AI Article Synopsis

  • * Advanced technologies like digital pathology, AI, and graft transcriptomics are being explored to enhance diagnosis and stratify risks for graft failure using donor-derived cell-free DNA.
  • * Innovative therapies and combined strategies, such as targeting the complement cascade and immune cell depletion, aim to improve outcomes for lung transplant recipients, especially those at higher risk of humoral responses.

Article Abstract

Humoral immunity is a major waypoint towards chronic allograft dysfunction in lung transplantation (LT) recipients. Though allo-immunization and antibody-mediated rejection (AMR) are well-known entities, some diagnostic gaps need to be addressed. Morphological analysis could be enhanced by digital pathology and artificial intelligence-based companion tools. Graft transcriptomics can help to identify graft failure phenotypes or endotypes. Donor-derived cell free DNA is being evaluated for graft-loss risk stratification and tailored surveillance. Preventative therapies should be tailored according to risk. The donor pool can be enlarged for candidates with HLA sensitization, with strategies combining plasma exchange, intravenous immunoglobulin and immune cell depletion, or with emerging or innovative therapies such as imlifidase or immunoadsorption. In cases of insufficient pre-transplant desensitization, the effects of antibodies on the allograft can be prevented by targeting the complement cascade, although evidence for this strategy in LT is limited. In LT recipients with a humoral response, strategies are combined, including depletion of immune cells (plasmapheresis or immunoadsorption), inhibition of immune pathways, or modulation of the inflammatory cascade, which can be achieved with photopheresis. Altogether, these innovative techniques offer promising perspectives for LT recipients and shape the 21st century's armamentarium against AMR.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC11336419PMC
http://dx.doi.org/10.3389/ti.2024.12973DOI Listing

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