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Tuesday, May 26, 2020

Hydroxychloroquine is useless as a treatment for coronavirus: "Let the science speak for itself"

Hydroxychloroquine fails to help hospitalized coronavirus patients in US funded study

More Evidence to squash Hydroxychloroquine. The drug is ineffective and harmful in COVID-19.
By Batya Swift Yasgur MA, LSW
Hydroxychloroquine and chloroquine, with or without azithromycin or clarithromycin, offer no benefit in treating patients with COVID and, instead, are associated with ventricular arrhythmias and higher rates of mortality, according to a major new international study.

In the largest observational study of its kind, including close to 100,000 people in 671 hospitals on six continents, investigators compared outcomes in 15,000 patients with COVID-19 treated with hydroxychloroquine and chloroquine alone or in combination with a macrolide with 80,000 control patients with COVID-19 not receiving these agents.

Treatment with any of these medications, either alone or in combination, was associated with increased death during hospitalization: compared with about 10% in control group patients, mortality rates ranged from more than 16% to almost 24% in the treated groups.

Patients treated with hydroxychloroquine plus a macrolide showed the highest rates of serious cardiac arrhythmias, and, even after accounting for demographic factors and comorbidities, this combination was found to be associated with a more than 5-fold increase in the risk of developing a serious arrhythmia while in the hospital.

"In this real-world study, the biggest yet, we looked at 100,000 patients [with COVID-19] across 6 continents and found not the slightest hint of benefits and only risks, and the data is pretty straightforward," study coauthor Frank Ruschitzka, MD, director of the Heart Center at University Hospital, Zurich, Switzerland, told theheart.org | Medscape Cardiology.

The study was published online May 22 in The Lancet.
'Inconclusive' Evidence

The absence of an effective treatment for COVID-19 has led to the "repurposing" of the antimalarial drug chloroquine and its analogue hydroxychloroquine, which is used for treating autoimmune disease, but this approach is based on anecdotal evidence or open-label randomized trials that have been "largely inconclusive," the authors write.

'Inconclusive' Evidence

The absence of an effective treatment for COVID-19 has led to the "repurposing" of the antimalarial drug chloroquine and its analogue hydroxychloroquine, which is used for treating autoimmune disease, but this approach is based on anecdotal evidence or open-label randomized trials that have been "largely inconclusive," the authors write.

Additional agents used to treat COVID-19 are second-generation macrolides (azithromycin or clarithromycin), in combination with chloroquine or hydroxychloroquine, "despite limited evidence" and the risk for ventricular arrhythmias, the authors note.

"Our primary question was whether there was any associated benefits of the use of hydroxychloroquine, chloroquine, or a combined regimen with macrolides in treating COVID-19, and — if there was no benefit — would there be harm?" lead author Mandeep R. Mehra, MD, MSc, William Harvey Distinguished Chair in Advanced Cardiovascular Medicine, Brigham and Women’s Hospital, Boston, Massachusetts, told theheart.org | Medscape Cardiology.

The investigators used data from a multinational registry comprising 671 hospitals that included patients (n = 96,032, mean age 53.8 years, 46.3% female) who had been hospitalized between December 20, 2019, and April 14, 2020, with confirmed COVID-19 infection.

Demographics collected included underlying comorbidities, and medical history, and medications that patients were taking at baseline.

Patients receiving treatment (n = 14,888) were divided into four groups: those receiving chloroquine alone (n = 1868), those receiving chloroquine with a macrolide (n = 3783), those receiving hydroxychloroquine alone (n = 3016) and those receiving hydroxychloroquine with a macrolide (n = 6221).

The remaining patients not treated with these regimens (n = 81,144) were regarded as the control group.

Most patients (65.9%) came from North America, followed by Europe (17.39%), Asia (7.9%), Africa (4.6%), South America (3.7%), and Australia (0.6%). Most (66.9%) were white, followed by patients of Asian origin (14.1%), black patients (9.4%), and Hispanic patients (6.2%).

Comorbidities and underlying conditions included obesity, hyperlipidemia, and hypertension in about 30%.

The investigators conducted multiple analyses to control for confounding variables, including Cox proportional hazards regression and propensity score matching analyses.

"In an observational study, there is always a chance of residual confounding, which is why we did propensity score based matched analyses," Ruschitzka explained.

No significant differences were found in distribution of demographics and comorbidities between the groups.

As Good as It Gets

"We found no benefit in any of the 4 treatment regimens for hospitalized patients with COVID-19 but we did notice higher rates of death and serious ventricular arrhythmias in these patients, compared to the controls,” Mehra reported.

Of the patients in the control group, roughly 9.3% died during their hospitalization compared with 16.4% of patients treated with chloroquine alone, 18.0% of those treated with hydroxychloroquine alone, 22.2% of those treated with chloroquine and a macrolide, and 23.8% of those treated with hydroxychloroquine and a macrolide.

After accounting for confounding variables, the researchers estimated that the excess mortality risk attributable to use of the drug regimen ranged from 34% to 45%.

Patients treated with any of the four regimens sustained more serious arrhythmias compared with those in the control group (0.35), with the biggest increase seen in the group treated with the combination of hydroxychloroquine plus a macrolide (8.1%), followed by chloroquine with a macrolide (6.5%), hydroxychloroquine alone (6.1%), and chloroquine alone (4.3%).


"We were fairly reassured that, although the study was observational, the signals were robust and consistent across all regions of the world in diverse populations, and we did not see any muting of that signal, depending on region," Mehra commented.

"Two months ago, we were all scratching our heads about how to treat patients with COVID-19, and then came a drug [hydroxychloroquine] with some anecdotal evidence but now we have 2 months more experience, and we looked to science to provide some answer," Ruschitzka said.

"Although this was not a randomized controlled trial, so we do not have a definite answer, the data provided in this [large, multinational] real-world study is as good as it gets and the best data we have," he concluded.

"Let the Science Speak for Itself"

Commenting on the study for theheart.org | Medscape Cardiology, Christian Funck-Brentano, MD, from the Hospital Pitie-Salpetriere and Sorbonne University in Paris, France, said that although the study is observational and therefore not as reliable as a randomized controlled trial, it is "nevertheless well-documented, studied a huge amount of people, and utilized several sensitivity methods, all of which showed the same results."

Funck-Brentano, who is the coauthor of an accompanying editorial and was not involved with the study, said that "we now have no evidence that hydroxychloroquine and chloroquine alone or in combination with a macrolide do any good and we have potential evidence that they do harm and kill people."


Also commenting on the study for theheart.org | Medscape Cardiology, David Holtgrave, PhD, dean of the University at Albany School of Public Health said that, "while no one observational study alone would lead to a firm clinical recommendation, I think it is helpful for physicians and public health officials to be aware of the findings of the peer-reviewed observational studies to date and the NIH COVID-19 treatment guidelines and FDA statement of drug safety concern about hydroxychloroquine to inform their decision-making as we await the results of randomized clinical trials of these drugs for the treatment of COVID-19," said Holtgrave, who was not involved with the study.

He added that, to his knowledge, there are "still no published studies of prophylactic use of these drugs to prevent COVID-19."

Mehra emphasized that a cardinal principle of practicing medicine is "first do no harm" and "even in situations where you believe a desperate disease calls for desperate measures, responsible physicians should take a step back and ask if we are doing harm, and until we can say we aren't, I don’t think it's wise to push something like this in the absence of good efficacy data."

Ruschitzka added that those who are encouraging use of these agents "should review their decision based on today's data and let the science speak for itself."

The study was supported by the William Harvey, Distinguished Chair in Advanced Cardiovascular Medicine at Brigham and Women’s Hospital (Boston, MA, USA). Mehra reports personal fees from Abbott, Medtronic, Janssen, Mesoblast, Portola, Bayer, Baim Institute for Clinical Research, NuPulseCV, FineHeart, Leviticus, Roivant, and Triple Gene. Ruschitzka has been paid for time spent as a committee member for clinical trials, advisory boards, other forms of consulting, and lectures or presentations; these payments were made directly to the University of Zurich and no personal payments were received in relation to these trials or other activities. Funck-Brentano, his coauthor, and Holtgrave have declared no relevant financial relationships.

Lancet. Published online May 22, 2020.

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