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SAD/MAD Safety and PK Study of RBN-3143 in Healthy and Atopic Dermatitis Subjects

PHASE1RECRUITING

RBN-3143 Background: PARP proteins are members of a family of seventeen ADP-ribosyltransferase (ART) enzymes that regulate cellular processes including gene expression, protein degradation, and multiple cellular stress responses. RBN-3143 is a PARP-14 inhibitor. PARP14 is over-expressed in tissues with inflammatory diseases.

RBN-3143 is a novel, orally administered PARP14 inhibitor that was developed to be evaluated as therapy for a range of inflammatory diseases, with an initial focus on Atopic Dermatitis. Study Overview: The study consists of 2 parts. Part A: This part of the study is being conducted in a clinical research unit (CRU) and is enrolling healthy adult subjects to determine the safety of RBN-3143; its absorption, metabolism, and excretion (what the body does to this drug); and will assess its potential pharmacodynamic properties (what the drug does to the body).

There are 3 subsections to this part of the study. The first segment was conducted in a double-blind manner (neither the investigator nor subject knew if placebo or RBN-3143 was given) to assess dosing regimens of RBN-3143 when taken in a fasted state (before food). The last two segments are currently recruiting and are Open Label (all subjects will receive RBN-3143) and will assess RBN-3143 when taken with food, with pantoprazole, a medication that decreases the amount of acid in the stomach, and with midazolam.

Part B: In early 2023 the second part of the study will be conducted in patients with moderate to severe atopic dermatitis to measure the pharmacodynamic activity of RBN-3143 and evaluate preliminary efficacy of 28 days administration of the study drug. All patients will receive the same dose of RBN-3143.

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Study details:

The study consists of 2 parts. Part A: This part of the study is being conducted in a clinical research unit (CRU) and will enroll healthy adult subjects to determine the safety of RBN-3143; its absorption, metabolism, and excretion (what the body does to this drug); and will assess its potential pharmacodynamic properties (what the drug does to the body). There are 3 subsections to this part of the study.

The first subsection has completed enrollment and the 2 open-label subsections are now actively enrolling. 1. Double-Blind Cohorts- Fasting: In the first segment of the study, subjects were randomized in a double-blind manner using a 3:1 ratio (RBN-3143: placebo) to receive either RBN-3143 or placebo.

Subjects were enrolled in groups of ascending doses. 2. Open Label Cohorts:.

1. Food Effect/Proton Pump Inhibitor (FE/PPI) Open Label Cohort:. Twelve (12) additional subjects are being enrolled and will receive RBN-3143 with food (fed), fasted, or with pantoprazole, PPI, a drug to determine if the amount of acid in the stomach, as well as the presence or absence of food changes how RBN-3143 is absorbed.

Subjects will be required to stay in the CRU for up to 16 days. Two sequences will be studied, either fasted then fed or fed then fasted with both sequences followed by administration of a proton pump inhibitor. 2.

Drug-Drug Interaction (DDI) Open Label Cohort: A further 12 subjects are being enrolled into a DDI cohort, to evaluate the effect of RBN-3143 on the exposure of midazolam, a sensitive CYP3A4 substrate. Subjects will be required to stay in the CRU 19 days. Subjects will also return for a final visit approximately 1 week later.

This cohort will have 2 Treatment Periods as follows:. * Treatment Period 1: On Day 1, subjects will be administered a single oral dose of 2 mg midazolam in the fasted state. * Treatment Period 2: Subjects will be administered RBN-3143 in the fasted state from Day 3 through Day 17 (14- day treatment period).

On Day 16, subjects will also receive a single oral dose of 2 mg midazolam in the fasted state. Part B: In early 2023 the second part of the study will be initiated in approximately 12 patients with moderate to severe atopic dermatitis. All patients will receive the same doses of RBN-3143 for 28 days.

On Day 1 and Day 28 patients will fast overnight until after the morning dose administration then fast for 4 hours post-dose. On all other days fasted state will be 2 hours prior to dosing and 2 hours after dosing. Patients will be required to present at the CRU on Day -1 for required study assessments after which they may return home.

Patients will return to the CRU on Day 1 for the day 1 dose and the completion of required study assessments. Patients will then return home with sufficient study drug to complete dosing on Days 2 to Day 27 (inclusive). Patients will be required to attend the CRU for completion of required assessments on Day 7, Day 14, Day 21, and Day 28, and will return any remaining study drug on the Day 28 visit.

Patients will return for an EOS/Follow-up visit at 4 weeks after the last dose of study drug. Collection of data will cease at the time of database lock for final safety and PK analysis.

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Eligibility criteria

Researchers look for people who fit a certain description, called eligibility criteria. See if you qualify.

Inclusion criteria

Healthy male or female subjects between 18 and 65 years of age (inclusive at the time of informed consent)

Body mass index (BMI) between ≥18 and ≤30 kg/m2 (inclusive) at Screening

Good general health, with no significant medical history, have no clinically significant abnormalities on physical examination at Screening and/or before administration of the initial dose of study drug

Clinical laboratory values within normal range as specified by the testing laboratory, unless deemed not clinically significant by the Investigator

Willingness and ability to speak, read, and understand English, and provide written informed consent

Must be a non-smoker or former smoker. Subjects must have negative cotinine results in drug tests at Screening and Baseline

Females must be: Non-pregnant Non-lactating Must use a non-hormonal, acceptable, highly effective double contraception from Screening until study completion, including the Follow-up Period Acceptable non-hormonal double contraception is defined as a condom AND one other form of the following: An IUD (non-hormonal) Documented evidence of surgical sterilization at least 6 months prior to Screening (e.g., tubal occlusion, hysterectomy, bilateral salpingectomy, or bilateral oophorectomy for women or vasectomy for men [with appropriate post-vasectomy documentation of the absence of sperm in semen] provided the male partner is a sole partner) Women of child-baring potential (WOCBP) must have: A negative pregnancy test at Screening and Day -1 and be willing to have additional pregnancy tests as required throughout the study Post-menopausal Women: Women not of childbearing potential must be: Postmenopausal for ≥12 months Postmenopausal status will be confirmed through testing of FSH levels ≥ 40 IU/L at Screening for amenorrhoeic female subjects Abstinence: Females who are abstinent from heterosexual intercourse will also be eligible. Complete abstinence by the subject for the duration of the study and for 1 month after the last study treatment is acceptable. Note: Periodic abstinence (eg, calendar, ovulation, symptothermal, post ovulation methods) and withdrawal are not considered highly effective methods of birth control. Female subjects who are in same-sex relationships are not required to use contraception. Males: If engaged in sexual relations with a WOCBP: The subject or his partner must be surgically sterile (eg, >30 days since vasectomy with no viable sperm, tubal occlusion, hysterectomy, bilateral salpingectomy, bilateral oophorectomy) Must use an acceptable, highly effective contraceptive method from Screening until study completion, including the Follow-up Period. Acceptable methods of contraception include the use of condoms and the use of an effective contraceptive for the female partner that includes: OCPs Long acting implantable hormones Injectable hormones Vaginal ring Use of an IUD Subjects with same-sex partners (abstinence from penile-vaginal intercourse) are eligible

For at least 90 days after the last dose of study drug, male subjects must not donate sperm and female subjects must not donate ovum

Willingness to comply with the drawing of all blood samples for the PK/PD analysis.

Willing and able to attend the necessary visits to the CRU and comply with all testing, fasting, and requirements defined in the protocol.

Willing and able to remain at the study site unite for the duration of the confinement period and return for outpatient visit/s defined in the protocol.

Chronic atopic dermatitis (AD) diagnosed by the Eichenfield revised criteria of Hanifin and Rajka, that has been present for at least 6 months before the Screening visit

EASI score ≥ 8 at the Screening and Baseline visits

IGA score ≥ 3 at the Screening and Baseline visits

Equal to or greater than 10% body surface area of AD involvement in areas affected beyond palms and soles at the Screening and Baseline visits, as per SCORAD

A documented history by the Investigator or delegate of inadequate response to treatment with topical medications within the past 6 months defined as failure to achieve or maintain remission or mild disease activity state (IGA score ≤ 2) despite daily treatment with topical corticosteroids of medium or higher potency (with or without topical calcineurin inhibitors) applied for at least 4 weeks or for the maximum recommended by the product manufacturer, whichever is shorter.

The patient must be applying stable doses of an additive-free, basic bland emollient twice-daily for at least 7 days before the Baseline visit

The patient must be willing to comply with skin biopsy/specimen collections

Exclusion criteria

Any medical condition that is considered by the Investigator or delegate that may interfere with study assessments, may adversely affect the subject's participation in the study, may make the subject's participation in the study unreliable, or be of such severity as to present an increased risk to the subject because of participation in the study.

Prior or ongoing medical conditions, physical findings, laboratory abnormality or a history of neurological, hepatic, renal, endocrine, cardiovascular, gastrointestinal, pulmonary, or metabolic disease that is considered as significant by the Investigator or delegate, and in the Investigator's opinion, could adversely affect the safety of the subject

Abnormal ECG findings at Screening that are considered by the Investigator to be clinically significant: Significant history of cardiovascular disease ECG results showing QTcF >450 msec or the presence of clinically significant abnormalities as determined by the investigator (Screening or Day -1) Elevation of blood pressure (BP), i.e., supine systolic BP >140 mmHg and/or diastolic BP >90 mmHg, or heart rate >100 beats per minute at rest

Use of any prescription medication within 14 days of dosing or over-the-counter (OTC) medication (including vitamins) within 48 hours of dosing or intends to use any prescription medication or OTC medication during the study that may interfere with the evaluation of study medication. Co-administration of medications known to have high risk of prolonging the QT interval are also prohibited. The use of other concomitant medications that present a low risk of QT prolongation may be considered, with the approval of the Medical Monitor. Simple analgesia (paracetamol, nonsteroidal anti-inflammatory drug [NSAID]) may be permitted at the discretion of the Investigator or delegate. Use of a low dose corticosteroid and β2 agonist inhalers to treat concomitant Asthma are allowed.

Ingestion of herbal medicines within 3 weeks before Screening, and grapefruit, grapefruit juice, star fruit or orange marmalade (made with Seville oranges) within 2 weeks prior to dosing, or intends to use any of these products during the study

Relevant dietary restrictions or unwilling to consume standard meals provided.

Ingestion of caffeine- or xanthine-containing products (e.g., coffee, tea, cola drinks, and chocolate) on days scheduled for full PK sample collection from 10 hours prior to the start of dosing through 12 hours post-dose. Must refrain from the consumption of alcohol for 2 days prior to Day 1 through the end of the study

A history of substance abuse or dependency or history of recreational intravenous (IV) drug use over the last 1 year (by self-declaration); or a positive ethanol breath test, urine cotinine, or urine drug screen at Screening and at Day -1

A positive test for hepatitis C antibody (HCV), hepatitis B surface antigen (HBsAg), human immunodeficiency virus (HIV) antibody, or COVID-19 (if conducted, at the Investigator's discretion) at Screening

Pregnant or lactating at Screening or planning to become pregnant (self or partner) at any time during the study, including the Follow-up Period

Use of any investigational product (IP) or investigational medical device within 30 days prior to Screening, or 5 half-lives of the product (whichever is the longest) or participation in more than 4 investigational drug studies within 1 year prior to Screening

Donated or lost a significant volume of blood (>450 mL) within 4 weeks prior to the first study drug administration

Unwilling to reside in the study unit for the duration of the study or to cooperate fully with the Investigator, delegate or site personnel.

Alkaline phosphatase (ALP), aspartate aminotransferase (AST), alanine aminotransferase (ALT), and/or total bilirubin >1.5 × upper limit of normal at Screening. Repeat testing at Screening is acceptable for out-of-range values following approval by the Investigator or delegate

Estimated Glomerular Filtration Rate (eGFR) < 90 mL/min/1.73m2

Presence of any underlying physical or psychological medical condition that, in the opinion of the Investigator, would make it unlikely that the subject will comply with the protocol or complete the study per protocol

Plasma donation within 7 days prior to the first study drug administration

Fever (temperature >38°C) or symptomatic viral or bacterial infection within 2 weeks prior to Screening

History of severe allergic or anaphylactic reactions to medicines or vaccines

History of malignancy, except for non-melanoma skin cancer, excised more than 2 years ago and cervical intraepithelial neoplasia that has been successfully cured more than 5 years prior to Screening

History or presence of a condition associated with significant immunosuppression

History of life-threatening infection (e.g., meningitis)

Infections requiring parenteral antibiotics within the 6 months prior to Screening

For the Food effect cohort only: a diet that in the opinion of the Investigator is incompatible with the on-study diet (e.g., lactose intolerance diet)

Unwilling to refrain from strenuous exercise within 48 hours prior to visits and during confinement at the CRU

Use of any IP or investigational medical device within 8 weeks prior to Screening, or participation in more than 2 investigational drug studies within 1 year prior to Screening

Estimated Glomerular Filtration Rate (eGFR) < 60 mL/min/1.73 m2 at Screening

Vaccination with a live (attenuated) vaccine within 8 weeks before the Baseline visit

Treatment with allergen immunotherapy within 6 months before Screening

Treatment with leukotriene inhibitors within 4 weeks before the Baseline visit

Treatment with systemic corticosteroids within 4 weeks before the Baseline visit

Treatment with topical corticosteroids, tacrolimus, and/or pimecrolimus within 1 week before the Baseline visit

Systemic treatment for AD with an immunosuppressive or immunomodulating substance, eg, cyclosporine, mycophenolate-mofetil, IFN-γ, phototherapy (narrow band ultraviolet B [NBUVB], ultraviolet B [UVB], ultraviolet A1 [UVA1], psoralen + ultraviolet A [PUVA]), azathioprine, methotrexate, within 4 weeks before the Baseline visit and within 8 weeks for biologics

Use of any concomitant medication that is a moderate or strong inhibitor or inducer of CYP3A4 unless stopped 14 days prior to start of study treatment. Please refer to Section 28 (Appendix 1) for examples of such medications.

Use of any concomitant medication that is an inhibitor or inducer of P glycoprotein (P-gp) unless stopped 14 days prior to the start of study treatment. Please refer to Section 28 (Appendix 1) for examples of such medications.

Use of any concomitant medication that is a sensitive substrate of CYP3A4 and that, if underdosed, would constitute a significant risk to the subject. Individual cases may be discussed with the MM. Please refer to Section 28 (Appendix 1) for examples of such medications.

Use of a necessary concomitant medication where the exposure is dependent on drug transporters organic anion transporting polypeptide1B3 (OATP1B3) or multidrug and toxin extrusion protein 1 or 2-K (MATE1, MATE2-K) and that if overdosed would constitute a significant risk to the patient. Individual cases may be discussed with the MM

Subjects who have failed prior systemic treatment to selective inhibitor agents that regulate the interleukin signaling pathway (eg, dupilumab, JAK1 inhibitors except for veracitinib)

Treatment of AD with active medications (eg, Atopiclair®, MimyX®, Epicerum®, Cerave®, etc) within 1 week before the Baseline visit

Chronic or acute infection requiring treatment with oral or IV antibiotics, anti-virals, anti-parasitics, anti-protozoals, or anti-fungals within 4 weeks before the Baseline visit, or superficial skin infections within 1 week before the Baseline visit

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Eligibility

Age eligible for study : 18 and older

Healthy volunteers accepted : Yes

Gender eligible for study: All

Things to know

Study dates

Study start: 2022-03-07

Primary completion: 2024-06-30

Study completion finish: 2024-09-30

Study type

TREATMENT

Phase

PHASE1

Trial ID

NCT05215808

Intervention or treatment

DRUG: RBN-3143

Conditions

• Atopic Dermatitis

Condition: Atopic Dermatitis
DRUG: RBN-3143
Woolloongabba, Queensland, Australia and more
Sponsor: Ribon Therapeutics, Inc.

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Find a site

Closest Location:

Veracity Clinical Research

Research sites nearby

Select from list below to view details:

Veracity Clinical Research
Woolloongabba, Queensland, Australia
CMAX Clinical Research Pty Ltd
Adelaide, Not Specified, Australia

Study Plan

This section provides details of the study plan, including how the study is designed and what the study is measuring.

How is the study designed?

Participant Group/Arm	Intervention/Treatment
EXPERIMENTAL: RBN-3143 RBN-3143 in single ascending dose followed by multiple ascending dose cohorts, randomized 3:1 ratio	DRUG: RBN-3143 Oral Administration of tablets
ACTIVE_COMPARATOR: Placebo Placebo randomized in 1:3 ratio with ascending RBN-3143 single and multiple dosing	DRUG: RBN-3143 Oral Administration of tablets
OTHER: Pantoprazole Open Label PPI cohort to evaluate concurrent administration of pantoprazole on RBN-3143 pharmacokinetics	DRUG: RBN-3143 Oral Administration of tablets
OTHER: Midazolam Open Label DDI Cohort (12 subjects) to evaluate the effect of RBN-3143 on the exposure of midazolam, a sensitive CYP3A4 substrate	DRUG: RBN-3143 Oral Administration of tablets

What is the study measuring?

Primary outcome

Primary Outcome Measure	Primary Outcome Description	Primary Outcome Time Frame
Safety determined by DLTs	Incidence rate of Dose limiting Toxicities (DLTs) of RBN 3143	30 days

Secondary outcome

Secondary Outcome Measure	Secondary Outcome Description	Secondary Outcome Time Frame
Cmax of RBN-3143	Assessment of maximum plasma concentration (Cmax) of RBN-3143	Predose through 72 hours
Tmax of RBN-3143	Time to maximum plasma concentration (Tmax)	Predose through 72 hours
AUC of RBN-3143	Assessment of area under the curve (AUC)	Predose through 72 hours
T1/2 of RBN-3143	Assessment of terminal half-life (T1/2)	Predose through 72 hours
CYP3A4 Assessment	Evaluate the effect of RBN-3143 on the exposure of midazolam	Through Day 19
QTc	Assessment of corrected QT intervals via Fridericia's formula	Predose through Day 7

Frequently Asked Questions

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References

Clinical Trials Gov: SAD/MAD Safety and PK Study of RBN-3143 in Healthy and Atopic Dermatitis Subjects