Variability in biopsy quality informs translational research applications in hepatocellular carcinoma

Kelley Weinfurtner; Joshua Cho; Daniel Ackerman; James X. Chen; Abashai Woodard; Wuyan Li; David Ostrowski; Michael C. Soulen; Mandeep Dagli; Susan Shamimi-Noori; Jeffrey Mondschein; Deepak Sudheendra; S. William Stavropoulos; Shilpa Reddy; Jonas Redmond; Tamim Khaddash; Darshana Jhala; Evan S. Siegelman; Emma E. Furth; Stephen J. Hunt; Gregory J. Nadolski; David E. Kaplan; Terence P. F. Gade

doi:10.1038/s41598-021-02093-6

Scientific Reports (Nov 2021)

Variability in biopsy quality informs translational research applications in hepatocellular carcinoma

Kelley Weinfurtner,
Joshua Cho,
Daniel Ackerman,
James X. Chen,
Abashai Woodard,
Wuyan Li,
David Ostrowski,
Michael C. Soulen,
Mandeep Dagli,
Susan Shamimi-Noori,
Jeffrey Mondschein,
Deepak Sudheendra,
S. William Stavropoulos,
Shilpa Reddy,
Jonas Redmond,
Tamim Khaddash,
Darshana Jhala,
Evan S. Siegelman,
Emma E. Furth,
Stephen J. Hunt,
Gregory J. Nadolski,
David E. Kaplan,
Terence P. F. Gade

Affiliations

Kelley Weinfurtner: Division of Gastroenterology and Hepatology, University of Pennsylvania
Joshua Cho: Penn Image-Guided Interventions Laboratory, University of Pennsylvania
Daniel Ackerman: Penn Image-Guided Interventions Laboratory, University of Pennsylvania
James X. Chen: Vascular & Interventional Specialists of Charlotte Radiology
Abashai Woodard: Department of Radiology, University of Pennsylvania
Wuyan Li: Penn Image-Guided Interventions Laboratory, University of Pennsylvania
David Ostrowski: Penn Image-Guided Interventions Laboratory, University of Pennsylvania
Michael C. Soulen: Division of Interventional Radiology, University of Pennsylvania
Mandeep Dagli: Division of Interventional Radiology, University of Pennsylvania
Susan Shamimi-Noori: Division of Interventional Radiology, University of Pennsylvania
Jeffrey Mondschein: Division of Interventional Radiology, University of Pennsylvania
Deepak Sudheendra: Division of Interventional Radiology, University of Pennsylvania
S. William Stavropoulos: Division of Interventional Radiology, University of Pennsylvania
Shilpa Reddy: Division of Interventional Radiology, University of Pennsylvania
Jonas Redmond: Division of Interventional Radiology, University of Pennsylvania
Tamim Khaddash: Division of Interventional Radiology, University of Pennsylvania
Darshana Jhala: Department of Pathology and Laboratory Medicine, University of Pennsylvania
Evan S. Siegelman: Department of Radiology, University of Pennsylvania
Emma E. Furth: Department of Pathology and Laboratory Medicine, University of Pennsylvania
Stephen J. Hunt: Penn Image-Guided Interventions Laboratory, University of Pennsylvania
Gregory J. Nadolski: Penn Image-Guided Interventions Laboratory, University of Pennsylvania
David E. Kaplan: Division of Gastroenterology and Hepatology, University of Pennsylvania
Terence P. F. Gade: Penn Image-Guided Interventions Laboratory, University of Pennsylvania

DOI: https://doi.org/10.1038/s41598-021-02093-6
Journal volume & issue: Vol. 11, no. 1
pp. 1 – 10

Abstract

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Abstract In the era of precision medicine, biopsies are playing an increasingly central role in cancer research and treatment paradigms; however, patient outcomes and analyses of biopsy quality, as well as impact on downstream clinical and research applications, remain underreported. Herein, we report biopsy safety and quality outcomes for percutaneous core biopsies of hepatocellular carcinoma (HCC) performed as part of a prospective clinical trial. Patients with a clinical diagnosis of HCC were enrolled in a prospective cohort study for the genetic, proteomic, and metabolomic profiling of HCC at two academic medical centers from April 2016 to July 2020. Under image guidance, 18G core biopsies were obtained using coaxial technique at the time of locoregional therapy. The primary outcome was biopsy quality, defined as tumor fraction in the core biopsy. 56 HCC lesions from 50 patients underwent 60 biopsy events with a median of 8 core biopsies per procedure (interquartile range, IQR, 7–10). Malignancy was identified in 45/56 (80.4%, 4 without pathology) biopsy events, including HCC (40/56, 71.4%) and cholangiocarcinoma (CCA) or combined HCC-CCA (5/56, 8.9%). Biopsy quality was highly variable with a median of 40% tumor in each biopsy core (IQR 10–75). Only 43/56 (76.8%) and 23/56 (41.1%) samples met quality thresholds for genomic or metabolomic/proteomic profiling, respectively, requiring expansion of the clinical trial. Overall and major complication rates were 5/60 (8.3%) and 3/60 (5.0%), respectively. Despite uniform biopsy protocol, biopsy quality varied widely with up to 59% of samples to be inadequate for intended purpose. This finding has important consequences for clinical trial design and highlights the need for quality control prior to applications in which the presence of benign cell types may substantially alter findings.

Published in Scientific Reports

ISSN: 2045-2322 (Online)
Publisher: Nature Portfolio
Country of publisher: United Kingdom
LCC subjects: Medicine; Science
Website: https://www.nature.com/srep/

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