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NCT06401213 Clinical Trial

A First-in-Human Safety Trial of MTX-463

Healthy Clinical Trial

Official title:
MTX-463-I101: A Phase 1 Randomized, Double-Blind, Dose-Escalating Study to Assess the Safety, Tolerability, and Pharmacokinetics of MTX-463 in Healthy Adults

Clinical Trial Details — Status: Recruiting

Administrative data
NCT number NCT06401213
Other study ID # MTX-463-I101
Secondary ID
Status Recruiting
Phase Phase 1
First received
Last updated
Start date April 15, 2024
Est. completion date November 16, 2024

Study information
Verified date May 2024
Source Mediar Therapeutics
Contact Jeffrey Bornstein, MD
Phone 6176203403
Email jeffrey@mediartx.com
Is FDA regulated No
Health authority
Study type Interventional

Clinical Trial Summary

A randomized, double-blind, placebo-controlled, single ascending dose (SAD) and multiple ascending dose (MAD) study to assess the safety, tolerability, and PK of single and multiple ascending doses of MTX-463 administered in healthy adults.

Description:

This is a randomized, double-blind, placebo-controlled, single ascending dose (SAD) and multiple ascending dose (MAD) study to assess the safety, tolerability, and PK of single and multiple ascending doses of MTX-463 administered in healthy adults. SAD Portion The SAD portion of the study will consist of 4 planned dosing cohorts each comprising 8 healthy participants. The starting dose will be 4 mg/kg (Cohort 1) with subsequent planned doses of 8 mg/kg (Cohort 2), 16 mg/kg (Cohort 3), and 30 mg/kg (Cohort 4). Planned doses may be adjusted in response to the data. Additional participants and/or additional dosing cohorts may be added as needed based on the data. Within each cohort, participants will be randomly assigned to receive MTX-463 or matched placebo. The first 2 participants (sentinel participants) within each cohort will be randomized 1:1 to receive MTX-463 or placebo on Day 1. These participants will be monitored for 24 hours, and after review of the safety data from both participants and approval by the study Investigator and Sponsor's responsible medical officer (SRMO), the additional 6 participants will be randomized to study drug (n=5 MTX-463; n=1 placebo). Each participant will undergo assessments at specified timepoints on Days 1 through 60. End-of-Study (EOS) procedures will be completed on Day 28 or upon early termination (ET). An End-of-Follow-up (EOF) assessment of PK and ADA will be completed on Day 60. MAD Portion The MAD portion of the study will consist of 3 planned dosing cohorts. Each cohort will comprise 8 healthy participants (n=6 MTX-463; n=2 placebo). The starting dose will be a 6.6 mg/kg loading dose and 4 mg/kg maintenance doses (Cohort 1) with subsequent planned doses of a 13 mg/kg loading dose and 8 mg/kg maintenance doses (Cohort 2), and a 27 mg/kg loading dose and 16 mg/kg maintenance doses (Cohort 3). Planned doses may be adjusted in response to the data. Additional participants and/or additional dosing cohorts may be added as needed based on the data. On Day 1, participants will be randomized to receive either MTX-463 or matched placebo. The randomized participants will receive a single loading dose on Day 1 followed by 2 maintenance doses of study drug on Day 8 and Day 22. Participants will be housed inpatient from Day -1 through post-dose observation on Day 8 and from Day 21 through assessments on Day 29. All other visits will be conducted in the outpatient setting. Each participant will undergo assessments at specified timepoints on Days 1 through 82. End-of-study procedures will be completed on Day 50, or upon ET. An EOF assessment of PK and ADA will be completed on Day 82. Safety and tolerability of MTX-463 will be reviewed through Day 29 by the study Investigator and SRMO to inform dose escalation decisions for the next dose cohort. Additional cohorts for the SAD and MAD portions of the study may be added as needed to potentially explore lower doses.

Recruitment information / eligibility
Status Recruiting
Enrollment 56
Est. completion date November 16, 2024
Est. primary completion date November 16, 2024
Accepts healthy volunteers Accepts Healthy Volunteers
Gender All
Age group 18 Years to 60 Years
Eligibility Key Inclusion Criteria: - All genders, ages 18 to 60 years, inclusive - Willing and able to complete all protocol-required study visits and procedures - Non-smoker and has not used nicotine- or cotinine-containing products (including tobacco, nicotine gum, patches, and e-cigarettes) for at least 90 days before Screening and until the last study visit - Willing to refrain from marijuana- or cannabinol-containing products for 90 days before Screening and until the last study visit - Willing to refrain from ingestion of alcohol from 7 days before Screening until the last study visit - Agree to a highly effective method of contraception for 28 days prior to the first dose of study drug, and persist through 28 days after the last dose of study drug Key Exclusion Criteria: - - Any history of clinically significant lung disease as determined by the Investigator, including but not limited to asthma, chronic obstructive pulmonary disease, pulmonary fibrosis, pulmonary embolus, or pulmonary arterial hypertension - Any other concurrent active medical condition determined clinically significant by the Investigator - Body mass index (BMI) >40 kg/m2 - Use of any systemic immunosuppressant medications, medications to treat diabetes, antipsychotics, anticoagulants, or other medications within 90 days of Screening - Cancer or a history of cancer or lymphoproliferative disorder within 5 years of Screening other than adequately treated non-melanomatous skin cancers or cervical carcinoma in situ - Current infection with hepatitis B, hepatitis C, or human immunodeficiency virus (HIV) as evidenced by a positive hepatitis B-surface antigen or a positive HIV test at Screening - Currently pregnant, lactating, or planning to conceive or contribute to pregnancy during the trial and up to 28 days after the participant's last dose of study drug, if applicable - History of severe depression, psychosis, or suicidal ideation within 5 years of Screening - History of substance use disorder as specified in Diagnostic and Statistical Manual of Mental Disorders, Fifth Edition, within 1 year of Screening - Any clinically significant disease or laboratory abnormality detected at Screening that might interfere with a participant's ability to complete the study, on-study evaluations, or participant safety - Any surgical procedure, including planned procedures within 12 weeks of Screening - Participation in another research study of an investigational agent within 30 days of Screening or 5 half-lives of the agent, whichever is longer

Study Design

Related Conditions & MeSH terms

Intervention

Biological:
MTX-463
MTX-463 is an immunoglobin G1 (IgG1) monoclonal antibody directed against WNT-inducible signaling pathway protein 1 (WISP1). WISP1 (aka CCN-4) is a matricellular protein that appears to be upregulated locally in response to certain chronic diseases and malignancies.
Other:
Placebo
Matching Placebo-- Normal Saline

Locations
Country Name City State
United States ICON Salt Lake City Utah

Sponsors (2)
Lead Sponsor Collaborator
Mediar Therapeutics ICON plc

Country where clinical trial is conducted

United States, 

Outcome
Type Measure Description Time frame Safety issue
Other To assess the effect of MTX-463 on PD biomarker PRO-C3 for fibrosis in healthy adult participants Change from Baseline in fibrosis biomarker PRO-C3 will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker PRO-C6 for fibrosis in healthy adult participants Change from Baseline in fibrosis biomarker PRO-C6 will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker C7M for fibrosis in healthy adult participants Change from Baseline in fibrosis biomarker C7M will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker IFN-? for inflammation Baseline levels and change from Baseline of PD biomarker IFN-? for inflammation will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker IL-1ß for inflammation Baseline levels and change from Baseline of PD biomarker IL-1ß for inflammation will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker IL-2 for inflammation Baseline levels and change from Baseline of PD biomarker IL-2 for inflammation will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker IL-4 for inflammation Baseline levels and change from Baseline of PD biomarker IL-4 for inflammation will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker IL-6 for inflammation Baseline levels and change from Baseline of PD biomarker IL-6 for inflammation will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker IL-10 for inflammation Baseline levels and change from Baseline of PD biomarker IL-10 for inflammation will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker IL-12p70 for inflammation Baseline levels and change from Baseline of PD biomarker IL-12p70 for inflammation will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker IL-17A for inflammation Baseline levels and change from Baseline of PD biomarker IL-17A for inflammation will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker TNF-a for inflammation Baseline levels and change from Baseline of PD biomarker TNF-a for inflammation will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker IFN-? for inflammation in healthy adult participants Change from Baseline in pro-inflammatory biomarker IFN-? will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker IL-1ß for inflammation in healthy adult participants Change from Baseline in pro-inflammatory biomarker IL-1ß will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker IL-2 for inflammation in healthy adult participants Change from Baseline in pro-inflammatory biomarker IL-2 will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker IL-4 for inflammation in healthy adult participants Change from Baseline in pro-inflammatory biomarker IL-4 will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker IL-6 for inflammation in healthy adult participants Change from Baseline in pro-inflammatory biomarker IL-6 will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker IL-10 for inflammation in healthy adult participants Change from Baseline in pro-inflammatory biomarker IL-10 will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker IL-12p70 for inflammation in healthy adult participants Change from Baseline in pro-inflammatory biomarker IL-12p70 will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker IL-17A for inflammation in healthy adult participants Change from Baseline in pro-inflammatory biomarker IL-17A will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of MTX-463 on PD biomarker TNF-a for inflammation in healthy adult participants Change from Baseline in pro-inflammatory biomarker TNF-a will be evaluated. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker PRO-C3 for fibrosis Baseline levels and change from Baseline of PD biomarker PRO-C3 for fibrosis will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker PRO-C6 for fibrosis Baseline levels and change from Baseline of PD biomarker PRO-C6 for fibrosis will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Other To assess the effect of baseline BMI on PD biomarker C7M for fibrosis Baseline levels and change from Baseline of PD biomarker C7M for fibrosis will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 36 (MAD Cohort)
Primary Incidence of Treatment-Related Adverse Events in healthy volunteers Clinical Safety Labs are collected, and Adverse Events are assessed in both inpatient and outpatient clinic visits Through Day 60 (SAD Cohort) or Day 82 (MAD Cohort)
Primary MTX-463 PK by dose will be evaluated for Cmax, as feasible Blood serum samples will be collected at protocol-specified timepoints throughout the study Through Day 60 (SAD Cohort) or Day 82 (MAD Cohort)
Primary Serum sample results will be summarized for presence of Anti-Drug Antibodies during the SAD and MAD portions of the study. Blood serum samples will be collected at protocol-specified timepoints throughout the study to assess for the presence and titer (if applicable) of Anti-Drug Antibodies. Through Day 60 (SAD Cohort) or Day 82 (MAD Cohort)
Primary MTX-463 PK by dose will be evaluated for AUC0-t, as feasible. Blood serum samples will be collected at protocol-specified timepoints throughout the study Through Day 60 (SAD Cohort) or Day 82 (MAD Cohort)
Primary MTX-463 PK by dose will be evaluated for AUC0-tau (MAD only), as feasible Blood serum samples will be collected at protocol-specified timepoints throughout the study Through Day 82 (MAD Cohort)
Primary MTX-463 PK by dose will be evaluated for AUC0-8, as feasible Blood serum samples will be collected at protocol-specified timepoints throughout the study Through Day 60 (SAD Cohort) or Day 82 (MAD Cohort)
Secondary Blood serum samples will be collected to determine the level of WISP1 engagement of MTX-463 in healthy adult participants These assessments will be summarized as:
Change from Baseline in total WISP1 levels
Change from Baseline in free WISP1 levels		 Through Day 60 (SAD Cohort) or Day 82 (MAD Cohort)
Secondary To assess the effect of baseline body mass index (BMI) on total and free WISP1 levels Baseline levels and change from Baseline of the total and free WISP1 levels will be compared in those with BMIs =30 kg/m2 to those with BMIs <30 kg/m2. Through Day 60 (SAD Cohort) or Day 82 (MAD Cohort)
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