Publication selection and identification of cases and controls

For the time period of March 12 to April 12, 2020 (i.e., during the early outbreak phase of the COVID-19 pandemic), we identified all of the publications from the top three general medical journals by impact factor (the New England Journal of Medicine (NEJM), the Journal of the American Medical Association (JAMA), and The Lancet). We conducted a PubMed database search on April 17, 2020, using the following search string: ((("The New England journal of medicine"[Journal]) OR "Lancet (London, England)"[Journal]) OR "JAMA"[Journal]) AND ("2020/03/12"[Date—Publication]: "2020/04/12"[Date—Publication]). The resulting publications were stratified into COVID-19–related and nonCOVID-19–related. We matched the nonCOVID-19 publications with COVID-19 publications according to article types within each journal, with the exclusion of nonmatching article types. Secondary studies, correspondence letters on previously published articles, unauthored publications, and specific article types not matching any of the six categories on the levels of the evidence pyramid [22–24] (e.g., infographic, erratum) were excluded (Fig 1).

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Fig 1. Flow chart of the processing of the publications included in this study.

The article types in the NEJM are grouped (by the publisher) into Original Research (Research Articles and Special Articles for research on economics, ethics, law and health care systems), Clinical Cases (Brief Reports and Clinical Problem Solving), Review Articles (Clinical Practice Review or Other Reviews), Commentaries (Editorials, Perspectives, Clinical Implications of Basic Research, Letters to the Editor, Images and Videos in Clinical Medicine), and other articles (Special Reports, Policy Reports, Sounding Board, Medicine and Society and Case Records of the Massachusetts General Hospital). The JAMA articles are grouped by the publisher into Research (Original Investigation, Clinical Trials, Caring for the Critically Ill Patient, Meta-Analysis, Brief Reports and Research letters), Clinical Review and Education (Systematic Reviews, Advances in Diagnosis and Treatment, Narrative Reviews, Special Communications, Clinical Challenges, Diagnostic Test Interpretation, Clinical Evidence Synopsis), Opinion (Viewpoints), Humanities (The Arts and Medicine, A Piece of My Mind, Poetry) and Correspondence (Letters to the Editor). The Lancet’s articles are grouped into a Red Section (Articles and Clinical Pictures), a Blue Section (Comments, World Reports, Perspectives, Obituaries, Correspondence, Adverse Drug Reactions and Department of Error) and a Green Section (Seminars, Reviews, Therapeutics, Series, Hypothesis, Other Departments and Commissions).

https://doi.org/10.1371/journal.pone.0241826.g001

Multi-step design

We performed a multi-step 360-degree assessment of the studies. It consisted of their classification according to level of evidence for a quantitative appraisal of their methodological quality using a validated tool, and a narrative analysis of the strengths and weaknesses of the COVID-19 publications, as is often used in social sciences [25]. Early citation frequencies of the original articles was determined.

Levels of evidence

All of the publications included were assessed for number of authors and level of evidence. We used the Oxford Quality Rating Scheme for Studies and Other Evidence [22] to categorize the level of evidence, as adjusted to include animal and in-vitro research [23, 24]. The highest level is attributed to research as randomized trials, followed by nonrandomized controlled studies and cohort trials. The lower levels are represented by descriptive studies, expert opinion, and animal or in-vitro research, commonly represented in the form of a pyramid [22, 23, 26]. For secondary analysis, we split the six levels of evidence into the upper and lower halves, which reflected higher (i.e., 1–3) and lower (i.e., 4–6) levels of evidence, respectively. The number of authors per publication was counted manually.

Quantitative appraisal using the “Standard quality assessment criteria for evaluating primary research papers from a variety of fields (QUALSYST)”

After the hierarchical grading of included publications, the original articles (i.e., published as ‘original research articles’ in each of the journals; Fig 1) were defined for further in-depth analysis using the study quality checklist proposed by Kmet et al. [27]. This checklist is consistent with the recommendations from the Center for Reviews and Dissemination [28, 29]. Four authors in pairs (MZ–DB, JBE–BZ; each pair assessing one half of the publications) independently assessed the original articles on 14 quality criteria (see S1 File). The 14 items covered the research question, design, measures to reduce bias, and data reporting and interpretation, and these were scored according to the degree to which each specific criterion was met (“yes” = 2; “partial” = 1; “no” = 0; “not applicable” = n/a) with the help of a prespecified manual [27]. The total score ranged from 0 to 28. The summary percentage scores were calculated for each original article by summing the total score obtained across the applicable items and dividing by the total possible score (i.e., 28 –[number of “n/a” × 2] ×100). Disagreements between the reviewers (defined as >2 difference in the total score, or >10% difference in the summary percentage scores), were resolved through one round of discussion between each 2-author pair.

Narrative analysis of COVID-19 original articles

The COVID-19 original research articles (n = 13) were assessed in narrative form to report on their major weaknesses, potential conflicts of interest, and likely influence on further research and clinical practice.

Citation frequencies

The early citation frequencies were tracked every 5 days from April 25^th to May 25^th 2020 for all of the original scientific articles through GoogleScholar [30], to determine how strongly these COVID-19 original articles had impacted upon further publications, in comparison to the nonCOVID-19 original articles. A comparison to an original article set in the same time frame of 2019 was done. Citations per month were calculated to reduce lead time bias. The Google scholar search engine has been shown to reliably identify the most highly-cited academic documents [31].

Statistical analysis

The distributions of the COVID-19 and nonCOVID-19 publications on the levels of evidence pyramid were analyzed using Pearson’s Chi-squared statistics and Cramer’s V as the measure of strength of association (weak: >0.05; moderate: >0.10; strong: >0.15; very strong: >0.25) [32]. Further effect size estimations were performed on two by two contingency tables (split by level of evidence into high and low quality groups) and are reported as odds ratios with 95% confidence intervals (CI).

The retrospectively calculated sample size for the summary percentage scores [27] to detect a 20% change from 90 (nonCOVID-19) to 72 (COVID-19), with 4:1 allocation (52:13 original articles, respectively) on a t-test, with a standard deviation of 15, 85% power, and 0.05 alpha, was 8 original articles [33, 34]. Thus, we deemed our collected data sufficient.

We also planned for a secondary analysis if the comparison above resulted in a significant difference (defined as P <0.05) in the mean percentage scores between the COVID-19 and nonCOVID-19 original articles. The secondary analysis aimed to compare the 2:1 allocation of nonCOVID-19:COVID-19 original articles, for which the allocation was carried out with the 26 original articles with the lowest overall percentage scores in the nonCOVID-19 group versus all of the 13 original articles in the COVID-19 group. The threshold p-value for significance was set at P <0.025, to adjust for multiple testing.

Assessment of the original articles’ quality is reported as a two-reviewer mean score (95% CI) and was analyzed using Welch’s t-tests. Hedges’s g was used as the effect size measure based on a standardized mean difference [35] (small: d = 0.20; medium: d = 0.50; large: d = 0.80; very large: d = 1.20; huge: d >2.00) [36, 37]. To confirm the reliability of the scoring, Cronbach’s alpha was calculated for the total score and the summary percentage score (internal consistency), and the Intraclass Correlation Coefficient with absolute agreement for the inter-rater reliability. The percentage agreement between the two reviewers was also calculated for each individual item (see S2 File).

The data distributions were tested for normality with Kolmogorov-Smirnov tests, and are reported accordingly. Tests between two groups were done with Mann-Withney tests, between multiple groups with Kurskal-Wallis test. Significance was set at P <0.05 or adjusted for multiple testing. All of the tests were two-tailed. The statistical analysis was performed using SPSS Statistics 20 (IBM Inc., Armonk, NY, USA) and Prism 8 (GraphPad Software, San Diego, CA, USA).

Levels of evidence and number of authors

The nonCOVID-19 publications were associated with higher quality on the level of evidence pyramid (P <0.001; Chi squared), with a strong association measure (Cramer’s V: 0.452, Table 1). When comparing the higher evidence group to the lower evidence group, the COVID-19 publications were 18-fold more likely (i.e., odds ratio) to be in the lower evidence group (95% CI: 7.0–47; P <0.001). When comparing only the original articles on the levels of evidence pyramid (Table 2), the nonCOVID-19 publications were also associated with higher quality (P <0.001; Chi squared), with a strong association measure (Cramer’s V: 0.641, Table 2). When comparing the higher evidence group to the lower evidence group, the COVID-19 original articles were 26-fold more likely (i.e., odds ratio) to be in the lower evidence group (95% CI: 5.4–120; P <0.001).

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Table 1. Frequency distribution of the publications included on the levels of evidence pyramid [23, 24].

https://doi.org/10.1371/journal.pone.0241826.t001

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Table 2. Frequency distribution of the original articles on the levels of evidence pyramid [23, 24].

https://doi.org/10.1371/journal.pone.0241826.t002

Numbers of authors were similar between groups (median [interquartile range]: 3 [2–6.5] versus 3 [2–13.5]; P = 0.394; Mann-Whitney). In an a posteriori subgroup analysis in the lower evidence group (adjusted threshold p-value as P <0.017), there were significantly more authors in the COVID-19 publications (median [interquartile range]: 3 [2–6]) than in the nonCOVID-19 publications (median: 2 [1–3]) (P <0.001; Mann-Whitney). Obvious outliers were a NEJM case report [38] with 35 authors, an opinion correspondence piece in The Lancet [39] with 29 authors, and a comment piece in The Lancet with 77 authors in a coalition [40].

Quantitative appraisal

Due to >2 difference in the total scores, or >10% difference in the summary percentage scores, the reviewer pairs discussed 8 (of 32) and 12 (of 33), respectively, of the original articles after the individual scoring. The internal consistency reliability of the total score was 0.987, and of the summary percentage score was 0.964 (Cronbach’s alphas) for the reviewer pair MZ–DB, and 0.988 and 0.928, respectively, for the reviewer pair JBE–BZ (P < 0.001, for all). The inter-rater reliabilities of the total scores was 0.975, and the summary percentage score was 0.930 (Intraclass Correlation Coefficient, absolute agreement) for pair MZ–DB, and 0.974 and 0.860, respectively, for pair JBE–BZ (Intraclass Correlation Coefficient, absolute agreement) (P < 0.001, for all).

The mean total scores in the COVID-19 and nonCOVID-19 groups were 12.6 (95% CI 10.1–15.1) and 23.7 (95% CI 22.9–24.6) respectively (Fig 2A), and the mean summary percentage scores were 71.8% (95% CI 62.4–81.1) and 91.1% (95% CI 89.0–93.2), respectively (Fig 2C). The mean total score and the mean summary percentage scores were significantly different between the groups, favoring the nonCOVID-19 original articles (P <0.001, for both; Welch’s t-test; Hedges’ g = 3.37, 2.02, respectively). For the total scores, the difference between the means was 11.1 (95% CI 8.5–13.7; P <0.001), and for the summary percentage scores, 19.3% (95% CI 9.8%–28.8%; P <0.001). Also, in the secondary analysis, when the COVID-19 original articles were compared to the lower quality half of the nonCOVID-19 original articles (i.e., the 26 scoring lower instead of all 52), the differences in the mean total scores (Fig 2B; 12.6 [95% CI 10.1–15.1] vs 21.4 [95% CI 20.4.1–22.3] points, respectively; P = 0.008; Welch’s t-test; Hedges’ g = 2.86) and the mean summary percentage scores (Fig 2D; 71.8% [95% CI 62.4–81.1] vs 85.6% [95% CI 82.8–88.5], respectively; P <0.001; Welch’s t-test; Hedges’ g = 1.31) were significant. For this secondary analysis, the threshold P value for significance was set at p = 0.025.

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Fig 2. Quantitative appraisal of the quality of the COVID-19 versus nonCOVID-19 original articles.

The “Standard quality assessment criteria for evaluating primary research papers from a variety of fields”²⁵ was used, for a maximum total score of 28. (A, C) Primary analysis for mean total scores (A) and mean summary percentage scores (C) for all COVID-19 (n = 13) and nonCOVID-19 (n = 52) original articles. (B, D) Secondary analysis for mean total scores (B) and mean summary percentage scores (D) that included all of the COVID-19 original articles (n = 13) and the lower quality half of the nonCOVID-19 original articles (n = 26). Data are means with 95% CI. An adjusted threshold P value of 0.025 defines significance (adjusted for multiple testing. Welch’s t-tests).

https://doi.org/10.1371/journal.pone.0241826.g002

In a secondary sensitivity analysis that also included research letters, the mean total scores in the COVID-19 (n = 21) and nonCOVID-19 (n = 55) groups were 12.3 (95% CI 10.6–14) and 23.3 (95% CI 22.2–24.2) respectively, and the mean summary percentage scores were 72.6% (95% CI 66.1–79.1) and 90.9% (95% CI 88.9–92.9), respectively. The mean total score and the mean summary percentage scores were significantly different between the groups, favoring the nonCOVID-19 original articles (P <0.001, for both; Welch’s t-test; Hedges’ g = 2.98, 1.87, respectively). For the total scores, the difference between the means was 11.0 (95% CI 9.1–12.9; P <0.001), and for the summary percentage scores, 18.3% (95% CI 11.6%–25.0%; P <0.001).

Citation frequency

There was a significant difference in the median number of citations according to GoogleScholar at each of the seven dates tested, favoring COVID-19 original research papers (P <0.001, for all; Mann-Whitney, Table 3). A comparison to a set of original articles from the same dates in 2019 revealed 53 (25 to 90) citations in 2019 vs. 334 (222 to 1001) citations for COVID articles in August 2020 and 10 (4 to 18) for non COVID articles (p<0.002 for all comparisons). When corrected for lead-time with citations per month, the articles in 2019 have 4 (2 to 6) cites per month, the non-Covid articles in 2020 2.5 (1 to 4.5) without significance. The COVID articles in 2020 have 83.5 (55 to 250) cites per month (p<0.001).

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Table 3. Google Scholar citations of original articles published between March 12 and April 12, 2020.

https://doi.org/10.1371/journal.pone.0241826.t003

Narrative appraisal

The major weaknesses of the 13 COVID-19 original research articles were assessed (Table 4). The selection included one randomized trial [41], four retrospective cohort studies or case series [42–45], five epidemiological descriptive studies [46–50], three epidemiologic modeling studies [51–53], with most of the designs reflecting low grades of evidence [22]. Most of these studies had limitations in terms of missing data or under-reporting. The randomized trial was not blinded. Ten studies showed no apparent conflicts of interest. Two studies were based on data collected by the World Health Organization [51, 52], and in another study [54] a pharmaceutical company screened the patients for treatment, collected the data, and supported the trial financially. Two studies had a patient:author ratio <1 [43, 46]. Two studies were close to 1 [55, 56]. Three studies were considered not relevant for further research [46, 48, 55], and four studies were deemed not relevant for clinical practice [43, 46, 55, 56], because the findings were neither new nor generalizable. The 13 COVID-19 original articles have already been cited in 52 sets of published guidelines.

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Table 4. Narrative assessment of the quality of the COVID-19 original articles.

https://doi.org/10.1371/journal.pone.0241826.t004

Conclusions

The quality of the COVID-19–related research in the top three scientific medical journals is below the quality average of these journals. Unfortunately, our numbers do not contribute to a solution as to how to preserve scientific rigor under the pressure of a pandemic.