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c19early.org COVID-19 treatment researchSelect treatment..Select..
Metformin Meta
Bromhexine Meta
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Colchicine Meta Nigella Sativa Meta
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Curcumin Meta PPIs Meta
Fluvoxamine Meta Quercetin Meta
Hydroxychlor.. Meta
Ivermectin Meta Thermotherapy Meta
Melatonin Meta

COVID-19 early treatment: real-time analysis of 5,366 studies

 
Hu
926 patients ursodeoxycholic acid prophylaxis: 89% lower severe cases (p=0.02) and 25% fewer symptomatic cases (p<0.0001)
Luetkemeyer
2,085 patient ensitrelvir early treatment RCT: 203% higher hospitalization (p=0.37), 5% faster recovery (p=0.14), and 19% improved viral clearance (p=0.02)
Sun
2,924 patients azvudine late treatment PSM: 27% lower mortality (p=0.02) and 15% higher progression (p=0.16)
$0 $1,000 $2,000+ -25+% 0% 25% 50% Treatment cost (US$) Efficacy vs. cost for COVID-19 treatments Donidalorsen -151% >$2,000 Glenzocimab -60% >$2,000 Olokizumab -50% >$2,000 PPIs -46% BMS mAbs -36% >$2,000 Acetaminophen -28% Lufotrelvir >$2,000 Cannabidiol Trimodulin >$2,000 Plitidepsin >$2,000 Losartan Sargramostim >$2,000 Vitamin B9 Conv. Plasma $5,000 Remdesivir $3,120 Sarilumab >$2,000 Acebilustat >$2,000 Ibuprofen Aspirin Molnupiravir mutagenic/teratogenic Favipiravir Paxlovid Famotidine Vitamin C Amubarvimab/r.. Sotrovimab $2,100 NAC Vilobelimab $6,350 Colchicine Budesonide Probiotics Zinc HCQ Azvudine Antiandro.. Metformin Nitric Oxide Sleep Vitamin A Bebtelovimab H1RAs Vitamin D Sunlight H. Peroxide Exercise Fluvox. Curcumin Tixagevimab/c.. Casirivimab/i.. $2,100 N. Sativa NaHCO₃ Melatonin Ensovibep >$2,000 Quercetin Bamlanivimab/e.. pH+ Diet PVP-I Thermotherapy Ivermectin Regdanvimab $2,100 Lifestyle / free No prescription Prescription required High-cost Lowerrisk Higherrisk c19early.org February 2025 COVID-19 involves the interplay of 50+ host/viral proteins/factors, modulated by many treatments. 0.5% of 8,000+proposed treatments show efficacy with ≥3 studies.Protocols combine treatments, none are 100% effective.c19early analyzes over 5,300 studies for 115 treatments.
$0 $1,000 $2,000+ -20+% 0% 25% 50% Treatment cost (US$) Efficacy vs. cost for COVID-19 treatments Donidalorsen -151% Glenzocimab -60% Olokizumab -50% PPIs -46% BMS mAbs -36% Acetaminophen -28% Lufotrelvir -22% CBD -21% Trimodulin Plitidepsin Losartan Sargramostim Vit. B9 C. Plasma Remdesivir Sarilumab Acebilustat Ibuprofen Aspirin Molnupiravir mutagenic/teratogenic Favipiravir Paxlovid Famotidine Vitamin C Amubarvimab/r.. Sotrovimab NAC Vilobelimab Colchicine Budesonide Probiotics Zinc HCQ Azvudine Antiandro.. Metformin Nitric Oxide Sleep Vitamin A Bebtelovimab H1RAs Vitamin D Sunlight H. Peroxide Exercise Fluvox. Curcumin Tixagevimab/c.. Casirivim.. N. Sativa NaHCO₃ Melatonin Ensovibep Quercetin Bamlan.. pH+ Diet PVP-I Thermotherapy Ivermectin Regdanvimab Lifestyle / free No prescription Prescription required High-cost Lowerrisk Higherrisk c19early.org February 2025 COVID-19 involves the interplay of50+ host/viral proteins/factors.0.5% of 8,000+ treatments showefficacy. Protocols combinetreatments. c19early analyzes5,300+ studies for 115 treatments.
$0 $500 $1,000+ COVID-19 treatment protocols average efficacy and cost Philippines Argentina Pakistan USA Russia Bangladesh South Africa Brazil United Kingdom Iran Vietnam Turkey Italy France Spain Germany Kenya Japan India China Egypt Thailand Ukraine Mexico South Korea Indonesia Uganda Nigeria Ethiopia DR Congo Algeria Angola Peru Bosnia-Herzegovina New Zealand Poland Congo Sri Lanka Morocco Panama Bahrain Ghana Qatar Cameroon Dominican Republic Paraguay Treatment protocols varied widely around the world.Low-cost and non-prescription treatments reduce barriersto treatment—especially early treatment—and providecomplementary and synergistic benefits. More effective More expensive c19early.org February 2025 75% 50% 25% ≤0%
$0 $500 $1,000+ C19 treatment protocols avg. efficacy/cost Philippines Argentina Pakistan USA Russia Bangladesh South Africa Brazil United Kingdom Iran Vietnam Turkey Italy France Spain Germany Kenya Japan India China Egypt Thailand Ukraine Mexico South Korea Indonesia Uganda Nigeria Ethiopia DR Congo Algeria Angola Peru Israel Congo Sri Lanka Morocco Bahrain Ghana Qatar Cameroon Dominican Rep. Treatment protocols varied widely.Low-cost and non-prescription treatmentsreduce barriers to treatment—especiallyearly treatment—and provide complementaryand synergistic benefits. More effective More expensive c19early.org February 2025 75% 50% 25% ≤0%
Azvudine Evusheld Sodium Bicarbonate Paxlovid Regdanvimab Vitamin B12 Sunlight Phthalocyanine Montelukast Alkalinization Fluvoxamine Famotidine Molnupiravir Quercetin Diet Bamlanivimab/e.. Hydrogen Peroxide Budesonide Probiotics Casirivimab/i.. Sleep Curcumin Povidone-Iodine Nigella Sativa Melatonin Antihistamine H1RAs Acetaminophen ↑risk Exercise Vitamin D Antiandrogens Vitamin C PPIs ↑risk Colchicine Ivermectin Metformin Zinc HCQ 2020 2021 2023 2024 Pooled outcomes Specific outcome RCT pooled RCT specific Statistically significant ≥10% improvement ≥3 studies c19early.org February 2025 Time when COVID-19 studies showed efficacy
Azvudine Evusheld Sodium Bicarb.. Paxlovid Regdanvimab Vitamin B12 Sunlight Phthalocyanine Montelukast Alkalinization Fluvoxamine Famotidine Molnupiravir Quercetin Diet Bamlanivimab/e.. Hydrogen Peroxide Budesonide Probiotics Casirivimab/i.. Sleep Curcumin Povidone-Iodine Nigella Sativa Melatonin H1RAs Acetaminophen ↑risk Exercise Vitamin D Antiandrogens Vitamin C PPIs ↑risk Colchicine Ivermectin Metformin Zinc HCQ 2020 2021 2023 2024 Pooled outcomes Specific outcome RCT pooled RCT specific Statistically significant ≥10% improvement ≥3 studies c19early.org February 2025 Time when COVID-19 studies showed efficacy
Timeline for when studies showed efficacy - details and limitations. 0.5% of treatments show efficacy.
February 2025
c19early.org
Cost per life saved from NNT in
studies to date
Melatonin
9
48%
  $8
Vitamin D
70
37%
  $10
Alkalinization
8
46%
  $11
Zinc
21
30%
  $15
Vitamin C
44
20%
  $18
Colchicine
43
28%
  $26
HCQ
251
27%
  $26
Ivermectin
53
47%
  $26
Aspirin
66
9%
  $33
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
22
30%
  $1,248
Favipiravir
40
11%
  $1,935
Tixagev../c..
10
42%
  $74,506
Regdanvimab
7
63%
  $139,860
Sotrovimab
14
46%
  $299,464
Bamlaniv../e..
13
54%
  $301,549
Casirivimab/..
11
20%
  $452,469
Paxlovid
39
25%
  $543,982
Bebtelovimab
4
60%
  $737,601
Remdesivir
66
1%
  $1,558,440
Molnupiravir
27
13%
  $2,400,867
Conv. Plasma
52
-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. 0.5% of treatments show efficacy.
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All clinical results for selected treatments. 0.5% of treatments show efficacy.
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0 0.25 0.5 0.75 1 1.25 1.5 1.75 2+ Iota-carragee.. 80% [22-95%] 1 $1 394 very limited data Cost Studies Patients Improvement Relative Risk Chlorhexidine 79% [66-87%] 3 $1 509 limited data Proxalutamide 78% [70-83%] 4 $500 1,953 limited data Indomethacin 74% [-20-94%] 4 $5 605 limited data Cetylpyridin.. 68% [-620-99%] 1 $1 23 very limited data Regdanvimab 63% [51-71%] 11 $2,100 7,430 Ivermectin 60% [52-67%] 105 $1 220,423 Chlorphenira.. 56% [46-64%] 3 $5 806 very limited data Thermotherapy 56% [9-78%] 4 $0 217 very limited data Povidone-Iod.. 51% [38-61%] 21 $1 3,202 Diet 50% [41-57%] 29 $0 693,504 Alkalinization 49% [36-59%] 13 $1 6,304 HH-120 49% [-60-84%] 2 $500 345 very limited data pHOXWELL 47% [29-62%] 1 $10 556 very limited data Bemnifosbuvir 47% [-57-82%] 3 $500 359 very limited data Bamlaniv../e.. 47% [25-62%] 21 $1,250 35,320 variant dependent Quercetin 46% [20-64%] 12 $5 1,496 Ensovibep 46% [-173-89%] 2 $2,100 885 limited data Resveratrol 44% [-4-70%] 3 $1 360 limited data Adintrevimab 43% [-169-88%] 2 $2,100 2,483 intramuscular Melatonin 43% [30-54%] 18 $1 14,301 Bromhexine 43% [-5-69%] 7 $5 875 very limited data Sodium Bicar.. 43% [23-58%] 6 $1 1,013 Casirivimab/i.. 43% [24-57%] 33 $2,100 59,746 variant dependent Nigella Sativa 43% [24-57%] 14 $5 3,333 Tixagev../c.. 41% [24-55%] 18 $855 29,862 variant dependent Propolis 41% [-13-69%] 3 $1 410 very limited data Curcumin 41% [30-51%] 27 $5 14,886 Fluvoxamine 39% [21-52%] 21 $4 38,283 Montelukast 39% [14-56%] 9 $2 2,943 limited data Exercise 39% [33-44%] 68 $0 1,939,060 Hydrogen Per.. 38% [5-59%] 7 $1 835 very limited data Phthalocyan.. 38% [20-51%] 4 $5 5,245 Xiannuoxin 38% [-46-73%] 2 $106 1,027 very limited data Sunlight 37% [22-50%] 5 $0 19,665 Vitamin D 37% [32-42%] 123 $1 195,858 H1RAs 36% [20-48%] 17 $5 72,015 Nitazoxanide 35% [-8-61%] 14 $4 3,632 Selenium 34% [-40-69%] 4 $1 21,452 Bebtelovimab 34% [-24-65%] 6 $1,200 13,329 intravenous Vitamin A 31% [11-47%] 15 $2 22,297 Sleep 31% [23-39%] 16 $0 429,222 Spironolactone 31% [15-44%] 12 $5 28,019 Nitric Oxide 31% [-1-52%] 12 $11 2,236 Metformin 31% [27-34%] 104 $10 358,299 Antiandrogens 30% [21-38%] 49 $5 120,172 Vitamin B12 30% [5-48%] 4 $1 11,407 Hydroxychlor.. 28% [25-31%] 419 $1 591,536 Zinc 28% [18-36%] 46 $1 55,762 Probiotics 28% [18-36%] 28 $5 19,646 Budesonide 28% [18-36%] 15 $4 28,194 Colchicine 27% [18-36%] 56 $1 33,066 Ibuzatrelvir 27% [15-38%] 1 $1,390 126 very limited data Azvudine 27% [18-35%] 30 $25 35,229 Andrographol.. 27% [-8-50%] 7 $5 1,245 Vilobelimab 26% [-4-48%] 1 $6,350 368 intravenous N-acetylcys.. 25% [14-35%] 24 $1 26,243 Sotrovimab 25% [10-37%] 27 $2,100 56,351 variant dependent Amubarv../r.. 25% [-70-66%] 4 $1,380 1,568 intravenous Lactoferrin 24% [-24-53%] 8 $5 1,419 Ensitrelvir 23% [-19-50%] 4 $500 3,535 very limited data Vitamin C 21% [15-28%] 73 $1 89,000 Niclosamide 21% [-47-57%] 6 $50 2,091 very limited data Leritrelvir 21% [3-35%] 2 $50 1,399 very limited data Azelastine 21% [-3-39%] 3 $5 310 very limited data UDCA 19% [-3-36%] 21 $15 45,286 Camostat 18% [-3-34%] 16 $1 2,020 Famotidine 17% [8-24%] 30 $5 114,119 Paxlovid 16% [12-19%] 75 $1,390 164,459 independent trials refused Favipiravir 15% [5-24%] 71 $20 36,281 worse w/longer followup Vitamin K 14% [0-25%] 2 $1 7,806 very limited data Atilotrelvir 13% [1-23%] 1 $65 1,213 very limited data Deuremidevir 11% [-1-21%] 2 $112 1,432 very limited data Molnupiravir 11% [3-18%] 49 $707 183,723 mutagenic/teratogenic Aspirin 9% [2-14%] 77 $1 187,919 Peg.. Lambda 7% [-138-63%] 4 $500 2,143 subcutaneous Ibuprofen 0% [-9-9%] 13 $1 54,707 Acebilustat 0% [-1462-94%] 1 $2,000 120 very limited data Levilimab 0% [-289-74%] 1 $2,000 206 subcutaneous Sarilumab -0% [-21-17%] 11 $2,000 2,231 intravenous/subcutaneous Remdesivir -1% [-9-7%] 79 $3,120 202,845 worse w/longer followup Pomotrelvir -1% [-104-50%] 1 $1,390 230 very limited data Conv. Plasma -2% [-6-2%] 54 $5,000 31,210 intravenous Apremilast -3% [-42-25%] 2 $2,000 594 limited data Ravulizumab -5% [-45-24%] 2 $2,000 481 intravenous Lanadelumab -7% [-135-52%] 1 $10,000 55 very limited data Vitamin B9 -8% [-41-18%] 12 $1 54,954 Plasma-activ.. -9% [-234-64%] 1 $100 23 very limited data Razuprotafib -10% [-116-44%] 2 $2,000 134 subcutaneous Sargramostim -13% [-85-31%] 4 $2,000 870 very limited data Brexanolone -14% [-129-43%] 1 $34,000 28 very limited data Losartan -15% [-127-42%] 5 $5 665 very limited data Plitidepsin -16% [-356-71%] 2 $2,000 163 intravenous Trimodulin -17% [-116-37%] 1 $2,000 166 intravenous Cannabidiol -21% [-97-25%] 9 $25 17,978 Lufotrelvir -22% [-198-50%] 1 $2,000 58 intravenous Pacritinib -28% [-210-47%] 1 $2,000 200 very limited data Cenicriviroc -28% [-66-1%] 3 $2,000 1,000 limited data Acetaminoph.. -28% [-41--17%] 27 $1 543,459 Crizanlizumab -29% [-103-18%] 2 $2,500 463 intravenous BMS mAbs -36% [-492-69%] 1 $2,100 210 subcutaneous Brensocatib -41% [-88--6%] 1 $2,000 404 very limited data Danicopan -43% [-168-24%] 1 $2,000 201 very limited data PPIs -46% [-67--28%] 40 $5 228,512 Olokizumab -50% [-309-45%] 1 $2,000 248 subcutaneous TRV027 -54% [-202-22%] 2 $2,000 318 intravenous Glenzocimab -60% [-236-24%] 1 $2,000 62 intravenous Siltuximab -64% [-252-23%] 1 $2,000 149 intravenous rNAPc2 -65% [-304-32%] 1 $2,000 156 very limited data Posaconazole -131% [-200--78%] 1 $2,000 249 very limited data Emvododstat -132% [-628-26%] 1 $2,000 187 very limited data Goflikicept -135% [-492-7%] 1 $2,000 247 subcutaneous Pemivibart -150% [-6014-90%] 1 $5,775 477 intravenous Donidalorsen -151% [-602-11%] 1 $2,000 103 intravenous/subcutaneous Astodrimer So.. -205% [-7302-87%] 1 $10 197 very limited data All studies (pooled effects, all stages) c19early.org February 2025 Favors treatment Favors control
0 0.25 0.5 0.75 1 1.25 1.5 1.75 2+ Iota-carragee.. 80% 1 very limited data Studies, Improvement Relative Risk Chlorhexidine 79% 3 limited data Proxalutamide 78% 4 limited data Indomethacin 74% 4 limited data Cetylpyridin.. 68% 1 very limited data Regdanvimab 63% 11 Ivermectin 60% 105 Chlorphenira.. 56% 3 very limited data Thermotherapy 56% 4 very limited data Povidone-Iod.. 51% 21 Diet 50% 29 Alkalinization 49% 13 HH-120 49% 2 very limited data pHOXWELL 47% 1 very limited data Bemnifosbuvir 47% 3 very limited data Bamlaniv../e.. 47% 21 variant dependent Quercetin 46% 12 Ensovibep 46% 2 limited data Resveratrol 44% 3 limited data Adintrevimab 43% 2 intramuscular Melatonin 43% 18 Bromhexine 43% 7 very limited data Sodium Bicar.. 43% 6 Casirivimab/.. 43% 33 variant dependent Nigella Sativa 43% 14 Tixagev../c.. 41% 18 variant dependent Propolis 41% 3 very limited data Curcumin 41% 27 Fluvoxamine 39% 21 Montelukast 39% 9 limited data Exercise 39% 68 Hydrogen Per.. 38% 7 very limited data Phthalocyan.. 38% 4 Xiannuoxin 38% 2 very limited data Sunlight 37% 5 Vitamin D 37% 123 H1RAs 36% 17 Nitazoxanide 35% 14 Selenium 34% 4 Bebtelovimab 34% 6 intravenous Vitamin A 31% 15 Sleep 31% 16 Spironolactone 31% 12 Nitric Oxide 31% 12 Metformin 31% 104 Antiandrogens 30% 49 Vitamin B12 30% 4 Hydroxychlor.. 28% 419 Zinc 28% 46 Probiotics 28% 28 Budesonide 28% 15 Colchicine 27% 56 Ibuzatrelvir 27% 1 very limited data Azvudine 27% 30 Andrographol.. 27% 7 Vilobelimab 26% 1 intravenous N-acetylcys.. 25% 24 Sotrovimab 25% 27 variant dependent Amubarv../r.. 25% 4 intravenous Lactoferrin 24% 8 Ensitrelvir 23% 4 very limited data Vitamin C 21% 73 Niclosamide 21% 6 very limited data Leritrelvir 21% 2 very limited data Azelastine 21% 3 very limited data UDCA 19% 21 Camostat 18% 16 Famotidine 17% 30 Paxlovid 16% 75 independent trials refused Favipiravir 15% 71 worse w/longer followup Vitamin K 14% 2 very limited data Atilotrelvir 13% 1 very limited data Deuremidevir 11% 2 very limited data Molnupiravir 11% 49 mutagenic/teratogenic Aspirin 9% 77 Peg.. Lambda 7% 4 subcutaneous Ibuprofen 0% 13 Acebilustat 0% 1 very limited data Levilimab 0% 1 subcutaneous Sarilumab -0% 11 intravenous/subcutaneous Remdesivir -1% 79 worse w/longer followup Pomotrelvir -1% 1 very limited data Conv. Plasma -2% 54 intravenous Apremilast -3% 2 limited data Ravulizumab -5% 2 intravenous Lanadelumab -7% 1 very limited data Vitamin B9 -8% 12 Plasma-activ.. -9% 1 very limited data Razuprotafib -10% 2 subcutaneous Sargramostim -13% 4 very limited data Brexanolone -14% 1 very limited data Losartan -15% 5 very limited data Plitidepsin -16% 2 intravenous Trimodulin -17% 1 intravenous Cannabidiol -21% 9 Lufotrelvir -22% 1 intravenous Pacritinib -28% 1 very limited data Cenicriviroc -28% 3 limited data Acetaminoph.. -28% 27 Crizanlizumab -29% 2 intravenous BMS mAbs -36% 1 subcutaneous Brensocatib -41% 1 very limited data Danicopan -43% 1 very limited data PPIs -46% 40 Olokizumab -50% 1 subcutaneous TRV027 -54% 2 intravenous Glenzocimab -60% 1 intravenous Siltuximab -64% 1 intravenous rNAPc2 -65% 1 very limited data Posaconazole -131% 1 very limited data Emvododstat -132% 1 very limited data Goflikicept -135% 1 subcutaneous Pemivibart -150% 1 intravenous Donidalorsen -151% 1 intravenous/subcutaneous Astodrimer S.. -205% 1 very limited data All studies (pooled effects, all stages) c19early.org February 2025 Rotate device for details Favors treatment Favors control
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.
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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. 0.5% 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. 0.5% 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. 0.5% 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. 0.5% 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. 0.5% 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. 0.5% 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. 0.5% of proposed treatments show efficacy in clinical studies.
LATE TREATMENT
Physician / TeamLocationPatients HospitalizationHosp. MortalityDeath
Dr. David Uip (*) Brazil 2,200 38.6% (850) Ref. 2.5% (54) Ref.
EARLY TREATMENT - 40 physicians/teams
Physician / TeamLocationPatients 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.
Hu
926 patients prophylaxis: 89% lower severe cases (p=0.02) and 25% fewer symptomatic cases (p<0.0001)
Luetkemeyer
2,085 patient early treatment RCT: 203% higher hospitalization (p=0.37), 5% faster recovery (p=0.14), and 19% improved viral clearance (p=0.02)
Sun
2,924 patients late treatment PSM: 27% lower mortality (p=0.02) and 15% higher progression (p=0.16)
Soff
7,430 patients prophylaxis: 18% lower PASC (p=0.001)
Wimalawansa
Systematic review examining the evidence for vitamin D deficiency as a causative factor in COVID-19 susceptibility, complications, and mortality,..
Sümegi
148 patients late treatment: 67% lower mortality (p=0.0002)
Rahman
In Vitro study showing potential genotoxic side effects of remdesivir and molnupiravir linked to DNA repair pathway deficiencies. Remdesivir..
Rahman
In Vitro study showing potential genotoxic side effects of remdesivir and molnupiravir linked to DNA repair pathway deficiencies. Remdesivir..
Kızılet
Cross-sectional study of 153 COVID-19 patients and 78 healthy controls showing significantly lower serum zinc levels in COVID-19 patients compared..
Tassakos
Review of 15 studies examining associations between diet quality and COVID-19 severity and outcomes. Authors found that adherence to high-quality,..
Su
In Vitro study showing that inhalable spray-dried dry powders combining ivermectin and niclosamide exhibit enhanced anti-SARS-CoV-2 activity..
Recent studies (see the individual treatment pages for all studies):

Feb 17
Luetkemeyer et al., Clinical Infectious Diseases, doi:10.1093/cid/ciaf029 Ensitrelvir for the Treatment of Nonhospitalized Adults with COVID-19: Results from the SCORPIO-HR, Phase 3, Randomized, Double-blind, Placebo-Controlled Trial
203% higher hospitalization (p=0.37), 5% faster recovery (p=0.14), and 19% improved viral clearance (p=0.02). RCT 2,093 outpatients with mild-to-moderate COVID-19 showing improved viral clearance but no significant difference in time to symptom resolution with ensitrelvir. Participants were randomized to receive ensitrelvir or placebo within five..
Feb 15
Jarczak et al., RPS Pharmacy and Pharmacology Reports, doi:10.1093/rpsppr/rqae028 Potential drug interactions with nirmatrelvir/ritonavir in critically ill patients with COVID-19 – a retrospective observational study
Retrospective 500 critically ill COVID-19 patients in Germany showing potential drug-drug interactions with paxlovid in 48% of patients, with higher age and number of comorbidities significantly associated with drug-drug interactions. Aut..
Feb 6
Wimalawansa, S., Nutrients, doi:10.3390/nu17030599 Vitamin D Deficiency Meets Hill’s Criteria for Causation in SARS-CoV-2 Susceptibility, Complications, and Mortality: A Systematic Review
Systematic review examining the evidence for vitamin D deficiency as a causative factor in COVID-19 susceptibility, complications, and mortality, evaluated using Bradford Hill's criteria for causality. Author analyzed 294 studies, finding..
Feb 6
Hu et al., Frontiers in Medicine, doi:10.3389/fmed.2025.1494248 Ursodeoxycholic acid relieves clinical severity of COVID-19 in patients with chronic liver diseases
89% lower severe cases (p=0.02) and 25% fewer symptomatic cases (p<0.0001). Retrospective 926 outpatients with chronic liver diseases in China showing lower incidence of symptomatic COVID-19 and milder symptoms with ursodeoxycholic acid (UDCA) treatment.
Feb 5
Sun et al., VIEW, doi:10.1002/VIW.20240133 Antiviral effectiveness and safety of azvudine in hospitalized SARS‐CoV‐2 patients with pre‐existing chronic respiratory diseases: A multicenter, retrospective cohort study
27% lower mortality (p=0.02) and 15% higher progression (p=0.16). Retrospective 2,924 hospitalized COVID-19 patients with chronic respiratory diseases in China, showing lower all-cause mortality with azvudine, but no significant difference in composite disease progression.
Feb 4
Soff et al., BMJ Open Diabetes Research & Care, doi:10.1136/bmjdrc-2024-004536 Association of glycemic control with Long COVID in patients with type 2 diabetes: findings from the National COVID Cohort Collaborative (N3C)
18% lower PASC (p=0.001). Retrospective 7,430 COVID-positive patients with type 2 diabetes showing lower risk of long COVID or death with metformin use, and higher risk with insulin use.
Feb 1
Okushin et al., Internal Medicine, doi:10.2169/internalmedicine.4856-24 Use of Ursodeoxycholic Acid and the Risk of Severe Coronavirus Disease 2019 in Elderly Patients with Viral Hepatitis
72% higher mortality (p=0.03), 57% higher ventilation (p=0.48), 3% higher need for oxygen therapy (p=0.83), and 4% higher hospitalization (p=0.52). Retrospective 6,413 elderly patients with viral hepatitis in Japan showing increased mortality with ursodeoxycholic acid (UDCA) use in COVID-19 patients. There was no significant difference in hospitalization or oxygen therapy.
Feb 1
Tassakos et al., Current Nutrition Reports, doi:10.1007/s13668-025-00618-3 The Impact of Diet Quality on COVID-19 Severity and Outcomes—A Scoping Review
Review of 15 studies examining associations between diet quality and COVID-19 severity and outcomes. Authors found that adherence to high-quality, anti-inflammatory diets like the Mediterranean and DASH diets was generally associated with..
Jan 31
Tavares et al., Biophysica, doi:10.3390/biophysica5010004 Investigation of Interactions Between the Protein MPro and the Vanadium Complex VO(metf)2∙H2O: A Computational Approach for COVID-19 Treatment
In Silico study showing that the vanadium complex VO(metf)2∙H2O (VC) and metformin (MF) may be beneficial for COVID-19 treatment by interacting with the main protease (Mpro) of SARS-CoV-2. Using docking simulations, authors found that VC ..
Jan 31
Najih et al., Cureus, doi:10.7759/cureus.78291 Impact of Vitamin D Levels on Clinical Outcomes in SARS-CoV-2 Infections
53% fewer symptomatic cases (p=0.002). Cross-sectional study of 100 COVID-19 patients showing low vitamin D levels associated with increased symptom severity.
Jan 30
Su et al., International Journal of Pharmaceutics, doi:10.1016/j.ijpharm.2025.125302 Inhalable spray-dried dry powders combining ivermectin and niclosamide to inhibit SARS-CoV-2 infection in vitro
In Vitro study showing that inhalable spray-dried dry powders combining ivermectin and niclosamide exhibit enhanced anti-SARS-CoV-2 activity compared to the individual drugs. Authors developed stable, amorphous powders with aerodynamic pr..
Jan 30
Sümegi et al., Nutrients, doi:10.3390/nu17030507 Effect of Moderately High-Dose Vitamin D3 Supplementation on Mortality in Patients Hospitalized for COVID-19 Infection
67% lower mortality (p=0.0002). Retrospective 148 hospitalized COVID-19 patients showing significantly lower mortality (67% reduction) with moderately high-dose vitamin D3 treatment (30,000 IU for 3 days or 12,000 IU for 7 days followed by 3,000 IU daily), regardless of..
Jan 29
Bramante et al., Open Forum Infectious Diseases, doi:10.1093/ofid/ofae631.016 Metformin reduces the risk of Long COVID or Death over 6 months in an Emulated Target Trial of Primarily Omicron-infected Adults without Diabetes or Prediabetes: a New-User, Active-Comparator Analysis Using the National COVID Cohort Collaborative (N3C) Electronic Health Record Database. This research was supported in part by the Intramural/Extramural research program of the National Center for Advancing Translational Science, NIH
Emulated target trial of Omicron-infected outpatients without diabetes or prediabetes, showing significantly lower long COVID or death with metformin treatment.
Jan 29
Chua et al., Open Forum Infectious Diseases, doi:10.1093/ofid/ofae631.2172 Evaluating the use of Monoclonal Antibodies - Sotrovimab, Casirivimab/Imedvimab (REGEN-COV) and Tixagevimab/Cilgavimab (EVUSHELD) for COVID-19 Treatment in Singapore
PSM retrospective 366 hospitalized COVID-19 patients in Singapore showing no statistically significant reduction in severe outcomes with monoclonal antibodies (mAbs), except for lower oxygen use in patients treated with sotrovimab during ..
Jan 29
Nowak et al., Clinical Kidney Journal, doi:10.1093/ckj/sfaf030 COVID-19 among Kidney Transplant Recipients: Evaluating Risk Factors During the Initial Phase of the Pandemic
58% higher combined mortality/hospitalization (p=0.0002). Retrospective 5,824 kidney transplant recipients in Sweden showing proton pump inhibitor use associated with higher risk of severe COVID-19.
Jan 29
Jorda et al., Open Forum Infectious Diseases, doi:10.1093/ofid/ofae631.2173 Nirmatrelvir-ritonavir and molnupiravir for the outpatient treatment of Covid-19: a population-based cohort study
27% higher mortality (p=0.5) and 1% higher hospitalization (p=0.93). Retrospective 113,399 outpatients in Austria showing lower hospitalization and mortality with paxlovid treatment in patients over 60, but no significant differences with molnupiravir. Viral rebound was observed after treatment with both a..
Jan 29
Holmes et al., Open Forum Infectious Diseases, doi:10.1093/ofid/ofae631.2185 Results from a Phase 1 First in Human Study of Pemivibart: An Extended Half-Life Monoclonal Antibody (mAb)
Phase 1 RCT with 30 healthy participants showing pemivibart was well-tolerated at doses up to 4500 mg, with no serious adverse events or adverse events leading to drug discontinuation reported. Pemivibart demonstrated linear and dose-prop..
Jan 29
Holmes et al., Open Forum Infectious Diseases, doi:10.1093/ofid/ofae631.2191 Pharmacokinetics (PK) and Serum Virus Neutralizing Antibody (sVNA) Titers Following the 2nd dose of Pemivibart in the Phase 3 CANOPY Trial
Pharmacokinetics (PK) and Serum Virus Neutralizing Antibody (sVNA) analysis for the CANOPY trial showing a second dose boosted serum virus neutralizing antibody titers by 17% compared to the first dose. A population pharmacokinetic model ..
Jan 27
Horby et al., medRxiv, doi:10.1101/2025.01.24.25321081 Sotrovimab versus usual care in patients admitted to hospital with COVID-19: a randomised, controlled, open-label, platform trial (RECOVERY)
5% lower mortality (p=0.64), 4% lower hospital discharge (p=0.51), and 2% lower combined mortality/ICU admission (p=0.82). RCT 1,723 hospitalized COVID-19 patients showing lower 28-day mortality with sotrovimab in patients with high serum nucleocapsid antigen levels, but no significant benefit in the overall population. Sotrovimab reduced mortality from 29% t..
Jan 27
Zvornicanin et al., bioRxiv, doi:10.1101/2025.01.24.634813 Molecular Mechanisms of Drug Resistance and Compensation in SARS-CoV-2 Main Protease: The Interplay Between E166 and L50
In Vitro study showing that mutations at position E166 in the SARS-CoV-2 main protease (Mpro) confer resistance to nirmatrelvir, the active component of paxlovid, while preserving substrate cleavage. Authors found that E166A and E166V mut..
Jan 24
Moharram et al., PLOS ONE, doi:10.1371/journal.pone.0313616 Secondary metabolites of Alternaria alternate appraisal of their SARS-CoV-2 inhibitory and anti-inflammatory potentials
In Silico and In Vitro study showing that compounds isolated from the fungus Alternaria alternate inhibit SARS-CoV-2 infection by blocking the ACE2-Spike protein interaction and reducing ACE2 expression and inflammatory cytokines. Quercet..
Jan 24
Spinelli et al., Chemistry & Biodiversity, doi:10.1002/cbdv.202403202 Amphibian‐Derived Peptides as Natural Inhibitors of SARS‐CoV‐2 Main Protease (Mpro): A Combined In Vitro and In Silico Approach
In Vitro and In Silico study showing that amphibian-derived peptides inhibit SARS-CoV-2 main protease (Mpro). Authors tested 23 peptides from Hylidae and Leptodactylidae amphibians and found five with significant Mpro inhibition, with IC5..
Jan 20
Knez et al., Frontiers in Immunology, doi:10.3389/fimmu.2024.1490478 TLR10 overexpression modulates immune response in A549 lung epithelial cells challenged with SARS-CoV-2 S and N proteins
In Vitro study showing that overexpression of TLR10 in A549 lung epithelial cells immunostimulated with SARS-CoV-2 S and N proteins mainly downregulated proinflammatory cytokines and interferons and affected gene expression in cocultured ..
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 5,366 studies, 2,560 present results comparing with a control group, 2,348 are treatment studies, and 212 analyze outcomes based on serum levels. There are 100 animal studies, 196 in silico studies, 362 in vitro studies, 419 reviews, and 234 meta analyses.
Please send us corrections, updates, or comments. c19early involves the extraction of 100,000+ 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. FLCCC and WCH provide treatment protocols.
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