and O’Callaghan2002; Kingston et al., Reference Kingston, Owoeye, Kinsella, Russell, O’Callaghan, Waddington and Ritsner2011; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella, Owens, O’Callaghan and Waddington2003; Owoeye et al., Reference Owoeye, Kingston, Scully, Baldwin, Browne, Kinsella, Russell, O’Callaghan and Waddington2013; Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014; Keatinge Reference Keatinge1988l; Browne et al., Reference Browne, Scully, Quinn, Morgan, Baldwin, Kinsella, Owens, O’Callaghan and Waddington2005; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992), including seven principal citations (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Keatinge Reference Keatinge1986; Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014; Keatinge Reference Keatinge1988; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992) on the overall incidence of schizophrenia. We rated study quality as high (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992) or medium (Keatinge Reference Keatinge1986; Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014; Keatinge Reference Keatinge1988; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987). These seven citations provided nine overall incidence rates of schizophrenia (with data from the Monaghan and Waterford (Keatinge Reference Keatinge1988), and Clare and Wexford (Keatinge Reference Keatinge1986) citations disaggregated by county). Incidence rates ranged from 6.4 (95%CI: 5.2–8.0) in Cavan-Monaghan (Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021) to 57.0 (95%CI: 41.5–77.8) per 100,000 person-years in Waterford (Keatinge Reference Keatinge1988), representing an almost 9-fold variation.

We estimated the pooled incidence of schizophrenia as 20.0 per 100,000 person-years (95%CI: 10.6–37.5; Fig. 3), despite very high heterogeneity between estimates (I²: 97.6%), from eight estimates of incidence provided by six of the seven citations identified here (Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Keatinge Reference Keatinge1986; Keatinge Reference Keatinge1988; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992); one citation could not be included as no standard error was derivable (Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014). In a random effects meta-regression, higher study quality was associated with lower incidence of schizophrenia (p < 0.001; Fig. 4). We found no evidence of ’small study effects’ (Supplemental Figure 3; Egger’s test p = 0.77).

Figure 3. Forest plot of the incidence of schizophrenia in the Republic of Ireland, 1974–2016. Legend: 100 kpy: 100,000 person-years. The citation from Keatinge which reported data from ‘Likely Monaghan’ and ‘Likely Waterford’ is included despite the author not explicitly reporting the catchment areas of this study, only that the study took place in two Irish counties. However in that publication, the author does acknowledge the two hospitals involved in the data collection for this study, which can be traced back to the counties of Monaghan and Waterford, respectively.

Figure 4. Correlation between study quality and (log) incidence of schizophrenia in the Republic of Ireland, 1974–2016. Legend: 100 kpy: 100,000 person-years. The figure indicates strong, statistically significant (p = 0.04) negative correlation between (higher) study quality (x-axis) and (lower) (log) incidence of schizophrenia.

Five principal citations reported incidence rates of schizophrenia separately for men and women (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987; Kelly et al., Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992), with higher point estimates consistently found for men (Supplemental Figure 4); two recent citations from separate samples in Cavan and Monaghan, including the CAMFEPS study (Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021) (IRR: 3.1; 95%CI: 1.9–5.2) and COPE EIP service (IRR: 3.3; 95%CI: 1.6–7.0) reported rates that were three times higher for men than women.

Although three principal citations reported the number of new cases of schizophrenia by age group (Keatinge Reference Keatinge1986; Keatinge Reference Keatinge1988; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987), only one provided accompanying estimates of incidence (Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987), and this was underpowered to detect trends by age (Supplemental Figure 2b).

Affective psychotic disorders

We identified two principal citations (and five further non-principal citations from the same studies (Scully et al., Reference Scully, Owens, Kinsella and Waddington2004; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Baldwin et al., Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O’Callaghan and Waddington2005; Morgan et al., Reference Morgan, Scully, Quinn, Kinsella, Owens and Waddington2001; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella, Owens, O’Callaghan and Waddington2003; Browne et al., Reference Browne, Scully, Quinn, Morgan, Baldwin, Kinsella, Owens, O’Callaghan and Waddington2005)) which provided data to derive incidence rates of affective psychotic disorders (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014). In recent data from the DETECT EIP service in South Dublin and Wicklow (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021), we derived the crude incidence as 6.4 cases per 100,000 person-years (95%CI: 5.5–7.6), using data ascertained between 2006 and 2014. From the principal Cavan-Monaghan citation (Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014), using data ascertained between 1995-2007, we derived a slightly higher crude incidence of 9.5 cases per 100,000 person-years (95%CI: 8.0–11.3) in people aged 16 and older (Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014).

Two unique citations provided rates separately for men and women (Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014). Derived rates from the CAMFEPS were similar for men (9.2; 95%CI: 7.2–11.8) and women (9.8; 95%CI: 7.6–12.6), as well as in published data from a separate study conducted in South Dublin and the Cavan-Monaghan region (Kelly et al., Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010).

We did not identify any study which had published rates of affective psychotic disorders by age. One citation provided rates by migrant status and region-of-birth (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021), but found no differences in a small sample of cases (N = 33).

Bipolar disorders with psychotic features

Three unique citations (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Daly et al., Reference Daly, Webb and Kaliszer1995) from 11 reports containing overlapping data (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Baldwin et al., Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O’Callaghan and Waddington2005; Morgan et al., Reference Morgan, Scully, Quinn, Kinsella, Owens and Waddington2001; Daly et al., Reference Daly, Webb and Kaliszer1995; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella and O’Callaghan2002; Waddington et al., Reference Waddington, Baldwin, Morgan, Quinn, Scully and Kinsella2004; Kingston et al., Reference Kingston, Owoeye, Kinsella, Russell, O’Callaghan, Waddington and Ritsner2011; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella, Owens, O’Callaghan and Waddington2003; Owoeye et al., Reference Owoeye, Kingston, Scully, Baldwin, Browne, Kinsella, Russell, O’Callaghan and Waddington2013; Browne et al., Reference Browne, Scully, Quinn, Morgan, Baldwin, Kinsella, Owens, O’Callaghan and Waddington2005) provided incidence rates on bipolar disorders or mania separately. First admission rates of mania in Dublin South Central between 1975 and 1981 for people aged 18–60 years old were reported as 8.2 per 100,000 person-years (95%CI: 5.6–11.9), although a lower figure was reported for people aged 15 years and older (4.5; 95%CI: 3.1–6.5) (Daly et al., Reference Daly, Webb and Kaliszer1995). In Cavan and Monaghan, the incidence of Bipolar I Disorders between 1995 and 2010 was estimated as 6.9 per 100,000 person-years (95%CI: 5.6–8.5) for people aged 15 years and older (Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021). A more recent estimate of the incepted rate of Bipolar I Disorders from the COPE EIP service in this area (2012–2016) reported a lower estimate of 2.8 cases per 100,000 person-years (95%CI: 1.6–4.8) (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021). All citations reported similar rates for men and women.

One study (Daly et al., Reference Daly, Webb and Kaliszer1995) reported first admission rates of mania by age group, with higher rates in younger age groups (18–19, 20-29 years). This study also reported gradients by social class, with higher point estimates of incidence in people from lower social classes (groups V and VI: 8.2 per 100,000 person-years; 95%CI: 4.5–14.8) compared with social class groups I and II (4.7; 95%CI: 2.4–9.0) and III and IV (4.5; 95%CI: 2.4–8.4), though the small sample sizes precluded any conclusions being drawn.

Depression with psychotic features

We identified two unique citations (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021) from nine overlapping reports (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Baldwin et al., Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O’Callaghan and Waddington2005; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella and O’Callaghan2002; Waddington et al., Reference Waddington, Baldwin, Morgan, Quinn, Scully and Kinsella2004; Kingston et al., Reference Kingston, Owoeye, Kinsella, Russell, O’Callaghan, Waddington and Ritsner2011; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella, Owens, O’Callaghan and Waddington2003; Owoeye et al., Reference Owoeye, Kingston, Scully, Baldwin, Browne, Kinsella, Russell, O’Callaghan and Waddington2013; Browne et al., Reference Browne, Scully, Quinn, Morgan, Baldwin, Kinsella, Owens, O’Callaghan and Waddington2005) which provided data on the incidence of depression with psychotic features. Both were conducted in the Cavan-Monaghan region, in either the CAMFEPS epidemiological study (1995–2010) (Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021) or the COPE EIP service (2012–2016) (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021). Both studies estimated similar incidence/incepted rates of depression with psychotic features (CAMFEPS, 15 years and older: 7.3 per 100,000 person-years; 95%CI: 6.0–8.9. COPE EIP service, 16 years and older: 5.6; 95%CI:3.8–8.2). Neither study found statistically significant difference in rates for men and women.

Substance-induced psychotic disorders

The same two citations (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021) provided unique data on the incidence of substance-induced psychotic disorders, from four overlapping citations (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Kingston et al., Reference Kingston, Owoeye, Kinsella, Russell, O’Callaghan, Waddington and Ritsner2011; Owoeye et al., Reference Owoeye, Kingston, Scully, Baldwin, Browne, Kinsella, Russell, O’Callaghan and Waddington2013). In CAMFEPS, incidence was estimated as 2.0 per 100,000 person-years (95%CI: 1.4–3.0) (Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021), with a similar rate reported in the COPE EIP service (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021) (3.2; 95%CI: 1.9–5.3). Both studies reported substantially higher rates for men than women (IRR_CAMFEPS: 7.0; 95%CI: 2.1–23.4, IRR_COPE: 13.9; 95%CI: 1.8–105.7), albeit with imprecision around these estimates.

Other psychotic outcomes

See Supplemental Results.

Variation in incidence rates by area-level characteristics

We identified four principal citations (O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Keatinge Reference Keatinge1988; Kelly et al., Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014) and one overlapping citation (Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2012) which reported the incidence of any psychotic disorder outcome by area-level characteristics, including socioeconomic deprivation (O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014), social fragmentation (O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014), population density (O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016), or rural-urban classification (Keatinge Reference Keatinge1988; Kelly et al., Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014). Three of the four studies, all rated as high quality (6 or 7 out of 8) were published since 2010 (O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Kelly et al., Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014), with one older, lower quality (4 out of 8) study published in 1988 (Keatinge Reference Keatinge1988); this study reported overlapping first admission rates of schizophrenia in rural Monaghan (51.0 per 100,000 person-years; 95%CI: 39.1–66.6) and more urban Waterford (57.0; 95%CI: 41.7–78.0).

Kelly et al. (Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010) reported first admission rates of various psychotic outcomes between 1995 and 2001 in a rural setting (Cavan-Monaghan) and an urban setting (South Dublin), and found higher crude rates of schizophrenia in men (IRR: 1.92; 95%CI: 1.52–2.44) and women (IRR: 1.34; 95%CI: 1.00–1.80) living in urban areas. By contrast, crude rates of affective psychotic disorders appeared lower in the urban setting (IRR_men: 0.48; 95%CI: 0.34–0.67) and women (IRR_women: 0.60; 95%CI: 0.43–0.83).

In Cavan and Monaghan, Omer et al. (Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014) found sex-specific effects of place on the incidence of all psychotic disorders, such that women living in the most urban (IRR: 1.34; 95%CI: 1.03–1.73) and most social fragmented (IRR: 1.72; 95%CI: 1.33–2.24) parts of the region had higher rates. By contrast, these effects were not observed for men, but their rates were higher in the most deprived part of the region (IRR: 1.58; 95%CI: 1.25–2.01). Following multivariable adjustment only material deprivation remained associated with increased rates of psychotic disorder (IRR per standard deviation increase in deprivation: 1.13; 95%CI: 1.03–1.24) in this sample. This finding accords with further evidence from the DETECT service, which reported that age-standardised incidence rates of FEP were 3.43 times higher in the most-versus-least deprived quartile (95%CI: 1.24–7.75). Partial evidence (third vs first quartile) of increased rates in more socially fragmented areas was also observed (IRR: 2.40; 95%CI: 1.05–5.51) (O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016). No statistically significant variation by population density or social capital was observed, although we noted a trend-level association in incidence between quartiles with the highest and lowest levels of social capital (IRR: 1.43; 95%CI: 0.99–2.06). Similarly to Omer et al. (Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014), findings from DETECT indicated a stronger effect for deprivation on FEP rates in men, and a stronger effect for social capital on FEP rates in women.

Discussion

Principal findings

We identified 23 citations which met criteria for our systematic review of the incidence of psychotic disorders in Ireland, published between 1950 and 2021. Although our review highlights heterogeneity in estimates of various psychotic disorders in Ireland, some consistent trends emerged. For example, three out of four principal citations reported the overall incidence of psychotic disorders to be between 22 and 25 per 100,000 person-years in working age adults up to 65 years old, including in two recent studies based on incepted rates via EIP services in rural and more urban parts of Ireland (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021). Only one study, based on a population-based case finding approach over a 15-year period in people aged 15 years and older, reported higher rates in the rural Cavan-Monaghan region of 34.1 per 100,000 person-years (Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021). Nonetheless, this apparent variation falls within internationally reported estimates. For example, the lower estimates are consistent with pooled rates reported in the most recent systematic review of the international literature since 2002 (26.6 per 100,000 person-years) (Jongsma et al., Reference Jongsma, Turner, Kirkbride and Jones2019). Meanwhile, the upper figure from Cavan and Monaghan is consistent with pooled estimates in England for working aged adults (16–64 years old; 31.7 per 100,000 person-years) (Kirkbride et al., Reference Kirkbride, Errazuriz, Croudace, Morgan, Jackson, Boydell, Murray and Jones2012; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016).

In our review, we identified sufficient data to pool the overall incidence of schizophrenia in Ireland, estimated as 20.0 per 100,000 person-years (95%CI: 10.6–37.5; N = 8 settings). This is similar to the latest available estimate reported in the international systematic review (18.6; 95%CI: 15.1–22.9) (Jongsma et al., Reference Jongsma, Turner, Kirkbride and Jones2019; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021). Fewer studies in Ireland had published rates of affective psychotic disorders, but available data placed rates between 6-10 per 100,000 person-years. This range falls between a slightly lower figure reported in the latest international review (4.6; 95%CI: 3.1–6.8) (Jongsma et al., Reference Jongsma, Turner, Kirkbride and Jones2019; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021) and a higher figure reported from a review of English studies (12.4; 95%CI:9.0–17.1) (Kirkbride et al., Reference Kirkbride, Errazuriz, Croudace, Morgan, Jackson, Boydell, Murray and Jones2012; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016). Data on the incidence of substance-induced psychoses in Ireland were sparse, but where available, were very low.

We found consistent evidence of higher rates of most psychotic outcomes in men versus women, although affective psychotic disorders occurred more equally, again consistent with the wider literature (Jongsma et al., Reference Jongsma, Turner, Kirkbride and Jones2019; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Kirkbride et al., Reference Kirkbride, Errazuriz, Croudace, Morgan, Jackson, Boydell, Murray and Jones2012). Very few studies in our review published incidence data by age, and no studies reported incidence by ethnicity, with only one recent study (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021) reporting rates by migrant status and region- and country-of-birth. Finally, limited available evidence in Ireland (O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Keatinge Reference Keatinge1988; Kelly et al., Reference Kelly, O’Callaghan, Waddington, Feeney, Browne, Scully, Clarke, Quinn, McTigue, Morgan, Kinsella and Larkin2010; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014) found support for an association between higher levels of deprivation and social fragmentation and greater psychosis rates, in studies which included both rural (Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2014) and more urban (O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016) catchment areas. There was no clear evidence that population density or urban-rural status was associated with incidence.

Meaning of the findings

Our systematic review is drawn from a longstanding tradition of high quality epidemiological studies of the incidence of psychotic disorders in Ireland since the late 1970s. Notably, over half of the identified citations are based on the population of Cavan and Monaghan, providing a rich characterisation of the incidence (and in other reports, prevalence (Youssef et al., Reference Youssef, Kinsella and Waddington1991; Scully et al., Reference Scully, Owens, Kinsella and Waddington2004)) of psychotic disorders in one rural part of Ireland. One possible reason for the higher incidence rates observed in this region than elsewhere could be that the CAMFEPS study used epidemiological principles and true community case finding to ascertain cases all cases occurring in the population, regardless of help-seeking. A further 26% of works were conducted in parts of Dublin, providing evidence from a contrasting, urban setting. These data have the potential to inform planning need for care in EIP services in Ireland, particularly with the availability of recent data on the incepted rate of psychotic disorders published from the COPE (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021) and DETECT (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016) EIP services operating in these catchments, respectively. Similar initiatives have provided evidence-based predictions of future need for EIP care in England (McDonald et al., Reference McDonald, Ding, Ker, Dliwayo, Osborn, Wohland, Coid, French, Jones, Baio and Kirkbride2021; Kirkbride et al., Reference Kirkbride, Jackson, Perez, Fowler, Winton, Coid, Murray and Jones2013), which are currently incorporated in official guidelines from the National Institute of Health and Clinical Excellence [NICE] to inform service planning and commissioning (NHS England, 2016; NHS England 2020).

Despite this, we observed less evidence about the incidence in other parts of Ireland, for some diagnostic outcomes including affective psychotic disorders and substance use disorders, and by some important characteristics (including age, ethnicity and migrant status). Future studies could address these gaps to build a more complete epidemiological understanding of psychosis in Ireland.

We identified only one study, published in 2021, which presented data on the incidence of psychotic disorders in different groups by migrant status and region-of-birth (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021). While there was no overall evidence that migrants had elevated rates of FEP (including non-affective and affective psychotic disorders separately), there was some evidence of heterogeneity by country-of-birth, with the most robust finding that rates were approximately doubled in people born in Africa compared with the Irish-born population. This effect size is somewhat lower than reported for people of Black African or Black Caribbean heritage consistently reported in studies in England (Kirkbride et al., Reference Kirkbride, Errazuriz, Croudace, Morgan, Jackson, Boydell, Murray and Jones2012; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016), including in rural populations (Kirkbride et al., Reference Kirkbride, Hameed, Ioannidis, Ankireddypalli, Crane and Nasir2017), where rates are typically reported to be between 4-6 times greater than the White or White British comparison group. Although several explanations for this discrepancy are possible, it is worth noting that the findings in Ireland (by region-of-birth) may not be directly comparable with findings elsewhere based on ethnicity. As the Irish population becomes increasingly ethnically diverse, it will be important to precisely delineate psychosis risk by ethnicity in the future, and data from the 2022 Census will provide information about the extent of ethnic diversity in the country (the proportion of the population identifying as White Irish has decreased from 87.6% in the 2006 Census (Central Statistics Office, 2006) to 82.2% in 2016 (Central Statistics Office 2021)). This important issue emphasises the need to understand the intersectional roles of ethnicity, migrancy and region-of-origin in the aetiopathology of psychotic disorders.

To some extent the findings of our review accord with the international literature on the incidence of psychotic disorders and socioenvironmental factors in Global North contexts. Both deprivation (Croudace et al., Reference Croudace, Kayne, Jones and Harrison2000; Richardson et al., Reference Richardson, Hameed, Perez, Jones and Kirkbride2018; Lewis et al., Reference Lewis, Dykxhoorn, Karlsson, Khandaker, Lewis, Dalman and Kirkbride2020; Kirkbride et al., Reference Kirkbride, Jones, Ullrich and Coid2014) and social fragmentation (Allardyce et al., Reference Allardyce, Gilmour, Atkinson, Rapson, Bishop and McCreadie2005) have been consistently associated with the incidence of (at least) non-affective psychotic disorders. Interestingly, the non-linear association between deprivation and psychosis risk observed in the DETECT catchment by O’Donoghue et al. (Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021) (with elevated risk confined to the most deprived group only) has been reported frequently elsewhere (Croudace et al., Reference Croudace, Kayne, Jones and Harrison2000; Richardson et al., Reference Richardson, Hameed, Perez, Jones and Kirkbride2018). This suggests that a threshold of deprivation may exist, after which presentations for new onset cases of psychosis begin to increase in rate. While population density has also been longitudinally and cross-sectionally associated with the incidence of psychotic disorders in some (Richardson et al., Reference Richardson, Hameed, Perez, Jones and Kirkbride2018; Lewis et al., Reference Lewis, Dykxhoorn, Karlsson, Khandaker, Lewis, Dalman and Kirkbride2020; Kirkbride et al., Reference Kirkbride, Jones, Ullrich and Coid2014), but not all (Kirkbride et al., Reference Kirkbride, Morgan, Fearon, Dazzan, Murray and Jones2007) studies outside of the Republic of Ireland, no consistent gradient emerged in the limited data identified on this issue in this review.

Limitations

To our knowledge this was the first systematic review to examine the incidence of psychotic disorders in the Republic of Ireland. We prospectively registered our systematic review methodology and conformed to the PRISMA guidelines. Nonetheless, we acknowledge some limitations of our review. We restricted data and papers to published material identified via four major scientific databases, which may have omitted grey or unpublished data. Nonetheless, we identified rare works including PhD theses on this topic (Keatinge Reference Keatinge1986). Together with the absence of evidence of small study effects, this suggests that the number of omitted citations from this review was small. We also contacted authors of some included works, which led to the identification and inclusion of two recently published papers not identified during our original search (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021). We recommend caution in interpreting rates from the recent COPE EIP service (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021) alongside other rates reported in this study; findings from COPE are reported as ‘incepted’ rather than ‘incidence’ rates, given that (unlike the earlier CAMFEPS study in the same region) rates were based on the number of new cases taken on by the EIP team, which may not be the same as the total number of new cases arising in this population.

One major limitation of our review was the marked heterogeneity and low number of studies generally available for any single outcome reported here. Moreover, we note that higher quality studies tended to report lower incidence rates of schizophrenia. Thus, the heterogeneity identified in this review may be explained by several factors, including differing age ranges of the studies, differences in case finding procedures, or stochastic variation. To mitigate against these issues, we relied on a narrative synthesis rather than meta-analysis.

We also note that 19 of the 23 citations included in this review were based on studies which collected data prior to (and including) 2010. Only four citations have provided more recent data on the incidence of psychotic disorder in Ireland, with the latest based on data up until 2016 (Fayyaz et al., Reference Fayyaz, Nkire, Nwosu, Amjad, Kinsella, Gill, McDonough, Russell and Waddington2021). We also noted that better study quality was strongly correlated with reporting of lower rates of schizophrenia (Fig. 4). While we found no formal evidence of small study effects (including publication bias), the Egger’s test may be underpowered when few data points (N = 8) are available. Together, these findings call for ongoing, high quality epidemiological studies of the incidence of psychotic disorder in Ireland. Importantly, these studies should collect a core set of minimum data aligned to age, sex/gender, ethnicity, migration and deprivation/urbanisation to allow precise characterisation of need for care for psychosis across the country. Although our review focussed on the adult age range, 16–64 years old, the lowest age range for any study included in our review was 15 years old (Scully et al., Reference Scully, Owens, Kinsella and Waddington2004; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021; Keatinge Reference Keatinge1986; Baldwin et al., Reference Baldwin, Browne, Scully, Quinn, Morgan, Kinsella, Owens, Russell, O’Callaghan and Waddington2005; Morgan et al., Reference Morgan, Scully, Quinn, Kinsella, Owens and Waddington2001; Omer et al., Reference Omer, Kirkbride, Pringle, Russell, O’Callaghan and Waddington2012; Keatinge Reference Keatinge1987; Daly et al., Reference Daly, Webb and Kaliszer1995; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella and O’Callaghan2002; Waddington et al., Reference Waddington, Baldwin, Morgan, Quinn, Scully and Kinsella2004; Kingston et al., Reference Kingston, Owoeye, Kinsella, Russell, O’Callaghan, Waddington and Ritsner2011; Baldwin et al., Reference Baldwin, Scully, Quinn, Morgan, Kinsella, Owens, O’Callaghan and Waddington2003; Owoeye et al., Reference Owoeye, Kingston, Scully, Baldwin, Browne, Kinsella, Russell, O’Callaghan and Waddington2013; Keatinge Reference Keatinge1988; Browne et al., Reference Browne, Scully, Quinn, Morgan, Baldwin, Kinsella, Owens, O’Callaghan and Waddington2005; Ninuallain et al., Reference Ninuallain, O’Hare and Walsh1987; Jablensky et al., Reference Jablensky, Sartorius, Ernberg, Anker, Korten and Cooper1992), highlighting the paucity of evidence on psychosis incidence during childhood and early adolescence. Finally, our quality criteria were designed by the authors, adapted from previously published systematic reviews (Kirkbride et al., Reference Kirkbride, Errazuriz, Croudace, Morgan, Jackson, Boydell, Murray and Jones2012; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016). They may not necessarily reflect all criteria that other stakeholders in the field consider vital or relevant, and future work could explore this issue.

Conclusion

The epidemiological data identified here is broadly consistent with the wider international literature in understanding variation in the incidence of psychotic disorders. Rates were broadly higher for men, younger people – and in the one published study in Ireland on the topic to date (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021) – certain migrant groups, most notably those born in Africa. Rates were also increased in more deprived and socially fragmented communities. These findings have implications for public mental health in Ireland, since they can potentially facilitate and inform accurate resource allocation for the delivery of EIP services, as well as other primary and secondary healthcare services involved in care for those experiencing psychosis. Future efforts to continually monitor changes in the incidence of psychotic disorders in Ireland will help inform accurate, effective and timely public health responses. The continued rollout of EIP services in Ireland is providing new data and information about the epidemiology of psychotic disorders, as evidenced by recent publications from the DETECT service in South Dublin and County Wicklow (O’Donoghue et al., Reference O’Donoghue, Lyne, Roche, Mifsud, Renwick, Behan and Clarke2021; O’Donoghue et al., Reference O’Donoghue, Lyne, Renwick, Lane, Madigan, Staines, O’Callaghan and Clarke2016; Lyne et al., Reference Lyne, Renwick, O’Donoghue, Madigan, Kinsella and Turner2014). Combining these evidence-based services with rigorous epidemiological intelligence available in Ireland (Nkire et al., Reference Nkire, Scully, Browne, Baldwin, Kingston, Owoeye, Kinsella, O’Callaghan, Russell and Waddington2021), will lead to actionable insights to inform the delivery of effective, early intervention for psychosis services in local communities according to population need.

Supplementary material

The supplemental material for this article can be found at https://doi.org/10.1017/ipm.2023.35.

Acknowledgements

We are grateful to Professors John Waddington and Mary Clarke, and Dr Brian O’Donoghue for providing additional data during the review searches.

Competing interests

TD, GB, JBK received consultancy fees from the Health Services Executive, Ireland, to conduct this systematic review, as part of a wider project to predict the incidence of psychotic disorders in Ireland using statistical modelling. HSE were not involved in the design, conduct, drafting or final decision to approve this work for peer-reviewed academic publication. The views contained in this publication are not the views of HSE. No other conflicts of interest are declared.

Ethical standard

The authors assert that all procedures contributing to this work comply with the ethical standards of the relevant national and institutional committee on human experimentation and with the Helsinki Declaration of 1975, as revised in 2008. No specific ethical approval was required due to the secondary nature of this work.

Financial support

JBK is supported by the UCLH National Institute of Health Research Biomedical Research Centre. TD, GB, JBK received consultancy fees from the Health Services Executive, Ireland, to conduct this systematic review, as part of a wider project to predict the incidence of psychotic disorders in Ireland using statistical modelling.

Preprint information

A preprint version of this manuscript, supplemental materials, data extraction template, detailed screening decision-making, and extracted data can be found on PsyArXiv at: 10.31234/osf.io/dhfys

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Figure 1. PRISMA flow diagram of search strategy.

Table 1. Overview of included citations on the incidence of psychotic disorders in Ireland

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Article contents

The incidence of psychotic disorders in the Republic of Ireland: a systematic review

Abstract

Keywords

Introduction

Methods

Eligibility criteria

Information sources and search strategy

Study selection

Data extraction

Diagnostic outcomes

Methodological quality and risk of bias of included studies

Data synthesis

Results

Study selection

Study characteristics

Risk of bias within studies

Variation in incidence rates by individual characteristics

All first episode psychotic disorders

Non-affective psychotic disorders

Schizophrenia

Affective psychotic disorders

Bipolar disorders with psychotic features

Depression with psychotic features

Substance-induced psychotic disorders

Other psychotic outcomes

Variation in incidence rates by area-level characteristics

Discussion

Principal findings

Meaning of the findings

Limitations

Conclusion

Supplementary material

Acknowledgements

Competing interests

Ethical standard

Financial support

Preprint information

References

Jacinto et al. supplementary material

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