Study Results
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Basic Information
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RECRUITING
590 participants
OBSERVATIONAL
2017-12-17
2025-12-31
Brief Summary
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Detailed Description
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Population 1: Sensitivity and Specificity Thresholding.
In this phase, the technical feasibility of the intended use case will be assessed in the intended use population relative to known cancer status as established by standard clinical methods. ctDNA samples from enrolled patients will be assessed in each of the following cohorts:
Cohort 1A: High-risk patients negative for lung cancer by CT screening and clinical follow-up.
Cohort 1B: Patients with lung nodules ≥6 mm by CT but negative for lung cancer by extended (3 years) CT screening follow-up.
Cohort 1C: Patients with lung cancer (histologically proven or by consensus tumor board opinion of ≥90% probability of cancer) prior to definitive therapy.
Population 2: Clinical Intended Use Performance. In this phase, the clinical performance of the ctDNA assay will be evaluated in patients with high clinical suspicion for lung cancer. ctDNA will be compared to the clinical diagnosis made according to the standard of care (e.g. biopsy, CT surveillance, etc.). ctDNA samples from enrolled patients will be assessed in each of the following cohorts:
Cohort 2A: High-risk patients newly positive (Lung imaging Reporting And Data System (Lung-RADS) \>=3) by CT screening.
Cohort 2B: Patients with \>= 6 mm lung nodules suspicious for lung cancer by treating physician judgment.
Cohort 2C: Patients with a personal history of lung cancer after completion of curative intent treatment but without evidence of recurrence.
Specific Aim 1: To estimate the ctDNA assay sensitivity and specificity requirements in the specific clinical use populations using patients with known non-small cell lung cancer status.
Specific Aim 2: To prospectively estimate the ctDNA assay clinical performance in the clinical application of interest.
ENDPOINTS
Primary Endpoints
Specific Aim 1: Estimation of the ctDNA assay's clinical sensitivity and specificity in patients with lung cancer as proven by histology or tumor board consensus opinion\* and in patients with lung nodule ≥6 mm but without cancer as proven by extended CT screening follow-up\*\*.
\*Patients may be treated with curative-intent Stereotactic Body Radiotherapy (SBRT) without tissue confirmation IF pretest probability for lung cancer by tumor board consensus opinion is ≥90% and the biopsy risk is high.
\*\*Extended CT screening follow-up defined by documentation of ≥3 years of radiographic stability and consensus clinical opinion.
Specific Aim 2: Estimation of the ctDNA assay's clinical predictive value relative to standard of care diagnostic work-up in suspicious nodule adjudication in both the high-risk and general populations (the clinical applications of interest).
Secondary Endpoints
* Correlation of the ctDNA assay performance with Lung-RADS radiographic criteria
* Correlation of Lung-RADS with disease truth defined by clinical follow up as the definite gold standard
Exploratory Endpoints
* Correlation of plasma and tissue genotyping results
* Correlation of the ctDNA assay with orthogonal reference technologies (e.g. ddPCR)
* Correlation of the ctDNA assay performance with histologic sub-type and clinical course (e.g. aggressive vs. indolent disease)
* Correlation of the ctDNA assay performance with clinical lung cancer risk factors
* Correlation of the ctDNA assay results pre-and post-resection
* Correlation of follow-up the ctDNA assay results and kinetics vs. clinical recurrence post-resection or radiotherapy
* Estimation of theoretical biopsy avoidance rate in clinical use population.
Conditions
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Study Design
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COHORT
PROSPECTIVE
Study Groups
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Cohort 1A: Benign nodule on screening CT
High-risk patients eligible for lung cancer screening but with negative radiographic findings on CT screening (Lung RADS ≤2).
1. ≥30 pack-year history of cigarette smoking
2. ≥55 years of age
3. Current smoker or quit within the past 15 years
Guardant Health ct-DNA LUNAR assay
Guardant Health is focused on conquering cancer by using its breakthrough blood-based assays, vast data sets, and advanced analytics. In 2016, it announced Project LUNAR, an effort to apply Guardant Health's technology platform to early detection, recurrence monitoring, and assessing minimal residual disease.
Cohort 1B: Incidental benign nodule
Patients with lung nodules ≥ 6 mm on routine (non-lung cancer screening) CT evaluation deemed suspicious for malignancy by initial physician judgment but not malignant by ≥2 years of radiographic stability and consensus clinical opinion.
1- Age ≥40 years.
Guardant Health ct-DNA LUNAR assay
Guardant Health is focused on conquering cancer by using its breakthrough blood-based assays, vast data sets, and advanced analytics. In 2016, it announced Project LUNAR, an effort to apply Guardant Health's technology platform to early detection, recurrence monitoring, and assessing minimal residual disease.
Cohort IC: Presumed lung cancer
Patients with lung cancer (histologically proven or presumed by consensus opinion of tumor board); prior to definitive therapy.
1- Age ≥40 years.
Guardant Health ct-DNA LUNAR assay
Guardant Health is focused on conquering cancer by using its breakthrough blood-based assays, vast data sets, and advanced analytics. In 2016, it announced Project LUNAR, an effort to apply Guardant Health's technology platform to early detection, recurrence monitoring, and assessing minimal residual disease.
Cohort 2A: Suspicious nodule
High-risk patients with newly diagnosed suspicious nodule of Lung RADS ≥3 on CT screening.
1. ≥30 pack-year history of cigarette smoking
2. ≥55 years of age
3. Current smoker or quit within the past 15 years
Guardant Health ct-DNA LUNAR assay
Guardant Health is focused on conquering cancer by using its breakthrough blood-based assays, vast data sets, and advanced analytics. In 2016, it announced Project LUNAR, an effort to apply Guardant Health's technology platform to early detection, recurrence monitoring, and assessing minimal residual disease.
Cohort 2B: Suspicious incidental nodule
Patients with newly diagnosed incidentally-found lung nodules ≥ 6 mm on routine CT evaluation deemed suspicious for malignancy by physician judgment.
1- Age ≥40 years.
Guardant Health ct-DNA LUNAR assay
Guardant Health is focused on conquering cancer by using its breakthrough blood-based assays, vast data sets, and advanced analytics. In 2016, it announced Project LUNAR, an effort to apply Guardant Health's technology platform to early detection, recurrence monitoring, and assessing minimal residual disease.
Cohort 2C: Post-treatment lung cancer
Patients with previously treated lung cancer (histologically proven or by consensus opinion); status-post completion of definitive therapy (resection +/- chemotherapy or SBRT with curative intent) within the previous year with no current evidence of disease.
1- Age ≥40 years.
Guardant Health ct-DNA LUNAR assay
Guardant Health is focused on conquering cancer by using its breakthrough blood-based assays, vast data sets, and advanced analytics. In 2016, it announced Project LUNAR, an effort to apply Guardant Health's technology platform to early detection, recurrence monitoring, and assessing minimal residual disease.
Interventions
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Guardant Health ct-DNA LUNAR assay
Guardant Health is focused on conquering cancer by using its breakthrough blood-based assays, vast data sets, and advanced analytics. In 2016, it announced Project LUNAR, an effort to apply Guardant Health's technology platform to early detection, recurrence monitoring, and assessing minimal residual disease.
Other Intervention Names
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Eligibility Criteria
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Inclusion Criteria
* Ability to understand and provide written informed consent
* Willingness to comply with study protocols and provide blood samples.
* Willingness to complete 3-year clinical follow up
Exclusion Criteria
* Anemia - measured by hematocrit level of less than 30%, measured after the first blood draw.
* Malnourishment - determined by BMI less than 19. If subject has BMI greater or equal to 19, but has a history of malnourishment, study staff will measure albumin level of subject's blood after initial blood draw. Albumin level must be greater than 2.5 mg per deciliter, or subject will be excluded.
* Severe Chronic Obstructive Pulmonary Disease (COPD) - defined by Gold Stage IV.
* Unstable heart conditions - defined by stable or unstable angina, recent myocardial infarction (within the last 2 years), active congestive heart failure, ischemic cardiomyopathy, or history of complications because of previous blood donation.
* Liver cirrhosis.
40 Years
ALL
No
Sponsors
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Northern California Institute of Research and Education
OTHER
Guardant Health, Inc.
INDUSTRY
University of California, San Francisco
OTHER
Responsible Party
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Principal Investigators
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Mehrdad Arjomandi, M.D.
Role: PRINCIPAL_INVESTIGATOR
University of California, San Francisco
Locations
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Zuckerberg San Francisco General Hospital and Trauma Center
San Francisco, California, United States
San Francisco VA Medical Center
San Francisco, California, United States
University of California, San Francisco
San Francisco, California, United States
Countries
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Central Contacts
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Facility Contacts
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Other Identifiers
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176517
Identifier Type: OTHER
Identifier Source: secondary_id
17-22915
Identifier Type: -
Identifier Source: org_study_id
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