COPD Clinical Trial
Official title:
The Mechanisms of Inflammation and Immunity in COPD and Their Relationship to Exacerbations and Disease Progression.
The UK Medical Research Council (MRC) together with the Association of British Pharmaceutical Industries (ABPI) have recently funded a program designed to foster collaboration between academic COPD researchers and the pharmaceutical industry in the UK, with the aim of developing and furthering our research capacity and expertise for the benefit of patients living with this prevalent and disabling condition. This builds on the strong international track record of COPD research in the UK. The program is divided into four work packages (WP1-4), each with specific aims. WP1 will collate and establish data from patient cohorts and share this information through the development of knowledge management platforms. WP2 will specifically assess how airway micro-organisms impact on COPD and how the effects of bacteria and viruses may be modified. WP3 is concerned with tissue injury and repair which are fundamental processes in the development of COPD. WP4 will examine in detail the potential for improving patient outcomes by targeting the skeletal muscle dysfunction that can profoundly affect exercise capacity.
This study is a multi-centre UK based observational study of a cohort of patients with
chronic obstructive pulmonary disease (COPD) funded by the MRC, as part of the MRC/ABPI
Inflammation and Immunology Initiative in COPD. This consortium brings together key
researchers in the COPD research community with long-standing expertise in understanding
bacterial infection, inflammation and immunity.
Understanding the role of bacterial and viral infections, which are often the trigger for
exacerbations, and the mechanism of tissue re-modelling and repair following exacerbations
is extremely important. Exacerbations and the progression of the disease impose a
considerable disability on patients and a financial burden on the health service. In
additional, pulmonary inflammation in COPD may result in systemic inflammation. This is
associated skeletal muscle dysfunction, as well as worsening other common diseases, such as
cardiovascular disease.
We now have a much better understanding of the cellular and molecular mechanisms that
underlie COPD and cause the chronic inflammatory process, both locally within the lung and
systemically. However, current therapy for COPD is inadequate and relies on long-acting
bronchodilators, which do not ameliorate the underlying chronic inflammatory process.
Currently available anti-inflammatory therapies are incompletely effective. An improved
understanding of the complex mechanisms in COPD is required in order to develop future
effective treatments, for which there is a pressing need.
Patients will be recruited from existing cohorts of COPD patients, and indirectly through
their general practitioner and outpatient clinics. Patients must have COPD, and all patients
will be assessed to ensure the correct diagnosis.
Study patients will be phenotyped by lung morphology and function, biomarkers in blood,
sputum and urine, bacterial and viral load in sputum, cardiovascular behaviour,
co-morbidities and skeletal muscle function. The patients will be followed up over initially
18 months, with a planned extension to 5 years, to accurately determine the relationship
between bacterial and viral infections, tissue re-modelling and skeletal muscle dysfunction
with exacerbation frequency and disease progression.
Patients will be phenotyped by:
1. Chest CT-Scan for quantitative measures of lung morphology at baseline
2. ECG and blood pressure to assess cardiovascular risk conferred by systemic inflammation
4)Biomarkers of infection, inflammation and cardiovascular disease in blood, sputum (both
spontaneously produced and induced) and urine 5)Quality of life, respiratory symptoms,
fatigue, depression, history of cigarette smoking, housing, contact with children and pets
and daily activity will be assessed by questionnaire 6)A 6 minute walk test and 4 meter gait
speed to determine exercise tolerance and disability 7)Lung function using a spirometer and
whole body plethymograph 8)Arterialised blood gases using ear-lobe blood gas analysis
9)Bioimpedance for assessing blood flow and body composition 10)Isometric Muscle strength
using quadriceps strain gauge
Patients will be asked to complete a daily diary card on which they will record an increase
in two respiratory symptoms, from which we will identify exacerbations, based on our
validated criteria of two consecutive days with increase in two symptoms that must include
either dyspnoea, sputum purulence or sputum volume. Patients unable to complete the diary
cards will be judged incapable of taking part in the research. All patients will provide
informed, written consent. Patients will be seen at enrollment, every 6 months thereafter
for baseline measurements, at exacerbation and at week 2 and 6 post exacerbation to monitor
their recovery.
All patients will undergo a baseline CT scan, at full suspended inspiration with the
smallest field of view that includes both lungs. The maximum dose of radiation that each
patient with receive from the CT scan is estimated at 2 milli-Sieverts. This is equivalent
to about 100 front chest X rays. This compares to an average exposure of 2 milli-Sieverts
per year from naturally occurring radioactive material (background radiation). Patients may
benefit from detection of previously unknown lung carcinoma and lung abnormalities. At
exacerbation visits, some patients may require a chest X-ray as part of standard clinical
emergency care e.g. to exclude a pneumothorax or detect pneumonia. The estimated dose of
radiation per plain chest X-ray is 0.02 milli-Sieverts.
Blood tests will only be taken by trained personnel. The blood will be analysed for routine
haematological parameters, and other body chemicals that might be linked to COPD, ischaemic
heart disease and other co-morbridities. The volume of blood taken should not cause any
anaemia and routine blood counts will be made to monitor haemoglobin levels.
Both spontaneous and induced sputum specimens will be taken. The induced sputum may cause
coughing and some shortness of breath. Patients will be closely monitored and their lung
function checked to ensure their safety. We have previously shown that induced sputum
sampling is a safe procedure in COPD.
Patients will be asked to walk for 6 minutes and the distance recorded. Patients heart rate
and oxygen saturation will be monitored before and after the walk. Patients may experience
shortness of breath during this test. Supplementary oxygen will be available if the patient
desaturates during the test. Additional assessment of muscle strength and disability will be
carried out using a quadriceps strain gauge, the four meter gait speed test and the short
physical performance battery. The patient should not experience any more dyspnoea than they
would normally encounter in everyday life and the quadriceps strain gauge will only be
performed if there are no underlying musculoskeletal or neurological contra-indications.
Some investigations described above are specific to certain centres collaborating in this
study and not all tests will be performed on all patients. The tests which will be requested
for each individual patient will be fully explained during their initial visit at the
appropriate study site.
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