Idiopathic Pulmonary Fibrosis Clinical Trial
Official title:
The Edinburgh Lung Fibrosis Molecular Endotyping (ELFMEN) Study
To prospectively study novel blood and lung biomarkers of disease activity in patients with IPF and other interstitial lung disease with the aims of prognostic modelling and disease clustering
BACKGROUND
Idiopathic pulmonary fibrosis (IPF) is a progressive form of lung scarring for which there is
no proven treatment. Steroids and other potentially toxic drugs are often used but their
efficacy is uncertain. The management of patients with IPF is particularly complex because
firstly there are a number of closely related fibrosing lung conditions that 'look' like IPF
but in which the prognosis is generally better and which more often respond to steroids and
secondly even within the group of patients with IPF, there is a variability in the rate of
progression so that it is hard to provide individual patients with a reasonable estimate of
prognosis.
Currently the best the investigators can offer patients with IPF or probable IPF is serial
measurement of lung function over time and observation of decline. The uncertainty regarding
disease prognosis and progression in a given patient is hugely unsettling for both the
individual and the clinician. A far more powerful tool would be a measurement or 'biomarker'
of disease activity that one could monitor from the time of diagnosis and throughout the
illness and which predicted for decline in lung function or poor prognosis. This biomarker
(or biomarkers) might include molecules associated with inflammation and scarring in blood or
in lung fluid, new more sensitive measures of lung function (e.g. the six-minute walking
test) or novel non-invasive imaging methods. Once established, a robust biomarker would serve
several important functions including:
1. A means of distinguishing definite IPF from other closely related conditions;
2. Categorisation of individuals with IPF into 'good' and 'poor' prognosis
3. Identifying targets for potential new therapies in IPF
4. A marker of disease response to drugs used in therapeutic trials in IPF.
AIMS To prospectively study novel blood and lung biomarkers of disease activity in
patients with IPF and other interstitial lung disease
STUDY DESIGN Inclusion criteria Patients attending or referred to the Edinburgh Royal
Infirmary and the Western General Hospital lung fibrosis clinics with a diagnosis of
definite or probable idiopathic pulmonary fibrosis. For comparison patients with other
idiopathic interstitial pneumonias, hypersensitivity pneumonitis, asbestosis or
interstitial lung disease associated with connective tissue diseases will also be
recruited since these conditions often have a similar clinical presentation to IPF but a
more variable prognosis. All clinical details for these patients are already being
collated in a REC-approved clinical database (REC 06/S0703/53). Patients aged 18 through
99 years, inclusive.
Exclusion criteria and restrictions Candidates not a suitable for enrolment or unlikely
to comply with the requirements of this study, in the opinion of the investigator, will
be excluded.
The biomarkers will include assays that test the activity of circulating blood
inflammatory cells in laboratory conditions. A relatively large volume of blood (up to
80ml a time) is required to purify sufficient numbers of these inflammatory cells for
use in laboratory studies. It is anticipated however that as data is gathered,
subsequent experiments can be refined such that less blood is required.
No more than 320ml of blood over a 12 month period will be taken from any study
participant for research purposes. No more than 100ml of blood over a twelve month
period will be taken from any study participant with a moderate or severe anaemia,
defined as a haemoglobin >10% below lower limit of normal. Anaemia is not a recognised
complication of idiopathic pulmonary fibrosis.
Participants that are deemed unsuitable for bronchoscopy, based on established national
and local guidelines, will be excluded from this aspect of the study.
WHAT WILL HAPPEN TO THE RESEARCH PARTICIPANTS
* indicates routine clinical investigations performed on all patients with IPF or other
interstitial lung disease
- indicates study investigations, some of which are may performed as part of routine
clinical care
Within 1 month of presentation or recruitment to the study participants will undergo:
*Blood samples for routine biochemistry, haematology, auto-immune screen and other
clinically relevant tests
*Full lung function tests and incremental walking test
*HRCT scan
•Bronchoalveolar lavage (BAL) - note that this may be performed for clinical diagnostic
indications in many patients with suspected IPF.
•Blood sample for biomarkers (average 40ml, not >80ml)
At 3 months following recruitment participants will undergo:
*Blood sample for biomarkers (average 40ml, not >80ml)
At 6 months following recruitment participants will undergo:
- Blood sample for biomarkers (average 40ml, not >80ml)
At 9 months following recruitment participants will undergo:
•Blood sample for biomarkers (average 40ml, not >80ml)
At 12 months following recruitment participants will undergo:
•Bronchoalveolar lavage
•Blood sample for biomarkers (average 40ml, not >80ml)
Thereafter repeated every 6 months for up to 3 years, participants will undergo:
•Blood sample for biomarkers (average 40ml, not >80ml)
In patients that have a lung biopsy for clinical indications, resected lung tissue that
is deemed not critical to the diagnostic process by pathologist i.e. excess fresh
tissue, will be used for research purposes. To ensure this is safely achieved, excess
lung tissue will stored and not used for research until the pathologist has confirmed
that available material is sufficient for clinical purposes. In practice, this means a
sample of fresh tissue form the 'staple' margins of the resected specimen. Formalin
fixed archived tissue from subjects will be included for use in this study. This
protocol was used in a previous ethically approved study (09/S1101/52, Molecular markers
of hypoxia, cell injury and fibrosis in lung tissue. This study ended 31/3/15 having
collected 40 consecutive fresh lung fibrosis specimens without incident.
STUDY OUTCOMES (see endpoints) Identification of prognostics biomarkers in all entities
of ILD including IPF that define disease progression and death Identification of novel
disease entity clusters define by clinical, imaging and molecular features
;
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