Literature DB >> 34126803

Identifying Phenotypically Distinct Fibroblast Subsets in Type 2 Diabetes-Associated Iatrogenic Laryngotracheal Stenosis.

Ioan A Lina1, Alexandra Berges1, Rafael Ospino1, Ruth J Davis1, Kevin M Motz1, Hsiu-Wen Tsai1, Samuel Collins1, Alexander T Hillel1.   

Abstract

OBJECTIVE: Iatrogenic laryngotracheal stenosis (iLTS) is the pathologic narrowing of the glottis, subglottis, and/or trachea secondary to intubation or tracheostomy related injury. Patients with type 2 diabetes mellitus (T2DM) are more likely to develop iLTS. To date, the metabolomics and phenotypic expression of cell markers in fibroblasts derived from patients with T2DM and iLTS are largely unknown. STUDY
DESIGN: Controlled in vitro cohort study.
SETTING: Tertiary referral center (2017-2020).
METHODS: This in vitro study assessed samples from 6 patients with iLTS who underwent surgery at a single institution. Fibroblasts were isolated from biopsy specimens of laryngotracheal scar and normal-appearing trachea and compared with controls obtained from the trachea of rapid autopsy specimens. Patients with iLTS were subcategorized into those with and without T2DM. Metabolic substrates were identified by mass spectrometry, and cell protein expression was measured by flow cytometry.
RESULTS: T2DM iLTS-scar fibroblasts had a metabolically distinct profile and clustered tightly on a Pearson correlation heat map as compared with non-T2DM iLTS-scar fibroblasts. Levels of itaconate were elevated in T2DM iLTS-scar fibroblasts. Flow cytometry demonstrated that T2DM iLTS-scar fibroblasts were associated with higher CD90 expression (Thy-1; mean, 95%) when compared with non-T2DM iLTS-scar (mean, 83.6%; P = .0109) or normal tracheal fibroblasts (mean, 81.1%; P = .0042).
CONCLUSIONS: Scar-derived fibroblasts from patients with T2DM and iLTS have a metabolically distinct profile. These fibroblasts are characterized by an increase in itaconate, a metabolite related to immune-induced scar remodeling, and can be identified by elevated expression of CD90 (Thy-1) in vitro.

Entities:  

Keywords:  CD34; CD90; FAP; T2DM; Thy-1; fibroblast subsets; laryngotracheal stenosis; myofibroblast; subglottic stenosis; type 2 diabetes mellitus

Mesh:

Year:  2021        PMID: 34126803      PMCID: PMC8671571          DOI: 10.1177/01945998211014790

Source DB:  PubMed          Journal:  Otolaryngol Head Neck Surg        ISSN: 0194-5998            Impact factor:   3.497


  37 in total

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3.  Causes and consequences of adult laryngotracheal stenosis.

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Review 4.  Metabolomics and Isotope Tracing.

Authors:  Cholsoon Jang; Li Chen; Joshua D Rabinowitz
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Journal:  Cell Metab       Date:  2016-06-30       Impact factor: 27.287

6.  Inhibition of glutaminase to reverse fibrosis in iatrogenic laryngotracheal stenosis.

Authors:  Hsiu-Wen Tsai; Kevin M Motz; Dacheng Ding; Ioan Lina; Michael K Murphy; Dimitri Benner; Michael Feeley; Jody Hooper; Alexander T Hillel
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7.  Increased Expression of PD-1 and PD-L1 in Patients With Laryngotracheal Stenosis.

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Authors:  Justin R Shinn; Kyle S Kimura; Benjamin R Campbell; Anne Sun Lowery; Christopher T Wootten; C Gaelyn Garrett; David O Francis; Alexander T Hillel; Liping Du; Jonathan D Casey; E Wesley Ely; Alexander Gelbard
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10.  MetaboAnalyst: a web server for metabolomic data analysis and interpretation.

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Review 2.  Molecular Mechanisms and Physiological Changes behind Benign Tracheal and Subglottic Stenosis in Adults.

Authors:  Alessandro Marchioni; Roberto Tonelli; Alessandro Andreani; Gaia Francesca Cappiello; Matteo Fermi; Fabiana Trentacosti; Ivana Castaniere; Riccardo Fantini; Luca Tabbì; Dario Andrisani; Filippo Gozzi; Giulia Bruzzi; Linda Manicardi; Antonio Moretti; Serena Baroncini; Anna Valeria Samarelli; Massimo Pinelli; Giorgio De Santis; Alessandro Stefani; Daniele Marchioni; Francesco Mattioli; Enrico Clini
Journal:  Int J Mol Sci       Date:  2022-02-22       Impact factor: 5.923

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