Covid19 Clinical Trial - Hydrogen-oxygen Gas Mixture NCT04594460

Clinical Trial Details — Status: Not yet recruiting

Administrative data
NCT number	NCT04594460
Other study ID #	AMS-H-03-101
Secondary ID
Status	Not yet recruiting
Phase	N/A
First received
Last updated
Start date	October 31, 2020
Est. completion date	December 31, 2021

Study information
Verified date	October 2020
Source	Guangzhou Institute of Respiratory Disease
Contact	Wei-jie Guan, PhD
Phone	+86-13826042052
Email	battery203[@]163.com
Is FDA regulated	No
Health authority
Study type	Interventional

Clinical Trial Summary

This study is a multicenter, randomized, open, parallel-controlled study. Qualified subjects will randomly be assigned to the experimental arm or the control arm according to the ratio of 1:1, with age (> 60 years or ≤ 60 years), smoking status (yes/no) and forced expiratory volume in one second/prediction (FEV1 %pred > 60% or ≤ 60%) as the random stratification factors.

Description:

Subjects in the experimental arm and the control arm will receive hydrogen-oxygen mixed gas inhalation (Hydrogen-Oxygen Generator with Nebulizer, AMS-H-03, output: 3 L/min (hydrogen concentration: 66.7%, oxygen concentration: 33.3%)) and oxygen inhalation (OLO-1 Medical Molecular Sieve Oxygen Generator, output: 3 L/min (oxygen concentration: 33.3%), Shanghai Ouliang Medical Devices Co., Ltd.), respectively; the treatment duration will not be less than 8 hours per day, for 12 weeks. Subjects in the experimental arm and the control arm will also receive other medications (excluding antiviral drugs) by the investigator as clinically indicated. Six visits are required for each subject in this study, including Visit 1 (D-7~-1), Visit 2 (D1), Visit 3 (D14±3d), Visit 4 (D28±3d), Visit 5 (D56±7d), Visit 6 (D84±7d).

Recruitment information / eligibility
Status	Not yet recruiting
Enrollment	198
Est. completion date	December 31, 2021
Est. primary completion date	October 31, 2021
Accepts healthy volunteers	No
Gender	All
Age group	18 Years to 75 Years
Eligibility	Inclusion Criteria: - 1) Male or female, aged between 18 and 75 (including boundary values) at screening. 2) Severe or critically ill patients who have been diagnosed with a novel coronavirus during hospitalization (COVID-19). 3) After treatment, the patients have met the discharge criteria of "COVID-19 Diagnosis and Treatment Guideline", and the time from hospital discharge is at least 1 month at the time of enrollment. The clinical symptoms of the subjects did not worsen significantly as compared with that at the time of discharge, and the COVID-19 nucleic acid test results are negative for at least 2 consecutive times (one of which could be the nucleic acid test before discharge). 4) Forced vital capacity/per predicted (FVC% pred) = 50%. 5) 50% = FEV1 %pred =80%? 6) Subject (or legally authorized representative) provides written informed consent prior to initiation of any study procedures. Understands and agrees to comply with planned study procedures. 7) Agrees not to participate in other drug/device studies until the study is completed. Exclusion Criteria: - 1) With one of the following respiratory diseases: 1. Subjects with asthma history, or cannot rule out asthma based on the diagnosis of investigator; 2. Subjects with chronic obstructive pulmonary disease (COPD); 3. Subjects with following respiratory diseases such as active tuberculosis, lung cancer, sarcoidosis, pulmonary hypertension, pneumothorax, uncontrolled pleural effusion through intervention, pulmonary embolism, etc.; 4. Lung volume reduction: subjects have had lung volume reduction surgery, pulmonary lobectomy, or bronchoscopic lung volume reduction surgery. 2) Subjects with pulmonary heart disease. 3) Patients who are scheduled for elective surgery during the study period, such as thoracic and abdominal major surgery. 4) Subjects, judged by investigators, with previous or current diseases, which may affect the participation in this study or the outcome of this study: such as cancer, diseases of heart, liver, kidney, hematopoietic system and other vital organs or systems, etc. 5) Patients who have undergone surgery within 1 month prior to screening and have not fully recovered. 6) Occurrence of congestive heart failure, uncontrolled or unstable angina or myocardial infarction, cerebrovascular accident, or history of pulmonary embolism within 6 months prior to screening. 7) Patients with active tuberculosis infection within 12 months prior to screening. 8) Pregnancy or lactating women, or women of childbearing potential not agree to either abstinence or use at least one primary form of contraception from the time of screening till the study is completed. 9) Subjects with mental disorders or other conditions that are unable to cooperate effectively with the conduct of the clinical trial. 10) Subjects intolerance to inhalation therapy. 11) Others whom the investigator or sub-investigator judged inappropriate for participation in the study.

Study Design

Related Conditions & MeSH terms

Intervention

Device:
• Hydrogen-Oxygen Generator with Nebulizer, AMS-H-03
the experimental arm will receive hydrogen-oxygen mixed gas inhalation (Hydrogen-Oxygen Generator with Nebulizer, AMS-H-03, output: 3 L/min (hydrogen concentration: 66.7%, oxygen concentration: 33.3%)) ,the treatment duration will be 8 hours per day, for 12 weeks.
• OLO-1 Medical Molecular Sieve Oxygen Generator
the control arm will receive oxygen inhalation (OLO-1 Medical Molecular Sieve Oxygen Generator, output: 3 L/min (oxygen concentration: 33.3%), Shanghai Ouliang Medical Devices Co., Ltd.)the treatment duration will be 8 hours per day, for 12 weeks.

Locations
Country	Name	City	State
China	First Affiliated Hospital of Guangzhou Medical University	Guangzhou	Guangdong
China	Guangzhou Institute of Respiratory Disease	Guangzhou	Guangdong

Sponsors *(1)*
Lead Sponsor	Collaborator
Guangzhou Institute of Respiratory Disease

Country where clinical trial is conducted

China,

References & Publications (11)

Chinese Clinical Guidance for COVID-19 Penumonia Diagnosis and Treatment (7th edition)

Guan WJ, Wei CH, Chen AL, Sun XC, Guo GY, Zou X, Shi JD, Lai PZ, Zheng ZG, Zhong NS. Hydrogen/oxygen mixed gas inhalation improves disease severity and dyspnea in patients with Coronavirus disease 2019 in a recent multicenter, open-label clinical trial. J Thorac Dis. 2020 Jun;12(6):3448-3452. doi: 10.21037/jtd-2020-057. Erratum in: J Thorac Dis. 2020 Aug;12(8):4591-4592. — View Citation

Huang X, Wei F, Hu L, Wen L, Chen K. Epidemiology and Clinical Characteristics of COVID-19. Arch Iran Med. 2020 Apr 1;23(4):268-271. doi: 10.34172/aim.2020.09. Review. — View Citation

Kannan S, Shaik Syed Ali P, Sheeza A, Hemalatha K. COVID-19 (Novel Coronavirus 2019) - recent trends. Eur Rev Med Pharmacol Sci. 2020 Feb;24(4):2006-2011. doi: 10.26355/eurrev_202002_20378. Review. — View Citation

Li K, Wu J, Wu F, Guo D, Chen L, Fang Z, Li C. The Clinical and Chest CT Features Associated With Severe and Critical COVID-19 Pneumonia. Invest Radiol. 2020 Jun;55(6):327-331. doi: 10.1097/RLI.0000000000000672. — View Citation

Li LQ, Huang T, Wang YQ, Wang ZP, Liang Y, Huang TB, Zhang HY, Sun W, Wang Y. COVID-19 patients' clinical characteristics, discharge rate, and fatality rate of meta-analysis. J Med Virol. 2020 Jun;92(6):577-583. doi: 10.1002/jmv.25757. Epub 2020 Mar 23. Review. — View Citation

Mo X, Jian W, Su Z, Chen M, Peng H, Peng P, Lei C, Chen R, Zhong N, Li S. Abnormal pulmonary function in COVID-19 patients at time of hospital discharge. Eur Respir J. 2020 Jun 18;55(6). pii: 2001217. doi: 10.1183/13993003.01217-2020. Print 2020 Jun. — View Citation

Ong KC, Ng AW, Lee LS, Kaw G, Kwek SK, Leow MK, Earnest A. Pulmonary function and exercise capacity in survivors of severe acute respiratory syndrome. Eur Respir J. 2004 Sep;24(3):436-42. — View Citation

Yang Y, Zhu Y, Xi X. Anti-inflammatory and antitumor action of hydrogen via reactive oxygen species. Oncol Lett. 2018 Sep;16(3):2771-2776. doi: 10.3892/ol.2018.9023. Epub 2018 Jun 26. Review. — View Citation

Zhang N, Deng C, Zhang X, Zhang J, Bai C. Inhalation of hydrogen gas attenuates airway inflammation and oxidative stress in allergic asthmatic mice. Asthma Res Pract. 2018 Mar 15;4:3. doi: 10.1186/s40733-018-0040-y. eCollection 2018. — View Citation

Zhou ZQ, Zhong CH, Su ZQ, Li XY, Chen Y, Chen XB, Tang CL, Zhou LQ, Li SY. Breathing Hydrogen-Oxygen Mixture Decreases Inspiratory Effort in Patients with Tracheal Stenosis. Respiration. 2019;97(1):42-51. doi: 10.1159/000492031. Epub 2018 Sep 18. — View Citation

* Note: There are 11 references in all — Click here to view all references

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Hydrogen-oxygen Gas Mixture Inhalation in Patients With Convalescent Coronavirus Disease 2019 (COVID-19)

Clinical Trial Details — Status: Not yet recruiting

Administrative data

Study information

Clinical Trial Summary

Description:

Recruitment information / eligibility

Study Design

Related Conditions & MeSH terms

Intervention

Locations

Sponsors (1)

Country where clinical trial is conducted

References & Publications (11)

Outcome

Type	Measure	Description	Time frame
Primary	(VO2max)	The change from baseline in maximum oxygen consumption (VO2max) at maximum exercise load at Week 12 of treatment.	The change from baseline in maximum oxygen consumption (VO2max) at maximum exercise load at Week 12 of treatment.
Secondary	(VO2max)	The change from baseline in maximum oxygen consumption (VO2max) at maximum exercise load at Week 4 of treatment.	The change from baseline in maximum oxygen consumption (VO2max) at maximum exercise load at Week 4 of treatment.
Secondary	(VO2max)	The change from baseline in maximum oxygen consumption (VO2max) at maximum exercise load at Week 8 of treatment.	The change from baseline in maximum oxygen consumption (VO2max) at maximum exercise load at Week 8 of treatment.
Secondary	(VE /VCO2)	Differences in the change from baseline in ventilatory equivalent for carbon dioxide (VE /VCO2) at maximum exercise load at Week 4 of treatment.	Differences in the change from baseline in ventilatory equivalent for carbon dioxide (VE /VCO2) at maximum exercise load at Week 4 of treatment.
Secondary	(VE /VCO2)	Differences in the change from baseline in ventilatory equivalent for carbon dioxide (VE /VCO2) at maximum exercise load at Week 8 of treatment.	Differences in the change from baseline in ventilatory equivalent for carbon dioxide (VE /VCO2) at maximum exercise load at Week 8 of treatment.
Secondary	(VE /VCO2)	Differences in the change from baseline in ventilatory equivalent for carbon dioxide (VE /VCO2) at maximum exercise load at Week 12 of treatment.	Differences in the change from baseline in ventilatory equivalent for carbon dioxide (VE /VCO2) at maximum exercise load at Week 12 of treatment.
Secondary	(VE /VO2)	Differences in the change from baseline in ventilatory equivalent for oxygen (VE /VO2) at maximum exercise load at Week 4 of treatment.	Differences in the change from baseline in ventilatory equivalent for oxygen (VE /VO2) at maximum exercise load at Week 4 of treatment.
Secondary	(VE /VO2)	Differences in the change from baseline in ventilatory equivalent for oxygen (VE /VO2) at maximum exercise load at Week 8 of treatment.	Differences in the change from baseline in ventilatory equivalent for oxygen (VE /VO2) at maximum exercise load at Week 8 of treatment.
Secondary	(VE /VO2)	Differences in the change from baseline in ventilatory equivalent for oxygen (VE /VO2) at maximum exercise load at Week 12 of treatment.	Differences in the change from baseline in ventilatory equivalent for oxygen (VE /VO2) at maximum exercise load at Week 12 of treatment.
Secondary	(VO2 /HR)	Differences in the change from baseline in oxygen pulse (VO2 /HR) at maximum exercise load at Week 4 treatment.	Differences in the change from baseline in oxygen pulse (VO2 /HR) at maximum exercise load at Week 4 of treatment.
Secondary	(VO2 /HR)	Differences in the change from baseline in oxygen pulse (VO2 /HR) at maximum exercise load at Week 8 of treatment.	Differences in the change from baseline in oxygen pulse (VO2 /HR) at maximum exercise load at Week 8 of treatment.
Secondary	(VO2 /HR)	Differences in the change from baseline in oxygen pulse (VO2 /HR) at maximum exercise load at Week 12 of treatment.	Differences in the change from baseline in oxygen pulse (VO2 /HR) at maximum exercise load at Week 12 of treatment.
Secondary	(P (A-a) O2)	The change from baseline in the alveolar-arterial oxygen tension gradient (P (A-a) O2) at maximum exercise load at Week 4 of treatment.	The change from baseline in the alveolar-arterial oxygen tension gradient (P (A-a) O2) at maximum exercise load at Week 4 of treatment.
Secondary	(P (A-a) O2)	The change from baseline in the alveolar-arterial oxygen tension gradient (P (A-a) O2) at maximum exercise load at Week 8 of treatment.	The change from baseline in the alveolar-arterial oxygen tension gradient (P (A-a) O2) at maximum exercise load at Week 8 of treatment.
Secondary	(P (A-a) O2)	The change from baseline in the alveolar-arterial oxygen tension gradient (P (A-a) O2) at maximum exercise load at Week 12 of treatment.	The change from baseline in the alveolar-arterial oxygen tension gradient (P (A-a) O2) at maximum exercise load at Week 12 of treatment.
Secondary	(P (a-et) CO2)	The change from baseline in the arterial-to-end-tidal CO2 difference (P (a-et) CO2) at maximum exercise load at Week 4 of treatment.	The change from baseline in the arterial-to-end-tidal CO2 difference (P (a-et) CO2) at maximum exercise load at Week 4 of treatment.
Secondary	(P (a-et) CO2)	The change from baseline in the arterial-to-end-tidal CO2 difference (P (a-et) CO2) at maximum exercise load at Week 8 of treatment.	The change from baseline in the arterial-to-end-tidal CO2 difference (P (a-et) CO2) at maximum exercise load at Week 8 of treatment.
Secondary	(P (a-et) CO2)	The change from baseline in the arterial-to-end-tidal CO2 difference (P (a-et) CO2) at maximum exercise load at Week 12 of treatment.	The change from baseline in the arterial-to-end-tidal CO2 difference (P (a-et) CO2) at maximum exercise load at Week 12 of treatment.
Secondary	maximum exercise power	The change from baseline in maximum exercise power at Week 4 of treatment.	The change from baseline in maximum exercise power at Week 4 of treatment.
Secondary	maximum exercise power	The change from baseline in maximum exercise power at Week 8 of treatment.	The change from baseline in maximum exercise power at Week 8 of treatment.
Secondary	maximum exercise power	The change from baseline in maximum exercise power at Week 12 of treatment.	The change from baseline in maximum exercise power at Week 12 of treatment.
Secondary	RER	The change from baseline in respiratory quotient (RER) at maximum exercise load at Week 4 of treatment.	The change from baseline in respiratory quotient (RER) at maximum exercise load at Week 4 of treatment.
Secondary	RER	The change from baseline in respiratory quotient (RER) at maximum exercise load at Week 8 of treatment.	The change from baseline in respiratory quotient (RER) at maximum exercise load at Week 8 of treatment.
Secondary	RER	The change from baseline in respiratory quotient (RER) at maximum exercise load at Week 12 of treatment.	The change from baseline in respiratory quotient (RER) at maximum exercise load at Week 12 of treatment.
Secondary	The change from baseline in total exercise duration at maximum exercise load at Week 4 of treatment.	The change from baseline in total exercise duration at maximum exercise load at Week 4 of treatment.	The change from baseline in total exercise duration at maximum exercise load at Week 4 of treatment.
Secondary	The change from baseline in total exercise duration at maximum exercise load at Week 8 of treatment.	The change from baseline in total exercise duration at maximum exercise load at Week 8 of treatment.	The change from baseline in total exercise duration at maximum exercise load at Week 8 of treatment.
Secondary	The change from baseline in total exercise duration at maximum exercise load at Week 12 of treatment.	The change from baseline in total exercise duration at maximum exercise load at Week 12 of treatment.	The change from baseline in total exercise duration at maximum exercise load at Week 12 of treatment.
Secondary	(SpO2)	The change from baseline in fingertip oxygen saturation (SpO2) at rest and without oxygen inhalation at Week 4 of treatment.	The change from baseline in fingertip oxygen saturation (SpO2) at rest and without oxygen inhalation at Week 4 of treatment.
Secondary	(SpO2)	The change from baseline in fingertip oxygen saturation (SpO2) at rest and without oxygen inhalation at Week 8 of treatment.	The change from baseline in fingertip oxygen saturation (SpO2) at rest and without oxygen inhalation at Week 8 of treatment.
Secondary	(SpO2)	The change from baseline in fingertip oxygen saturation (SpO2) at rest and without oxygen inhalation at Week 12 of treatment.	The change from baseline in fingertip oxygen saturation (SpO2) at rest and without oxygen inhalation at Week 12 of treatment.
Secondary	(mMRC)	The change from baseline in the modified Medical Research Council (mMRC) Dyspnea Scale score at week 4 of treatment.	The change from baseline in the modified Medical Research Council (mMRC) Dyspnea Scale score at week 4 of treatment.
Secondary	(mMRC)	The change from baseline in the modified Medical Research Council (mMRC) Dyspnea Scale score at week 8 of treatment.	The change from baseline in the modified Medical Research Council (mMRC) Dyspnea Scale score at week 8 of treatment.
Secondary	(mMRC)	The change from baseline in the modified Medical Research Council (mMRC) Dyspnea Scale score at week 12 of treatment.	The change from baseline in the modified Medical Research Council (mMRC) Dyspnea Scale score at week 12 of treatment.