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| Name | Class |
|---|---|
| Johns Hopkins Bloomberg School of Public Health | OTHER |
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Zika virus (ZIKV) is an illness people can get from mosquitoes. The infection is generally mild with symptoms that include a fever, rash, red eyes, and joint pain, though most of those infected have no symptoms. Preventing ZIKV is important because if a pregnant person is infected with ZIKV, it can cause birth defects in their unborn child.
The goals of this study are to find out if people who have already been infected with one type of ZIKV can get infected with ZIKV a second time, and to test the ability of the TV003 dengue vaccine to prevent people from getting infected with the ZIKV-SJRP challenge virus.
This study is an open label with 2 study arms. Arm 1 will evaluate the protective efficacy of TV003 against ZIKV challenge. Arm 1 will include infectivity controls who will receive PlasmaLyte (the TV003 diluent) and the treatment assignment will be blinded to reduce bias in the assessment of adverse events. The PlasmaLyte recipients will serve as infectivity controls to ensure the potency of the ZIKV challenge. The treatment assignment of the infectivity controls may be unblinded as early as 28 days after receipt of TV003/PlasmaLyte if they are needed for ZIKV-challenge of volunteers in Arm 2 and may be challenged earlier than the TV003 cohort. Arm 2 will evaluate the protective efficacy of previous ZIKV infection against subsequent ZIKV challenge. Both arms will be compared to historical controls who previously received ZIKV infection. Infectivity controls will not be included in the efficacy analysis.
This study will include 16 flavivirus-naïve subjects for Arm 1. Twelve subjects will receive the live attenuated dengue vaccine candidate TV003 at Study Day 0 and 4 subjects will receive PlasmaLyte at Study Day 0. These subjects will be randomized in blocks of 4 (3 TV003:1 PlasmaLyte). At Study Day 180, Arm 1 subjects will receive the controlled human infection strain of ZIKV SJRP/2016-184 as a challenge virus. These subjects will include those volunteers who received TV003 and at least 1 of the infectivity controls who received PlasmaLyte. Subjects in Arm 1 will be followed for approximately 52 weeks (approximately 360 days) from the time of vaccination.
Ten subjects who had a ZIKV infection, either from a previous ZIKV controlled human infection study where they had received either ZIKV SJRP/2016-184 or ZIKV Nicaragua/2016 or were excluded during screening for previous studies as having ZIKV infection, will be enrolled as a group in Arm 2. Subjects enrolled in Arm 2 will be challenged with the ZIKV SJRP/2016-184 challenge virus separately from TV003 recipients. At least 1 of the PlasmaLyte recipients enrolled in Arm 1 on Day 0 will be included in this group to receive ZIKV SJRP/2016-184 as an infectivity control. Arm 2 subjects will be followed after ZIKV challenge for approximately 26 weeks (approximately 180 days). Subjects will be screened for eligibility up to 60 days prior to vaccination on Study Day 0.
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| Label | Type | Description | Intervention Names |
|---|---|---|---|
| Arm 1: DENV/ZIKV naive subjects receiving TV003 | Experimental | Twelve volunteers will receive TV003 followed by challenge with ZIKV on Day 180 (6 months post-vaccination). |
|
| Infectivity Controls: DENV/ZIKV naive subjects receiving PlasmaLyte | Placebo Comparator | Four volunteers will receive PlasmaLyte as control followed by challenge with ZIKV at least 28 days after vaccination. |
|
| Arm 2: Subjects with previous ZIKV infection | Experimental | Previous ZIKV-infected volunteers will be challenged with ZIKV on Arm 2 Day 0. |
|
| Name | Type | Description | Arm Group Labels | Other Names |
|---|---|---|---|---|
| TetraVax-DV-TV003 (TV003) | Biological | 0.5 ml of TV003 delivered via subcutaneous injection. TV003 contains 10^3.3 plaque forming units (PFU)/mL of rDEN1Δ30, 10^3.3 PFU/mL of rDEN2/4Δ30(ME), 10^3.3 PFU/mL of rDEN3Δ30/31- 7164 and 10^3.3 PFU/mL of rDEN4Δ30 |
| Measure | Description | Time Frame |
|---|---|---|
| Incidence, magnitude, and duration of infectious ZIKV-SJRP/2016-184 recovered from serum following administration of ZIKV-SJRP/2016-184 in subjects who received TV003 | Compared to historical controls | Through 180 days post challenge |
| Incidence, magnitude, and duration of infectious ZIKV-SJRP/2016-184 recovered from serum following administration of ZIKV-SJRP/2016-184 in ZIKV-exposed subjects | Compared to historical controls | Through 180 days post challenge |
| Proportion of subjects who received TV003 who develop clinical signs/symptoms of Zika infection | Compared to historical controls | Through 180 days post challenge |
| Proportion of subjects who were previously infected with ZIKV who develop clinical signs/symptoms of Zika infection | Compared to historical controls | Through 180 days post challenge |
| Frequency of immediate, systemic, and local adverse events (AEs) following vaccination with TV003 | Through 28 days post vaccination | |
| Frequency of immediate, systemic, and local AEs following inoculation with ZIKV-SJRP/2016-184 | Through 28 days post challenge |
| Measure | Description | Time Frame |
|---|---|---|
| Incidence, magnitude, and duration of ZIKV viremia induced by administering 10^2 PFU of ZIKV-SJRP/2016-184 in subjects who received TV003 | Measured by quantitative polymerase chain reaction (PCR) induced, compared to historical controls. | Through 6 months post challenge |
| Incidence, magnitude, and duration of ZIKV viremia induced by administering 10^2 PFU of ZIKV-SJRP/2016-184 in previously ZIKV-exposed subjects |
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Inclusion Criteria:
Adults between 18 and 40 years of age, inclusive.
Good general health as determined by physical examination, laboratory screening, and review of medical history.
Available for the duration of the study, approximately 52 weeks.
Willingness to participate in the study as evidenced by signing the informed consent document.
Must be able to complete the informed consent process and comprehension assessment independently and without assistance.
Subjects assigned male at birth: Willingness to use barrier contraception during cervico-vaginal, anal, and oral intercourse from Study Day 0 through 90 days post ZIKV challenge (in accordance with CDC guidance).
Subjects assigned female at birth: Willingness to use barrier contraception during cervico-vaginal, anal, and oral intercourse from Study Day 0 through 56 days post ZIKV challenge (in accordance with CDC guidance).
Subjects of childbearing potential must be willing to use effective contraception through 56 days post-ZIKV challenge, in accordance with CDC guidance. Reliable methods of contraception include hormonal birth control* (implantable, hormonal patch, hormonal vaginal ring, oral contraception, Depo-Provera injection, etc.), surgical sterilization (hysterectomy, tubal ligation, or tubal coil at least 3 months prior to inoculation with TV003/PlasmaLyte and/or ZIKV challenge), and intrauterine device. All subjects assigned female at birth will be considered having child-bearing potential except for those with post-menopausal status documented as at least 1 year since last menstrual period, those assigned female at birth who have sex with partners assigned female at birth (exclusively) and have no intention of conceiving a child during the study, and for the vaccination phase of the study only, participants who practice abstinence (≥ 6 months with no sexual contact). Subjects who are not considered to be of childbearing potential will not be required to use contraception other than barrier contraception for the purpose of reducing potential transmission.
Inclusion Criteria for Challenge with ZIKV SJRP/2016-184:
Additional Inclusion Criteria for Arm 2 Subjects with a Previous History of ZIKV Infection Only:
-History or serologic evidence of previous ZIKV or identified as an infectivity control.
Exclusion Criteria:
Additional Exclusion Criteria for TV003/PlasmaLyte Group Only:
Exclusion Criteria for ZIKV SJRP/2016-184:
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| Name | Affiliation | Role |
|---|---|---|
| Anna Durbin, M.D. | Johns Hopkins Bloomberg School of Public Health | Principal Investigator |
| Facility | Status | City | State | ZIP | Country | Contacts |
|---|---|---|---|---|---|---|
| Center for Immunization Research, Johns Hopkins School of Public Health | Baltimore | Maryland | 21205 | United States | ||
| PubMed Identifier | Type | Citation | Retractions |
|---|---|---|---|
| 37971871 | Background | Pierce KK, Durbin AP, Walsh MR, Carmolli M, Sabundayo BP, Dickson DM, Diehl SA, Whitehead SS, Kirkpatrick BD. TV005 dengue vaccine protects against dengue serotypes 2 and 3 in two controlled human infection studies. J Clin Invest. 2024 Feb 1;134(3):e173328. doi: 10.1172/JCI173328. | |
| 21781997 | Background | Durbin AP, Kirkpatrick BD, Pierce KK, Schmidt AC, Whitehead SS. Development and clinical evaluation of multiple investigational monovalent DENV vaccines to identify components for inclusion in a live attenuated tetravalent DENV vaccine. Vaccine. 2011 Sep 23;29(42):7242-50. doi: 10.1016/j.vaccine.2011.07.023. Epub 2011 Jul 21. |
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| Plasmalyte | Biological | 0.5 mL of PlasmaLyte delivered via subcutaneous injection |
|
| Challenge virus ZIKV-SJRP/2016-184 | Biological | 0.5 ml of ZIKV-SJRP/2016-184 delivered via subcutaneous injection. ZIKV-SJRP/2016-184 contains a dose of 10^2 plaque-forming units (PFU). |
|
Measured by quantitative PCR induced, compared to historical controls. |
| Through 6 months post challenge |
| Number of TV003 vaccinees infected with DENV-1, DENV-2, DENV-3, and DENV-4 following administration of TV003 | Infection is defined as recovery of vaccine virus from the blood or serum of a subject and/or by seropositivity to DENV measured by quantitative PCR | Through 270 days post vaccination |
| Peak neutralizing antibody titer (NT) to DENV-1, DENV-2, DENV-3, and DENV-4 | Measured by the NT50 at 28, 56, and 90 days after TV003 vaccination. | Through 90 days post vaccination |
| Peak NT to ZIKV-SJRP/2016-184 | Measured by NT50 at 0, 28, 56, and 90 days post-administration of ZIKV-SJRP | Through 90 days post challenge |
| Number of volunteers who become infected following primary ZIKV-SJRP administration | Through 16 days post challenge |
| Peak NT50 against ZIKV following TV003 vaccination correlates with protection against ZIKV infection | Through 90 days post challenge |
| Evaluate boost in neutralizing antibody titers to DENV-1, DENV-2, DENV-3, and DENV-4 post-ZIKV challenge in subjects who received TV003 | Peak NT50 achieved through 90 days post-ZIKV challenge in TV003 recipients. A boost in antibody titer is defined as a ≥ 4-fold rise through 90 days post challenge compared with the titer just prior to ZIKV challenge. | Through 90 days post challenge |
| Evaluate boost in neutralizing antibody titers to ZIKV post challenge in subjects with previous ZIKV infection | Peak NT50 achieved through 90 days post-ZIKV challenge. A boost in antibody titer is defined as a ≥ 4-fold rise in peak ZIKV neutralizing antibody titer through 90 days post challenge compared with the ZIKV neutralizing antibody titer in serum collected just prior to ZIKV challenge. | Through 90 days post-ZIKV challenge of previous ZIKV recipients |
| Quantity and duration of ZIKV in blood, cervico-vaginal secretions and semen | Measured by culture (infectious virus) and by reverse transcriptase - PCR in all participants receiving ZIKV-SJRP/2016-184 | Through 6 months post challenge |
| Center for Immunization Research |
| Baltimore |
| Maryland |
| 21224 |
| United States |
| 38294972 | Background | Kallas EG, Cintra MAT, Moreira JA, Patino EG, Braga PE, Tenorio JCV, Infante V, Palacios R, de Lacerda MVG, Batista Pereira D, da Fonseca AJ, Gurgel RQ, Coelho IC, Fontes CJF, Marques ETA, Romero GAS, Teixeira MM, Siqueira AM, Barral AMP, Boaventura VS, Ramos F, Elias Junior E, Cassio de Moraes J, Covas DT, Kalil J, Precioso AR, Whitehead SS, Esteves-Jaramillo A, Shekar T, Lee JJ, Macey J, Kelner SG, Coller BG, Boulos FC, Nogueira ML. Live, Attenuated, Tetravalent Butantan-Dengue Vaccine in Children and Adults. N Engl J Med. 2024 Feb 1;390(5):397-408. doi: 10.1056/NEJMoa2301790. |
| ID | Term |
|---|---|
| D000071243 | Zika Virus Infection |
| ID | Term |
|---|---|
| D000096724 | Mosquito-Borne Diseases |
| D000079426 | Vector Borne Diseases |
| D007239 | Infections |
| D001102 | Arbovirus Infections |
| D014777 | Virus Diseases |
| D018177 | Flavivirus Infections |
| D018178 | Flaviviridae Infections |
| D012327 | RNA Virus Infections |
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| ID | Term |
|---|---|
| C048013 | Plasmalyte A |
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