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Clinical Trial Details — Status: Completed

Administrative data

NCT number NCT04505722
Other study ID # CR108876
Secondary ID VAC31518COV3001
Status Completed
Phase Phase 3
First received
Last updated
Start date September 7, 2020
Est. completion date March 31, 2023

Study information

Verified date May 2024
Source Janssen Vaccines & Prevention B.V.
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The study will evaluate the efficacy of Ad26.COV2.S in the prevention of molecularly confirmed moderate to severe/critical COVID-19, as compared to placebo, in adult participants.


Recruitment information / eligibility

Status Completed
Enrollment 44325
Est. completion date March 31, 2023
Est. primary completion date March 31, 2023
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 18 Years and older
Eligibility Inclusion Criteria: - Contraceptive (birth control) use should be consistent with local regulations regarding the acceptable methods of contraception for those participating in clinical studies - All participants of childbearing potential must: have a negative highly sensitive urine pregnancy test at screening; and have a negative highly sensitive urine pregnancy test immediately prior to each study vaccine administration - Participant agrees to not donate bone marrow, blood, and blood products from the first study vaccine administration until 3 months after receiving the last dose of study vaccine - Must be willing to provide verifiable identification, has means to be contacted and to contact the investigator during the study - Must be able to read, understand, and complete questionnaires in the electronic clinical outcome assessment (eCOA) (that is, the coronavirus disease-2019 [COVID 19] signs and symptoms surveillance question, the e-Diary, and the electronic patient-reported outcomes (ePROs). Note: Participants with visual impairment are eligible for study participation and may have caregiver assistance in completing the electronic clinical outcome assessment (eCOA) questionnaires Exclusion Criteria: - Participant has a clinically significant acute illness (this does not include minor illnesses such as diarrhea or mild upper respiratory tract infection) or temperature greater than or equal to (>=) 38.0 degree Celsius (100.4-degree Fahrenheit) within 24 hours prior to the planned first dose of study vaccine; randomization at a later date is permitted at the discretion of the investigator and after consultation with the sponsor - Participant received or plans to receive: (a) licensed live attenuated vaccines - within 28 days before or after planned administration of study vaccine ; and (b) other licensed (not live) vaccines - within 14 days before or after planned administration of study vaccine - Participant previously received a coronavirus vaccine - Participant received an investigational drug (including investigational drugs for prophylaxis of COVID-19) within 30 days or used an invasive investigational medical device within 30 days or received investigational immunoglobulin (Ig) or monoclonal antibodies within 3 months, or received convalescent serum for COVID-19 treatment within 4 months or received an investigational vaccine (including investigational Adenoviral-vectored vaccines) within 6 months before the planned administration of the first dose of study vaccine or is currently enrolled or plans to participate in another investigational study during the course of this study

Study Design


Intervention

Biological:
Ad26.COV2.S
Ad26.COV2.S will be administered at a single dose of 5*10^10 virus particles (vp) on Day 1 (or Month 6 for placebo recipients) and as a single booster dose at Year 1.
Other:
Placebo
Participants will receive Placebo.

Locations

Country Name City State
Argentina CEMEDIC Buenos Aires
Argentina CIPREC Buenos Aires
Argentina Helios Salud Sa Buenos Aires
Argentina Centro Medico Viamonte SRL Ciudad Autonoma Buenos Aires
Argentina Clinical Trials Division-Stamboulian Servicios de Salud Ciudad Autonoma Buenos Aires
Argentina Fundacion Huesped Ciudad Autonoma De Buenos Aire
Argentina Clínica y Maternidad Suizo Argentina Ciudad Autonoma de Buenos Aires
Argentina CEMIC Saavedra Ciudad de Buenos Aires
Argentina Hospital J. M. Ramos Mejía Ciudad de Buenos Aires
Argentina Hospital Italiano de La Plata La Plata
Argentina Instituto Medico Platense La Plata
Argentina DIM Clinica Privada Ramos Mejia
Brazil Faculdade de Medicina Barretos FACISB Barretos
Brazil Santa Casa de Misericordia de Belo Horizonte Belo Horizonte
Brazil Universidade Federal De Minas Gerais - Hospital das Clínicas Belo Horizonte
Brazil L2IP Instituto de Pesquisas Clinicas Brasilia
Brazil Sociedade Campineira de Educacao e Instrucao Hospital e Maternidade Celso Pierro Campinas
Brazil Fundacao Universidade Federal de Mato Grosso do Sul Campo Grande
Brazil Sociedade Literaria e Caritativa Santo Agostinho Hospital Sao Jose Criciúma
Brazil Oncovida - Centro de Onco-Hematologia de Mato Grosso Cuiaba
Brazil Hospital Nossa Senhora Das Gracas Curitiba
Brazil Centro de Estudos e Pesquisas em Moléstias Infecciosas Natal
Brazil Hospital das Clinicas de Porto Alegre Porto Alegre
Brazil Hospital Nossa Senhora da Conceicao S A Porto Alegre
Brazil Hospital Das Clinicas Da Faculdade De Medicina De RPUSP HCRP Ribeirao Preto
Brazil Fundacao Oswaldo Cruz Rio de Janeiro
Brazil Instituto Brasil de Pesquisa Clinica Rio de Janeiro
Brazil Ministerio da Saude - Hospital dos Servidores do Estado - RJ Rio de Janeiro
Brazil Municipio de Nova Iguacu - Hospital Geral de Nova Iguacu Rio de Janeiro
Brazil Fundacao Bahiana De Infectologia Salvador
Brazil Universidade Municipal de Sao Caetano do Sul Sao Caetano do Sul
Brazil Fundacao Faculdade Regional de Medicina de Sao Jose do Rio Preto - Hospital de Base Sao Jose do Rio Preto
Brazil Centro de Referencia E Treinamento Dst/Aids Sao Paulo
Brazil CEPIC - Centro Paulista de Investigação Clínica e Serviços Médicos Sao Paulo
Brazil Hospital Das Clinicas Da Faculdade De Medicina Da USP Sao Paulo
Brazil Instituto de infectologia Emilio Ribas Sao Paulo
Brazil Real e Benemerita Associacao Portuguesa de Beneficencia Sao Paulo
Brazil CPQuali Pesquisa Clinica LTDA ME São Paulo
Brazil Sociedade Beneficente de Senhoras - Hospital Sírio Libanês São Paulo
Chile Centro de Estudios Clínicos e Investigación Médica (CeCim) Santiago
Chile Facultad de Medicina Universidad de Chile Santiago
Chile Hospital Padre Hurtado Santiago
Chile Centro de Investigacion del Maule Talca
Chile Hospital Dr Hernan Henriquez Aravena Temuco
Chile Centro de Estudios Clinicos V Region Ltda Vina del Mar
Colombia Centro de Reumatologia y Ortopedia Barranquilla
Colombia Clinica de la Costa Barranquilla
Colombia Hospital Universidad del Norte Barranquilla
Colombia Centro de Atencion e Investigacion Medica S.A. - CAIMED Bogota
Colombia Medplus Medicina Prepagada S.A. Bogota
Colombia Solano y Terront Servicios Médicos Ltda. Bogota
Colombia Centro de Investigaciones Clinicas S A S Cali
Colombia Fundación Valle del Lili Cali
Colombia Fundación Cardiovascular de Colombia - Instituto del Corazón Floridablanca Floridablanca
Colombia Fundacion Oftalmologica de Santander - FOSCAL Floridablanca
Colombia Fundacion Centro de Investigacion Clinica CIC Medellin
Colombia Programa de Estudio y Control de Enfermedades Tropicales Medellin
Colombia Hospital Pablo Tobon Uribe Medellín
Mexico Instituto Nacional de Ciencias Medicas y Nutricion Salvador Zubiran Ciudad de Mexico
Mexico Instituto Nacional de Salud Publica Cuernavaca
Mexico Hospital Civil Fray Antonio Alcalde Guadalajara
Mexico Unidad de Atención Medica e Investigacion en Salud (UNAMIS) Merida
Mexico CAIMED Investigacion en salud S.A de C.V. Mexico
Mexico Centro Medico Nacional Siglo XXI IMSS Mexico
Mexico Instituto Nacional de Enfermedades Respiratorias Mexico
Mexico Hospital Universitario de Nuevo Leon 'Dr Jose Eleuterio Gonzalez' Monterrey
Mexico Infectolab Tijuana
Peru Centro de Investigaciones Tecnologicas, Biomedica y medio ambientales (CITBM) Callao
Peru Centro de Invetigaciones Medicas Callao
Peru Hospital Nacional Daniel Alcides Carrion Callao
Peru Asociacion Civil Selva Amazonica (ACSA) Iquitos
Peru Asociacion Civil Impacta Salud y Educacion- San Miguel CRS Lima
Peru Asociacion Civil Via Libre Lima
Peru Hospital Nacional Arzobispo Loayza Lima
Peru Hospital Nacional Edgardo Rebagliati Martins Lima
Peru Instituto de Investigacion Nutricional Lima
Peru Asociacion Civil Impacta Salud y Educacion - Barranco Lima - Barranco
South Africa Josha Research Bloemfontein
South Africa Desmond Tutu HIV Foundation Cape Town
South Africa Desmond Tutu Hiv Foundation - University Of Cape Town Cape Town
South Africa Family Clinical Research Unit FAM-CRU Cape Town
South Africa Masiphumelele Research Centre Cape Town
South Africa Synexus Helderberg Clinical Research Centre Cape Town
South Africa TASK Central Cape Town
South Africa University of Cape Town IDM/CIDRI Research Site Cape Town
South Africa Ndlovu Elandsdoorn Site Dennilton
South Africa SA Medical Research Council Durban
South Africa SA Medical Research Council Durban
South Africa CRISMO Bertha Gxowa Research Centre Johannesburg
South Africa Shandukani Research Centre Johannesburg
South Africa The Aurum Institute Klerksdorp Clinical Research Centre Klerksdorp
South Africa Centre for the AIDS Programme of Research in South Africa KwaZulu-Natal
South Africa Qhakaza Mbokodo Research Centre KwaZulu-Natal
South Africa South African Medical Research Council Chatsworth Clinical Research Site KwaZulu-Natal
South Africa Stanza Clinical Research Centre : Mamelodi Mamelodi East
South Africa Mzansi Ethical Research Centre Middelburg
South Africa Nelson Mandela Academic Clinical Research Unit 'NeMACRU' Mthatha
South Africa PHOENIX PHARMA (Pty) Ltd Port Elizabeth
South Africa MeCRU Clinical Research Unit Pretoria
South Africa Synexus Watermeyer Pretoria
South Africa The Aurum Institute Rustenburg Clinical Research Site Rustenburg
South Africa Setshaba Research Centre Soshanguve
South Africa Perinatal HIV Research Unit (PHRU), Kliptown Soweto
South Africa Perinatal HIV Research Unit, Chris Hani Baragwanath Hospital Soweto
South Africa The Aurum Institute: Tembisa - Clinic 4 Tembisa
South Africa CAPRISA Vulindlela Clinic Vulindlela
South Africa University of Witwatersrand - Helen Joseph Hospital - Themba Lethu Hiv Research Centre Westdene Johannesburg Gauteng
South Africa SATVI, Brewelskloof Hospital Worcester
United States Synexus Clinical Research US Inc Akron Ohio
United States Raymond G. Murphy VA Medical Center Albuquerque New Mexico
United States Anaheim Clinical Trials, LLC Anaheim California
United States Synexus Clinical Research US Inc Anderson South Carolina
United States University of Michigan Neuorsurgery A. Alfred Taubman Health Care Center Ann Arbor Michigan
United States Emory University of Medicine Atlanta Georgia
United States Childrens Hospital Colorado Aurora Colorado
United States Benchmark Research Austin Texas
United States Optimal Research, LLC Austin Texas
United States Baltimore VA Medical Center Baltimore Maryland
United States Alabama Vaccine Research Clinic at UAB Birmingham Alabama
United States Synexus Clinical Research US Inc Birmingham Alabama
United States University of Alabama Birmingham Birmingham Alabama
United States Massachusetts General Hospital Boston Massachusetts
United States The Brigham and Women's Hospital, Inc. Boston Massachusetts
United States Bronx Veterans Affairs Medical Center Bronx New York
United States Tryon Medical Group Charlotte North Carolina
United States Jesse Brown VAMC Department of Surgery Chicago Illinois
United States Northwestern University Chicago Illinois
United States Rush University Medical Center Chicago Illinois
United States The University Of Chicago Medicine Chicago Illinois
United States University of IL Chicago Chicago Illinois
United States CTI Clinical Trial and Consulting Services Cincinnati Ohio
United States Synexus Clinical Research US Inc Cincinnati Ohio
United States Velocity Clinical Research Cincinnati Ohio
United States Rapid Medical Research Cleveland Ohio
United States VA Medical Center Columbia South Carolina
United States Synexus Clinical Research US Inc Columbus Ohio
United States Corvallis Clinic PC Corvallis Oregon
United States AIDS Arms Incorporated Trinity Health and Wellness Center Dallas Texas
United States Baylor Scott & White Research Institute Dallas Texas
United States North Texas Infectious Diseases Consultants Dallas Texas
United States Synexus Clinical Research US Inc Dallas Texas
United States Atlanta VA Medical Center Decatur Georgia
United States The Hope Clinic at Emory University Decatur Georgia
United States Avail Clinical Research, LLC DeLand Florida
United States Rocky Mountain Regional VA Medical Center Denver Colorado
United States Henry Ford Health System Detroit Michigan
United States Meridian Clinical Research, LLC Endwell New York
United States Carolina Institute for Clinical Research Fayetteville North Carolina
United States North Florida South Georgia Veteran Health System Gainesville Florida
United States Synexus Clinical Research US Inc Glendale Arizona
United States Cherry Street Services, Inc. Grand Rapids Michigan
United States Velocity Clinical Research, Hallandale Beach Hallandale Beach Florida
United States Research Centers of America, LLC Hollywood Florida
United States Gordon Crofoot, MD Houston Texas
United States Texas Center for Drug Development Inc Houston Texas
United States The University of Texas Health Science Center at Houston Houston Texas
United States Optimal Research Huntsville Alabama
United States University of Mississippi Medical Center Jackson Mississippi
United States The Center For Pharmaceutical Research Kansas City Missouri
United States Clinical Research Center of Nevada Las Vegas Nevada
United States Clinical Research Consortium, an AMR company Las Vegas Nevada
United States Johnson County Clin-Trials Lenexa Kansas
United States Central Kentucky Research Associates, Inc. Lexington Kentucky
United States University of Kentucky Lexington Kentucky
United States Central Arkansas Veterans Healthcare System Little Rock Arkansas
United States University of Arkansas for Medical Sciences Little Rock Arkansas
United States Ark Clinical Research Long Beach California
United States Anthony Mills Medical, Inc Los Angeles California
United States University of Louisville Louisville Kentucky
United States Clinical Research Institute of Southern Oregon, P.C. Medford Oregon
United States St Jude Children's Research Hospital Memphis Tennessee
United States Benchmark Research Metairie Louisiana
United States Clinical Trials Management, LLC Metairie Louisiana
United States Suncoast Research Group Miami Florida
United States University of Miami - Miller School of Medicine Miami Florida
United States Abbott Northwestern Hospital Clinic Minneapolis Minnesota
United States Coastal Carolina Research Center Mount Pleasant South Carolina
United States PMG Research of Charleston, LLC Mount Pleasant South Carolina
United States Synexus Clinical Research US Inc Murray Utah
United States Vanderbilt University Medical Center Nashville Tennessee
United States Rutgers Robert Wood Johnson Medical School New Brunswick New Jersey
United States New Orleans Adolescent Trials Unit CRS New Orleans Louisiana
United States Ochsner Clinic Foundation New Orleans Louisiana
United States Southeast Louisiana Veterans Health Care Center New Orleans Louisiana
United States Harlem Hospital Center New York New York
United States Icahn School of Medicine at Mount Sinai New York New York
United States New York Blood Center New York New York
United States Saint Michaels Medical Center Newark New Jersey
United States Advent Health Orlando Orlando Florida
United States Orlando Immunology Center Orlando Florida
United States Synexus Clinical Research US Inc Orlando Florida
United States Stanford University Medical Center Palo Alto California
United States Optimal Research Peoria Illinois
United States MediSync Clinical Research Petal Mississippi
United States Temple University Hospital Philadelphia Pennsylvania
United States University of Pennsylvania Philadelphia Pennsylvania
United States Central Phoenix Medical Clinic Phoenix Arizona
United States VA Medical Center Phoenix Arizona
United States Synexus Clinical Research US Inc Pinellas Park Florida
United States University of Pittsburgh Pittsburgh Pennsylvania
United States Oregon Health And Science University Portland Oregon
United States Durham VAMC Raleigh North Carolina
United States Wake Research Associates Raleigh North Carolina
United States VA Sierra Nevada Health Care System Reno Nevada
United States Rochester Clinical Research, Inc Rochester New York
United States Meridian Clinical Research, LLC Rockville Maryland
United States Optimal Research Rockville Maryland
United States Saint Louis University Saint Louis Missouri
United States Synexus Clinical Research US Inc Saint Louis Missouri
United States Washington University School of Medicine Saint Louis Missouri
United States University of Utah Salt Lake City Utah
United States Clinical Trials of Texas, Inc San Antonio Texas
United States Synexus Clinical Research US Inc San Antonio Texas
United States UCSD Antiviral Research Center AVRC San Diego California
United States Wr-McCr, Llc San Diego California
United States VA Medical Center San Francisco California
United States Kaiser Permanente Washington Health Research Institute Seattle Washington
United States Spartanburg Medical Research Spartanburg South Carolina
United States James A Haley VA Hospital GNS Tampa Florida
United States Synexus Clinical Research US Inc The Villages Florida
United States Quality of Life Medical & Research Center, LLC Tucson Arizona
United States Synexus Clinical Research US Inc Tucson Arizona
United States Buynak Clinical Research Valparaiso Indiana
United States Advanced Clinical Research West Jordan Utah
United States Wake Forest Baptist Medical Center Winston-Salem North Carolina

Sponsors (1)

Lead Sponsor Collaborator
Janssen Vaccines & Prevention B.V.

Countries where clinical trial is conducted

United States,  Argentina,  Brazil,  Chile,  Colombia,  Mexico,  Peru,  South Africa, 

Outcome

Type Measure Description Time frame Safety issue
Primary Number of Participants With First Occurrence of Molecularly Confirmed Moderate to Severe/Critical Coronavirus Disease (COVID-19) With Seronegative Status With Onset at Least 14 Days After Double-blind Vaccination on Day 1 (Day 15): Double-blind Phase Molecularly confirmed moderate to severe/critical COVID-19 was defined as a severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) positive reverse transcription/polymerase chain reaction (RT-PCR) or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample. Moderate included one sign or symptom such as respiratory rate >= 20 breaths per minute and symptoms such as shortness of breath or two signs or symptoms such as heart rate >= 90 beats per minute (beats/minute) and symptoms such as cough from a list of signs and symptoms and severe/critical included one of the following signs and symptoms: respiratory rate >=30 breaths/minute, heart rate >=125 beats/minute, oxygen saturation (SpO2) <= 93% on room air at sea level respiratory failure, evidence of shock, significant acute renal, hepatic, or neurologic dysfunction, admission to the ICU, death defined as per FDA guidance. From 14 days after double-blind vaccination on Day 1 (Day 15) up to Month 6
Primary Number of Participants With First Occurrence of Molecularly Confirmed Moderate to Severe/Critical COVID-19 With Seronegative Status With Onset at Least 28 Days After Double-blind Vaccination on Day 1 (Day 29): Double-blind Phase Molecularly confirmed moderate to severe/critical COVID-19 was defined as a SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample. Moderate included one sign or symptom such as respiratory rate >=20 breaths per minute and symptoms such as shortness of breath or two signs or symptoms such as heart rate >= 90 beats/minute and symptoms such as cough from a list of signs and symptoms and severe/critical included one of the following signs and symptoms: respiratory rate >=30 breaths/minute, heart rate >=125 beats/minute, SpO2 less than or equal to (<=) 93 percent (%) on room air at sea level respiratory failure, evidence of shock, significant acute renal, hepatic, or neurologic dysfunction, admission to the Intensive Care Unit (ICU), death defined as per Food and Drug Administration (FDA) guidance. From 28 days after double-blind vaccination on Day 1 (Day 29) up to Month 6
Primary Number of Participants With Solicited Local Adverse Events (AEs) Up to 7 Days After Booster Vaccination (Open-label Booster Vaccination Phase) Participants who received the booster dose were asked to note in the e-Diary occurrences of injection site pain/tenderness, erythema, and swelling at the study vaccine injection site daily for 7 days post-booster vaccination (day of vaccination and the subsequent 7 days). Up to Day 372 (7 Days after booster vaccination on Day 365 [Year 1])
Primary Number of Participants With Solicited Systemic AEs Up to 7 Days After Booster Vaccination (Open-label Booster Vaccination Phase) Participants recorded the temperature in the e-Diary in the evening of the day of vaccination, and then daily for the next 7 days approximately at the same time each day. If more than 1 measurement was made on any given day, the highest temperature of that day was recorded in the e-Diary. Fever was defined as endogenous elevation of body temperature >= 38.0 degree Celsius or >=100.4-degree Fahrenheit, as recorded in at least 1 measurement. Participants also noted the signs and symptoms in the e-Diary on a daily basis for 7 days post-booster vaccination (day of vaccination and the subsequent 7 days), if feasible, for the following events: fatigue, headache, nausea, myalgia. Up to Day 372 (7 Days after booster vaccination on Day 365 [Year 1])
Primary Number of Participants With Unsolicited AEs Up to 28 Days After Booster Vaccination (Open-label Booster Vaccination Phase) Unsolicited AEs were all AEs for which the participant is not specifically questioned in the participant diary. Up to Day 393 (28 Days after booster vaccination on Day 365 [Year 1])
Secondary Number of Participants With First Occurrence of Molecularly Confirmed Severe/Critical COVID-19 With Seronegative Status With Onset at Least 14 Days After Double-blind Vaccination on Day 1 (Day 15): Double-blind Phase Molecularly confirmed severe/critical COVID-19 was defined as a SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample and one of the following signs and symptoms: respiratory rate >=30 breaths/minute, heart rate >=125 beats/minute,SpO2 <=93% on room air at sea level respiratory failure, evidence of shock, significant acute renal, hepatic, or neurologic dysfunction, admission to the ICU, death defined as per FDA guidance. Seronegative is defined as N-serology seronegative at the time of boosting or at the Year 1 visit if not boosted. From 14 days after double-blind vaccination on Day 1 (Day 15) up to Month 6
Secondary Number of Participants With First Occurrence of Molecularly Confirmed Severe/Critical COVID-19 With Seronegative Status With Onset at Least 28 Days After Double-blind Vaccination on Day 1 (Day 29): Double-blind Phase Severe/critical COVID-19 was defined as a SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample and one of the following signs and symptoms: respiratory rate >=30 breaths/minute, heart rate >=125 beats/minute,SpO2 <=93% on room air at sea level respiratory failure, evidence of shock, significant acute renal, hepatic, or neurologic dysfunction, admission to the ICU, death defined as per FDA guidance. From 28 days after double-blind vaccination on Day 1 (Day 29) up to Month 6
Secondary Number of Participants With First Occurrence of Molecularly Confirmed Moderate to Severe/Critical COVID-19 Regardless of Their Serostatus (Double Blind Phase) Molecularly confirmed moderate to severe/critical COVID-19 was defined as a SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample. Moderate included one sign or symptom such as respiratory rate >= 20 breaths per minute and symptoms such as shortness of breath or two signs or symptoms such as heart rate >= 90 beats per minute (beats/minute) and symptoms such as cough from a list of signs and symptoms and severe/critical included one of the following signs and symptoms: respiratory rate >=30 breaths/minute, heart rate >=125 beats/minute,SpO2 <=93% on room air at sea level respiratory failure, evidence of shock, significant acute renal, hepatic, or neurologic dysfunction, admission to the ICU, death defined as per FDA guidance. 1 day after double-blind vaccination on Day 1 (Day 2)
Secondary Number of Participants With First Occurrence of Molecularly Confirmed Moderate to Severe/Critical COVID-19 Regardless of Their Serostatus (Double Blind Phase) Molecularly confirmed moderate to severe/critical COVID-19 was defined as a SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample. Moderate included one sign or symptom such as respiratory rate >= 20 breaths per minute and symptoms such as shortness of breath or two signs or symptoms such as heart rate >= 90 beats per minute (beats/minute) and symptoms such as cough from a list of signs and symptoms and severe/critical included one of the following signs and symptoms: respiratory rate >=30 breaths/minute, heart rate >=125 beats/minute,SpO2 <=93% on room air at sea level respiratory failure, evidence of shock, significant acute renal, hepatic, or neurologic dysfunction, admission to the ICU, death defined as per FDA guidance. 14 days after double-blind vaccination on Day 1 (Day 15)
Secondary Number of Participants With First Occurrence of Molecularly Confirmed Moderate to Severe/Critical COVID-19 Regardless of Their Serostatus (Double Blind Phase) Molecularly confirmed moderate to severe/critical COVID-19 was defined as a SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample. Moderate included one sign or symptom such as respiratory rate >= 20 breaths per minute and symptoms such as shortness of breath or two signs or symptoms such as heart rate >= 90 beats per minute (beats/minute) and symptoms such as cough from a list of signs and symptoms and severe/critical included one of the following signs and symptoms: respiratory rate >=30 breaths/minute, heart rate >=125 beats/minute,SpO2 <=93% on room air at sea level respiratory failure, evidence of shock, significant acute renal, hepatic, or neurologic dysfunction, admission to the ICU, death defined as per FDA guidance. 28 days after double-blind vaccination on Day 1 (Day 29)
Secondary Number of Participants With First Occurrence of COVID-19 Requiring Medical Intervention (Double Blind Phase) Number of participants with first occurrence of COVID-19 requiring medical intervention (such as a composite endpoint of hospitalization, ICU admission, mechanical ventilation, and extracorporeal membrane oxygenation [ECMO], linked to objective measures such as decreased oxygenation, X-ray or computed tomography [CT] findings) or linked to any molecularly confirmed, COVID-19 at least 14 days post vaccination were reported. 14 days after double-blind vaccination on Day 1 (Day 15)
Secondary Number of Participants With First Occurrence of COVID-19 Requiring Medical Intervention (Double Blind Phase) Number of participants with first occurrence of COVID-19 requiring medical intervention (such as a composite endpoint of hospitalization, ICU admission, mechanical ventilation, and ECMO, linked to objective measures such as decreased oxygenation, X-ray or CT findings) or linked to any molecularly confirmed, COVID-19 at least 28 days post vaccination were reported. 28 Days after double-blind vaccination on Day 1 (Day 29)
Secondary Area Under the Curve (AUC) of SARS-CoV-2 Viral Load as Assessed by Quantitative Reverse-Transcriptase Polymerase Chain Reaction (RT-PCR) in Participants With Molecularly Confirmed, Moderate to Severe/Critical COVID-19 (Double Blind Phase) AUC of SARS-CoV-2 Viral Load was assessed in confirmed COVID-19 cases using RT-PCR. Nasal swabs were used to detect and/or quantify SARS-CoV-2. From Day 15 to end of the COVID-19 episode (Day 189)
Secondary Number of Participants With First Occurrence of Molecularly Confirmed Mild COVID-19 (Double Blind Phase Molecularly confirmed mild Covid-19 was defined as a SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample and one of the following signs and symptoms: fever (>=38°C or >=100.4°F), sore throat, malaise (loss of appetite, generally unwell, fatigue, physical weakness), headache, muscle pain (myalgia), gastrointestinal symptoms, cough, chest congestion, runny nose, wheezing, skin rash, eye irritation or discharge, chills, new or changing olfactory or taste disorders, red or bruised looking feet or toes, or shaking chills or rigors. 14 Days after double-blind vaccination on Day1 (Day 15)
Secondary Number of Participants With First Occurrence of Molecularly Confirmed Mild COVID-19 (Double Blind Phase) Molecularly confirmed mild Covid-19 was defined as a SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample and one of the following signs and symptoms: fever (>=38°C or >=100.4°F), sore throat, malaise (loss of appetite, generally unwell, fatigue, physical weakness), headache, muscle pain (myalgia), gastrointestinal symptoms, cough, chest congestion, runny nose, wheezing, skin rash, eye irritation or discharge, chills, new or changing olfactory or taste disorders, red or bruised looking feet or toes, or shaking chills or rigors. 28 Days after double-blind vaccination on Day 1 (Day 29)
Secondary Number of Participants With First Occurrence of Molecularly Confirmed COVID-19 Defined by the US Food and Drug Administration (FDA) Harmonized Case Definition (Double Blind Phase) Molecularly confirmed COVID-19 was defined as a positive SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample; and COVID-19 symptoms consistent with those defined by the US FDA harmonized case definition at the time of finalization of the study protocol: fever or chills, cough, shortness of breath or difficulty breathing, fatigue, muscle or body aches, headache, new loss of taste or smell, sore throat, congestion or runny nose, nausea or vomiting, diarrhea. 14 Days after double-blind vaccination on Day 1 (Day 15)
Secondary Number of Participants With First Occurrence of Molecularly Confirmed COVID-19 Defined by the US Food and Drug Administration (FDA) Harmonized Case Definition (Double Blind Phase) Molecularly confirmed COVID-19 was defined as a positive SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample; and COVID-19 symptoms consistent with those defined by the US FDA harmonized case definition at the time of finalization of the study protocol: fever or chills, cough, shortness of breath or difficulty breathing, fatigue, muscle or body aches, headache, new loss of taste or smell, sore throat, congestion or runny nose, nausea or vomiting, diarrhea. 28 Days after double-blind vaccination on Day 1 (Day 29)
Secondary Number of Participants With Burden of Disease (BOD) Based on First Occurrence of Molecularly Confirmed Symptomatic COVID-19 (Double Blind Phase) BOD is a weighted version of the mild, moderate, and severe/critical vaccine efficacies and was evaluated based on the first occurrence of molecularly confirmed COVID-19, including mild, moderate or severe/critical COVID-19 case. 14 Days after double-blind vaccination on Day 1 (Day 15)
Secondary Number of Participants With BOD Based on First Occurrence of Molecularly Confirmed Symptomatic COVID-19 (Double Blind Phase) BOD is a weighted version of the mild, moderate, and severe/critical vaccine efficacies and was evaluated based on the first occurrence of molecularly confirmed COVID-19, including mild, moderate or severe/critical COVID-19 case. 28 Days after double-blind vaccination on Day 1 (Day 29)
Secondary Number of Participants With SARS-CoV-2 Seroconversion Based on Antibodies to N Protein Using ELISA and/or SARS-CoV-2 Immunoglobulin Assay (Double Blind Phase) Number of participants with SARS-CoV-2 seroconversion based on antibodies to nucleocapsid (N) protein using enzyme-linked immunosorbent assay (ELISA) and/or SARS-CoV- 2 immunoglobulin assay that is dependent on the SARS-CoV-2 N protein was reported. From Day 29 until end of double-blind phase at Month 6
Secondary Number of Participants With Asymptomatic Infection Detected by RT-PCR at the Time of the Month 6/Unblinding Visit (Double Blind Phase) Number of participants with asymptomatic infection detected by RT-PCR at the time of the Month 6/unblinding visit were reported. Month 6
Secondary Number of Participants With First Occurrence of SARS-CoV-2 Infection (Serologically and/or Molecularly Confirmed) (Double Blind Phase) Number of participants with first occurrence of SARS-CoV-2 infection (serologically and/or molecularly confirmed) were reported. 28 days after double-blind vaccination on Day 1 (Day 29)
Secondary Number of Participants With First Occurrence of Molecularly Confirmed, Moderate to Severe/Critical COVID-19 for Seronegative Participants (Double Blind Phase) Molecularly confirmed moderate to severe/critical COVID-19 was defined as a SARS-CoV-2 positive RT-PCR or molecular test result from any available respiratory tract sample (example, nasal swab sample, sputum sample, throat swab sample, saliva sample) or other sample. Moderate included one sign or symptom such as respiratory rate >= 20 breaths per minute and symptoms such as shortness of breath or two signs or symptoms such as heart rate >= 90 beats per minute (beats/minute) and symptoms such as cough from a list of signs and symptoms and severe/critical included one of the following signs and symptoms: respiratory rate >=30 breaths/minute, heart rate >=125 beats/minute,SpO2 <=93% on room air at sea level respiratory failure, evidence of shock, significant acute renal, hepatic, or neurologic dysfunction, admission to the ICU, death defined as per FDA guidance. Seronegative is defined as N-serology seronegative at the time of boosting or at the Year 1 visit if not boosted. 1 day after double-blind vaccination on Day 1 (Day 2)
Secondary Number of Participants With Serious Adverse Events (SAEs) (Double Blind Phase) An AE is any untoward medical occurrence in a participant participating in a clinical study that does not necessarily have a causal relationship with the pharmaceutical/biological agent under study. SAE is any untoward medical occurrence that at any dose may result in death, is life-threatening, requires inpatient hospitalization or prolongation of existing hospitalization, results in persistent or significant disability/incapacity, is a congenital anomaly/birth defect, is a suspected transmission of any infectious agent via a medicinal product. Baseline (Day 1) up to 35 weeks
Secondary Number of Participants With Adverse Events of Special Interest (AESI) (Double Blind Phase) Number of participants with AESIs were reported. AESIs are significant AEs that are judged to be of special interest because of clinical importance, known or suspected class effects, or based on nonclinical signals. Thrombosis with Thrombocytopenia Syndrome (TTS), a syndrome characterized by a combination of both a thrombotic event and thrombocytopenia, is considered to be an AESI in this study. A suspected TTS case is defined as: Thrombotic events: suspected deep vessel venous or arterial thrombotic events; Thrombocytopenia, defined as platelet count below 150,000/micro liter. Baseline (Day 1) up to 35 weeks
Secondary Number of Participants With Medically-Attended Adverse Events (MAAEs) (Double Blind Phase) An AE is any untoward medical occurrence in a participant participating in a clinical study that does not necessarily have a causal relationship with the pharmaceutical/biological agent under study. MAAEs were defined as AEs with medically-attended visits including hospital, emergency room, urgent care clinic, or other visits to or from medical personnel for any reason. Up to 6 months after double-blind vaccination on Day 1 (up to 6 months)
Secondary Number of Participants With MAAEs Leading to Study Discontinuation (Double Blind Phase) MAAEs were defined as AEs with medically-attended visits including hospital, emergency room, urgent care clinic, or other visits to or from medical personnel for any reason. Routine study visits were not considered medically-attended visits. New onset of chronic diseases was collected as part of the MAAEs. Up to 35 weeks
Secondary Number of Participants With Solicited Local Adverse Events (AEs) During 7 Days Following Vaccination (Double Blind Phase) An AE is any untoward medical occurrence in a participant participating in a clinical study that does not necessarily have a causal relationship with the pharmaceutical/biological agent under study. Participants who were enrolled in safety subset were asked to note in the e-Diary occurrences of injection site pain/tenderness, erythema, and swelling at the study vaccine injection site daily for 7 days post-vaccination (day of vaccination and the subsequent 7 days). Up to Day 8 (7 Days after double-blind vaccination on Day 1)
Secondary Number of Participants With Solicited Systemic AEs During 7 Days Following Vaccination (Double Blind Phase) An AE is any untoward medical occurrence in a participant participating in a clinical study that does not necessarily have a causal relationship with pharmaceutical/biological agent under study. Participants who were enrolled in safety subset were instructed on how to record daily temperature using a thermometer provided for home use. Participants recorded the temperature in the e-Diary in the evening of the day of vaccination, and then daily for the next 7 days approximately at the same time each day. If more than 1 measurement was made on any given day, the highest temperature of that day was recorded in the e-Diary. Fever was defined as endogenous elevation of body temperature >= 38.0 degree Celsius or >=100.4-degree Fahrenheit, as recorded in at least 1 measurement. Participants also noted the signs and symptoms in the e-Diary on a daily basis for 7 days post vaccination (day of vaccination and the subsequent 7 days), for the following events: fatigue, headache, nausea, myalgia. Up to Day 8 (7 Days after double-blind vaccination on Day 1)
Secondary Number of Participants With Unsolicited AEs During 28 Days Post-vaccination (Double Blind Phase) An AE is any untoward medical occurrence in a participant participating in a clinical study that does not necessarily have a causal relationship with the pharmaceutical/biological agent under study. Unsolicited AEs were all AEs for which the participant is not specifically questioned in the participant diary. Up to Day 29 (28 Days after double-blind vaccination on Day 1)
Secondary Binding Antibodies to SARS-CoV-2 S Protein Assessed by ELISA (Double Blind Phase) Binding antibodies to SARS-CoV-2 S protein as assessed by enzyme-linked immunosorbent assay (ELISA) to measure humoral immune response was reported. The lower limit of quantification (LLOQ) and upper limit of quantification (ULOQ) were 50.3 EU/mL and 58,158.10 EU/mL, respectively. A sample was considered positive if the value was strictly greater than the LLOQ (>LLOQ). Baseline (Day 1), Day 29, and Day 71
Secondary Number of Participants With Antibody Titers to Ad26.COV2.S (Booster Phase) Number of participants with antibody titers to Ad26.COV2.S to measure immune response were reported. 28 days after booster vaccination on Day 365 (up to Day 393)
Secondary Number of Participants With Binding Antibodies to SARS- CoV-2S Protein as Measured by ELISA (Booster Phase) Number of participants with binding antibodies to SARS- CoV-2S protein as measured by ELISA was reported. 29 days after booster vaccination on Day 365 (Day 394)