Influenza Clinical Trial
Official title:
Evaluation of The Safety and Immunogenicity of an Influenza A/H1N1 Vaccine (IVACFLU), Produced by IVAC, in Healthy Adults in Vietnam
The study hypothesis is that two 0.5 ml doses of non-adjuvanted whole virion monovalent A/H1N1 influenza vaccine (IVACFLU)-—each dose with an HA content of 15 mcg from A/California/07/2009 (H1N1)-like virus-—will be safe and immunogenic in healthy adults.
This is a phase I, double-blind, individually-randomized (1:1, vaccine:placebo), controlled
trial with two groups, IVACFLU (A/H1N1) and placebo. Healthy male and female adults 18
through 40 years of age will be invited to participate. In addition to sponsor monitoring of
safety, Program for Appropriate Technology in Health (PATH) will review safety data. Safety
data through 7 days post-dose one for all subjects will be reviewed in a blinded fashion
prior to administration of dose two of study vaccine or placebo. PATH will review all adverse
events (AEs), including clinical laboratory evaluations (pre- and post-vaccination) and will
advise if the volunteers may receive dose two of study vaccine or placebo. For all subjects,
the procedures and timelines are summarized below.
On the day of first screening (S1), about 14 days (between 5 and 30 days) prior to
administration of dose one of study vaccine or placebo, subjects will be screened for
eligibility through medical history review, physical examination, testing for serologic
evidence of chronic viral infection [human immunodeficiency virus (HIV), hepatitis B virus
(HBV) or hepatitis C virus (HCV)], routine biochemical and hematological blood tests and
urinalysis by dipstick. For screening for serologic evidence of chronic viral infections,
appropriate pre- and post-test counseling must be provided.
Subject screening for eligibility will continue and be completed on the second screening day
(S2). This second screening day will occur the same day as scheduled enrollment into the
trial and administration of study vaccine or placebo (Day 0). Women will undergo pregnancy
tests using urine samples on Day 0. Fully eligible subjects will be enrolled into the trial.
At that time, blood specimens will be collected for immunological testing prior to
administration of study vaccine or placebo. Subjects will be unaware of which allocation,
IVACFLU or placebo, is received; study vaccine and placebo will be masked. Subjects will be
carefully monitored for adverse reactions for 60 minutes after vaccination.
During the first week following vaccination, subjects will be asked to record local and
general signs and symptoms using preprinted diary cards, thermometer, and small ruler.
Concomitant medications will also be recorded. In addition to solicited signs, subjects will
be asked to report any other adverse events, whether or not they believe that the event is
related to the vaccination. Member of the investigator's clinical team will visit subjects
one and five days after vaccination to check that subjects are correctly completing the diary
card and to check on the subjects' well-being. Subjects will then return to the study clinic
7 days after dose one. At that time, the investigator will check the subjects' diary cards
and transcribe all adverse events onto the case report forms using medical language. Blood
and urine specimens will also be collected for routine biochemical and hematological blood
tests and urinalysis by dipstick.
Two days before subjects are scheduled to receive dose two, subjects will be visited or
called to remind them of the next visit to the study clinic and to check on the subjects'
well-being. Subjects will return to the study clinic at 3 weeks after administration of dose
one of study vaccine or placebo in order to receive dose two. At that time, interim histories
and concomitant medications will be reviewed. Women will again undergo urine pregnancy tests.
All subjects will undergo collection of blood and urine specimens for routine biochemical and
hematological blood tests and urinalysis by dipstick and collection of blood serum specimens
for immunologic analyses. Then subjects will receive dose two of study vaccine or placebo and
be monitored for 60 minutes.
After receipt of dose two, subjects will again complete diary cards for 7 days after
vaccination with visits by members of the investigator's clinical team again at days one and
five after vaccination to check that the subjects are correctly completing diary cards and to
check on the subjects' well-being. Subjects will then return to the study clinic 7 days after
dose two (Day 28) for review of diary cards by the investigator and collection of blood and
urine specimens for routine biochemical and hematological blood tests and urinalysis by
dipstick.
Two days before the subjects' next scheduled visit at 3 weeks after administration of dose
two, subjects will be visited or called to remind them of the next visit to the study clinic
and to check on the subjects' well-being. Subjects will then return to the study clinic at 3
weeks after administration of dose two (Day 42) of study vaccine or placebo for another study
visit. At that time, interim histories and concomitant medications will again be reviewed and
final blood specimens will be collected for immunogenicity analyses. Women will also undergo
a final pregnancy screen.
Subjects will then be asked to immediately report severe adverse events (SAEs) which occur
from Day 42 to Day 201 (approximately 6 months after receipt of dose two). To facilitate this
reporting, a member of the investigator's team will visit or call the subjects monthly to
check on their well-being. At last study visit on Day 201, subjects will be interviewed and
examined one last time before completing the study.
For the evaluation of serum antibodies (by hemagglutination inhibition and
microneutralization), serum specimens will be collected on Day 0 (prior to administration of
dose one of study vaccine or placebo), on Day 21 (prior to administration of dose two of
study vaccine or placebo) and on Day 42.
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