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Clinical Trials/NCT02729220
NCT02729220
Completed
Not Applicable

Respiratory and Cardiovascular Effects in COPD - Report From a Bronchoscopy Investigation Based on the Obstructive Lung Disease In the Northern Sweden (OLIN) Studies

Dr Annelie F Behndig, MD PhD1 site in 1 country52 target enrollmentJanuary 2012

Overview

Phase
Not Applicable
Intervention
Not specified
Conditions
Pulmonary Disease, Chronic Obstructive
Sponsor
Dr Annelie F Behndig, MD PhD
Enrollment
52
Locations
1
Primary Endpoint
Matrix metalloproteinase 12 (MMP12) and the inhibitor TIMP1
Status
Completed
Last Updated
10 years ago

Overview

Brief Summary

The purpose of this study is to find out if subjects with chronic obstructive pulmonary disease have signs of accelerated ageing in their airways.

Detailed Description

The age-related impairment of innate immunity and antioxidant defenses likely impacts on development and disease progression of chronic obstructive pulmonary disease, COPD. It has been suggested that aging-related declines in function are accelerated in COPD due to recurrent cycles of inflammation, tissue injury and repair, associated with long-term exposure to cigarette smoke or other airway irritants. Here, the investigators aim to follow up on previous observations of impaired antioxidant responses in the lung of COPD patients, to establish the extent to which this reflects an accelerated aging phenotype, to characterize the molecular mechanisms resulting in this functional deficiency. The proposed studies will employ well-characterized patients with COPD of varying severity and smoking habits, as well as carefully age and smoking history-matched controls. Accelerated aging within the COPD lung will be assessed in endobronchial mucosal biopsies and airway macrophages by assessment of established senescence markers using immunohistochemical, biochemical and PCR-based methods. These markers of tissue age will then be related to the functional activation of transcription factors, known to be induced by oxidative stress and related to cytoprotection such as Nrf2 and AP1. The investigators will also examine whether COPD is associated with an enhanced secretion of inflammatory mediators from senescent cells, consistent with the accelerated aging paradigm and establish how this influences cell function. Deficiencies in metal handling, antioxidant defenses and diminished airway innate immune defenses at the air-lung interface will be assessed. The aim is to identify biomarkers for the risk of rapid lung function deterioration in COPD patients.

Registry
clinicaltrials.gov
Start Date
January 2012
End Date
December 2014
Last Updated
10 years ago
Study Type
Interventional
Study Design
Parallel
Sex
All

Investigators

Sponsor
Dr Annelie F Behndig, MD PhD
Responsible Party
Sponsor Investigator
Principal Investigator

Dr Annelie F Behndig, MD PhD

Investigator

University Hospital, Umeå

Eligibility Criteria

Inclusion Criteria

  • Clinical diagnosis of COPD, GOLD stage 2-
  • Smoking history of at least 10 packyears.

Exclusion Criteria

  • Severe ischemic heart disease.
  • Other severe disease.
  • Respiratory infection within four weeks.

Outcomes

Primary Outcomes

Matrix metalloproteinase 12 (MMP12) and the inhibitor TIMP1

Time Frame: Baseline

Airway lavages collected by bronchoscopy and serum will be analysed for MMP and TIMP using ELISAs.

Levels of oxidized proteins, 4 HNE

Time Frame: Baseline

The accumulation of oxidized proteins, 4-Hydroxynonenal, will be assessed in bronchial biopsies.

Antioxidant-related transcription factor Nrf2

Time Frame: Baseline

Nuclear factor (erythroid-derived 2)-like 2 (Nrf2) is a transcription factor known to be induced by oxidative stress and related to cytoprotection.

Cellular senescence marker - Ki67

Time Frame: Baseline

Endobronchial mucosal biopsies collected by bronchoscopy. Immunohistochemistry for the cellular senescence markers Ki67 will be performed.

Secondary Outcomes

  • Lymphocyte subsets in bronchoalveolar lavage(Baseline)
  • Arterial stiffness(Baseline)
  • Metals in airway lavages(Baseline)

Study Sites (1)

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