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HepatoScore ‐14: Measures of Biological Heterogeneity Significantly Improve Prediction of Hepatocellular Carcinoma Risk
Author(s) -
Morris Jeffrey S.,
Hassan Manal M.,
Zohner Ye Emma,
Wang Zeya,
Xiao Lianchun,
Rashid Asif,
Haque Abedul,
AbdelWahab Reham,
Mohamed Yehia I.,
Ballard Karri L.,
Wolff Robert A.,
George Bhawana,
Li Liang,
Allen Genevera,
Weylandt Michael,
Li Donghui,
Wang Wenyi,
Raghav Kanwal,
Yao James,
Amin Hesham M.,
Kaseb Ahmed Omar
Publication year - 2021
Publication title -
hepatology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.488
H-Index - 361
eISSN - 1527-3350
pISSN - 0270-9139
DOI - 10.1002/hep.31555
Subject(s) - hepatocellular carcinoma , biomarker , medicine , oncology , risk stratification , clinical trial , biology , biochemistry
Background and Aims Therapeutic, clinical trial entry and stratification decisions for hepatocellular carcinoma (HCC) are made based on prognostic assessments, using clinical staging systems based on small numbers of empirically selected variables that insufficiently account for differences in biological characteristics of individual patients’ disease. Approach and Results We propose an approach for constructing risk scores from circulating biomarkers that produce a global biological characterization of individual patient’s disease. Plasma samples were collected prospectively from 767 patients with HCC and 200 controls, and 317 proteins were quantified in a Clinical Laboratory Improvement Amendments–certified biomarker testing laboratory. We constructed a circulating biomarker aberration score for each patient, a score between 0 and 1 that measures the degree of aberration of his or her biomarker panel relative to normal, which we call HepatoScore . We used log‐rank tests to assess its ability to substratify patients within existing staging systems/prognostic factors. To enhance clinical application, we constructed a single‐sample score, HepatoScore‐14 , which requires only a subset of 14 representative proteins encompassing the global biological effects. Patients with HCC were split into three distinct groups (low, medium, and high HepatoScore) with vastly different prognoses (medial overall survival 38.2/18.3/7.1 months; P < 0.0001). Furthermore, HepatoScore accurately substratified patients within levels of existing prognostic factors and staging systems ( P < 0.0001 for nearly all), providing substantial and sometimes dramatic refinement of expected patient outcomes with strong therapeutic implications. These results were recapitulated by HepatoScore‐14, rigorously validated in repeated training/test splits, concordant across Myriad RBM (Austin, TX) and enzyme‐linked immunosorbent assay kits, and established as an independent prognostic factor. Conclusions HepatoScore‐14 augments existing HCC staging systems, dramatically refining patient prognostic assessments and therapeutic decision making and enrollment in clinical trials. The underlying strategy provides a global biological characterization of disease, and can be applied broadly to other disease settings and biological media.