The primary aim of this open-label, randomized control trial is to compare the immunogenicity at week 28 after 20µg HBV vaccine (at week 0, 4, 24) versus 40µg HBV vaccine (40-µg at week 0, 4, 24 week) among HIV-positive patients or HIV-negative MSM who were born in Taiwan after July 1986 and tested negative for all HBV serological markers. The secondary aims are to assess the safety of double-dose HBV vaccination, the proportions of high-level responders (anti-HBs antibody \>100 mIU/ml) at weeks 28 and 48, the serological responses at week 48, and incident HBV infection (indicated by appearance of anti-HBc and/or HBsAg) at week 48.
I. Study procedures: 1. Well explain, complete inform and consent documents 2. A blood test for hepatitis B surface antigen (HBsAg), anti-hepatitis B surface antibody (anti-HBs antibody), anti-hepatitis B core antibody (anti-HBc antibody), anti-HCV and RPR will be performed first. 3. The patients with all negative seromarkers (within 1 month) will be allocated to two groups (random blank=4), a standard-dose booster of 20µg and a double-dose booster of 40µg. For patients receiving 40µg, two 20µg of vaccines are injected at both sides of deltoid muscles. The schedules of booster vaccination are the same in two groups, which is at 0, 1, 6 months. 4. To detect and manage possible immediate and severe allergic reaction, patients who received vaccination will be observed for 30 minutes after injection. 5. The solicited adverse effect will be recorded on the diary card if occurred in 7 days after each dose of vaccination. 6. The titer of hepatitis B surface antibody will be examined before booster vaccination, at the 4th week, the 24th week, 28th week, 48th week. By comparing the responses in the two groups, the effect of different doses of booster vaccination can be evaluated. For those HIV-negative individuals at baseline, HIV screening test will be evaluated every 6 months during the study, at the 24th week, the 48th. 7. To screen the acquisition of hepatitis B, the anti-HBc antibody and HBsAg will be examined at the 48th week 8. To screen the acquisition of hepatitis C and syphilis, anti-HCV and RPR will be examined at the 24th week, the 48th week 9. The results of the study will be informed by phone or the physician during the follow-up care. 10. The serum/blood samples will be preserved in the research lab of the department of internal medicine and kept for 20 years. During this period, the sample will be applied or used in other studies after the patients and the Research Ethics Committee both agreed. 11. During the follow-up care, the treatment or record of hospitalization will be recorded or reviewed. 12. The participants will drop out of clinical trial when protocol violation occurred or the participant is not willing to continue.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
PREVENTION
Masking
NONE
Enrollment
575
The vaccine contains HBsAg which was produced by genetic engineering yeast. It stimulates the active immunity generated by human immune system toward the HBsAg.
National Taiwan University Hospital
Taipei, Taiwan
RECRUITINGVaccine efficacy
The proportion of patients with Anti-HBs antibody higher than 10mIU/ml
Time frame: week 28
High-titer response
The proportion of patients with Anti-HBs antibody higher than 100mIU/ml
Time frame: week 28
Long-term efficacy
The proportion of anti-HBs antibody titers higher than 10mIU/ml
Time frame: 48 weeks
Long-term high-titer response
The proportion of anti-HBs antibody titers higher than 100mIU/ml
Time frame: 48 weeks
Hepatitis B incident infection rate
new HBsAg and anti-HBc antibody seroconversion
Time frame: 48 weeks,
Hepatitis C infection and syphilis infection rate
new hepatitis C infection and syphilis infection
Time frame: at 24 week, 48 weeks
HIV seroconversion among HIV-negative MSM
new HIV seroconversion among HIV-negative MSM
Time frame: at 24 weeks, 48 weeks
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