Real-World Evidence of the Clinical and Economic Impact of Long-Acting Injectable Versus Oral Antipsychotics Among Patients with Schizophrenia in the United States: A Systematic Review and Meta-Analysis

A systematic literature review was conducted by searching MEDLINE^® and MEDLINE In-Process & Other Citations through the OvidSP interface. The search strategy included a combination of terms to identify schizophrenia, medications indicated for the treatment of schizophrenia, and outcomes of interest. The complete search strategy and screening criteria for the electronic search are presented in Online Resource Table S1 (see the electronic supplementary material). Additional relevant abstracts and posters from recent key congresses were added manually to supplement the electronic search.

Peer-reviewed English language articles published between January 1, 2010 and February 10, 2020 (date of the electronic search) were screened for eligibility. Publications were retained if they met the following inclusion criteria: (1) conducted in a real-world setting (i.e., retrospective administrative claims analyses, retrospective chart review studies, pragmatic trials), (2) included adult patients with schizophrenia, (3) had at least one patient treated in the US, (4) reported at least one outcome of interest, and (5) reported these outcomes comparatively among patients treated with LAI versus OA (two-cohort design) or in the same group of patients before versus after initiation of an LAI (mirror-image design). Since the clinical endpoints of interest were expected to vary a lot across different countries’ healthcare systems, the research was restricted to studies that included patients treated in the US. In addition, only articles published on or after 2010 were retained as treatment patterns prior to 2010 were expected to be meaningfully different, notably through the less prevalent use of LAI.

The clinical endpoints of interest were all-cause hospitalizations and ER admissions. In addition, all-cause healthcare costs and medication adherence were reported. All-cause healthcare costs included medical, pharmacy, and total costs. Adherence to the medication of interest (i.e., LAI or OA) was evaluated using the proportion of days covered (PDC).

Two reviewers (IG and HN) independently assessed each publication for inclusion based on the aforementioned inclusion criteria. Following inclusion, each reviewer independently extracted data, including study design, interventions, sample characteristics, and outcomes, in an Excel-based data extraction grid. All information was taken from the published articles, and authors of the original publications were not contacted. Both extractions were reconciled. Discrepancies in the selection and extraction processes were reviewed and resolved by a third adjudicator (PT-L).

Descriptive statistics including means, medians, and standard deviations (SDs) were extracted for continuous outcomes, while counts and proportions were extracted for binary outcomes. When available in the source publications, odds ratios (ORs) were extracted for binary outcomes, incidence rate ratios (IRRs) were extracted for count outcomes, and mean differences (MDs) were extracted for continuous outcomes.

Because of the heterogeneous study designs and various outcomes of interest included in the scope of this review, a quality assessment exercise was not performed. Rather, a qualitative appraisal of the potential sources of heterogeneity was conducted [43].

Meta-analyses were conducted to evaluate the association of LAI versus OA use on hospitalizations, ER admissions, healthcare costs, and medication adherence. Hospitalizations and ER admissions during the 12-month period following the initiation of an LAI or an OA were analyzed through the number of admissions (12-month pooled IRR) and the odds of having at least one admission (12-month pooled OR). Pharmacy, medical, and total costs per patient per year (PPPY) were analyzed through the cost difference between treatment arms (12-month pooled MD). Adherence was analyzed through the difference in PDC between treatment arms (12-month pooled MD) and the odds of having a PDC ≥ 80% (12-month pooled OR).

Given the substantial heterogeneity expected between studies, DerSimonian and Laird random effects models were conducted using STATA 16 statistical package (StataCorp LP, College Station, TX, USA). Effect sizes (i.e., ORs, IRRs, and MDs) and confidence intervals (CIs) reported in the source publications were inputted directly in the meta-analyses, when available. For source publications that only reported descriptive statistics, effect sizes and CIs were estimated [44‐46].

Among all studies meeting inclusion criteria and reporting outcomes of interest, it happened that multiple publications reported the same outcome from the same data source covering a similar time frame (e.g., cited the same Medicaid or commercial claims insurance database for similar years). Therefore, to avoid the inclusion of overlapping samples, the most representative publication was retained for the meta-analysis based on the following criteria: studies of general schizophrenia populations were prioritized over studies of specific subsets of patients with schizophrenia; studies of LAI overall were prioritized over studies of a single, specific LAI; studies with a cohort design (i.e., LAI vs OA) were prioritized over mirror-image studies (i.e., before vs after LAI initiation).

A sensitivity analysis was performed whereby meta-analyses were conducted on studies for which LAI was paliperidone palmitate once monthly (PP1M), exclusively, which was the most common LAI among the publications identified and which had previously been found to be used by the majority of patients initiating a second-generation LAI [47].

A total of 1083 articles were identified by the electronic literature search, and subsequently, two publications presented at relevant conferences at the time that the analysis was conducted were manually added. Partial content was available at the time of the electronic search, and these two studies have since been published as full manuscripts: Zhdanava [48], and Patel [49]). Of these, 57 articles were retained for data extraction (Fig. 1). In total, 25 publications reported at least one outcome of interest for inclusion in meta-analyses. One of these publications presented results on two separate populations (Offord [20], presented outcomes among commercially insured patients and Medicare patients, separately) (Table 1).

Studies were published between 2013 and 2020, and the data included ranged between 2005 and 2018. Study types included 21 retrospective cohort studies (84%), three pre-post studies (12%), and one pragmatic trial (4%). Among retrospective cohort studies (n = 21), methods of adjustment to control for confounding included multivariable regressions (n = 7, 33%), inverse probability of treatment weighting (n = 6, 29%), matching based on propensity scores (n = 4, 19%), and use of multiple techniques (n = 2, 10%), and two studies (10%) did not specify whether methods of adjustment were used.

Data sources included Medicaid (14 studies/25, 56%), data from the Veterans Health Administration (VHA) (4/25, 16%), other administrative claims databases (4/25, 16%), and other data types (3/25, 12%).

Sample size varied widely, ranging between 24 [50] and 45,625 [30]. The proportion of females in the publications was noticeably lower (10% or less) in studies using data from the VHA and in one chart review study on cannabis users [50]. Patients’ mean ages among studies using Medicaid data were in the late-thirties and forties, and in the early fifties among studies using VHA data.

Additional details on study designs and samples are available in Online Resource Table S2 and Online Resource Table S3 (see the electronic supplementary material).

Fifteen studies reported on rates of hospitalization (Online Resource Table S4B). Among the eight studies that were included in the meta-analysis (one of which reported outcomes on two separate samples of patients [20]), patients initiated on an LAI had 25% fewer all-cause hospitalizations (IRR [95% CI] 0.75 [0.65–0.88], n = 9; Fig. 2).

Thirteen studies reported the rate of ER visits following initiation of an LAI compared with an OA (Online Resource Table S4D). Among the six studies that were included in the meta-analysis, patients initiated on an LAI had 14% fewer all-cause ER admissions (IRR [95% CI] 0.86 [0.77–0.97], n = 6; Fig. 3).

Fifteen studies reported total costs following the initiation of an LAI compared with an OA (Online Resource Table S4E; see the electronic supplementary material). Among the seven studies included in the meta-analysis, there was no significant difference in total all-cause healthcare costs PPPY between patients initiated on an LAI versus an OA (MD [95% CI] $327 [− 1565 to 2219], n = 7; Fig. 4). Of these seven studies, six reported pharmacy and medical costs, separately. While the initiation of an LAI was associated with higher PPPY pharmacy costs (MD [95% CI] $5603 [3799–7407], n = 6, Online Resource Table S4F), this was offset by lower PPPY medical costs (MD [95% CI] − $5404 [− 7745 to − 3064], n = 6, Online Resource Table S4G).

Sixteen studies reported the likelihood of being adherent to an LAI compared with an OA (Online Resource Table S4I). Among the nine studies that were included in the meta-analysis, patients initiated on an LAI were 89% more likely to be adherent to their medication (OR [95% CI] 1.89 [1.52–2.35], n = 9) compared with those initiated on an OA (Fig. 5).

Articles comparing PP1M with OA, which included 16 publications out of the 25 articles retained, also found similar associations to those of the main analysis across all outcomes. Patients initiated on PP1M had fewer all-cause hospitalizations (IRR [95% CI] 0.74 [0.62–0.89], n = 6, Online Resource Fig. S1, see the electronic supplementary material) and ER admissions (IRR [95% CI] 0.82 [0.69–0.98], n = 6, Online Resource Fig. S2) compared with patients initiated on an OA. Similarly to the main analysis, the difference in PPPY total healthcare costs between patients treated with PP1M and those treated with an OA was not significant (MD [95% CI] $107 [− 2268 to 2482], n = 7, Online Resource Fig. S3). Treatment with PP1M was also associated with greater likelihood of medication adherence as compared to OA (OR [95% CI] 1.93 [1.54–2.42], n = 8, Online Resource Figure S4).

The results of the present study should be interpreted in the context of certain limitations. First, this review identified studies through MEDLINE^® and MEDLINE In-Process, a broad medical literature database, but did not include other databases, unpublished articles, or articles published in languages other than English. While it is expected that MEDLINE contains the vast majority of studies published in the US, it is possible that articles indexed in other international databases were missed. Second, due to the expected heterogeneity of study types and the multiple outcomes included in the analyses, a qualitative appraisal of the potential sources of heterogeneity was conducted instead of a formal quality assessment using a standardized tool (such as the Cochrane Collaboration’s tool for assessing risk of bias [63] or the Risk Of Bias In Non-randomised Studies—of Interventions [64]). Third, effect sizes and their variance directly extracted from publications and those calculated based on study results, as well as adjusted and unadjusted values, were included and treated similarly in the meta-analyses. Fourth, because of the relatively low number of studies included in the meta-analyses, sub-group analyses (e.g., based on study types, year of publication) or meta-regressions could not be conducted to control for potentially confounding factors. Fifth, the presence of statistical heterogeneity between studies was confirmed by a high I² statistic in all analyses. While random effects meta-analyses aimed to account for heterogeneity between studies, differences may have remained in the studies’ definitions of outcomes and patient populations.