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A Study to Assess the Safety, Pharmacodynamics, and Immunogenicity of PXVX0047

Phase 1
Terminated
Conditions
Adenoviral Infection
Interventions
Biological: Teva Ad4/Ad7 Vaccine
Biological: PXVX0047 Vaccine
Registration Number
NCT03160339
Lead Sponsor
Emergent BioSolutions
Brief Summary

PXVX0047 (Adenovirus Type 4 and Type 7 Vaccine \[A549 Cells\], Live, Oral) is an investigational vaccine in development for the indication of active immunization against adenovirus infection. The primary goals of this Phase 1 study are to evaluate safety, pharmacodynamics (viral shedding), and immunogenicity of PXVX0047.

Detailed Description

Not available

Recruitment & Eligibility

Status
TERMINATED
Sex
All
Target Recruitment
25
Inclusion Criteria
  • Male or female
  • Age 18 to 35
  • Seronegative for Ad4 and Ad7 by CPE-based assay
  • (if female of childbearing potential) Using an acceptable method of contraception
  • If male, subject agrees to use a highly effective method of contraception with female sexual partners of childbearing potential
  • Able and willing to provide informed consent for study participation
Exclusion Criteria
  • Current acute febrile illness
  • Current acute gastrointestinal illness
  • Clinically significant cardiac, respiratory, or gastrointestinal disease
  • (if female of childbearing potential) Pregnant or nursing, or who plan to become pregnant or nurse during the study
  • Persons with occupations which may create an increased risk of transmission of vaccine virus (including but not limited to health care workers, child or elderly care providers, food handlers or preparers) who also have expected occupational contact with children less than 7 years of age, pregnant or nursing women, women of childbearing potential not using an acceptable method of contraception, or chronically ill or immunosuppressed individuals through Day 29.
  • Expected household contact with children less than 7 years of age, pregnant or nursing women, women of childbearing potential not using an acceptable method of contraception, or chronically ill or immunosuppressed individuals through Day 29.
  • Laboratory evidence of infection with Hepatitis B/C or HIV.
  • History of severe allergic reaction (e.g. anaphylaxis) to any component of the vaccine.
  • Inability to swallow capsules or tablets whole without chewing or crushing.
  • Immunosuppressed individuals, including those treated or planned to be treated with systemic immunosuppressive medications within the 30 days prior to enrollment through 30 days after study treatment.
  • Concomitant or planned use of other vaccines, investigational agents, cidofovir, ribavirin, or medications expected by the Investigator to have antiviral activity against adenovirus within 30 days prior to enrollment through Day 29.
  • Any other condition that, in the opinion of the Investigator, creates an unacceptable risk to the subject.
  • Any other condition that, in the opinion of the Investigator, may interfere with the conduct of the study or the validity of the data.

Study & Design

Study Type
INTERVENTIONAL
Study Design
PARALLEL
Arm && Interventions
GroupInterventionDescription
Teva Ad4/Ad7 treatment groupTeva Ad4/Ad7 VaccineSubjects will receive Teva Ad4/Ad7 vaccine and PXVX0047 Placebo-to-Match
PXVX0047 treatment groupPXVX0047 VaccineSubjects will receive PXVX0047 vaccine and Teva Placebo-to-Match
Primary Outcome Measures
NameTimeMethod
Evaluate the induction of anti-Ad7 neutralizing activity by measuring the Ad7 seroconversion rateFrom Day 1 to Day 29

The Ad7 seroconversion rate is defined as the percent of subjects seroconverted (i.e. with a 4-fold or greater rise over baseline in neutralizing antibody titer) to Ad7 as determined by cytopathic-effect (CPE)-based assay

Evaluate the induction of anti-Ad4 neutralizing activity by measuring the Ad4 and Ad7 seroconversion rateFrom Day 1 to Day 29

The Ad4 seroconversion rate is defined as the percent of subjects seroconverted (i.e. with a 4-fold or greater rise over baseline in neutralizing antibody titer) to Ad4 as determined by cytopathic-effect (CPE)-based assay

Evaluate safety and tolerability of PXVX0047 by documenting the incidence of severity of solicited adverse eventsFrom Day 1 through Day 15

Incidence of severity of solicited adverse events include abdominal pain, nausea, vomiting, diarrhea, cough, nasal congestion, dyspnea, sore throat, headache, fever fatigue chills myalgia, arthralgia

Evaluate the safety and tolerability of PXVX0047 by documenting the incidence and severity of adverse events that are not solicited.From Day 1 through Day 29

Unsolicited adverse events include clinical significant laboratory abnormalities

Secondary Outcome Measures
NameTimeMethod
Evaluate the pharmacodynamics of PXVX0047 by measuring the shedding of Ad7 viruses via the GI tractDays 4, 8, 15, 22, and 29

Shedding of Ad7 via the GI tract, as assessed by rectal swabs

Evaluate the pharmacodynamics of PXVX0047 by measuring the shedding of Ad4 viruses via the GI tractDays 4, 8, 15, 22, and 29

Shedding of Ad4 via the GI tract, as assessed by rectal swabs

Evaluate the pharmacodynamics of PXVX0047 by measuring the shedding of Ad4 viruses via the respiratory tractDays 4, 8, 15, 22, and 29

Shedding of Ad4 via the respiratory tract, as assessed by throat swabs.

Evaluate the pharmacodynamics of PXVX0047 by measuring the presence of Ad4 viremiaDays 4, 8, 15, 22, and 29

Presence of Ad4 viremia in the blood

Evaluate the pharmacodynamics of PXVX0047 by measuring the presence of Ad7 viremiaDays 4, 8, 15, 22, and 29

Presence of Ad7 viremia in the blood

Evaluate the immunogenicity of PXVX0047 by measuring cumulative Ad4 seroconversion ratesThrough Day 57

The cumulative Ad4 seroconversion rates, measured independently, where cumulative seroconversion through a particular visit is defined as having seroconverted at or prior to that visit.

Evaluate the immunogenicity of PXVX0047 by measuring the fold-rise over baseline of neutralizing antibodies to Ad4 virusesThrough Day 57

The fold-rise over baseline in neutralizing antibodies to Ad4, measured independently

Evaluate the pharmacodynamics of PXVX0047 by measuring the shedding of Ad7 viruses via the respiratory tractDays 4, 8, 15, 22, and 29

Shedding of Ad7 via the respiratory tract, as assessed by throat swabs.

Evaluate the immunogenicity of PXVX0047 by measuring the fold-rise over baseline of neutralizing antibodies to Ad7 virusesThrough Day 57

The fold-rise over baseline in neutralizing antibodies to Ad7, measured independently

Evaluate the immunogenicity of PXVX0047 by measuring Ad7 seroconversion ratesThrough Day 57

The Ad7 seroconversion rates, measured independently, determined by luciferase and CPE-based assays

Evaluate the immunogenicity of PXVX0047 by measuring Ad4 seroconversion ratesThrough Day 57

The Ad4 seroconversion rates, measured independently, determined by luciferase and CPE-based assays

Evaluate the immunogenicity of PXVX0047 by measuring cumulative Ad7 seroconversion ratesThrough Day 57

The cumulative Ad7 seroconversion rates, measured independently, where cumulative seroconversion through a particular visit is defined as having seroconverted at or prior to that visit.

Evaluate the immunogenicity of PXVX0047 by measuring geometric mean titerThrough Day 57

The geometric mean titer (GMT) of neutralizing antibodies to Ad7, measured independently

Evaluate the immunogenicity of PXVX0047 by measuring the cellular immune responses to Ad4 virusesAt Days 29 and 57.

The cellular immune responses to Ad4, measured independently

Evaluate the immunogenicity of PXVX0047 by measuring the cellular immune responses to Ad7 virusesAt Days 29 and 57.

The cellular immune responses to Ad7, measured independently

Trial Locations

Locations (2)

Cincinnati Children's Hospital Medical Center

🇺🇸

Cincinnati, Ohio, United States

University of Vermont Medical Center

🇺🇸

Burlington, Vermont, United States

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