Hereditary haemorrhagic telangiectasia (HHT), is a rare genetic vascular disorder with autosomal dominant inheritance. Its prevalence is estimated at approximately 1 in 6,000 individuals in France. Clinical manifestations include recurrent nosebleeds (epistaxis), cutaneous telangiectasias, and visceral arteriovenous malformations (AVMs) that may affect the lungs, gastrointestinal tract, liver, and brain. Beyond vascular abnormalities, patients often present with a decrease in circulating T lymphocytes (T-cell lymphopenia), which can be profound but remains unexplained. There is also a distinct infectious risk profile associated with the disease: brain abscesses in the presence of pulmonary AVMs (pAVMs), and osteoarticular infections in patients with the longest durations of epistaxis. However, no definitive correlation has been established between T-cell lymphopenia and infection risk. Iron-deficiency anemia is a frequent complication in HHT, affecting about 50% of patients, with a mean age of onset around 36 years. Its prevalence increases with age. These patients typically require prolonged and high-dose iron supplementation, administered either orally or intravenously, which may expose them to side effects not observed in other clinical contexts. In a previous study, we identified a correlation between the level of iron supplementation (none, oral, or intravenous) and the severity of T-cell lymphopenia. This association may be explained by two potential mechanisms linking iron metabolism to immune function: * A direct toxic effect of iron on immune system homeostasis * Impaired lymphocyte production resulting from iron deficiency, with the type of supplementation serving as an indirect marker of deficiency severity We propose a prospective study designed to differentiate between these two hypotheses. The aim of the study is to characterize the impact of iron deficiency and iron supplementation on the immune system of patients with HHT.
Study Type
INTERVENTIONAL
Allocation
NON_RANDOMIZED
Purpose
HEALTH_SERVICES_RESEARCH
Masking
NONE
Enrollment
155
Six extra blood collection tubes (28 mL) will be drawn during the visit (D0), in addition to the routine blood samples, at the blood collection center
six extra blood collection tubes (28 mL) will be drawn during the visit (D+3 months) for group 3 patients, in addition to the routine blood samples, at the blood collection center
Hôpital Femme-Mère-Enfant
Bron, Rhone, France
RECRUITINGHelper T-cell concentration (number of CD3⁺CD4⁺ lymphocytes per mm^³ of blood).
Samples will be analyzed by spectral cytometry to determine the concentration of each leukocyte population of interest.
Time frame: Baseline for all the 3 groups and 3 months after iron supplementation for group 3.
Naive/effector memory/terminal effector memory/central memory helper T lymphocytes concentration (number per mm^³ of blood).
Samples will be analyzed by spectral cytometry to determine the concentration of each leukocyte population of interest.
Time frame: Baseline for all the 3 groups and 3 months after iron supplementation for group 3.
Naive/effector memory/terminal effector memory/central memory cytotoxic T lymphocytes concentration (number per mm^³ of blood).
Samples will be analyzed by spectral cytometry to determine the concentration of each leukocyte population of interest.
Time frame: Baseline for all the 3 groups and 3 months after iron supplementation for group 3.
γδ T cells, mucosal-associated invariant T (MAIT) cells, and natural killer T (NKT) cells concentration (number per mm^³ of blood).
Samples will be analyzed by spectral cytometry to determine the concentration of each leukocyte population of interest.
Time frame: Baseline for all the 3 groups and 3 months after iron supplementation for group 3.
Natural killer (NK) cells concentration (number per mm^³ of blood).
Samples will be analyzed by spectral cytometry to determine the concentration of each leukocyte population of interest.
Time frame: Baseline for all the 3 groups and 3 months after iron supplementation for group 3.
Naive/memory/class-switched B lymphocytes concentration (number per mm^³ of blood).
Samples will be analyzed by spectral cytometry to determine the concentration of each leukocyte population of interest.
Time frame: Baseline for all the 3 groups and 3 months after iron supplementation for group 3.
Plasmablasts concentration (number per mm^³ of blood).
Samples will be analyzed by spectral cytometry to determine the concentration of each leukocyte population of interest.
Time frame: Baseline for all the 3 groups and 3 months after iron supplementation for group 3.
Classical/intermediate/non-classical/Tie2⁺ monocytes concentration (number per mm^³ of blood).
Samples will be analyzed by spectral cytometry to determine the concentration of each leukocyte population of interest.
Time frame: Baseline for all the 3 groups and 3 months after iron supplementation for group 3.
Myeloid and plasmacytoid dendritic cells concentration (number per mm^³ of blood).
Samples will be analyzed by spectral cytometry to determine the concentration of each leukocyte population of interest.
Time frame: Baseline for all the 3 groups and 3 months after iron supplementation for group 3.
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