Poliomyelitis Clinical Trial
Official title:
Phase III Clinical Trial to Assess the Immunogenicity of a Sequential Dose of Fractional Inactivated Polio Vaccine (f-IPV) and Oral Polio Vaccine (OPV)
This study is an open-label phase III randomized clinical trial that would compare
immunogenicity after receiving one of five different combinations of polio vaccines. Infants
will be enrolled and randomized at 6 weeks of age to one of five different arms:
A) Three doses of trivalent oral poliovirus vaccine (tOPV) at 6, 10 and 14 weeks of age B)
Three doses of bivalent OPV (bOPV) at 6, 10 and 14 weeks of age C) Two doses of
intramuscular (IM) inactivated poliovirus vaccine (IPV) at 6 and 14 weeks of age D) Two
doses of intra-dermal (ID) fractional IPV (f-IPV) at 6 and 14 weeks of age E) Sequential
administration of ID f-IPV at 6 and 14 weeks of age with bOPV at 10 weeks of age To assess
the immunogenicity of each study vaccine and vaccination schedule, antibody titers against
poliovirus types 1, 2 and 3 will be determined in sera extracted from blood collected before
(at 6 weeks of age) and after receiving 3 doses of study vaccine (18 weeks of age).
Seroconversion will be defined as a titer 4-fold higher than the expected fall in maternally
derived antibodies, assuming a half-life of 28 days. The initial antibody titer at 6 weeks
of age will be used as the starting point for the expected decline in maternal antibody.
This study will compare the immunogenicity of:
1. Sequential dose of intra-dermal f-IPV and bOPV to bOPV alone administered at 6, 10 and
14 weeks of age
2. tOPV to bOPV administered at 6,10 and 14 weeks of age
3. IM IPV to ID f-IPV administered at 6 and 14 weeks of age The answer to these questions
will guide the global polio eradication program in designing new routine immunization
schedule for children that eliminates the risks of paralysis due to vaccine derived
poliovirus (VDPV) from type 2 vaccine poliovirus.
Global polio eradication initiative (GPEI)
In 1988, the World Health Assembly adopted the resolution of polio eradication by 2000. This
launched the Global Polio Eradication Initiative (GPEI), spearheaded by World Health
Organization (WHO), Rotary International, US Centers for Disease Control and Prevention
(CDC) and United Nations Children's Emergency Fund (UNICEF). The major strategies to achieve
polio eradication included: 1) provision of 3-4 doses of tOPV to young infants through
routine immunization programs; 2) provision of additional doses to all children < 5 years of
age through immunization campaigns (supplementary immunization activities or SIAs); 3)
surveillance for all cases of acute flaccid paralysis in children <15 years of age; and 4)
mop-up immunizations campaigns following the detection of poliovirus circulation.
OPV was the vaccine of choice for polio eradication due to its low cost, ease of
administration, ability to induce intestinal immunity and community spread to aid in
induction of immunity.
Limitations of trivalent oral polio vaccine (tOPV)
tOPV is a mixture of all three types of polioviruses and there is interference among the
strains during intestinal replication. Type 2 especially interferes with uptake of types 1
and 3. tOPV has higher seroconversion rates in industrialized countries compared to that in
developing countries. A study conducted in Brazil and Gambia reported tOPV seroconversion
rates of 85% for Type 1, 94% for type 2 and 68% for Type 3 with three doses of tOPV.
Compared to monovalent OPVs, trivalent OPV has lower seroconversion rates. To address
concerns of lower efficacy of tOPV for type 1 and type 3 compared to monovalent vaccines,
monovalent vaccines were re-introduced in the polio eradication initiative. Monovalent OPVs
are more immunogenic than tOPV. In India, compared to two doses of tOPV given at birth and
after 30 days, type-specific seroconversion was significantly higher with two doses of mOPV1
(90% vs. 63%) and mOPV3 (84% vs. 52%). In South Africa, compared to one dose of tOPV given
at birth, type-specific seroconversion was significantly higher with one dose of mOPV1 (73%
vs. 39%) and mOPV3 (58% vs. 21%).
While the higher immunogenicity of monovalent vaccines compared to trivalent vaccine is
highly desirable especially in the presence of a poliovirus outbreak caused by one antigenic
type, the monovalent vaccines increase the complication in vaccine selection. Wild type 2
poliovirus was eradicated in 1999 and at the present time there is global circulation of
wild poliovirus Type 1 and 3. Weak routine immunization with poor immunization coverage will
lead to immunity gaps against all three types of polioviruses. In the presence of Type 1
poliovirus outbreak in a country with weak routine immunization, use of a monovalent Type 1
poliovirus vaccine will contribute to reducing the immunity gap to Type 1 poliovirus,
however, this would not address the existing immunity gap to Type 3 poliovirus and vice
versa. Additionally, in the presence of an outbreak of Type 1 and Type 3 polioviruses,
vaccine selection becomes further complicated. To address these concerns, bivalent OPV
(bOPV), mixture of type 1 and type 3, was introduced in the polio eradication program in
2010. The only published clinical trial on bOPV reported that two doses of bOPV given at
birth and 30 days later was comparable in immunogenicity to two doses of mOPV1 and mOPV3 and
significantly better than two doses of tOPV.
Oral poliovirus vaccines are live attenuated viral vaccines and the vaccine virus in OPV can
mutate and acquire neurovirulence causing paralysis either due to vaccine-associated
paralytic polio (VAPP) or due to circulating vaccine-derived polioviruses (cVDPV), in which
the attenuated vaccine virus not only acquires the ability to cause paralysis but can also
circulate similar to wild poliovirus (WPV). The potential of vaccine virus to acquire
neurovirulence and cause paralytic poliomyelitis is incompatible with eradication of polio.
Therefore, polio eradication will require eventual cessation of all OPVs.
The last case of type 2 WPV (WPV2) was reported in 1999 in India. Type 2 vaccine virus in
tOPV is most likely to cause cVDPVs and over 80% of cVDPVs over the past decade have been
cVDPV2. Of the estimated 250-500 annual VAPP cases almost 40% are due to type 2. Thus, with
the eradication of WPV2 it is imperative to prioritize removal of type 2 containing OPV.
Role of bivalent oral polio vaccine (bOPV) and inactivated polio vaccine (IPV)
The licensing and availability of bivalent OPV (bOPV) containing type 1 and 3 offers the
option of an OPV that does not contain OPV2. No studies have assessed the immunogenicity of
bOPV when administered in the Expanded Program on Immunization (EPI) schedule of 6, 10 and
14 weeks of age. Additionally, no studies have compared the immunogenicity of bOPV to that
of tOPV when administered at 6, 10 and 14 weeks of age. Thus, this comparison has been
proposed in this study with inclusion of a bOPV and a tOPV arm.
At the same time, while a switch in routine immunization from tOPV to bOPV has been
proposed, there are significant challenges that need to be addressed prior to implementing
this possible switch. Removing type 2 OPV from routine immunization will rapidly increase
the proportion of population susceptible to type 2. This is turn could facilitate the
transmission of cVDPV2 from countries experiencing an outbreak of cVDPV2. Ideally, all
cVDPV2 outbreaks will need to be stopped prior to replacement of tOPV with bOPV. Equally
important is the need for synchronization of cessation of type 2 OPV globally or regionally
to reduce the risk of cVDPV2 importation from countries that continue to use tOPV. The IPV
working group of Strategic Advisory Group of Experts on Immunization (SAGE) has endorsed a
set of necessary pre-requisites for type 2 OPV cessation and these include: formal
validation of absence of WPV2, interruption of cVDPV2 prior to OPV2 cessation, laboratory
containment of WPV2, availability of sufficient bOPV for the switch and stockpile of
monovalent oral vaccines (mOPV) for outbreak response. At the same time, there is a clear
recognition that it would take few more years to achieve the necessary pre-requisites while
the balance has already shifted from benefit to risk for type 2 OPV.
Another potential option is to switch from tOPV to IPV but IPV is substantially more
expensive than OPV and is not as immunogenic as OPV in inducing mucosal immunity. Hence, the
polio eradication program is exploring ways to make IPV affordable for polio eradication
that include reducing the number of IPV doses, reducing the antigen content for each dose,
manufacturing IPV in developing countries and optimizing other production processes. One of
the possible methods of reducing the antigen content of each dose of IPV is to use a
fractional injection of IPV (f-IPV) of one-fifth of standard IPV dose given intra-dermally.
Compared to intra-muscular injection of IPV, it appears that f-IPV has sub-optimal
immunogenicity when administered at 6, 10 and 14 weeks of age (EPI schedule) [ID f-IPV vs IM
IPV: Type 1: 53% vs 89%; Type 2: 85% vs 96%; Type 3: 69% vs 99%] though the immunogenicity
is comparable when administered at 2, 4 and 6 months of age [ID f-IPV vs IM IPV: Type 1: 97%
vs 100%; Type 2: 96% vs 100%; Type 3: 98% vs 100%]. Prior studies have reported that the
interval between multiple doses of IPV plays an important role in the immunogenicity of IPV
11. A study conducted in Cuba reported seroconversion rates of 94%, 83% and 100% for Type 1,
2 and 3 respectively with 3 doses of IM IPV administered at 6, 10 and 14 weeks of age. These
seroconversion rates were similar to seroconversion observed after 2 doses of IPV
administered at 8 and 16 weeks of age (Type 1: 90%; Type 2: 89%; Type 3: 90%). Hence, it is
hypothesized that the 1-month interval between the 3 doses in EPI schedule is a major
contributor in the sub-optimal immunogenicity of f-IPV compared to the immunogenicity
reported with the 2, 4 and 6 month schedule, which has a 2-month interval between doses. As
a result in this study the immunogenicity of IM IPV and ID f-IPV administered at 6 and 14
weeks is being assessed where the interval between doses is 2 months.
Justification for this study
There are significant risks associated with switching from tOPV to bOPV in routine
immunization. IM IPV is substantially more expensive than tOPV and not as immunogenic in
inducing mucosal immunity. These are the principal reasons that prevent use of IM IPV in EPI
schedule. ID f-IPV has sub-optimal immunogenicity when used in EPI schedule. Therefore, the
polio program needs to test the immunogenicity of combination of poliovirus vaccines as this
could potentially address concerns of risks of using bOPV alone and suboptimal
immunogenicity of ID f-IPV. Prior studies have shown that IPV and OPV given together as a
combination or sequentially with OPV followed by IPV achieves a higher seroconversion than
IPV or OPV alone and the mucosal immunity induced by combined IPV and OPV is similar to that
induced by OPV. However, seroconversion of sequential f-IPV and bOPV has not yet been
determined. Consequently, this study will assess the immunogenicity of a sequential dose of
f-IPV and bOPV. Combining bOPV and f-IPV in an immunization schedule has multiple
advantages. Firstly, f-IPV will aid in development of Type 2 immunity. Secondly, bOPV
combined with f-IPV is likely to be more immunogenic than f-IPV alone. Finally, bOPV is
likely to contribute substantially to development of Type 1 and 3 mucosal immunity.
Rationale for the location of the study and the study population
Polio immunization in Bangladesh is provided through the Expanded Program on Immunization to
achieve high routine coverage with 3 doses of tOPV in infants younger than 12 months and
through National Immunization Days that are usually conducted twice a year. The 3 doses of
tOPV through routine immunization services is administered to infants at 6, 10 and 14 weeks
of age and WHO/UNICEF estimate coverage of 95% for 2010 with three doses of polio vaccine.
With these strategies, Bangladesh interrupted endemic transmission in 2000 and has
successfully prevented outbreaks or re-establishment of circulation following importations
from neighboring India. With the interruption of polio transmission, Bangladesh is at a
critical juncture where it needs to consider steps to reduce the risks associated with
emergence of VDPV2. Therefore, it is advantageous to test a potential new combination of
existing polio vaccines to reduce risks of VDPV2 emergence in Bangladesh. The results of the
study will be applicable in Bangladesh as well as important for the global polio eradication
program. ICDDR, B has long-standing expertise in conducting clinical trials and has
conducted a polio clinical trial in the proposed site Mirpur, Dhaka. This study reported a
seroconversion of 86% for Type1, 97% for Type 2 and 75% for Type 3 after 3 doses of tOPV at
6, 10 and 14 weeks of age.
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Allocation: Randomized, Endpoint Classification: Efficacy Study, Intervention Model: Parallel Assignment, Masking: Open Label, Primary Purpose: Prevention
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