4.7 Article

Adenosine deaminase modulates metabolic remodeling and orchestrates joint destruction in rheumatoid arthritis

SCIENTIFIC REPORTS (2021)

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Journal

SCIENTIFIC REPORTS
Volume 11, Issue 1, Pages -

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41598-021-94607-5

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Multidisciplinary Sciences

Funding

  1. Administration of Sri Sathya Sai Institute of Higher Learning
  2. Department of Biosciences, Sri Sathya Sai Institute of Higher Learning, Prasanthi Nilayam, Anantapur, India
  3. University Grants Commission, Basic Scientific Research, New Delhi, India [F.4-1/2006 (BSR)/7-164/2007 (BSR)]
  4. Council of Scientific and Industrial Research, New Delhi, India [CSIR-UGC-NET-2121530422]
  5. Department of Biotechnology (DBT) Project, New Delhi, India [BT/PR8226/BRB/10/1224/2013]
  6. Department of Science and Technology (DST), New Delhi, India [EMR/2017/005381]
  7. Department of Science and Technology (DST)-FIST, New Delhi, India [SR/FST/LSI-616/2014]
  8. Department of Biotechnology-Bioinformatics (DBT-BIF) Facility, New Delhi, India [BT/BI/25/063/2012]
  9. University Grants Commission (UGC)-special assistance program (SAP), New Delhi, India [UGC-SAP III: F.3-19/2018/DRS-III(SAP-II)]

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The study shows that different levels of adenosine deaminase (ADA), an arthritis-associated factor, can lead to varying cytokine levels and metabolic characteristics in rheumatoid arthritis (RA) patients. ADA may play a crucial role in the pathophysiology of RA joints, serving as a potential biomarker and therapeutic target for RA patients.
Rheumatoid Arthritis (RA) is a chronic autoimmune disease associated with inflammation and joint remodeling. Adenosine deaminase (ADA), a risk factor in RA, degrades adenosine, an anti-inflammatory molecule, resulting in an inflammatory bias. We present an integrative analysis of clinical data, cytokines, serum metabolomics in RA patients and mechanistic studies on ADA-mediated effects on in vitro cell culture models. ADA activity differentiated patients into low and high ADA sets. The levels of the cytokines TNF alpha, IFN gamma, IL-10, TGF beta and sRANKL were elevated in RA and more pronounced in high ADA sets. Serum metabolomic analysis shows altered metabolic pathways in RA which were distinct between low and high ADA sets. Comparative analysis with previous studies shows similar pathways are modulated by DMARDs and biologics. Random forest analysis distinguished RA from control by methyl-histidine and hydroxyisocaproic acid, while hexose-phosphate and fructose-6-phosphate distinguished high ADA from low ADA. The deregulated metabolic pathways of High ADA datasets significantly overlapped with high ADA expressing PBMCs GEO transcriptomics dataset. ADA induced the death of chondrocytes, synoviocyte proliferation, both inflammation in macrophages and their differentiation into osteoclasts and impaired differentiation of mesenchymal stem cells to osteoblasts and mineralization. PBMCs expressing elevated ADA had increased expression of cytokines and P2 receptors compared to synovial macrophages which has low expression of ADA. Our data demonstrates increased cytokine levels and distinct metabolic signatures of RA based on the ADA activity, suggests an important role for ADA in the pathophysiology of RA joints and as a potential marker and therapeutic target in RA patients.

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