Moonshots and metastatic disease: the need for a multi-faceted approach when studying atypical responses

Abstract Clinical research generally focuses on results involving a statistical mean with little attention in trial design to patients who respond considerably better or worse than average. Exploring the reasons underlying an “atypical response” will increase understanding of the mechanisms involved...

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Main Authors: Kristine De La Torre, Elly Cohen, Anne Loeser, Marc Hurlbert, on behalf of the Metastatic Breast Cancer Alliance
Format: Article
Language:English
Published: Nature Publishing Group 2017-03-01
Series:npj Breast Cancer
Online Access:https://doi.org/10.1038/s41523-017-0010-1
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spelling doaj-e7649f26f6ab49d3870900bb82fb14bf2020-12-07T18:44:04ZengNature Publishing Groupnpj Breast Cancer2374-46772017-03-01311510.1038/s41523-017-0010-1Moonshots and metastatic disease: the need for a multi-faceted approach when studying atypical responsesKristine De La Torre0Elly Cohen1Anne Loeser2Marc Hurlbert3on behalf of the Metastatic Breast Cancer AllianceMetastatic Breast Cancer AllianceMetastatic Breast Cancer AllianceMetastatic Breast Cancer AllianceMetastatic Breast Cancer AllianceAbstract Clinical research generally focuses on results involving a statistical mean with little attention in trial design to patients who respond considerably better or worse than average. Exploring the reasons underlying an “atypical response” will increase understanding of the mechanisms involved in cancer progression and treatment resistance, accelerate biomarker identification, and improve precision medicine by allowing clinicians to prospectively select optimal treatments. Based on our review, we suggest two ways to move this field forward. First, we suggest that clear categorization of “atypical responders” is needed. This encompasses three sub-categories of patients: “exceptional responders” (those with an unusually favorable treatment response), “rapid progressors” (patients demonstrating an unusually poor or no therapeutic response), and “exceptional survivors” (patients who have far outlived their initial prognosis). Such categorization may depend upon the clinical context and disease subtype. Second, we suggest that atypical responses may be due not only to somatic mutations in tumors, but also to inherited polymorphisms in non-tumor tissue, host and tumor environments, lifestyle factors, co-morbidities, use of complementary and integrative medicine, and the interaction among these components. Here, we summarize new research initiatives exploring atypical responses, the potential reasons for atypical responses, and a strategic call to action. Rigorous studies of normal and atypical responses to treatment will be needed to strengthen understanding of the role of non-tumor factors. Clinical trial design for targeted and other types of therapies should be enhanced to collect data in a standardized manner beyond tumor genetics, resulting in more thorough study of the whole patient.https://doi.org/10.1038/s41523-017-0010-1
collection DOAJ
language English
format Article
sources DOAJ
author Kristine De La Torre
Elly Cohen
Anne Loeser
Marc Hurlbert
on behalf of the Metastatic Breast Cancer Alliance
spellingShingle Kristine De La Torre
Elly Cohen
Anne Loeser
Marc Hurlbert
on behalf of the Metastatic Breast Cancer Alliance
Moonshots and metastatic disease: the need for a multi-faceted approach when studying atypical responses
npj Breast Cancer
author_facet Kristine De La Torre
Elly Cohen
Anne Loeser
Marc Hurlbert
on behalf of the Metastatic Breast Cancer Alliance
author_sort Kristine De La Torre
title Moonshots and metastatic disease: the need for a multi-faceted approach when studying atypical responses
title_short Moonshots and metastatic disease: the need for a multi-faceted approach when studying atypical responses
title_full Moonshots and metastatic disease: the need for a multi-faceted approach when studying atypical responses
title_fullStr Moonshots and metastatic disease: the need for a multi-faceted approach when studying atypical responses
title_full_unstemmed Moonshots and metastatic disease: the need for a multi-faceted approach when studying atypical responses
title_sort moonshots and metastatic disease: the need for a multi-faceted approach when studying atypical responses
publisher Nature Publishing Group
series npj Breast Cancer
issn 2374-4677
publishDate 2017-03-01
description Abstract Clinical research generally focuses on results involving a statistical mean with little attention in trial design to patients who respond considerably better or worse than average. Exploring the reasons underlying an “atypical response” will increase understanding of the mechanisms involved in cancer progression and treatment resistance, accelerate biomarker identification, and improve precision medicine by allowing clinicians to prospectively select optimal treatments. Based on our review, we suggest two ways to move this field forward. First, we suggest that clear categorization of “atypical responders” is needed. This encompasses three sub-categories of patients: “exceptional responders” (those with an unusually favorable treatment response), “rapid progressors” (patients demonstrating an unusually poor or no therapeutic response), and “exceptional survivors” (patients who have far outlived their initial prognosis). Such categorization may depend upon the clinical context and disease subtype. Second, we suggest that atypical responses may be due not only to somatic mutations in tumors, but also to inherited polymorphisms in non-tumor tissue, host and tumor environments, lifestyle factors, co-morbidities, use of complementary and integrative medicine, and the interaction among these components. Here, we summarize new research initiatives exploring atypical responses, the potential reasons for atypical responses, and a strategic call to action. Rigorous studies of normal and atypical responses to treatment will be needed to strengthen understanding of the role of non-tumor factors. Clinical trial design for targeted and other types of therapies should be enhanced to collect data in a standardized manner beyond tumor genetics, resulting in more thorough study of the whole patient.
url https://doi.org/10.1038/s41523-017-0010-1
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