Predicting Treatment Response with Sensory Phenotyping in Post-Traumatic Neuropathic Pain

Jennifer S Gewandter; Michael B Sohn; Rachel De Guzman; Maria E Frazer; Valerie Chiodo; Sonia Sharma; Paul Geha; John D Markman

doi:10.1093/pm/pnac045

Predicting Treatment Response with Sensory Phenotyping in Post-Traumatic Neuropathic Pain

Pain Med. 2022 Sep 30;23(10):1726-1732. doi: 10.1093/pm/pnac045.

Authors

Jennifer S Gewandter¹, Michael B Sohn², Rachel De Guzman³, Maria E Frazer³, Valerie Chiodo³, Sonia Sharma⁴, Paul Geha⁵, John D Markman³

Affiliations

¹ Department of Anesthesiology and Perioperative Medicine, University of Rochester, Rochester, New York.
² Department of Biostatistics and Computational Biology, University of Rochester, Rochester, New York.
³ Department of Neurosurgery, University of Rochester, Rochester, New York.
⁴ Department of Oral Diagnostic Sciences, University at Buffalo School of Dental Medicine, Buffalo, New York.
⁵ Department of Psychiatry, University of Rochester, Rochester, New York, USA.

Abstract

Objective: Currently available treatments for neuropathic pain are only modestly efficacious when assessed in randomized clinical trials and work for only some patients in the clinic. Induced-pain or gain-of-function phenotypes have been shown to predict response to analgesics (vs placebos) in patients with neuropathic pain. However, the predictive value of these phenotypes has never been studied in post-traumatic neuropathic pain.

Methods: Mixed-effects models for repeated measures were used to evaluate the efficacy of pregabalin vs placebo in subgroups with induced-pain phenotypes (i.e., hyperalgesia or allodynia) in data from a recent, multinational randomized clinical trial (N = 539) that identified phenotypic subgroups through the use of a structured clinical exam.

Results: The difference in mean pain score between the active and placebo groups (i.e., delta) after 15 weeks of treatment for the subgroup with hyperalgesia was -0.76 (P = 0.001), compared with 0.19 (P = 0.47) for the subgroup that did not have hyperalgesia. The treatment-by-phenotype interaction, which tests whether subgroups have statistically different treatment responses, was significant (P = 0.0067). The delta for the subgroup with allodynia was -0.31 (P = 0.22), compared with -0.30 (P = 0.22) for the subgroup that did not have allodynia (treatment-by-phenotype interaction P = 0.98).

Conclusions: These data suggest that hyperalgesia, but not allodynia, predicts response to pregabalin in patients with chronic post-traumatic neuropathic pain. This study extends the growing data supporting the utility of induced-pain phenotypes to predict response to analgesics in post-traumatic neuropathic pain. Sensory phenotyping in large, multisite trials through the use of a structured clinical exam has the potential to accelerate the development of new analgesics and improve the generalizability of clinical trial results.

Keywords: Clinical Trials; Hyperalgesia; Phenotyping; Post-Traumatic Neuropathic Pain.

Publication types

Randomized Controlled Trial
Research Support, Non-U.S. Gov't

MeSH terms

Analgesics / therapeutic use
Double-Blind Method
Humans
Hyperalgesia* / drug therapy
Hyperalgesia* / etiology
Neuralgia* / drug therapy
Neuralgia* / etiology
Pregabalin / therapeutic use

Substances

Analgesics
Pregabalin