RecruitingObservational

Multicenter International Durability and Safety of Sirolimus in LAM Trial (MIDAS)

NCT ID: NCT02432560Sponsor: University of CincinnatiLast updated: 2024-12-24

Summary

The MIDAS study aims to follow male and female LAM patients who are currently taking, have previously failed or been intolerant of, or may (at some time in the future) take mTOR inhibitors (sirolimus or everolimus) as part of their clinical care. Adult female TSC patients may also enroll, with or without lung cysts.

Detailed description

Lymphangioleiomyomatosis (LAM) is an uncommon disease affecting women. It is associated with cystic lung destruction and progressive respiratory failure. The Multicenter International LAM Efficacy of Sirolimus (MILES) Trial, led by the investigators' research team, demonstrated that mTOR (mammalian target of rapamycin) inhibition with sirolimus was an effective therapy that stabilized decline in FEV1 (forced expiratory volume). However, lung function decline resumed when the drug was stopped at the one year point in MILES, suggesting that therapy is suppressive rather than remission-inducing, and may need to be lifelong. There is therefore a need to understand whether long-term therapy with sirolimus is safe and effective. To accomplish this goal, the investigators will conduct the Multicenter International Durability and Safety of Sirolimus in LAM Trial (MIDAS). This is an observational, real world registry. The investigators propose to enroll 600 LAM patients who are on, have previously failed or been intolerant of or are considering taking sirolimus or everolimus for clinical reasons in a longitudinal observational study. This registry will follow lung function tests and adverse events that are obtained for clinical purposes over periods of at least 2 years. The decision to treat with mTOR inhibitor therapy is made by the clinician and the patient, and will be managed by the participant's clinician. This study will help us to refine treatment for patients with LAM and determine if long term suppressive therapy with sirolimus can prevent progression to later stages of disease. This research will be accomplished as part of the NIH/NCATS Rare Lung Disease Consortium, with data stored and analyzed by the Database Management Coordinating Center (DMCC) at the University of South Florida.

Arms & interventions

DrugSirolimus
Sirolimus treatment will be part of a participant's clinical care and will be managed by their physician.
DrugEverolimus
Everolimus treatment will be part of a participant's clinical care and will be managed by their physician.

Outcome measures

Primary

Long term safety of mTOR inhibitor treatment in LAM
Symptoms and adverse events will be recorded
Time frame: 2-5 years
Efficacy - FEV1 slope
Rate of change in FEV1 in ml/month
Time frame: 2-5 years
Efficacy -10% reduction in FEV1
time from enrollment to 10% or greater reduction in FEV1(forced expiratory volume) in months
Time frame: 2-5 years

Secondary

Effect of long term sirolimus on quality of life
Time frame: 2-5 years

Eligibility criteria

Sex: FemaleAge: 18 Years and olderHealthy volunteers: No

Inclusion Criteria: * Female or male, age 18 or over * Diagnosis of LAM based on ATS/JRS criteria * Signed and dated informed consent * On chronic therapy, newly treated or may be considered for therapy with mTOR inhibitors or previously intolerant of or having failed mTOR inhibitor therapy Exclusion Criteria: * Inability to attend at least one RLD Clinic visit per year * Inability to give informed consent * Inability or unwillingness to perform pulmonary function testing

Study locations (20)

Stanford University Medical Center

Stanford, California, 94305

Recruiting

Stephen Ruoss, MD · Contact

650-723-6381 ruoss@stanford.edu

National Jewish Health

Denver, Colorado, 80206

Recruiting

Gregory Downey, MD · Contact

303-398-1436 gregory.downey@gmail.com

Mayo Clinic Jacksonville

Jacksonville, Florida, 32224

Recruiting

Charles Burger, MD · Contact

904-953-2381 charles.burger@mayo.edu

Emory University School of Medicine

Atlanta, Georgia, 33136

Recruiting

Sirhari Veeraraghavan, MD · Contact

veeraraghavan@emory.edu

Loyola University Medical Center, Chicago

Maywood, Illinois, 60153

Active Not Recruiting

Brigham and Women's Hospital

Boston, Massachusetts, 02115

Recruiting

Elizabeth Henske, MD · Contact

857-307-0784 ehenske@partners.org

University of Michigan

Ann Arbor, Michigan, 48109

Recruiting

Mei Lan Han, MD · Contact

734-936-5047 mrking@umich.edu

Mayo Clinic Rochester

Rochester, Minnesota, 55905

Active Not Recruiting

Washington University School of Medicine

St Louis, Missouri, 63110

Recruiting

Adrian Shifren, MD · Contact

314-362-6904 ashifren@wustl.edu

University of Rochester Medical Center

Rochester, New York, 14642-8692

Recruiting

MaryAnne Morgan, MD · Contact

585-275-4161 maryanne_morgan@urmc.rochester.edu

University of Cincinnati

Cincinnati, Ohio, 45267

Active Not Recruiting

Cleveland Clinic

Cleveland, Ohio, 44195

Active Not Recruiting

Oregon Health and Science University

Portland, Oregon, 97239

Active Not Recruiting

University of Pennsylvania Medical Center

Philadelphia, Pennsylvania, 19104

Active Not Recruiting

Medical University of South Carolina

Charleston, South Carolina, 29425

Active Not Recruiting

Vanderbilt University Medical Center

Nashville, Tennessee, 37232-2650

Active Not Recruiting

University of Texas Southwestern Medical Center

Dallas, Texas, 75390

Active Not Recruiting

University of Texas Health Center

Houston, Texas, 77030

Active Not Recruiting

University of Utah School of Medicine

Salt Lake City, Utah, 84132

Active Not Recruiting

Swedish Medical Center

Seattle, Washington, 98104

Active Not Recruiting