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RecruitingInterventionalPhase 4

National Liver Cancer Screening Trial

NCT ID: NCT06084234Sponsor: University of Texas Southwestern Medical CenterLast updated: 2025-11-26

Summary

The National Liver Cancer Screening Trial is an adaptive randomized phase IV Trial comparing ultrasound-based versus biomarker-based screening in 5500 patients with cirrhosis from any etiology or patients with chronic hepatitis B infection. Eligible patients will be randomized in a 1:1 fashion to Arm A using semi-annual ultrasound and AFP-based screening or Arm B using semi-annual screening using GALAD alone. Randomization will be stratified by sex, enrolling site, Child Pugh class (A vs. B), and HCC etiology (viral vs. non-viral). Patients will be recruited from 15 sites (mix of tertiary care and large community health systems) over a 3-year period, and the primary endpoint of the phase IV trial, reduction in late-stage HCC, will be assessed after 5.5 years.

Detailed description

The TRACER phase IV biomarker study is a randomized trial comparing ultrasound-based screening versus a biomarker-based strategy in patients with cirrhosis. In brief, 5500 patients with cirrhosis from any etiology would be randomized in a 1:1 fashion to Arm A offering semi-annual ultrasound +/- AFP-based screening or Arm B offering semi-annual biomarker-based screening. Randomization will be stratified by site, Child Pugh class (A vs. B), liver disease etiology (viral, non-viral, and non-cirrhotic HBV infection) and sex. Patients will be recruited from 15 sites (mix of tertiary care and large community health systems) over a 3-year period, and reduction in the proportion of late-stage HCC, will be assessed at the end of Year 5.5. If the results are promising, study team will continue extended follow-up and compare the incidence of late-stage HCC between the two arms at Year 8 and reduction in HCC mortality during long term follow up. Study team will include adult patients, age ≥ 18 years, with Child Pugh class A or B cirrhosis of any etiology or non-cirrhotic chronic hepatitis B virus infection with PAGE-B score \>9. Study team will exclude patients post liver transplantation, patients with Child Pugh C cirrhosis, patients with significant comorbidity and limited life expectancy, and those with history of other malignancy, except non-melanoma skin cancer or indolent tumors, within 3 years prior to enrollment given lack of screening recommendations in those patient populations. Study team will also exclude patients with suspicious liver masses at baseline as well as those with a solid lesion ≥1 cm on ultrasound or AFP ≥20 ng/mL without diagnostic evaluation to exclude HCC. Study team will also exclude patients in whom the provider plans to follow the patient with CT or MRI-based surveillance. GALAD is not recommended in patients with pregnancy or active warfarin use given known impact on biomarker performance, so these patients will be excluded. At enrollment, study team will record patient demographics and clinical characteristics using a combination of electronic medical records and patient questionnaires. Patients will then be offered semi-annual surveillance as defined by their study arm: ultrasound and AFP for patients in Arm A and the biomarker, GALAD, for patients in Arm B. Repeat surveillance tests will be offered every six months (per assigned arm) for patients with normal surveillance results. Diagnostic evaluation with multi-phasic CT or contrast-enhanced MRI will be recommended for any patients with abnormal screening results. Patients with normal diagnostic testing (i.e., false positive result) will be recommended to return to their assigned surveillance arm. Standardized criteria from the AASLD and LI-RADS will be used to define incident HCC. Study team will use a set of validated surveys (e.g., Psychological Consequences Questionnaire, Decision Regret scale, FACIT-COST) to measure secondary outcomes of interest including psychological and financial harms.

Arms & interventions

  • Diagnostic TestGALAD

    GALAD is a 3 biomarker panel incorporating AFP, AFP-L3% and DCP (all FDA approved), with patient age and sex.

  • Diagnostic TestLiver Ultrasound with or without AFP

    This intervention consists of current standard of care ultrasound based surveillance with or without alpha-fetoprotein measurement.

Outcome measures

Primary

  • Proportion of HCC detected at late stage

    Proportion of HCC detected at a late stage, defined as HCC beyond Milan Criteria (one tumor less than or equal to 5 cm or 2-3 tumors each less than or equal to 3 cm, in the absence of vascular invasion or extra-hepatic metastases)

    Time frame: 5.5 years

Secondary

  • HCC Screening utilization

    Time frame: 5.5 years

  • Proportion of HCC detected at a late-stage (defined based on BCLC stage)

    Time frame: 5.5 years

  • Incidence of late-stage HCC

    Time frame: 8 years

  • Proportion of HCC cases that receive Curative therapy

    Time frame: 5.5 years

  • Number of participants who encountered screening related physical harm

    Time frame: 5.5 years

  • Number of participants who encountered screening related financial harm

    Time frame: 5.5 years

  • Number of participants who encountered screening related Psychological harm

    Time frame: 5.5 years

Eligibility criteria

Sex: AllAge: 18 Years to 85 YearsHealthy volunteers: No
Inclusion Criteria: Patient must meet all of the following inclusion criteria: 1. Adult patients ages 18-85 with cirrhosis from any etiology or with chronic hepatitis B with a PAGE-B score greater than 9 within 12 months of enrollment 2. Patient is eligible for HCC surveillance according to treating physician or by the site investigator 3. Able to provide informed consent 4. Life expectancy \>6 months (after consent) as determined by the treating provider or site investigator Exclusion Criteria: Patient will be excluded for any of the following exclusion criteria: 1. Child Pugh C cirrhosis 2. History or clinical symptoms of hepatocellular carcinoma or cholangiocarcinoma 3. History of solid nodule on baseline ultrasound (i.e., lesion 1cm or greater) within 9 months prior to consent without subsequent diagnostic CT/MRI demonstrating benign nature) 4. AFP \>20 ng/mL within 6 months prior to consent, in the absence of a contrast-enhanced CT or MRI within 6 months of AFP (before or after) level demonstrating lack of suspicious liver lesions 5. Newly diagnosed LR-3 greater than or equal to 1 cm within 6 months prior to consent 6. History of LR-4, LR-5, or LR-M on multi-phase CT or contrast-enhanced MRI within 6 months prior to consent 7. Presence of another active cancer besides non-melanomatous skin cancer or indolent cancer under active surveillance (e.g., prostate cancer or renal cell carcinoma) within the 2 years prior to consent 8. Patient's provider is planning to use MRI- or CT- based surveillance moving forward 9. History of a transjugular intrahepatic portosystemic shunt (TIPS) 10. History of Fontan associated liver disease or cardiac cirrhosis 11. History of solid organ transplantation 12. Actively listed for liver transplantation 13. Diagnosis of alcohol-associated hepatitis within 3 months prior to consent 14. Documented current or continued signs and symptoms of acute Wilson disease (acute liver failure, acute neurological deficits, hemolysis) 15. In patients with primary sclerosing cholangitis (PSC): Current active cholangitis within 90 days prior to consent 16. Known or documented habitual non-adherence to previous research studies or medical procedures or unwillingness to adhere to protocol (e.g., unwilling to obtain consent or samples) 17. In patients living with HIV: CD4+ T cell count less than 100 cells/mm3 within 60 days prior to consent 18. Known pregnancy at consent 19. Active warfarin use

Study locations (18)

University of Southern California

Los Angeles, California, 90089

Recruiting
Kali Zhou, MD · Contact
Kali Zhou, MD · Principal Investigator

Stanford University

Redwood City, California, 94063

Recruiting
Paul Kwo, MD · Contact
650-723-5135pkwo@stanford.edu
Jennifer Smart · Contact
650-721-8517Jsmart2@stanford.edu
Paul Kwo, MD · Principal Investigator

Kaiser Permanente

Roseville, California, 95661

Recruiting
Sreepriya Balasubramanian, MD, MPH · Contact
916-474-6221Sreepriya.Balasubramanian@kp.org
Quyen Chau · Contact
4158333468Quyen.X.Chau@kp.org
Sreepriya Balasubramanian, MD, MPH · Principal Investigator

University of California, San Francisco

San Francisco, California, 94117

Recruiting
Rae Davis · Contact
rayshawnda.davis@ucsf.edu
Neil Mehta, MD · Principal Investigator

Northwestern University

Chicago, Illinois, 60611

Recruiting
Laura Kulik, MD · Contact
312-694-1293laura.kulik@nm.org
Kimberly Sipich · Contact
312-694-1293k-sipich@northwestern.edu
Laura Kulik, MD · Principal Investigator

Indiana University

Indianapolis, Indiana, 46202

Recruiting
Sherri Cummins · Contact
shcummin@iu.edu
Naga Chalasani, MD · Principal Investigator

Massachusetts General Hospital

Boston, Massachusetts, 02114

Recruiting
Megan Michta · Contact
MMICHTA@mgh.harvard.edu
Irun Bhan, MD · Principal Investigator

University of Michigan

Ann Arbor, Michigan, 48109

Recruiting
Shay Robison · Contact
roshay@med.umich.edu
Neehar Parikh, MD, MS · Principal Investigator

Henry Ford Health System

Detroit, Michigan, 48202

Recruiting
Jessica Peruski · Contact
jperusk1@hfhs.org
Reena Salgia, MD · Principal Investigator

Hennepin Healthcare

Minneapolis, Minnesota, 55415

Recruiting
Jose Debes, MD · Contact
952-737-9762debes003@umn.edu
Daniel Akah · Contact
9527379762Dakah@bermancenter.org
Jose Debes, MD · Principal Investigator

University of Minnesota

Minneapolis, Minnesota, 55455

Recruiting
Elizabeth Aby, MD · Contact
612-625-8999abyxx002@umn.edu
Erin Wesley · Contact
wesle091@umn.edu
Elizabeth Aby, MD · Principal Investigator

The Feinstein Institutes, Northwell Health, Inc.

Manhasset, New York, 11030

Recruiting
Dibnain Nanda · Contact
dnanda1@northwell.edu
Sanjaya Satapathy, MBBS, MS · Principal Investigator

University of North Carolina

Chapel Hill, North Carolina, 27599

Recruiting
Andrew Moon, MD · Contact
919-843-5936Andrew.Moon@unchealth.unc.edu
Bhagyashree Behera · Contact
919-843-5936BB_Behera@med.unc.edu
Andrew Moon, MD · Principal Investigator

Case Western Reserve University

Cleveland, Ohio, 44106

Recruiting
Pierre Gholam, MD · Contact
216-286-6757pierre.gholam@case.edu
Paul Harris · Contact
216.983.5144Paul.Harris2@UHhospitals.org
Pierre Gholam, MD · Principal Investigator

University of Pennsylvania

Philadelphia, Pennsylvania, 19104

Recruiting
Grace Kim · Contact
gracekim.lee@pennmedicine.upenn.edu
Jorge Marrero, MD,MS · Principal Investigator

UT Southwestern Medical Center and Parkland Hospital

Dallas, Texas, 75390

Recruiting
Sneha Deodhar, MS · Contact
214-645-1378TRACER@UTSouthwestern.edu
Amit Singal, MD, MS · Principal Investigator

Baylor College of Medicine

Houston, Texas, 77021

Recruiting
Emad Sorial · Contact
713-798-7370Emad.Sorial@bcm.edu
· Contact
Sara.Fares@bcm.edu
Fasiha Kanwal, MD, MSHS · Principal Investigator

Virginia Commonwealth University

Richmond, Virginia, 23219

Not Yet Recruiting
Hannah Lee, MD · Contact
804-828-4060Hannah.Lee@vcuhealth.org
Hannah Cook · Contact
804-628-9312Hannah.Cook1@vcuhealth.org
Hannah Lee, MD · Principal Investigator

References

  • Singal AG, Parikh ND, Kanwal F, Marrero JA, Deodhar S, Page-Lester S, Lopez C, Feng Z, Tayob N. National Liver Cancer Screening Trial (TRACER) study protocol. Hepatol Commun. 2024 Nov 4;8(11):e0565. doi: 10.1097/HC9.0000000000000565. eCollection 2024 Nov 1.(PubMed)
National Liver Cancer Screening Trial | Cancerify