key: cord-0741400-xawav0b3
authors: Bignardi, Paulo Roberto; Vengrus, Carolina Santos; Aquino, Bruno Matos; Cerci Neto, Alcindo
title: Use of hydroxychloroquine and chloroquine in patients with COVID-19: a meta-analysis of randomized clinical trials
date: 2021-02-11
journal: Pathogens and global health
DOI: 10.1080/20477724.2021.1884807
sha: a71fb80bb1daaf2dc6e3989eca4aa8e22c91db57
doc_id: 741400
cord_uid: xawav0b3

COVID-19 has quickly become a public health problem worldwide, and treatment for this new disease is needed. Hydroxychloroquine is an antimalarial that in vitro studies have shown action against SARS-CoV-2, which is why it has been the target of clinical studies with conflicting results. Therefore, the aim of this systematic review was to assess the association of hydroxychloroquine use with the virological cure, clinical recovery, mortality, and development of adverse effects in patients with COVID-19. PubMed, Cochrane Library, and Lilacs were searched until 7 January 2021, for randomized clinical trials with COVID-19 patients treated with hydroxychloroquine or chloroquine. Of the 130 studies found, 12 met the inclusion criteria. Compared to the patient’s control group, the risk ratio (RR) for the virological cure and clinical recovery with hydroxychloroquine or chloroquine use was 1.04 (95%CI 0.91–1.17) and 1.03 (95%CI 0.92–1.13), respectively. Hydroxychloroquine (with or without azithromycin) was also not associated with mortality (RR = 1.09, 95%CI 0.98–1.20). Treatment with hydroxychloroquine was associated with any adverse effects (RR = 1.50, 95%CI 1.18–1.81). Hydroxychloroquine or chloroquine use did not have a significant effect on virological cure, the time of clinical recovery, and improvement in survival in COVID-19 patients. However, patients who used hydroxychloroquine showed an increase in adverse effects.

On 31 December 2019, the World Health Organization's China Country Office was informed by local authorities of pneumonia deaths of unknown etiology in Wuhan, Hubei Province of China [1] . After a few weeks, the causative agent was identified as a new coronavirus (SARS-CoV-2) and the disease called COVID-19 [2, 3] . In less than 3 months, on 11 March 2020, the World Health Organization (WHO) declared the COVID-19 as a pandemic disease [4] .

Increased mortality and the fast spread of the disease worldwide have made the scientific community engage in a global effort to find the best treatment for COVID-19. Chloroquine (CQ) and Hydroxychloroquine (HCQ), drugs that belong to the quinolone family and are used to prevent and treat malaria, showed effectiveness against SARS-CoV-2 in the first in vitro studies [5, 6] . Two initial small clinical trials reported a decrease in the viral load and better clinical recovery with high doses of HCQ use in patients with COVID-19 [7, 8] . Following these results, other observational studies have found unclear results on the beneficial use of HCQ/CQ in any disease phase.

Recent randomized clinical trials have not shown better outcomes in patients treated with these drugs. There is much controversy about using this treatment worldwide, and some advocate that these drugs could be helpful at the beginning of the disease in the viral phase. Therefore, considering the contrast of conclusions, we decided to perform a systematic review and meta-analysis of data involving the administration of CQ and HCQ in patients with COVID-19 and virological cure, clinical recovery, mortality, adverse effects, need for mechanical ventilation, and hospital discharge.

This study is a systematic review of randomized clinical trials. We conducted a review of the databases: PubMed, Lilacs, and Cochrane Library. Studies published until 7 January 2021, were included. The following keywords were used as search terms: 'coronavirus', 'coronavirus disease', 'COVID-19ʹ, 'treatment', 'hydroxychloroquine', 'chloroquine', 'clinical trial'. The references for all selected articles were also retrieved and, due to the urgency of publications related to COVID-19, additional references were searched manually on the MedRxiv prepress server.

Two independent authors screened this review. Disagreements were solved through discussion among all authors. Titles and abstracts of retrieved articles were revised to exclude irrelevant studies, followed by screening. Clinical trials were included when they met the following inclusion criteria: (1) COVID-19 patients using HCQ or CQ; (2) patients who did not use HCQ or CQ as a comparison group;

(3) randomized controlled trial; (4) examination of the relationship between HCQ or CQ use and time to negative viral nucleic acid test, time to clinical recovery, mortality, adverse effects, use of mechanical ventilation (MV), hospital discharges, or kidney and thromboembolic complications. The study was conducted in accordance with the Preferred Items guidelines for Reporting for Systematic Reviews and Meta-Analysis (PRISMA), and this study has not been registered.

Data extraction was performed by two independent authors according to a data collection form. Possible conflicts were discussed with all authors. The information extracted includes authors, year of publication, study design, country of origin, population characteristics (age and sample size), type of treatment, disease severity, duration of follow-up, and measurement of effects for the researched outcomes. They should provide odds ratio (OR), ratio risk (RR), or hazard ratio (HR) with 95% confidence intervals (CI). Inclusion was not restricted by study size.

Two authors independently assessed the quality of the studies according to the Cochrane guidelines [9] . The following five domains were assessed: (1) bias arising from the randomization process; (2) bias due to deviations from the intended interventions; (3) bias due to missing outcome data; (4) bias in the measurement of the outcome; (5) bias in selection of the reported result. Any disagreements were resolved through discussion with a third author.

The primary analysis focused on the outcomes: (1) time for negative detection of the viral nucleic acid; (2) time for clinical recovery; (3) mortality of the treated group in comparison to the control group.

The secondary analysis focused on the effect of treatment on the emergence of adverse effects, the use of MV, hospital discharge, renal and thromboembolic complications.

We performed a stratified analysis by type of treatment: HCQ only, CQ, and HCQ with azithromycin. In addition, a sensitivity analysis was performed when necessary omitting each study to detect the influence on the estimate of the overall effect.

Studies included in the meta-analysis reported RR, OR, or HR. For studies that did not report these measures of effects, the RR calculation was based on the Cochrane Handbook for Systematic Reviews [10] . For studies that reported OR, a corrected RR was computed as already described [11] . HR was considered comparable to RR.

Pooled RR and 95% confidence interval (CI) were calculated using a fixed or random effects model according to the homogeneity of the studies. The Cochran's Q test and the I 2 statistic were used to evaluate the statistical significance and degree of heterogeneity between the studies, respectively. The result of p ≤ 0.05 for the Q test represents statistical significance, and the statistic I 2 ≥ 50% reveals substantial heterogeneity. Finally, the publication bias will be examined by the Egger test. All analyses were performed with Stata/ SE v.14.1 software (StataCorpLP, USA).

The initial search identified one hundred and thirty studies. Of these, 49 were excluded because they were duplicated. Inconsistent trials, non-clinical trials, non-therapeutic, and non-randomized studies were excluded. Of the remaining studies, 12 met the inclusion criteria and were selected for qualitative analysis, and eleven studies were included for the meta-analysis ( Figure 1 ), totaling 7,629 patients. The investigated therapies found were as follows: HCQ in 10 studies, one study investigated HCQ only and HCQ plus azithromycin, and one study CQ therapy. One trial [12] investigated the effect of HCQ on individuals exposed to someone with confirmed COVID-19. The basic characteristics of the studies are shown in Table 1 .

The data were extracted and pooled from four studies. Three trials [13] [14] [15] studied HCQ only therapy versus usual care, and one trial [16] studied CQ therapy versus lopinavir/ritonavir combination. All trials used throat swab SARS-CoV-2 real-time reverse transcriptionpolymerase chain reaction (RT-PCR) nucleic acid at the beginning of the study to confirm COVID-19 and at the end to confirm the virological cure.

Comparing the HCQ group with the control group, the results suggested no significant change in time for the virological cure (RR = 0.96, 95%CI 0.74-1.18). Combined with CQ study results, there was also no change in time for the negative RT-PCR (RR = 1.04, 95%CI 0.91-1.17, P > 0.05) ( Figure 2 ).

The data were extracted from six studies that showed no decrease in time for clinical recovery in patients in the treated groups. Five trials [7, 14, 15, 17, 18] studied HCQ only therapy versus usual care, and one trial [16] studied CQ therapy versus lopinavir/ritonavir combination.

Combining the six studies, there was also no decrease in the time for clinical recovery (RR = 1.03, 95%CI 0.92-1.13, P > 0.05) ( Figure 3 ).

Cavalcanti et al. [19] studied treatments with HCQ only and HCQ plus azithromycin, while Abd-Elsalam et al. [17] , Horby et al. [20] , Lyngbakken et al. [21] , and Self et al. 2020 [18] studied the treatment with HCQ only. The risk estimate for HCQ only was not different from the control group (RR = 1.09, 95%CI 0.98-1.20, P > 0.05). When HCQ with azithromycin was included, the result was similar without statistically significant differences (RR = 1.08, 95% CI 0.-97-1.20, P > 0.05) (Figure 4) .

The data were extracted from seven studies. Five trials (11, 17) studied HCQ only versus usual care, one trial [19] HCQ only versus usual care and HCQ plus azithromycin therapy versus usual care, and one trial [16] studied CQ therapy versus lopinavir/ ritonavir combination. In the first analysis, the treatment with HCQ showed an increased risk of adverse effects (RR = 1.50, 95%CI 1.18-1.81, P < 0.05) compared to the control group. The analysis of all therapies also showed a significant increase in any adverse effects (RR = 1.44, 95%CI 1.21-1.68, P < 0.05) ( Figure 5 ). 

The need to use MV was extracted from three trials [17, 19, 20] . Analysis of the HCQ only treatment showed no difference when compared to the control group (RR = 1.15, 95%CI 0.92-1.38, P > 0.05). Analysis including the HCQ plus azithromycin treatment also showed no difference with the control group (RR = 1.17, 95%CI 0.94-1.40, P > 0.05) ( Figure 6 ). Hospital discharge analysis was extracted from three trials. Two trials [18, 20] studied HCQ therapy versus usual care and one trial [16] CQ versus lopinavir/ritonavir combination. The analysis revealed that HCQ treatment did not favor the hospital discharge (RR = 0.97, 95%CI 0.74-1.20, P > 0.05). Combined analysis of HCQ and CQ showed no difference when compared to the control group, but with substantial heterogeneity (RR = 1.05, 95%CI 0.73-1.38, P > 0.05, I 2 = 54.6.1%) (Figure 7) .

Renal and thromboembolic complications were described by Cavalcanti et al. [19] , but with no differences between the control group and treatment group.

The heterogeneity of adverse effects analyses and clinical recovery was investigated by sensitivity analyses. Sensitivity analyses showed that excluding one study at a time from the analysis did not change the findings ( Table 2) .

For hospital discharges, the exclusion of Horby et al. [20] from the analysis changed the heterogeneity from substantial to moderate (I2 = 54.6% to 27.2%), yet did not alter the results.

The results of the estimated bias coefficient were from −0.177 to 0.195, giving a P-value > 0.05 for all analyses. Therefore, the tests provide weak evidence for the presence of publication bias.

Among the studies selected for the meta-analysis, four trials [18] [19] [20] [21] were considered as low risk of bias, five [7, [14] [15] [16] 22] as some concerns, and two [13, 17] as high risk of bias. Two trials were randomized, double-blind, placebo-controlled trial, and nine trials were randomized, open-label, controlled study. The quality assessments of the studies included in the meta-analysis are shown in Figure 8 .

Despite all the controversy about HCQ and CQ use for COVID-19 treatment, this meta-analysis did not show any better outcomes in patients using HCQ or CQ when compared to the control group. The results showed no statistical significance in the treatment with HCQ or CQ in achieving virological cure and faster clinical recovery.

Yao et al. [23] compared the in vitro effect of HCQ and CQ and showed that both have good antiviral activity, decreasing the replication of SARS-CoV-2. The conclusion of the study that HCQ is more potent in inhibiting viral replication led to prophylactic use. In contrast, Boulware et al. [12] show in their randomized, double-blind clinical trial that prophylactic use of HCQ after exposure to SARS-CoV-2 did not prevent patients' contamination.

The literature shows previous in vitro studies with Zika viruses, which demonstrated the efficacy of the antibiotic's inhibitory viral replication effect. However, the drug has not been proven to be effective in humans [24, 25] . Likewise, another in vitro study addressing HCQ and azithromycin in the Ebola viral replication does not bring clear evidence of possible antiviral effect in vivo of the drugs, neither to the increase in the prevention or delay of time of death [26] . That previous evidence of in vitro antiviral effects made the rationale for justifying the use of those drugs as off-label therapy in the COVID-19 pandemic and was disseminated by social media in Brazil [27] .

After in vitro studies demonstrated the efficacy of CQ and HCQ against SARS-COV-2, clinical studies were performed. Gautret et al. [8] pointed out a significant decrease in the viral load of patients infected with SARS-CoV-2 after treatment with HCQ plus azithromycin compared to the control group. Chen et al. [7] reported a faster clinical recovery in patients with COVID-19 who used HCQ. However, both clinical trials have come under strong criticism. Chen et al. [7] did not disclose the results regarding the use of different doses of HCQ, as previously specified in the study protocol, while the nonrandomized clinical trial by Gautret et al. [8] was harshly questioned for the methodologies adopted and by the exclusion of six patients who had been treated with HCQ from the final results. In addition, Tang et al. [14] found no significant reduction in viral load and faster clinical recovery. This review shows no association between the use of HCQ only or HCQ plus azithromycin and the improved survival of COVID-19 patients. These findings corroborate the meta-analysis of observational studies by Fiolet et al. [28] . The author also reports no substantial evidence to support increased mortality associated with HCQ or HCQ plus azithromycin intake.

Nevertheless, the use of these drugs in patients with COVID-19 deserves attention. Additional findings from this review show that the use of these drugs is associated with a 1.44-fold increased risk of adverse effects. The use of CQ and HCQ off-label is highly critical when addressing the adverse effects caused by these drugs. Among them, the most considered is the prolongation of the QTc interval, particularly in individuals with previous risk factors, in whom lethal ventricular arrhythmias are described, such as Torsades de Pointes [29] .

Other effects have been described, such as psychosis, delirium, agitation, personality disorder, depression, and sleep disorders [30, 31] . As for the effects of cardiac conduction, other than those already mentioned, we must consider branch block and atrioventricular block [29] . CQ and HCQ uses, when associated with azithromycin, increase the risk of hepatotoxicity [32] , cardiotoxicity, and hypoglycemia [33] .

Among the randomized clinical studies included in the meta-analysis, we observed a similarity between the reported adverse effects. Cavalcanti et al. [19] show that side effects were more evident in those patients who used HCQ + azithromycin, with 9 patients presenting complications due to adverse effects. Extending the QTc interval has been described in patients using HCQ and HCQ + azithromycin. Other conduction changes described were arrhythmias, bradycardia, and supraventricular tachycardia. Cavalcanti et al. [19] also highlighted the occurrence of pulmonary thromboembolism and acute kidney infection as potential complications. Vomiting, abdominal pain, changes in liver enzymes, nausea, diarrhea, skin rash, itching, coughing, and shortness of breath were other adverse effects also described [13, 16, 34] .

Lastly, our results also suggest no association between the use of these drugs in patients with COVID-19 and the decreased need for MV and hospital discharges. Similarly, Geleris et al. [35] indicated that the risk of intubation or death was not significantly higher or lower among patients who received HCQ when compared with the control group. Furthermore, Magagnoli et al. [36] showed that the length of stay among hospitalized COVID-19 patients was not shortened by the administration of HCQ with or without azithromycin.

This study has several strengths. To our knowledge, this is the first meta-analysis using only randomized clinical trials of patients with COVID-19. This study informs physicians and patients regarding the efficiency of HCQ and CQ in treating COVID-19. Despite the few published clinical trials, the studies selected in this systematic review a total of 7,629 patients. Some limitations of our study were the small number of randomized trials on the use of CQ, different follow-up times between studies, studies performed without blinding, an analysis that mixed different treatments and doses and different treatments in the control group.

These results suggest that the use of HCQ or CQ is not associated with decreased viral load, faster clinical recovery, improved survival, decreased need for mechanical ventilation, and decreased hospitalization time for patients with COVID-19. However, it suggests that the use of HCQ or CQ can be associated with an increased risk of adverse effects.

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The authors declare that there is no conflict of interests. 

This research did not receive any specific grant from funding agencies in the public, commercial, or not-for-profit sectors.