Long Term Follow-up of Mesothelioma Patients and Their Family Members With Germline Mutations in BAP1 and Other Genes
NCT ID: NCT03830229
Last Updated: 2025-12-19
Study Results
The study team has not published outcome measurements, participant flow, or safety data for this trial yet. Check back later for updates.
Basic Information
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RECRUITING
1000 participants
OBSERVATIONAL
2019-03-13
2027-07-05
Brief Summary
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-A gene provides instructions to the body. Mutated genes can sometimes cause cancer. Germline mutations are those people are born with. These mutations in the BAP1 gene can cause mesothelioma and other cancers. Researchers want to study people with germline mutations of BAP1 and other genes known to cause cancer.
Objective:
-To learn how cancer might develop in people with certain gene mutations.
Eligibility:
-People ages 2 and older with a germline mutation in BAP1 or another gene that might cause cancer
Design:
* Participants will be screened with:
* Medical and family history
* Saliva test
* Participants with mesothelioma will be in the NIH Group. Participants without mesothelioma can choose to be in either the NIH Group or the Remote Group.
* Remote Group participants will have a medical and family history by phone. If they have tumor tissue from a previous surgery, it will be tested. They will be contacted once a year by phone.
* NIH Group participants will have a baseline visit. This can take up to 4 days. They may have to stay in the area overnight. The visit will include:
* Physical exam
* Evaluation of tumor tissue if available
* Optional tumor biopsy
* Blood tests
* Scans: A machine will take pictures of the body.
* Photographs of skin lesions or other issues
* Skin exam
* Eye exam
* NIH Group participants will have visits once or twice a year. These will include a physical exam, lab tests, scans, and other tests as needed.
* Participants who have a confirmed mutation will be asked to contact any relatives who may be at risk and ask them about joining the study.
Detailed Description
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* BRCA1-Associated Protein-1 (BAP1), a deubiquitinase involved in regulating DNA repair enzymes, is believed to be a prominent mutation in malignant mesothelioma
* Germline mutations involving BAP1 have been reported in familial studies. These have been associated with a higher likelihood of mesothelioma as well as several other malignancies, including uveal melanoma, cutaneous melanomas, renal cell carcinoma and cholangiocarcinoma
* BAP1 mutations, if found, have a high probability of detecting multiple malignancies in family members.
Objectives:
-To characterize the natural and clinical history of malignant mesothelioma patients and their family members who have germline mutations in BAP1 and other DNA repair/cancer predisposition genes
Eligibility for Genetic Testing:
Cohort 1
-Individual with mesothelioma with deleterious germline mutations in BAP1 or another DNA-repair/cancer predisposition gene(s) (previous testing may have been research or clinical)
OR
* Individual with a diagnosis of mesothelioma who is otherwise eligible for testing on Cohort 2
* Age greater than or equal to 2
Cohort 2
-Individual with a germline BAP1 mutation who does not have a history of mesothelioma (previous testing may have been research or clinical)
OR
-Individual with no personal history of mesothelioma with:
--a first degree biological relative (living or deceased) with a history of mesothelioma
OR
--a first degree biological relative with a CLIA (or equivalent) confirmed germline mutation in BAP1
OR
--a second degree biological relative with a CLIA (or equivalent) confirmed germline mutation in BAP1 if relevant first degree relative is deceased or unavailable for testing
OR
--a first degree biological relative with mesothelioma and a CLIA (or equivalent) confirmed germline mutation in another DNA-repair/cancer predisposition genes
OR
--a second degree biological relative with mesothelioma and a CLIA (or equivalent) confirmed germline mutation in BAP1
-Age greater than or equal to 16 unless participant has a BAP1 mutation or a first degree biological relative with a confirmed TP53 or BAP1 germline mutation; in such cases, will begin screening at age greater than or equal to 2
Eligibility for Surveillance:
Cohort 1
-No additional criteria
Cohort 2
-Testing performed on study must confirm presence of germline mutation in BAP1 or another DNA repair/cancer predisposition gene(s)
Design:
* Individuals with suspected hereditary predisposition to mesothelioma and their families will be recruited to assess for genetic mutations, and to study the natural history of malignancies occurring in germline BAP1 mutations as well as other mutations involved in DNA repair.
* Screening examinations will be offered to those with germline BAP1 mutations as well as other mutations involved in DNA repair/cancer predisposition.
* We will determine if there is a relationship between germline mutation and disease phenotype.
Conditions
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Keywords
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Study Design
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COHORT
PROSPECTIVE
Study Groups
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1/Germline positive mesothelioma
Individuals with mesothelioma who have a BAP1 or other DNA repair/cancer predisposition mutation regardless of CLIA (or equivalent) confirmation
No interventions assigned to this group
2/CLIA confirmed germline mutation without mesothelioma
Individuals with a CLIA (or equivalent) confirmed BAP1 or other DNA repair/cancer predisposition mutation who do not have a diagnosis of mesothelioma
No interventions assigned to this group
Eligibility Criteria
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Inclusion Criteria
* Participant with pathology confirming a diagnosis of mesothelioma.
* Participant must have a deleterious germline BAP1 mutation. Results from either research or clinical analyses are sufficient for this criterion.
OR
-Participant with mesothelioma otherwise eligible for genetic testing in Cohort 2
OR
* Participant must have deleterious germline mutation in another DNA repair/cancer predisposition gene(s) that is listed on a commercially available, cancer-associated common or customized gene panel. Results from either research or clinical analyses are sufficient for this criterion.
* Age greater than or equal to 2 years
Cohort 2:
-Individual with a germline BAP1 mutation who does not have a history of mesothelioma (other cancers are allowed). Results from either research or clinical analyses are sufficient for this criterion.
OR
-Individual with no history of mesothelioma with:
--A biological first degree relative (living or deceased) with a history of mesothelioma
OR
--A first degree biological relative with a CLIA (or equivalent) confirmed germline mutation in BAP1
OR
--A second degree biological relative with a CLIA (or equivalent) confirmed germline mutation in BAP1 if relevant first degree relative is deceased or unavailable for testing,
OR
--A first degree biological relative with mesothelioma and a CLIA (or equivalent) confirmed germline mutation in another DNA-repair/cancer predisposition gene that is listed on a commercially available, cancer-associated common or customized gene panel
OR
* A second degree biological relative with mesothelioma and a CLIA (or equivalent) confirmed germline mutation in BAP1
-Age:
* greater than or equal to 2 years for participants with a BAP1 or TP53 mutation or with a first degree relative that has a germline mutation in TP53 or BAP1
* greater than or equal to 16 years for all other eligible potential mutations
All participants must understand and be willing to sign a written informed consent
* Genetic testing criteria including age restrictions for respective cohorts must be met
* Participants in Cohort 1 may be enrolled with positive results for germline BAP1 mutation or another DNA repair/cancer predisposition gene(s) that is listed on a commercially available, cancer-associated common or customized gene panel regardless of CLIA (or equivalent) confirmation
* Participants in Cohort 2 must have CLIA (or equivalent) confirmed germline BAP1 mutation or another DNA repair/cancer predisposition gene(s) that is listed on a commercially available, cancer-associated common or customized gene panel
OR
-if germline status negative, have a biological relative that is enrolled for surveillance
Exclusion Criteria
None
2 Years
ALL
No
Sponsors
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National Cancer Institute (NCI)
NIH
Responsible Party
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Principal Investigators
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Raffit Hassan, M.D.
Role: PRINCIPAL_INVESTIGATOR
National Cancer Institute (NCI)
Locations
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National Institutes of Health Clinical Center
Bethesda, Maryland, United States
Countries
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Central Contacts
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Facility Contacts
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For more information at the NIH Clinical Center contact National Cancer Institute Referral Office
Role: primary
Related Links
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NIH Clinical Center Detailed Web Page
Other Identifiers
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19-C-0049
Identifier Type: -
Identifier Source: secondary_id
190049
Identifier Type: -
Identifier Source: org_study_id