Description Module
The Description Module contains narrative descriptions of the clinical trial, including a brief summary and detailed description. These descriptions provide important information about the study's purpose, methodology, and key details in language accessible to both researchers and the general public.
Description Module path is as follows:
Study -> Protocol Section -> Description Module
Description Module
Ignite Creation Date:
2025-12-25 @ 1:41 AM
Ignite Modification Date:
2025-12-25 @ 1:41 AM
NCT ID:
NCT00864994
Brief Summary:
There is increasing evidence in the literature that COPD should not be considered as a localised pulmonary disorder but as a systemic disease involving pathology in several extra pulmonary tissues. Well characterized systemic features are a chronic low grade systemic inflammation, altered body composition and a skeletal muscle fibre type shift. There are indications that an absolute or relative increase of fat mass puts COPD patients at increased risk for cardiovascular pathology while muscle atrophy is associated with a high prevalence of osteoporosis and with impaired physical function. The origin of systemic inflammation is poorly understood. Both endogenous and exogenous risk factors contribute to systemic inflammation and extra-pulmonary manifestations of COPD.
Overall objective of study 3:
To compare the pattern and severity of the systemic inflammatory profile in relation to skeletal muscle weakness and cardiovascular risk profile in COPD patients with mild to moderate disease compared to non-susceptible smokers.
Specific objectives:
1. To study the relative contribution of pulmonary and extra pulmonary factors on exercise capacity, skeletal muscle function and health status
2. To relate diet, physical activity and cardiovascular risk factors to body composition, skeletal muscle function and exercise capacity status
3. To study the influence of the emphysema phenotype on extra pulmonary pathology in COPD
4. To study muscle fibre type size and composition and to relate muscle oxidative phenotype with insulin sensitivity, inflammation (local and systemic) and molecular signatures of oxidative energy and protein metabolism.
Study design:
Cross-sectional study. Healthy smoking subjects and COPD patients will undergo extensive clinical, metabolic and inflammatory assessment at the university clinics in Groningen, Maastricht and CIRO Horn.
Study population:
Totally 60 subjects will be included
* 30 healthy subjects who after 20 pack years smoking have no signs of COPD (age 40-75 years)
* 30 COPD patients with GOLD stage II (age 40-75 years)
Detailed Description:
Primary study parameters/outcome of the study:
1. Smoking history and behaviour, diet and physical activity level assessed by questionnaire
2. Extensive lung function and CT scanning of the lung, ECG
3. Candidate genes for muscle dysfunction and CVD risk
4. Body composition (BIA, waist-hip ratio, DEXA-scan)
5. Systemic inflammation
6. Advanced Glycosylated Endproduct (AGE)
7. Glucose tolerance test
8. Risk factors of metabolic syndrome
9. 6 minute walking distance
10. Handgrip strength
11. Skeletal muscle function by isokinetic dynamometry
12. Physical activity level and pattern by accelerometry
13. Muscle oxidative phenotype, fibre cross-sectional area and molecular signatures obtained in vastus lateralis muscle biopsies before and after incremental cycle ergometry
Nature and extent of the burden and risks associated with participation, benefit and group relatedness (if applicable):
* Totally 22 hours will be spend in the hospital during 3 visits
* CT-scanning of the lung is associated with a radiation burden of 0.8-1.6 mSv (dependent of body weight)
* 50 ml peripheral blood (v. cubiti)
* Muscle biopsy may be associated with temporary pain and haematoma
* Drawing of arterial blood from the radial artery rarely leads to bleeding and transitory nerve damage (numb feeling in wrist/hand area).
Study:
NCT00864994
Study Brief:
Protocol Section:
NCT00864994