The goal of this Phase Ia clinical trial is to evaluate the safety, tolerability, and pharmacokinetics of EB070 injection following single ascending subcutaneous doses in healthy adult volunteers. The main questions it aims to answer are: Is EB070 injection safe and well tolerated at increasing single subcutaneous dose levels in healthy subjects? What are the pharmacokinetic characteristics of EB070 after single-dose administration? This is a single-center, randomized, double-blind, placebo-controlled, single ascending-dose (SAD) study. A total of 36 healthy volunteers will be enrolled and assigned to one of five dose cohorts (21 mg, 75 mg, 225 mg, 450 mg, or 600 mg). Subjects in each cohort will be randomized in a 3:1 ratio to receive a single subcutaneous injection of EB070 or placebo. A sentinel dosing strategy will be applied. In the 21 mg cohort, one subject will initially receive EB070. In the remaining cohorts, two sentinel subjects (one receiving EB070 and one receiving placebo) will be dosed first. Dose escalation and enrollment of the remaining subjects will proceed after evaluation of safety and tolerability within 48 hours after dosing. Participants will: Undergo screening assessments prior to dosing Receive a single subcutaneous injection of EB070 or placebo Stay in the Phase I unit for approximately 3 days for safety monitoring and pharmacokinetic and anti-drug antibody (ADA) sample collection Return for scheduled outpatient visits for PK, ADA, and safety assessments through Day 113 Safety will be assessed throughout the study by monitoring adverse events, vital signs, physical examinations, 12-lead ECGs, and laboratory tests. Pharmacokinetic parameters and anti-drug antibodies (ADA) will be evaluated as secondary outcomes.
Study Type
INTERVENTIONAL
Allocation
RANDOMIZED
Purpose
TREATMENT
Masking
QUADRUPLE
Enrollment
36
Anti-TSLP Monoclonal Antibody
AEs
including Adverse events defined by CTCAE 5.0(Common Terminology Criteria for Adverse Events version 5.0)
Time frame: From ICF signed to day 113 after investigational drug administration
t1/2
is the time required for the concentration of EB070 in the bloodstream to decrease by exactly 50%. It is a measure of how quickly the body eliminates EB070.
Time frame: From day 1 to day 113
Cmax
is the highest concentration of EB070 measured in the blood plasma after a dose is administered.
Time frame: From day 1 to day 113
Tmax
is the time elapsed from drug administration until the maximum plasma concentration (Cₘₐₓ) is reached.It is a measure of the rate of drug absorption.
Time frame: From day 1 to day 113
AUC 0-t
It is calculated by plotting plasma concentration against time and measuring the total area under that curve up to the last sampled time point.
Time frame: From day 1 to day 113
AUC0-∞
Area Under the Plasma Concentration-Time Curve from time zero extrapolated to infinity. It is calculated as AUC₀-ₜ + (Cₜ / λz), where Cₜ is the last measurable concentration and λz is the terminal elimination rate constant.
Time frame: From day 1 to day 113
Vz
is a theoretical volume that relates the total amount of drug in the body to its plasma concentration during the terminal elimination phase.
Time frame: From day 1 to day 113
CL
Clearance is the volume of plasma (or blood) from which EB070 is completely removed per unit of time
Time frame: From day 1 to day 113
ADA
Anti-Drug Antibodies are immune proteins (antibodies) produced by a patient's immune system that specifically bind to EB070,using sensitive immunoassays (like ECL/ELISA) often combined with acid-dissociation techniques to overcome drug interference and accurately quantify the immune response.
Time frame: From day 1 to day 113
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