Interrupters of VAscular daMAge in Malignant Hypertension

Centre Hospitalier de PAU45 enrolled

Overview

The pathophysiology of malignant hypertension is poorly understood. The objective of this translational research project is to evaluate the relationship between activation of vasoactive systems (renin-angiotensin and endothelin systems), angiogenic signal deficiency (VEGF and sFlt-1) and the occurrence of malignant hypertension episodes in humans.

The pathophysiology of malignant hypertension is poorly understood. The current dogma is based on an overwhelming renin-angiotensin-aldosterone system activation, leading to arterial hypertension that overcomes target organ auto-regulatory mechanisms and leads to subacute microvascular lesions. However, some patients present with normal or lowered renin in the acute phase of malignant hypertension, suggesting other pathophysiological pathways. Malignant hypertension was reported following anti-VEGF treatment, suggesting that this pathway may be involved. Recent unpublished animal data highlight 1/ the possibility of severe deregulation of the VEGF (vascular endothelial growth factor) system in malignant hypertension 2/ the possibility of compensation of the vasculotoxic effects of VEGF deficiency by inflammasome components. These systems have never been studied together in human hypertension. Investigators will analyze the angiogenic, vasoactive and VEGF systems through blood and urine sampling. These samples will be collected at the time of malignant hypertension diagnosis and repeated one month later in 30 patients. The same tests will be performed in 15 patients with severe non-malignant hypertension, constituting the control group.

Study Type

OBSERVATIONAL

Enrollment

Conditions

Malignant Hypertension

Interventions

analyse of angiogenic, vasoactive and VEGF systemsBIOLOGICAL

the angiogenic, vasoactive and VEGF systems will be analysed through blood and urine sampling. These samples will be collected at the time of malignant hypertension diagnosis and repeated one month later, in 30 patients (patients group). The same tests will be performed once in 15 patients with severe non-malignant hypertension, constituting the control group.

Eligibility

Sex: ALLMin age: 18 Years

Medical Language ↔ Plain English

Inclusion Criteria: Patients group : * Patients included in the HAMA cohort * Who is willing to take part in the IVAMA project Control group : * Grade 2 or 3 hypertension with office blood pressure measurement (above 160 and/or 100 mmHg for systolic and diastolic) * Persistence of blood pressure above 160 / 100 mmHg on the average of 3 "attended" blood pressure measurements Exclusion criteria: Patients group : * Age \< 18 years old * Patients with chronic renal failure of stage 3 or higher. * Patients with any type of diabetes * Patient in per partum * Patients who cannot freely give their consent, or patients who refuse to participate * Chronic dialysis patient Control group: * Evidence of subacute involvement of one of the following target organs: brain, kidney, eye, heart, thrombotic microangiopathy. Target organ impairment is defined in the inclusion criteria for the "Patients" group. * Presence of known chronic kidney insufficiency of grade 3 or higher * Chronic dialysis patient * Diabetes of any type * Patients who cannot freely give their consent, or patients who refuse to participate

Locations (7)

Hôpital Avicenne

Bobigny, France

CHU de Bordeaux

Bordeaux, France

Hôpital Bichat

Paris, France

Hôpital Européen Georges Pompidou

Paris, France

Outcomes

Primary Outcomes

sFLT1 concentration at inclusion

The primary endpoint will be the difference in sFLT1 concentrations between patients and controls at enrolment