2006
DOI: 10.1111/j.1600-6143.2006.01483.x
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Tubulitis and Epithelial Cell Alterations in Mouse Kidney Transplant Rejection Are Independent of CD103, Perforin or Granzymes A/B

Abstract: One of the defining lesions of kidney allograft rejection is epithelial deterioration and invasion by inflammatory cells (tubulitis). We examined epithelial changes and their relationship to effector T cells and to CD103/E-cadherin interactions in mouse kidney allografts. Rejecting allografts showed interstitial mononuclear infiltration from day 5. Loss of epithelial mass, estimated by tubular surface area, and tubulitis were minimal through day 7 and severe by day 21. Tubules in day 21 allografts manifested s… Show more

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Cited by 43 publications
(39 citation statements)
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“…Interstitial inflammation is established by day 5 post transplant, followed later by tubulitis and epithelial deterioration (1). Tubulitis is preceded by molecular changes of the epithelium (3,4), which are readily apparent by days [5][6][7], and even earlier by sophisticated methods (3,4). The (2,11,12).…”
Section: Rejection-damage To the Organ Parenchyma By The Adaptive Allmentioning
confidence: 99%
“…Interstitial inflammation is established by day 5 post transplant, followed later by tubulitis and epithelial deterioration (1). Tubulitis is preceded by molecular changes of the epithelium (3,4), which are readily apparent by days [5][6][7], and even earlier by sophisticated methods (3,4). The (2,11,12).…”
Section: Rejection-damage To the Organ Parenchyma By The Adaptive Allmentioning
confidence: 99%
“…ligand-has no effect on the development of the diagnostic TCMR lesions in mouse kidney allografts (11,12). (14,15).…”
Section: And Loss Of Kidney Transcripts (Kts) (10) Although Cytotoximentioning
confidence: 99%
“…This concept may provide insight into allograft rejection injury because there have been disparate results regarding the role of effector T-cell expression of perforin-granzyme in mediating kidney allograft rejection. In previous studies, the absence of perforin-granzyme in recipient effector cells did not prevent tubular injury or rejection but these studies used ''non-lifesupporting'' murine renal transplant models and multiple effector mechanisms apart from perforin-granzyme provide redundant pathways of rejection in vivo (10,11). Moreover, transcript levels of perforin and granzyme B were upregulated in grafts after transplantation which supports a potential role for perforin-granzymeYmediated cytotoxicity (10).…”
mentioning
confidence: 58%