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Evaluate the PK, Safety, Tolerability of Ferric Maltol at 3 Dosage Levels in Paediatric Subjects With Iron Deficiency

Primary Purpose

Iron Deficiency, Anaemia in Children, Iron-Deficiency

Status

Completed

Phase

Phase 1

Locations

United Kingdom

Study Type

Interventional

Intervention

Ferric Maltol

About this trial

This is an interventional other trial for Iron Deficiency, Anaemia in Children

Eligibility Criteria

10 Years - 17 Years (Child)All SexesDoes not accept healthy volunteers

Inclusion Criteria:

Ability to understand the information given in the Independent Ethics Committee (IEC) approved Information Sheet and Consent form. The parent or guardian of the study subject must sign and date the informed consent and authorisation to use protected health information (PHI) in accordance with national and local subject privacy regulations prior to any study mandated procedure. The study participant will be asked to provide their assent to participate in the study using the IEC approved Assent form.
Willing and able to comply with study requirements.
Age ≥10 to ≤17 years at the time of informed consent and throughout duration of the study.
A current diagnosis of iron deficiency (with or without anaemia); iron deficiency defined by ferritin <30 µg/L, or ferritin <50 µg/L with transferrin saturation (TSAT) <20%, as measured by the central laboratory at the Screening visit (subjects with or without anaemia may be enrolled providing Hb is ≥8.5 g/dL as measured at the Screening visit).
Where appropriate, female subjects of childbearing potential must agree to use a reliable method of contraception until study completion and for at least 4 weeks following their final study visit. Reliable contraception is defined as a method which results in a low failure rate, i.e., less than 1% per year when used consistently and correctly, such as implants, injectables, some intrauterine contraceptive devices (IUDs), complete sexual abstinence, a vasectomized partner and oral contraceptive medications.

Exclusion Criteria:

Has untreated or untreatable severe malabsorption syndrome e.g., untreated coeliac disease
Has received within 28 days prior to Screening intramuscular or intravenous (IV) injection or administration of depot iron preparation.
Has received oral iron supplementation within 7 days prior to Screening
Has received blood transfusion within 12 weeks prior to Screening or is scheduled to have blood transfusion or donations during the study period.
Has concomitant disease that would significantly compromise iron absorption or absorbed iron utilisation such as swallowing disorders and/or extensive small bowel resection.
Has chronic renal disease (eGFR <30mL/min), as assessed at Screening based on serum creatinine.
Known hypersensitivity or allergy to either the active substance or excipients of Ferric Maltol capsules.
Has a known contraindication for treatment with iron preparations, e.g. haemochromatosis, chronic haemolytic disease, sideroblastic anaemia, thalassemia, or lead intoxication induced anaemia.
Impaired liver function as indicated by alanine aminotransferase (ALT) or aspartate transaminase (AST)>2.0 times upper normal limit as measured at the Screening visit.
Active acute inflammatory disease, including IBD flare or disease exacerbation, which in the opinion of the Investigator, is clinically significant.
Active chronic or acute infectious diseases requiring antibiotic treatment.
Pregnant or breast feeding.
Concomitant medical conditions with extensive active bleeding, other than menstrual cycles; subjects who suffer from menorrhagia may be included at the Investigator's discretion.
Scheduled or expected hospitalisation and/or surgery during the course of the study
Participation in any other interventional clinical study within 28 days prior to Screening.
Cardiovascular, liver, renal, hematologic, psychiatric, neurologic, gastrointestinal, immunologic, endocrine, metabolic, respiratory or central nervous system disease that, in the opinion of the Investigator, may adversely affect the safety of the subject and/or objectives of the study drug or severely limit the lifespan of the subject.
Any other unspecified reason that, in the opinion of the Investigator or the Sponsor make the subject unsuitable for enrolment.

Sites / Locations

Leicester Royal Infirmary
Alder Hey Children's NHS Foundation Trust
University College London Hospitals NHS Foundation Trust
King's College Hospital NHS Foundation Trust
Great Ormond Street Hospital
Royal Manchester Children's Hospital
Nottingham University Hospital

Arms of the Study

Arm 1

Arm 2

Arm 3

Arm Type

Active Comparator

Arm Label

30 mg Ferric Maltol

16.6 mg Ferric Maltol

7.8 mg Ferric Maltol

Arm Description

12 subjects will receive 30 mg Ferric Maltol twice daily for 9 days (Days 1-9) plus a final 30mg dose on the morning of Day 10. PK study Day 1 & Day 10.

12 subjects will receive 16.6 mg Ferric Maltol twice daily for 9 days (Days 1-9) plus a final 16.6mg dose on the morning of Day 10. PK study Day 1 & Day 10.

12 subjects will receive 7.8 mg Ferric Maltol twice daily for 9 days (Days 1-9) plus a final 7.8mg dose on the morning of Day 10. PK study Day 1 & Day 10.

Outcomes

Primary Outcome Measures

Maximum Plasma Concentration [Cmax] of Maltol Glucuronide on Day 1

Descriptive statistics and population PK analysis of maltol glucuronide Cmax from PK samples collected on Day 1. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Maximum Plasma Concentration [Cmax] of Maltol Glucuronide on Day 10

Descriptive statistics and population PK analysis of maltol glucuronide Cmax from PK samples collected on Day 10. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Area Under The Curve [AUC] of Maltol Glucuronide on Day 1

Descriptive statistics and population PK analysis of maltol glucuronide AUC from PK samples collected on Day 1. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Area Under The Curve [AUC] of Maltol Glucuronide on Day 10

Descriptive statistics and population PK analysis of maltol AUC from PK samples collected on Day 10. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Average Plasma Concentration [Cave(0-6h)] of Maltol Glucuronide on Day 10

Descriptive statistics and population PK analysis of maltol glucuronide Cave(0-6h) from PK samples collected on Day 10. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Time of Maximum Plasma Concentration [Tmax] of Maltol Glucuronide on Day 1

Descriptive statistics and population PK analysis of maltol glucuronide Tmax from PK samples collected on Day 1. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Time of Maximum Plasma Concentration [Tmax] of Maltol Glucuronide on Day 10

Descriptive statistics and population PK analysis of maltol glucuronide Tmax from PK samples collected on Day 10. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Half Life [t1/2] of Maltol Glucuronide on Day 1

Descriptive statistics and population PK analysis of maltol glucuronide t1/2 from PK samples collected on Day 1. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Ratio of Maximum Plasma Concentration [Cmax] of Maltol Glucuronide on Day 10/Day 1

Descriptive statistics of ratio maltol glucuronide Cmax Day 10/Day 10 from PK samples collected on Day 1 and Day 10. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Ratio of Area Under The Curve [AUC] of Maltol Glucuronide on Day 10/Day 1

Descriptive statistics of ratio maltol glucuronide AUC Day 10/Day 10 from PK samples collected on Day 1 and Day 10. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Average Serum Concentration [Cave(0-6h)] of Iron on Day 10

Descriptive statistics and population PK analysis of iron Cave(0-6h) from PK samples collected on Day 10. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Change From Pre-Dose (Ctrough) to Maximum Post-Dose (Cmax) in Serum Iron on Day 1

Descriptive statistics and population PK analysis of change in serum iron [Ctrough to Cmax] from PK samples collected on Day 1. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Change From Pre-Dose (Ctrough) to Maximum Post-Dose (Cmax) in Serum Iron on Day 10

Descriptive statistics and population PK analysis of change in serum iron [Ctrough to Cmax] from PK samples collected on Day 10. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Pre-dose Adjusted Incremental Area Under the Curve [AUC(0-6h)] of Serum Iron on Day 1

Descriptive statistics and population PK analysis of pre-dose adjusted incremental AUC(0-6h) of serum iron from PK samples collected on Day 1. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Pre-dose Adjusted Incremental Area Under the Curve [AUC(0-6h)] of Serum Iron on Day 10

Descriptive statistics and population PK analysis of pre-dose adjusted incremental AUC(0-6h) of serum iron from PK samples collected on Day 10. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Pre-dose Adjusted Incremental Area Under the Curve [AUC(0-6h)] of Transferrin Saturation (TSAT) on Day 1

Descriptive statistics and population PK analysis of pre-dose adjusted incremental AUC(0-6h) of TSAT from PK samples collected on Day 1. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Pre-dose Adjusted Incremental Area Under the Curve [AUC(0-6h)] of Transferrin Saturation (TSAT) on Day 10

Descriptive statistics and population PK analysis of pre-dose adjusted incremental AUC(0-6h) of TSAT from PK samples collected on Day 10. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Apparent Systemic Clearance (CL/F) of Iron on Day 1

Descriptive statistics and population PK analysis of serum iron CL/F from PK samples collected on Day 1

Apparent Systemic Clearance (CL/F) of Iron on Day 10

Descriptive statistics and population PK analysis of serum iron CL/F from PK samples collected on Day 10

Apparent Volume of Distribution (V/F) of Iron on Day 1

Descriptive statistics and population PK analysis of iron V/F from PK samples collected on Day 1. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Apparent Volume of Distribution (V/F) of Transferrin Saturation (TSAT) on Day 1

Descriptive statistics and population PK analysis of TSAT V/F from PK samples collected on Day 1

Apparent Volume of Distribution (V/F) of Transferrin Saturation (TSAT) on Day 10

Descriptive statistics and population PK analysis of TSAT V/F from PK samples collected on Day 10

Ratio Auc(0-6) Maltol Glucuronide Day 10/Day 1

Ratio AUC0-6h measured after last dose of Ferric Maltol on Day 10 vs first dose Day 1.

Serum Iron - RAUC(0-6h) D10/D1

Serum Iron - RAUC(0-6h) Day 10/Day 1

Transferrin Saturation (%) Day 1, Baseline

Transferrin Saturation (TSAT%) Day 1, baseline

Transferrin Saturation (%) Day 1, Maximum Response (%)

Transferrin Saturation (TSAT%) Day 1, maximum response (%)

Transferrin Saturation Day 1, Time to Maximum Response Tmax

Transferrin Saturation (TSAT%) Day 1, time to maximum response Tmax (h). Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Transferrin Saturation (%) Day 10, Maximum Response (%)

Transferrin Saturation (TSAT%) Day 10, maximum response (%). Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Transferrin Saturation Day 10, Time to Maximum Response Tmax

AUC0-inf Day 1 for Maltol Glucuronide

AUC0-inf for Maltol Glucuronide from PK samples collected on Day 1. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

AUC0-tau Day 10 for Maltol Glucuronide

AUC0-tau for Maltol Glucuronide from PK samples collected on Day 10. Area under the plasma concentration versus time curve from time 0 to tau.

Cthrough for Maltol Glucuronide Day 10

Change from pre-dose to last PK samples collected on Day 10 for maltol glucuronide.Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Serum Iron Cmax Day 1

Maximum serum concentration of serum iron on Day 1. Each subject had 1 pre-dose (0h) and 2 post dose PK blood sampling between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h). Subjects were assigned to PK blood sampling schedule. For each individual subject the PK blood sampling schedule was the same on Day 1 and Day 10.

Serum Iron Cmax on Day 10

Maximum serum concentration of serum iron on Day 10.

Plasma Maltol Glucuronide Cthrough D10/Day1

Minimum concentration between dose time and dose time+TAU

Apparent Systemic Clearance (CL/F) of Transferrin Saturation (TSAT) on Day 1

Descriptive statistics and population PK analysis of serum TSAT CL/F from PK samples collected on Day 1

Apparent Systemic Clearance (CL/F) of Transferrin Saturation (TSAT) on Day 10

Descriptive statistics and population PK analysis of serum TSAT CL/F from PK samples collected on Day 10

Apparent Systemic Clearance (CL/F) of Maltol Glucuronide on Day 1

Descriptive statistics and population PK analysis of plasma maltol glucuronide CL/F from PK samples collected on Day 1.

Apparent Systemic Clearance (CL/F) of Maltol Glucuronide on Day 10

Descriptive statistics and population PK analysis of plasma maltol glucuronide CL/F from PK samples collected on Day 10.

Secondary Outcome Measures

Transferrin - Change From Baseline to Day 10, Predose

Change calculated as difference in values measured at Day 1, predose (Baseline) and on Day 10, predose

Ferritin - Change From Baseline to Day 10, Predose

Change calculated as difference in values measured at Day 1, predose (Baseline) and on Day 10, predose.

Total Iron Binding Capacity - Change From Day 1 to Day 10, Predose

Change calculated as difference in values measured at Day 1, predose and on Day 10, predose

UIBC - Change From Day 1 to Day 10, Predose

Change calculated as difference in values measured at Day 1, predose and on Day 10, predose

Negative and Positive NTBI Tests on Day 1

Negative and Positive Non-Transferrin Bound Iron [NTBI] tests on Day 1, predose

Change From Baseline to Day 10 in Haemoglobin Concentration

Change calculated as difference in values measured at Screening (Baseline) and on Day 10

Change From Baseline to Day 10 in Absolute Reticulocyte Count

Change from Baseline to Day 10 in Absolute Reticulocyte Count collected from PK samples

Treatment-emergent Adverse Events (AEs) Leading to Premature Discontinuation of Study Drug/PK Assessments

Descriptive summary of incidence and causal relationship of treatment-emergent adverse events leading to discontinuation of study drug/PK assessments according to MedDRA preferred term (PT) and system organ class (SOC)

Changes in 12-lead ECG Parameters From Screening to Day 10

Overall clinical interpretation of routine ECG parameters from Screening to Day 10

Concomitant Medications

Number of subjects with concomitant medications Taken by >5% of Subjects

Negative and Positive NTBI Tests on Day 10, Predose

Negative and Positive Non-Transferrin Bound Iron [NTBI] tests on Day 10, predose

Treatment-emergent Serious Adverse Event (TESAE)

Descriptive summary of TESAE according to MedDRA preferred Term

Full Information

NCT ID

NCT03181451

First Posted

May 23, 2017

Last Updated

September 13, 2021

Sponsor

Shield Therapeutics

Collaborators

Medpace, Inc.

1. Study Identification

Unique Protocol Identification Number

NCT03181451

Brief Title

Evaluate the PK, Safety, Tolerability of Ferric Maltol at 3 Dosage Levels in Paediatric Subjects With Iron Deficiency

Official Title

A Phase 1, Open-Label, Randomised, Repeat Dose, Parallel Group Study to Evaluate the PK, Safety, Tolerability of Ferric Maltol at 3 Dosage Levels in Paediatric Subjects Aged 10-17 Years of Age With Iron Deficiency

Study Type

Interventional

2. Study Status

Record Verification Date

September 2021

Overall Recruitment Status

Completed

Study Start Date

March 14, 2017 (Actual)

Primary Completion Date

March 28, 2018 (Actual)

Study Completion Date

March 28, 2018 (Actual)

3. Sponsor/Collaborators

Responsible Party, by Official Title

Sponsor

Name of the Sponsor

Shield Therapeutics

Collaborators

Medpace, Inc.

4. Oversight

Studies a U.S. FDA-regulated Drug Product

Studies a U.S. FDA-regulated Device Product

Data Monitoring Committee

5. Study Description

Brief Summary

The study has been designed to establish the pharmacokinetics (PK) and iron uptake of Ferric Maltol in children and adolescents aged 10-17 years using two (2) lower dose strengths in comparison to the EU-approved 30mg BID dose in adults with IDA in IBD.

Detailed Description

Phase I, open label, randomized, repeat dose, multicentre, pharmacokinetic study to assess the Safety and Tolerability of Ferric Maltol in 3 different dosages. 36 eligible patients will be randomized in a 1:1:1 ratio to one of the following 3 dosages for 9 days BID and a single dose on Day 10: 30mg ferric maltol capsules 16.6 mg ferric maltol capsules 7.8 mg ferric maltol capsules Subject participation in the study will consist of 3 stages: Screening: up to 14 days Treatment period: 10 days treatment period with 2 visits on Day 1 and Day 10 for PK blood sampling. Patients will be randomly allocated to one of the three Ferric Maltol dose groups according to centralized treatment allocation scheme. Post-treatment Safety Follow-up:3-10 days following completion of the treatment period or premature discontinuation of study medication

6. Conditions and Keywords

Primary Disease or Condition Being Studied in the Trial, or the Focus of the Study

Iron Deficiency, Anaemia in Children, Iron-Deficiency

7. Study Design

Primary Purpose

Other

Study Phase

Phase 1

Interventional Study Model

Parallel Assignment

Model Description

Subjects will be randomized in a 1:1:1 ratio and stratified by co-variates for age and sex. This will ensure that a minimum of 25% of each gender and at least 3 children per age group are enrolled in each Ferric Maltol dose group.

Masking

None (Open Label)

Allocation

Randomized

Enrollment

37 (Actual)

8. Arms, Groups, and Interventions

Arm Title

30 mg Ferric Maltol

Arm Type

Active Comparator

Arm Description

12 subjects will receive 30 mg Ferric Maltol twice daily for 9 days (Days 1-9) plus a final 30mg dose on the morning of Day 10. PK study Day 1 & Day 10.

Arm Title

16.6 mg Ferric Maltol

Arm Type

Active Comparator

Arm Description

12 subjects will receive 16.6 mg Ferric Maltol twice daily for 9 days (Days 1-9) plus a final 16.6mg dose on the morning of Day 10. PK study Day 1 & Day 10.

Arm Title

7.8 mg Ferric Maltol

Arm Type

Active Comparator

Arm Description

12 subjects will receive 7.8 mg Ferric Maltol twice daily for 9 days (Days 1-9) plus a final 7.8mg dose on the morning of Day 10. PK study Day 1 & Day 10.

Intervention Type

Drug

Intervention Name(s)

Ferric Maltol

Other Intervention Name(s)

ST10, Feraccru

Intervention Description

To assess the pharmacokinetics and iron uptake of Ferric Maltol through measurement of serum iron, transferrin saturation (TSAT) and plasma concentrations of maltol and maltol glucuronide.

Primary Outcome Measure Information:

Title

Maximum Plasma Concentration [Cmax] of Maltol Glucuronide on Day 1

Description

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Maximum Plasma Concentration [Cmax] of Maltol Glucuronide on Day 10

Description

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Area Under The Curve [AUC] of Maltol Glucuronide on Day 1

Description

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Area Under The Curve [AUC] of Maltol Glucuronide on Day 10

Description

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Average Plasma Concentration [Cave(0-6h)] of Maltol Glucuronide on Day 10

Description

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Time of Maximum Plasma Concentration [Tmax] of Maltol Glucuronide on Day 1

Description

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Time of Maximum Plasma Concentration [Tmax] of Maltol Glucuronide on Day 10

Description

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Half Life [t1/2] of Maltol Glucuronide on Day 1

Description

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Ratio of Maximum Plasma Concentration [Cmax] of Maltol Glucuronide on Day 10/Day 1

Description

Time Frame

Day 1 and Day 10, pre-dose and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Ratio of Area Under The Curve [AUC] of Maltol Glucuronide on Day 10/Day 1

Description

Time Frame

Day 1 and Day 10, pre-dose and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Average Serum Concentration [Cave(0-6h)] of Iron on Day 10

Description

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Change From Pre-Dose (Ctrough) to Maximum Post-Dose (Cmax) in Serum Iron on Day 1

Description

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Change From Pre-Dose (Ctrough) to Maximum Post-Dose (Cmax) in Serum Iron on Day 10

Description

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Pre-dose Adjusted Incremental Area Under the Curve [AUC(0-6h)] of Serum Iron on Day 1

Description

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Pre-dose Adjusted Incremental Area Under the Curve [AUC(0-6h)] of Serum Iron on Day 10

Description

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Pre-dose Adjusted Incremental Area Under the Curve [AUC(0-6h)] of Transferrin Saturation (TSAT) on Day 1

Description

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Pre-dose Adjusted Incremental Area Under the Curve [AUC(0-6h)] of Transferrin Saturation (TSAT) on Day 10

Description

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (between (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Apparent Systemic Clearance (CL/F) of Iron on Day 1

Description

Descriptive statistics and population PK analysis of serum iron CL/F from PK samples collected on Day 1

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Apparent Systemic Clearance (CL/F) of Iron on Day 10

Description

Descriptive statistics and population PK analysis of serum iron CL/F from PK samples collected on Day 10

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Apparent Volume of Distribution (V/F) of Iron on Day 1

Description

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Apparent Volume of Distribution (V/F) of Transferrin Saturation (TSAT) on Day 1

Description

Descriptive statistics and population PK analysis of TSAT V/F from PK samples collected on Day 1

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Apparent Volume of Distribution (V/F) of Transferrin Saturation (TSAT) on Day 10

Description

Descriptive statistics and population PK analysis of TSAT V/F from PK samples collected on Day 10

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Ratio Auc(0-6) Maltol Glucuronide Day 10/Day 1

Description

Ratio AUC0-6h measured after last dose of Ferric Maltol on Day 10 vs first dose Day 1.

Time Frame

Day 1 to Day 10 (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Serum Iron - RAUC(0-6h) D10/D1

Description

Serum Iron - RAUC(0-6h) Day 10/Day 1

Time Frame

Measured after first and last dose of Ferric Maltol on Day 1 & Day 10 (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Transferrin Saturation (%) Day 1, Baseline

Description

Transferrin Saturation (TSAT%) Day 1, baseline

Time Frame

Measured after first dose of Ferric Maltol on Day 1 (0h)

Title

Transferrin Saturation (%) Day 1, Maximum Response (%)

Description

Transferrin Saturation (TSAT%) Day 1, maximum response (%)

Time Frame

Measured after first dose of Ferric Maltol on Day 1 (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Transferrin Saturation Day 1, Time to Maximum Response Tmax

Description

Time Frame

Measured after first dose of Ferric Maltol on Day 1. (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Transferrin Saturation (%) Day 10, Maximum Response (%)

Description

Time Frame

Measured after last dose of Ferric Maltol on Day 10. (0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Transferrin Saturation Day 10, Time to Maximum Response Tmax

Description

Time Frame

Measured after first dose of Ferric Maltol on Day 10. (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h).

Title

AUC0-inf Day 1 for Maltol Glucuronide

Description

Time Frame

Measured after first dose of Ferric Maltol on Day 1 (0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

AUC0-tau Day 10 for Maltol Glucuronide

Description

AUC0-tau for Maltol Glucuronide from PK samples collected on Day 10. Area under the plasma concentration versus time curve from time 0 to tau.

Time Frame

Measured after last dose of Ferric Maltol on Day 10. (0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Cthrough for Maltol Glucuronide Day 10

Description

Time Frame

Day 10 pre-dose to last (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Serum Iron Cmax Day 1

Description

Time Frame

Day 1 (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Serum Iron Cmax on Day 10

Description

Maximum serum concentration of serum iron on Day 10.

Time Frame

Day 10 (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Plasma Maltol Glucuronide Cthrough D10/Day1

Description

Minimum concentration between dose time and dose time+TAU

Time Frame

Day 10 (0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Apparent Systemic Clearance (CL/F) of Transferrin Saturation (TSAT) on Day 1

Description

Descriptive statistics and population PK analysis of serum TSAT CL/F from PK samples collected on Day 1

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h

Title

Apparent Systemic Clearance (CL/F) of Transferrin Saturation (TSAT) on Day 10

Description

Descriptive statistics and population PK analysis of serum TSAT CL/F from PK samples collected on Day 10

Time Frame

Day 10 pre-final dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h)

Title

Apparent Systemic Clearance (CL/F) of Maltol Glucuronide on Day 1

Description

Descriptive statistics and population PK analysis of plasma maltol glucuronide CL/F from PK samples collected on Day 1.

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h

Title

Apparent Systemic Clearance (CL/F) of Maltol Glucuronide on Day 10

Description

Descriptive statistics and population PK analysis of plasma maltol glucuronide CL/F from PK samples collected on Day 10.

Time Frame

Day 1 pre-first dose of Ferric Maltol and up to 6 hours post-dose (0h, 0.5-1h, 1-2h, 2-3h, 3-4h, 4-6h

Secondary Outcome Measure Information:

Title

Transferrin - Change From Baseline to Day 10, Predose

Description

Change calculated as difference in values measured at Day 1, predose (Baseline) and on Day 10, predose

Time Frame

Day 1 pre-dose to Day 10 pre-dose (0h on each day)

Title

Ferritin - Change From Baseline to Day 10, Predose

Description

Change calculated as difference in values measured at Day 1, predose (Baseline) and on Day 10, predose.

Time Frame

Pre-dose on Day 1 to Day 10 (0h)

Title

Total Iron Binding Capacity - Change From Day 1 to Day 10, Predose

Description

Change calculated as difference in values measured at Day 1, predose and on Day 10, predose

Time Frame

Predose from Day 1 to Day 10 (0h on each day)

Title

UIBC - Change From Day 1 to Day 10, Predose

Description

Change calculated as difference in values measured at Day 1, predose and on Day 10, predose

Time Frame

Pre-dose on Day 1 to Day 10 (0h each day)

Title

Negative and Positive NTBI Tests on Day 1

Description

Negative and Positive Non-Transferrin Bound Iron [NTBI] tests on Day 1, predose

Time Frame

Day 1 (0h)

Title

Change From Baseline to Day 10 in Haemoglobin Concentration

Description

Change calculated as difference in values measured at Screening (Baseline) and on Day 10

Time Frame

Screening and Day 10 (1-4 hours post-dose)

Title

Change From Baseline to Day 10 in Absolute Reticulocyte Count

Description

Change from Baseline to Day 10 in Absolute Reticulocyte Count collected from PK samples

Time Frame

Change calculated as difference in values measured at Screening (Baseline) and on Day 10.

Title

Treatment-emergent Adverse Events (AEs) Leading to Premature Discontinuation of Study Drug/PK Assessments

Description

Time Frame

From first dose of Ferric Maltol on Day 1 through study completion, on average 4 weeks

Title

Changes in 12-lead ECG Parameters From Screening to Day 10

Description

Overall clinical interpretation of routine ECG parameters from Screening to Day 10

Time Frame

Screening and Day 10 (1-4 hours post-dose)

Title

Concomitant Medications

Description

Number of subjects with concomitant medications Taken by >5% of Subjects

Time Frame

Screening, Day 1, Day 10 and Post-Study Follow-up visit, on average 4 weeks

Title

Negative and Positive NTBI Tests on Day 10, Predose

Description

Negative and Positive Non-Transferrin Bound Iron [NTBI] tests on Day 10, predose

Time Frame

Day 10

Title

Treatment-emergent Serious Adverse Event (TESAE)

Description

Descriptive summary of TESAE according to MedDRA preferred Term

Time Frame

From first dose of ferric maltol Day 1 through study completions, on average 4 weeks

10. Eligibility

Sex

All

Minimum Age & Unit of Time

10 Years

Maximum Age & Unit of Time

17 Years

Accepts Healthy Volunteers

Eligibility Criteria

Inclusion Criteria: Ability to understand the information given in the Independent Ethics Committee (IEC) approved Information Sheet and Consent form. The parent or guardian of the study subject must sign and date the informed consent and authorisation to use protected health information (PHI) in accordance with national and local subject privacy regulations prior to any study mandated procedure. The study participant will be asked to provide their assent to participate in the study using the IEC approved Assent form. Willing and able to comply with study requirements. Age ≥10 to ≤17 years at the time of informed consent and throughout duration of the study. A current diagnosis of iron deficiency (with or without anaemia); iron deficiency defined by ferritin <30 µg/L, or ferritin <50 µg/L with transferrin saturation (TSAT) <20%, as measured by the central laboratory at the Screening visit (subjects with or without anaemia may be enrolled providing Hb is ≥8.5 g/dL as measured at the Screening visit). Where appropriate, female subjects of childbearing potential must agree to use a reliable method of contraception until study completion and for at least 4 weeks following their final study visit. Reliable contraception is defined as a method which results in a low failure rate, i.e., less than 1% per year when used consistently and correctly, such as implants, injectables, some intrauterine contraceptive devices (IUDs), complete sexual abstinence, a vasectomized partner and oral contraceptive medications. Exclusion Criteria: Has untreated or untreatable severe malabsorption syndrome e.g., untreated coeliac disease Has received within 28 days prior to Screening intramuscular or intravenous (IV) injection or administration of depot iron preparation. Has received oral iron supplementation within 7 days prior to Screening Has received blood transfusion within 12 weeks prior to Screening or is scheduled to have blood transfusion or donations during the study period. Has concomitant disease that would significantly compromise iron absorption or absorbed iron utilisation such as swallowing disorders and/or extensive small bowel resection. Has chronic renal disease (eGFR <30mL/min), as assessed at Screening based on serum creatinine. Known hypersensitivity or allergy to either the active substance or excipients of Ferric Maltol capsules. Has a known contraindication for treatment with iron preparations, e.g. haemochromatosis, chronic haemolytic disease, sideroblastic anaemia, thalassemia, or lead intoxication induced anaemia. Impaired liver function as indicated by alanine aminotransferase (ALT) or aspartate transaminase (AST)>2.0 times upper normal limit as measured at the Screening visit. Active acute inflammatory disease, including IBD flare or disease exacerbation, which in the opinion of the Investigator, is clinically significant. Active chronic or acute infectious diseases requiring antibiotic treatment. Pregnant or breast feeding. Concomitant medical conditions with extensive active bleeding, other than menstrual cycles; subjects who suffer from menorrhagia may be included at the Investigator's discretion. Scheduled or expected hospitalisation and/or surgery during the course of the study Participation in any other interventional clinical study within 28 days prior to Screening. Cardiovascular, liver, renal, hematologic, psychiatric, neurologic, gastrointestinal, immunologic, endocrine, metabolic, respiratory or central nervous system disease that, in the opinion of the Investigator, may adversely affect the safety of the subject and/or objectives of the study drug or severely limit the lifespan of the subject. Any other unspecified reason that, in the opinion of the Investigator or the Sponsor make the subject unsuitable for enrolment.

Facility Information:

Facility Name

Leicester Royal Infirmary

City

Leicester

ZIP/Postal Code

LE1 5WW

Country

United Kingdom

Facility Name

Alder Hey Children's NHS Foundation Trust

City

Liverpool

ZIP/Postal Code

L14 5AB

Country

United Kingdom

Facility Name

University College London Hospitals NHS Foundation Trust

City

London

ZIP/Postal Code

NW1 2PG

Country

United Kingdom

Facility Name

King's College Hospital NHS Foundation Trust

City

London

ZIP/Postal Code

SE5 9RS

Country

United Kingdom

Facility Name

Great Ormond Street Hospital

City

London

ZIP/Postal Code

WC1N 3JH

Country

United Kingdom

Facility Name

Royal Manchester Children's Hospital

City

Manchester

ZIP/Postal Code

M13 9WL

Country

United Kingdom

Facility Name

Nottingham University Hospital

City

Nottingham

ZIP/Postal Code

NG7 2UH

Country

United Kingdom

12. IPD Sharing Statement

Plan to Share IPD

Learn more about this trial

Evaluate the PK, Safety, Tolerability of Ferric Maltol at 3 Dosage Levels in Paediatric Subjects With Iron Deficiency

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