2013
DOI: 10.1165/rcmb.2012-0349rt
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Humoral Immunity and the Development of Obliterative Bronchiolitis after Lung Transplantation

Abstract: Lung transplantation is considered the definitive treatment for many end-stage lung diseases. However, the lung is rejected more commonly than other solid organ allografts. Obliterative bronchiolitis (OB) is the leading cause of chronic allograft dysfunction, and the key reason why the 5-year survival of lung transplant recipients is only 50%. The pathophysiology of OB is incompletely understood. Although a clear role for the immune response to donor antigens has been observed (also known as anti-human leukocy… Show more

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Cited by 4 publications
(4 citation statements)
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“…Human lung transplant recipients develop antibodies against col(V), a protein mainly located in the lung interstitium and not ordinarily exposed to the immune system. In the rat lung transplant model, allografts in minor histocompatibility complex-mismatched recipients induce col(V)-specific T and B immunity after transplantation and appear to be an important source of autoantigen that autoantibodies ligate (74). Better understanding of the exact roles of allo-and autoantibodies in AR, like chronic rejection, will clearly benefit from improved modeling and biomarkers that delineate disease phenotypes and also incorporate orthotopic lung transplant mouse models.…”
Section: Armentioning
confidence: 99%
“…Human lung transplant recipients develop antibodies against col(V), a protein mainly located in the lung interstitium and not ordinarily exposed to the immune system. In the rat lung transplant model, allografts in minor histocompatibility complex-mismatched recipients induce col(V)-specific T and B immunity after transplantation and appear to be an important source of autoantigen that autoantibodies ligate (74). Better understanding of the exact roles of allo-and autoantibodies in AR, like chronic rejection, will clearly benefit from improved modeling and biomarkers that delineate disease phenotypes and also incorporate orthotopic lung transplant mouse models.…”
Section: Armentioning
confidence: 99%
“…The use of immunosuppressive drugs in clinical practice has significantly reduced the morbidity of hyperacute and acute rejection in lung transplant recipients. However, the long‐term survival of these patients is often impacted by chronic rejection, which is primarily manifested as BO and affects approximately 50% of recipients within the first 3 years posttransplantation 63 . While immunosuppressants can effectively treat rejection, they may also lead to immunodeficiency and increase the risk of infection.…”
Section: Perspectivesmentioning
confidence: 99%
“…However, the long‐term survival of these patients is often impacted by chronic rejection, which is primarily manifested as BO and affects approximately 50% of recipients within the first 3 years posttransplantation. 63 While immunosuppressants can effectively treat rejection, they may also lead to immunodeficiency and increase the risk of infection. Thus, achieving a balance between immune defense and immune tolerance is crucial for long‐term survival.…”
Section: Perspectivesmentioning
confidence: 99%
“…Trigger events likely include T-cell-mediated ACR, CARV infections with lower respiratory tract tropism (such as respiratory syncytial virus), certain coronavirus infections, bacterial infections (such as P. aeruginosa, mycoplasma, and chlamydia) and inflammation from aspiration of gastric contents [112]. The possibility of autoimmunity to cryptic self-antigens liberated by these triggers is supported by the presence of self-antigens in microvesicles and the development of autoantibodies against Type V collagen and K-α1 tubulin [113,114]. Novel therapies will need to embrace these concepts to successfully prevent tissue damage and modify aberrant repair.…”
Section: Hypothesis-driven Novel Approachesmentioning
confidence: 99%