Prospective registration

Phase III clinical study for freeze-dried Haemophilus influenzae type b combined vaccine

Evaluation of immunogenicity and safety of lyophilized Haemophilus influenzae type b combined vaccine

Fang Wenjian 

Ma Jingchen 

22 Tongji Road North, Economic and Technological Development Zone, Beijing, China

97 Huai'an Road East, Shijiazhuang, Hebei, China

Beijing Zhifei Lvzhu Biopharmaceutical Co., Ltd.

Hebei Center for Disease Control and Prevention

Yes

Ethics Committee of Hebei Center for Disease Control and Prevention

Guo Yu

97 Huaian Road East, Shi-Jia-Zhuang, Hebei, China

Hebei Center for Disease Control and Prevention

97 Huaian Road East, Shi-Jia-Zhuang, Hebei, China

Beijing Zhifei Lvzhu Biopharmaceutical Co., Ltd.

Invasive infection caused by Haemophilus influenzae type B (including meningitis, pneumonia, septicemia, cellulitis, arthritis, epiglottis, etc.)

Interventional study

3

Parallel 

Immunogenic objectives: Main objectives: 1. It was proved that 30 days after three doses of test vaccine or control vaccine were inoculated with 0,1,2 months program in infants of 2-5 months old, the positive rate (≥ 0.15 μ g / ml) of antibody in the test group (lyophilized Haemophilus influenzae B combined vaccine) was not inferior to that in the control group, and the non inferior value was - 10%; 2. It was proved that the long-term protection rate (≥ 1.0 μ g / ml) of antibody in the experimental group (lyophilized Haemophilus influenzae B combined vaccine) was not inferior to that in the control group, and the non inferiority threshold was - 10% 30 days after three doses of experimental vaccine or control vaccine were inoculated with 0,1,2-month program in infants of 2-5 months old. Secondary objectives: 1. Describe and analyze the antibody positive rate, antibody positive rate (quadruple increase), long-term protection level antibody positive rate (quadruple increase) and geometric mean concentration (GMC) of the whole population 30 days after the infants were inoculated with three doses of test vaccine or control vaccine in 0, 1 and 2 months; Describe and analyze the antibody positive rate, antibody long-term protection rate and antibody GMC in the population with antibody concentration < 0.15 μ g / ml, antibody positive rate, antibody positive rate (quadruple growth), antibody positive rate (quadruple growth) and GMC in the whole population 30 days after the 6-11 month old infants were inoculated with two doses of test vaccine or control vaccine in 0 and 1 month procedures; 2. Describe and analyze the antibody positive rate, antibody long-term protection rate and antibody GMC in the population with antibody concentration < 0.15 μ g / ml, antibody positive rate, antibody positive rate (4-fold increase), antibody positive rate (4-fold increase) and GMC in the whole population 30 days after 1-5-year-old children are inoculated with 1 dose of test vaccine or control vaccine; 3. To describe and analyze the antibody positive rate, antibody long-term protection rate and GMC of the population aged 2-5 months and 6-11 months at the age of 18 months, and to evaluate the antibody positive rate, antibody long-term protection rate and GMC 30 days after the completion of one dose of experimental vaccine.

Basic immune stage:
(1) People aged 2 months and above, including 18 years and above and 6-17 years old, are limited to pretest;
(2) 2-11 month old infants should be full-term (37-42 weeks of gestation) and the birth weight should reach the standard (weight 2500g to 4000g);
(3) Women of childbearing age were not pregnant (negative urine pregnancy test), were not breastfeeding and had no birth plan within the first month after selection;
(4) Axillary temperature <=37.0 degree C;
(5) I / the legal guardian voluntarily participate and sign the informed consent;
(6) According to the opinion of the investigator, the subject and / or the legal guardian of the subject can comply with the requirements of the clinical trial scheme;
(7) 2-11 months old has not been vaccinated with any unit price or combined with Haemophilus influenzae B vaccine, 1-5 years old has not been immunized with any unit price or combined with Haemophilus influenzae B vaccine.
Strengthening immunity stage:
(1) At the age of 2-5 months and 6-11 months, infants and young children who were enrolled in the clinical trial and now aged 18 months were enrolled;
(2) Those who have completed basic immunization in this clinical trial;
(3) According to the opinion of the investigator, the legal guardian of the subject can comply with the requirements of the clinical trial scheme.

Basic immune stage:

(1) Have a history of serious allergic reactions requiring medical intervention (such as swelling of the mouth and throat, dyspnea, hypotension or shock); have a history of allergy to vaccines or vaccine ingredients or other serious adverse reactions to vaccines;

(2) Definite diagnosis of thrombocytopenia or other coagulation disorders may lead to the contraindication of intramuscular injection;

(3) Abnormal birth process, asphyxia rescue history, or congenital malformations, developmental disorders or serious chronic diseases;

(4) Severe cardiovascular, hepatorenal and other diseases, hypertension (systolic blood pressure ≥ 140mmHg and / or diastolic blood pressure ≥ 90mmHg, applicable to the group aged 18 years and over in the pre test stage), or congenital abnormality and HIV infection or parents with HIV infection;

(5) Congenital or acquired immune deficiency, and receiving immunosuppressant treatment after birth or within the last 3 months, such as long-term application of systemic glucocorticoid treatment (systemic glucocorticoid treatment, such as prednisone or similar drugs, has been applied for more than 2 weeks);

(6) Patients with encephalopathy, epilepsy, convulsion and other progressive nervous system diseases;

(7) The subjects had acute disease, severe chronic disease or were in the acute phase of chronic disease;

(8) Plans to participate or is participating in any other drug clinical study;

(9) Immunoglobulin and / or any blood products were given within 3 months before admission;

(10) According to the investigator's judgment, the subject has any other factors that are not suitable for the clinical trial.

Strengthening immunity stage:

(1) After the completion of basic immunization, the subjects were inoculated with any monovalent or combined Haemophilus influenzae type B combined vaccine before blood sampling;

(2) After participating in this clinical trial, the subjects have been known or suspected to have immunologic functional defects, including being treated with immunosuppressive drugs (such as radiotherapy, chemotherapy, corticosteroids, antimetabolic drugs, cytotoxic drugs, etc.) and HIV infection;

(3) Immunoglobulins and / or any blood products were given within 3 months before the enhancement of immunity;

(4) According to the investigator's judgment, the subject has any other factors that are not suitable for the clinical trial.

Pre experimental randomization is not applicable. Phase III clinical trial Phase III clinical trial plans to enroll 1700 subjects, and adopt the area group random method by age stratification (including 2-5 months old, 6-11 months old, 1-5 years old). Each age group and the control group are randomized accord

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This data includes the original records, Electronic Data Capture System, the data will be stored in the qualifying data archives. The EDC will be used to entry and manage the participant data