4.2 Article

Immunohistochemical Assays for Bladder Cancer Molecular Subtyping: Optimizing Parsimony and Performance of Lund Taxonomy Classifiers

期刊

JOURNAL OF HISTOCHEMISTRY & CYTOCHEMISTRY
卷 70, 期 5, 页码 357-375

出版社

SAGE PUBLICATIONS LTD
DOI: 10.1369/00221554221095530

关键词

CDKN2A; histopathology; LundTax; urothelial carcinoma

资金

  1. Ontario Institute for Cancer Research through Government of Ontario
  2. Bladder Cancer Canada
  3. Swedish Cancer Society
  4. Cancer Research Society

向作者/读者索取更多资源

A study classified bladder cancers into molecular subtypes and developed compact algorithms, demonstrating that simple immunohistochemistry classifiers can accurately distinguish different subtypes, providing appealing options for clinical implementation.
Transcriptomic and proteomic profiling classify bladder cancers into luminal and basal molecular subtypes, with controversial prognostic and predictive associations. The complexity of published subtyping algorithms is a major impediment to understanding their biology and validating or refuting their clinical use. Here, we optimize and validate compact algorithms based on the Lund taxonomy, which separates luminal subtypes into urothelial-like (Uro) and genomically unstable (GU). We characterized immunohistochemical expression data from two muscle-invasive bladder cancer cohorts (n=193, n=76) and developed efficient decision tree subtyping models using 4-fold cross-validation. We demonstrated that a published algorithm using routine assays (GATA3, KRT5, p16) classified basal/luminal subtypes and basal/Uro/GU subtypes with 86%-95% and 67%-86% accuracies, respectively. KRT14 and RB1 are less frequently used in pathology practice but achieved the simplest, most accurate models for basal/luminal and basal/Uro/GU discrimination, with 93%-96% and 85%-86% accuracies, respectively. More complex models with up to eight antibodies performed no better than simpler two- or three-antibody models. We conclude that simple immunohistochemistry classifiers can accurately identify luminal (Uro, GU) and basal subtypes and are appealing options for clinical implementation.

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