Study design
This systematic review has been designed in accordance with the Preferred Reporting Items for Systematic Reviews and Meta-Analyses Protocols (PRISMA-P) statement and has been registered on PROSPERO (CRD42020196610) [15].
Eligibility criteria
Population
COVID-19 patients who were diagnosed with four types of psychiatric and neuropsychiatric syndromes (depression, anxiety, delirium, and PTSD). Studies that investigated the indirect effects of SARS-CoV-2 on family members, care providers, or isolated people who did not infect the prevalence of depression, anxiety, delirium, and PTSD will be excluded.
Type of outcomes
The primary outcomes
- Number of signs or symptom (depression, anxiety, delirium, and PTSD);
- The degree of diagnoses (depression, anxiety, delirium, and PTSD).
The secondary outcomes:
- Symptom severity;
- Incidence of mortality in COVID-19 patients with depression, anxiety, delirium or PTSD;
- The measurement of health-related quality of life using a validated scale, such as the Short Form 36 Health Survey questionnaire.
Studies design
We will include only peer-reviewed RCT, cohort/case-control/cross-sectional studies, case reports, case series, and qualitative studies. Conference abstracts and letters will be excluded because they lack adequate information for meta-analysis.
Search strategy
A senior investigator (Y.G.) would examine the published and gray literature sources to extract the studies reporting the prevalence of depression, PTSD, anxiety, or delirium in COVID-19 patients. An experienced medical information specialist (J.H.T.) would further check and approve the search methodology. We will conduct a comprehensive search of Cochrane library, PubMed, Web of Science, Embase, and Chinese Biomedicine Literature to extract articles/abstracts published between the date of database initiation and July 5, 2020. There will be no restrictions on language or year of publication. An additional file, which would describe the complete search strategy for PubMed as well as other electronic databases will be provided. We will also thoroughly search the reference lists of the relevant reviews and research trials. We have presented the search strategy using PubMed as an example in Table 1. The search strategy will be adapted to fit other online databases as well.
Update plan
We will perform identical search operations at regular pre-defined intervals to identify newly published data. There are no robust standards for the update frequency based on current research; however, due to the unprecedented number of publications on COVID-19, we will update the literature searches every month, and perform meta-analysis if any new eligible studies or data are obtained. We will submit an updated systematic review if we observe any changes in the outcomes and heterogeneity after the addition of new studies or provide data on additional outcomes [11, 12]. We chose this updating frequency to allow quick updates and to highlight the most recent information to the researchers, clinicians, nurses, and policy makers [11, 14, 16].
Study selection
Original literature search records will be imported into Endnote X9 software tool (Thomson Reuters, New York, NY, USA) management software. Two authors (JYS and YG) will independently retrieve full-text of potentially studies after deduplication to assess their eligibility according to the abovementioned inclusion criteria. Any disagreement will be resolved by the third reviewer (JHT).
Data extraction
Two independent reviewers (JYS and MMN) will be involved in data extraction; we will extract country of patients, population type (e.g., old people and children), age, study design (such as RCT/cohort/case-control), diagnostic criteria for the viral infection (such as WHO criteria), stage and severity of disease, length of follow-up, sample size (such as number of cohort, number of cases), and gender.
Risk of bias (quality) assessment.
Two independent reviewers will use the following tools to examine the risk of bias in the included studies: the revised Cochrane risk-of-bias tool (RoB 2) for RCT [17], the Risk Of Bias In Non-randomized Studies of interventions (ROBINS-I Scale) for non-randomized controlled trials, the Newcastle-Ottawa Scale (NOS) for cohort and case-control studies, confidence in the Evidence from Reviews of Qualitative research for qualitative studies, and the Agency for Healthcare Research and Quality (AHRQ) for cross-sectional studies.
Processing missing data
We will contact the corresponding or other primary authors to obtain missing data or insufficiently reported data after selecting the studies. Randomized controlled trials will be treated as cohort studies; all data from the control and experimental group will be extracted if they met our criteria. In addition, we will estimate missing data if they can be extracted from tables or figures. Trials with missing data that cannot be obtained will be excluded for reasons.
Differences between the protocol and the final review
Any significant deviations between the protocol and final review will be reported clearly.
Data analysis
The Stata (v13.0; StataCorp) and Revman 5 were used for statistical analysis. The statistical heterogeneity will be examined using the Cochran's Q and the I² statistic. An I² > 50%, and a p-value < 0.05 will correspond to significant heterogeneity, and a random-effects model will be used for the subgroup analyses and pooled estimates. On the contrary, an I² < 50% and a p-value > 0.05 will correspond to insignificant heterogeneity, and the fixed-effect model shall be used for the subsequent meta-analysis. The effect size measures were mean difference with 95% CI (for severity of the symptoms and degree of diagnoses) and prevalence with 95% CI (number of psychiatric diagnoses (depression, anxiety, delirium, and PTSD); severity of depression, anxiety, delirium, and PTSD). The heterogeneity/publication bias will be examined using the Egger's test or the symmetry of the funnel plot. In the Egger's test, bias will be significant when p-value < 0.05.
Subgroup analysis
The following subgroup analyses will be planned for main outcomes if data are sufficient: Age (< 60 vs. ≥ 60 years), symptom severity (mild vs. severe vs. ICU patients), high and middle-high vs. middle-low and low-income countries, databases (data from Chinese databases vs. data from English databases), study design (RCT, cross-sectional, non-randomized control trials, cohort-study case-control trials, and qualitative studies), and follow-up time (1, 3, 6 months of acute and post-illness for COVID-19 patients).
Sensitivity analyses
We will exclude the studies with high risk-of-bias based on a sensitivity analysis.
Quality of the evidence
The Grades of Recommendations, Assessment, Development, and Evaluation (GRADE) Working Group method will be used to examine the quality of the evidence for each outcome. We will assess each outcome based on each of the following five aspects: imprecision, inconsistency, limitations, indirectness, and publication bias. They will be rated as very-low, low, moderate, or high level [18].