Interstitial Lung Diseases Clinical Trial
Idiopathic pulmonary fibrosis (IPF) is a highly heterogeneous and lethal pathological
process with limited therapeutic options, which is the most common and severe of the
idiopathic interstitial pneumonias (IIPs). During the past 20 years, the incidence of IPF
increased significantly. Most of IPF patients show a median survival time of 2-3 years after
diagnosis. Five-year survival rate is 30%-50%. It's difficult to diagnose in the early stage
of IPF. Once the patients go to hospital, it's already in the late stage. Now there is no
effective therapy except lung transplant for IPF in clinical application.
Acute exacerbation of idiopathic pulmonary fibrosis (AE-IPF) is a fatal condition with high
mortality (over 80%). Its etiology and pathogenesis remain unknown. There is a lack of
effective treatment for it. Based on the investigators' long-term clinical observation, most
cases of AE-IPF initially got "common cold" and had coryza, more cough, nasal
obstruction,rhinorrhea, sore throat, some patients had fever, headache, and etc. Some of
these patients' condition developed very rapidly and then became very severe similar to the
situation of acute respiratory distress syndrome (ARDS). Why these AE-IPF patients were so
hypersensitive to "cold"? What were the immunologic and pathological mechanisms of their
lung lesions after patients exposed to "common cold"? How to effectively offer
interventional treatment for AE-IPF? All the above questions are yet to be explained
clearly.
In the investigators' previous retrospective study, the investigators found that there were
some obviously imbalanced immune responses in IPF patients, including increased cluster of
differentiation 4 (CD4) T cell population, immunoglobulin and complements. The investigators
also found highly expressed inflammatory cytokines (IL-17, MIG and IL-9) and high detection
rates of pathogens in AE-IPF patients, especially serum immunoglobulin M (IgM) antibody of
some respiratory virus. These findings provide a strong suggestion that there are some
imbalance of immunologic function in IPF and there are relationship between AE-IPF and
infection, especially "Cold" virus infection might be a key trigger for AE-IPF.
IPF has become the focus of study in the area of pulmonary fibrosis, accounting for over 25%
of all interstitial lung diseases (ILD) 1 and over 60% of all idiopathic interstitial
pneumonia (IIP). The past 20 years have observed the remarkable tendency of increase of IPF
incidence, accompanied by only 2-3 years of medium survival after diagnosis and 30-50% of
5-year survival2. Due to limited diagnosis method at early stage of the disease, the
patients are most likely diagnosed only when they reach middle or late stage. Other issue is
lack of effective treatment, except for lung transplantation. Most of the deaths are caused
by acute exacerbation, which is defined by clinicians as acute exacerbation of IPF (AE-IPF)
and characterized by the rapid deterioration during relatively stable period of IPF
(Stable-IPF). Exacerbation may occur at all stages of IPF development (see the below figure)
and is accompanied by hazardous and quick development, high mortality and very poor
prognosis.
The incidence and mortality of AE-IPF varies in different studies. Kubo etc. reported that
acute exacerbation occurs within 3 years in around 57% of IPF patients, with the mortality
of 53%. Study by Kim etc. show that the mortality of AE-IPF reaches 78%. Study by Song
etc.demonstrated that the incidence of acute exacerbation of IPF is 35.4%, with over 50% of
in-hospital morality, 56% of 1-year mortality and 18.4% of 3-year mortality. Other studies
showed that 1-year post-exacerbation mortality is nearly 100%. Data based on the 178
in-hospital IPF patients in the investigators' department during the latest 4 years showed
that 58% (102/178) of those patients experienced acute exacerbation at certain stage of
disease, with 70 deaths occurred. Among those deaths, 56 cases (83%) were caused by acute
exacerbation. It is clear that the high incidence and mortality of AE-IPF is the most
essential factors impacting the survival and quality of life of IPF patients, therefore lead
to the poor prognosis of IPF.
Hypothesis and key scientific questions Based on analysis above, the investigators propose
the following hypothesis: certain level of immunological imbalance exists in those
relatively stable IPF patients, making them susceptible to infection by various pathogens.
Once infected, especially by viruses (e.g. common cold related viruses), AE-IPF can be
quickly triggered, leading to ARDS-like reaction. To validate this hypothesis, four key
scientific questions need to be answered by studies with scrupulous design: 1) what are the
characteristic changes of immunological function in IPF/AE-IPF patients so as to make the
patients more susceptible to common cold viruses? 2) What kind of pathogens, especially
those common cold viruses, are the key triggering factors during the development of AE-IPF?
3) What kind of inflammatory cascade reaction occurs in AE-IPF leading to ARDS-like prompt
development of pulmonary inflammation? Key research direction and scientific rationale In
order to address the key scientific questions above, the investigators will conduct
comprehensive studies based on detailed screen and analysis of large amount of clinical
cases, integrated research methods in such areas as immunology, molecular, cytology and
animal model, as well as high throughput data collection and big data analysis: 1) Extensive
screening and identification of those pathogens closely related with AE-IPF; 2)
Comprehensive analysis of the change of immunology function, focusing on the
pathological-physiological alteration in virus induced immunologic imbalance in IPF, as well
as the characteristic changes in relevant cytological signal transduction, so as to identify
important AE-IPF bio-markers and explain the pathological molecular mechanism and network of
ARDS-like inflammatory cascade reaction, which will be significant efforts in terms of
prevention of AE-IPF, reduction of mortality, improvement of quality of life, delaying of
disease progression and increase of survival.
Similar clinical deterioration like AE-IPF will also occur in almost all the other types of
pulmonary fibrosis, especially connective tissue disease-ILD (CTD-ILD), nonspecific
interstitial pneumonia (NSIP), drug induced ILD, fibrotic allergic pneumonia and cryptogenic
organizing pneumonia (COP) etc. Therefore, this program will also provide insight into the
basic research and clinical management of acute exacerbation of other interstitial lung
diseases, which is one common problem extensively exists in the area of interstitial lung
disease and the key factor in terms of improving patients' quality of life and survival.
;
Observational Model: Case Control, Time Perspective: Retrospective
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