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Informations générales
  • Catégorie de maladie Maladie coronarienne (BASEC)
  • État du recrutement recrutement pas encore commencé (BASEC/ICTRP)
  • Lieu de l’étude
    Genève
    (BASEC)
  • Responsable de l'étude Juan Fernando Iglesias juanfernando.iglesias@hug.ch (BASEC)
  • Source(s) de données BASEC: Importé de 05.03.2026 ICTRP: N/A
  • Date de mise à jour 05.03.2026 16:45
HumRes67905 | SNCTP000006833 | BASEC2025-D0080

Safety and clinical performance of the magnesium bioresorbable coronary stent (Freesolve) in the treatment of subjects with long de novo lesions in native coronary arteries: BIOMAG-LL

  • Catégorie de maladie Maladie coronarienne (BASEC)
  • État du recrutement recrutement pas encore commencé (BASEC/ICTRP)
  • Lieu de l’étude
    Genève
    (BASEC)
  • Responsable de l'étude Juan Fernando Iglesias juanfernando.iglesias@hug.ch (BASEC)
  • Source(s) de données BASEC: Importé de 05.03.2026 ICTRP: N/A
  • Date de mise à jour 05.03.2026 16:45

Résumé de l'étude

This clinical trial will be conducted at 20 sites in Germany, Switzerland, Spain, Poland, Latvia, and Italy. It is planned to include 100 patients. After patients have given their consent to participate in the study, a vascular assistance device will be used. Follow-up clinical examinations will be performed at 1, 6, and 12 months, and then at 36 and 60 months after the intervention. In a smaller group of study participants, after giving their consent, the concentration of the drug released by the bioresorbable stent Freesolve will be measured. Blood samples will be used to measure the amount of drug released by the bioresorbable stent present in the blood at different times after the implantation of Freesolve in the artery. This is called pharmacokinetic evaluation. As part of the pharmacokinetic evaluation, additional blood samples will be taken before implantation and at 10 minutes, 30 minutes, and 1, 2, 3, 4, 6, 12, 24, 48, and 72 hours, as well as 7 days after the implantation of Freesolve.

(BASEC)

Intervention étudiée

In BIOMAG-LL, an extension of the size range of Freesolve (scaffold lengths of 35 and 40 mm) will be studied. The aim of the study is to evaluate the safety and clinical performance of Freesolve 35 and 40 mm in de novo coronary lesions up to 38 mm in length. Patients with clinical symptoms are referred to the investigation center for diagnostic testing. Patients who have agreed to participate and received Freesolve (35 mm and 40 mm) will be followed up at 30 days, 1, 6, 12 months, and after 36 and 60 months post-procedure. A pharmacokinetic evaluation will also be conducted in a small group of patients who have given additional consent.

(BASEC)

Maladie en cours d'investigation

Coronary arteries (blood vessels in the heart) may have a narrowing that can require treatment. This narrowing can be caused by deposits on the walls of the arteries (atherosclerosis). As a result, the heart does not receive enough oxygen and nutrients, which impairs heart function. This condition is called coronary artery stenosis and can be the cause of clinical symptoms.

(BASEC)

Critères de participation
1. Subjects with a maximum of two unique lesions in two distinct coronary arteries, which must be de novo lesions and can each be covered by a single device. 2. Reference vessel diameter between 2.7 and 4.2 mm based on visual estimation, depending on the size of the scaffold used. 3. Target lesion length > 28 and ≤ 38 mm based on visual estimation, depending on the size of the scaffold used. (BASEC)

Critères d'exclusion
1. The subject is pregnant and/or breastfeeding or intends to become pregnant during the study duration. 2. The subject has clinical symptoms and/or electrocardiogram (ECG) changes consistent with ST-segment elevation myocardial infarction (STEMI) less than 72 hours prior to the reference procedure. 3. Known allergies: to aspirin, P2Y12 inhibitors, heparin and bivalirudin, sirolimus (or similar drugs), poly L-lactide, or scaffold material (magnesium, aluminum, tantalum). (BASEC)

Lieu de l’étude

Genève

(BASEC)

non disponible

Sponsor

BIOTRONIK AG Ackerstrasee 6, 8180 Bülach, Switzerland

(BASEC)

Contact pour plus d'informations sur l'étude

Personne de contact en Suisse

Juan Fernando Iglesias

+41 (0)79 347 48 49

juanfernando.iglesias@hug.ch

Hopitaux Universitaires de Genève

(BASEC)

Informations scientifiques

non disponible

Nom du comité d'éthique approbateur (pour les études multicentriques, uniquement le comité principal)

Commission cantonale d'éthique de Genève

(BASEC)

Date d'approbation du comité d'éthique

05.03.2026

(BASEC)


Identifiant de l'essai ICTRP
non disponible

Titre officiel (approuvé par le comité d'éthique)
BIOTRONIK – Safety and Clinical Performance of the Drug Eluting Resorbable MAGnesium Scaffold (Freesolve) in the Treatment of Subjects with Long de Novo Lesions in Native Coronary Arteries: BIOMAG-LL (BASEC)

Titre académique
non disponible

Titre public
non disponible

Maladie en cours d'investigation
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Intervention étudiée
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Type d'essai
non disponible

Plan de l'étude
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Critères d'inclusion/exclusion
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non disponible

Critères d'évaluation principaux et secondaires
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non disponible

Date d'enregistrement
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Inclusion du premier participant
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Sponsors secondaires
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Contacts supplémentaires
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ID secondaires
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Résultats-Données individuelles des participants
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Informations complémentaires sur l'essai
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Résultats de l'essai

Résumé des résultats

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Lien vers les résultats dans le registre primaire

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