Purpose

The Idiopathic Pulmonary Fibrosis Prospective Outcomes (IPF-PRO) Registry started recruiting in 2014 with the objective of studying Idiopathic Pulmonary Fibrosis. In 2018, the registry expanded to include recruitment of participants with other chronic fibrosing interstitial lung diseases (ILDs) with progressive phenotype also referred to as progressive fibrosing interstitial lung diseases in the Chronic Fibrosis Interstitial Lung Disease with Progressive Phenotype (ILD-PRO) Registry. When the third phase of the registry begins, the IPF-PRO registry will enroll additional patients with idiopathic pulmonary fibrosis. This IPF-PRO registry is a prospective registry that will collect information regarding the natural history, health care interactions, participant reported questionnaire data to assess quality of life, and the methods of treatment of participants with a diagnosis of idiopathic pulmonary fibrosis (IPF) or of another chronic fibrosing interstitial lung disease (ILD) with progressive phenotype established at the enrolling centers. In addition, blood samples and chest image studies will be collected and banked for future research projects.

Condition

Eligibility

Eligible Ages
Over 21 Years
Eligible Sex
All
Accepts Healthy Volunteers
No

Inclusion Criteria

  • Willing and able to provide informed consent - Established a new diagnosis (within 12 months) of IPF by the enrolling center. - Age 21 years or older, or - Diagnosis of a non-IPF ILD of any duration, including, but not limited to Idiopathic Non-Specific Interstitial Pneumonia (iNSIP), Unclassifiable Idiopathic Interstitial Pneumonias (IIPs), Interstitial Pneumonia with Autoimmune Features (IPAF), Autoimmune ILDs such as Rheumatoid Arthritis (RA-ILD) and Systemic Sclerosis (SSc-ILD), Chronic Hypersensitivity Pneumonitis (HP), Sarcoidosis or Exposure-related ILDs such as asbestosis with progressive phenotype during the last 24 months by the enrolling center that meets the following criteria: - Chronic fibrosing ILD as defined by reticular abnormality with traction bronchiectasis with or without honeycombing confirmed by chest HRCT scan and/or lung biopsy. - Progressive phenotype as defined by fulfilling at least one of the criteria below of fibrotic changes (progression set point) within the last 24 months regardless of treatment considered appropriate in individual ILDs (8): - decline in FVC % predicted (% pred) based on ≥10% relative decline - decline in FVC % pred based on ≥5 - <10% relative decline in FVC combined with worsening of respiratory symptoms as assessed by the site investigator - decline in FVC % pred based on ≥5 - <10% relative decline in FVC combined with increasing extent of fibrotic changes on chest imaging (HRCT scan) as assessed by the site investigator - decline in DLCO % pred based on≥ 10% relative decline - worsening of respiratory symptoms as well as increasing extent of fibrotic changes on chest imaging (HRCT scan) as assessed by the site investigator independent of FVC change. The relative decline for FVC % predicted is calculated using the formula: Relative Decline= (FVC % Pred (Reference)-FVC % Pred (Screening))/(FVC % Pred (Reference))×100%, where FVC % Pred (Reference) is the greatest measurement of FVC % predicted in the 24 months prior to screening and FVC % Pred (Screening) is the measurement of FVC % predicted at screening. The relative decline for DLCO % predicted is calculated using the formula: Relative Decline= (DLCO % Pred (Reference)-DLCO % Pred (Screening))/(DLCO % Pred (Reference))×100%, Where DLCO % Pred (Reference) is the greatest measurement of DLCO % Pred in the 24 months prior to screening and DLCO % Pred (Screening) is the measurement of DLCO % Pred at screening

Exclusion Criteria

  • Malignancy, treated or untreated, other than skin or early -stage prostate cancer, within the past 5 years - Currently listed for lung transplantation at the time of enrollment - Currently enrolled in an interventional clinical trial at the time of enrollment in this registry - For the additional IPF cohort of 1000 individuals, previous enrollment in this registry.

Study Design

Phase
Study Type
Observational [Patient Registry]
Observational Model
Cohort
Time Perspective
Prospective

Arm Groups

ArmDescriptionAssigned Intervention
Subjects with a new IPF diagnosis Subjects with a new diagnosis of IPF established at the time of enrollment in the registry
Subjects with a non-IPF ILD diagnosis Subjects with a diagnosis of a non-IPF ILD of any duration, including, but not limited to Idiopathic Non-Specific Interstitial Pneumonia (iNSIP), Unclassifiable Idiopathic Interstitial Pneumonias (IIPs), Interstitial Pneumonia with Autoimmune Features (IPAF), Autoimmune ILDs such as Rheumatoid Arthritis (RA-ILD) and Systemic Sclerosis (SSc-ILD), Chronic Hypersensitivity Pneumonitis (HP), Sarcoidosis or Exposure-related ILDs such as asbestosis with progressive phenotype
New Subjects with a new IPF diagnosis Subjects with a new diagnosis of IPF established at the time of enrollment in the registry not previously enrolled in the registry.

Recruiting Locations

University of Alabama - Birmingham
Birmingham, Alabama 35294
Contact:
Arnissa Hopson
205-934-1657
agoggins@uabmc.edu

University of Arizona
Tucson, Arizona 85721
Contact:
Surya Olguin
602-827-2462
suryaolguin@arizona.edu

University of California - Los Angeles
Los Angeles, California 90024
Contact:
Paul Lopez
310-794-8595
plopez@mednet.ucla.edu

University of Southern California
Los Angeles, California 90033
Contact:
Lynn Fukusima
Lynn.Fukushima@med.usc.edu

Stanford University
Stanford, California 94305
Contact:
Summer Zhu
650-724-5424
szhuye@stanford.edu

University of Colorado
Aurora, Colorado 80045
Contact:
Olivia Brohl
303-724-0641
Olivia.brohl@cuanschutz.edu

Yale University
New Haven, Connecticut 06520
Contact:
Maksym Minasyan
203-785-4177
maksym.minasyan@yale.edu

University of Florida
Gainesville, Florida 32610-3175
Contact:
Lisbetty Lugo
lisbetty.lugo@medicine.ufl.edu

University of South Florida
Tampa, Florida 33606
Contact:
Abigail Eglinton
813-660-6955
ahughes@tgh.org

Emory University
Atlanta, Georgia 30322
Contact:
Tracy Halabi
404-712-7458
tracy.halaby@emory.edu

Piedmont Healthcare
Austell, Georgia 30106
Contact:
Munachi (Muna) Iwotor
404-291-9062
munachi.iwotor@piedmont.org

University of Chicago
Chicago, Illinois 60637
Contact:
Vanita Patel
vpatel4@bsd.uchicago.edu

Northwestern University
Evanston, Illinois 60611
Contact:
Phillip Cooper
312-503-0406
p-cooper@northwestern.edu

Loyola University Health System
Maywood, Illinois 60153
Contact:
Sloan White
swhite29@luc.edu

Tulane University
New Orleans, Louisiana 70112
Contact:
Sandy Ditta
504-988-4040
sditta@tulane.edu

University of Minnesota
Minneapolis, Minnesota 55455
Contact:
Mandi DeGrote
612-626-7609
carl1032@umn.edu

University of Mississippi Medical Center
Jackson, Mississippi 39216
Contact:
Rachael Thompson-Duffin
rthompson3@umc.edu

Washington University
St Louis, Missouri 63110
Contact:
Mona Noroozi
314-362-3705
mnoroozi@wustl.edu

Weill Medical College of Cornell University
New York, New York 10065
Contact:
Alicia Morris
646-692-2741
ajm2017@med.cornell.edu

UNC Chapel Hill
Chapel Hill, North Carolina 27514
Contact:
Jackson Pettee
Jackson_pettee@med.unc.edu

Duke University
Durham, North Carolina 27705
Contact:
Lauren Gray
919-684-7317
lauren.gray@duke.edu

Pulmonix LLC
Greensboro, North Carolina 27403
Contact:
Mei Zheng
336-522-8870
mei.zheng@pulmonix.com

Wake Forest Baptist Health
Winston-Salem, North Carolina 27157
Contact:
Bob Hmieleski
336-713-8550
bhmieles@wakehealth.edu

Cleveland Clinic
Cleveland, Ohio 44195
Contact:
Ron Wehrmann
2164450574
wehrmar@ccf.org

The Ohio State University
Columbus, Ohio 43210
Contact:
Benjamin Hood
benjamin.hood2@osumc.edu

University of Oklahoma
Oklahoma City, Oklahoma 73104
Contact:
Maria Mason
405-271-6173
maria-l-mason@ouhsc.edu

Oregon Clinic
Portland, Oregon 97220
Contact:
Meg Day
503-963-3182
mday@orclinic.com

Thomas Jefferson University
Philadelphia, Pennsylvania 19144
Contact:
Ramya Talluri, BSN, RN
RamyaPriya.Talluri@jefferson.edu

Medical University of South Carolina
Charleston, South Carolina 29425
Contact:
Audra Wiser
wisera@musc.edu

Vanderbilt University
Nashville, Tennessee 37232
Contact:
James Del Greco
615-343-7068
james.del.greco@vumc.org

University of Texas Southwestern
Dallas, Texas 75235
Contact:
Maira Ortiz
214-645-1295
Maira.OrtizBerrio@UTSouthwestern.edu

Baylor University Medical Center at Dallas
Dallas, Texas 75246
Contact:
Kristina Perez
817-922-2570
Kristina.Perez@BSWHealth.org

Baylor College of Medicine
Houston, Texas 77030
Contact:
Maria C Perea
Maria.Perea@bcm.edu

Houston Methodist Lung Center
Houston, Texas 77030
Contact:
Jennifer Lee
713-363-7537
jllee@houstonmethodist.org

The University of Texas Health Science Center At Houston
Houston, Texas 77030
Contact:
Beverly Rios
713-486-6152
Beverly.Rios@uth.tmc.edu

University of Utah
Salt Lake City, Utah 84108
Contact:
Adeline Langer
801-581-5811
adeline.langer@hsc.utah.edu

Inova
Falls Church, Virginia 22042-3307
Contact:
Taruni Maganti
703-776-3230
Taruni.Maganti@inova.org

More Details

Status
Recruiting
Sponsor
Duke University

Study Contact

Rosalia Blanco
919-660-0890
rosalia.blanco@duke.edu

Detailed Description

This registry originally enrolled a total of 1002 participants newly diagnosed with IPF and continues to enroll patients with other chronic fibrosing ILDs with newly identified progressive phenotype to reach an enrollment of 1000 patients. Participants will be enrolled in three phases, (IPF-PRO and ILD-PRO) over a span of 8 years at approximately 50 sites experienced in the diagnosis and treatment of ILD in the United States. Enrollment for the original IPF cohort started in 2014 and ended in October 2018, with 1002 total participants enrolled. In the third phase of the registry new enrollment for patients with IPF will restart in 2023-2024 with the plan to enroll up to 1000 new IPF patients, for a total IPF enrollment of 2000. Enrollment for other chronic fibrosing ILDs with newly identified progressive phenotype cohort was initiated in February 2019 and will end when enrollment reaches 1000 participants with the potential of enrolling another 1000 participants with other chronic fibrosing ILDs with newly identified without a progressive phenotype. Data and samples will be collected from participants for approximately 5 years for the IPF cohort. For the chronic fibrosing ILD with progressive phenotype cohort, data and samples will be collected for a minimum of 3 years, up to approximately 5 years. Participant management and treatment decisions will be determined by participants and their health care professionals.

Notice

Study information shown on this site is derived from ClinicalTrials.gov (a public registry operated by the National Institutes of Health). The listing of studies provided is not certain to be all studies for which you might be eligible. Furthermore, study eligibility requirements can be difficult to understand and may change over time, so it is wise to speak with your medical care provider and individual research study teams when making decisions related to participation.