Heterogeneous treatment effects represent a major issue for medicine as they undermine reliable inference and clinical decision-making. To overcome the issue, the current vision of precision and personalized medicine acknowledges the need to control individual variability in response to treatment. In this paper, we argue that gene-treatment-environment interactions (G x T x E) undermine inferences about individual treatment effects from the results of both genomics-based methodologies-such as genome-wide association studies (GWAS) and genome-wide interaction studies (GWIS)-and randomized controlled trials (RCTs). Then, we argue that N-of-1 trials can be a solution to overcome difficulties in handling individual variability in treatment response. Although this type of trial has been suggested as a promising strategy to assess individual treatment effects, it nonetheless has limitations that limit its use in everyday clinical practice. We analyze the existing variability within the designs of N-of-1 trials in terms of a continuum where each design prioritizes epistemic and pragmatic considerations. We then support wider use of the designs located at the pragmatic end of the explanatory-pragmatic continuum.

Averaged versus individualized: pragmatic N-of-1 design as a method to investigate individual treatment response / D. Serpico, M. Maziarz. - In: EUROPEAN JOURNAL FOR PHILOSOPHY OF SCIENCE. - ISSN 1879-4912. - 13:4(2023), pp. 59.1-59.28. [10.1007/s13194-023-00559-0]

Averaged versus individualized: pragmatic N-of-1 design as a method to investigate individual treatment response

D. Serpico
Co-primo
;
2023

Abstract

Heterogeneous treatment effects represent a major issue for medicine as they undermine reliable inference and clinical decision-making. To overcome the issue, the current vision of precision and personalized medicine acknowledges the need to control individual variability in response to treatment. In this paper, we argue that gene-treatment-environment interactions (G x T x E) undermine inferences about individual treatment effects from the results of both genomics-based methodologies-such as genome-wide association studies (GWAS) and genome-wide interaction studies (GWIS)-and randomized controlled trials (RCTs). Then, we argue that N-of-1 trials can be a solution to overcome difficulties in handling individual variability in treatment response. Although this type of trial has been suggested as a promising strategy to assess individual treatment effects, it nonetheless has limitations that limit its use in everyday clinical practice. We analyze the existing variability within the designs of N-of-1 trials in terms of a continuum where each design prioritizes epistemic and pragmatic considerations. We then support wider use of the designs located at the pragmatic end of the explanatory-pragmatic continuum.
Conflicting results; Gene-environment interactions; Genome-wide association studies (GWAS); N-of-1 trials; P-medicine; Randomized controlled trials (RCTs)
Settore M-FIL/02 - Logica e Filosofia della Scienza
2023
Article (author)
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Utilizza questo identificativo per citare o creare un link a questo documento: https://hdl.handle.net/2434/1045468
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