A Phase 1 Ascending Dose Study to Assess the Safety and Immunogenicity of Adenovirus Anthrax Vector Candidate Vaccines

Phase 1CompletedNCT01979406

Emergent BioSolutions120 enrolled

Overview

The purpose of this study is to evaluate 2 vaccine candidates against anthrax compared to the positive (vaccine) control as studied in normal healthy volunteers.

A Phase 1, randomized, double-blind, positive controlled, increasing dose clinical trial in healthy adult subjects at multiple sites. The study will assess safety and immunogenicity of two adenovirus vaccine candidates against anthrax compared to the positive control, Anthrax Vaccine Adsorbed (AVA). The trial will enroll 108 subjects in the anthrax vector vaccine arms and 12 subjects in the AVA positive control subjects. The study will look at three different dose of oral dosages of Ad4-PA (protective antigen) and Ad4-PA-GPI (10\^9, 10\^10, 10\^11 vp/dose)as well as 3 vaccine administration schedules (1 and 15 days; 1 and 29 days; 1, 15, and 29 days); 2 of 3 schedules will include an intramuscular (IM) AVA booster immunization, 1 schedule will include 3 vaccine administrations of Ad4-PA or Ad4-PA-GPI (glycosylphosphatidylinositol) alone, and 1 schedule will include 3 vaccine administrations of AVA alone.

Study Type

INTERVENTIONAL

Allocation

RANDOMIZED

Purpose

PREVENTION

Masking

QUADRUPLE

Enrollment

120

Conditions

Anthrax Infection

Interventions

AVABIOLOGICAL

Anthrax Vaccine Adsorbed (0.5 mL) as the placebo control on Days 1, 15 and 29

Ad4-PA-1BIOLOGICAL

Ad4-PA will be given at 10\^9, 10\^10 and 10\^11 on Day, followed by an oral placebo on Day 15 and an AVA boost on Day 29

Ad4-PA-GPI-1BIOLOGICAL

Given at 10\^9, 10\^10 and 10\^11 viral particles Ad4 PA-GPI at Day 1 + oral placebo on Day 29 + AVA boost at Day 15

Eligibility

Sex: ALLMin age: 18 YearsMax age: 40 YearsHealthy volunteers:

Medical Language ↔ Plain English

Inclusion Criteria: * Able to understand the study and give written informed consent. * Healthy men or women aged 18-40 years old, * BMI between 18 to 36 kg/m2 * Women of child bearing potential must have a negative serum pregnancy test at screening and a negative urine pregnancy test prior to vaccination on all vaccination days; they must also be willing to use adequate birth control for the duration of the study and have additional pregnancy tests if indicated. * Intact upper arms with sufficient muscular tissue in the deltoid region for IM vaccine administration. * Subject must be available for the study duration * Subject must avoid strenuous exercise for at least 72 hours prior to each study vaccine administration. Exclusion Criteria: * Subject is a healthcare worker who has direct contact with patients or has an household contact (HHC) who is immunodeficient or HIV-positive, pregnant, has an unstable medical condition, or is under the age of 18. * Subject is a childcare worker or a parent who has direct contact with children 5 years old and younger. * Subject directly prepares food in the food industry. * Pregnant or breastfeeding throughout the duration of the study until the final visit * Military service between 1971 and 1999, or after 2012 when Ad4 vaccine was/is routinely given * Employment in an industry involved in contact with ruminant animals, veterinary sciences, or other potential exposure to B. anthracis * Received previous Ad4 vaccination or experimental Ad4 vector vaccines * Received previous anthrax vaccine * Received or plans to receive any other approved or investigational vaccines from 30 days prior to the first study vaccination until 30 days after the final study vaccination for live attenuated vaccines and from 15 days prior to the first study vaccination until 15 days after the final study vaccination for inactivated vaccines * HIV or Hepatitis B or C positive * Immunodeficient or has an unstable medical condition including psychiatric conditions * Active or past history of acute or chronic gastrointestinal conditions * Active or past history of cancer except basal cell carcinoma * Recipient of bone marrow or solid organ transplant * Received or plans to receive systemic antiviral medication, within 30 days prior to the first study vaccination * Known allergy to any component of the study vaccine * Known allergy to, or known medical condition that precludes use of any systemic antiviral medication * Received or plans to receive medications indicated for decreasing acidity of stomach including: * Proton pump inhibitors or antacids or histamine 2-receptor antagonists * Received or plans to receive immunoglobulin or other blood products within 60 days prior to the first study vaccination * Received or plans to receive other investigational drugs within 30 days prior to the first study vaccination * Received or plans to receive systemic immunosuppressive therapy, radiation therapy, or inhaled steroids within 30 days prior to the first study vaccination * Asthmatic or requires asthmatic medications on a daily basis * Use of systemic chemotherapy within 5 years prior to study * Body temperature \>38.1°C or acute illness within 3 days prior to vaccination * History of excessive alcohol consumption, drug abuse, or significant psychiatric illness * History of Guillain-Barré Syndrome * Blood donation within 2 months prior to first study vaccination * Expected to be noncompliant with study visits or plans to move away or be living with different HHCs during the next 8 months * Drinks more than 1200 mL of tea/coffee/cocoa/cola or other caffeinated beverage per day. * Any condition or finding that in the view of the primary investigator would impede full study participation

Locations (4)

The Center for Pharmaceutical Research

Kansas City, Kansas, United States

Walter Reed Army Institute for Research

Silver Spring, Maryland, United States

St. Louis University

St Louis, Missouri, United States

Coastal Carolina Research Center

Mt. Pleasant, South Carolina, United States

Outcomes

Primary Outcomes

The safety, tolerability and immunogenicity of the Ad4 PA and Ad4 PA GPI vaccines across a range of dosages and schedules.

Safety will be measured by looking at safety labs, Adverse Events (AEs) and vaccine reactogenicity data from Baseline through Day 211. Immunogenicity will be measured by the peak serum antibody response to the PA transgene defined as the highest toxin-neutralizing antibody (TNA) titer achieved by a subject at any time between the first post-vaccination visit though Day 85 (and Day 211 if Day 85 is positive).

Time frame: Day 1 through Day 211

Secondary Outcomes

Antibody response of the Ad4-PA formulation to Ad4 PA GPI

Antibody response will be tested via enzyme-linked immunosorbent assay (ELISA) and the peak PA-ELISA titer defined as the highest ELISA titer achieved by a subject at any time between the first post-vaccination visit and Day 85

Time frame: Day 1 through Day 85 (Day 211 if Day 85 is positive)

Antibody response of the Ad4-PA and Ad4-PA-GPI vaccination regimens to the anticipated AVA PEP regimen.

Antibody response will be tested via ELISA and the peak PA-ELISA titer defined as the highest ELISA titer achieved by a subject at any time between the first post-vaccination visit and Day 85.

Time frame: Days 1 through 85 (Day 211 if Day 85 is positive)

Antibody response induced by 3 different dosages of Ad4 PA and Ad4 PA GPI.

Antibody response will be tested via ELISA and the peak PA-ELISA titer defined as the highest ELISA titer achieved by a subject at any time between the first post-vaccination visit and Day 85 and titers will be compared across the 3 different dosages of Ad4 PA and Ad4 PA GPI (10\^9, 10\^10, 10\^11).

Time frame: Days 1 through 85 (Day 211 if Day 85 is positive)

TNA and antibody response induced by Ad4 PA and Ad4 PA GPI on 3 different vaccination schedules.

Data from ClinicalTrials.gov

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