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Related Experiment Videos

Acute and chronic rejection.

A Tejani1, L Emmett

  • 1Department of Pediatrics and Surgery, New York Medical College, Valhalla, NY, USA. Atejani@aol.com

Seminars in Nephrology
|September 18, 2001
PubMed
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Graft rejection is driven by T-cell recognition of major histocompatibility complex molecules. While acute rejection decreases with therapy, chronic rejection is rising, impacting long-term renal transplant success, especially in children.

Area of Science:

  • Immunology
  • Transplantation Biology
  • Nephrology

Background:

  • Major histocompatibility complex (MHC) molecules are key antigens in graft rejection.
  • T-cell recognition of alloantigens initiates cellular rejection, with direct and indirect pathways implicated in acute and chronic rejection, respectively.
  • Cytotoxic T-lymphocyte molecules are upregulated in rejecting human renal allografts.

Purpose of the Study:

  • To elucidate the mechanisms of acute and chronic graft rejection.
  • To highlight the differential incidence and trends of acute versus chronic rejection.
  • To emphasize the need for improved strategies for long-term renal transplant outcomes in children.

Main Methods:

  • Analysis of rejecting human renal allograft biopsy tissues.

Related Experiment Videos

  • Review of current concepts in T-cell mediated allorecognition.
  • Examination of epidemiological data on graft rejection rates and trends.
  • Main Results:

    • Direct allorecognition is linked to acute rejection, while indirect allorecognition is associated with chronic rejection.
    • Upregulation of cytotoxic T-lymphocyte molecules observed in rejecting renal allografts.
    • Acute rejection incidence is decreasing due to improved immunosuppression, but chronic rejection-related graft loss is increasing.
    • Acute rejection is more prevalent in pediatric recipients.

    Conclusions:

    • Understanding T-cell mediated allorecognition is crucial for managing graft rejection.
    • The shift towards increased chronic rejection necessitates novel therapeutic approaches.
    • Improving graft half-life in pediatric renal transplantation requires addressing chronic rejection mechanisms.