Study to Evaluate GR1801's Efficacy and Safety
- Conditions
- Rabies Post-exposure Prophylaxis
- Interventions
- Registration Number
- NCT05846568
- Lead Sponsor
- Genrix (Shanghai) Biopharmaceutical Co., Ltd.
- Brief Summary
The goal of this clinical trial is to compare the efficacy and safety of GR1801 injection with Human Rabies Immunoglobulin(HRIG) in patients with WHO Category 3 rabies exposure.
Patients will receive GR1801 injection or HRIG. Each group will receive rabies vaccine as the WHO Essen regime after Study Drug.
- Detailed Description
This is a randomized, double-blind, Human Rabies Immunoglobulin(HRIG) controlled Phase III clinical trial evaluating the efficacy, safety, pharmacokinetic and immunogenicity of GR1801 injection as a part of post-exposure prophylaxis (PEP) in patients with WHO Category 3 rabies exposure who have met all inclusion/exclusion criteria for their treatment group.
1200 patients aged 18 and above with WHO Category III rabies exposure should be enrolled as planned and randomly assigned to the experimental group and the control group based on a ratio of 3: 1. The random stratification factors include time of exposure (within or beyond 24 hours), bite location (above or below the neck), and number of bites (1 or more).
All the patients should receive wound infiltration injection of GR1801 or HRIG on Study Day 0 (wound conditions should be described and recorded both before and post injection by photos, including diameter, depth, expansion treatment, etc.), and should also receive intramuscular injection of one dose of the freeze-dried rabies vaccine for human use (Vero cells) into the deltoid muscle after the infiltration injection. Patients should also be given one dose of the freeze-dried rabies vaccine for human use (Vero cells) on Study Days 3, 7, 14, and 28 respectively according to the WHO Essen regime.
Rabies virus neutralizing antibodies (RVNA) should be collected 9 times from each subject prior to administration and on Study Day1, 3, 5, 7, 14, 42, 90, 365 post administration of Study Drug. RVNA should be assayed through rapid fluorescence focus inhibition test (RFFIT). The occurrence of rabies and survival conditions should be collected through every follow-up visit.
Adverse events should be classified in accordance with solicited adverse events and unsolicited adverse events. Solicited adverse events include local adverse events (such as injection sites pain, induration, swelling, redness, rash and pruritus) and systemic adverse events (such as fever, hypersensitivity, headache, fatigue, nausea, vomiting, arthralgia and myalgia). Unsolicited adverse events are those except solicited adverse events or solicited adverse events beyond 7 days after the first administration.
Solicited adverse events should be collected 7 days after the first administration. Unsolicited adverse events should be collected in 3 months after the first administration and serious adverse events(SAE) should be collected throughout the trial.
Recruitment & Eligibility
- Status
- RECRUITING
- Sex
- All
- Target Recruitment
- 1200
- Chinese males or females aged 18 years or above on Study Day 0 with legal identification documents and plan to live in the local area during the study;
- WHO Category III rabies exposure;
- Those who have an armpit temperature ≤ 37.0 °C;
- Completed written informed consent process, signed the informed consent forms and Agreed to complete all follow-ups.
- WHO Category III rabies exposure but received wound suture treatment;
- WHO Category III rabies exposure over 72 hours;
- Previous receipt of rabies vaccination or rabies passive immunization;
- History of bitten by animals such as dogs, cats, bats etc. within the 6 months before the Study Day 0;
- History of any severe allergy for vaccination;
- Had fever (armpit temperature ≥ 38.5 °C) or received any antipyretic, analgesic or anti-allergic drug within 3 days before Study Day 0;
- History of severe autoimmune diseases;
- History of any severe neurological disease;
- History of receiving any immunoglobulin or vaccine within 30 days before Study Day 0, or plan to use any such product during the study;
- History of addiction to any narcotic, alcohol or drugs;
- Previous receipt of any study product (drug, vaccine, biological product or device) within 6 months before Study Day 0, or plan to participate in any other clinical study during this study period;
- Females who are pregnant or with urine pregnancy test positive.
Study & Design
- Study Type
- INTERVENTIONAL
- Study Design
- PARALLEL
- Arm && Interventions
Group Intervention Description Control Group:HRIG(BOYA-BIO)+Rabies vaccine(CHENGDA PHARMACEUTICALS) Rabies Vaccine HRIG is administered by wound infiltration injection or by intramuscular injection. Dosage form: 200 IU/2mL/vial, liquid, Dosage: 20 IU/kg, Frequency/duration: at Day 0. Rabies vaccine should be administered in deltoid muscle Dosage form: \>=2.5 IU, freeze-dried vaccine, 0.5 mL after reconstitution, Frequency/duration: at Day 0, 3, 7, 14, 28. Control Group:HRIG(BOYA-BIO)+Rabies vaccine(CHENGDA PHARMACEUTICALS) Human Rabies Immunoglobulin(HRIG) HRIG is administered by wound infiltration injection or by intramuscular injection. Dosage form: 200 IU/2mL/vial, liquid, Dosage: 20 IU/kg, Frequency/duration: at Day 0. Rabies vaccine should be administered in deltoid muscle Dosage form: \>=2.5 IU, freeze-dried vaccine, 0.5 mL after reconstitution, Frequency/duration: at Day 0, 3, 7, 14, 28. Experimental Group: GR1801+Rabies vaccine(CHENGDA PHARMACEUTICALS) Rabies Vaccine GR1801 injections are administered by wound infiltration injection or by intramuscular injection.GR1801 injections are a bispecific monoclonal antibody that exhibit a wide spectrum of activity against various wild-type rabies strains in vitro. Dosage form:2mg/1mL/vial, liquid, Dosage: 0.05mg/kg of GR1801 Frequency/duration: at Day 0. Rabies vaccine should be administered in deltoid muscle Dosage form: \>=2.5 IU, freeze-dried vaccine, 0.5 mL after reconstitution, Frequency/duration: at Day 0, 3, 7, 14, 28. Experimental Group: GR1801+Rabies vaccine(CHENGDA PHARMACEUTICALS) GR1801 GR1801 injections are administered by wound infiltration injection or by intramuscular injection.GR1801 injections are a bispecific monoclonal antibody that exhibit a wide spectrum of activity against various wild-type rabies strains in vitro. Dosage form:2mg/1mL/vial, liquid, Dosage: 0.05mg/kg of GR1801 Frequency/duration: at Day 0. Rabies vaccine should be administered in deltoid muscle Dosage form: \>=2.5 IU, freeze-dried vaccine, 0.5 mL after reconstitution, Frequency/duration: at Day 0, 3, 7, 14, 28.
- Primary Outcome Measures
Name Time Method To evaluate the Geometric mean RVNA Concentration (accessd by Rapid Fluorescent Foci Inhibition Test(RIFFIT)) for GR1801 recipients is non-inferior to the Geometric mean RVNA Concentration for HRIG recipients on Study Day 7. 7 days RVNA(Rabies Virus Neutralizing Antibodies) geometric mean concentration of GR1801 recipients and HRIG recipients in combination with rabies vaccines.
To evaluate the rabies post-exposure protection rate for GR1801 recipients is non-inferior to the protection rate for HRIG recipients on Study Day 365. 365 days The percentage of subjects with no case of rabies death in GR1801 recipients and HRIG recipients in combination with rabies vaccines.
To evaluate the percentage of subjects with RVNA concentration ≥ 0.5 IU/mL on Study Day 14 in GR1801 recipients is non-inferior to the percentage of subjects with RVNA concentration ≥ 0.5 IU/mL for HRIG. 14 days The percentage of subjects with the RVNA geometric mean concentration ≥ 0.5 IU/mL in GR1801 recipients and HRIG recipients in combination with rabies vaccines.
- Secondary Outcome Measures
Name Time Method To evaluate the rabies post-exposure mortality of GR1801 compared to HRIG within 90 days and 365 days after administration. 365 days The percentage of subjects with cases of rabies death.
To evaluate the rabies post-exposure morbidity of GR1801 compared to HRIG within 90 days and 365 days after administration. 365 days The percentage of subjects with probable or confirmed cases of rabies.
To evaluate the Area under the plasma concentration versus time curve (AUC0-last,AUC0-inf) of GR1801 within 365 days. 365 days The Area under the plasma concentration versus time curve (AUC0-last,AUC0-inf) of GR1801 will be estimated at D3,D7,D14 and D42,using non compartmental analysis.
To evaluate the safety of GR1801 compared to HRIG within 365 days. 365 days Number of participants with treatment-related adverse events or serious adverse events as assessed by CTCAE v5.0
To evaluate the Geometric mean RVNA Concentration of GR1801 compared to HRIG within 1,3,5,14,42,90 and 365 days after administration. 365 days RVNA geometric mean concentration.
To evaluate the detection rate of RVNA concentration of GR1801 compared to HRIG within 1,3,5,7,14,42,90 and 365 days after administration. 365 days The percentage of subjects whose RVNA geometric mean concentration are below the quantization limit.
To evaluate the peak plasma concentration(Cmax) of GR1801 within 365 days. 365 days The peak plasma concentration of GR1801 will be estimated at D3,D7,D14 and D42,using non compartmental analysis.
To evaluate the rabies post-exposure survival rate of GR1801 compared to HRIG within 90 days and 365 days after administration. 365 days The percentage of subjects with rabies-free survival.
To evaluate the percentage of subjects with RVNA concentration ≥ 0.5 IU/mL of GR1801 compared to HRIG within 1,3,5,7,42,90 and 365 days after administration. 365 days The percentage of subjects with RVNA geometric mean concentration ≥ 0.5 IU/mL.
To evaluate the immunogenicity of GR1801 within 365 days. 365 days To assess the anti-drug-antibodies (ADA) and neutralizing antibodies (NAb) of GR1801.
Trial Locations
- Locations (1)
Center for Disease Control and Prevention (CDC)
🇨🇳Kunming, Yunnan, China