4.6 Review

Review: The transcripts associated with organ allograft rejection

期刊

AMERICAN JOURNAL OF TRANSPLANTATION
卷 18, 期 4, 页码 785-795

出版社

WILEY
DOI: 10.1111/ajt.14600

关键词

basic (laboratory) research; science; biopsy; kidney transplantation; nephrology; organ transplantation in general; rejection

资金

  1. Industrial Research Assistance Program (IRAP) of the National Research Council of Canada
  2. Canada Foundation for Innovation
  3. University of Alberta Hospital Foundation
  4. Roche Molecular Systems
  5. Hoffmann-La Roche Canada Ltd.
  6. Genome Canada
  7. Alberta Ministry of Advanced Education and Technology
  8. Roche Organ Transplant Research Foundation
  9. Astellas

向作者/读者索取更多资源

The molecular mechanisms operating in human organ transplant rejection are best inferred from the mRNAs expressed in biopsies because the corresponding proteins often have low expression and short half-lives, while small non-coding RNAs lack specificity. Associations should be characterized in a population that rigorously identifies T cell-mediated (TCMR) and antibody-mediated rejection (ABMR). This is best achieved in kidney transplant biopsies, but the results are generalizable to heart, lung, or liver transplants. Associations can be universal (all rejection), TCMR-selective, or ABMR-selective, with universal being strongest and ABMR-selective weakest. Top universal transcripts are IFNG-inducible (eg, CXCL11 IDO1, WARS) or shared by effector T cells (ETCs) and NK cells (eg, KLRD1, CCL4). TCMR-selective transcripts are expressed in activated ETCs (eg, CTLA4, IFNG), activated (eg, ADAMDEC1), or IFNG-induced macrophages (eg, ANKRD22). ABMR-selective transcripts are expressed in NK cells (eg, FGFBP2, GNLY) and endothelial cells (eg, ROBO4, DARC). Transcript associations are highly reproducible between biopsy sets when the same rejection definitions, case mix, algorithm, and technology are applied, but exact ranks will vary. Previously published rejection-associated transcripts resemble universal and TCMR-selective transcripts due to incomplete representation of ABMR. Rejection-associated transcripts are never completely rejection-specific because they are shared with the stereotyped response-to-injury and innate immunity The transcripts most strongly associated with organ graft rejection in biopsies include those selective for T cell-mediated rejection or antibody-mediated rejection, and those expressed in both, including IFNG-induced transcripts and transcripts shared by effector T cells and NK cells, but exact rankings will reflect the composition of the biopsy population.

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