COVID-19 early treatment: real-time analysis of 1,352 studies

Assessing the therapeutic potential of angomelatine, ramelteon, and melatonin against SARS-Cov-2

Kumar Yadalam et al., Saudi Journal of Biological Sciences, doi:10.1016/j.sjbs.2022.01.049 (Peer Reviewed)

In Silico study of melatonin, angomelatine, and ramelteon for SARS-CoV-2, predicting significant SARS-CoV-2 RBD and ACE2 binding with all three.

Kumar Yadalam et al., 1/25/2022, peer-reviewed, 14 authors.

In Silico studies are an important part of preclinical research, however results may be very different in vivo.

Systematic review and meta-analysis of randomized trials of hydroxychloroquine for the prevention of COVID-19

Garcia-Albeniz et al., medRxiv, doi:10.1101/2020.09.29.20203869 (Preprint) (meta analysis)

Systematic review and meta-analysis of HCQ prophylaxis RCTs showing a statistically significant reduction in cases for pre-exposure prophylaxis.

For PEP trials there were very long treatment delays - in one trial about a third of participants were enrolled 4 days after exposure with an additional shipping delay of ~46 hours on average, and in another trial participants were enrolled up to 7 days after exposure, with an unknown additional delay before treatment, and results suggesting that exposure detection was delayed.

risk of case, 28.0% lower, RR 0.72, p = 0.004, PrEP.

risk of case, 9.0% lower, RR 0.91, p = 0.46, PEP.

Garcia-Albeniz et al., 1/25/2022, preprint, 5 authors.

Is There a Crucial Link Between Vitamin D Status and Inflammatory Response in Patients With COVID-19?

Saponaro et al., Frontiers in Immunology, doi:10.3389/fimmu.2021.745713 (Peer Reviewed)

Retrospective 93 COVID-19 pneumonia patients in Italy, showing low vitamin D levels associated with severe ARDS, and significantly lower vitamin D levels for non-survivors.

risk of ARDS, 36.5% lower, RR 0.64, p = 0.43, high D levels (≥20ng/ml) 5 of 32 (15.6%), low D levels (<20ng/ml) 15 of 61 (24.6%), NNT 11, severe ARDS.

Saponaro et al., 1/24/2022, retrospective, Italy, Europe, peer-reviewed, 13 authors, study period March 2020 - May 2020.

Lack of Ronapreve (REGN-CoV; casirivimab and imdevimab) virological efficacy against the SARS-CoV 2 Omicron variant (B.1.1.529) in K18-hACE2 mice

Tatham et al., bioRxiv, doi:10.1101/2022.01.23.477397 (Preprint)

K18-hACE2 mouse study showing that casirivimab/imdevimab was not effective for omicron at doses 2x higher than those effective for previous variants.

Tatham et al., 1/24/2022, preprint, 15 authors.

SARS-CoV-2 Viral Genes Compromise Survival and Functions of Human Pluripotent Stem Cell-derived Cardiomyocytes via Reducing Cellular ATP Level

Liu et al., bioRxiv, doi:10.1101/2022.01.20.477147 (Preprint) (In Vitro)

In Vitro study showing that ivermectin and meclizine may be protective for heart muscle damage due to SARS-CoV-2.

Liu et al., 1/23/2022, preprint, 15 authors.

In Vitro studies are an important part of preclinical research, however results may be very different in vivo.

Comparative Analysis of Serum Zinc, Copper and Magnesium Level and Their Relations in Association with Severity and Mortality in SARS-CoV-2 Patients

PVSN et al., Biological Trace Element Research, doi:10.1007/s12011-022-03124-7 (Peer Reviewed)

Analysis of 150 COVID+ hospitalized patients in India, showing lower zinc levels associated with higher severity.

PVSN et al., 1/22/2022, India, South Asia, peer-reviewed, 14 authors.

Serum zinc levels in pediatric patients with COVID-19

Ekemen Keleş et al., European Journal of Pediatrics, doi:10.1007/s00431-021-04348-w (Peer Reviewed)

Prospective study of 100 COVID+ pediatric patients in Turkey, showing significantly increased risk of hospitalization for patients with zinc deficiency.

risk of hospitalization, 75.3% lower, RR 0.25, p = 0.01, high zinc levels (≥70μg/dL) 10 of 89 (11.2%), low zinc levels (<70μg/dL) 5 of 11 (45.5%), NNT 2.9.

Ekemen Keleş et al., 1/22/2022, prospective, Turkey, Europe, peer-reviewed, 7 authors, study period 3 August, 2020 - 15 November, 2020.

COVID-19 pneumonia patients with 25(OH)D levels lower than 12 ng/ml are at increased risk of death

Juraj et al., International Journal of Infectious Diseases, doi:10.1016/j.ijid.2022.01.044 (Peer Reviewed)

Retrospective 357 COVID-19 pneumonia patients in Slovakia, showing higher mortality with vitamin D deficiency (<12ng/mL). All patients received vitamin D supplementation in hospital. In multivariable linear regression, vitamin D levels were independently associated with mortality (p=0.0398).

risk of death, 19.0% lower, RR 0.81, p = 0.05, high D levels (≥12ng/mL) 127 of 283 (44.9%), low D levels (<12ng/mL) 41 of 74 (55.4%), NNT 9.5.

Juraj et al., 1/22/2022, retrospective, Slovakia, Europe, peer-reviewed, 13 authors, study period 1 November, 2020 - 30 April, 2021.

Inhibitory effects of specific combination of natural compounds against SARS-CoV-2 and its Alpha, Beta, Gamma, Delta, Kappa, and Mu variants

Goc et al., European Journal of Microbiology and Immunology, doi:10.1556/1886.2021.00022 (Peer Reviewed) (In Vitro)

In Vitro study testing combinations of plant extracts and micronutrients with several variants of SARS-CoV-2. A combination of vitamin C, N-acetylcysteine, curcumin, quercetin, resveratrol, theaflavin, naringenin, baicalin, and broccoli extract showed the highest inhibition of RBD binding, and also decreased RdRp, furin, and cathepsin L activity.

Goc et al., 1/21/2022, peer-reviewed, 5 authors.

In Vitro studies are an important part of preclinical research, however results may be very different in vivo.

Cannabidiol inhibits SARS-CoV-2 replication through induction of the host ER stress and innate immune responses

Nguyen et al., Science Advances, doi:10.1126/sciadv.abi6110 (preprint 3/10/2021) (Peer Reviewed)

Retrospective 1,212 patients in the USA with a history of seizure-related conditions, showing patients treated with CBD100 had significantly lower incidence of COVID-19 cases compared to a matched control group.

In Vitro study showing CBD inhibits SARS-CoV-2 with Vero E6 and Calu-3 cells. Mouse study showing CBD significantly inhibited viral replication in the lung and nasal turbinate.

Authors note that CBD does not inhibit ACE2 expression or the main viral proteases, inhibition occurs after viral entry. Authors stress several limitations for use at this time, including purity, quality, and the formulation of products, and potential lung damage based on administration method.

Authors recommend clinical trials, but do not mention the existing RCT by Crippa et al.

risk of case, 49.6% lower, RR 0.50, p = 0.006, treatment 26 of 531 (4.9%), control 48 of 531 (9.0%), NNT 24, OR converted to RR, active CBD100 users.

risk of case, 32.9% lower, RR 0.67, p = 0.009, treatment 75 of 1,212 (6.2%), control 108 of 1,212 (8.9%), NNT 37, OR converted to RR, all CBD100 users.

Nguyen et al., 1/20/2022, retrospective, USA, North America, peer-reviewed, 34 authors.

Metformin use in patients hospitalized with COVID-19: lower inflammation, oxidative stress, and thrombotic risk markers and better clinical outcomes

Usman et al., Journal of Thrombosis and Thrombolysis, doi:10.1007/s11239-022-02631-7 (Peer Reviewed)

Retrospective 75 diabetes patients, 34 on metformin, showing improved clinical outcomes with treatment, without statistical significance.

risk of death, 59.8% lower, RR 0.40, p = 0.21, treatment 3 of 34 (8.8%), control 9 of 41 (22.0%), NNT 7.6.

risk of mechanical ventilation, 75.9% lower, RR 0.24, p = 0.05, treatment 2 of 34 (5.9%), control 10 of 41 (24.4%), NNT 5.4.

hospitalization time, 33.7% lower, relative time 0.66, p = 0.13, treatment 34, control 41.

Usman et al., 1/18/2022, retrospective, USA, North America, peer-reviewed, 10 authors.

The effect of ivermectin on non-severe and severe COVID-19 disease and gender-based difference of its effectiveness

Zubair et al., Monaldi Archives for Chest Disease, doi:10.4081/monaldi.2022.2062 (Peer Reviewed)

Retrospective 188 hospitalized patients in Pakistan, 90 treated with ivermectin, showing no significant differences with treatment. The ivermectin group had more severe disease (66% vs 58%, with 6x higher risk for severe disease patients), and more male patients (70% vs. 65%). Higher use of remdesivir and steroids in the ivermectin group also suggests that ivermectin was more likely to be given to patients in more severe condition. There were no side effects seen with ivermectin. Authors note that significantly improved ferritin levels were seen with treatment. Authors state that ivermectin patients received 2 12mg doses, 24 hours apart, but later state that the dosage was not standardized.

risk of death, 8.9% higher, RR 1.09, p = 1.00, treatment 5 of 90 (5.6%), control 5 of 98 (5.1%), unadjusted.

hospitalization time, 8.0% higher, relative time 1.08, p = 0.40, treatment 90, control 98, unadjusted, Table 3, mean number of days.

Excluded in after exclusion results of meta analysis: substantial unadjusted confounding by indication likely, unadjusted results with no group details.

Zubair et al., 1/18/2022, retrospective, Pakistan, South Asia, peer-reviewed, 8 authors, study period October 2020 - February 2021, dosage 12mg single dose.

Antiinflammatory potential of nano-curcumin as an alternative therapeutic agent for the treatment of mild-to-moderate hospitalized COVID-19 patients in a placebo-controlled clinical trial

Asadirad et al., Phytotherapy Research, doi:10.1002/ptr.7375 (Peer Reviewed)

RCT 60 hospitalized patients in Iran, 30 treated with nano-curcumin, showing significant improvements in inflammatory cytokines, and improvements in clinical outcomes without statistical significance. 240 mg/day nano-curcumin for 7 days.

risk of death, 25.9% lower, RR 0.74, p = 0.74, treatment 5 of 27 (18.5%), control 6 of 24 (25.0%), NNT 15, excluding patients that stopped treatment due to progression - 3 for curcumin and 6 for control.

risk of progression, 50.0% lower, RR 0.50, p = 0.47, treatment 3 of 30 (10.0%), control 6 of 30 (20.0%), NNT 10.0.

risk of unresolved fever, 45.3% lower, RR 0.55, p = 0.09, treatment 8 of 27 (29.6%), control 13 of 24 (54.2%), NNT 4.1.

risk of unresolved dyspnea, 28.9% lower, RR 0.71, p = 0.72, treatment 4 of 27 (14.8%), control 5 of 24 (20.8%), NNT 17.

risk of unresolved cough, 40.7% lower, RR 0.59, p = 0.36, treatment 6 of 27 (22.2%), control 9 of 24 (37.5%), NNT 6.5.

risk of O2 <92%, 36.5% lower, RR 0.63, p = 0.51, treatment 5 of 27 (18.5%), control 7 of 24 (29.2%), NNT 9.4.

risk of O2 <97%, 20.0% lower, RR 0.80, p = 0.21, treatment 18 of 27 (66.7%), control 20 of 24 (83.3%), NNT 6.0.

Asadirad et al., 1/17/2022, Randomized Controlled Trial, placebo-controlled, Iran, Middle East, peer-reviewed, 7 authors.

Effect of Subcutaneous Casirivimab and Imdevimab Antibody Combination vs Placebo on Development of Symptomatic COVID-19 in Early Asymptomatic SARS-CoV-2 Infection: A Randomized Clinical Trial

O'Brien et al., JAMA, doi:10.1001/jama.2021.24939768 (Peer Reviewed)

RCT 204 asymptomatic COVID+ patients, 100 treated with subcutaneous casirivimab/imdevimab, showing lower development of symptoms, lower hospitalization, and faster viral clearance with treatment. Study conducted prior to widespread circulation of delta and omicron in the study locations.

risk of hospitalization, 85.5% lower, RR 0.15, p = 0.25, treatment 0 of 100 (0.0%), control 3 of 104 (2.9%), NNT 35, relative risk is not 0 because of continuity correction due to zero events.

risk of hospitalization/ER, 92.2% lower, RR 0.08, p = 0.03, treatment 0 of 100 (0.0%), control 6 of 104 (5.8%), NNT 17, relative risk is not 0 because of continuity correction due to zero events.

risk of symptomatic case, 33.0% lower, RR 0.67, p = 0.04, treatment 29 of 100 (29.0%), control 44 of 104 (42.3%), NNT 7.5, OR converted to RR, day 14.

relative weeks with high viral load, 39.7% better, RR 0.60, p = 0.001, treatment 100, control 104.

O'Brien et al., 1/14/2022, Double Blind Randomized Controlled Trial, placebo-controlled, multiple countries, multiple regions, peer-reviewed, 38 authors, study period 13 July, 2020 - 28 January, 2021.

Efficacy of Melatonin in the Treatment of Patients With COVID-19: A Systematic Review and Meta-Analysis of Randomized Controlled Trials

Lan et al., Journal of Medical Virology, doi:10.1002/jmv.27595 (Peer Reviewed)

Systematic review and meta analysis including 3 of the 5 melatonin RCTs at the time, showing significantly higher recovery with treatment, and lower ICU admission and mortality without statistical signficance. The analysis only includes trials before 9/11/21. Adding Hasan (October 2021) results in statistically significant lower mortality.

Lan et al., 1/14/2022, peer-reviewed, 6 authors.

Low Rates of Hospitalization and Death in 4,376 COVID-19 Patients Given Early Ambulatory Medical and Supportive Care. A Case Series and Observational Study.

Tyson et al., Preprint (Preprint)

Retrospective 4,376 patients with mild/moderate COVID-19 in the USA treated with multiple medications including HCQ/ivermectin, favipiravir, vitamin C, D, quercetin, zinc, mAbs, budesonide, dexamethasone, prednisone, and colchicine (exact treatments specific to each patient), showing significantly lower hospitalization and mortality compared to the surrounding community.

risk of death, 99.8% lower, RR 0.002, p < 0.001, treatment 0 of 3,962 (0.0%), control 471 of 20,921 (2.3%), NNT 44, relative risk is not 0 because of continuity correction due to zero events, All AVUC mild patients vs. Imperial County (corrected).

risk of hospitalization, 99.8% lower, RR 0.002, p < 0.001, treatment 2 of 3,962 (0.1%), control 4,343 of 20,921 (20.8%), NNT 4.8, All AVUC mild patients vs. Imperial County (corrected).

risk of death, 97.0% lower, RR 0.03, p < 0.001, treatment 3 of 4,375 (0.1%), control 471 of 20,921 (2.3%), NNT 46, All AVUC patients vs. Imperial County (corrected).

risk of hospitalization, 99.0% lower, RR 0.010, p < 0.001, treatment 9 of 4,375 (0.2%), control 4,343 of 20,921 (20.8%), NNT 4.9, All AVUC patients vs. Imperial County (corrected).

Tyson et al., 1/13/2022, retrospective, USA, North America, preprint, 13 authors.

Effect of nanocurcumin supplementation on the severity of symptoms and length of hospital stay in patients with COVID-19: A randomized double-blind placebo-controlled trial

Honarkar Shafie et al., Phytotherapy Research, doi:10.1002/ptr.7374 (Peer Reviewed)

RCT 48 hospitalized patients in Iran, 24 treated with nanocurcumin, showing lower hospitalization time with treatment. The number of patients shown in Table 3 (31 and 27 for each arm) is inconsistent with the number reported as randomized to each arm (24). 160 mg/day nanocurcumin for 6 days. IRCT20131125015536N13.

hospitalization time, 28.9% lower, relative time 0.71, p = 0.22, treatment mean 6.31 (±5.26) n=23, control mean 8.87 (±8.12) n=21.

relative pulmonary involvement score, 9.1% better, RR 0.91, treatment 23, control 21.

Excluded in meta analysis: unresolved data inconsistency.

Honarkar Shafie et al., 1/12/2022, Randomized Controlled Trial, Iran, Middle East, peer-reviewed, 10 authors.

Favipiravir, umifenovir and camostat mesylate: a comparative study against SARS-CoV-2

Unal et al., bioRxiv, doi:10.1101/2022.01.11.475889 (Preprint) (In Vitro)

In Vitro and In Silico study showing that the combination of favipiravir and umifenovir or camostat mesylate has greater antiviral efficacy than single drug treatment.

Unal et al., 1/12/2022, preprint, 10 authors.

In Vitro studies are an important part of preclinical research, however results may be very different in vivo.

Effect of colchicine on mortality in patients with COVID-19 – A systematic review and meta-analysis

Zein et al., Diabetes & Metabolic Syndrome: Clinical Research & Reviews, doi:10.1016/j.dsx.2022.102395 (Peer Reviewed) (meta analysis)

Systematic review and meta analysis showing that colchicine was associated with lower mortality in COVID-19 patients:

All studies: RR 0.66 [95%CI 0.53, 0.83], p < 0.001; I2: 42%
RCTs: RR 0.81 [95%CI 0.54, 1.20], p = 0.29; I2: 10%

The RCT result is non-significant, but is highly affected by the very late stage RECOVERY trial, which is not generalizable to earlier usage.

Zein et al., 1/12/2022, peer-reviewed, 2 authors.

Prediction of mortality in hospitalized Egyptian patients with Coronavirus disease-2019: A multicenter retrospective study

AbdelGhaffar et al., PLOS ONE, doi:10.1371/journal.pone.0262348 (Peer Reviewed)

Retrospective 3,712 hospitalized patients in Egypt, showing lower mortality with HCQ treatment in unadjusted results. According to the official treatment protocol, HCQ was recommended with higher risk and/or more serious cases.

risk of death, 99.9% lower, RR 0.001, p < 0.001, treatment 0 of 238 (0.0%), control 900 of 3,474 (25.9%), NNT 3.9, relative risk is not 0 because of continuity correction due to zero events.

AbdelGhaffar et al., 1/11/2022, retrospective, Egypt, Africa, peer-reviewed, 17 authors, study period April 2020 - July 2020.

Efficacy of favipiravir in adults with mild COVID-19: a randomized, double-blind, multicenter, placebo-controlled trial clinical trial

Bosaeed et al., Clinical Microbiology and Infection, doi:10.1016/j.cmi.2021.12.026 (Peer Reviewed)

RCT with 112 favipiravir and 119 control patients showing no significant differences in outcomes. Viral clearance and clinical recovery for patients treated within 48 hours was better than those treated later. NCT04464408.

risk of ICU admission, 618.8% higher, RR 7.19, p = 0.11, treatment 3 of 112 (2.7%), control 0 of 119 (0.0%), continuity correction due to zero event.

risk of hospitalization, 218.8% higher, RR 3.19, p = 0.16, treatment 6 of 112 (5.4%), control 2 of 119 (1.7%).

time to clinical improvement, 11.9% higher, RR 1.12, p = 0.51, treatment 112, control 119, adjusted.

time to viral clearance, 14.9% higher, RR 1.15, p = 0.51, treatment 112, control 119, adjusted.

Bosaeed et al., 1/11/2022, Double Blind Randomized Controlled Trial, Saudi Arabia, Middle East, peer-reviewed, 31 authors, study period 23 July, 2020 - 4 August, 2021, average treatment delay 3.0 days.

Cannabinoids Block Cellular Entry of SARS-CoV-2 and the Emerging Variants

van Breemen et al., Journal of Natural Products, doi:10.1021/acs.jnatprod.1c00946 (Peer Reviewed) (In Vitro)

In Vitro study showing that cannabigerolic acid and cannabidiolic acid inhibited SARS-CoV-2 entry into cells.

van Breemen et al., 1/10/2022, peer-reviewed, 7 authors.

In Vitro studies are an important part of preclinical research, however results may be very different in vivo.

Metformin use is associated with a decrease in risk of hospitalization and mortality in COVID-19 diabetic patients: a population-based study in Lombardy

Ojeda-Fernández et al., Diabetes, Obesity and Metabolism, doi:10.1111/dom.14648 (Peer Reviewed)

Retrospective 31,966 COVID+ patients using anti-hyperglycemic drugs in Italy, showing lower mortality and ICU admission with metformin use.

risk of death, 16.2% lower, RR 0.84, p < 0.001, treatment 1,476 of 6,556 (22.5%), control 1,787 of 6,556 (27.3%), NNT 21, OR converted to RR, propensity score matching.

risk of death, 22.1% lower, RR 0.78, p < 0.001, treatment 968 of 6,556 (14.8%), control 1,261 of 6,556 (19.2%), NNT 22, OR converted to RR, in-hospital mortality, propensity score matching.

risk of ICU admission, 22.4% lower, RR 0.78, p = 0.01, treatment 166 of 6,556 (2.5%), control 212 of 6,556 (3.2%), NNT 143, OR converted to RR, propensity score matching.

risk of hospitalization, 2.7% lower, RR 0.97, p = 0.11, treatment 3,551 of 6,556 (54.2%), control 3,670 of 6,556 (56.0%), NNT 55, OR converted to RR, propensity score matching.

risk of death, 8.3% lower, RR 0.92, p = 0.06, treatment 793 of 3,297 (24.1%), control 876 of 3,297 (26.6%), NNT 40, OR converted to RR, excluding patients previously treated with insulin, propensity score matching.

risk of death, 16.0% lower, RR 0.84, p = 0.003, treatment 512 of 3,297 (15.5%), control 618 of 3,297 (18.7%), NNT 31, OR converted to RR, excluding patients previously treated with insulin, in-hospital mortality, propensity score matching.

risk of ICU admission, 39.2% lower, RR 0.61, p = 0.002, treatment 64 of 3,297 (1.9%), control 102 of 3,297 (3.1%), NNT 87, OR converted to RR, excluding patients previously treated with insulin, propensity score matching.

risk of hospitalization, 2.2% higher, RR 1.02, p = 0.36, treatment 1,822 of 3,297 (55.3%), control 1,792 of 3,297 (54.4%), OR converted to RR, excluding patients previously treated with insulin, propensity score matching.

Ojeda-Fernández et al., 1/10/2022, retrospective, Italy, Europe, peer-reviewed, 11 authors.

Novartis and Molecular Partners report positive topline data from Phase 2 study for ensovibep (MP0420), a DARPin antiviral therapeutic for COVID-19

Novartis Press Release (News)

EMPATHY Part A RCT with 407 patients, 301 treated with ensovibep, showing statistically significant viral load reduction (details not provided), and lower mortality and hospitalization. For discussion see [1].

[1] twitter.com/boulware_dr/status/1480505035113091073

risk of death, 89.0% lower, RR 0.11, p = 0.06, treatment 0 of 301 (0.0%), control 2 of 99 (2.0%), NNT 49, relative risk is not 0 because of continuity correction due to zero events.

risk of hospitalization, 86.8% lower, RR 0.13, p = 0.01, treatment 2 of 301 (0.7%), control 5 of 99 (5.1%), NNT 23.

risk of hospitalization/ER, 78.1% lower, RR 0.22, p = 0.02, treatment 4 of 301 (1.3%), control 6 of 99 (6.1%), NNT 21.

Novartis et al., 1/10/2022, Randomized Controlled Trial, multiple countries, multiple regions, preprint, 1 author.

Mechanisms of action of fluvoxamine for COVID-19: a historical review

Hashimoto et al., Molecular Psychiatry, doi:10.1038/s41380-021-01432-3 (Review) (Peer Reviewed)

Review of the potential mechanisms of action of fluvoxamine for COVID-19.

Hashimoto et al., 1/7/2022, peer-reviewed, 3 authors.

Effectiveness of Curcumin on Outcomes of Hospitalized COVID-19 Patients: A Systematic Review of Clinical Trials

Vahedian-Azimi et al., Nutrients, doi:10.3390/nu14020256 (Peer Reviewed)

Review of 6 COVID-19 curcumin studies showing that treatment resulted in significant improvement in symptoms, duration of hospitalization, and mortality, and a significant decrease in proinflammatory cytokines and increase in anti-inflammatory cytokines.

Vahedian-Azimi et al., 1/7/2022, peer-reviewed, 9 authors.

Hydroxychloroquine pre-exposure prophylaxis provides no protection against COVID-19 among health care workers: a cross-sectional study in a tertiary care hospital in North India

Juneja et al., Journal of Basic and Clinical Physiology and Pharmacology, doi:10.1515/jbcpp-2021-0221 (Peer Reviewed)

Retrospective 2,200 healthcare workers in India, 996 taking HCQ prophylaxis, showing no significant differences. There were large differences in the occupation of participants and therefore exposure, and the authors make no adjustments.

risk of severe case, 141.8% higher, RR 2.42, p = 0.59, treatment 2 of 996 (0.2%), control 1 of 1,204 (0.1%).

risk of case, 6.4% higher, RR 1.06, p = 0.67, treatment 103 of 996 (10.3%), control 117 of 1,204 (9.7%).

Excluded in after exclusion results of meta analysis: excessive unadjusted differences between groups.

Juneja et al., 1/7/2022, retrospective, India, South Asia, peer-reviewed, 9 authors, study period 2 April, 2020 - 3 September, 2020.

Daily Lactobacillus Probiotic versus Placebo in COVID-19-Exposed Household Contacts (PROTECT-EHC): A Randomized Clinical Trial

Wischmeyer et al., medRxiv, doi:10.1101/2022.01.04.21268275 (Preprint)

RCT 182 COVID-19 exposed patients, 91 treated with daily probiotic Lactobacillus rhamnosus GG starting a median of 3 days from exposure, showing lower symptomatic COVID-19 with treatment. There were no hospitalizations or deaths. PROTECT-EHC. NCT04399252.

risk of moderate/severe case, 33.3% lower, RR 0.67, p = 0.15, treatment 16 of 91 (17.6%), control 24 of 91 (26.4%), NNT 11.

risk of symptomatic case, 38.5% lower, RR 0.62, p = 0.02, treatment 24 of 91 (26.4%), control 39 of 91 (42.9%), NNT 6.1.

recovery time, 27.3% lower, relative time 0.73, p = 0.37, treatment 91, control 91.

risk of case, 42.9% lower, RR 0.57, p = 0.17, treatment 8 of 91 (8.8%), control 14 of 91 (15.4%), NNT 15.

Wischmeyer et al., 1/5/2022, Double Blind Randomized Controlled Trial, USA, North America, preprint, 21 authors.

Promising Effects of 3-Month Period of Quercetin Phytosome® Supplementation in the Prevention of Symptomatic COVID-19 Disease in Healthcare Workers: A Pilot Study

Rondanelli et al., Life, doi:10.3390/life12010066 (Peer Reviewed)

RCT 120 healthcare workers, 60 treated with quercetin phytosome, showing lower risk of cases with treatment. Quercetin phytosome 250mg twice a day. NCT05037240.

risk of symptomatic case, 92.9% lower, RR 0.07, p = 0.04, treatment 1 of 60 (1.7%), control 4 of 60 (6.7%), NNT 20, adjusted, Cox proportional risk.

Rondanelli et al., 1/4/2022, Double Blind Randomized Controlled Trial, placebo-controlled, Italy, Europe, peer-reviewed, 12 authors.

The SARS-CoV-2 variant, Omicron, shows rapid replication in human primary nasal epithelial cultures and efficiently uses the endosomal route of entry

Peacock et al., bioRxiv, doi:10.1101/2021.12.31.474653 (Preprint) (In Vitro)

In Vitro study showing that omicron can efficiently enter cells via the endosomal route, independent of TMPRSS2.

Peacock et al., 1/3/2022, preprint, 10 authors.

In Vitro studies are an important part of preclinical research, however results may be very different in vivo.

The hyper-transmissible SARS-CoV-2 Omicron variant exhibits significant antigenic change, vaccine escape and a switch in cell entry mechanism

Willett et al., medRxiv, doi:10.1101/2022.01.03.21268111 (Preprint) (In Vitro)

In Vitro study showing that the entry process for omicron has moved towards TMPRSS2-independent fusion, indicating that TMPRSS2 inhibitors may be less effective for omicron.

Willett et al., 1/3/2022, preprint, 38 authors.

In Vitro studies are an important part of preclinical research, however results may be very different in vivo.

Melatonin drugs inhibit SARS-CoV-2 entry into the brain and virus-induced damage of cerebral small vessels

Cecon et al., bioRxiv, doi:10.1101/2021.12.30.474561 (Preprint)

K18-hACE2 mouse study showing treatment with melatonin and derived drugs agomelatine and ramelteon inhibited SARS-CoV-2 infection in the brain.

Cecon et al., 1/3/2022, preprint, 14 authors.

Association of Vitamin D Status and COVID-19-Related Hospitalization and Mortality

Seal et al., Journal of General Internal Medicine, doi:10.1007/s11606-021-07170-0 (Peer Reviewed)

Retrospective 4,599 COVID+ veterans in the USA with vitamin D levels measured 15 to 90 days prior to testing positive, showing a significant independent inverse dose-response relationship between vitamin D levels (from 15 to 60ng/mL) and decreasing risk of hospitalization (24.1% to 18.7%, p = 0.009) and mortality (10.4% to 5.7%, p = 0.001).

risk of death, 45.1% lower, RR 0.55, p = 0.001, adjusted, 60ng/mL vs. 15 ng/mL.

risk of death, 40.5% lower, RR 0.60, p = 0.001, adjusted, 50ng/mL vs. 15 ng/mL.

risk of death, 34.6% lower, RR 0.65, p = 0.001, adjusted, 40ng/mL vs. 15 ng/mL.

risk of death, 25.9% lower, RR 0.74, p = 0.001, adjusted, 30ng/mL vs. 15 ng/mL.

risk of death, 20.0% lower, RR 0.80, p = 0.001, adjusted, 25ng/mL vs. 15 ng/mL.

risk of death, 11.5% lower, RR 0.88, p = 0.001, adjusted, 20ng/mL vs. 15 ng/mL.

risk of hospitalization, 22.5% lower, RR 0.78, p = 0.01, adjusted, 60ng/mL vs. 15 ng/mL.

risk of hospitalization, 20.0% lower, RR 0.80, p = 0.009, adjusted, 50ng/mL vs. 15 ng/mL.

risk of hospitalization, 16.7% lower, RR 0.83, p = 0.007, adjusted, 40ng/mL vs. 15 ng/mL.

risk of hospitalization, 12.3% lower, RR 0.88, p = 0.008, adjusted, 30ng/mL vs. 15 ng/mL.

risk of hospitalization, 9.1% lower, RR 0.91, p = 0.01, adjusted, 25ng/mL vs. 15 ng/mL.

risk of hospitalization, 4.8% lower, RR 0.95, p = 0.02, adjusted, 20ng/mL vs. 15 ng/mL.

Seal et al., 1/1/2022, retrospective, USA, North America, peer-reviewed, 6 authors.

In vitro Potential Antiviral SARS-CoV-19- Activity of Natural Product Thymohydroquinone and Dithymoquinone from Nigela sativia

Esharkawy et al., Bioorganic Chemistry, doi:10.1016/j.bioorg.2021.105587 (Peer Reviewed) (In Vitro)

In Vitro and In Silico study of nigella sativa components, showing anti-SARS-CoV-2 activity at non-cytotoxic nanomolar concentrations for thymohydroquinone with selectivity index 1.4.

Esharkawy et al., 1/1/2022, peer-reviewed, 3 authors.

In Vitro studies are an important part of preclinical research, however results may be very different in vivo.

Does Vitamin D Supplementation Reduce Cytokine Storm and Mortality in Geriatric Intensive Care Patients Diagnosed with COVID-19

Bilir et al., Journal of Contemporary Medicine, doi:10.16899/jcm.990057 (Peer Reviewed)

Retrospective 80 elderly ICU patients in Turkey, 40 with vitamin D levels <30ng/ml received vitamin D treatment, showing no significant differences in outcomes. Although not statistically significant, results favored treatment which suggests that supplemention was beneficial because low vitamin D levels are typically associated with worse results.

risk of death, 23.1% lower, RR 0.77, p = 0.26, treatment 20 of 40 (50.0%), control 26 of 40 (65.0%), NNT 6.7.

risk of mechanical ventilation, 3.3% lower, RR 0.97, p = 1.00, treatment 29 of 40 (72.5%), control 30 of 40 (75.0%), NNT 40.

risk of no weaning from intubation, 20.4% lower, RR 0.80, p = 0.13, treatment 20 of 29 (69.0%), control 26 of 30 (86.7%), NNT 5.6.

ICU time, 10.3% lower, relative time 0.90, p = 0.44, treatment 40, control 40.

hospitalization time, 2.9% lower, relative time 0.97, p = 0.98, treatment 40, control 40.

Excluded in meta analysis: control group formed from patients with high vitamin D levels.

Bilir et al., 1/1/2022, retrospective, Turkey, Europe, peer-reviewed, 7 authors, study period March 2021 - July 2021, dosage 50,000IU days 1, 8.

The efficacy of probiotics in patients with severe COVID-19

Wang et al., Annals of Palliative Medicine, doi:10.21037/apm-21-3373 (Peer Reviewed)

Retrospective 156 COVID-19 patients in China, showing that diarrhea was significantly more common in severe/critical cases, and for severe/critical patients experiencing diarrhea, the duration of diarrhea was shorter with probiotic treatment. There was also significant improvements in inflammatory markers and time to PCR-. Details of the treatment and control groups are not supplied.

Wang et al., 12/31/2021, retrospective, China, Asia, peer-reviewed, 8 authors.

Efficacy of Colchicine and Budesonide in Improvement Outcomes of Patients with Coronavirus Infection 2019 in Damascus, Syria: A Randomized Control Trial

Alsultan et al., Interdisciplinary Perspectives on Infectious Diseases, doi:10.1155/2021/2129006 (Peer Reviewed)

Small RCT 49 severe condition hospitalized patients in Syria, showing lower mortality with colchicine and shorter hospitalization time with both colchicine and budesonide (all of these were not statistically significant).

risk of death, 35.7% lower, RR 0.64, p = 0.70, treatment 3 of 14 (21.4%), control 7 of 21 (33.3%), NNT 8.4.

hospitalization time, 20.0% lower, relative time 0.80, treatment 14, control 21.

Alsultan et al., 12/31/2021, Randomized Controlled Trial, Syria, Middle East, peer-reviewed, 11 authors.

The Effect of Ivermectin on Reducing Viral Symptoms in Patients with Mild COVID-19

Abbas et al., Indian Journal of Pharmaceutical Sciences, doi:10.36468/pharmaceutical-sciences.spl.416 (Peer Reviewed)

RCT 99 ivermectin and 103 control low risk patients in China, up to 7 days from symptom onset, showing statistically significant improvement in recovery with treatment, and non-statistically significant improvements in recovery time and deterioration.

Authors selectively omitted the p-value for recovery which shows statistical significance. Very little information on the patients is provided (only age, gender, and insurance status). The table, text, and abstract show three different versions of recovery numbers. The table and abstract show two different versions of recovery time. The abstract contains a hazard ratio that is not in the text, and no statistical methods are reported. Given the selective omission of the statistically significant recovery p-value, three different sets of numbers for that outcome, and other inconsistencies, the data in this study does not appear to be very reliable. Administration was specified on an empty stomach, reducing lung tissue concentration by ~2.5x according to Guzzo et al. Patients >50 were excluded.

risk of death, 4.0% higher, RR 1.04, p = 1.00, treatment 1 of 99 (1.0%), control 1 of 103 (1.0%).

deterioration of 2 or more points, 40.5% lower, RR 0.59, p = 0.54, treatment 4 of 99 (4.0%), control 7 of 103 (6.8%), NNT 36.

escalation of care, 14.9% lower, RR 0.85, p = 0.82, treatment 9 of 99 (9.1%), control 11 of 103 (10.7%), NNT 63.

fever during study, 17.9% lower, RR 0.82, p = 0.58, treatment 15 of 99 (15.2%), control 19 of 103 (18.4%), NNT 30.

risk of no recovery, 35.6% lower, RR 0.64, p = 0.04, treatment 26 of 99 (26.3%), control 42 of 103 (40.8%), NNT 6.9.

recovery time, 30.8% lower, relative time 0.69, p = 0.08, treatment 99, control 103.

Excluded in after exclusion results of meta analysis: very minimal patient information, three different results for the recovery outcome, selective omission of the statistically significant recovery p-value, and other inconsistencies.

Abbas et al., 12/31/2021, Double Blind Randomized Controlled Trial, placebo-controlled, China, Asia, peer-reviewed, 3 authors, dosage 300μg/kg days 1-5.

COVID-19 In-Hospital Mortality Rate is Reduced by Prophylactic Use of Ivermectin: Findings From a City-Wide, Prospective Observational Study Using Propensity Score Matching (PSM)

Kerr et al., Research Gate, doi:10.13140/RG.2.2.26793.52327 (Preprint)

PSM retrospective 378 hospitalized patients in Brazil, showing lower mortality for patients that were on ivermectin prophylaxis before admission (not taking into account the lower risk of being hospitalized shown in the related larger study). 47124221.2.0000.5485.

risk of death, 45.0% lower, RR 0.55, p = 0.046, treatment 12 of 52 (23.1%), control 22 of 52 (42.3%), NNT 5.2, propensity score matching, multivariable.

Excluded in meta analysis: patients in this study are a subset of those in a larger study, not taking into account the lower risk of hospitalization shown in the related larger study.

Kerr et al., 12/31/2021, retrospective, propensity score matching, Brazil, South America, preprint, 9 authors, study period July 2020 - December 2020, dosage 200μg/kg days 1, 2, 16, 17, 0.2mg/kg/day for 2 days every 15 days.

The Interaction of Vitamin D and Corticosteroids: A Mortality Analysis of 26,508 Veterans Who Tested Positive for SARS-CoV-2

Efird et al., International Journal of Environmental Research and Public Health, doi:10.3390/ijerph19010447 (Peer Reviewed)

Retrospective 26,508 COVID+ veterans in USA, showing lower mortality with vitamin D use after testing positive (defined as being administered ≥7 days or half of the survival time within 2 weeks after testing), with statistical significance for hospitalized patients.

risk of death, 48.9% lower, RR 0.51, p = 0.10, treatment 11 of 544 (2.0%), control 413 of 15,794 (2.6%), NNT 169, adjusted, non-hospitalized patients, vitamin D + no corticosteroids vs. no vitamin D + no corticosteroids.

risk of death, 54.5% lower, RR 0.45, p = 0.02, treatment 11 of 192 (5.7%), control 553 of 4,340 (12.7%), NNT 14, adjusted, hospitalized patients, vitamin D + no corticosteroids vs. no vitamin D + no corticosteroids.

Efird et al., 12/31/2021, retrospective, USA, North America, peer-reviewed, 10 authors, study period 1 March, 2020 - 10 September, 2020, dosage varies.

Ivermectin administration is associated with lower gastrointestinal complications and greater ventilator-free days in ventilated patients with COVID-19: A propensity score analysis

Shimizu et al., Journal of Infection and Chemotherapy, doi:10.1016/j.jiac.2021.12.024 (Peer Reviewed)

Retrospective 88 ventilated COVID-19 patients in Japan, 39 treated with ivermectin within 3 days of admission, showing significantly reduced incidence of GI complications and mortality, and increased ventilator-free days with treatment.

risk of death, 99.9% lower, RR 0.001, p < 0.001, treatment 0 of 39 (0.0%), control 8 of 49 (16.3%), NNT 6.1, adjusted, Cox proportional hazard regression.

ventilator free days, 47.9% lower, RR 0.52, p = 0.03, treatment 39, control 49, adjusted, proportional odds logistic regression, RR approximated with OR.

ventilation time, 38.5% lower, relative time 0.62, p < 0.001, treatment 39, control 49.

ICU free days, 42.8% lower, RR 0.57, p = 0.06, treatment 39, control 49, adjusted, proportional odds logistic regression, RR approximated with OR.

ICU time, 37.5% lower, relative time 0.62, p < 0.001, treatment 39, control 49.

GI complications while ventilated, 77.9% lower, RR 0.22, p = 0.03, treatment 39, control 49, adjusted, Cox proportional hazard regression.

Shimizu et al., 12/31/2021, retrospective, Japan, Asia, peer-reviewed, 11 authors, study period December 2020 - May 2021, dosage 200μg/kg days 1, 14.

Inhaled remdesivir reduces viral burden in a nonhuman primate model of SARS-CoV-2 infection

Vermillion et al., Science Translational Medicine, doi:10.1126/scitranslmed.abl8282 (Peer Reviewed)

African green monkey study of inhaled versus IV remdesivir, showing similar efficacy with inhalation. Comparable concentrations of the active triphosphate in the lower respiratory tract were found with ~20x lower dose using inhalation, and there was lower systemic exposure to remdesivir and metabolites.

Vermillion et al., 12/30/2021, peer-reviewed, 26 authors.

SIT1 transporter as a potential novel target in treatment of COVID-19

Semiz, S., Biomolecular Concepts, doi:10.1515/bmc-2021-0017 (Review) (Peer Reviewed)

Review of the potential connections between SLC6A20/SIT1, ACE2, Type 2 Diabetes, and COVID-19 severity. This provides another potential mechanism of action for ivermectin as a partial agonist of glycine-gated chloride channels, interfering with cytokine storm by inducing activation of glycine receptors. Author recommends investigating targeting of the SIT1 transporter and glycine levels in the treatment of COVID-19, particularly for severe cases associated with hyperglycemia, inflammation, and T2D.

Semiz et al., 12/30/2021, peer-reviewed, 1 author.

Pattern of medication utilization in hospitalized patients with COVID-19 in three District Headquarters Hospitals in the Punjab province of Pakistan

Mustafa et al., Exploratory Research in Clinical and Social Pharmacy, doi:10.1016/j.rcsop.2021.100101 (Peer Reviewed)

Retrospective 444 hospitalized patients in Pakistan, showing lower mortality with aspirin treatment in unadjusted results, not reaching statistical significance.

risk of death, 44.1% lower, RR 0.56, p = 0.28, treatment 4 of 66 (6.1%), control 41 of 378 (10.8%), NNT 21.

Excluded in after exclusion results of meta analysis: unadjusted results with no group details.

Mustafa et al., 12/29/2021, retrospective, Pakistan, South Asia, peer-reviewed, 7 authors.

Characteristics of the COVID-19 patients treated at Gulu Regional Referral Hospital, Northern Uganda: A cross-sectional study

Baguma et al., Research Square, doi:10.21203/rs.3.rs-1193578/v1 (Preprint)

Retrospective COVID+ hospitalized patients in Uganda, showing no statistically significant difference in mortality with ivermectin, however there was only 7 patients receiving ivermectin.

risk of death, 96.8% lower, RR 0.03, p = 0.31, treatment 7, control 474, OR converted to RR, multivariable, control prevalance approximated with overall prevalence.

Baguma et al., 12/28/2021, retrospective, Uganda, Africa, preprint, 16 authors, study period March 2020 - October 2021, dosage not specified.

Quercetin and Luteolin Are Single-digit Micromolar Inhibitors of the SARS-CoV-2 RNA-dependent RNA Polymerase

Munafò et al., Research Square, doi:10.21203/rs.3.rs-1149846/v1 (Preprint) (In Vitro)

In Vitro and In Silico study showing quercetin and luteolin inhibiting SARS-CoV-2 RNA-dependent RNA polymerase (RdRp).

Munafò et al., 12/28/2021, preprint, 6 authors.

In Vitro studies are an important part of preclinical research, however results may be very different in vivo.

Kintor Pharma Provides Update on One of its Three Multi-Regional Phase 3 Trials of Proxalutamide for COVID-19

Kintor, News Releease (News)

News release reporting on interim analysis of NCT04870606, showing that statistical criteria were not met, there was a very low event rate, and that Kintor plans to amend the protocol and continue to enroll higher risk patients.

Kintor et al., 12/27/2021, preprint, 1 author.

Antiandrogens	(meta)	Melatonin	(meta)
Aspirin	(meta)	Metformin	(meta)
Bamlaniv../e..	(meta)	Molnupiravir	(meta)
Bromhexine	(meta)	N-acetylcys..	(meta)
Budesonide	(meta)	Nigella Sativa	(meta)
Cannabidiol	(meta)	Nitazoxanide	(meta)
Casirivimab/i..	(meta)	Paxlovid	(meta)
Colchicine	(meta)	Povidone-Iod..	(meta)
Conv. Plasma	(meta)	Probiotics	(meta)
Curcumin	(meta)	Proxalutamide	(meta)
Ensovibep	(meta)	Quercetin	(meta)
Favipiravir	(meta)	Remdesivir	(meta)
Fluvoxamine	(meta)	Sotrovimab	(meta)
Hydroxychlor..	(meta)	Vitamin A	(meta)
Iota-carragee..	(meta)	Vitamin C	(meta)
Ivermectin	(meta)	Vitamin D	(meta)
Lactoferrin	(meta)	Zinc	(meta)

Other Treatments		Global Adoption


Random effects meta-analysis of all studies combined (pooled effects, all stages). Treatments with ≤3 studies with distinct authors or with <50 control events are shown in grey. Pooled results across all stages and outcomes depend on the distribution of stages and outcomes tested - for example late stage treatment may be less effective and if the majority of studies are late stage this may obscure the efficacy of early treatment. Please see the specific stage and outcome analyses. Protocols typically combine multiple treatments which may be complementary and synergistic, and the SOC in studies often includes other treatments.


Random effects meta-analysis of early treatment studies (pooled effects). Treatments with ≤3 studies with distinct authors or with <50 control events are shown in grey. Pooled results across all outcomes are affected by the distribution of outcomes tested, please see detail pages for specific outcome analysis. Protocols typically combine multiple treatments which may be complementary and synergistic, and the SOC in studies often includes other treatments.


Random effects meta-analysis of all mortality results (all stages). Treatments with ≤3 studies with distinct authors or with <25 control events are shown in grey. Pooled results across all stages depend on the distribution of stages tested - for example late stage treatment may be less effective and if the majority of studies are late stage this may obscure the efficacy of early treatment. Please see the specific stage analyses. Protocols typically combine multiple treatments which may be complementary and synergistic, and the SOC in studies often includes other treatments.


Random effects meta-analysis of early treatment mortality results. Treatments with ≤3 studies with distinct authors or with <25 control events are shown in grey. Protocols typically combine multiple treatments which may be complementary and synergistic, and the SOC in studies often includes other treatments.