19 MEI 2020
https://www.medicineuncensored.com/
Updated May 6, 2020
By James M. Todaro, MD
Twitter: @JamesTodaroMD
covidtrial.io
Table of Contents
Recent publications by James Todaro, MD on COVID-19
COVID-19 antibody prevalence results and new estimates of
infection fatality rates
Evidence on hydroxychloroquine, azithromycin and zinc in early
treatment of COVID-19
Upcoming clinical trials on efficacy of HCQ in prevention of
COVID-19
Antiviral properties of azithromycin
Cardiac injury and myocarditis in COVID-19
Safety profile of hydroxychloroquine and azithromycin
Antiviral effects of zinc supplements and synergy with chloroquine
Efficacy of chloroquine against SARS-CoV-1
Given the nature of this rapidly spreading pandemic, some of this
evidence is anecdotal or expert opinion.
This is not medical advice and is for informational purposes only. Any
mention of dosages is for informational purposes only and not for medical use.
Please consult a medical professional.
The list is organized such that the newest evidence
is continually added to the top of the list
Recent
publications by James Todaro, MD on COVID-19
·
An Effective Treatment for Coronavirus (COVID-19) by
James M. Todaro, MD and Gregory J. Rigano, Esq. March 13, 2020.
·
A two-step strategy to reopen America by James M.
Todaro, MD, Joey Krug, Moshe E. Praver, MD and Vladimir Zelenko, MD. April 23,
2020.
COVID-19
antibody prevalence results and new estimates of infection fatality rates
·
Miami antibody study in a sample of nearly 1,800 people in
mid-April showed a population prevalence of COVID-19 between 4.4% and 7.9%,
projecting an estimated 165,000 adults already infected in Miami-Dade County.
This is a 17-fold higher prevalence than confirmed cases in the area at the
time, and has a projected infection fatality rate of
0.2%.
·
New York antibody study in a sample of 3,000 people in mid-April showed
a population prevalence of COVID-19 to be ~21% in NYC, projecting an estimated
1.8 million already infected. This is approximately a 15-fold higher prevalence
than confirmed cases in the area at the time. Based on these estimates,
the infection fatality rate of novel-coronavirus is ~0.5%. Source: Governor Andrew Cuomo, daily news briefing, April 23, 2020.
·
USC antibody study in LA County in a sample of nearly 1,000 people in
early April showed a population prevalence of COVID-19 between 2.8% and 5.6%,
projecting an estimated 221,000-442,000 adults already infected in LA County.
This is a 28 to 55-fold higher prevalence than confirmed cases in the area at
the time. Based on these estimates, the infection fatality rate of
novel-coronavirus is between 0.14% and 0.27%.
·
German antibody study near the border of the Netherlands in 500
residents in early April showed a population prevalence of
COVID-19 to be ~14% with an estimated infection fatality rate of
0.37%.
·
Stanford antibody study in Santa Clara County in a sample of 3,330
people in early April showed a population prevalence of
COVID-19 between 2.49% and 4.16%, projecting an estimated 48,000-81,000 people
already infected in Santa Clara County. This is a 50 to 85-fold higher
prevalence than confirmed cases in the area at the time. Based on these
estimates, the infection fatality rate (IFR) of
novel-coronavirus is between 0.12% and 0.2%.
Evidence on hydroxychloroquine, azithromycin and zinc in early treatment of COVID-19
·
Observational study in Spain of early treatment with
hydroxychloroquine in 166 COVID-19 patients showed a
significant survival benefit in patients started on hydroxychloroquine in the
mild stage of disease. Patients were categorized into one of three groups at
initial presentation: mild, moderate or severe. There was a significant
survival benefit in the mild group compared to controls (1.8 times, p = 0.032)
and a trend toward survival benefit in the moderate and severe groups (1.4
times and 1.6 times, respectively). Of note, the average time between symptom
onset and treatment was 7 days.
·
Prospective observational study assessing cardiac risk of
hydroxychloroquine, chloroquine and azithromycin in treatment of 201 COVID-19
patients resulted in no episodes of Torsade de pointes, no
arrhythmogenic deaths and prolonged QT interval requiring discontinuation of
therapy in 3.5% of patients. Of note, 59% of patients received azithromycin in
combination with hydroxychloroquine or chloroquine.
·
Didier Raoult challenges the results of the VA study on
hydroxychloroquine (Magagnoli et al) pointing to flaws that
could result in a higher mortality rate in the hydroxychloroquine treatment
group. Of note, there was a significant difference in baseline characteristics
between the treatment and control arms in this retrospective analysis. The
hydroxychloroquine treatment arms had significantly higher proportions of
patients with lymphopenia (low levels of lymphocytes–a type of white blood
cell), which has been shown previously to correlate with higher mortality risk.
Dr. Raoult also points out the severity of illness in the cohort, such that a
substantial percent of the patients were likely intubated prior to receiving
hydroxychloroquine treatment out of desperation, and resulting in a higher
mortality rate.
·
In a letter to Arizona Governor Ducey, the Association of American
Physicians and Surgeons (AAPS) reported treatment of 2,333
COVID-19 patients in Phoenix with hydroxychloroquine +/- azithromycin and zinc.
Of this cohort, 91.6% of patients treated with hydroxychloroquine improved
clinically. There were 63 deaths, with the vast majority (52/63) attributed to
a single VA report of hydroxychloroquine use in severely ill patients.
·
Observational, non-comparative study of 1061 COVID-19 patients treated
early with hydroxychloroquine and azithromycin in Marseille resulted in 91.7%
virologically cured within 10 days (prior studies report viral shedding
duration over 20 days in 50% and 30% of patients, F Zhou et al (The Lancet) and KKW To et al (The Lancet)). Mortality rate in the
total cohort was 0.75%, lower than the mortality rates for other treatment
regimens in all other Marseille public hospitals (p < 0.01). The mean time
between symptom onset and treatment with HCQ+AZ was 6.4 days. To date, this is the largest cohort study published on the
efficacy of early treatment with HCQ+AZ.
·
Zelenko reports successfully treating hundreds of COVID-19 positive and
suspected patients in New York with a regimen of hydroxychloroquine,
azithromycin and zinc with only two deaths as of April 12, 2020—a mortality
rate of 0.14%.
·
Preliminary results from a study in New York on hydroxychloroquine with
or without azithromycin in treatment of COVID-19 show no effect on critically
ill patients, announced Governor Andrew Cuomo in a press conference on April
23, 2020. These results are in agreement with other studies below that late treatment with hydroxychloroquine has little to no beneficial
effect on patient outcomes.
·
Retrospective analysis of 368 hospitalized patients at the VA in
Virginia who received hydroxychloroquine, hydroxychloroquine +
azithromycin or standard therapy in treatment of COVID-19. Rates of death were
27.8%, 22.1% and 11.4% in the HCQ, HCQ+AZ and standard therapy groups,
respectively. The risk of all-cause mortality in the HCQ group was
significantly higher than in the standard therapy group. Of note, it is unclear
how long from time of symptom onset patients began treatment. However, with
mortality rates over 10% in all groups (far higher than the national average
among confirmed cases), it is apparent that this was a very sick cohort of
patients likely in the advanced stages of illness. This is further evidence
that late treatment with HCQ may have minimal or no benefit.
·
A non-randomized, prospective study in Sao Paulo, Brazil of 636
symptomatic outpatients treated with hydroxychloroquine for 7
days and azithromycin for 5 days vs control group showed a significant decrease
in need for hospitalization. Only 1.9% versus 5.4% of patients in the treatment
group needed hospitalization compared to the control group (p < 0.001) with
a number needed to treat (NNT) of 28. In a subgroup analysis of outpatients who
started treatment within the first 7 days of symptoms, the need for
hospitalization decreased to 1.17%. Of note, the treatment group was clinically
sicker at baseline than the control group with dyspnea of 22.1% vs 16% (p <
0.0001). Lastly, inclusion criteria was based on flu-like symptoms as opposed
to positive COVID-19 testing.
·
Randomized controlled trial in China of 150 patients hospitalized
for COVID-19 who received either hydroxychloroquine or standard therapy for 2-3
weeks with a primary endpoint of negative conversion rates at 28 days. There
was no significant difference in conversion rates between the two arms, but
authors did note greater symptomatic relief in patients who received
hydroxychloroquine over standard therapy. There were no safety concerns
observed in the hydroxychloroquine arm and the most common adverse event was
diarrhea (10%). Also of note, treatment was started an average 16.6 days after
symptom onset.
·
Non-randomized trial of 181 COVID-19 patients hospitalized
for hypoxic pneumonia were treated with either 600 mg daily of
hydroxychloroquine or standard therapy with primary endpoint of transfer to
ICU. Of the patients treated with hydroxychloroquine, 20% also received
azithromycin. There was no difference between treatment groups in transfer to
ICU or death 7 days after hospital admission. The authors comment that based on
C-reactive protein levels, most patients were already in a cytokine storm by
the time treatment was initiated. This is further evidence that
hydroxychloroquine may not be effective once patients are in a cytokine storm.
·
A prospective pharmacokinetics study of 13 critical care patients treated
with hydroxychloroquine 200 mg three times daily (600 mg daily) showed that
only 61% of patients achieved the supposed minimum HCQ therapeutic threshold of
1 mg/L with a mean time of 2.7 days. The authors propose a new regimen
consisting of a loading dose of hydroxychloroquine 800 mg on day 1 followed by
200 mg twice daily for 7 days with the goal of rapidly achieving therapeutic
level while not exceeding potentially toxic levels above 2 mg/L.
·
Quasi-randomized comparative study of 63 COVID-19 patients in
Detroit treated with either hydroxychloroquine or standard therapy with primary
endpoint escalation in respiratory support. Hydroxychloroquine arm required
increased respiratory support (p=0.013). Authors don’t mention any adjunctive
therapy with zinc or azithromycin. Of note, patients in the hydroxychloroquine
treatment arm were sicker with greater respiratory distress before treatment
than in the control arm (p=0.012). Per my understanding, this manuscript
submission has since been retracted and will not be published. I am leaving
this summary here temporarily because many people have asked me about the
study, but take caution as the data is not validated.
·
Randomized, double blind clinical trial of 81 patients in
Brazil comparing different dosages of chloroquine (1200 mg daily vs 450 mg
daily) in the treatment of COVID-19. Study found increased incidence of
prolonged QT and a trend toward lethality in the high dose treatment arm. Total
fatality rate in the cohort was 13.5%. Of note, patients over age 75 were only
enrolled in the high dose treatment arm (12.2% of patients in high dose arm),
and the age of the high dose arm was significantly higher than the low dose
treatment arm (p=0.02). Lastly, this was a fairly sick cohort of patients at
baseline with 43.2% of patients in the ICU and 88.9% on some form of
respiratory therapy prior to treatment.
·
Randomized controlled trial of 22 COVID-19 positive, symptomatic
patients treated with either chloroquine 500mg twice daily or
Lopinavir/Rotinavir 400/100mg twice daily for 10 days. All chloroquine treated
patients were PCR negative for SARS-CoV-2 by day 13 and 92% of
Lopinavir/Rotinavir treated patients were PCR negative by day 14. All
chloroquine treated patients were discharged from the hospital by day 14
compared to only 50% of Lopinavir/Rotinavir treated patients. Of note, the
average time from symptom onset to treatment was 2.5 days and 6.5 days in the
chloroquine and Lopinavir/Rotinavir groups, respectively (P = < 0.001).
·
Case report of symptomatic COVID-19 positive patient admitted
with irregular ECG, prolonged QT interval and diagnosis of acute myocarditis.
The patient was then treated with hydroxychloroquine and lopinavir/ritonavir.
Shortly thereafter, ECG normalized, prolonged QT resolved and the patient was
discharged.
·
In SĆ£o Paulo, the Prevent Senior hospital had 96 deaths from coronavirus
until March 22, 2020. Since the hospital adopted a protocol of early treatment with
HCQ, AZ and zinc, it has not registered any additional deaths
from COVID-19 and had only one patient in the ICU. April 4, 2020
·
Of 3005 COVID-19 positive patients at the MƩditerranƩe Infection
hospitals (APHM/IHU) in France (as of April 4), 1818 patients have been treated with HCQ and AZ. Below
are the outcomes:
COVID-19 patients NOT treated with HCQ+AZ: 1187
Deaths: 28 (2.4%)
COVID-19 patients treated with HCQ+AZ: 1818
Deaths: 5 (0.3%)
Assuming randomization of these patients to treatment and control groups
(unknown if this was actually the case), the Chi-square test p-value
would be <0.00001. April 4, 2020
·
The COVID-19 Global Rheumatology Alliance says no
evidence of a protective effect from hydroxychloroquine against COVID-19 in a
self-report survey of patients on the medication. April 4, 2020
·
Vladimir Zelenko, a board-certified family practitioner in New York, treated his 700th coronavirus patient with
combination therapy of HCQ, AZ and Zinc. Of these patients, 694 recovered with outpatient therapy and, of the
6 requiring hospitalization, only one patient died after, per Dr. Zelenko, not
following his treatment protocol. April 3, 2020
·
A global survey by Sermo of 6,227 verified physicians found
that hydroxychloroquine (HCQ) and azithromycin (AZ) were the most used
treatments (outside of analgesics) in the treatment of COVID-19. Out of 15 drug options, HCQ was also voted the most effective
therapy. April 2, 2020
·
The US FDA issued an
Emergency Use Authorization for hydroxychloroquine
and chloroquine in treatment of novel-coronavirus. March 29, 2020
·
In an opinion piece in the Wall Street Journal on “An
Update on the Coronavirus Treatment”, Dr. Jeff Colyer, former governor of
Kansas, states:
For my entire career, I have taken a conservative
approach to medicine. I don’t want to give false or premature hope. All of this
is subject to further refinement as more information arrives. But likewise I
can’t ignore the available evidence. This [HCQ + AZ] appears to be the best
widely available option for treating Covid-19 and not merely easing the
suffering from the disease. It would be irresponsible not to pursue
this option aggressively. March 29, 2020
·
In a non-randomized trial of 11 COVID-19 positive patients (10/11
with fever and on nasal oxygen) at the Saint Louis Hospital in France,
treatment with hydroxychloroquine (600mg for 10 days) and azithromycin (500mg
day 1 and 250mg days 2-5) showed no antiviral activity or clinical benefit. One
patient experienced a prolonged QT interval from 405ms to 460/470ms on day 4 of
treatment. March 28, 2020
·
In a trial by Dr. Didier Raoult in South France of 80
patients treated with HCQ and AZ, 98% of patients had negative viral cultures
on day 5 and 93% with negative PCR tests on day 8. When compared with prior
studies by F Zhou et al (The Lancet) and KKW To et al (The Lancet) that demonstrated 50% and 30% of patients with
viral shedding by day 20, respectively, Raoult et al shows that viral shedding
times may substantially decrease with early HCQ and AZ treatment in
COVID-19. This suggests that early treatment may
decrease the spread of novel-coronavirus infection. March 27, 2020
·
Unpublished data from an open-label, multicenter, non-randomized trial
in China of 197 patients showed that COVID-19 positive patients treated with chloroquine for 10 days had a higher rate of
negative PCR testing by day 10 compared to controls (91.4% vs 57.4%,
P < 0.001) and a shorter duration of fever (P
= 0.003). Video and results slide here. March 26, 2020
·
Energetics based modeling of hydroxychloroquine
and azithromycin binding to the SARS-CoV-2 Spike (S)Protein-ACE2 Complex shows
that hydroxychloroquine may increase the acidity of the ACE2 system in the
interaction between the ACE2 and SARS-CoV-2 spike that results in degradation
of the spike, and potentially the discontinuation of the virus’ ability to
spread further. Azithromycin on the other hand, may more directly block the
binding interaction between SARS-CoV-2 spike and ACE2 complex. March 23, 2020
·
In a randomized clinical trial by Z Chen et al (preprint) of
62 patients who received standard therapy vs standard therapy and HCQ, the patients who received HCQ had a significantly shorter time to
body temperature recovery and cough remission. Also of note, 4
patients (13%) in the control group progressed to severe illness whereas no
patients treated with HCQ progressed. March 22, 2020
·
A review of available clinical evidence on chloroquine and
hydroxychloroquine in the treatment of COVID-19 in patients
with or without diabetes concluded that these therapies
had minimal risk and should be carefully considered for clinical use as
experimental drugs. March 22, 2020
·
The National Task Force for
COVID-19 in India recommends
hydroxychloroquine for prophylaxis in “Asymptomatic healthcare
workers involved in the care of suspected or confirmed cases of
COVID-19.” March 21, 2020
·
Dr, Hu Bijie, Shanghai Combined Task Force on COVID-19 on treatment options for COVID-19 states:
In regard to the use of antiviral drugs, anti-HIV
medication Lopinavir/Ritonavir, and a broad spectrum anti-viral drug, Abitor,
the overall result compared to placebo group showed no significant difference…We
truly felt hydroxychloroquine is the specific drug of choice for COVID-19. March
20, 2020
·
A Nature article in Cell Discovery demonstrated
that hydroxychloroquine is effective in inhibiting SARS-CoV-2 infection in
vitro by blocking the transport of SARS-CoV-2 from EEs to ELs—a requirement to
release viral genome. Authors conclude that “In combination with its
anti-inflammatory function, we predict that the drug [hydroxychloroquine] has a
good potential to combat the disease.” March 18, 2020
·
Didier Raoult publishes on hydroxychloroquine and azithromycin as a treatment of COVID-19 in
an open-label non-randomized clinical trial of 36 patients (14 treated with
HCQ, 6 treated with HCQ+AZ, and 16 controls) that demonstrated significantly
faster elimination of virus by PCR testing in the treatment group. All 6 patients in the HCQ+AZ treatment arm were virologically cured
by day 6 of treatment. March 17, 2020
·
In a report disseminated by Elon Musk on
Twitter, James Todaro, MD and Gregory Rigano, Esq explore the growing
evidence of Chloroquine as a highly effective treatment and prophylaxis for
COVID-19. Full report available here. March 13, 2020
·
In vitro study published by Oxford University Press of
the antiviral activity of hydroxychloroquine in treatment of SARS-CoV-2
showed hydroxychloroquine to be about three times more potent than
chloroquine in inhibiting SARS-CoV-2. March 9, 2020
·
An expert consensus by the Guangdong Provincial Department of Science
and Technology and Guangdong Provincial Health Commission determined
that chloroquine may shorten hospital stay and improve patient
outcomes. Treatment of COVID-19 was standardized with 500mg
chloroquine phosphate, twice a day for 10 days. February
20, 2020
·
South Korea guidelines from the COVID-19 Central
Clinical Task Force propose treatment with daily chloroquine or, alternatively,
daily hydroxychloroquine if chloroquine is unavailable. February 13, 2020
Upcoming clinical trials on efficacy of HCQ in prevention of COVID-19
Active trials, no longer recruiting:
1.
Randomized, double-blind, placebo controlled trial comparing prophylaxis of daily single dose of tenofovir
disoproxil fumarate (245 mg)/ Emtricitabine (200 mg), a daily single dose of hydroxychloroquine (200 mg), a
daily single dose of TDF (245 mg)/FTC (200 mg) plus HCQ (200 mg) versus
placebo, during 12 weeks in hospital healthcare workers with primary outcome of
incidence of symptomatic COVID-19.
2.
Estimated enrollment: 4000 participants
3.
Research organization: Plan Nacional sobre el Sida
(Spain)
4.
Estimated completion date: July 31, 2020
Trials recruiting:
1.
Non-randomized open-label trial comparing prophylaxis of hydroxychloroquine (400mg twice
a day) in healthcare workers versus those healthcare workers
who opt out of receiving hydroxychloroquine that will serve as controls with
primary outcome of rate of COVID-19 positive conversion on weekly NP sampling.
2.
Estimated enrollment: 360 participants
3.
Research organization: Baylor Research Institute (USA)
4.
Estimated completion date: July 30, 2020
1.
Randomized, quadruple-blind, placebo controlled trial comparing prophylaxis of weekly hydroxychloroquine
(400mg) versus placebo in healthcare works for 6 months with
primary outcome confirmed positive testing for COVID-19.
2.
Estimated enrollment: 440 participants
3.
Research organization: Barcelona Institute for Global
Health (Spain)
4.
Estimated completion date: October 30, 2020
1.
Pre-exposure Prophylaxis for SARS-Coronavirus-2: A Pragmatic
Randomized Clinical Trial
1.
Randomized, quadruple-blind, placebo controlled trial comparing prophylaxis of weekly hydroxychloroquine (400
mg) or twice weekly hydroxychloroquine (400 mg) versus placebo
in healthcare works for 12 weeks with primary outcome negative testing for
COVID-19.
2.
Estimated enrollment: 3500 participants
3.
Research organization: University of Minnesota (USA)
4.
Estimated completion date: August 2020
Trials not yet recruiting:
1.
The PATCH Trial (Prevention And Treatment of COVID-19 With
Hydroxychloroquine)
1.
Randomized, double-blind, placebo controlled trial comparing prophylaxis of daily hydroxychloroquine (600
mg) versus placebo in healthcare works for 2 months with
primary outcome positive testing for COVID-19.
2.
Estimated enrollment: 400 participants
3.
Research organization: University of Pennsylvania
(USA)
4.
Estimated completion date: December 1, 2021
1.
Randomized, quadruple-blind, placebo controlled trial comparing prophylaxis of daily hydroxychloroquine (400
mg twice daily for day 1, followed by 200 mg twice daily for days 2-5) versus
placebo in household contacts of COVID-19 patients with primary outcome
symptomatic, positive testing for COVID-19 within 14 days.
2.
Estimated enrollment: 1600 participants
3.
Research organization: Columbia University (USA)
4.
Estimated completion date: March 2021/2022
1.
Randomized, triple-blind, placebo controlled trial comparing prophylaxis of daily hydroxychloroquine (400
mg twice daily for day 1, followed by 200 mg daily) versus
placebo in healthcare works for 2.5 months with primary outcome positive
testing for COVID-19.
2.
Estimated enrollment: 1200 participants
3.
Research organization: Centre Hospitalier
Universitaire de Saint Etienne (France)
4.
Estimated completion date: November 30, 2020
1.
Randomized, single-blind, placebo controlled trial comparing prophylaxis of daily hydroxychloroquine (400
mg daily for days 1-3, followed by 200 mg daily for an additional 11
days) versus placebo comparator ascorbic acid in household
contacts of COVID-19 patients with primary outcome positive PCR testing for
COVID-19 within 14 days.
2.
Estimated enrollment: 2000 participants
3.
Research organization: University of Washington in
collaboration with NYU and Bill and Melinda Gates Foundation (USA)
4.
Estimated completion date: October 31, 2020
1.
Will Hydroxychloroquine Impede or Prevent COVID-19: WHIP COVID-19
Study
1.
Randomized, triple-blind, placebo controlled trial comparing prophylaxis of daily hydroxychloroquine (400
mg loading dose on day 1 followed by 200 mg daily), weekly hydroxychloroquine
(400 mg weekly) versus placebo in healthcare workers with
primary outcome positive testing for COVID-19 within 8 weeks
2.
Estimated enrollment: 3000 participants
3.
Research organization: Henry Ford Hospital (USA)
4.
Estimated completion date: June 30, 2020
Antiviral
properties of azithromycin
·
A Schƶgler, et al. Novel antiviral properties of
azithromycin in cystic fibrosis airway epithelial cells. European Respiratory
Journal Feb 2015, 45 (2) 428-439; DOI: 10.1183/09031936.00102014.
·
Summary: The antibiotic azithromycin
demonstrates antiviral properties in human bronchial epithelial cells possibly
by amplifying the response mediated by the IFN pathway.
·
Kakeya H, Seki M, Izumikawa K, et al. Efficacy of
combination therapy with oseltamivir phosphate and azithromycin for influenza:
a multicenter, open-label, randomized study. PLoS One. 2014;9(3):e91293.
Published 2014 Mar 14. doi:10.1371/journal.pone.0091293.
·
Summary: A randomized trial of 107 patients with influenza A who
received either combination therapy with oseltamivir and azithromycin or monotherapy
with oseltamivir that showed combination therapy with
azithromycin resulted in early resolution of symptoms.
·
V Gielen, SL Johnston, MR Edwards. Azithromycin
induces anti-viral responses in bronchial epithelial cells. European
Respiratory Journal 2010 36: 646-654; DOI: 10.1183/09031936.00095809.
·
Summary: Azithromycin has anti-rhinoviral activity in bronchial
epithelial cells and increases the production of interferon-stimulated genes
upon infection. This benefit was not seen with erythromycin or telithromycin.
·
MT Labro. Anti-inflammatory activity of
macrolides: a new therapeutic potential?, Journal of Antimicrobial
Chemotherapy, Volume 41, Issue suppl_2, 1 March 1998, Pages 37–46,
https://doi.org/10.1093/jac/41.suppl_2.37.
·
Summary: A review of in vitro and ex vivo studies that short-term administration of macrolide antibiotics may enhance the
immune response while long-term administration results in
immunosuppression.
·
Menzel M, Akbarshahi H, Bjermer L, Uller L. Azithromycin
induces anti-viral effects in cultured bronchial epithelial cells from COPD
patients. Sci Rep. 2016;6:28698. Published 2016 Jun 28. doi:10.1038/srep28698.
·
Summary: Azithromycin increased rhinovirus-induced expression of
interferons in bronchial epithelial cells from COPD donors compared to cells
from healthy donors. These effects could reduce bronchial viral load, and
support azithromycin’s role in prevention of exacerbations of COPD.
Cardiac injury
and myocarditis in COVID-19
·
S Sala, et al. Acute myocarditis presenting as a reverse
Tako-Tsubo syndrome in a patient with SARS-CoV-2 respiratory infection,
European Heart Journal, ehaa286, https://doi.org/10.1093/eurheartj/ehaa286
·
Summary: Case report of a symptomatic COVID-19 positive
patient admitted with irregular ECG, prolonged QT interval and biopsy confirmed
diagnosis of acute myocarditis. The patient was then treated with hydroxychloroquine and
lopinavir/ritonavir. Shortly thereafter, ECG normalized, prolonged QT resolved and the patient was
discharged.
·
Arentz M, Yim E, Klaff L, et al. Characteristics
and Outcomes of 21 Critically Ill Patients With COVID-19 in Washington State.
JAMA. Published online March 19, 2020. doi:10.1001/jama.2020.4326.
·
Summary: In a case series of 21 critically ill novel-coronavirus
patients in Washington State, 7 patients (33%) developed
cardiomyopathy.
·
Shi S, Qin M, Shen B, et al. Association of
Cardiac Injury With Mortality in Hospitalized Patients With COVID-19 in Wuhan,
China. JAMA Cardiol. Published online March 25, 2020.
doi:10.1001/jamacardio.2020.0950.
·
Summary: In a cohort of 416 hospitalized patients in
Wuhan, China, 82 patients (19.7%) had cardiac injury. ECGs were
performed on only 22 patients with cardiac injury (26.8%), with 14 patients
undergoing ECG during periods of elevated cardiac biomarkers. All 14 ECGs were
abnormal. The article does not specify if any patients received
hydroxychloroquine or chloroquine.
·
Bansal M. Cardiovascular disease and COVID-19
[published online ahead of print, 2020 Mar 25]. Diabetes Metab Syndr.
2020;14(3):247–250. doi:10.1016/j.dsx.2020.03.013.
·
Summary: A literature search shows that approximately
8-12% of all COVID-19 patients experience cardiac abnormality/myocardial injury.
Safety profile
of hydroxychloroquine and azithromycin
·
H Jung, et al. The protective effect of
antimalarial drugs on thrombovascular events in systemic lupus erythematosus.
07 January 2010. https://doi.org/10.1002/art.27289.
·
Summary: Case control study of 162 SLE patients treated with
hydroxychloroquine or other antimalarial drugs vs those untreated were assessed
for rate of thrombovascular events. Antimalarial drugs including
hydroxychloroquine were shown to be thromboprotective with a risk reduction in
thrombovascular events of 68%.
·
N Costedoat-Chalumeau, et al. Heart conduction
disorders related to antimalarials toxicity: an analysis of electrocardiograms
in 85 patients treated with hydroxychloroquine for connective tissue diseases,
Rheumatology, Volume 46, Issue 5, May 2007, Pages 808–810, https://doi.org/10.1093/rheumatology/kel402.
·
Summary: Study of 85 patients with autoimmune disorders treated with hydroxychloroquine for at least one year showed no
significant increase in PR interval, QTc interval, heart rate or conduction
disorders, demonstrating safety of hydroxychloroquine.
·
CI Wu, et al. SARS-CoV-2, COVID-19 and inherited
arrhythmia syndromes. Heart Rhythm. March 28, 2020. DOI:
https://doi.org/10.1016/j.hrthm.2020.03.024
·
Summary: The QT-prolonging effect of chloroquine is “very modest, and in
general it does not result in clinically significant QT-prolongation in
patients without LQTS.” The combination of hydroxychloroquine with remdesivir
or azithromycin may result in QT-prolongation, however, and ECG monitoring is
recommended.
·
NJ White. Cardiotoxicity of antimalarial drugs.
Lancet Infect Dis. 2007 Aug;7(8):549-58. DOI: 10.1016/S1473-3099(07)70187-1.
·
Summary: Chloroquine can result in hypotension when injected rapidly and
cardiovascular collapse with self-poisoning. Transiently hypotensive plasma
concentrations of chloroquine can occur with intramuscular or subcutaneous
injections of 5mg base/kg or more.
·
Kimani J, Phiri K, Kamiza S, et al. Efficacy and
Safety of Azithromycin-Chloroquine versus Sulfadoxine-Pyrimethamine for
Intermittent Preventive Treatment of Plasmodium falciparum Malaria Infection in
Pregnant Women in Africa: An Open-Label, Randomized Trial. PLoS One. 2016;11(6):e0157045.
Published 2016 Jun 21. doi:10.1371/journal.pone.0157045.
·
Summary: Randomized, Phase 3 trial showing no drug related deaths in 1446 pregnant women treated with 620mg
chloroquine in combination with 1000mg azithromycin daily for 3
days.
·
Cook JA, Randinitis EJ, Bramson CR, Wesche DL. Lack
of a pharmacokinetic interaction between azithromycin and chloroquine. Am J
Trop Med Hyg 2006; 74:407–12.
·
Summary: Randomized, Phase 1 trial showing no clinically relevant pharmacokinetic interaction in 24 subjects
receiving 500-1000mg chloroquine & 1000mg azithromycin daily for
3 days.
·
Chico RM, Chandramohan D. Azithromycin plus
chloroquine: combination therapy for protection against malaria and sexually
transmitted infections in pregnancy. Expert Opin Drug Metab Toxicol.
2011;7(9):1153–1167. doi:10.1517/17425255.2011.598506.
·
Summary: Expert opinion finds chloroquine and
azithromycin safely given any time in pregnancy. Pharmacokinetics
in pregnancy suggest dose adjustments not necessary for azithromycin but
chloroquine dosing needs to be 600 mg.
·
Ray WA, Murray KT, Hall K, Arbogast PG, Stein CM. Azithromycin
and the risk of cardiovascular death. N Engl J Med. 2012;366(20):1881–1890.
doi:10.1056/NEJMoa1003833.
·
Summary: Out of a cohort of 347,795 prescriptions of azithromycin,
1,348,672 prescriptions of amoxicillin and 1,391,180 control periods, there was an additional 47 cardiovascular deaths per million
prescription courses in the azithromycin cohort compared to amoxicillin cohort (P
= 0.002).
·
MW Dunne, et al. A Multicenter Study of
Azithromycin, Alone and in Combination with Chloroquine, for the Treatment of
Acute Uncomplicated Plasmodium falciparum Malaria in India, The Journal of
Infectious Diseases, Volume 191, Issue 10, 15 May 2005, Pages 1582–1588, https://doi.org/10.1086/429343.
·
Summary: Open-label study of combination therapy of hydroxychloroquine
and azithromycin in treatment of falciparum malaria in 64 subjects demonstrated
only mild side effects of medication that did not require
discontinuation of therapy.
·
World Health Organization. The cardiotoxicity of
antimalarials. WHO Evidence Review Group Meeting, 13–14 October 2016. VarembĆ©
Conference Centre, Geneva, Switzerland.
·
Summary: “Apart from halofantrine, antimalarial medicines that prolong
the QT/QTc interval, such as quinine, chloroquine,
artesunate-amodiaquine and dihydroartemisinin-piperaquine, have been associated with a low risk of cardiotoxicity.”
·
Chun-Yu Chen, Feng-Lin Wang & Chih-Chuan Lin (2006).
Chronic Hydroxychloroquine Use Associated with QT Prolongation and Refractory
Ventricular Arrhythmia, Clinical Toxicology, 44:2, 173-175, DOI:
10.1080/15563650500514558.
·
Summary: A case report of a 67-year-old female with SLE treated with
daily hydroxychloroquine for one year who developed prolonged QT interval and,
subsequently, Torsades de pointes that resolved after discontinuation of
hydroxychloroquine.
·
JP O’Laughlin, PH Mehta, BC Wong. Life Threatening
Severe QTc Prolongation in Patient with Systemic Lupus Erythematosus due to
Hydroxychloroquine. Hindawi, Case Reports on Cardiology, Volume 2016, Article
ID 4626279, 4 pages, DOI: 10.1155/2016/4626279.
·
Summary: A case report of a 50-year-old female with SLE and renal
failure treated with daily hydroxychloroquine for two years who developed
prolonged QT interval and, subsequently, syncope. The prolonged QT interval did
not improve after discontinuation of hydroxychloroquine, and was possibly due
to underlying SLE cardiomyopathy.
·
Mitra, Raman L. et al. An algorithm for managing
QT prolongation in Coronavirus Disease 2019 (COVID-19) patients treated with
either chloroquine or hydroxychloroquine in conjunction with azithromycin:
Possible benefits of intravenous lidocaine. HeartRhythm Case Reports. https://doi.org/10.1016/j.hrcr.2020.03.016.
·
Summary: A case report of a 66-year-old female with RA, pulmonary
fibrosis and asthma (not on hydroxychloroquine) presenting with COVID-19.
Patient was treated with azithromycin for 3 days before adding
hydroxychloroquine. After one dose of hydroxychloroquine, however, the QT
interval prolonged to 620ms. Hydroxychloroquine was discontinued and IV
lidocaine was started with improvement of QT interval. The patient was then
able to complete the course of hydroxychloroquine, but expired shortly
thereafter from multi-organ system failure.
Antiviral
effects of zinc supplements and synergy with chloroquine
·
Xue J, Moyer A, Peng B, Wu J, Hannafon BN, Ding WQ. Chloroquine
is a zinc ionophore. PLoS One. 2014;9(10):e109180. Published 2014 Oct 1.
doi:10.1371/journal.pone.0109180.
·
Summary: The combination of zinc with chloroquine
enhanced chloroquine’s cytotoxicity in human cancer cells. Addition
of copper or iron ions had no effect on chloroquine-induced zinc uptake.
·
A Velthuis, et al. Zn Inhibits Coronavirus and
Arterivirus RNA Polymerase Activity In Vitro and Zinc Ionophores Block the
Replication of These Viruses in Cell Culture. (2010). PLoS pathogens. 6.
e1001176. 10.1371/journal.ppat.1001176.
·
Summary: In vitro study showing that increased intracellular zinc
concentration via zinc-ionophores can impair the replication of RNA viruses,
including SARS-CoV-1, in cell cultures.
·
The Zinc Against Plasmodium Study Group. Effect of zinc
on the treatment of Plasmodium falciparum malaria in children: a randomized
controlled trial, The American Journal of Clinical Nutrition, Volume 76, Issue
4, October 2002, Pages 805–812, https://doi.org/10.1093/ajcn/76.4.805.
·
Summary: Zinc in combination with chloroquine does not
reduce fever, parasitemia or appear to have a beneficial effect in the treatment
of acute, uncomplicated falciparum malaria in children compared
to monotherapy with chloroquine.
·
Singh M, Das Zinc for the common cold.
Cochrane Database of Systematic Reviews 2013, Issue 6. Art. No.: CD001364. DOI:
10.1002/14651858.CD001364.pub4.
·
Summary: Systematic review of randomized, double-blind,
placebo-controlled trials shows zinc administered within the
first 24 hours of symptom onset and in doses ≥ 75 mg/day significantly reduces
the duration of symptoms caused by the common cold. There was
insufficient data to assess a prophylactic effect.
·
Singh M, Das Zinc for the common cold.
Cochrane Database of Systematic Reviews 2011, Issue 2. Art. No.: CD001364. DOI:
10.1002/14651858.CD001364.pub3.
·
Summary: Systematic review of randomized, double-blind,
placebo-controlled trials shows zinc administered within the first 24 hours of
symptom onset significantly reduces the severity and duration of symptoms
caused by viruses in the common cold.
·
HemilƤ H. Zinc lozenges may shorten the duration
of colds: a systematic review. Open Respir Med J. 2011;5:51–58. doi:10.2174/1874306401105010051.
·
Summary: A meta-analysis of 13 placebo-controlled trials on the
therapeutic effect of zinc lozenges on the common cold demonstrates that zinc supplements over 75mg daily significantly reduced the
duration of the common cold. There was no significant difference in zinc
supplement doses under 75 mg daily.
Efficacy of
chloroquine against SARS-CoV-1
·
Vincent, M.J., Bergeron, E., Benjannet, S. et al. Chloroquine
is a potent inhibitor of SARS coronavirus infection and spread. Virol J 2, 69
(2005). https://doi.org/10.1186/1743-422X-2-69.
·
Summary: Chloroquine is effective in preventing the spread of SARS-CoV
in cell culture before and after exposure to the virus in primate cells,
suggesting both prophylactic and therapeutic advantage.
·
Keyaerts, L. Vijgen, P. Maes, J. Neyts, M. Van Ranst. In
vitro inhibition of severe acute respiratory syndrome coronavirus by
chloroquine. Biochem Biophys Res Commun, 323 (2004), pp. 264-268,
10.1016/j.bbrc.2004.08.085.
·
Summary: Chloroquine is an effective inhibitor of the replication of
SARS-CoV in vitro.
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This is not medical advice and is for informational purposes only. Any
mention of dosages is for informational purposes only and not for medical use.
Please consult a medical professional.
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