Clinical Trials/NCT03987152

NCT03987152

Unknown

Phase 3

Treatment of Congenital Vascular Malformations Using Sirolimus: Improving Quality of Life

Radboud University Medical Center1 site in 1 country75 target enrollmentSeptember 18, 2017

ConditionsVascular Malformations

InterventionsSirolimus

DrugsSirolimus

Overview

Phase: Phase 3
Intervention: Sirolimus
Conditions: Vascular Malformations
Sponsor: Radboud University Medical Center
Enrollment: 75
Locations: 1
Primary Endpoint: Quality of life using Sirolimus measured with survey (Research and development Rand-36).
Last Updated: 5 years ago

Overview Investigators Eligibility Criteria Arms & Interventions Outcomes Sites Similar Trials

Overview

Brief Summary

Congenital vascular anomalies are uncommon and belong to the group of rare diseases.These vascular malformations can cause serious complications including obstruction of vital organs and their function, recurrent infection and significantly reduced quality of life of persons affected.Treatment options range from conservative to surgical extirpation or intralesional embolisation/sclerosis. Unfortunately, this is often not enough. Many patients still have complaints like severe pain and invalidation due to the lymphatic or venous malformation making a normal functional life impossible. Recent case reports mention the positive effects of refractory patients with Sirolimus. Sirolimus, also known as rapamycin, is currently the only FDA-approved mammalian target of rapamycin (mTOR) inhibitor.

Detailed Description

Congenital vascular anomalies are uncommon and belong to the group of rare diseases. In 1996, the International Society of the Study of Vascular Anomalies adopted a new classification, distinguishing vascular malformations from vascular tumors. This classification was revised in 2014 and newly identified genetic features were taken into account. Vascular malformations feature dysplastic malformed vessels and are a consequence of a defective development of the embryonic vascular system. Vascular malformations can involve lymphatic vessels, capillaries, veins and arteries or even combinations. These vascular malformations are present at birth and grow with the child. Treatment options range from conservative to surgical extirpation or intralesional embolisation/sclerosis. Unfortunately, this is often not enough. Many patients still have complaints like severe pain and invalidation due to the lymphatic or venous malformation making a normal functional life impossible. These vascular malformations can cause serious complications including obstruction of vital organs and their function, recurrent infection and significantly reduced quality of life of persons affected. As the natural course of the disease affects multiple body systems, the therapeutic management is challenging. To date, no other medical treatment options are available. Although standard pain medication is given according the (inter) national pain protocols, patients still suffer pain and are not able to function normally in daily life. Majority (60-70% percent of the patients) of the patients is not able to have a normal life, with a normal job and normal social activities. Children are often not able to go to school normally, cannot play outside and have pain at the site of the malformation. The vast majority of literature reporting medical therapies for vascular anomalies consists of case reports and small series and is complicated by publication bias (negative findings are often not published), inconsistent use of nomenclature, and the absence of clinical trials. Recent case reports mention the positive effects of refractory patients with Sirolimus. Sirolimus, also known as rapamycin, is currently the only FDA-approved mammalian target of rapamycin (mTOR) inhibitor, indicated for prevention of kidney allograft rejection in adults and children 13 years or older, but is commonly used to manage organ rejection in younger children.

Registry

clinicaltrials.gov

Start Date

September 18, 2017

End Date

March 1, 2023

Last Updated

5 years ago

Study Type

Interventional

Study Design

Sequential

Sex

All

Investigators

Sponsor

Radboud University Medical Center

Responsible Party

Sponsor

Eligibility Criteria

Inclusion Criteria

•Diagnosis of Congenital venous malformation, or lymphatic malformation or combined.
•Age older than 1 yr.
•Patients (or legal guardians for children) have to be able to sign the informed consent
•Patients are either refractory to standard care such as medical treatment (low molecular weight heparins, pain medication etc.), surgical resection and/or sclerotherapy/embolization (ineffective or accompanied by major complications) or there is no possibility for surgical intervention anymore. Only patients that have a normal clinical screening (no signs for infection, normal bone marrow function, normal liver and kidney function, normal glucose metabolism etc.) can be included.
•Patients included have no cardiac impairment
•Patients have no gastrointestinal impairment as Sirolimus is absorbed gastro-intestinal and normal function is needed
•No other underlying medical disorder like Down syndrome or other syndromes
•Women of reproductive age have to be informed that contraceptive methods are
•mandatory during the study time, pregnant women are excluded
•Karnofsky score \> 50

Exclusion Criteria

•No written informed consent
•Known hypersensitivity to drugs or metabolites from similar classes as study treatment.
•Patient has other concurrent severe and /or uncontrolled medical condition that would, in the investigator's judgment, contraindicated participation in the clinical study (e.g. acute or chronic pancreatitis, liver cirrhosis, active chronic hepatitis, severely impaired lung function with a spirometry ≤ 50% of the normal predicted value and/or O2 saturation ≤ 88% at rest, etc.)
•Recent history of primary malignancy ≤ 5 years
•Impaired cardiac function or clinically significant cardiac diseases
•Immunocompromised patients, including known seropositivity for HIV
•Patient with any other concurrent severe and /or uncontrolled medical condition that would,in the investigator's judgment, contraindicated participation in the clinical study.
•Pregnant or lactating women
•Karnofsky score \< 50

Arms & Interventions

Sirolimus

Sirolimus administration: during Challenge and Rechallenge phase. Compared with the period 2 months before start of Sirolimus.

Intervention: Sirolimus

Outcomes

Primary Outcomes

Quality of life using Sirolimus measured with survey (Research and development Rand-36).

Time Frame: hange from baseline Quality of life at 6 months QoL in challenge phase, and 12 months QoL in Rechallenge phase

Quality of life: Rand-36 (adults) eight health domains; physical functioning, social functioning, role limitations due to physical health problems, role limitations due to emotional problems, mental health, vitality, pain and general health perception. Outcomes at each domain will be defined on a scale from a minimum score of 0 to a maximum score of 100. A higher score is equivalent to a better health.

Difference in pain scores after using Sirolimus measured with VAS score

Time Frame: Daily pain scores will be compared after 6 months in Challenge phase, after Challenge phase: starts the phase, and pain during 12 months in the Rechallenge phase

Daily pain score (daily visual analogue scale (VAS-score 0-10) for children, and numeric rating scale (NRS-score 0-10) for adults)

Quality of life using Sirolimus measured with survey (PedsQl)

Time Frame: Change from baseline Quality of life at 6 months QoL in challenge phase, and 12 months QoL in Rechallenge phase.

Quality of life: Pediatric Quality of Life Inventory (PedsQl) (children) 23 items questionnaire, 0-100 scale, so that higher scores indicate better HRQOL (Health-Related Quality of Life). Psychosocial Health Summary Score, Physical Health Summary Score and Total score will be measured.

Difference in pain scores after using Sirolimus measured with NRS score

Time Frame: Daily pain scores will be compared after 6 months in Challenge phase, after Challenge phase: starts the phase without Sirolimus treatment, and pain during 12 months in the Rechallenge phase

Daily pain score (daily numeric rating scale (NRS-score 0 no pain -10 extreme pain) for adults)

Quality of life using Sirolimus measured with survey (TAPQOL)

Time Frame: Change from baseline Quality of life at 6 months QoL in challenge phase, and 12 months QoL in Rechallenge phase.

Quality of life: Questionnaire for Preschool Children's Health-Related Quality of Life (TAPQOL). Preschool Children Quality of Life, parent-reported questionnaire clustered into 12 multi-item scales, with higher scores range 0-100) indicating better HRQOL)

Secondary Outcomes

Return of pain after treatment and duration of lowered pain or pain free period in days(After 6 months Sirolimus intake till one year follow up.)
Severity of adverse events related to Sirolimus(4 years)
Cost-effectiveness of administration of Sirolimus: Quality Adjusted Life Year (QALY) estimate for each patient(4 years)
Growth/progression of vascular malformation(MRI baseline compared with MRI after 6 months in challenge phase and 12 months in rechallenge phase)
Rate and occurence of adverse events related to Sirolimus(4 years)
Genetic mutations in the vascular malformation that can predict outcome of treatment with Sirolimus using Single Molecule Molecular Inversion Probes (smMIPs)(4 years)
Pharmacogenetic profile in the vascular malformation that can predict outcome of treatment with Sirolimus(4 years)