First-In-Human Clinical Study of the C3 Complement Inhibitor AMY- 101 in Healthy Male Volunteers

Safety, Tolerability, Pharmacokinetics (PK) and Pharmacodynamics (PD) of a Single Ascending Dose (SAD) and a Multiple Dose (MD) of the Complement Inhibitor AMY-101. A Prospective, Single-center, Open-label, First-In-Human (FIH) Clinical Study in Healthy Male Volunteers

Status

Completed

Phases

Phase 1

Study type

Interventional

Source

ClinicalTrials.gov

Registry ID

NCT03316521

Enrollment

Registered

2017-10-20

Start date

2017-04-24

Completion date

2017-11-30

Last updated

2018-01-16

For informational purposes only — not medical advice. Sourced from public registries and may not reflect the latest updates. Terms

Conditions

Complement Mediated Diseases

Keywords

complement inhibition, C3 complement inhibitor, AMY-101, Compstatin Cp40, Paroxysmal Nocturnal Hemoglobinuria (PNH), C3 glomerulopathy (C3G), Periodontal disease, Age-related macular degeneration (AMD), ABO incompatible kidney transplantation

Brief summary

Safety, tolerability, pharmacokinetics (PK) and pharmacodynamics (PD) of a Single Ascending Dose (SAD) and a Multiple Dose (MD) of the complement inhibitor AMY-101. A prospective, single-center, open-label, First-In-Human (FIH) clinical study in healthy male volunteers.

Detailed description

AMYNDAS is developing a novel peptidic complement inhibitor AMY-101, based on the third-generation compstatin analogue Cp40. AMY-101 is a selective inhibitor of complement activation in humans and in NHP. It binds to the complement component C3, the central functional hub that controls the upstream activation/amplification and downstream effector functions of complement. By binding to C3, AMY-101 inhibits the cleavage of native C3 to its active fragments C3a and C3b. As a consequence, the deposition of C3b, amplification via the alternative pathway and all downstream complement responses are prevented. AMY-101 is being developed to treat complement-mediated diseases, which are largely driven by aberrant C3 activation. This first-in-human study of the C3-targeting complement inhibitor AMY-101 investigates the safety and PK/PD profile of AMY-101 in healthy male volunteers after Single Ascending Dose (SAD) and Multiple Doses (MD) using subcutaneous (SQ) or intravenous (IV) administration. The study is a prospective, single-center, open-label evaluation in healthy male volunteers.

Interventions

DRUGAMY-101

AMY-101 is a selective inhibitor of complement activation, which binds to the complement component C3.

Study design

Allocation

RANDOMIZED

Intervention model

SEQUENTIAL

Primary purpose

TREATMENT

Masking

NONE

Intervention model description

This is a prospective, single-center, open-label FIH study investigating the safety, tolerability, PK and PD after single and multiple doses of AMY-101 in healthy male volunteers. In the SAD part of the study, a single dose at ascending dose levels of AMY-101 will be administered to different cohorts, following a careful dose-escalation strategy. In the MD part of the study, multiple doses will be administered using different dosing intervals; the cohorts will include a minimum of four (4) subjects each. Additional subjects may be added in the cohorts if necessary.

Eligibility

Sex/Gender

MALE

Age

18 Years to 60 Years

Healthy volunteers

Yes

Inclusion criteria

1. Willing and able to give written informed consent for participation in the study. 2. Healthy male subject aged 18-60 years, inclusive at the time of signing the informed consent. 3. Body Mass Index (BMI) ≥ 18 and ≤ 30 kg/m2 and weight at least 50 kg. 4. Clinically normal medical history, physical findings, vital signs, ECG and laboratory values at the time of screening, as judged by the Investigator. 5. Willing to use condom and contraceptive methods with a failure rate of \< 1% to prevent pregnancy and drug exposure of a partner and to refrain from donating sperm from the date of dosing until three (3) months after dosing of the IMP. 6. Willing and able to complete all procedures according to the Protocol.

Exclusion criteria

1. History of any clinically significant disease or disorder which, in the opinion of the Investigator, may either put the subject at risk because of participation in the study, or influence the results or the subject's ability to participate in the study. 2. History of any Neisseria meningitidis infection 3. History of unexplained, recurrent infection, or infection requiring treatment with systemic antibiotics within the last 60 days prior to dosing. 4. History of latent or active tuberculosis, as assessed by the investigator based on chest X-ray and positive Quantiferon-TB Gold test. 5. History of complement deficiency. 6. History of any type of malignancy. However, completely resolved minor malignancies, at the discretion of the Investigator, may not be an exclusion criterion (for example: Non-Melanoma Skin Cancer). 7. Diagnosis of autoimmune, immunologic or rheumatologic disease (eg, systemic lupus erythematosus, rheumatoid arthritis). 8. Any clinically significant illness, medical/surgical procedure or trauma within four (4) weeks of the administration of IMP. 9. High CRP at screening (\> 0.5 mg/dL). 10. Current evidence or history of bacterial, viral or fungal infection within 14 days prior to (first) dosing or longer according to the judgment of the investigator for e.g. viral infections including herpes simplex or herpes zoster. 11. Any current condition or risk, which, in the opinion of the Investigator, may interfere with the subject's participation in the study, poses an added risk for the subject, or confounds the assessment of the subject or outcome of the study 12. Any clinically significant abnormality in clinical chemistry, hematology, or urinalysis results at the time of screening, as judged by the Investigator. 13. Any positive result on screening for serum hepatitis B surface antigen, hepatitis C antibody and/or Human Immunodeficiency Virus (HIV). 14. After 10 minutes supine rest abnormal vital signs defined as any of the following: * Systolic BP \> 140 mm Hg * Diastolic BP \> 95 mm Hg * HR \< 40 or \> 90 beats per minute 15. Prolonged QTcF (\>450 ms), cardiac arrhythmias or any clinically significant abnormality in the resting ECG, as judged by the Investigator. 16. Any history of any allergy/hypersensitivity or anaphylactic reaction or on-going allergy/hypersensitivity. History of hypersensitivity to antibiotics or drugs with a similar chemical structure or class to AMY-101. 17. Use of any prescribed or non-prescribed medication including antacids, analgesics, herbal remedies, vitamins and minerals within two (2) weeks prior to the administration of IMP, except the occasional intake of paracetamol/acetominophen (maximum 2000 mg/day; and not exceeding 3000 mg/week) or nasal decongestant without cortisone or antihistamine, at the discretion of the Investigator. 18. Administration of another new chemical entity (defined as a compound that has not been approved for marketing) or having participated in any other clinical study that included drug treatment within 30 day or 5 half lives of the last administration of the other IMP. Subjects consented and screened but not dosed in previous phase I studies are not excluded. 19. Immunization with a live-attenuated vaccine one (1) month prior to the first administration of IMP. 20. Current smokers or users of nicotine products. Irregular use of nicotine (e.g. smoking, snuffing, chewing tobacco) less than three (3) times per week is allowed before screening visit. 21. History of alcohol abuse or excessive intake of alcohol, as judged by the Investigator. 22. Positive screen for drugs of abuse at screening or on admission to the unit or positive screen for alcohol at screening or on admission to the unit prior to administration of the IMP. 23. Use of anabolic steroids. 24. Plasma donation within one (1) month of screening or any blood donation/blood loss \> 450 mL during the three (3) months prior to screening. 25. Investigator considers the subject unlikely to comply with study procedures, restrictions and requirements.

Design outcomes

Primary

Measure	Time frame
Number of participants with treatment-related adverse events as assessed by CTCAE v4.0	Up to 21 days after treatment.

Secondary

Measure	Time frame	Description
Area under the plasma concentration time curve from zero to infinity (AUC 0->∞) after a single dose	Up to 14 days after treatment.	—
Peak Plasma Concentration (Cmax) after single and multiple doses	Up to 14 days after treatment.	—
Time to Cmax (Tmax) after single and multiple doses	Up to 14 days after treatment.	—
Terminal elimination rate constant (lambdaz) after single and multiple doses	Up to 14 days after treatment.	—
Terminal half-life (T1/2) after single and multiple doses	Up to 14 days after treatment.	—
Total apparent clearance of drug from plasma/serum (CL/F) after single and multiple doses	Up to 14 days after treatment.	—
Volume of distribution (Vz) / fraction of drug absorbed (F) after single and multiple doses	Up to 14 days after treatment.	—
Area under the plasma concentration time curve (AUCt) after a single dose	Up to 14 days after treatment.	—
Activation of the classical complement pathway	Up to 14 days after treatment.	CH50
Activation of the alternative complement pathway	Up to 14 days after treatment.	AP50
Complement protein C3 plasma levels	Up to 14 days after treatment.	—
Complement protein C4 plasma levels	Up to 14 days after treatment.	—
Measurement of immune response (plasma protein electrophoresis - IgG,IgA, IgM) after single and multiple administrations of AMY-101.	Up to 14 days after treatment.	—
Investigation for anti-drug antibodies after single and multiple administrations of AMY-101.	Up to 14 days after treatment.	—
Measurement of lymphocyte subsets after multiple administrations of AMY-101.	Up to 14 days after treatment.	—
Area under the curve at steady state (AUCss) after multiple doses	Up to 14 days after treatment.	—

Countries

United States

Outcome results

None listed

Source: ClinicalTrials.gov · Data processed: Feb 4, 2026