Technology in Cancer Research & Treatment (Sep 2022)

A Multimodal Approach to Discover Biomarkers for Taxane-Induced Peripheral Neuropathy (TIPN): A Study Protocol

  • Anukriti Sharma PhD,
  • Ken B. Johnson MD,
  • Bihua Bie MD, PhD,
  • Emily E. Rhoades PhD,
  • Alper Sen MD,
  • Yuri Kida MS,
  • Jennifer Hockings PharmD, PhD,
  • Alycia Gatta BS,
  • Jacqueline Davenport MS,
  • Connie Arcangelini BS,
  • Jennifer Ritzu BS,
  • Jennifer DeVecchio BS,
  • Ron Hughen BS,
  • Mei Wei MD,
  • G. Thomas Budd MD,
  • N. Lynn Henry MD,
  • Charis Eng MD, PhD,
  • Joseph Foss MD,
  • Daniel M. Rotroff PhD

DOI
https://doi.org/10.1177/15330338221127169
Journal volume & issue
Vol. 21

Abstract

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Introduction: Taxanes are a class of chemotherapeutics commonly used to treat various solid tumors, including breast and ovarian cancers. Taxane-induced peripheral neuropathy (TIPN) occurs in up to 70% of patients, impacting quality of life both during and after treatment. TIPN typically manifests as tingling and numbness in the hands and feet and can cause irreversible loss of function of peripheral nerves. TIPN can be dose-limiting, potentially impacting clinical outcomes. The mechanisms underlying TIPN are poorly understood. As such, there are limited treatment options and no tools to provide early detection of those who will develop TIPN. Although some patients may have a genetic predisposition, genetic biomarkers have been inconsistent in predicting chemotherapy-induced peripheral neuropathy (CIPN). Moreover, other molecular markers (eg, metabolites, mRNA, miRNA, proteins) may be informative for predicting CIPN, but remain largely unexplored. We anticipate that combinations of multiple biomarkers will be required to consistently predict those who will develop TIPN. Methods: To address this clinical gap of identifying patients at risk of TIPN, we initiated the Genetics and Inflammatory Markers for CIPN (GENIE) study. This longitudinal multicenter observational study uses a novel, multimodal approach to evaluate genomic variation, metabolites, DNA methylation, gene expression, and circulating cytokines/chemokines prior to, during, and after taxane treatment in 400 patients with breast cancer. Molecular and patient reported data will be collected prior to, during, and after taxane therapy. Multi-modal data will be used to develop a set of comprehensive predictive biomarker signatures of TIPN. Conclusion: The goal of this study is to enable early detection of patients at risk of developing TIPN, provide a tool to modify taxane treatment to minimize morbidity from TIPN, and improved patient quality of life. Here we provide a brief review of the current state of research into CIPN and TIPN and introduce the GENIE study design.