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ID
Source
Brief title
Health condition
Heart failure with preserved ejection fraction and iron deficiency
Sponsors and support
Intervention
Outcome measures
Primary outcome
- Is skeletal muscle metabolism impaired in HFpEF patients with iron deficiency, measured using CMR spectroscopy?
Secondary outcome
- Is microvascular function impaired in HFpEF patients with iron deficiency?
- Is exercise tolerance decreased in HFpEF patients with iron deficiency?
Background summary
Rationale:
Diabetes, obesity and hypertension, all highly present comorbidities in HFpEF, seem to drive this disease by inducing low-grade systemic inflammation which in turn induces microvascular dysfunction and activates a cascade of events. Several studies have demonstrated that HFpEF is a systemic disease that affects not only cardiac, but also peripheral muscle energy metabolism. Iron deficiency (ID) could be an important contributor in this pathophysiological process.
Iron deficiency is present in 50% of chronic HF patients. Although HFpEF was not excluded from these cohort studies, it mainly included HF with reduced ejection fraction (HFrEF).
We hypothesize that ID is an important factor in the limitation of exercise capacity in HFpEF. Systemic low-grade inflammation does not only lead to microvascular dysfunction but also to iron deficiency. Iron deficiency has a direct effect on the muscle. Not only on the cardiac muscle but also the skeletal muscle is affected, impairing muscle contraction strength but also energy metabolism. The primary focus of this study will be delivering proof that the alterations in the muscle are more severe in HFpEF patients with ID compared to without ID.
Objective:
To assess if skeletal muscle metabolism is impaired in HFpEF patients with iron deficiency compared to HFpEF patients without iron deficiency
Study design: Cross sectional study
Study population: All patients (>18 yr) with HFpEF
Main study parameters/endpoints:
The main study parameters is PCR recovery time, a measurement of PCR recovery time using MR spectroscopy
Secondary parameters/endpoints are:
- Microvascular function
o Glycocalyx thickness (um)
o Heat induced hyperaemic response (% skin hyperaemic response)
- Exercise tolerance
o 6 minute walk test distance (m)
o maximum exercise capacity (METs on exercise test)
Nature and extent of the burden and risks associated with participation, benefit and group relatedness:
There is a minimal burden associated with participation in this study. Measurements of ID are performed as part of routine examinations in the outpatient clinic.
1. MR spectroscopy is a non-invasive, non-radiation imaging technique. CMR has a low risk of contrast reaction. To date, MRI investigations have been performed in over 200 million patients. Worldwide and are regarded as extremely safe. MRI is painless and has no known short-term or long-term biological adverse effects. Deaths have only been reported when proper safety precautions were not taken.
Risks: There are very few risks known to be associated with MRI:
Changing radiofrequency pulses may produce heat. This is not known to cause any side effects. Loose metal objects in the patient or in the scanner room may cause damage to
the patient. When appropriate precautions are taken, this is rare to occur.
2.Glycocalyx thickness measurement is a non-invasive, endothelial function measurement method. This method has no contra-indications or adverse effects.
3.Heat-induced skin hyperaemic response, is a non-invasive, endothelial function measurement method. This method has no contraindications or adverse effects. The warm electrodes (warmth until 44° C) are not painful and just a slight local warmth can be felt.
Study objective
We hypothesize that ID is an important factor in the limitation of exercise capacity in HFpEF. Systemic low-grade inflammation does not only lead to microvascular dysfunction but also to iron deficiency. Iron deficiency has a direct effect on the muscle. Not only on the cardiac muscle but also the skeletal muscle is affected, impairing muscle contraction strength but also energy metabolism. The primary focus of this study will be delivering proof that the alterations in the muscle are more severe in HFpEF patients with ID compared to without ID.
Objective:
To assess if skeletal muscle metabolism is impaired in HFpEF patients with iron deficiency compared to HFpEF patients without iron deficiency
Study design
From October 2019 until December 2020: patient inclusion. First trimester 2021 data analysis and prepare publication
Intervention
The main study parameters is PCR recovery time, a measurement of PCR recovery time using MR spectroscopy
Secondary parameters/endpoints are:
- Microvascular function
o Glycocalyx thickness (um)
o Heat induced hyperaemic response (% skin hyperaemic response)
- Exercise tolerance
o 6 minute walk test distance (m)
o maximum exercise capacity (METs on exercise test)
Arantxa Barandiaran Aizpurua
0640020684
arantxa.barandiaranaizpurua@mumc.nl
Arantxa Barandiaran Aizpurua
0640020684
arantxa.barandiaranaizpurua@mumc.nl
Inclusion criteria
In order to be eligible to participate in this study, a subject must meet all of the following criteria:
Group I HFpEF with iron deficiency
Group II HFpEF without iron deficiency
• HFpEF: according to the ESC guidelines
(1) Signs and/or symptoms of heart failure,
(2) LVEF ≥ 50%,
(3) Elevated levels of natriuretic peptide (NT-proBNP > 125 pg/ml
~ 15 pmol/L)
(4) one of the following additional criteria
a) Relevant structural heart disease; LV hypertrophy, (LVmass index > 95 g/m2 in women, or >115 g/m2 in men) and/or LA enlargement (LA volume index >34 l/m2)
b) Diastolic dysfunction (E/e’ ≥ 13, mean e’ septal and lateral wall < 9 cm/s)
• Iron deficiency: serum ferritin < 100 µg/L or serum ferritin between 100-299 µg/L in combination with a transferrin saturation < 20%.
Exclusion criteria
A potential subject who meets any of the following criteria will be excluded from participation in this study:
- Reproductive age women
- Any iron supplement (oral, iv) during the last 6 months prior to inclusion
- Any chemotherapy in last year
- Significant peripheral artery disease
- Contraindication for CMR
• ODIN protocol:
• “Uitvoering van MRI onderzoek bij patiënten met een cardiaal implanteerbaar elektronisch device (CIED), waaronder een pacemaker en ICD”
• ODIN protocol:
• “Voorbereiding klinische patiënten voor MRI onderzoek”
• Metallic implant (vascular clip, neuro-stimulator, cochlear implant)
• Pacemaker or implantable cardiac defibrillator(ICD)
• Claustrophobia
- Body weight > 130kg
Design
Recruitment
IPD sharing statement
Followed up by the following (possibly more current) registration
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Other (possibly less up-to-date) registrations in this register
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In other registers
| Register | ID |
|---|---|
| NTR-new | NL8095 |
| Other | metc AZM/MUMC : METC181034 |