RSV001 - A New Vaccine to Prevent Severe Viral Chest Infections.
NCT ID: NCT01805921
Last Updated: 2016-04-26
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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COMPLETED
PHASE1
72 participants
INTERVENTIONAL
2013-05-31
2015-08-31
Brief Summary
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This virus can cause respiratory infections such as bronchiolitis and pneumonia. It affects all ages, but especially infants, adults with a suppressed immune system, and the elderly. RSV only infects humans and occurs in epidemics each winter. It is the single most common cause of severe respiratory illness in children.
There is no effective anti-viral medication to treat RSV infections. There is a monoclonal antibody, which can be given to 'at-risk' children given by injection on a monthly basis during winter to provide short term protection against infection, but it is only partially effective and prohibitively expensive. Currently, there is no licensed vaccine to prevent RSV infection and there remains a real need to develop a vaccine as a cost-effective method to save lives and reduce the cost of disease caused by RSV.
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Detailed Description
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The two vaccines in this study contain all three of these proteins. However, they are delivered into the body using different 'vectors', which are harmless carrier viruses. In this study, we have employed two different vectors:a simian adenoviruses (PanAd3) and Modified Vaccinia virus Ankara (MVA).
We administer these vaccines using a 'prime-boost' strategy, in which one of these vaccines is used to 'prime' the immune system, which is then 'boosted' 4 or 8 weeks later, depending on the groups, by administration of an alternative vaccine or the same vaccine given by a different route.
Conditions
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Study Design
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NON_RANDOMIZED
PARALLEL
PREVENTION
NONE
Study Groups
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Arm 1. Prime PanAd3-RSV (IM), boost MVA-RSV (IM)
Group 1A. Low dose prime PanAd3-RSV given by intra-muscular injection (IM) - low dose boost MVA-RSV given by intra-muscular injection (IM). 2 volunteers, 18-50 years. Interval: 8 weeks.
Group 1B. High dose prime PanAd3-RSV given by intra-muscular injection (IM) - high dose boost MVA-RSV given by intra-muscular injection (IM). 8 volunteers, 18-50 years. Interval: 8 weeks.
MVA-RSV given by intra-muscular injection (high dose)
High dose = 1x10\^8 pfu
PanAd3-RSV given by intra-muscular injection (high dose)
High dose = 5x10\^10 vp
MVA-RSV given by intra-muscular injection (low dose)
Low dose = 1x10\^7 pfu
PanAd3-RSV given by intra-muscular injection (low dose)
Low dose = 5x10\^9 vp
Arm 2. Prime PanAd3-RSV (IM), boost PanAd3-RSV (IM)
Group 2A. Low dose prime PanAd3-RSV given by intra-muscular injection (IM) - low dose boost PanAd3-RSV given by intra-muscular injection (IM). 2 volunteers, 18-50 years. Interval: 4 weeks.
Group 2B. High dose prime PanAd3-RSV given by intra-muscular injection (IM) - high dose boost PanAd3-RSV given by intra-muscular injection (IM). 8 volunteers, 18-50 years. Interval: 4 weeks.
PanAd3-RSV given by intra-muscular injection (high dose)
High dose = 5x10\^10 vp
PanAd3-RSV given by intra-muscular injection (low dose)
Low dose = 5x10\^9 vp
Arm 3. Prime PanAd3-RSV (IN), boost MVA-RSV (IM)
Group 3A. Low dose prime PanAd3-RSV given intra-nasally (IN) - low dose boost MVA-RSV given by intra-muscular injection (IM). 2 volunteers, 18-50 years. Interval: 8 weeks.
Group 3B. High dose prime PanAd3-RSV given intra-nasally (IN) - high dose boost MVA-RSV given by intra-muscular injection (IM). 8 volunteers, 18-50 years. Interval: 8 weeks.
PanAd3-RSV given intra-nasally (high dose)
High dose = 5x10\^10 vp
MVA-RSV given by intra-muscular injection (high dose)
High dose = 1x10\^8 pfu
PanAd3-RSV given intranasally (low dose)
Low dose = 5x10\^9 vp
MVA-RSV given by intra-muscular injection (low dose)
Low dose = 1x10\^7 pfu
Arm 4. Prime PanAd3-RSV (IN), boost PanAd3-RSV (IM)
Group 4A. Low dose prime PanAd3-RSV given intra-nasally (IN) - low dose boost PanAd3-RSV given by intra-muscular injection (IM). 2 volunteers, 18-50 years. Interval: 8 weeks.
Group 4B. High dose prime PanAd3-RSV given intra-nasally (IN) - high dose boost PanAd3-RSV given by intra-muscular injection (IM). 8 volunteers, 18-50 years. Interval: 8 weeks.
PanAd3-RSV given intra-nasally (high dose)
High dose = 5x10\^10 vp
PanAd3-RSV given by intra-muscular injection (high dose)
High dose = 5x10\^10 vp
PanAd3-RSV given intranasally (low dose)
Low dose = 5x10\^9 vp
PanAd3-RSV given by intra-muscular injection (low dose)
Low dose = 5x10\^9 vp
Arm 5. No vaccine
Group 5. Non-vaccinated control group. 6 volunteers, 60-75 years.
No interventions assigned to this group
Arm 6. MVA-RSV (IM)
Group 6. Single high dose MVA-RSV given by intra-muscular injection (IM). 6 volunteers, 60-75 years.
MVA-RSV given by intra-muscular injection (high dose)
High dose = 1x10\^8 pfu
Arm 7. Prime PanAd3-RSV (IM), boost PanAd3-RSV (IM)
Group 7. High dose prime PanAd3-RSV given by intra-muscular injection (IM) - high dose boost PanAd3-RSV given by intra-muscular injection (IM). 6 volunteers, 60-75 years. Interval: 4 weeks.
PanAd3-RSV given by intra-muscular injection (high dose)
High dose = 5x10\^10 vp
Arm 8. Prime PanAd3-RSV (IN), boost MVA-RSV (IM)
Group 8. High dose prime PanAd3-RSV given intra-nasally - high dose boost MVA-RSV given by intra-muscular injection (IM). 6 volunteers, 60-75 years. Interval: 8 weeks.
PanAd3-RSV given intra-nasally (high dose)
High dose = 5x10\^10 vp
MVA-RSV given by intra-muscular injection (high dose)
High dose = 1x10\^8 pfu
Arm 9. Prime PanAd3-RSV (IM), boost MVA-RSV (IM)
Group 9. High dose prime PanAd3-RSV given by intra-muscular injection (IM) - high dose boost MVA-RSV given by intra-muscular injection (IM). 6 volunteers, 60-75 years. Interval: 8 weeks.
MVA-RSV given by intra-muscular injection (high dose)
High dose = 1x10\^8 pfu
PanAd3-RSV given by intra-muscular injection (high dose)
High dose = 5x10\^10 vp
Interventions
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PanAd3-RSV given intra-nasally (high dose)
High dose = 5x10\^10 vp
MVA-RSV given by intra-muscular injection (high dose)
High dose = 1x10\^8 pfu
PanAd3-RSV given by intra-muscular injection (high dose)
High dose = 5x10\^10 vp
PanAd3-RSV given intranasally (low dose)
Low dose = 5x10\^9 vp
MVA-RSV given by intra-muscular injection (low dose)
Low dose = 1x10\^7 pfu
PanAd3-RSV given by intra-muscular injection (low dose)
Low dose = 5x10\^9 vp
Eligibility Criteria
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Inclusion Criteria
* Willing and able to give informed consent for participation in the study
* Aged between 18 and 50 years (Groups 1-4) or aged 60-75 years (Groups 5-9)
* In good health as determined by
* Medical history
* Physical examination
* Clinical judgment of the investigators
* Willing to use effective contraception
* Females: The oral contraceptive pill, contraceptive implant or barrier methods from one month prior and for the duration of the study (Groups 1-4 only)
* Males: Barrier contraception from V1 until 3 months after the last vaccination
* Able to attend the scheduled visits and to comply with all study procedures
* Willing to allow his or her General Practitioner and/or Consultant, if appropriate, to be notified of participation in the study
Exclusion Criteria
The participant may not enter the study if any of the following apply:
* History of significant organ/system disease that could interfere with trial conduct or completion. This includes any history of significant disease in the following;
* Cardiovascular disease including congenital heart disease, previous myocardial infarction, valvular heart disease (or history of rheumatic fever), previous bacterial endocarditis, history of cardiac surgery (including pacemaker insertion), personal or family history of cardiomyopathy or sudden adult death
* Respiratory disease such as asthma (excluding childhood asthma not treated in adulthood) and chronic obstructive pulmonary disease
* Endocrine disorders such as diabetes mellitus and Addison's disease
* Significant renal or bladder disease, including history of renal calculi
* Biliary tract disease
* Gastro-intestinal disease such as inflammatory bowel disease, abdominal surgery within the last two years, coeliac disease and liver disease
* Neurological disease such as seizures and myasthenia gravis
* Metabolic disease such as glucose-6-phosphate dehydrogenase deficiency
* Psychiatric illness requiring hospitalization or depression whose severity is deemed clinical significant by the Chief Investigator, Consultant or GP
* Non-benign cancer, including squamous cell carcinoma, basal cell carcinoma of the skin and cervical carcinoma in situ
* Clinically significant contact dermatitis
* Have any known or suspected impairment or alteration of immune function, resulting from, for example:
* Congenital or acquired immunodeficiency
* Human Immunodeficiency Virus infection or symptoms/signs suggestive of an HIV-associated condition
* Autoimmune disease
* Receipt of immunosuppressive therapy such as anti-cancer chemotherapy or radiation therapy within the preceding 12 months or long-term systemic corticosteroid therapy
* Receipt of immunoglobulin or any blood product transfusion within 3 months of study start
* A vaccination history indicative of;
* Planning to receive any vaccine other than the study vaccine within 4 weeks following vaccination
* A history of anaphylaxis reaction to a vaccine
* History of allergic disease or reactions likely to be exacerbated by any component of the vaccine, e.g. Kathon
* Previously having received a recombinant simian or human adenoviral vaccine
* Previously having received a recombinant MVA vaccine
* Detection of any of the following at screening
* IgA deficiency
* Anti-HIV antibody
* Hepatitis B surface antigen
* Anti-HCV antibody
* Any other significant abnormalities on screening investigations at the discretion of an Investigator
* Known or suspected drug and/or alcohol misuse (alcohol misuse defined as an intake exceeding 42 units per week)
* Nasal septal pathology including
* Congenital deformities such as an abnormal septum or polyps
* Previous cauterization, rhinoplasty or surgery of any kind
* Recurrent epistaxis
* Scheduled procedures requiring general anaesthesia during the study
* Participation in another research study involving an investigational product in the past 12 weeks, or are planning to do so within the 20 weeks of this study
* Inability, in the opinion of the Investigator, to comply with all study requirements
* Female participants who are pregnant, lactating or planning pregnancy during the course of the study
* Has donated blood within 4 months before starting the trial, or is intending to donate blood during the trial and up to 12 weeks after completing the study
* Any other significant disease or disorder which, in the opinion of the Investigator, may
* Put the participants at risk because of participation in the study
* Influence the result of the study
* Impair the participant's ability to participate in the study
18 Years
75 Years
ALL
Yes
Sponsors
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ReiThera Srl
INDUSTRY
Responsible Party
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Principal Investigators
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Andrew J Pollard, FRCPCH PhD
Role: PRINCIPAL_INVESTIGATOR
University of Oxford. Department of Paediatrics
Locations
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Centre for Clinical Vaccinology & Tropical Medicine (CCVTM)
Oxford, Oxfordshire, United Kingdom
Countries
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References
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Green CA, Scarselli E, Voysey M, Capone S, Vitelli A, Nicosia A, Cortese R, Thompson AJ, Sande CS, de Lara C, Klenerman P, Pollard AJ. Safety and immunogenicity of novel respiratory syncytial virus (RSV) vaccines based on the RSV viral proteins F, N and M2-1 encoded by simian adenovirus (PanAd3-RSV) and MVA (MVA-RSV); protocol for an open-label, dose-escalation, single-centre, phase 1 clinical trial in healthy adults. BMJ Open. 2015 Oct 28;5(10):e008748. doi: 10.1136/bmjopen-2015-008748.
Green CA, Scarselli E, Sande CJ, Thompson AJ, de Lara CM, Taylor KS, Haworth K, Del Sorbo M, Angus B, Siani L, Di Marco S, Traboni C, Folgori A, Colloca S, Capone S, Vitelli A, Cortese R, Klenerman P, Nicosia A, Pollard AJ. Chimpanzee adenovirus- and MVA-vectored respiratory syncytial virus vaccine is safe and immunogenic in adults. Sci Transl Med. 2015 Aug 12;7(300):300ra126. doi: 10.1126/scitranslmed.aac5745.
Related Links
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More study information will be available from the Oxford Vaccine Group website once recruitment opens
Other Identifiers
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2011-003589-34
Identifier Type: EUDRACT_NUMBER
Identifier Source: secondary_id
RSV001
Identifier Type: -
Identifier Source: org_study_id
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