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Clinical Trial Details — Status: Terminated

Administrative data

NCT number NCT03656510
Other study ID # CR108520
Secondary ID 2016-003642-9353
Status Terminated
Phase Phase 2
First received
Last updated
Start date November 29, 2018
Est. completion date April 18, 2022

Study information

Verified date September 2023
Source Janssen Research & Development, LLC
Contact n/a
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

The purpose of this study is to evaluate the antiviral activity, clinical outcomes, safety, tolerability, and pharmacokinetic/pharmacodynamic relationships of different oral dose levels of JNJ-53718678 in children greater than or equal to 28 days and less than or equal to 3 years of age with respiratory syncytial virus (RSV) disease (hospitalized participants [Cohort 1] or outpatients [Cohort 2]).


Description:

JNJ-53718678 is an investigational respiratory syncytial virus (RSV) specific fusion inhibitor and is under development for the treatment of RSV infection, which results in an upper and/or lower respiratory tract illness. The primary hypothesis of this study is that JNJ-53718678 has antiviral activity against RSV (that is, results in a decrease in RSV nasal viral load from immediately prior to first dose of study drug until Day 5). This will be assessed by a positive dose-response relationship of JNJ-53718678 compared to placebo. Besides the RSV nasal viral load through day 5, other timepoints will also be evaluated as well as other nasal viral load related parameters. In addition, the evolution of signs and symptoms of RSV disease will be evaluated. Participants' safety will be monitored throughout the study by evaluating the occurrence and severity of adverse events and by laboratory and electrocardiogram measurements. Study participants will be identified when they are hospitalized or expected to be hospitalized within 24 hours after presentation to the hospital (Cohort 1) or present for medical care as outpatients (Cohort 2) with symptoms of an acute respiratory illness supporting a diagnosis of RSV infection. Eligible participants will be randomized 1:1:1 to receive either a low or a high dose of JNJ 53718678 or placebo and will be receiving study treatment for 7 days. They will be followed up for 3 weeks after the last dose. The total study duration for each participant will be approximately 29 days.


Recruitment information / eligibility

Status Terminated
Enrollment 246
Est. completion date April 18, 2022
Est. primary completion date April 18, 2022
Accepts healthy volunteers No
Gender All
Age group 28 Days to 3 Years
Eligibility Inclusion Criteria: - Informed consent form (ICF) must be given - Laboratory diagnosis of respiratory syncytial virus (RSV) infection - The participant has an acute respiratory illness - The time of onset of RSV symptoms to the anticipated time of randomization must be less than or equal to (<=) 5 days - Except for the RSV-related illness, the Participant must be medically stable in case of allowed co-morbid conditions - The participant must have been assessed per local public health practice and considered not to have Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection during this respiratory infection Exclusion Criteria: - The participant is less than (<) 3 months postnatal age at screening and was born prematurely (i.e, <37 weeks and 0 days of gestation) OR if the participant weighs <2.4 kilogram (kg) or greater than (>) 16.8 kg - Participant is considered by the investigator to be immunocompromised within the past 12 months - Participant unwilling or unable to undergo mid-turbinate nasal swab procedures - Participant is receiving chronic home oxygen therapy at screening - Participant has other clinically significant abnormal electrocardiogram (ECG) findings not consistent with the present risk factor for severe RSV disease (if applicable) in the study population, as judged by the investigator based on the machine read ECG results at screening - The participant has a QTcF interval greater than (>)450 millisecond (ms) per the machine read (mean of triplicate) parameter result confirmed by repeat triplicate ECG recording during screening

Study Design


Related Conditions & MeSH terms


Intervention

Drug:
JNJ-53718678
Participants will receive JNJ-53718678 (high dose or low dose) orally twice daily for 7 days.
Placebo
Participants will receive matching placebo (high volume or low volume) orally twice daily for 7 days.

Locations

Country Name City State
Argentina Hospital Italiano Regional Del Sur Bahía Blanca
Argentina Hospital Central Militar Cirujano Mayor Dr Cosme Argerich Buenos Aires
Argentina CEMIC (Centro de Educación Médica e Investigaciones Clínicas) City of Buenos Aires
Argentina Hospital Pedro de Elizalde City of Buenos Aires
Argentina Fundación Respirar Ciudad Autonoma de Buenos Aires
Argentina Hospital Italiano de La Plata Ciudad De La Plata
Argentina Hospital Universitario Austral Pilar
Argentina Clinica Mayo de UMCB San Miguel de Tucuman
Argentina Hospital del Niño Jesús San Miguel de Tucumán
Belgium ULB Hôpital Erasme Anderlecht
Belgium UZ Antwerpen Edegem
Belgium C.H.R. Citadelle Liège
Brazil Universidade Federal De Minas Gerais - Hospital das Clínicas Belo Horizonte
Brazil Fundacao para o Desenvolvimento Medico Hospitalar (UNESP Botucatu) Botucatu
Brazil Sociedade Campineira de Educacao e Instrucao - Hospital e Maternidade Celso Pierro Campinas
Brazil Nucleo de Pesquisa do Hospital Pequeno Princípe Curitiba
Brazil Secretaria da Saude do Estado do Ceara - Hospital Doutor Carlos Alberto Studart Gomes Fortaleza
Brazil Centro de Estudos e Pesquisas em Moléstias Infecciosas - CEPCLIN Natal
Brazil Associacao Hospitalar Beneficente Sao Vicente de Paulo - Hospital Sao Vicente de Paulo Passo Fundo
Brazil Associacao Hospitalar Moinhos de Vento Porto Alegre
Brazil Irmandade Santa Casa de Misericordia de Porto Alegre Porto Alegre
Brazil Fundacao Faculdade Regional de Medicina de Sao Jose do Rio Preto - Hospital de Base Sao Jose do Rio Preto
Brazil Fundacao Jose Luiz Egydio Setubal Sao Paulo
Brazil CMPC - Consultoria Médica e Pesquisa Clínica Sorocaba
Brazil Santa Casa de Misericórdia de Votuporanga Votuporanga
Bulgaria UMHAT 'Dr. Georgi Stranski', EAD Pleven
Bulgaria UMHAT 'Sveti Georgi'-Plovdiv Plovdiv
Bulgaria UMHAT 'Kanev' EAD Ruse
Bulgaria Medical Center-1-Sevlievo EOOD Sevlievo
Bulgaria Acibadem City Clinic Tokuda Hospital Sofia
Bulgaria DCC 'Sv. Vrach and Sv. Sv. Kuzma and Damyan', OOD Sofia
Bulgaria SHATCD 'Prof. Ivan Mitev' EAD Sofia
Bulgaria UMHAT 'Aleksandrovska' EAD Sofia
France CHU de Caen Caen
France Hopital Antoine Beclere CLAMART Cedex
France CHU de Montpellier - Arnaud de Villeneuve Montpellier
France CHU de Nantes hôtel-Dieu Nantes
France Hopitaux pediatriques CHU Lenval Nice
France Hôpital Necker-Enfants Malades Paris
France Hopital Charles Nicolle Rouen
Germany Kinderarztpraxis Bramsche Bramsche
Germany Hürthpark Kinder & Jugendärzte Hürth
Germany Praxiszentrum Triftplatz Schönau am Königssee
Germany Kinderärztliche Gemeinschaftspraxis Wolfsburg
Germany Universitätsklinikum Würzburg Würzburg
Hungary Dél-pesti Centrumkórház - Országos Hematológiai és Infektológiai Intézet, Szent László Telephely Budapest
Hungary Semmelweis Egyetem, II. sz. Gyermekgyógyászati Klinika Budapest
Hungary Debreceni Egyetem Klinikai Kozpont Debrecen
Hungary Debreceni Egyetem Klinikai Központ,Infektológiai Klinika Debrecen
Hungary Futurenest Klinikai Kutato Kft. Miskolc
Hungary Kanizsai Dorottya Kórház Nagykanizsa
Hungary Szegedi Tudomanyegyetem Szeged
Hungary Fejer Varmegyei Szent Gyorgy Egyetemi Oktatokorhaz Székesfehérvár
Hungary Csolnoky Ferenc Korhaz Veszprém
Italy A.O.U Sant'Orsola-Malpighi Bologna
Italy Università degli Studi di Milano, Fondazione IRCCS Ca' Granda Ospedale Maggiore Policlinico Milan
Italy ASST Fatebenefratelli Sacco / Ospedale dei Bambini V. Buzzi Milano
Italy Dipartimento di Pediatria dell'Ospedale Luigi Sacco Milano
Italy Azienda Ospedaliera di Padova Padova
Italy Department of Pediatrics University of Pavia, Policlinico San Matteo Pavia
Italy Ospedale degli Infermi Ponderano
Japan Hosaka Kodomo Clinic Bunkyo-Ku
Japan Kobayashi Pediatric Clinic Fujieda
Japan Fukui-ken Saiseikai Hospital Fukui City
Japan Fukuyama City Hospital Fukuyama
Japan National Hospital Organization Fukuyama Medical Center Fukuyama
Japan Tanabe Pediatrics Clinic Hatsukaichi
Japan Kagoshima Children's Hospital Hioki
Japan National Hospital Organization Hirosaki General Medical Center Hirosaki
Japan Shirao Clinic of Pediatrics and Pediatric Allergy Hiroshima
Japan National Hospital Organization Kanazawa Medical Center Kanazawa
Japan Daido Hospital Nagoya
Japan Kojunkai Daido Clinic Nagoya
Japan National Hospital Organization Beppu Medical Center Oita
Japan Momotaro Clinic Okayama City
Japan National Hospital Organization Saitama National Hospital Saitama
Japan KKR Sapporo Medical Center Sapporo
Japan Tsuda Pediatrics Clinic Setagaya-ku
Japan INAMI Pediatric clinic Tokyo
Japan Okawa Children & Family Clinic Tokyo
Korea, Republic of The Catholic University of Korea, Incheon St. Mary's Hospital Incheon
Korea, Republic of Inje University Sanggye Paik Hospital Seoul
Korea, Republic of Kangbuk Samsung Hospital Seoul
Korea, Republic of Nowon Eulji Medical Center, Eulji University Seoul
Malaysia Hospital Selayang Batu Caves
Malaysia Hospital Miri Miri
Malaysia Hospital Tuanku Fauziah Pusat Bandar Kangar
Malaysia Hospital Sibu Sibu
Mexico RM Pharma Specialists Benito Juarez
Mexico Hospital Infantil de Mexico Federico Gomez Ciudad De Mexico
Mexico Instituto Nacional de Pediatría Coyoacan
Mexico Hospital Civil de Guadalajara Guadalajara
Mexico Hospital Universitario 'Dr. Jose Eleuterio Gonzalez' Monterrey
Poland Osrodek Badan Klinicznych In-Vivo Sp. z o.o. Bydgoszcz
Poland Zespol Opieki Zdrowotnej w Debicy, Oddzial Dzieciecy Debica
Poland Krakowski Szpital Specjalistyczny im. Jana Pawla II, Oddzial Pediatrii i Neurologii Dzieciecej Krakow
Poland NZOZ Salmed Leczna
Poland Instytut Gruzlicy i Chorob Pluc Oddzial Terenowy im. Rudnikow w Rabce-Zdroj, Oddzial Pulmonologii Rabka-Zdroj
Poland ALERGO-MED Specjalistyczna Przychodnia Lekarska Sp. z o.o. Tarnow
Poland Szpital im. Swietej Jadwigi Slaskiej, Oddzial Pediatryczny z Pododdzialem Niemowlecym Trzebnica
Russian Federation Infectious Clinical Hospital #1 Of The Moscow City Health Department Moscow
Russian Federation OOO MDP-Medical Group Odintsovo
Russian Federation City Children Clinical Outpatient Clinic #5 Perm
Russian Federation Children Outpatient Clinic 45 Of Nevskiy Region St. Petersburg
Russian Federation LLC Kurator St. Petersburg
Russian Federation LLC Piterclini?a St. Petersburg
Russian Federation OOO 'Arsvite North-West' St. Petersburg
Russian Federation OOO 'Medical Technologies' St. Petersburg
Russian Federation Siberian State Medical University Tomsk
Russian Federation Bashkir State Medical University Ufa
Russian Federation Yaroslavl State Medical University Based On Children Polyclinics #5 Yaroslavl
South Africa Tygrberg Hospital Bellville
South Africa Josha Research Bloemfontein
South Africa VX Pharma Pretoria
South Africa Two Military Hospital Wynberg
Spain Hosp. Univ. Germans Trias I Pujol Badalona
Spain Hosp. Del Mar Barcelona
Spain Hosp. Univ. de Burgos Burgos
Spain Hosp. Univ. de Getafe Getafe
Spain Hosp. Univ. 12 de Octubre Madrid
Spain Hosp. Univ. Fund. Jimenez Diaz Madrid
Spain Hosp. Univ. La Paz Madrid
Spain Hosp. Univ. Pta. de Hierro Majadahonda Majadahonda
Spain Hosp. Regional Univ. de Malaga Malaga
Spain Hosp. Puerta Del Sur Mostoles
Spain Hosp. Quiron Madrid Pozuelo Pozuelo de Alarcon
Spain Hosp. Clinico Univ. de Salamanca Salamanca
Spain Hosp. Clinico Univ. de Santiago Santiago de Compostela
Sweden Barn- Och Ungdomsmedicin Malmö
Sweden Astrid Lindgrens barnsjukhus Solna Stockholm
Sweden Sachsska barn-och ungdomssjukhuset Stockholm
Taiwan Hsinchu MacKay Memorial Hospital Hsinchu
Taiwan Kaohsiung Chang Gung Memorial Hospital Kaohsiung
Taiwan Taichung Veterans General Hospital Taichung
Taiwan National Taiwan University Hospital Taipei
Taiwan Taipei Municipal Wanfang Hospital Taipei
Taiwan Chang Gung Memorial Hospital- Linkou Taoyuan City
Thailand Queen Sirikit National Institute of Child Health Bangkok
Thailand Siriraj Hospital Mahidol University Bangkok
Thailand Tropical Medicine Hospital, Mahidol University Bangkok
Thailand Chiang Mai University Chiang Mai
Thailand Research Institute for Health Sciences Chiang Mai
Thailand Srinagarind Hospital Khon Kaen
Turkey Cukurova University Medical Faculty Balcali Hospital Adana
Turkey Ankara Bilkent Sehir Hastanesi Ankara
Turkey Ankara University Medical Faculty Ankara
Turkey Gazi University Medical Faculty Ankara
Turkey Hacettepe University Medical Faculty Ankara
Turkey Istanbul University Istanbul Medical Faculty Istanbul
Turkey Ege University Medical Faculty Izmir
Turkey Saglik Bilimleri University Sariyer Hamidiye Etfal Training and Research Hospital Sariyer
Turkey Karadeniz Teknik University Medical Faculty Trabzon
United Kingdom Royal Devon & Exeter Hospital Exeter
United Kingdom Whipps Cross University Hospital London
United Kingdom The Adam Practice Poole
United States Children's Hospital Colorado Aurora Colorado
United States Elite Clinical Trials Blackfoot Idaho
United States Tufts Medical Center Boston Massachusetts
United States Craig A. Spiegel, MD Bridgeton Missouri
United States Ann & Robert H. Lurie Children's Hospital of Chicago Chicago Illinois
United States Madera Family Medical Group Madera California
United States West Virginia University Morgantown West Virginia
United States Saltzer Medical Group Nampa Idaho
United States Santiago Reyes, MD Oklahoma City Oklahoma
United States Children's Hospital of Richmond at VCU Richmond Virginia
United States Sanford Health Sioux Falls South Dakota
United States Coastal Pediatric Research Summerville South Carolina
United States SUNY Upstate Medical University - Upstate Golisano Children's Hospital (GCH) Syracuse New York
United States FOMAT Medical Research Ventura California

Sponsors (1)

Lead Sponsor Collaborator
Janssen Research & Development, LLC

Countries where clinical trial is conducted

United States,  Argentina,  Belgium,  Brazil,  Bulgaria,  France,  Germany,  Hungary,  Italy,  Japan,  Korea, Republic of,  Malaysia,  Mexico,  Poland,  Russian Federation,  South Africa,  Spain,  Sweden,  Taiwan,  Thailand,  Turkey,  United Kingdom, 

Outcome

Type Measure Description Time frame Safety issue
Primary Respiratory Syncytial Virus (RSV) Viral Load Area Under Curve (AUC) From Immediately Prior to First Dose of Study Drug (Baseline) Through Day 5 (AUC[Day 5]) RSV viral load AUC from immediately prior to first dose of study drug through Day 5 was determined. The RSV viral load was measured by quantitative reverse transcription polymerase chain reaction (qRT-PCR) assay in mid-turbinate nasal swab specimens. As planned, combined data for both the cohorts was collected, analyzed and reported for this outcome measure. Baseline through Day 5
Secondary RSV Viral Load Over Time RSV viral load actual values over time were measured by qRT-PCR in the nasal swab specimens collected at the clinic visits and at home. As planned, combined data for both the cohorts was collected, analyzed and reported for this outcome measure. Baseline, Days 3, 5, 8, 14, and 21
Secondary Change From Baseline in RSV Viral Load Over Time Change from baseline in RSV viral load over time was measured by qRT-PCR in the nasal swab specimens collected at the clinic visits and at home. As planned, combined data for both the cohorts was collected, analyzed and reported for this outcome measure. Baseline up to Days 3, 5, 8, 14, and 21
Secondary Least Squares (LS) Mean RSV Viral Load on Days 3, 8 and 14 LS mean RSV viral load on Days 3, 8, and 14 was reported. LS mean viral load (log10 copies/mL) was estimated per time point. The difference in RSV viral Load AUC (log10 copies*day/mL) from immediately prior to first dose of study drug (baseline) through Day 3, 8 and 14 was determined from the model estimating the LS Mean Viral Load per time point, and is presented in the statistical analysis. The RSV viral load was measured by qRT-PCR assay in mid-turbinate nasal swab specimens. As planned, combined data for both the cohorts was collected, and analyzed for this outcome measure at Days 3 and 8, however combined Cohort 1 and Cohort 2 data were not analyzed for this outcome measure at Day 14, due to the premature study termination. Baseline through Days 3, 8, and 14
Secondary Time to Undetectable RSV Viral Load Time to undetectable RSV viral load (as measured by qRT-PCR) was defined as the time in hours from first dose of study drug to first post-baseline timepoint at which the virus was undetectable and after which there were no more detectable virus assessments. As planned, combined data for both the cohorts was collected, analyzed and reported for this outcome measure. Up to Day 21
Secondary Percentage of Participants With Undetectable RSV Viral Load at Each Timepoint Throughout the Study Percentage of participants with undetectable RSV viral load (as measured by qRT-PCR) at each timepoint throughout the study was reported. As planned, combined data for both the cohorts were collected, analyzed and reported for this outcome measure. Baseline, Days 3, 5, 8, 14 and 21
Secondary Change From Baseline in Parent(s)/Caregiver(s) Pediatric RSV Electronic Severity and Outcomes Rating System (PRESORS) Scores PRESORS is a questionnaire recording presence and severity of signs and symptoms of RSV disease (fever, cough, sputum, wheezing, difficulty breathing, nasal congestion, and feeding issues). PRESORS overall RSV symptoms summary parameter consisted of 12-items, each item score ranges from 0 to 3. A summary score was derived (mean of the item scores) which also ranges from 0 to 3. The higher the score, the worse the symptom. Baseline up to Days 3, 5, 8, 14 and 21
Secondary Change From Baseline in Clinician PRESORS Score Change from baseline in clinician PRESORS scores (for concepts: activity level, sleep disturbance, breathing problems, retractions, tachypnea, feeding problem, cough, nasal secretions, wheezing, dehydration) was assessed. Clinician PRESORS is a questionnaire recording presence and severity of signs and symptoms of RSV disease and consisted of 10-items, each item score ranges from 0 to 3. Overall RSV symptoms summary parameter was derived (mean of the item scores) which also ranges from 0 to 3. The higher the score, the worse the symptom. Baseline, up to Days 3, 5, 8, 14 and 21
Secondary Time to Resolution of RSV Symptoms Based on PRESORS Caregiver (ObsRO) Time to resolution is defined as time from first dose of study drug until the first time of resolution of all RSV symptoms (breathing problems, retractions, tachypnea, breathing sounds, cough, tachycardia, nasal secretions, sleep disturbance, crying, illness behavior, feeding problems, and dehydration). Resolution occurs when all symptoms from the caregiver reported outcomes (ObsRO) are scored as none or mild (score of 0 or 1, respectively) for at least 24 hours. Up to Day 21
Secondary Time to Improvement on Overall Health Time to improvement based on general questions on overall health was assessed. Time from first dose of study drug until first time status of improvement of RSV symptoms reported as "very much improved" or "much improved" based on response to question 'Would you say the child's RSV symptoms have improved, are about the same or are worse than when the child entered the study'. Up to Day 21
Secondary Percentage of Participants by Status of RSV Symptoms Based on PRESORS Caregiver (ObsRO) General Question Over Time Percentage of participants by status of RSV symptoms based on PRESORS caregiver (ObsRO) general question over time was assessed. PRESORS is a questionnaire recording presence and severity of signs and symptoms of RSV disease (fever, cough, sputum, wheezing, difficulty breathing, nasal congestion, and feeding issues). Status of RSV symptoms was assessed by a question (how would you rate the child's RSV symptoms now?) of PRESORS questionnaire and responses were categorized as: 1) none, 2) very mild, 3) mild, 4) moderate, 5) severe, and 6) very severe. Baseline, Days 3, 5, 8, 14, and 21
Secondary Percentage of Participants by Health Status Assessment Based on PRESORS Caregiver (ObsRO) General Question Over Time Percentage of participants by health status assessment based on PRESORS caregiver (ObsRO) general question over time was assessed. PRESORS is a questionnaire recording presence and severity of signs and symptoms of RSV disease (fever, cough, sputum, wheezing, difficulty breathing, nasal congestion, and feeding issues). Health status was assessed by a question (how is the child's health now) of PRESORS questionnaire and responses were categorized as: 1) excellent, 2) very good, 3) good, 4) fair, 5) poor, and 6) very poor. Baseline, Days 3, 5, 8, 14, and 21
Secondary Percentage of Participants With Worsening or Improvement Status of RSV Disease Percentage of participants with worsening or improvement of RSV disease based on general questions of overall health was assessed. Improvement or worsening was assessed by a question 'Would you say the child's RSV symptoms have improved, are about the same or are worse than when the child entered the study' and responses were categorized as: 1) very much improved, 2) much improved, 3) a little improved, 4) about the same, 5) a little worse, 6) much worse, and 7) very much worse". Days 14 and 21
Secondary Percentage of Participants by Return to Pre-RSV Disease Health Status Assessment Based on PRESORS Caregiver (ObsRO) General Question Over Time Percentage of participants by return to pre-RSV disease health status assessment based on PRESORS caregiver (ObsRO) general question over time was assessed by a question (Has the child's health returned to normal [how it was before RSV?]) of PRESORS questionnaire and responses were categorized as: 1) No, and 2) Yes. PRESORS is a questionnaire recording presence and severity of signs and symptoms of RSV disease (fever, cough, sputum, wheezing, difficulty breathing, nasal congestion, and feeding issues). Below results are reported for category 'Yes'. Baseline, Days 3, 5, 8, 14, and 21
Secondary Respiratory Rate (RR) Over Time Respiratory rate (RR) was measured by the investigator over time. Baseline, Days 3, 5, 8, 14 and 21
Secondary Change From Baseline in Respiratory Rate Change from baseline in respiratory rate was derived based on the reported measurements of respiratory rate over time. The respiratory rate over time was reported by the investigator. Baseline to Days 3, 5, 8, 14 and 21
Secondary Heart Rate Over Time Heart rate was measured by the investigator over time. Baseline, Days 3, 5, 8, 14 and 21
Secondary Change From Baseline in Heart Rate Change from baseline in heart rate was assessed. Baseline to Days 3, 5, 8, 14 and 21
Secondary Body Temperature Over Time Body temperature was reported over time (either investigator or caregiver measured). Baseline, Days 3, 5, 8, 14 and 21
Secondary Change From Baseline in Body Temperature Change from baseline in body temperature (either investigator or caregiver measured) was assessed. Baseline to Days 3, 5, 8, 14 and 21
Secondary Peripheral Capillary Oxygen Saturation (SpO2) Over Time Peripheral capillary oxygen saturation was measured by the investigator over time. Baseline, Days 3, 5, 8, 14 and 21
Secondary Change From Baseline in Peripheral Capillary Oxygen Saturation (SpO2) Change from baseline in peripheral capillary oxygen saturation levels was derived based on reported values over time. Baseline to Days 3, 5, 8, 14, and 21
Secondary Percentage of Participants Who Required (re)Hospitalization During Treatment and Follow-up Percentage of participants who required (re)hospitalization during treatment and follow-up was assessed. Percentage of participants requiring re-hospitalization following the initial hospital discharge was assessed in Cohort 1 participants (hospitalized cohort) whilst percentage of participants requiring hospitalization after first dose of study drug was assessed in Cohort 2 participants (outpatient cohort). Up to Day 28
Secondary Cohort 1: Time to Return to Age-adjusted Normal Values for Vital Signs Time to return to age-adjusted normal values from first dose of study drug based on the reported vital signs (respiratory rate, heart rate, SpO2 >=92%, and SpO2 >=95%) values was assessed. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 28
Secondary Cohort 1: Time to Discharge From Hospital Time to discharge from hospital was derived from the reported discharge date/time and from first dose date/time. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 28
Secondary Cohort 1: Percentage of Participants Who Required Admission to the Intensive Care Unit (ICU) Percentage of participants who required admission to the ICU was assessed. This outcome measure was applicable for those participants that were not in ICU before first dose of study drug. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 21
Secondary Cohort 1: Duration of ICU Stay Duration of ICU stay was derived based on the reported admission/discharge date/time for ICU. Duration defined as total number of hours a participant was in ICU from first dose of study drug until study termination. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 21
Secondary Cohort 1: Time to Clinical Stability Evaluated by the Investigator Time to clinical stability was derived based on vital signs(SpO2 >= 92%, SpO2 >=95% on room air) assessments and supplementation end dates as collected. Time to clinical stability=time from initiation of study treatment until time at which following criteria were met: Time to return to age-adjusted normal value for otherwise healthy, pre-RSV infection status for participant with risk factor for severe RSV disease,no more oxygen supplementation in otherwise healthy participant, participant with risk factor for severe RSV disease and no more IV administered/nasogastric tube feeding/hydration supplementation in otherwise healthy participant or pre-RSV status of IV/nasogastric tube feeding/hydration in participant with risk factor for severe RSV disease. As per protocol and study design,this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 21
Secondary Cohort 1: Percentage of Participants Who Required Supplemental Oxygen Percentage of participants who required supplemental oxygen after first dose of study drug was reported. This parameter was only for participants that did not require oxygen supplementation before first dose of study drug. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 21
Secondary Cohort 1: Duration of Supplemental Oxygen Duration of supplemental oxygen was assessed. Duration was defined as total number of hours a participant used supplemental oxygen from first dose of study drug until study termination. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 28
Secondary Cohort 1: Percentage of Participants Who Required Non-invasive Mechanical Ventilation Support Percentage of participants who required non-invasive mechanical ventilation support (example: continuous positive airway pressure) after first dose of study drug was assessed. This parameter was only for participants who did not require non-invasive mechanical ventilation support before first dose of study drug. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 21
Secondary Cohort 1: Percentage of Participants Who Required Invasive Mechanical Ventilation Support Percentage of participants who required invasive mechanical ventilation support (example: endotracheal-mechanical ventilation) after first dose of study drug was assessed. This parameter was only for participants who did not require invasive mechanical ventilation support before first dose of study drug. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 21
Secondary Cohort 1: Percentage of Participants Who Required Non-invasive Non-mechanical Ventilation Support Percentage of participants who required non-invasive non-mechanical ventilation support (example: nasal cannula) after first dose of study drug was assessed. This parameter was only for participants who did not require non-invasive non-mechanical ventilation support before first dose of study drug. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 21
Secondary Cohort 1: Duration of Non-invasive Ventilation Support For the subset of participants who received non-invasive ventilation post dose, duration for non-invasive ventilation could not be derived by individual type as start/end dates and times were not collected in full to allow breakdown of duration derivation by ventilation type and only overall duration of oxygen supplementation (overall ventilation support) could be derived which is reported in the outcome measure "Duration of Supplemental Oxygen". As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure could only have been reported for Cohort 1. Up to Day 21
Secondary Cohort 1: Duration of Invasive Ventilation Support For the subset of participants who received invasive ventilation post dose, duration for invasive ventilation could not be derived by individual type as start/end dates and times were not collected in full to allow breakdown of duration derivation by ventilation type and only overall duration of oxygen supplementation (overall ventilation support) could be derived which is reported in the outcome measure "Duration of Supplemental Oxygen". As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure could only have been reported for Cohort 1. Up to Day 21
Secondary Cohort 1: Time to End of Supplemental Oxygen up to 72 Hours From First Hospital Discharge Time to end of supplemental oxygen up to 72 hours from first hospital discharge was assessed. Time to end of supplemental oxygen was defined as time (hours) from first dose of study drug to last end date/time of any oxygen supplementation received, but within 72 hours following first hospital discharge. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to end of supplemental oxygen including supplemental oxygen within 72 hours after first hospital discharge (up to Day 28)
Secondary Cohort 1: Percentage of Participants Who Needed Hydration and/or Feeding by Intravenous (IV) Administration or Nasogastric Tube Percentage of participants who needed hydration and/or feeding by IV Administration or nasogastric tube after the first dose of study drug was assessed. This parameter was only for participants who didn't require supplemental feeding/hydration before first dose of study drug. As per the study protocol and study design, this outcome measure was planned to be analyzed for participants who were hospitalized only. Only participants in Cohort 1 were hospitalized, hence this outcome measure is only reported for Cohort 1. Up to Day 28
Secondary Percentage of Participants With Adverse Events Percentage of participants with adverse events was assessed. An AE is any untoward medical occurrence in clinical study participants administered a medicinal (investigational or non-investigational) product. An adverse event does not necessarily have a causal relationship with the intervention. Up to Day 28
Secondary Percentage of Participants With Abnormal Laboratory Findings Percentage of participants with abnormal laboratory findings (chemistry and hematology) worst toxicity grade was assessed based on Division of Microbiology and Infectious Diseases (DMID) toxicity grading scale. DMID toxicity grades range from 1 to 4. Grade 1 = mild: transient or mild discomfort (<48 hours); no medical intervention/therapy required. Grade 2 = moderate: mild to moderate limitation in activity - some assistance may be needed; no or minimal medical intervention/therapy required. Grade 3 = severe: marked limitation in activity, some assistance usually required; medical intervention/therapy required, hospitalizations possible. Grade 4 = life-threatening or death: Extreme limitation in activity, significant assistance required; significant medical intervention/therapy required, hospitalization or hospice care probable. Up to Day 28
Secondary Percentage of Participants With Abnormal Electrocardiograms (ECGs) Findings Percentage of participants with abnormal ECG (PR interval [for age 0 to 2 years: >150 msec is abnormally high, for age group 2 to <3.5 years: <100 msec is abnormally low and >150 msec is abnormally high]; QRS interval [for 0 to 2 years: >79 msec is abnormally high, for age group 2 to <3.5 years: <40 msec is abnormally low and >79 msec is abnormally high]; QT interval [for age 0 to 2 years: >500 msec is abnormally high, for age group 2 to <18 years: <320 msec is abnormally low and >450 msec is abnormally high]; RR interval [for age 0 to 3 months: <333 msec is abnormally low and >750 msec is abnormally high; for age group 3 to 12 months: <400 msec is abnormally low and >860 msec is abnormally high; for age 1 to 2 years: <430 msec is abnormally low and >1000 msec is abnormally high; for age group 2 to <18 years: <600 msec is abnormally low and >1200 msec is abnormally high]) findings were assessed. Up to Day 28
Secondary Percentage of Participants With Categorized Change From Baseline in ECG Parameters (QT, QTcB, QTcF) Percentage of participants with categorized change from Baseline in ECG parameters (QT/ QTcB/ QTcF interval) was assessed. Abnormal ECG change from baseline in QTc and QTcB Interval is categorized as borderline QTc change: 30 ms (milliseconds) to <60 ms, and abnormally high QTc change: greater than [>] 60 ms), and QTcF Interval is categorized as borderline QTc change: 30 ms to <60 ms, and abnormally high QTc change: >60 ms. Baseline to Day 28
Secondary Percentage of Participants With Vital Signs Abnormalities Percentage of participants with vital signs (SBP,DBP, pulse rate, respiratory rate, body temperature and SpO2) abnormalities (abnormally low [ABL] and abnormally high [ABH]) were reported. DBP: ABL: <35 mmHg:0-3 months (mths), <40 mmHg:3 mths- <3.5 years,ABH: >65 mmHg:0-3 mths, >85 mmHg:3-12 mths, >90 mmHg:1-2 years, >70 mmHg: 2- <3.5 years; SBP:ABL: <60 mmHg:0-12 mths,<75 mmHg:1-2 years, <80:2- <3.5 years,ABH: >110:0-12 mths, >120 mmHg:1-2 years, >10 mmHg:2- <3.5 years; Pulse rate:ABL: <80 bpm:0-3 mths, <70 bpm:3 mths-12 mth,<60 bpm:1-2 years, <90 bpm:2- <3.5 years,ABH: >180 bpm:0-3 mths, >150 bpm:3 mths-12 mths, >140 bpm:1-2 years, >130:2- <3.5 years; Respiratory rate:ABL: <25 bpm:0-3 mths, <20 bpm: 3 mths-12 mths,<18 bpm:1-2 years, <20 bpm:2- <3.5 years, ABH:>70 bpm:0-3 mths, >60 bpm:3 mths-12 mths, >50 bpm:1-2 years, >35 bpm:2- <3.5 years; SpO2: ABL: <92%: 0-<3.5 years; Temperature (Celsius): ABH:>37.8:Tympanic, >38.0:forehead, oral, axillary, >37.2:rectal. Up to Day 28
Secondary Cohort 1: Area Under the Plasma Concentration-Time Curve From Timepoint 0 Hours Until 24 Hours Post Dose (AUC[0-24 Hours]) AUC (0-24) is defined as area under the plasma concentration-time curve from timepoint 0 hours until 24 hours post dose estimated by population PK model. 0 to 24 hours post dose on Days 1 and 7
Secondary Cohort 1: Maximum Plasma Concentration (Cmax) of JNJ-53718678 Cmax is the maximum plasma concentration of JNJ-53718678 estimated by population PK model. Days 1 and 7
Secondary Cohort 1: Trough Plasma Concentration (Ctrough) of JNJ-53718678 Ctrough is the trough plasma concentration of JNJ-53718678 estimated by population PK model. Days 1 and 7
Secondary Cohort 2: Plasma Concentration of JNJ-53718678 Plasma concentration of JNJ-53718678 was measured for Cohort-2. As per planned analysis in the protocol, PK sampling was performed on either Day 3 or Day 5 for participants receiving twice daily dosing, resulting in one combined timepoint of Day 3 or Day 5. Hence, the data collected on either Day 3 or Day 5 was pooled and is reported here collectively. Once daily dosing: Day 3 and Day 8 pre- or post-dose. Twice daily dosing: Day 1 at least 1 hour post-dose, and Days 3 or 5 (combined in one timepoint) at least 4 hours after morning dose but prior to evening dose
Secondary Percentage of Participants With Medical Resource Utilization (MRU) Percentage of participants with MRU (any medical care encounters) was reported. Up to Day 28
Secondary Percentage of Participants With Acceptability and Palatability of the JNJ-53718678 Formulation as Assessed by Parent(s)/Caregiver(s) Percentage of participants with acceptability and palatability of the JNJ-53718678 formulation was assessed through a questionnaire asking about the child's reaction when given the medicine, completed by parent(s)/caregiver(s) after last dosing that categorized as 1) child took medicine easily, 2) disgusted expressions after tasting medicine, 3) cried after tasting medicine, 4) would not open mouth or turned head away to avoid medicine, 5) spit out or coughed out medicine, 6) gagged, and 7) vomited (within 2 minutes of swallowing medicine). Below results are based on response to "child took medicine easily". Day 8
Secondary Number of Participants With Emerging Variations in the Viral Genome Potentially Associated With Resistance to JNJ-53718678 Number of participants with emerging variations in the viral genome potentially associated with resistance to JNJ-53718678 was reported. Number of participants with F gene sequencing data available and with emerging genetic variations post-baseline as compared to baseline, considering 24 RSV F protein positions of interest (positions 127, 137, 138, 140, 141, 143, 144, 323, 338, 339, 392, 394, 396, 397, 398, 399, 400, 401, 474, 486, 487, 488, 489, and 517) was reported. Up to Day 21
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