Collagen VI Is Upregulated in COPD and Serves Both as an Adhesive Target and a Bactericidal Barrier for &lt;b&gt;&lt;i&gt;Moraxella catarrhalis&lt;/i&gt;&lt;/b&gt;

Abdillahi, Suado M; Bober, Marta; Nordin, Sara L.; Hällgren, Oskar; Baumgarten, Maria; Erjefält, Jonas; Westergren‐Thorsson, Gunilla; Bjermer, Leif; Riesbeck, Kristian; Egesten, Arne; Mörgelin, Matthias

doi:10.1159/000381213

Cited by 32 publications

(44 citation statements)

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“…50 Collagen VI has a unique set of characteristics that includes roles in a plethora of signalling pathways such as for apoptosis, proliferation, inflammation and fibrosis as well as a role in innate immunity with antibacterial activity. 51,52 Collagen VI is not a common fibrillar collagen, but forms a network of thin fibres anchoring collagens types I and III to the reticular basement membrane, and has been found to be increased in idiopathic pulmonary fibrosis and suggested as a biomarker for hepatic fibrosis. 34,53,54 Collagen VI may also counteract apoptosis and alter lung elasticity.…”

Section: Discussionmentioning

confidence: 99%

Uncontrolled asthmatics have increased FceRI⁺ and TGF‐β–positive MC_TC mast cells and collagen VI in the alveolar parenchyma

Andersson

Weitoft

Rydell‐Törmänen

et al. 2018

Clin Experimental Allergy

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Summary Background Asthma has been associated with increased collagen deposition in both conducting airways and alveolar parenchyma. Mast cells (MCs) are key effector cells in asthma and have the ability to affect collagen synthesis. However, the link between clinical control and changes in bronchial and alveolar MC phenotypes and specific collagens in controlled and uncontrolled asthma remains unknown. Objective To investigate MC phenotypes in correlation with deposition of specific collagen subtypes in patients with controlled and uncontrolled asthma as well as to healthy controls. Methods The tissue expression of IgE+, FcεRI+ and TGF‐β+ MCs, as well as immunoreactivity of collagen I, III and VI, was assessed using immunohistochemistry on bronchial and transbronchial biopsies from controlled asthmatics (n = 9), uncontrolled asthmatics (n = 16) and healthy controls (n = 8). Results In the alveolar parenchyma, the total number of MCs, as well as the number of FcεRI+ MCs and pro‐fibrotic TGF‐β+ MCTC, was significantly increased in uncontrolled asthma compared to both controlled asthma and healthy controls. The proportion of TGF‐β+ MCTC correlated positively to an increased immunoreactivity of alveolar collagen VI but not collagen I and III. Collagen VI was increased in the alveolar parenchyma of uncontrolled asthmatics compared to controlled asthmatics. Controlled asthmatics had an increased deposition of alveolar collagen I. In bronchi, the immunoreactivity of collagen I was increased in both controlled and uncontrolled asthmatics while collagen III was increased only in controlled asthmatics. Conclusions Patients with uncontrolled atopic asthma have an altered pro‐fibrotic MCTC phenotype in the alveolar parenchyma that is associated with alveolar collagen VI. The present data thus support distal lung mast cell and matrix changes as histopathological features of asthma that may be of particular clinical relevance in patients who have remaining symptoms despite conventional inhaler therapy.

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Section: Discussionmentioning

confidence: 99%

Uncontrolled asthmatics have increased FceRI⁺ and TGF‐β–positive MC_TC mast cells and collagen VI in the alveolar parenchyma

Andersson

Weitoft

Rydell‐Törmänen

et al. 2018

Clin Experimental Allergy

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“…The same applies for the Chemistry Prize. Electron microscopy is an essential tool when studying innate immunity [6,7,8,9,10,11]. It will therefore be exciting to see how the new developments will advance the forthcoming research outcome.…”

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confidence: 99%

Bystander Cells Taking Action

Herwald

Egesten

2017

J Innate Immun

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“…In a series of elegant experiments the authors show that this effect relies on the PERK-dependent activation of p38 and ERK, and ATF6-mediated basal expression of p38. ER stress is also part of the pathology of chronic obstructive pulmonary disease (COPD) [7] and thus their findings may help to explain why antimicrobial agents such as collagen IV can be upregulated in lung tissue, as observed in biopsies and fibroblasts from COPD patients [8]. …”

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confidence: 99%

On PAMPs and DAMPs

Herwald¹,

Egesten

2016

J Innate Immun

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Collagen VI Is Upregulated in COPD and Serves Both as an Adhesive Target and a Bactericidal Barrier for <b><i>Moraxella catarrhalis</i></b>

Cited by 32 publications

References 32 publications

Uncontrolled asthmatics have increased FceRI⁺ and TGF‐β–positive MC_TC mast cells and collagen VI in the alveolar parenchyma

Uncontrolled asthmatics have increased FceRI⁺ and TGF‐β–positive MC_TC mast cells and collagen VI in the alveolar parenchyma

Bystander Cells Taking Action

On PAMPs and DAMPs

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Collagen VI Is Upregulated in COPD and Serves Both as an Adhesive Target and a Bactericidal Barrier for <b><i>Moraxella catarrhalis</i></b>

Cited by 32 publications

References 32 publications

Uncontrolled asthmatics have increased FceRI+ and TGF‐β–positive MCTC mast cells and collagen VI in the alveolar parenchyma

Uncontrolled asthmatics have increased FceRI+ and TGF‐β–positive MCTC mast cells and collagen VI in the alveolar parenchyma

Bystander Cells Taking Action

On PAMPs and DAMPs

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Uncontrolled asthmatics have increased FceRI⁺ and TGF‐β–positive MC_TC mast cells and collagen VI in the alveolar parenchyma

Uncontrolled asthmatics have increased FceRI⁺ and TGF‐β–positive MC_TC mast cells and collagen VI in the alveolar parenchyma