Evaluation of Safety and Pharmacokinetics of Oral Controlled-ileal-release Nicotinic Acid (CIR-NA) Compared to Immediate-release Nicotinic Acid and Placebo in Healthy Subjects and Subjects With Prediabetes

University Hospital Schleswig-Holstein (UKSH)

Status and phase

Completed

Phase 1

Conditions

Pharmacokinetic

Safety Issues

Treatments

Drug: Placebo controlled-ileal-release nicotinic acid (SAD/MAD)

Drug: Placebo immediate-release nicotinic acid (SAD)

Drug: controlled-ileal-release nicotinic acid (SAD/ MAD/MD) single- and multiple-ascending dose (SAD/MAD) or multiple dose (MD)

Drug: immediate-release nicotinic acid (SAD)

Study type

Interventional

Funder types

Other

Identifiers

NCT06378125

CIR-NA I

Details and patient eligibility

About

A double-blind, randomised, placebo-controlled, single-ascending and multiple-ascending dose trial to evaluate the safety and pharmacokinetics of oral controlled-ileal-release nicotinic acid (CIR-NA) compared to immediate-release nicotinic acid and placebo in healthy subjects and subjects with prediabetes.

Full description

Recently, administration of one form of vitamin B3, Nicotinamide (NAM), has been shown to improve the host-microbiome interaction in a mouse model, especially when administered in a controlled-release formulation targeting the ileocolic region. Thus, NAM and also the other form of vitamin B3, Nicotinicacid (NA), were identified as promising candidates for a gut-targeted microbiome intervention.

As the upper gastrointestinal tract efficiently absorbs amino acids and vitamins, simply increasing the NA and/or NAM content in human food would not be expected to deliver these molecules in sufficient amounts into the lower ileum and colon, where most of the microbiota are located. Moreover, adverse effects such as flushing or gastrointestinal symptoms can occur under high and immediately systemically available dosage of NA. Therefore, the novel CIR-NA formulation will be applied to deliver NA to the lower ileum and colon to tar-get the gut microbiome, while largely avoiding systemic exposure, as the terminal ileum and colon have a much lower absorptive capacity than the stomach and upper small intestine.

Both in the single- and multiple-ascending (SAD/MAD) part of the study, CIR-NA or placebo tablets will be self-administered orally, with daily doses of 100 mg (1 tablet), 200 mg (2 tablets), 500 mg (5 tablets) or 1,000 mg CIR-NA (10 tablets) or the corresponding amounts of placebo tablets. In the SAD part, an additional dose of 2,000 mg CIR-NA or placebo (20 tablets) will be self-administered.After completion of the SAD and the 200 mg MAD part in healthy subjects, an additional mul-tiple dose part (200 mg/d CIR-NA) in subjects with PreD (MD-PreD part) will start in parallel to the further dose groups of the MAD part.

Enrollment

60 patients

Sex

All

Ages

18 to 65 years old

Volunteers

Accepts Healthy Volunteers

Inclusion and exclusion criteria

Main inclusion and exclusion criteria

Inclusion criteria for the SAD and MAD parts with healthy subjects:

Male and female subjects aged 18 to 65 years.
Healthy subjects without relevant medical conditions.
Ability to understand and comply with the protocol.
Signed written Informed Consent.
A BMI of 18.5 to 29.99 kg/m².
Non-smoker or light smoker (average of <7 cigarettes per week) and no history of longterm, heavy smoking (>10 pack-years).

Inclusion criteria for the MD-Part (subjects with prediabetes):

Male and female subjects aged 18 to 65 years.
Previously diagnosed prediabetes with confirmation via the HbA1c level (5.7 to < 6.5%) at the screening visit.
Subjects without relevant medical conditions and without clinically significant impairment of renal or hepatic function.
Ability to understand and comply with the protocol.
Signed written Informed Consent.
A body mass index of 25 to 40 kg/m², both inclusive .
Non-smoker or light smoker (average of <7 cigarettes per week) and no history of longterm, heavy smoking (>10 pack-years).

Exclusion criteria for the SAD, MAD and MD part with healthy subjects and subjects with prediabetes:

Pre-existing relevant medical conditions.
Clinically relevant abnormal findings in medical history or screening assessments.
Participation in a clinical study.
Use of any prescribed or over-the-counter medication, food supplements or herbal preparations.
Use of antibiotics (systemic or gut-acting [non-absorbed]).
Pregnant or breastfeeding women or women of childbearing potential and male participants with female partners of childbearing age not using highly effective contraception till at least 1 month after last dosing of investigational medicinal product (IMP).
Legal incapacity.
Indications that the patient may be unable to comply with the study procedures, e.g. language barriers precluding adequate understanding or cooperation

Trial design

Primary purpose

Other

Allocation

Randomized

Interventional model

Sequential Assignment

Masking

Double Blind

60 participants in 2 patient groups

healthy subjects healthy subjects

Experimental group

Description:

single-ascending and multipleascending doses (SAD/MAD)

Treatment:

Drug: immediate-release nicotinic acid (SAD)

Drug: controlled-ileal-release nicotinic acid (SAD/ MAD/MD) single- and multiple-ascending dose (SAD/MAD) or multiple dose (MD)

Drug: Placebo immediate-release nicotinic acid (SAD)

Drug: Placebo controlled-ileal-release nicotinic acid (SAD/MAD)

subjects with prediabetes

Experimental group

Description:

multiple dose (MD)

Treatment:

Drug: controlled-ileal-release nicotinic acid (SAD/ MAD/MD) single- and multiple-ascending dose (SAD/MAD) or multiple dose (MD)

Trial contacts and locations

Central trial contact

Corinna Geisler, PhD

Data sourced from clinicaltrials.gov

Clinical trials

Find clinical trials Trials by location

Research sites

Find research sites Learn about CTV for professionals

Resources

Contact CTV support

Legal

Privacy Notice Terms