Indirect Allorecognition of Mismatched Donor HLA Class II Peptides in Lung Transplant Recipients with Bronchiolitis Obliterans Syndrome

Reznik, Scott I.; Jaramillo, Andrés; Sivasai, K. S. R.; Womer, Karl L.; Sayegh, Mohamed H.; Trulock, Elbert P.; Patterson, G. Alexander; Mohanakumar, Thalachallour

doi:10.1034/j.1600-6143.2001.001003228.x

Cited by 75 publications

(75 citation statements)

References 47 publications

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“…Although the exact role of CD30 in the pathogenesis of BOS is unknown, alloimmune response is considered as a major contributor in the immuno-pathogenesis of BOS (5,16,17). We have shown that BOS+ patients develop early post-transplant inflammation which may activate allo-as well as auto-immunity (18).…”

Section: Discussionmentioning

confidence: 90%

“…BOS is histologically characterized by cellular infiltration, fibrosis, collagen deposition and occlusion of small airways in the allograft (4). The role of T cell immunity in the pathogenesis of chronic lung allograft rejection both in clinical lung transplantation and in animal models of obliterative airway diseases has been well established (5,6). Therefore, it is reasonable to predict that sCD30 which is a marker for T cell activation may increase during rejection of the allograft.…”

Section: Introductionmentioning

confidence: 99%

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Soluble CD30 levels as a diagnostic marker for bronchiolitis obliterans syndrome following human lung transplantation

Golocheikine

Saini

Ramachandran

et al. 2008

Transplant Immunology

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The long term survival of human lung allograft is hampered by the occurrence of chronic rejection, Bronchiolitis Obliterans Syndrome (BOS). This end-stage disease is normally diagnosed clinically by using the pulmonary function tests. This results in delay of BOS diagnosis and consequently prevents early intervention. It is generally accepted that alloimmunity plays an important role in chronic rejection of the allograft. In this study we analyzed serial serum samples from BOS+ and BOS− patients for sCD30 levels to determine the role of sCD30 to predict the onset of BOS. In contrast to BOS negative patients and normal subjects, 6 out of 9 BOS+ patients (P<0.05) studied had an increase in the sCD30 levels. Significantly, the rise was noted 7.57 ±2.63 months before the clinical diagnosis was evident. Therefore, we propose that the rise in serum sCD30 levels can be used as a marker for the detection of patients who are at risk of development of BOS.

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Section: Discussionmentioning

confidence: 90%

Section: Introductionmentioning

confidence: 99%

Soluble CD30 levels as a diagnostic marker for bronchiolitis obliterans syndrome following human lung transplantation

Golocheikine

Saini

Ramachandran

et al. 2008

Transplant Immunology

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“…[51][52][53][54] Nonetheless, a gap exists between our understanding of how T cells are activated through the indirect pathway and how such activated T cells predominantly induce chronic pathology. The results presented in this report provide a potential explanation to bridge this gap.…”

Section: Discussionmentioning

confidence: 99%

Antigen Location Contributes to the Pathological Features of a Transplanted Heart Graft

Chen

Demir

Valujskikh

et al. 2004

The American Journal of Pathology

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Organ-specific injury after transplantation presents with a variety of clinical and pathological phenotypes, yet the factors influencing development of each outcome are poorly understood. Because primed T lymphocytes must re-encounter their antigen within the target organ to engage effector functions, we postulated that the cellular location of antigen within that organ could significantly impact the induced pathology. We challenged female Marilyn CD4 T-cell receptor transgenic mice, in which all T cells are specific for the male minor transplantation antigen, with male heart transplants expressing the rel- Naïve T lymphocytes are activated in secondary lymphoid organs in response to their specific antigens when such antigens are expressed on professional antigenpresenting cells (APCs) and in the context of appropriate co-stimulatory signals.

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“…In this regard, one important point is that over time after organ transplantation, T cells may recognize different epitopes of donor antigens in the same individuals, a process called epitope spreading. This phenomenon has been described in renal (39), cardiac (40), and lung transplant recipients (41). This process has been implicated as a mechanism for continual recruitment of naïve alloreactive T cells, which may contribute toward acute and chronic rejection.…”

Section: Antigen-specific Assays For Monitoring Transplantation Immunmentioning

confidence: 94%

How Can We Measure Immunologic Tolerance in Humans?

Najafian

Albin²,

Newell³

2006

Journal of the American Society of Nephrology

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Prevention and treatment of allograft rejection in organ transplant recipients relies primarily on non-antigen-specific immunosuppression, with all its associated potential hazards and costs. Currently, the status of the recipient immune response is measured by monitoring pharmacologic drug levels and clinical/pathologic evaluation of graft function. Development of reliable assays that can measure accurately the status of the immune response not only would help clinicians customize the prescription of immunosuppressive drugs in individual patients but also may allow their complete withdrawal in some patients with immunologic tolerance. Furthermore, these assays would facilitate the safe evaluation of novel tolerogenic regimens. Achieving this goal has proved to be very difficult because it requires both a more in-depth understanding of complex mechanisms of tolerance and also identification of transplant patients with acquired tolerance to an allograft that can be studied. This review discusses the current understanding of tolerance mechanisms and outlines the unique and specific challenges in development of tolerance/monitoring assays in the field of transplantation. In addition, several of the most promising candidate assays are discussed in detail.

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Indirect Allorecognition of Mismatched Donor HLA Class II Peptides in Lung Transplant Recipients with Bronchiolitis Obliterans Syndrome

Cited by 75 publications

References 47 publications

Soluble CD30 levels as a diagnostic marker for bronchiolitis obliterans syndrome following human lung transplantation

Soluble CD30 levels as a diagnostic marker for bronchiolitis obliterans syndrome following human lung transplantation

Antigen Location Contributes to the Pathological Features of a Transplanted Heart Graft

How Can We Measure Immunologic Tolerance in Humans?

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