ABSTRACT
Background. ADG20 is a fully human IgG1 monoclonal antibody engineered to have high potency and broad neutralization against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and other SARS-like CoVs with pandemic potential by binding to a highly conserved epitope in the receptor-binding domain (RBD) of the spike protein. The Fc region of ADG20 has been modified to provide an extended half-life. ADG20 is in clinical development for the treatment and prevention of COVID-19. Methods. This is an ongoing Phase 1, randomized, placebo (PBO)-controlled, single ascending-dose study of ADG20 administered intramuscularly (IM) or intravenously (IV) to healthy adults aged 18-50 years with no evidence of prior or current SARS-CoV-2 infection. Participants were randomized 8:2 in 3 cohorts (N=10/cohort: n=8 ADG20, n=2 PBO): ADG20 300 mg IM, 500 mg IV, and 600 mg IM. Safety, tolerability, PK, and sVNA titers were assessed up to 3 months post dose. Serum ADG20 concentrations were measured with a validated hybrid ligand binding liquid chromatography-mass spectrometry (MS)/MS assay. sVNA titers against authentic SARS-CoV-2 were determined by a plaque reduction neutralization assay. Results. Overall, 30 participants received ADG20 (n=24) or PBO (n=6). Blinded safety data for all cohorts and PK/sVNA titer data for the 300 mg IM cohort are reported. Through a minimum of 10 weeks post dose, no study drug-related adverse events (AEs), serious AEs, injection site reactions, or hypersensitivity reactions were reported. The observed preliminary PK profile was dose proportional, consistent with an extended half-life monoclonal antibody, and well predicted by translational physiologically-based PK modeling. The measured 50% sVNA titer (MN50;geometric mean [coefficient of variation, %]) was 1382 (32.7%) 13 days after a single 300 mg IM dose. These values are within the range of peak serum neutralizing antibody titers reported for COVID-19 mRNA vaccines. Conclusion. A single dose of ADG20, up to 600 mg IM, was well tolerated. Preliminary PK and sVNA titer profiles support the ongoing Phase 2/3 trials of ADG20 at a 300 mg IM dose for the prevention of COVID-19 (EVADE: NCT04859517) and treatment of ambulatory patients with mild to moderate COVID-19 (STAMP: NCT04805671).
ABSTRACT
Background. ADG20 is a fully human IgG1 monoclonal antibody engineered to have potent and broad neutralization against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and additional SARS-like CoVs with pandemic potential and an extended half-life. A QSP/PBPK model was constructed using ADG20-specific physiochemical properties and published non-human primate (NHP) and human PK data for other antibodies;it was used to a priori predict and confirm NHP and human PK. Methods. An existing QSP/PBPK model was modified to include 3 distinct lung sub-compartments: upper airway, lower airway, and alveolar tissue (Figure A). Each sub-compartment (Figure B) contained an epithelial lining fluid (ELF) space (Figure B). The model was fit separately to digitized NHP and human serum PK data for 7 extended half-life antibodies to estimate the apparent neonatal Fc receptor (FcRn) binding affinity (KD,FcRn) and bioavailability by drug. Nasopharyngeal swab (upper airway) and lung (lower airway) ELF PK data from 4 additional antibodies were used to optimize a single rate constant for transcytosis in lung. Patches of positive charge was a covariate on the rate of pinocytosis of antibody entry and exit from the endosomal space (Figure B). Observed NHP (ADG20 10 mg/kg IM) and human (ADG20 300 mg IM) PK data collected over the initial 21 days post dose were compared with model forecasts from a 1000-iteration simulation. Results. The distribution of fitted NHP KD,FcRn provided accurate predictions of NHP serum PK data (Figure C). NHP ADG20 KD,FcRn was optimized to be 35.7 nM and human ADG20 KD,FcRn (9.55 nM) was derived using a mean NHP:human KD,FcRn ratio of 3.74 across antibodies. Model-based simulated human serum PK data using inter-subject variability from NHP and actual weight distribution from an ongoing Phase 1 study aligned with initial 21-day data (Figure D). Using an adult CDC weight distribution (45-150 kg), the simulated median exceeded 74 days. Conclusion. The QSP/PBPK model a priori predicted NHP and human ADG20 PK. This innovative QSP-based modeling and simulation approach enabled the evaluation of candidate dose regimens prior to the availability of PK data, supporting the rapid advancement of the ADG20 clinical program during the COVID-19 pandemic.
ABSTRACT
Background. ADG20 is a fully human IgG1 monoclonal antibody engineered to have potent and broad neutralization against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and other SARS-like CoVs with pandemic potential and an extended half-life. ADG20 is administered intramuscularly (IM). A QSP/PBPK model was constructed to support dose selection for a Phase 2/3 trial of ambulatory patients with mild to moderate COVID-19 (STAMP: NCT04805671). Methods. A QSP/PBPK model was used to simulate receptor occupancy (RO) and drug exposure in the upper airway (nasopharyngeal/oropharyngeal epithelial lining fluid [ELF] compartment). RO was linked to an existing viral dynamic model to enable the prediction of the natural time course of viral load and the effect of ADG20 on viral clearance and infectivity rate. RO was calculated using: 1) in vitro ADG20-SARS-CoV-2 binding kinetics (association rate constant (kon) of 1.52E+06 M-1•s1 and dissociation rate constant (koff) of 2.81E-04 s-1 from a Biacore assay;2) time course of ADG20 concentrations in ELF;and 3) time course of viral load following ADG20 administration. Molar SARS-CoV-2 viral binding site capacity was calculated assuming 40 spike proteins per virion, 3 binding sites per spike, and an initial viral load of log 107 copies/mL for all patients. The QSP/PBPK model and a 2018 CDC reference body weight distribution (45-150 kg) were used to simulate 1000 concentration-time profiles for a range of candidate ADG20 regimens. ADG20 regimens were evaluated against 2 criteria: 1) ability to attain near complete ( >90%), and durable (28-day) SARS-CoV-2 RO in the ELF;and 2) ability to maintain ELF ADG20 concentrations relative to a concentration (0.5 mg/L) associated with 100% viral growth suppression in an in vitro post-infection assay. Results. A single 300 mg IM ADG20 dose met the dose selection criteria in terms of RO (Figure A) and viral growth suppression (Figure B). Conclusion. These data support the evaluation of an ADG20 300 mg IM dose for the treatment of mild to moderate COVID-19. ADG20 is forecasted to attain near complete ( >90%) SARS-CoV-2 RO in the ELF and maintain ELF ADG20 concentrations above that associated with 100% viral growth suppression in vitro.
ABSTRACT
Background. ADG20 is a fully human IgG1 monoclonal antibody engineered to have potent and broad neutralization against severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) and other SARS-like CoVs with pandemic potential as well as an extended-half-life. ADG20 is administered intramuscularly (IM). A QSP/PBPK model was constructed to support dose selection for a COVID-19 Phase 2/3 prevention trial (EVADE: NCT04859517). Methods. A QSP/PBPK model and a CDC reference adult body weight distribution (45-150 kg) were used to simulate 1000 concentration-time profiles for candidate single-dose regimens of ADG20 (150-450 mg IM). As serum virus neutralizing antibody (sVNA) titers are reportedly a key correlate of protection from COVID-19, a regression equation between time-matched serum ADG20 concentrations (following a 300 mg IM dose) and sVNA titers was developed using measured titers against authentic SARS-CoV-2 determined by a plaque reduction neutralization assay. Projected ADG20 serum concentrations relative to neutralization potency in vitro (90% inhibitory concentration [IC90]) for authentic SARSCoV-2 were also evaluated. Results. The measured 50% neutralization titer (MN50;geometric mean [coefficient of variation, %]) was 1382 (32.7%) 13 days after a single 300 mg IM dose of ADG20. This was within the range of peak sVNA titers reported for COVID-19 vaccine recipients. Using the linear equation relating serum ADG20 concentration to time matched individual MN50 titers and the QSP/PBPK median PK prediction, the anticipated median MN50 exceeded the threshold for protection from SARS-CoV-2 infection established in a non-human primate adoptive transfer model for up to 52 weeks. Based on the QSP/PBPK median PK prediction, median ADG20 serum concentrations are projected to remain >100-fold above the ADG20 IC90 value of 0.011 mg/L against authentic SARS-CoV-2 for up to 52 weeks (Figure). Conclusion. Following administration of a single 300 mg IM dose, sVNA titers and concentrations of ADG20 are projected to remain above thresholds anticipated to be required for protection against COVID-19 for up to 52 weeks. These data support the evaluation of a single ADG20 300 mg IM dose for the prevention of COVID-19.
ABSTRACT
Background In Response To The Covid-19 Pandemic And National Professional Gastroenterology Society Guidelines, Ucla Health Implemented System-Wide Policies For Safe Non-Urgent Endoscopy On 4/13/2020. These Policies Included Mandatory Nasopharyngeal Covid-19 Testing 48 Hours Prior To All Outpatient Procedures. We Aimed To Determine The Covid-19 Positive Rate Among Outpatients Presenting For Elective Gastrointestinal (Gi) Procedures And To Characterize Patients Who Tested Positive For Covid-19. Methods Ucla Health Is A Large, Integrated Healthcare System With 5 Outpatient Endoscopy Units Across Southern California. Our Study Cohort Included All Patients Scheduled For One Or More Outpatient Procedures (Colonoscopy, Egd, Sigmoidoscopy, Manometry, Ph Study, Small Bowel Enteroscopy, Manometry, Eus, Ercp) Who Underwent Pre-Procedure Covid-19 Testing From 4/13/2020 To 11/5/2020. We Developed An Electronic Dashboard To Track Procedure Date, Type, And Completion Status, Pre-Procedure Covid-19 Test Results 48 Hours Prior To Procedure, And Post-Procedure Covid-19 Test Results Up To 14 Days After A Procedure. We Queried The Electronic Health Record For Patient Data, Performed Manual Chart Review To Identify Covid-19 Symptoms, And Used Administrative Data To Determine Covid-19 Exposures To Gastroenterology Providers And Staff. Our Primary Outcome Was The Preprocedure Covid-19 Positive Rate. We Also Determined Covid-19 Symptom Prevalence And Cases Of New Covid-19 Positivity Post-Procedure. We Used Univariate And Multivariable Logistic Regression To Determine Factors Associated With A Positive Pre-Procedure Covid-19 Test, Controlling For Age, Sex, Race/Ethnicity, And Bmi. Results The Study Cohort Included 9,645 Patients, Representing 10,056 Total Outpatient Scheduled Gi Procedures (Table 1). The Cumulative Pre-Procedure Positive Rate Was 0.3% (N=28), And The Inconclusive Rate Was <0.1% (N=7, Figure 1). One Patient Had A New Positive Covid-19 Result Post-Procedure (Day 4), Associated With New Cough. There Were No Known Covid-19 Exposures Among Gastroenterology Faculty And Staff. Of Patients With A Preprocedure Positive Covid-19 Result, 13 (46.4%) Were Asymptomatic And 10 (35.7%) Had Symptoms Possibly Consistent With Covid-19 (25% Cough, 14.3% Fevers/Chills, 7.1% Diarrhea, 3.6% Myalgias, 3.6% Dyspnea). No Factors Were Significantly Associated With A Positive Pre-Procedure Covid-19 Result In The Multivariable Model. The Covid-19 Testing Positivity Rate Was 3-13% In Los Angeles County During The Study Period. Discussion Implementation Of Mandatory Covid-19 Testing Before Outpatient Gi Procedures Was Successful, And The Positive Rate Was Low. Common Symptoms Among Patients With A Positive Pre-Procedure Covid-19 Result Were Cough, Fevers, And Chills. Although They Were Not Mandated, Post-Procedure Positive Covid-19 Results Were Rare (Table Presented) Patient Characteristics Overall And By Pre-Procedure Covid-19 Test Result (Figure Presented) Pre-Procedure Covid-19 Testing By Result (Per Month And Overall).