COVID-19 early treatment: real-time analysis of 5,915 studies

Negru	Pharmacovigilance analysis of 64,776 adverse event reports from EudraVigilance comparing safety profiles of COVID-19 antivirals, showing remdesivir..
Chen	90,552 patients vitamin D sufficiency: 61% lower mortality (p=0.007)

COVID-19 involves the interplay of over 100 viral and host proteins and factors, providing many therapeutic targets. c19early analyzes over 5,900 studies for 172 treatments—over 17 million hours of research. US authorities believe only three high-profit early treatments reduce risk (remdesivir, paxlovid, molnupiravir). In reality, many treatments reduce risk, and 25 low-cost treatments have been approved across 163 countries. 0.6% of 9,000+ proposed treatments show reduced risk.

Naso/oropharyngeal treatment

Direct treatment to the primary source of initial infection reduces progression and transmission.

Healthy lifestyles

Exercise, sunlight, a healthy diet, and good sleep all reduce risk.

Immune support

Vitamins A, C, D, and zinc show reduced risk, as with other viruses.

Thermotherapy

Methods for increasing internal body temperature, comparable to natural fever, enhancing immune system function.

Systemic agents

Many systemic agents reduce risk, and may be required when infection progresses beyond the upper respiratory tract.

High-profit systemic agents

High-profit systemic agents are also effective, but have greater access and cost barriers.

Monoclonal antibodies

Highly effective for matching variants but rarely used, with high cost, variant dependence, and IV/SC administration.

Acetaminophen

Acetaminophen increases the risk of severe outcomes and mortality.

Remdesivir

Studies show increased mortality with longer followup.

c19early.org

We do not provide medical advice. No treatment is 100% effective, and all may have side effects. Protocols combine multiple treatments. Consult a qualified physician for personalized risk/benefit analysis.

Timeline for when studies showed efficacy - details and limitations. 0.6% of treatments show efficacy.

Top journals that accept positive studies for low cost treatments: Nutrients, PLOS ONE, Scientific Reports, International Journal of Infectious Diseases, Frontiers in Medicine, Cureus, more...

June 2025
c19early.org

Cost per life saved from NNT in
studies to date

Melatonin

10
48%

Alkalinization

9
46%

Vitamin D

73
38%

$10

Zinc

22
30%

$16

Vitamin C

46
20%

$18

HCQ

254
27%

$26

Ivermectin

53
47%

$26

Colchicine

43
28%

$31

Aspirin

68
8%

$45

Vitamin A

5
30%

$45

Curcumin

8
63%

$59

Famotidine

21
18%

$94

Metformin

71
37%

$121

Quercetin

5
61%

$127

Probiotics

10
59%

$172

Antiandrogens

32
37%

$179

Nigella Sativa

5
57%

$187

Fluvoxamine

10
44%

$411

Budesonide

12
26%

$574

Azvudine

25
29%

$1,259

Favipiravir

42
6%

$1,935

Tixagev../c..

10
40%

$74,506

Regdanvimab

7
63%

$139,860

Sotrovimab

14
46%

$299,464

Bamlaniv../e..

13
54%

$301,549

Casirivimab/..

11
20%

$452,469

Bebtelovimab

4
60%

$737,601

Remdesivir

67
1%

$1,558,440

Paxlovid

41
22%

$1,901,782

Molnupiravir

27
13%

$2,400,867

Conv. Plasma

55
-2%

N/A

Acetaminophen

14
-24%

N/A

PPIs

20
-40%

N/A

Brensocatib

1
-41%

N/A

Treatment cost times median NNT - details and limitations. 0.6% of treatments show efficacy.

All clinical results for selected treatments. 0.6% of treatments show efficacy.


Random effects meta-analysis of all studies (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. 0.6% of proposed treatments show efficacy in clinical studies.

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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. 0.6% of proposed treatments show efficacy in clinical studies.

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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. 0.6% of proposed treatments show efficacy in clinical studies.

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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. 0.6% of proposed treatments show efficacy in clinical studies.

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Random effects meta-analysis of prophylaxis 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. 0.6% of proposed treatments show efficacy in clinical studies.

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Random effects meta-analysis of prophylaxis 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. 0.6% of proposed treatments show efficacy in clinical studies.

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Random effects meta-analysis of long covid results. 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. 0.6% of proposed treatments show efficacy in clinical studies.

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Random effects meta-analysis of transmission results. 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. 0.6% of proposed treatments show efficacy in clinical studies.

LATE TREATMENT
Physician / Team	Location	Patients	HospitalizationHosp.		MortalityDeath
Dr. David Uip ^(*)	Brazil	2,200	38.6% (850)	Ref.	2.5% (54)	Ref.
EARLY TREATMENT - 40 physicians/teams
Physician / Team	Location	Patients	HospitalizationHosp.	ImprovementImp.	MortalityDeath	ImprovementImp.
Dr. Roberto Alfonso Accinelli 0/360 deaths for treatment within 3 days	Peru	1,265			0.6% (7)	77.5%
Dr. Mohammed Tarek Alam patients up to 84 years old	Bangladesh	100			0.0% (0)	100.0%
Dr. Oluwagbenga Alonge	Nigeria	310			0.0% (0)	100.0%
Dr. Raja Bhattacharya up to 88yo, 81% comorbidities	India	148			1.4% (2)	44.9%
Dr. Flavio Cadegiani	Brazil	3,450	0.1% (4)	99.7%	0.0% (0)	100.0%
Dr. Alessandro Capucci	Italy	350	4.6% (16)	88.2%
Dr. Shankara Chetty	South Africa	8,000			0.0% (0)	100.0%
Dr. Deborah Chisholm	USA	100			0.0% (0)	100.0%
Dr. Ryan Cole	USA	400	0.0% (0)	100.0%	0.0% (0)	100.0%
Dr. Marco Cosentino vs. 3-3.8% mortality during period; earlier treatment better	Italy	392	6.4% (25)	83.5%	0.3% (1)	89.6%
Dr. Jeff Davis	USA	6,000			0.0% (0)	100.0%
Dr. Dhanajay	India	500			0.0% (0)	100.0%
Dr. Bryan Tyson & Dr. George Fareed	USA	20,000	0.0% (6)	99.9%	0.0% (4)	99.2%
Dr. Raphael Furtado	Brazil	170	0.6% (1)	98.5%	0.0% (0)	100.0%
Rabbi Yehoshua Gerzi	Israel	860	0.1% (1)	99.7%	0.0% (0)	100.0%
Dr. Heather Gessling	USA	1,500			0.1% (1)	97.3%
Dr. Ellen Guimarães	Brazil	500	1.6% (8)	95.9%	0.4% (2)	83.7%
Dr. Syed Haider	USA	4,000	0.1% (5)	99.7%	0.0% (0)	100.0%
Dr. Mark Hancock	USA	24			0.0% (0)	100.0%
Dr. Sabine Hazan	USA	1,000			0.0% (0)	100.0%
Dr. Mollie James	USA	3,500	1.1% (40)	97.0%	0.0% (1)	98.8%
Dr. Roberta Lacerda	Brazil	550	1.5% (8)	96.2%	0.4% (2)	85.2%
Dr. Katarina Lindley	USA	100	5.0% (5)	87.1%	0.0% (0)	100.0%
Dr. Ben Marble	USA	150,000			0.0% (4)	99.9%
Dr. Edimilson Migowski	Brazil	2,000	0.3% (7)	99.1%	0.1% (2)	95.9%
Dr. Abdulrahman Mohana	Saudi Arabia	2,733			0.0% (0)	100.0%
Dr. Carlos Nigro	Brazil	5,000	0.9% (45)	97.7%	0.5% (23)	81.3%
Dr. Benoit Ochs	Luxembourg	800			0.0% (0)	100.0%
Dr. Ortore	Italy	240	1.2% (3)	96.8%	0.0% (0)	100.0%
Dr. Valerio Pascua one death for a patient presenting on the 5th day in need of supplemental oxygen	Honduras	415	6.3% (26)	83.8%	0.2% (1)	90.2%
Dr. Sebastian Pop	Romania	300			0.0% (0)	100.0%
Dr. Brian Proctor	USA	869	2.3% (20)	94.0%	0.2% (2)	90.6%
Dr. Anastacio Queiroz	Brazil	700			0.0% (0)	100.0%
Dr. Didier Raoult	France	8,315	2.6% (214)	93.3%	0.1% (5)	97.6%
Dr. Karin Ried up to 99yo, 73% comorbidities, av. age 63	Turkey	237			0.4% (1)	82.8%
Dr. Roman Rozencwaig patients up to 86 years old	Canada	80			0.0% (0)	100.0%
Dr. Vipul Shah	India	8,000			0.1% (5)	97.5%
Dr. Silvestre Sobrinho	Brazil	116	8.6% (10)	77.7%	0.0% (0)	100.0%
Dr. Unknown	Brazil	957	1.7% (16)	95.7%	0.2% (2)	91.5%
Dr. Vladimir Zelenko	USA	2,200	0.5% (12)	98.6%	0.1% (2)	96.3%
Mean improvement with early treatment protocols		238,381	HospitalizationHosp.	94.4%	MortalityDeath	94.9%

Physician results with early treatment protocols compared to no early treatment. These results are subject to selection and ascertainment bias and more accurate analysis requires details of the patient populations and followup, however results are consistently better across many teams, and consistent with the extensive controlled trial evidence that shows a significant reduction in risk with many early treatments, and improved results with the use of multiple treatments in combination. ^(*) Dr. Uip reportedly prescribed early treatment for himself, but not for patients.

Paxlovid

Negru

Pharmacovigilance analysis of 64,776 adverse event reports from EudraVigilance comparing safety profiles of COVID-19 antivirals, showing remdesivir..

Vitamin D

Chen	90,552 patients sufficiency: 61% lower mortality (p=0.007)
Blázquez-Cabrera	230 patients late treatment: 52% lower mortality (p=0.05)

Remdesivir

Negru

Pharmacovigilance analysis of 64,776 adverse event reports from EudraVigilance comparing safety profiles of COVID-19 antivirals, showing remdesivir..

Favipiravir

Rowland	RCT 24 hospitalized COVID-19 patients (16 treatment, 8 standard of care) evaluating safety and pharmacokinetics of intravenous favipiravir at..
Tate	302 patient early treatment RCT: 34% lower hospitalization (p=0.68), 21% improved 7-point scale results (p=0.61), 3% improved recovery (p=0.82), and 12% improved viral clearance (p=0.68)

Curcumin

Alcântara

131 patients early treatment: 37% improved recovery (p<0.0001)

Recent studies (see the individual treatment pages for all studies):


Jun 27	Madar et al., COVID, doi:10.3390/covid5070097	Vitamin D Status and SARS-CoV-2 Positivity in Lebanon Among Adults: A Cross-Sectional Study in South Lebanon
	34% fewer cases (p=0.15). Cross-sectional study of 384 adults showing no significant association between vitamin D levels and test positivity.
Jun 24	Li et al., Journal of Inflammation Research, doi:10.2147/JIR.S522566	Association Between Vitamin A and D Status and the Risk of COVID-19 in the Elderly Population: A Single-Center Experience
	99% fewer cases (p=0.002). Prospective study of 32 elderly COVID-19 patients and 30 healthy controls in China showing significantly lower vitamin A and D levels in COVID-19 patients. In multivariable analysis, vitamin A deficiency was associated with significantly ..
Jun 24	Tate et al., Antimicrobial Agents and Chemotherapy, doi:10.1128/aac.00054-25	Clinical effectiveness, safety, and viral mutagenicity of oral favipiravir for COVID-19: results from a community-based, open-label, randomized Phase III trial
	34% lower hospitalization (p=0.68), 21% improved 7-point scale results (p=0.61), 3% improved recovery (p=0.82), and 12% improved viral clearance (p=0.68). RCT 302 outpatients with mild COVID-19 showing no significant difference in outcomes with favipiravir treatment. The study population was relatively young and had few comorbidities, resulting in a low incidence of severe disease. Favipira..
Jun 18	Trimarco et al., npj Metabolic Health and Disease, doi:10.1038/s44324-025-00072-3	Aspirin reduces the risk of type 2 diabetes associated with COVID-19
	Retrospective 35,525 adults followed from 2018 to 2022, showing that daily low-dose aspirin (100 mg) significantly reduced the risk of new-onset type 2 diabetes (T2D). After propensity score matching, aspirin users had a 52% overall reduc..
Jun 17	Shamshirgardi et al., Journal of Health, Population and Nutrition, doi:10.1186/s41043-025-00958-4	Dietary glycemic index, glycemic load, and risk of COVID-19: a prospective cohort study
	84% fewer cases (p<0.0001). Prospective cohort study of 3,319 participants showing higher risk of COVID-19 infection associated with higher dietary glycemic index (GI) and glycemic load (GL). Authors suggest that diets with high GI/GL may increase COVID-19 susceptib..
Jun 12	Mothae et al., Virology, doi:10.1016/j.virol.2025.110607	SARS-CoV-2 host-pathogen interactome: insights into more players during pathogenesis
	Review of SARS-CoV-2 host-pathogen interactions during viral pathogenesis, focusing on protein-protein interactions that facilitate viral entry, replication, immune evasion, assembly, and release. Authors comprehensively analyze how SARS-..
Jun 10	Seijas-Otero et al., Japanese Dental Science Review, doi:10.1016/j.jdsr.2025.05.001	Antiseptics as effective virucidal agents against SARS-CoV-2: Systematic review and Bayesian network meta-analysis
	Bayesian network meta-analysis of 26 studies evaluating the effectiveness of oral and nasal antiseptics against SARS-CoV-2 viral load, finding that povidone-iodine was the most effective. Hydrogen peroxide and chlorhexidine also showed si..
Jun 10	Blázquez-Cabrera et al., Nutrients, doi:10.3390/nu17121968	ALBACOVIDIOL Study: Effect of Calcifediol Treatment on Mortality in Patients Hospitalized for COVID-19: A Retrospective Analysis
	52% lower mortality (p=0.05). Retrospective 230 hospitalized COVID‑19 patients in Spain, showing lower mortality with calcifediol treatment (p = 0.053).
Jun 9	Rowland et al., medRxiv, doi:10.1101/2025.06.09.25329141	Optimal dose and safety of intravenous favipiravir in hospitalised patients with SARS-CoV-2 infection: a Phase Ib, open-label, dose-escalating, randomised controlled study
	RCT 24 hospitalized COVID-19 patients (16 treatment, 8 standard of care) evaluating safety and pharmacokinetics of intravenous favipiravir at escalating doses. The study found that IV favipiravir was safe and well-tolerated up to 2400mg t..
Jun 5	Polasek et al., Frontiers in Medicine, doi:10.3389/fmed.2025.1565069	Povidone-iodine nasal spray (Nasodine®) for the common cold: a randomized, controlled, double-blind, Phase III clinical trial
	Non-COVID-19 RCT of 260 outpatients with early common-cold symptoms comparing 0.5% povidone-iodine (PVP-I) nasal spray and saline spray four-times daily for five days. PVP-I showed lower Global Severity Score (GSS) and improved quality-of..
Jun 4	Gan et al., NCT04481685	A Double-blind, Randomized, Controlled Trial of ATI-450 in Patients With Moderate-severe COVID-19
	no change in mortality (p=1) and 25% higher progression (p=1). RCT 20 hospitalized patients showing no significant difference in outcomes with ATI-450 (zunsemetinib).
Jun 4	Lumkul et al., PLOS One, doi:10.1371/journal.pone.0324903	In-hospital mortality outcomes of favipiravir in patients with moderate to severe COVID-19 infection: An emulated target trial using real-world data from the largest field hospital in Thailand
	4% improved survival (p=0.004). Retrospective 3,193 moderate to severe COVID-19 patients in Thailand showing modest survival benefits with favipiravir. This emulated target trial found that favipiravir alone increased restricted mean survival time by 1.32 days (p=0.042)..
Jun 4	Alcântara et al., Authorea Inc., doi:10.22541/au.174904567.74543434/v1	Earlier clinical improvement in mild-moderate acute COVID patients treated with pharmacological-grade Curcumin
	37% improved recovery (p<0.0001). Prospective study of 131 mild-moderate COVID-19 patients showing significant reduction in time to symptom relief and complete recovery with pharmaceutical-grade curcumin.
Jun 4	Xiong et al., Frontiers in Pharmacology, doi:10.3389/fphar.2025.1558054	Real-world data of Azvudine-induced hepatotoxicity among hospitalized COVID-19 patients in China: a retrospective case-control study
	Retrospective case-control study of 669 hospitalized COVID-19 patients in China showing significant hepatotoxicity associated with azvudine treatment.
Jun 3	Deschenes et al., The Journal of Infectious Diseases, doi:10.1093/infdis/jiaf294	Functional and structural characterization of treatment-emergent nirmatrelvir resistance mutations at low frequencies in the main protease (Mpro) reveals a unique evolutionary route for SARS-CoV-2 to gain resistance
	In Vitro and In Silico study showing that novel SARS-CoV-2 main protease (M^pro) mutations confer resistance to paxlovid. Authors identified new M^pro clinical variants, including D48D/L58F/P132H and D48D/L67V/K90R/P132H, in patients who re..
May 31	Wagner et al., Clinical Nutrition Open Science, doi:10.1016/j.nutos.2025.05.007	Exploring the association between vitamin D status and Corona Virus-19 infection in a cohort of adults aged 50 years and older
	74% fewer cases (p=0.01). Prospective study of 131 adults aged 50+ years showing lower vitamin D status was significantly associated with higher risk of COVID-19 infection and hospitalization. Adjusted results based on deficiency are only provided for cases (other..
May 31	Dalton et al., medRxiv, doi:10.1101/2025.05.30.25327809	Risk of Post-COVID Conditions among adolescents and adults who received nirmatrelvir-ritonavir for acute COVID-19: a retrospective cohort study
	Retrospective 291,433 paxlovid recipients matched 1:2 to 582,866 untreated COVID-19 outpatients in the USA reporting a modest reduction in long COVID in the primary model for patients 50+. Analysis requiring a positive laboratory test or ..
May 31	Leitch-Casey et al., American Journal of Respiratory and Critical Care Medicine, doi:10.1164/ajrccm.2025.211.Abstracts.A1193	Toxic as FK - A Case of Paxlovid-Induced Tacrolimus (FK506) Toxicity in a Kidney Transplant Recipient with COVID-19
	Case report of a 71-year-old kidney transplant recipient who developed fatal tacrolimus toxicity after being prescribed paxlovid for COVID-19.
May 31	Kulkarni-Munshi et al., Journal of Ayurveda and Integrative Medicine, doi:10.1016/j.jaim.2025.101135	Ashwagandha, Withania somnifera (L.) Dunal, for the prophylaxis against SARS-CoV-2 infection: A multicentric randomized hydroxychloroquine controlled clinical trial in Indian health care workers
	61% fewer cases (p=0.28). RCT 400 healthcare workers in India comparing HCQ and withania somnifera (WS) for COVID-19 prophylaxis, showing 2 cases for HCQ and 5 for WS. Both treatments had comparable safety profiles, with mostly mild gastrointestinal adverse events.
May 30	Sokolenko et al., Viruses, doi:10.3390/v17060792	Antiviral Intervention of COVID-19: Linkage of Disease Severity with Genetic Markers FGB (rs1800790), NOS3 (rs2070744) and TMPRSS2 (rs12329760)
	Genetic case-control study of 257 COVID-19 patients (197 moderate-severe, 60 mild) showing that carriers of the G-allele (especially GG genotype) of FGB gene rs1800790 and T-allele of TMPRSS2 gene rs12329760 had higher risk of developing..
May 29	Rao et al., Journal of Cellular and Molecular Medicine, doi:10.1111/jcmm.70581	Pathological Glucose Levels Enhance Entry Factor Expression and Hepatic SARS‐CoV‐2 Infection
	Analysis of high glucose levels on SARS-CoV-2 infection, showing that hyperglycemia significantly increases expression of viral entry factors (ACE2, TMPRSS2, TMPRSS4, FURIN, NRP1) in liver cells but not in lung and pancreatic cells, which..

We aim to cover the most promising early treatments for COVID-19. We use pre-specified effect extraction criteria that prioritizes more serious outcomes, for details see methods. For specific outcomes and different treatment stages see the individual pages. Not all treatments are covered here, effectiveness has been reported for many other treatments in studies. Of the 5,915 studies, 2,833 present results comparing with a control group, 2,611 are treatment studies, and 222 analyze outcomes based on serum levels. There are 111 animal studies, 219 in silico studies, 413 in vitro studies, 452 reviews, and 247 meta analyses.

Please send us corrections, updates, or comments. c19early involves the extraction of 200,000+ datapoints from thousands of papers. Community updates help ensure high accuracy. Treatments and other interventions are complementary. All practical, effective, and safe means should be used based on risk/benefit analysis. No treatment or intervention is 100% available and effective for all current and future variants. We do not provide medical advice. Before taking any medication, consult a qualified physician who can provide personalized advice and details of risks and benefits based on your medical history and situation. IMA and WCH provide treatment protocols.

Thanks for your feedback! Please search before submitting papers and note that studies are listed under the date they were first available, which may be the date of an earlier preprint.

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