FindTrial
Sign In

New Pathophysiological Pathways Involved in Iron Metabolism Disorder in Heart Failure

New Pathophysiological Pathways Involved in Iron Metabolism Disorder in Heart Failure: The IRON-PATH II Investigator Initiated Study

Status
UNKNOWN
Phases
Unknown
Study type
Observational
Source
ClinicalTrials.gov
Registry ID
NCT05000853
Acronym
IRON-PATH II
Enrollment
210
Registered
2021-08-11
Start date
2021-08-01
Completion date
2023-08-01
Last updated
2022-12-13

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

Conditions

Heart Failure

Keywords

Iron Deficiency, Machine Learning, Multi-Omics Approaches, Outcomes Research

Brief summary

The aim of our study is to understand the biological pathways involved in the occurrence of IDy in patients with HF since ID is very common and supposes a negative impact in terms of clinical outcomes in these patients. In this context, a deeper understanding of the mechanisms involved in the development of ID in these patients and the impact on the altered biological pathways after iron replenishment will pave the way for an improvement and simplification of the preventive strategies in patients with HF.

Detailed description

The IRON-PATH II Project is a pre-clinical and clinical study designed as a multicenter, prospective, observational (non-interventional), investigator initiated study. The total number of patients to be recruited will be 210 (80 patients without ID and 130 patients with ID). Patients will be recruited during 12 months in 7 centers across Spain and Portugal and followed for a fixed period of 12 months. The primary objective of the clinical study is to define pathways associated with systemic and tissue ID in HF patients compared with non-ID HF patients and explore the change in the patterns of pathway activation/suppression after irons status normalization in ID patients with intravenous iron treatment using an integrative omics and systems biology approach including whole-genome analysis of gene expression (transcriptome), protein synthesis (proteomics) and metabolic characterization (metabolomics) from blood samples. Key secondary objectives will include changes in patient-reported outcomes (PROMs) such as QoL, patient-reported experience measures (PREMs), the occurrence of events, among others between those with and without ID. The aims of the pre-clinical study is to confirm previous findings of the IRONPATH I study and to explore in vitro interventions in cardiac cells models with iron deficiency.

Interventions

DRUGIron Carboxymaltose

Iron supplementation when is needed according to usual care

Sponsors

Hospital Universitari de Bellvitge
Lead SponsorOTHER

Study design

Observational model
COHORT
Time perspective
PROSPECTIVE

Eligibility

Sex/Gender
ALL
Age
18 Years to No maximum
Healthy volunteers
No

Inclusion criteria

* Age ≥ 18 years old. * HF diagnosis according to European Society of Cardiology * LVEF≤50% (systolic HF). * Patients receiving oral standard medication for chronic HF. * Iron status evaluated in the last 3 months. * Written informed consent.

Exclusion criteria

* Age\<18 years old. * Intravenous or oral iron administration or under treatment with ESA (erythropoiesis-stimulating agents) in the previous 3 months. * Planned cardiac resynchronization therapy (CRT), revascularization and other major interventions including heart transplant or left ventricular assist device (LVAD) implantation in the next 3 months in patients with ID. * Planned uptitration of guideline-mandatory HF-modifying drugs in the next 3 months (except iron repletion) in patients with ID. * Moderate or severe anaemia (Hb\<11 g/dL). * The patient is unable or unwilling to give the informed consent to participate. * Unstable patients with signs of fluid overload or low cardiac output at the moment of enrollment. * Life expectancy less than 1 year (excluding HF). * The patient is considered not to be an adequate candidate for this study according to the decision of the local investigator.

Design outcomes

Primary

MeasureTime frameDescription
To define pathways associated with iron deficiency (ID) in heart failure (HF) patients compared with non-ID HF patientsTwelve months after inclusion the patientUsing an integrative omics and systems biology approach including whole-genome analysis of gene expression (transcriptome), protein synthesis (proteomics) and metabolic characterization (metabolomics) from blood samples.

Secondary

MeasureTime frameDescription
Functional Biomarkers (New York Heart Association [NYHA)Twelve months after inclusion the patientComparison between ID and non ID patients
Improvement of self-care using a validated scale (European Heart Failure Self-Care Behavior Scale).Twelve months after inclusion the patientComparison between ID and non ID patients
Patient-reported experience measures (PREMs) (IEXPAC)Twelve months after inclusion the patientComparison between ID and non ID patients
Prognostic biomarkers (NT-proBNP)Twelve months after inclusion the patientComparison between ID and non ID patients
Occurrence of events (all-cause death, HF-clinically related admissions, CV admissions)Twelve months after inclusion the patientComparison between ID and non ID patients
Functional Biomarkers (6-minutes walking test [6MWT] distance)Twelve months after inclusion the patientComparison between ID and non ID patients
Improvement of quality of life using a validated questionnaire (EUROQOL - 5D)Twelve months after inclusion the patientComparison between ID and non ID patients

Countries

Spain

Contacts

Primary ContactJosep Comin Colet, MD, PhD
jcomin@bellvitgehospital.cat+34 932607078
Backup ContactMaria del Mar Ras Jimenez, MD
mras@bellvitgehospital.cat+34 932607078

Outcome results

None listed

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