4.3 Review

Biomarkers of therapeutic response with immune checkpoint inhibitors

Journal

ANNALS OF TRANSLATIONAL MEDICINE
Volume 9, Issue 12, Pages -

Publisher

AME PUBLISHING COMPANY
DOI: 10.21037/atm-20-6396

Keywords

Biomarker; immune checkpoint inhibitors (ICPIs); predictive; prognostic

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While ICPI therapy has revolutionized the treatment paradigm and shown durable responses in a wide range of malignancies, only a small proportion of patients benefit from it. Development of biomarkers to predict response is crucial, but currently only a few markers are validated and approved for use, limiting their broad application.
Immune checkpoint inhibitors (ICPIs) have revolutionized the treatment paradigm of a wide range of malignancies with durable responses seen in even advanced, refractory cancers. Unfortunately, only a small proportion of patients with cancer derive meaningful benefit to ICPI therapy, and its use is also limited by significant immune and financial toxicities. Thus, there is a critical need for the development of biomarkers to reliably predict response to ICPI therapy. Only a few biomarkers are validated and approved for use with currently Food and Drug administration (FDA)-approved ICPIs. The development and broad application of biomarkers is limited by the lack of complete understanding of the complex interactions of tumor-host environment, the effect of immunotherapies on these already complex interactions, a lack of standardization and interpretation of biomarker assays across tumor types. Despite these challenges, the field of identifying predictive biomarkers is evolving at an unprecedented pace leaving the clinician responsible for identifying the patients that may derive optimal benefit from ICPIs. In this review, we provide clinicians with a current and practical update on the key, clinically relevant biomarkers of response to ICPIs. We categorize the current and emerging biomarkers of response to ICPIs in four major categories that govern anticancer response-the inflamed tumor, tumor antigens, immune suppression, and overall host environment.

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