Integration of metabolome, transcriptome and microbiome data to differentiate between chronic hypersensitivity pneumonitis and idiopathic pulmonary fibrosis
Implementing Organization
Indian Institute of Technology (IIT)
Principal Investigator
Prof. Koel Chaudhury
Indian Institute Of Technology (IIT) Kharagpur, West Bengal
CO-Principal Investigator
Dr. Ritobrata Goswami
Indian Institute of Technology (IIT)
CO-Principal Investigator
Dr. Riddhiman Dhar
Indian Institute of Technology (IIT)
CO-Principal Investigator
Dr. Karan Madan
All India Institute of Medical Sciences
About
Interstitial lung disease (ILD) encompasses about 300 parenchymal pulmonary disorders caused by inflammation and/or fibrosis in the lung interstitium. Pulmonary fibrosis is a hallmark of various ILDs, including hypersensitivity pneumonitis (HP), which is characterized by lung inflammation and immunological reaction when exposed to a particular antigen. Chronic HP can be fibrotic or non-fibrotic, while Idiopathic pulmonary fibrosis (IPF) is another aggressive type characterized by progressive lung function decline and early mortality. Diagnosis of fibrotic cHP and IPF is critical, as therapeutic management varies between these two subtypes. Identifying robust and reproducible biomarkers for distinguishing between fibrosing ILDs is essential for accurate diagnosis. Bronchoalveolar lavage fluid (BALF) provides a detailed snapshot of the lower respiratory tract in various pulmonary disorders. A recent study using NMR metabolomics indicated dysregulated metabolites in serum, exhaled breath condensate (EBC), and BALF of HP compared to controls. This motivated the study to identify metabolites in BALF that can effectively discriminate between cHP and IPF. Identification of unique microbial signatures in cHP and IPF is envisioned. Integration of these platforms will shed light on the relationship between altered metabolites, DEGs, and unique lung microbiota associated with the subtypes. If the combined expression of these signatures significantly differs between the diseases, tailored therapeutic approaches could be directed towards the specific type of ILD.
Source
Source
Anusandhan National Research Foundation/Science and Engineering Research Board (SERB), DST 2023-24
Science and Engineering Research Board (SERB), New Delhi
Anusandhan National Research Foundation (ANRF)
Quick Information
Area of Research
Life Sciences & Biotechnology
Start Year
2024
End Year
2027
Sanction Amount
₹ 43.14 L
Status
Ongoing
Contact
koel@smst.iitkgp.ac.in
Output
No. of Research Paper
00
Technologies (If Any)
00
No. of PhD Produced
00
No. of Patents
Filed :00
Grant :00
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