Study of Novel Types 1 and 3 Oral Poliomyelitis Vaccines

A serious adverse event is any adverse event that resulted in any of the following outcomes: * Death * Was life-threatening * Required inpatient hospitalization or prolongation of existing hospitalization * Resulted in persistent or significant incapacity or substantial disruption of the ability to conduct normal life functions * Congenital anomaly or birth defect * Important medical event that may not result in one of the above outcomes but may jeopardize the health of the study participant and/or require medical or surgical intervention to prevent one of the outcomes listed above

Time frame: From Day 1 to end of study, up to 169 days

Population: The Reactogenicity Population was defined as all participants who provided informed consent and received a study vaccine.

Solicited AEs are pre-specified AEs that are common or known to be associated with vaccination that are actively monitored as potential indicators of vaccine reactogenicity. Solicited AEs for this study included: * Fever (oral temperature ≥ 38.0°C or 100.4°F) * Chills * Fatigue * Headache * Muscle aches/myalgias * Joint aches/arthralgias * Nausea * Vomiting * Abdominal pain * Diarrhea

Time frame: From Day 29 to Day 35

Population: The Reactogenicity Population was defined as all participants who provided informed consent and received a study vaccine. The analysis includes groups / participants who received a 2nd vaccination.

Solicited AEs are pre-specified AEs that are common or known to be associated with vaccination that are actively monitored as potential indicators of vaccine reactogenicity. Solicited AEs for this study included: * Fever (oral temperature ≥ 38.0°C or 100.4°F) * Chills * Fatigue * Headache * Muscle aches/myalgias * Joint aches/arthralgias * Nausea * Vomiting * Abdominal pain * Diarrhea

Time frame: From vaccination to 7 days post vaccination (Days 1-7)

Population: The Reactogenicity Population was defined as all participants who provided informed consent and received a study vaccine.

Unsolicited AEs are any AEs reported spontaneously by the participant, observed by the study personnel during study visits or those identified during review of medical records or source documents. In the absence of a diagnosis, abnormal physical examination findings or abnormal clinical safety laboratory test results that are assessed by the investigator to be clinically significant were reported as an AE.

Time frame: From vaccination to 28 days post vaccination (Day 1-28 for 1st vaccination and Day 29-56 for the 2nd vaccination)

Population: Reactogenicity population; the analysis includes participants who received each vaccination

Samples positive for vaccine virus in stool as detected by PCR were quantified using a cell culture infectious dose assay. Participants who were PCR-positive for type 1 viral shedding but with log₁₀ CCID50 per gram ≤ LLOQ contributed a value equal to the LLOQ. This endpoint was pre-specified to be analyzed in participants with IPV vaccination history.

Time frame: Days 3, 5, 8, 10, 15, 22, 29, 36, 43, 50, and 57

Population: Participants in the Safety population who were PCR-positive for poliovirus type 1 viral shedding and with available CCID50 data. The analysis includes groups with prior IPV history who received vaccination with a type 1 OPV.

Samples positive for vaccine virus in stool as detected by PCR were quantified using a cell culture infectious dose assay. Participants who were PCR-positive for type 3 viral shedding but with log₁₀ CCID50 per gram ≤ LLOQ contributed a value equal to the LLOQ. This endpoint was pre-specified to be analyzed in participants with IPV vaccination history.

Time frame: Days 3, 5, 8, 10, 15, 22, 29, 36, 43, 50, and 57

Population: Participants in the Safety population who were PCR-positive for poliovirus type 3 viral shedding. The analysis includes groups with prior IPV history who received vaccination with a type 3 OPV.

Area under the curve (AUC) was computed for each participant using CCID50 per gram data collected through Day 29 using the linear trapezoidal rule. Participants were assumed to be not shedding at time of vaccination (i.e. there was no stool collection on Day 1). Participants who were PCR-positive for type-specific viral shedding but with log₁₀ CCID50 per gram ≤ LLOQ contributed a value equal to the LLOQ. This endpoint was pre-specified to be analyzed in participants with IPV vaccination history.

Time frame: Days 3, 5, 8, 10, 15, 22, and 29

Population: Participants with available CCID50/g shedding data (must have data from Day 3 and Day 29, and no 2 missing consecutive samples from Days 5, 8, 10, 15, and 22). The analysis includes groups with prior IPV history.

GMT and 95% confidence intervals are maximum likelihood estimates incorporating left and right censoring at the lower limit of quantitation (LLOQ) and ULOQ, respectively.

Time frame: Baseline and Day 29 (28 days post-vaccination)

Population: The Per-Protocol Population (PPP) for immunogenicity was defined as all participants in the Reactogenicity Population who provided a baseline and at least 1 post-vaccination evaluable serum sample and who received correct study vaccinations per randomization with no major protocol deviations that might interfere with the immunogenicity result. The PPP was determined separately for each time point.~The analysis includes groups with prior IPV history who received vaccination with a type 1 OPV.

Time frame: Baseline, Day 29 (28 days after 1st vaccination) and Day 57 (28 days after 2nd vaccination)

Population: The Per-Protocol Population (PPP) for immunogenicity was defined as all participants in the Reactogenicity Population who provided a baseline and at least 1 post-vaccination evaluable serum sample and who received correct study vaccinations per randomization with no major protocol deviations that might interfere with the immunogenicity result. The PPP was determined separately for each time point.~The analysis includes groups with prior OPV history who received vaccination with a type 1 OPV.

Time frame: Baseline and Day 29 (28 days post-vaccination)

Population: The Per-Protocol Population (PPP) for immunogenicity was defined as all participants in the Reactogenicity Population who provided a baseline and at least 1 post-vaccination evaluable serum sample and who received correct study vaccinations per randomization with no major protocol deviations that might interfere with the immunogenicity result. The PPP was determined separately for each time point.~The analysis includes groups with prior IPV history who received vaccination with a type 3 OPV.

Time frame: Baseline, Day 29 (28 days after 1st vaccination) and Day 57 (28 days after 2nd vaccination)

Population: The Per-Protocol Population (PPP) for immunogenicity was defined as all participants in the Reactogenicity Population who provided a baseline and at least 1 post-vaccination evaluable serum sample and who received correct study vaccinations per randomization with no major protocol deviations that might interfere with the immunogenicity result. The PPP was determined separately for each time point.~The analysis includes groups with prior OPV history who received vaccination with a type 3 OPV.

Blood samples collected from participants for type-specific poliovirus neutralizing antibodies were analyzed at the Polio and Picornavirus Laboratory Branch at the United States Centers for Disease Control and Prevention (CDC). For all immunogenicity endpoints, data are presented separately by: * Prior vaccination history (exclusively IPV vs OPV), and * Type-specific poliovirus vaccine received (type 1 vs type 3).

Time frame: Baseline and Day 29 (28 days post-vaccination)

Population: The Per-Protocol Population (PPP) for immunogenicity was defined as all participants in the Reactogenicity Population who provided a baseline and at least 1 post-vaccination evaluable serum sample and who received correct study vaccinations per randomization with no major protocol deviations that might interfere with the immunogenicity result. The PPP was determined separately for each time point.~The analysis includes groups with prior IPV history who received vaccination with a type 1 OPV.

Time frame: Baseline, Day 29 (28 days post-vaccination) and Day 57 (28 days after 2nd vaccination)

Population: The Per-Protocol Population (PPP) for immunogenicity was defined as all participants in the Reactogenicity Population who provided a baseline and at least 1 post-vaccination evaluable serum sample and who received correct study vaccinations per randomization with no major protocol deviations that might interfere with the immunogenicity result. The PPP was determined separately for each time point.~The analysis includes groups with prior OPV history who received vaccination with a type 1 OPV.

Time frame: Baseline and Day 29 (28 days post-vaccination)

Population: The Per-Protocol Population (PPP) for immunogenicity was defined as all participants in the Reactogenicity Population who provided a baseline and at least 1 post-vaccination evaluable serum sample and who received correct study vaccinations per randomization with no major protocol deviations that might interfere with the immunogenicity result. The PPP was determined separately for each time point.~The analysis includes groups with prior IPV history who received vaccination with a type 3 OPV.

Time frame: Baseline, Day 29 (28 days after the 1st vaccination) and Day 57 (28 days after 2nd vaccination)

Population: The Per-Protocol Population (PPP) for immunogenicity was defined as all participants in the Reactogenicity Population who provided a baseline and at least 1 post-vaccination evaluable serum sample and who received correct study vaccinations per randomization with no major protocol deviations that might interfere with the immunogenicity result. The PPP was determined separately for each time point.~The analysis includes groups with prior OPV history who received vaccination with a type 3 OPV.

Presence of the vaccine virus in stool samples was assessed by polymerase chain reaction (PCR). This endpoint was pre-specified to be analyzed in participants with IPV vaccination history.

Time frame: Days 3, 5, 8, 10, 15, 22, 29, 36, 43, 50, and 57

Population: Participants in the Safety Population with available PCR data at each time point. The analysis includes groups with prior IPV history who received vaccination with a type 1 OPV.

Presence of the vaccine virus in stool samples was assessed by polymerase chain reaction (PCR). This endpoint was pre-specified to be analyzed in participants with IPV vaccination history.

Time frame: Days 3, 5, 8, 10, 15, 22, 29, 36, 43, 50, and 57

Population: Participants in the Safety Population with available PCR data at each time point. The analysis includes groups with prior IPV history who received vaccination with a type 3 OPV

* Seroconversion (SCR) is defined as a minimum 4-fold increase in titer from Baseline (pre-vaccination) to 28 days post-vaccination among those participants with a 4-fold increase possible to observe, i.e., with a Baseline titer not greater than 8.5 log₂. * Minimum 2-fold-rise from Baseline to 28 days post-vaccination among those participants with a 2-fold increase possible to observe, i.e., with a Baseline titer not greater than 9.5 log₂. * Any fold-rise is defined as any increase in titer from Baseline to 28 days post-vaccination (log₂ neutralizing antibody titer post-dose minus Baseline \> 0), among those with an increase possible to observe, i.e., with a Baseline titer less than 10.5 log₂.

Time frame: Baseline, Day 29 (28 days post-vaccination) and Day 57 (28 days after 2nd vaccination)

Population: Per Protocol Population; The analysis includes groups with prior OPV history who received vaccination with a type 1 OPV; participants were only included in each analysis if the appropriate measure could be observed based on Baseline neutralizing antibody titer.

* Seroconversion (SCR) is defined as a minimum 4-fold increase in titer from Baseline (pre-vaccination) to 28 days post-vaccination among those participants with a 4-fold increase possible to observe, i.e., with a Baseline titer not greater than 8.5 log₂. * Minimum 2-fold-rise from Baseline to 28 days post-vaccination among those participants with a 2-fold increase possible to observe, i.e., with a Baseline titer not greater than 9.5 log₂. * Any fold-rise is defined as any increase in titer from Baseline to 28 days post-vaccination (log₂ neutralizing antibody titer post-dose minus Baseline \> 0), among those with an increase possible to observe, i.e., with a Baseline titer less than 10.5 log₂.

Time frame: Baseline (pre-vaccination) and Day 29 (28 days post-vaccination)

Population: Per Protocol Population. The analysis includes groups with prior IPV history who received vaccination with a type 1 OPV; participants were only included in each analysis if the appropriate measure could be observed based on Baseline neutralizing antibody titer.

* Seroconversion (SCR) is defined as a minimum 4-fold increase in titer from Baseline (pre-vaccination) to 28 days post-vaccination among those participants with a 4-fold increase possible to observe, i.e., with a Baseline titer not greater than 8.5 log₂. * Minimum 2-fold-rise from Baseline to 28 days post-vaccination among those participants with a 2-fold increase possible to observe, i.e., with a Baseline titer not greater than 9.5 log₂. * Any fold-rise is defined as any increase in titer from Baseline to 28 days post-vaccination (log₂ neutralizing antibody titer post-dose minus Baseline \> 0), among those with an increase possible to observe, i.e., with a Baseline titer less than 10.5 log₂.

Time frame: Baseline, Day 29 (28 days after 1st vaccination) and Day 57 (28 days after 2nd vaccination)

Population: Per Protocol Population; The analysis includes groups with prior OPV history who received vaccination with a type 3 OPV; participants were only included in each analysis if the appropriate measure could be observed based on Baseline neutralizing antibody titer.

* Seroconversion (SCR) is defined as a minimum 4-fold increase in titer from Baseline (pre-vaccination) to 28 days post-vaccination among those participants with a 4-fold increase possible to observe, i.e., with a Baseline titer not greater than 8.5 log₂. * Minimum 2-fold-rise from Baseline to 28 days post-vaccination among those participants with a 2-fold increase possible to observe, i.e., with a Baseline titer not greater than 9.5 log₂. * Any fold-rise is defined as any increase in titer from Baseline to 28 days post-vaccination (log₂ neutralizing antibody titer post-dose minus Baseline \> 0), among those with an increase possible to observe, i.e., with a Baseline titer less than 10.5 log₂.

Time frame: Baseline and Day 29 (28 days post-vaccination)

Population: Per Protocol Population. The analysis includes groups with prior IPV history who received vaccination with a type 3 OPV; participants were only included in each analysis if the appropriate measure could be observed based on Baseline neutralizing antibody titer.

The Shedding Index Endpoint (SIE) was computed as the mean of the log₁₀ cell culture infectious dose 50% (CCID50) per gram from nominal collection days 7, 14, 21, and 28 post-dose (i.e., study days 8, 15, 22, and 29). Participants who were PCR-positive for type-specific viral shedding but with log₁₀ CCID50 per gram ≤ LLOQ contributed a value equal to the LLOQ. This endpoint was pre-specified to be analyzed in participants with IPV vaccination history.

Time frame: Days 8, 15, 22, and 29

Population: Participants with complete data at all four time points (Days 8, 15, 22, and 29) were included in the analysis. The analysis includes groups with prior IPV history.

The presence of the vaccine virus in stool samples was assessed using polymerase chain reaction (PCR). Time to cessation of shedding is defined as the time between vaccination and the last PCR-positive stool prior to 2 consecutive PCR-negative stools (with a minimum 24-hour interval between the 2 negative stools). The time to cessation of fecal shedding of nOPV1 and nOPV3 in prior IPV recipients was estimated using Kaplan-Meier methodology with interval-censoring.

Time frame: Up to Day 57

Population: Participants in the Safety Population with available PCR data; the analysis includes groups with prior IPV history.

The presence of the vaccine virus in stool samples was assessed using polymerase chain reaction (PCR). Time to cessation of shedding is defined as the time between vaccination and the last PCR-positive stool prior to 2 consecutive PCR-negative stools (with a minimum 24-hour interval between the 2 negative stools). The time to cessation of fecal shedding of nOPV1 and nOPV3 in prior OPV recipients was evaluated separately after each dose, estimated using Kaplan-Meier methodology with interval-censoring.

Time frame: From vaccination through 28 days after each vaccination

Population: Participants in the Safety Population with available PCR data at each time point; the analysis includes groups with prior OPV history.