Immunogenicity and Safety of Hecolin® in HIV Positive/Negative Adults and in Children

April 24, 2025 updated by: International Vaccine Institute

A Phase 2b, Open-label Study to Evaluate the Immunogenicity and Safety of Hecolin® in HIV Positive/Negative Adult Participants Followed by a Randomized, Placebo-controlled, Observer-blind Study to Evaluate the Immunogenicity and Safety of Hecolin® in Children

The primary goal of this clinical trial is to demonstrate non-inferiority of 30 µg of Hecolin® in healthy children, compared to healthy adults as measured by seroresponse rates (SR) of anti-HEV IgG titers, 4 weeks after 3 doses (0, 1 and 6 months) and to assess and descriptively compare safety profile data intra and inter age Strata. As secondary objectives, Geometric Mean Concentration (GMC) of anti-HEV IgG ELISA will be evaluated 4 weeks after 3 doses (0, 1 and 6 months) and 4 weeks after 2 doses (0- and 6-months dose) in healthy children. SR and GMC will also be evaluated 24 weeks after 3 doses and 2 doses. The immune response will be compared among adult participants between HIV positive and HIV negative individuals and between virally suppressed and virally unsuppressed HIV positive individuals

Study Overview

Status

Status

Indicates the current recruitment status or the expanded access status.
Recruiting

Conditions

Conditions

The disease, disorder, syndrome, illness, or injury that is being studied. On ClinicalTrials.gov, conditions may also include other health-related issues, such as lifespan, quality of life, and health risks.

Intervention / Treatment

Intervention / Treatment

A process or action that is the focus of a clinical study. Interventions include drugs, medical devices, procedures, vaccines, and other products that are either investigational or already available. Interventions can also include noninvasive approaches, such as education or modifying diet and exercise.

Detailed Description

The primary objective of the study is to demonstrate immune non-inferiority of 30 µg Hecolin® when given to healthy children (2-17 years) as compared to healthy adults (18-45 years) as measured by seroresponse rates (SR) of anti- HEV IgG ELISA antibody titers, 4 weeks after the 3 doses given at 0, 1- & 6-months. Co-primary objective is to assess safety in each age cohort and descriptively compare lower age cohorts with higher age cohorts. Other immune parameters would be assessed as secondary objectives. Healthy children and adolescents collectively (2-17 years) will be compared for immune non-inferiority with healthy adults (18-45 years) as measured by geometric mean concentration (GMC) of anti-HEV IgG ELISA antibody titers, 4 weeks after the 3 doses given at 0, 1- & 6-months. Among children (2-17 years) 3 doses of Hecolin® given at 0, 1 and 6 months will be compared with 2 doses of Hecolin® given at 1 and 6 months in terms of immune non-inferiority of SR and GMC of anti-HEV IgG ELISA antibody titers. The immune response will be compared between HIV positive and HIV negative adults in terms of SR and GMC as measured by anti-HEV IgG ELISA antibody titers at 4 weeks after completing 3 doses of Hecolin® (0, 1 and 6 months).

A total of 860 participants will be enrolled in the main study and will be divided into 4 age strata; 18-45 years (Cohort A), 12-17 years (Cohort B), 6-11 years (Cohort C) and 2-5 years (Cohort D) having 410, 175, 175 and 100 participants respectively. Cohort A will be further divided into Arm A1 and A2 having 232 HIV -ve and 178 HIV +ve participants respectively. All participants in cohort A will receive intramuscular injection of 3 doses of 30 µg Hecolin® at 0, 1 and 6 months. Cohort B will be further divided into Arm B1, B2 and B3 having 70, 70 and 35 participants respectively. Arm B1 will receive intramuscular injection of 3 doses of 30 µg Hecolin® at 0, 1 and 6 months. Arm B2 will receive intramuscular injection of 2 doses of 30 µg Hecolin® at 0 and 6 months while Arm B3 will receive intramuscular injection of comparator (placebo) intramuscularly at 0, 1 and 6 months. Similarly, Cohort C will be further divided into Arm C1, C2 and C3 having 70, 70 and 35 participants respectively. Arm C1 will receive intramuscular injection of 3 doses of 30 µg Hecolin® at 0, 1 and 6 months. Arm C2 will receive intramuscular injection of 2 doses of 30 µg Hecolin® at 0 and 6 months while Arm C3 will receive intramuscular injection of comparator (placebo) intramuscularly at 0, 1 and 6 months. Cohort D will be further divided into Arm D1, D2 and D3 having 40, 40 and 20 participants respectively. Arm D1 will receive intramuscular injection of 3 doses of 30 µg Hecolin® at 0, 1 and 6 months. Arm D2 will receive intramuscular injection of 2 doses of 30 µg Hecolin® at 0 and 6 months while Arm D3 will receive intramuscular injection of comparator (placebo) intramuscularly at 0,1 and 6 months.

In the main study a total of 6 blood samples for immunogenicity will be collected from all participants at Day 0 (baseline), one month after first vaccination, one month after second vaccination, 6 months after first vaccination, one month after third vaccination, and at 6 months after third vaccination.

Blood samples will be collected at screening and one month after third vaccination from the HIV + arm to document CD4 T cells and HIV Viral load.

Out of the 860 participants enrolled in the main study, 2 additional blood samples after reconsent for the 2-year long term follow up period will be collected at V8 (12 months after 3rd dose) and V9 (24 months after 3rd dose) from any 100 HIV negative adults in Cohort A and from participants in Hecolin arms in Cohorts B, C and D (B1, B2, C1, C2, D1, and D2) for immunogenicity assessment. In the additional 0-1-month dose schedule component/arm, a total of 4 blood samples will be collected from all participants at V2 (Day 0), V3 (28 days after 1st dose), V4 (28 days after 2nd dose), V5 (6 months after 2nd dose), and 2 additional samples will be collected from participants in Hecolin arms in Cohorts B, C and D (B4, C4, and D4) at V6 (12months after 2nd dose), and V7 (24 months after 2nd dose) for immunogenicity assessment.

All participants will be observed at the study site for 30 minutes after each Investigational Product (IP) injection for any reactogenicity events. Local and systemic solicited adverse events will be recorded in a diary card during 7 days after each IP dose while unsolicited adverse events will be recorded during the 4 weeks after each IP injection. Serious adverse events (SAEs), Medically attended adverse events (MAAEs) and Adverse of special interest (AESI) will be recorded during the entire study period i.e., until 6 months post last dose.

Study Type

Study Type

Describes the nature of a clinical study. Study types include interventional studies (also called clinical trials), observational studies (including patient registries), and expanded access.
Interventional

Enrollment (Estimated)

Enrollment

The number of participants in a clinical study. The "anticipated" enrollment is the target number of participants that the researchers need for the study.
1040

Phase

Phase

The stage of a clinical trial studying a drug or biological product, based on definitions developed by the U.S. Food and Drug Administration (FDA). The phase is based on the study's objective, the number of participants, and other characteristics. There are five phases: Early Phase 1 (formerly listed as Phase 0), Phase 1, Phase 2, Phase 3, and Phase 4. Not Applicable is used to describe trials without FDA-defined phases, including trials of devices or behavioral interventions.
  • Phase 2

Contacts and Locations

This section provides the contact details for those conducting the study, and information on where this study is being conducted.

Study Contact

Study Contact

The name and contact information for the person who can answer enrollment questions for a clinical study. Each location where the study is being conducted may also have a specific contact, who may be better able to answer those questions.

Study Contact Backup

Study Locations

  • South Africa
      • Ga-Rankuwa, South Africa
      • Johannesburg, South Africa
        • Recruiting
        • Newtown Clinical Research Centre
        • Contact:
      • Paarl, South Africa
        • Recruiting
        • Be Part Research
        • Contact:

Participation Criteria

Researchers look for people who fit a certain description, called eligibility criteria. Some examples of these criteria are a person's general health condition or prior treatments.

Eligibility Criteria

Eligibility Criteria

The key requirements that people who want to participate in a clinical study must meet or the characteristics they must have. Eligibility criteria consist of both inclusion criteria (which are required for a person to participate in the study) and exclusion criteria (which prevent a person from participating). Types of eligibility criteria include whether a study accepts healthy volunteers, has age or age group requirements, or is limited by sex.

Ages Eligible for Study

  • Child
  • Adult

Accepts Healthy Volunteers

Yes

Description

Inclusion Criteria (healthy participants only):

  1. Healthy participants 2 to 45 years of age at enrollment,
  2. Participants/Parent(s)/LAR who have voluntarily given informed consent/assent,
  3. Participants/Parent(s)/LAR willing to follow the study procedures and available for the entire duration of the study and agrees to the collection of all biospecimens,
  4. HIV negative,
  5. Not pregnant,
  6. Agreement to practice effective contraception for female participants of childbearing potential and non-sterile males until at least 8 months after the first vaccination.
  7. Has practiced adequate contraception or has abstained from all activities that could result in pregnancy for at least 28 days prior to the first dose of vaccine, and
  8. Female participant not currently breastfeeding.

Exclusion Criteria:

An individual who meets any of the following criteria will be excluded from participation in this study:

  1. Has received any hepatitis E vaccine in the past,
  2. Febrile illness (body temperature ≥ 38°C) or acute illness within 3 days prior to the study vaccination,
  3. Known history or allergy to study vaccine components and/or excipients or other medications, or any other allergies or medical history deemed by the investigator to increase the risk of an adverse event if they were to participate in the trial (e.g., Guillain-Barre Syndrome),
  4. Major congenital abnormalities which in the opinion of the investigator may affect the participant's participation in the study,
  5. Known history of immune function disorders including immunodeficiency diseases (known HIV infection or other immune function disorders) and lupus,
  6. Chronic use of systemic steroids (>2 mg/kg/day or >20 mg/day prednisone equivalent for periods exceeding 10 days), cytotoxic or other immunosuppressive drugs within the past 6 weeks,
  7. Any abnormality or chronic disease which in the opinion of the investigator might be detrimental to the safety of the participant and interfere with the assessment of the study objectives,
  8. Behavioral or cognitive impairment, chronic substance abuse, or psychiatric disease or neural disorders, that, in the opinion of the investigator, could interfere with the participant's ability to participate in the trial,
  9. History of splenectomy,
  10. History of thrombocytopenia and/or thrombosis, myocarditis or pericarditis or any other significant cardiac condition,
  11. With a known bleeding diathesis or any condition that may be associated with a prolonged bleeding time resulting in contraindication for IM injections/blood extractions.,
  12. Receipt of blood or blood-derived products in the past 3 months,
  13. Receipt of other vaccines from 4 weeks prior to test vaccination or planned to receive any vaccine within 4 weeks of last dose of study vaccine,
  14. Concomitantly enrolled or scheduled to be enrolled in another trial,
  15. Research staff involved with the clinical study or family/household members of research staff,
  16. Body mass index (BMI) of ≥ 40 in adults and for children a BMI- index-for-age is ≥95th percentile, at the time of the screening visit, or
  17. As per the Investigator's medical judgement, an individual could be excluded from the study despite meeting all inclusion/exclusion criteria mentioned above.

Inclusion criteria for HIV-positive arm:

  1. Adults 18-45 years living with HIV on anti-retroviral (ARV) treatment and willing to have CD4 and viral load measured as per protocol,
  2. Able to provide a voluntary signed informed consent,
  3. Participants willing to follow the study procedures of the study and available for the entire duration of the study and agrees to the collection of all biospecimens,
  4. Agreement to practice effective contraception for female participants of childbearing potential and non-sterile males until at least 3 months after the last vaccination.
  5. Has practiced adequate contraception or has abstained from all activities that could result in pregnancy for at least 28 days prior to the last dose of vaccine, and
  6. Female participant is currently not breastfeeding.

Exclusion Criteria for HIV-positive arm:

An individual who meets any of the following criteria will be excluded from participation in this study:

  1. Has received any hepatitis E vaccine in the past,
  2. Newly diagnosed HIV-positive (diagnosed on screening) on ARVs for 0-4 weeks (Note: These participants can be re-screened and enrolled once they have been on ARVs for 4 weeks),
  3. Febrile illness (body temperature ≥ 38°C) or acute illness within 3 days prior to the study vaccination,
  4. Serious adverse reaction to any vaccine, or any component of the investigational vaccine, including a history of anaphylaxis and symptoms of a severe allergic reaction and history of allergies in the past,
  5. Current hospitalization,
  6. History of inherited blood disorders, heparin-induced thrombocytopenia, or thromboembolic disorders,
  7. History of any blood product transfusion up to 6 months before enrolment,
  8. Receipt of other vaccines from 4 weeks prior to test vaccination or planned to receive any vaccine within 4 weeks of last dose of study vaccine
  9. Currently taking anti-coagulation therapy, or chronic aspirin in the past 3 months,
  10. Pregnant or breastfeeding women throughout the study period,
  11. Extreme obesity (defined as BMI of 40 kg/m2 or higher),
  12. Chronic kidney disease requiring dialysis,
  13. Liver disease (Note mild chronic liver disease is not an exclusion criterion),
  14. Participants with acquired or hereditary immunodeficiencies other than HIV,
  15. History of hereditary, idiopathic, or acquired angioedema,
  16. No spleen or functional asplenia,
  17. Platelet disorder or other bleeding disorder that may cause injection contraindication,
  18. Chronic use (more than 14 continuous days) of any medications that may be associated with impaired immune responsiveness including, but not limited to, systemic corticosteroids exceeding 10 mg/day of prednisone equivalent, allergy injections, immunoglobulin, interferon, or immunomodulators. The use of low dose topical, ophthalmic, inhaled, and intranasal steroid preparations will be permitted,
  19. According to the judgement of the investigator, the participant has any other factors that might interfere with the results of the clinical trial or pose additional risk due to participation in the study,
  20. Assessed by the Investigator to be unable or unwilling to comply with the requirements of the protocol

Study Plan

This section provides details of the study plan, including how the study is designed and what the study is measuring.

How is the study designed?

Design Details

  • Primary Purpose: Prevention
  • Allocation: Randomized
  • Interventional Model: Parallel Assignment
  • Masking: Quadruple

Arms and Interventions

Participant Group / Arm

Participant Group / Arm

A group or subgroup of participants in a clinical trial that receives a specific intervention/treatment, or no intervention, according to the trial's protocol.
Intervention / Treatment

Intervention / Treatment

A process or action that is the focus of a clinical study. Interventions include drugs, medical devices, procedures, vaccines, and other products that are either investigational or already available. Interventions can also include noninvasive approaches, such as education or modifying diet and exercise.
Experimental: Group A1 (Three doses of Hecolin®; HIV negative adults aged 18-45 years)
Three doses of Hecolin® Recombinant Hepatitis E Vaccine administered at 0, 1 and 6 months to HIV negative participants, age 18-45 years old, 232 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Experimental: Group A2 (Three doses of Hecolin®; HIV positive adults aged 18-45 years)
Three doses of Hecolin® Recombinant Hepatitis E Vaccine, administered at 0, 1 and 6 months, to HIV positive participants, age 18-45 years old, 178 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Experimental: Group B1 (Three doses of Hecolin®; healthy adolescents aged 12-17 years)
Three doses of Hecolin® Recombinant Hepatitis E Vaccine, administered at 0, 1 and 6 months, to age 12-17 years old, 70 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Experimental: Group B2 (Two doses of Hecolin®; healthy adolescents aged 12-17 years)
Two doses of Hecolin® Recombinant Hepatitis E Vaccine, administered at 0, 1 and 6 months) and one dose of Placebo, administered at 1-month timepoint, to age 12-17 years old, 70 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Biological: Isotonic Sodium Chloride injection
0.5mL administered intramuscularly
Placebo Comparator: Group B3 (Placebo; healthy adolescents aged 12-17 years)
Three doses of Placebo, administered at 0, 1 and 6 months, to age 12-17 years old, 35 participants
Biological: Isotonic Sodium Chloride injection
0.5mL administered intramuscularly
Experimental: Group C1 (Three doses of Hecolin®; healthy children aged 6-11 years)
Three doses of Hecolin® Recombinant Hepatitis E Vaccine, administered at 0, 1 and 6 months, to age 6-11 years old, 70 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Experimental: Group C2 (Two doses of Hecolin®; healthy children aged 6-11 years)
Two doses of Hecolin® Recombinant Hepatitis E Vaccine, administered at 0 and 6 months and one dose of Placebo, administered at 1-month timepoint, to age 6-11 years old, 70 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Biological: Isotonic Sodium Chloride injection
0.5mL administered intramuscularly
Placebo Comparator: Group C3 (Placebo; healthy children aged 6-11 years)
Three doses of Placebo, administered at 0, 1 and 6 months, to age 6-11 years old, 35 participants
Biological: Isotonic Sodium Chloride injection
0.5mL administered intramuscularly
Experimental: Group D1 (Three doses of Hecolin®; healthy children aged 2-5 years)
Three doses of Hecolin® Recombinant Hepatitis E Vaccine, administered at 0, 1 and 6 months, to age 2-5 years old, 40 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Experimental: Group D2 (Two doses of Hecolin®; healthy children aged 2-5 years)
Two doses of Hecolin® Recombinant Hepatitis E Vaccine, administered at 0 and 6 months and of Placebo, administered at 1-month timepoint, to age 2-5 years old, 40 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Biological: Isotonic Sodium Chloride injection
0.5mL administered intramuscularly
Placebo Comparator: Group D3 (Placebo; healthy children aged 2-5 years)
Three doses of Placebo, administered at 0, 1 and 6 months, to age 2-5 years old, 40 participants
Biological: Isotonic Sodium Chloride injection
0.5mL administered intramuscularly
Experimental: Group B4 (Two doses of Hecolin®; healthy children aged 12-17 years)
Two doses of Hecolin® Recombinant Hepatitis E Vaccine, administered at 0, and 1 month, to age 12-17 years old, 50 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Experimental: Group B5 (Placebo; healthy children aged 12-17 years)
Two doses of Placebo, administered at 0, and 1 month, to age 12-17 years old, 10 participants
Biological: Isotonic Sodium Chloride injection
0.5mL administered intramuscularly
Experimental: Group C4 (Two doses of Hecolin®; healthy children aged 6-11 years)
Two doses of Hecolin® Recombinant Hepatitis E Vaccine, administered at 0, and 1 month, to age 6-11 years old, 50 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Experimental: Group C5 (Placebo; healthy children aged 6-11 years)
Two doses of Placebo, administered at 0, and 1 month, to age 6-11 years old, 10 participants
Biological: Isotonic Sodium Chloride injection
0.5mL administered intramuscularly
Experimental: Group D4 (Two doses of Hecolin®; healthy children aged 2-5 years)
Two doses of Hecolin® Recombinant Hepatitis E Vaccine, administered at 0, and 1 month, to age 2-5 years old, 50 participants
Biological: Hecolin® Recombinant Hepatitis E Vaccine
30㎍/dose, 0.5mL administered intramuscularly
Experimental: Group D5 (Placebo; healthy children aged 2-5 years)
Two doses of Placebo, administered at 0, and 1 month, to age 2-5 years old, 10 participants
Biological: Isotonic Sodium Chloride injection
0.5mL administered intramuscularly

What is the study measuring?

Primary Outcome Measures

Primary Outcome Measures

In a clinical study's protocol, the planned outcome measure that is the most important for evaluating the effect of an intervention/treatment. Most clinical studies have one primary outcome measure, but some have more than one.
Outcome Measure
Measure Description
Time Frame
Seroresponse rate
Time Frame: 4 weeks post third dose of Hecolin®
Seroresponse rate (antibody response greater than four times or more increase of anti-HEV IgG in paired sera) at 4 weeks post third dose of Hecolin® administered at 0, 1 and 6 months to healthy children (2-17 years) as compared to healthy adults (18-45 years)
4 weeks post third dose of Hecolin®
Proportion of immediate adverse events
Time Frame: Within 30 minutes post each dose of vaccination
Proportion of immediate adverse events within 30 minutes post each dose of vaccination in all study participants
Within 30 minutes post each dose of vaccination
Proportion of solicited local and systemic adverse events
Time Frame: Within 7 days post each dose
Proportion of solicited local and systemic adverse events within 7 days post each dose of vaccination in all study participants
Within 7 days post each dose
Proportion of unsolicited adverse events
Time Frame: Within 28 days post each dose
Proportion of unsolicited adverse events within 28 days post each dose of vaccination in all study participants
Within 28 days post each dose
Proportion of SAEs, MAAEs and AESIs
Time Frame: Post dose 1 until 6 months post last dose
Proportion of Serious adverse events (SAEs), Medically attended adverse events (MAAEs) and Adverse events of special interest (AESIs) post dose 1 until 6 months post last dose of vaccination
Post dose 1 until 6 months post last dose

Secondary Outcome Measures

Secondary Outcome Measures

In a clinical study's protocol, a planned outcome measure that is not as important as the primary outcome measure for evaluating the effect of an intervention but is still of interest. Most clinical studies have more than one secondary outcome measure.
Outcome Measure
Measure Description
Time Frame
GMC of anti-HEV IgG
Time Frame: 4 weeks post third dose
GMC of anti-HEV IgG at 4 weeks post third dose of Hecolin® administered at 0, 1 and 6 months to healthy children (2-17 years) as compared to healthy adults (18-45 years)
4 weeks post third dose
SR
Time Frame: 4 weeks post two doses of Hecolin®
SR (antibody response greater than four times or more increase of anti-HEV IgG in paired sera) 4 weeks post two doses of Hecolin® administered at 0, and 6 months as compared to three doses of Hecolin® administered at 0, 1 and 6 months to healthy children (2-17 years)
4 weeks post two doses of Hecolin®
GMC of anti-HEV IgG
Time Frame: 4 weeks post two doses of Hecolin®
GMC of anti-HEV IgG at 4 weeks post two doses of Hecolin® administered at 0, and 6 months as compared to three doses of Hecolin® administered at 0, 1 and 6 months to healthy children (2-17 years)
4 weeks post two doses of Hecolin®
SR and GMC of anti-HEV IgG
Time Frame: 4 weeks post third dose of Hecolin®
SR and GMC of anti-HEV IgG at 4 weeks post third dose of Hecolin® administered at 0, 1 and 6 months in healthy older children (6-17 years) and healthy adults (18-45 years)
4 weeks post third dose of Hecolin®
SR
Time Frame: 24 weeks post two doses of Hecolin®
SR (antibody response greater than four times or more increase of anti-HEV IgG in paired sera) at 24 weeks post two doses of Hecolin® administered at 0, and 6 months as compared to three doses of Hecolin® administered at 0, 1 and 6 months to healthy child
24 weeks post two doses of Hecolin®
GMC of anti-HEV IgG
Time Frame: 24 weeks post two doses of Hecolin®
GMC of anti-HEV IgG at 24 weeks post two doses of Hecolin® administered at 0, and 6 months as compared to three doses of Hecolin® administered at 0, 1 and 6 months to healthy children (2-17 years)
24 weeks post two doses of Hecolin®
SR
Time Frame: 4 weeks post third dose of Hecolin®
SR (antibody response greater than four times or more increase of anti-HEV IgG in paired sera) at 4 weeks post third dose of Hecolin® administered at 0, 1 and 6 months to HIV-positive adults as compared to HIV-negative healthy adults (18-45 years)
4 weeks post third dose of Hecolin®
GMC of anti-HEV IgG
Time Frame: 4 weeks post third dose of Hecolin®
GMC of anti-HEV IgG at 4 weeks post third dose of Hecolin® administered at 0, 1 and 6 months to HIV-positive adults as compared to HIV-negative healthy adults (18-45 years)
4 weeks post third dose of Hecolin®
SR
Time Frame: 4 weeks post third dose of Hecolin®
SR (antibody response greater than four times or more increase of anti-HEV IgG in paired sera) at 4 weeks post third dose of Hecolin® administered at 0, 1 and 6 months to virally suppressed (CD4 count < 350) and virally unsuppressed (CD4 count ≥ 350) HIV-positive adults (18-45 years)
4 weeks post third dose of Hecolin®
GMC of anti-HEV IgG
Time Frame: 4 weeks post third dose of Hecolin®
MC of anti-HEV IgG at 4 weeks post third dose of Hecolin® administered at 0, 1 and 6 months to virally suppressed (CD4 count < 350) and virally unsuppressed (CD4 count ≥ 350) HIV-positive adults (18-45 years)
4 weeks post third dose of Hecolin®
SR
Time Frame: 4 weeks post first, second and third dose of Hecolin® /Placebo
SR (antibody response greater than four times or more increase of anti-HEV IgG in paired sera) at 4 weeks post first, second and third dose of Hecolin® /Placebo administered at 0, 1 and 6 months in healthy children (12-17 years), (6-11 years), (2-5 years) and adults (18-45 years) individually
4 weeks post first, second and third dose of Hecolin® /Placebo
GMC of anti-HEV IgG
Time Frame: 4 weeks post first, second and third dose of Hecolin® /Placebo
GMC of anti-HEV IgG at 4 weeks post first, second and third dose of Hecolin® /Placebo administered at 0, 1 and 6 months in healthy children (12-17 years), (6-11 years), (2-5 years) and adults (18-45 years) individually
4 weeks post first, second and third dose of Hecolin® /Placebo
SR and GMC of anti-HEV IgG
Time Frame: 4 weeks post first, second and third dose of Hecolin® /Placebo
SR and GMC of anti-HEV IgG at 4 weeks post first, second and third dose of Hecolin® /Placebo administered at 0, 1 and 6 months in healthy children (12-17 years), (6-11 years), (2-5 years) and adults (18-45 years) collectively and individually as per sero- status at baseline.
4 weeks post first, second and third dose of Hecolin® /Placebo
GMC of anti-HEV IgG for additional 0-1 dose schedule
Time Frame: 4 weeks post first, second of Hecolin
GMC of anti-HEV IgG at 4 weeks post two doses of Hecolin® administered at 0 and 1 months as compared to three doses of Hecolin® administered at 0, 1 and 6 months to healthy children (2-17 years)
4 weeks post first, second of Hecolin
GMC of anti-HEV IgG for additional 0-1 dose schedule
Time Frame: 4 weeks post first, second and third dose of Hecolin® /Placebo
SR and GMC of anti-HEV IgG in paired sera at 4 weeks post each dose of Hecolin® /Placebo when administered two doses at 0 and 1 months or at 0 and 6 months or three doses at 0, 1 and 6 months in individual age groups in healthy children (12 - 17 years, 6 - 11 years, and 2 - 5 years) or three doses at 0, 1 and 6 months in adults (18 - 45 years).
4 weeks post first, second and third dose of Hecolin® /Placebo
SR and GMC of anti-HEV IgG for additional 0-1 dose schedule
Time Frame: 4 weeks post first, second and third dose of Hecolin® /Placebo
SR and GMC of anti-HEV IgG in paired sera at 4 weeks post each dose of Hecolin® /Placebo when administered two doses at 0 and 1 months or at 0 and 6 months or three doses at 0, 1 and 6 months in individual age groups in healthy children (12 - 17 years, 6 - 11 years, and 2 - 5 years) or three doses at 0, 1 and 6 months in adults (18 - 45 years).
4 weeks post first, second and third dose of Hecolin® /Placebo
SR and GMC of anti-HEV IgG for additional 0-1 dose schedule
Time Frame: 24 weeks post two doses of Hecolin®
SR (antibody response greater than four times or more increase of anti-HEV IgG in paired sera) at 24 weeks post two doses of Hecolin® administered at 0-, and 1- month in healthy children (2-17 years).
24 weeks post two doses of Hecolin®
SR and GMC of anti-HEV IgG for additional long-term follow up component
Time Frame: 1 and 2 years post two doses of Hecolin®
SR and GMC (defined as the percentage of participants with anti-HEV IgG antibodies above the detection limit, assessed at 1 year and 2 years post two doses of Hecolin® administered in healthy children (2-17 years) at 0- & 6-months or at 0- & 1-month or post 3 doses (0, 1 & 6 month) in healthy children (2-17 years) and healthy adults (18-45 years)
1 and 2 years post two doses of Hecolin®

Other Outcome Measures

Other Outcome Measures

For clinical trials, a planned measurement described in the protocol that is used to determine the effect of an intervention/treatment on participants. For observational studies, a measurement or observation that is used to describe patterns of diseases or traits, or associations with exposures, risk factors, or treatment. Types of outcome measures include primary outcome measure and secondary outcome measure.
Outcome Measure
Measure Description
Time Frame
SR and GMC of anti-HEV IgG
Time Frame: 4 weeks post first, second and third dose of Hecolin® /Placebo
SR and GMC of anti-HEV IgG at 4 weeks post first, second and third dose of Hecolin® /Placebo administered at 0, 1 and 6 months in healthy children (12-17 years), (6-11 years), (2-5 years) and adults (18-45 years) collectively and individually as per gender distribution
4 weeks post first, second and third dose of Hecolin® /Placebo
Safety in all participants as per gender distribution and serostatus
Time Frame: 1. Within 30 minutes post each dose of vaccination. 2. Within 7 days post each dose of vaccination. 3. Within 28 days post each dose of vaccination. 4.Until 6 months post last dose of vaccination.
  1. Proportion of immediate adverse events within 30 minutes post each dose of vaccination in all study participants.
  2. Proportion of solicited local and systemic adverse events within 7 days post each dose of vaccination in all study participants.
  3. Proportion of unsolicited adverse events within 28 days post each dose of vaccination in all study participants.
  4. Proportion of Serious adverse events (SAEs), Medically attended adverse events (MAAEs) and Adverse of special interest (AESI) until 6 months post last dose of vaccination.
1. Within 30 minutes post each dose of vaccination. 2. Within 7 days post each dose of vaccination. 3. Within 28 days post each dose of vaccination. 4.Until 6 months post last dose of vaccination.
Safety profile intra and inter age strata
Time Frame: 1. Within 30 minutes post each dose of vaccination. 2. Within 7 days post each dose of vaccination. 3. Within 28 days post each dose of vaccination. 4.Until 6 months post last dose of vaccination
  1. Proportion of immediate adverse events within 30 minutes post each dose of vaccination in all study participants.
  2. Proportion of solicited local and systemic adverse events within 7 days post each dose of vaccination in all study participants.
  3. Proportion of unsolicited adverse events within 28 days post each dose of vaccination in all study participants.
  4. Proportion of Serious adverse events (SAEs), Medically attended adverse events (MAAEs) and Adverse events of special interest (AESI) post dose 1 until 6 months post last dose of vaccination.
1. Within 30 minutes post each dose of vaccination. 2. Within 7 days post each dose of vaccination. 3. Within 28 days post each dose of vaccination. 4.Until 6 months post last dose of vaccination

Collaborators and Investigators

This is where you will find people and organizations involved with this study.

Sponsor

Sponsor

The organization or person who initiates the study and who has authority and control over the study.
International Vaccine Institute

Collaborators

Collaborators

An organization other than the sponsor that provides support for a clinical study. This support may include activities related to funding, design, implementation, data analysis, or reporting.
Bill and Melinda Gates Foundation
Xiamen Innovax Biotech Co., Ltd

Investigators

Investigators

A researcher involved in a clinical study. Related terms include site principal investigator, site sub-investigator, study chair, study director, and study principal investigator.
  • Principal Investigator: Tarun Saluja, International Vaccine Institute
  • Principal Investigator: Sanet Aspinall, Ardent Consulting (Pty) Ltd
  • Principal Investigator: Elizabeth Hellström, Be Part Research
  • Principal Investigator: Maphoshane Nchabeleng, MeCRU Clinical Research Unit
  • Principal Investigator: Essack Mitha, Newtown Clinical Research Centre

Study record dates

These dates track the progress of study record and summary results submissions to ClinicalTrials.gov. Study records and reported results are reviewed by the National Library of Medicine (NLM) to make sure they meet specific quality control standards before being posted on the public website.

Study Major Dates

Study Start (Actual)

Study Start

The actual date on which the first participant was enrolled in a clinical study. The "anticipated" study start date is the date that the researchers think will be the study start date.
April 4, 2024

Primary Completion (Estimated)

Primary Completion

The date on which the last participant in a clinical study was examined or received an intervention to collect final data for the primary outcome measure. Whether the clinical study ended according to the protocol or was terminated does not affect this date. For clinical studies with more than one primary outcome measure with different completion dates, this term refers to the date on which data collection is completed for all the primary outcome measures. The "anticipated" primary completion date is the date that the researchers think will be the primary completion date for the study.
January 1, 2026

Study Completion (Estimated)

Study Completion

The date on which the last participant in a clinical study was examined or received an intervention/treatment to collect final data for the primary outcome measures, secondary outcome measures, and adverse events (that is, the last participant's last visit). The "anticipated" study completion date is the date that the researchers think will be the study completion date.
January 1, 2026

Study Registration Dates

First Submitted

First Submitted

The date on which the study sponsor or investigator first submitted a study record to ClinicalTrials.gov. There is typically a delay of a few days between the first submitted date and the record's availability on ClinicalTrials.gov (the first posted date).
February 18, 2024

First Submitted That Met QC Criteria

First Submitted That Met QC Criteria

The date on which the study sponsor or investigator first submits a study record that is consistent with National Library of Medicine (NLM) quality control (QC) review criteria. The sponsor or investigator may need to revise and submit a study record one or more times before NLM's QC review criteria are met. It is the responsibility of the sponsor or investigator to ensure that the study record is consistent with the NLM QC review criteria.
March 5, 2024

First Posted (Actual)

First Posted

The date on which the study record was first available on ClinicalTrials.gov after National Library of Medicine (NLM) quality control (QC) review has concluded. There is typically a delay of a few days between the date the study sponsor or investigator submitted the study record and the first posted date.
March 12, 2024

Study Record Updates

Last Update Posted (Actual)

Last Update Posted

The most recent date on which changes to a study record were made available on ClinicalTrials.gov. There may be a delay between when the changes were submitted to ClinicalTrials.gov by the study's sponsor or investigator (the last update submitted date) and the last update posted date.
April 29, 2025

Last Update Submitted That Met QC Criteria

Last Update Submitted That Met QC Criteria

The most recent date on which the study sponsor or investigator submitted changes to a study record that are consistent with National Library of Medicine (NLM) quality control (QC) review criteria. It is the responsibility of the sponsor or investigator to ensure that the study record is consistent with the NLM QC review criteria.
April 24, 2025

Last Verified

Last Verified

The most recent date on which the study sponsor or investigator confirmed the information about a clinical study on ClinicalTrials.gov as accurate and current. If a study with a recruitment status of recruiting; not yet recruiting; or active, not recruiting has not been confirmed within the past 2 years, the study's recruitment status is shown as unknown.
April 1, 2025

More Information

Terms related to this study

Additional Relevant MeSH Terms

Other Study ID Numbers

Other Study ID Numbers

Identifiers or ID numbers other than the NCT number that are assigned to a clinical study by the study's sponsor, funders, or others. These numbers may include unique identifiers from other trial registries and National Institutes of Health grant numbers.
  • IVI Hecolin S001

Plan for Individual participant data (IPD)

Plan to Share Individual Participant Data (IPD)?

NO

Drug and device information, study documents

Studies a U.S. FDA-regulated drug product

No

Studies a U.S. FDA-regulated device product

No

This information was retrieved directly from the website clinicaltrials.gov without any changes. If you have any requests to change, remove or update your study details, please contact register@clinicaltrials.gov. As soon as a change is implemented on clinicaltrials.gov, this will be updated automatically on our website as well.

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