COVID-19 treatment: real-time analysis of 6,661 studies
c19early.org
COVID-19 involves the interplay of 500+ viral and host proteins and factors, providing many therapeutic targets.
c19early analyzes 6,600+ studies for 225 treatments—over 17 million hours of research.
Only three high-profit early treatments are approved in the US.
In reality, many treatments reduce risk,
with 25 low-cost treatments approved across 163 countries.
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Naso/
oropharyngeal treatment Effective Treatment directly to the primary source of initial infection. -
Healthy lifestyles Protective Exercise, sunlight, a healthy diet, and good sleep all reduce risk.
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Immune support Effective Vitamins A, C, D, and zinc show reduced risk, as with other viruses.
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Thermotherapy Effective Methods for increasing internal body temperature, enhancing immune system function.
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Systemic agents Effective Many systemic agents reduce risk, and may be required when infection progresses.
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High-profit systemic agents Conditional Effective, but with greater access and cost barriers.
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Monoclonal antibodies Limited Utility Effective but rarely used—high cost, variant dependence, IV/SC admin.
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Acetaminophen Harmful Increased risk of severe outcomes and mortality.
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Remdesivir Harmful Increased mortality with longer followup. Increased kidney and liver injury, cardiac disorders.
Timeline for when studies showed efficacy - details and limitations.
0.5% of treatments show efficacy.
Treatment cost times median NNT - details and limitations.
0.5% of treatments show efficacy.
All clinical results for selected treatments. 0.5% of treatments show efficacy.
Top journals that accept positive studies for low cost treatments:
Nutrients,
Scientific Reports,
PLOS ONE,
International Journal of Infectious Diseases,
Frontiers in Medicine,
Cureus,
more...
| 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. 0.5% of proposed treatments show efficacy in clinical studies. | |||||
| 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. 0.5% of proposed treatments show efficacy in clinical studies. | |||||
| 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. 0.5% of proposed treatments show efficacy in clinical studies. | |||||
| 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. 0.5% of proposed treatments show efficacy in clinical studies. | |||||
| 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. 0.5% of proposed treatments show efficacy in clinical studies. | |||||
| 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. 0.5% of proposed treatments show efficacy in clinical studies. | |||||
| 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. 0.5% of proposed treatments show efficacy in clinical studies. | |||||
| 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. 0.5% 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) | 2.5% (54) |
| Dr. Jake Scott (**) | USA | 1,000 | 10.0% (100) | |
| Average | 38.6% | 6.2% | ||
| EARLY TREATMENT PROTOCOLS - 40 physicians/teams | ||||
| Physician / Team | Location | Patients | HospitalizationHosp. | MortalityDeath |
| Dr. Roberto Alfonso Accinelli 0/360 deaths for treatment within 3 days |
Peru | 1,265 | 0.6% (7) | |
| Dr. Mohammed Tarek Alam patients up to 84 years old |
Bangladesh | 100 | 0.0% (0) | |
| Dr. Oluwagbenga Alonge | Nigeria | 310 | 0.0% (0) | |
| Dr. Raja Bhattacharya up to 88yo, 81% comorbidities |
India | 148 | 1.4% (2) | |
| Dr. Flavio Cadegiani | Brazil | 3,450 | 0.1% (4) | 0.0% (0) |
| Dr. Alessandro Capucci | Italy | 350 | 4.6% (16) | |
| Dr. Shankara Chetty | South Africa | 8,000 | 0.0% (0) | |
| Dr. Deborah Chisholm | USA | 100 | 0.0% (0) | |
| Dr. Ryan Cole | USA | 400 | 0.0% (0) | 0.0% (0) |
| Dr. Marco Cosentino earlier treatment results were better |
Italy | 392 | 6.4% (25) | 0.3% (1) |
| Dr. Jeff Davis | USA | 6,000 | 0.0% (0) | |
| Dr. Dhanajay | India | 500 | 0.0% (0) | |
| Dr. Bryan Tyson & Dr. George Fareed | USA | 20,000 | 0.0% (6) | 0.0% (4) |
| Dr. Raphael Furtado | Brazil | 170 | 0.6% (1) | 0.0% (0) |
| Rabbi Yehoshua Gerzi | Israel | 860 | 0.1% (1) | 0.0% (0) |
| Dr. Heather Gessling | USA | 1,500 | 0.1% (1) | |
| Dr. Ellen Guimarães | Brazil | 500 | 1.6% (8) | 0.4% (2) |
| Dr. Syed Haider | USA | 4,000 | 0.1% (5) | 0.0% (0) |
| Dr. Mark Hancock | USA | 24 | 0.0% (0) | |
| Dr. Sabine Hazan | USA | 1,000 | 0.0% (0) | |
| Dr. Mollie James | USA | 3,500 | 1.1% (40) | 0.0% (1) |
| Dr. Roberta Lacerda | Brazil | 550 | 1.5% (8) | 0.4% (2) |
| Dr. Katarina Lindley | USA | 100 | 5.0% (5) | 0.0% (0) |
| Dr. Ben Marble | USA | 150,000 | 0.0% (4) | |
| Dr. Edimilson Migowski | Brazil | 2,000 | 0.3% (7) | 0.1% (2) |
| Dr. Abdulrahman Mohana | Saudi Arabia | 2,733 | 0.0% (0) | |
| Dr. Carlos Nigro | Brazil | 5,000 | 0.9% (45) | 0.5% (23) |
| Dr. Benoit Ochs | Luxembourg | 800 | 0.0% (0) | |
| Dr. Ortore | Italy | 240 | 1.2% (3) | 0.0% (0) |
| Dr. Valerio Pascua one patient already on oxygen died |
Honduras | 415 | 6.3% (26) | 0.2% (1) |
| Dr. Sebastian Pop | Romania | 300 | 0.0% (0) | |
| Dr. Brian Proctor | USA | 869 | 2.3% (20) | 0.2% (2) |
| Dr. Anastacio Queiroz | Brazil | 700 | 0.0% (0) | |
| Dr. Didier Raoult | France | 8,315 | 2.6% (214) | 0.1% (5) |
| Dr. Karin Ried up to 99yo, 73% comorbidities |
Turkey | 237 | 0.4% (1) | |
| Dr. Roman Rozencwaig patients up to 86 years old |
Canada | 80 | 0.0% (0) | |
| Dr. Vipul Shah | India | 8,000 | 0.1% (5) | |
| Dr. Silvestre Sobrinho | Brazil | 116 | 8.6% (10) | 0.0% (0) |
| Dr. Unknown | Brazil | 957 | 1.7% (16) | 0.2% (2) |
| Dr. Vladimir Zelenko | USA | 2,200 | 0.5% (12) | 0.1% (2) |
| Average | 2.2% | 0.1% | ||
Physicians using early combined treatment protocols had much lower
hospitalization and mortality rates compared with those following guidelines focusing on
late treatment.
Results are subject to selection and ascertainment bias and accurate analysis requires
details of the patient populations and followup, however the results are consistent across
many teams, and consistent with the extensive controlled clinical evidence showing a
significant reduction in risk with many early treatments, and complementary/synergistic
benefits with combined treatments.
(*) Dr. Uip reportedly prescribed early treatment for himself, but not for
patients1.
(**) Dr. Scott reports treating hundreds of patients and losing over a hundred,
but has not provided specific numbers2.
Dr. Scott reports following (and helping create) US guidelines.
| Uddin | Mouse study showing that CXCR3 signaling is protective against SARS-CoV-2 infection, with CXCR3 blockade increasing disease severity in C57BL/6 mice.. |
| Fang | Phase I RCT of 26 healthy adults (20 STSA-1002, 6 placebo) showing STSA-1002, a fully human anti-C5a monoclonal antibody, was safe and well.. |
| Ma | In silico study using network pharmacology, molecular docking, and molecular dynamics simulation to investigate the mechanisms of Xiangxue Decoction.. |
| Porta | Review of SARS-CoV-2 non-structural proteins as targets for direct-acting small-molecule antivirals. |
| Soto Albrecht | In vitro study showing that inhibition of mitochondrial oxidative phosphorylation (OXPHOS) enhances SARS-CoV-2 replication, while restoration of.. |
| Jia | Review of strategies for developing and engineering broadly neutralizing antibodies against SARS-CoV-2 to counteract rapid viral mutation and immune.. |
| Schmidt | Cross-sectional study of 750 adults assessed on average 21.9 months after PCR-verified SARS-CoV-2 infection, showing that the combination of low.. |
| Oliveira | Syrian golden hamster study showing benefits of vitamin B12 treatment for mitigating long COVID neurological sequelae. Authors propose that B12's.. |
| Kim | Retrospective 581,379 older adults in South Korea showing a dose-dependent association between cumulative acetaminophen use and increased risk of.. |
| di Filippo | 114 patients prophylaxis: 50% fewer symptomatic cases (p=0.12) |
| Rahardjo | RCT 30 hospitalized COVID-19 patients in Indonesia showing significantly shorter length of hospital stay with convalescent plasma, however there are.. |
| Morikawa | Retrospective 283 hospitalized COVID-19 patients in Japan showing potential benefit with butyrate-producing Clostridium butyricum (CB)-containing.. |
| Bačić | Analysis of 74 participants (34 receiving a 12-week multi-strain probiotic containing Saccharomyces boulardii, Lacticaseibacillus rhamnosus GG, and.. |
| Soleimani | In vitro study showing benefit with postbiotics derived from Lacticaseibacillus rhamnosus GG and Bifidobacterium animalis subsp. lactis BB-12.. |
| Liu | Retrospective 300 elderly hospitalized COVID-19 patients in China, showing no mortality benefit with antivirals (paxlovid and molnupiravir) in.. |
| Kueper | 669 patients early treatment: 87% worse recovery (p=0.02) and 148% worse viral clearance (p=0.01) |
| Liu | Retrospective 300 elderly hospitalized COVID-19 patients in China, showing no mortality benefit with antivirals (paxlovid and molnupiravir) in.. |
| Kawai | 1,003 patient prophylaxis RCT: 67% lower hospitalization (p=0.5), 67% lower progression (p=0.5), and 1% fewer cases (p=1) |
| Torrejón-Guirado | 1,051 patients prophylaxis: 154% more cases (p=0.001) |
| Jara Rubio | 150 patient late treatment RCT: 23% higher mortality (p=0.56), 200% higher progression (p=0.14), no change in ICU admission (p=1), and 18% longer hospitalization (p=0.41) |
| Setz | In vitro study showing synergistic antiviral activity of black elderberry fruit extract and iota-carrageenan against SARS-CoV-2 Omicron, influenza A.. |
| Setz | In vitro study showing synergistic antiviral activity of black elderberry fruit extract and iota-carrageenan against SARS-CoV-2 Omicron, influenza A.. |
| Widyarman | RCT 40 COVID-19 outpatients showing lower salivary SARS-CoV-2 viral load with cetylpyridinium chloride (CPC), povidone-iodine (PVP-I), and sodium.. |
| Widyarman | RCT 40 COVID-19 outpatients showing lower salivary SARS-CoV-2 viral load with cetylpyridinium chloride (CPC), povidone-iodine (PVP-I), and sodium.. |
Recent studies (see the individual treatment pages for all studies):
Jul 1 |
et al., Scientific Reports, doi:10.1038/s41598-026-45496-z | Mechanisms of Xiangxue decoction in treating COVID-19 via HPLC‒Q-TOF‒MS/MS, network pharmacology, molecular docking and molecular dynamics simulation |
| In silico study using network pharmacology, molecular docking, and molecular dynamics simulation to investigate the mechanisms of Xiangxue Decoction (XXD) for COVID-19. | ||
Jul 1 |
et al., Research Square, doi:10.21203/rs.3.rs-9912983/v1 | Early vitamin B12 treatment mitigates hippocampal neuroinflammation and neurodegeneration in a hamster model of long COVID |
| Syrian golden hamster study showing benefits of vitamin B12 treatment for mitigating long COVID neurological sequelae. Authors propose that B12's neuroprotective mechanism involves DNA methylation-dependent downregulation of CCL11 transcr.. | ||
Jun 29 |
et al., NCT04483973 | A Phase 2, Randomized, Double-Blind, Placebo-Controlled, Dose Escalation Study to Evaluate the Safety and Efficacy of SPI-1005 in Severe COVID-19 Patients |
| 125% higher mortality (p=0.62) and 13% worse recovery (p=0.78). RCT 25 severe COVID-19 patients showing no significant differences with SPI-1005 (ebselen). | ||
Jun 27 |
et al., Redox Biology, doi:10.1016/j.redox.2026.104273 | Low serum selenium combined with SELENOP-autoantibodies are associated with persistent fatigue after SARS-CoV-2 infection |
| Cross-sectional study of 750 adults assessed on average 21.9 months after PCR-verified SARS-CoV-2 infection, showing that the combination of low serum selenium (<70 μg/L) or low SELENOP (<4.1 mg/L) with SELENOP autoantibodies (SELENOP-aAb.. | ||
Jun 25 |
et al., NCT04484025 | A Phase 2, Randomized, Double-Blind, Placebo-Controlled, Dose Escalation Study to Evaluate the Safety and Efficacy of SPI-1005 in Moderate COVID-19 Patients |
| 141% higher mortality (p=1) and 21% worse recovery (p=0.67). RCT 31 moderate COVID-19 patients showing no significant differences with SPI-1005 (ebselen). | ||
Jun 18 |
et al., NCT05648110 | Study Understanding Pre-Exposure pRophylaxis of NOvel Anitbodies (SUPERNOVA) |
| 139% higher mortality (p=1). RCT 57 patients showing no significant differences with AZD5156 (sipavibart + cilgavimab). | ||
Jun 18 |
et al., Frontiers in Pharmacology, doi:10.3389/fphar.2026.1838620 | Safety, tolerability, pharmacokinetics, pharmacodynamics, and immunogenicity of STSA-1002, recombinant anti-human C5a fully human monoclonal antibody, in a randomized, first-in-human phase I study in healthy adults |
| Phase I RCT of 26 healthy adults (20 STSA-1002, 6 placebo) showing STSA-1002, a fully human anti-C5a monoclonal antibody, was safe and well-tolerated at multiple intravenous doses (5, 10, and 20 mg/kg weekly for 4 weeks). | ||
Jun 16 |
et al., European Journal of Clinical Pharmacology, doi:10.1007/s00228-026-04108-5 | Acetaminophen exposure in an aging population and neurodegenerative outcomes |
| Retrospective 581,379 older adults in South Korea showing a dose-dependent association between cumulative acetaminophen use and increased risk of Alzheimer's disease and Parkinson's disease. Authors hypothesize that acetaminophen's metabo.. | ||
Jun 11 |
et al., Frontiers in Immunology, doi:10.3389/fimmu.2026.1823264 | CXCR3 ameliorates neutrophil-dependent disease severity in SARS-CoV-2 infection by regulating CD4+ T cell recruitment |
| Mouse study showing that CXCR3 signaling is protective against SARS-CoV-2 infection, with CXCR3 blockade increasing disease severity in C57BL/6 mice infected with mouse-adapted SARS-CoV-2 (MA-10). | ||
Jun 10 |
et al., Endocrine, doi:10.1007/s12020-026-04677-6 | Impact of chronic cholecalciferol supplementation and vitamin D status on risk of post-vaccination SARS-CoV-2 breakthrough infection |
| 50% fewer symptomatic cases (p=0.12). Retrospective 114 vaccinated outpatients showing lower risk of symptomatic COVID-19 cases with adequate vitamin D status and cholecalciferol supplementation (similar point estimate for the full and matched population, but without statisti.. | ||
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.
References