Literature DB >> 35126358

Investigating Molecular Signatures Underlying Trapeziometacarpal Osteoarthritis Through the Evaluation of Systemic Cytokine Expression.

Anusha Ratneswaran1,2,3, Jason S Rockel2,3, Daniel Antflek1,3, John J Matelski4, Konstantin Shestopaloff2,3, Mohit Kapoor2,3,5, Heather Baltzer1,3,6.   

Abstract

Purpose: Non-operative management of trapeziometacarpal osteoarthritis (TMOA) demonstrates only short-term symptomatic alleviation, and no approved disease modifying drugs exist to treat this condition. A key issue in these patients is that radiographic disease severity can be discordant with patient reported pain, illustrating the need to identify molecular mediators of disease. This study characterizes the biochemical profile of TMOA patients to elucidate molecular mechanisms driving TMOA progression.
Methods: Plasma from patients with symptomatic TMOA undergoing surgical (n=39) or non-surgical management (n=44) with 1-year post-surgical follow-up were compared using a targeted panel of 27 cytokines. Radiographic (Eaton-Littler), anthropometric, longitudinal pain (VAS, TASD, quick DASH) and functional (key pinch, grip strength) data were used to evaluate relationships between structure, pain, and systemic cytokine expression. Principal Component Analysis was used to identify clusters of patients.
Results: Patients undergoing surgery had greater BMI as well as higher baseline quick DASH, TASD scores. Systemically, these patients could only be distinguished by differing levels of Interleukin-7 (IL-7), with an adjusted odds ratio of 0.22 for surgery for those with increased levels of this cytokine. Interestingly, PCA analysis of all patients (regardless of surgical status) identified a subset of patients with an "inflammatory" phenotype, as defined by a unique molecular signature consisting of thirteen cytokines.
Conclusion: Overall, this study demonstrated that circulating cytokines are capable of distinguishing TMOA disease severity, and identified IL-7 as a target capable of differentiating disease severity with higher levels associated with a decreased likelihood of TMOA needing surgical intervention. It also identified a cluster of patients who segregate based on a molecular signature of select cytokines.
Copyright © 2022 Ratneswaran, Rockel, Antflek, Matelski, Shestopaloff, Kapoor and Baltzer.

Entities:  

Keywords:  cytokine; inflammation; molecular factors; osteoarthritis; trapeziometacarpal osteoarthritis

Mesh:

Substances:

Year:  2022        PMID: 35126358      PMCID: PMC8814933          DOI: 10.3389/fimmu.2021.794792

Source DB:  PubMed          Journal:  Front Immunol        ISSN: 1664-3224            Impact factor:   7.561


  51 in total

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Authors:  Benton E Heyworth; Jonathan H Lee; Paul D Kim; Carter B Lipton; Robert J Strauch; Melvin P Rosenwasser
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Journal:  Nat Rev Rheumatol       Date:  2018-11       Impact factor: 20.543

8.  Efficacy of treatments and pain management for trapeziometacarpal (thumb base) osteoarthritis: protocol for a systematic review.

Authors:  Tokiko Hamasaki; Lyne Lalonde; Patrick Harris; Nathalie J Bureau; Nathaly Gaudreault; Daniela Ziegler; Manon Choinière
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9.  Chemokine analysis as a novel diagnostic modality in the early prediction of the outcome of non-union therapy: a matched pair analysis.

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Journal:  J Orthop Surg Res       Date:  2018-10-10       Impact factor: 2.359

10.  Equivalent PROMIS Scores after Nonoperative or Operative Treatment of Trapeziometacarpal Osteoarthritis.

Authors:  Suresh K Nayar; Rebecca Glasser; E Gene Deune; John V Ingari; Dawn M LaPorte
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