Literature DB >> 20357253

Intragraft Th17 infiltrate promotes lymphoid neogenesis and hastens clinical chronic rejection.

Clémence Deteix1, Valérie Attuil-Audenis, Aurélie Duthey, Natacha Patey, Brigitte McGregor, Valérie Dubois, Giuseppina Caligiuri, Stéphanie Graff-Dubois, Emmanuel Morelon, Olivier Thaunat.   

Abstract

To evaluate the influence of intragraft inflammatory infiltrate on the course of chronic rejection, 11 human renal grafts, detransplanted for terminal failure, were analyzed. Samples were divided into two groups according to their graft survival (> or < or = 8 y). In both groups, the main cell population infiltrating the graft interstitia was T lymphocytes. The extent of the lymphocytic infiltration and the distribution of naive and memory, CD4(+) and CD8(+) T cells, were similar in both groups. Although all types of Th polarization profiles can lead to terminal chronic rejection, a correlation between shorter graft survival and the presence of Th17 cells that produce IL-17 and IL-21 was observed. In contrast, grafts infiltrated by regulatory T cells survived significantly longer. The correlation between the expressions of activation-induced cytidine deaminase (the key enzyme of the germinal center reaction) and IL-21 suggests that Th17 could exert their deleterious effect by promoting lymphoid neogenesis, namely, the organization of inflammatory effectors into ectopic germinal centers in which a local humoral immune response is elicited. Further studies will determine whether Th17 infiltration can be used as a prognosis tool and whether the Th17 subset constitutes a therapeutic target for slowing down chronic rejection.

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Year:  2010        PMID: 20357253     DOI: 10.4049/jimmunol.0902999

Source DB:  PubMed          Journal:  J Immunol        ISSN: 0022-1767            Impact factor:   5.422


  71 in total

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3.  Loss of IL-27Rα Results in Enhanced Tubulointerstitial Fibrosis Associated with Elevated Th17 Responses.

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4.  Characterization of ectopic lymphoid structures in different types of acute renal allograft rejection.

Authors:  K de Leur; M C Clahsen-van Groningen; T P P van den Bosch; G N de Graav; D A Hesselink; J N Samsom; C C Baan; K Boer
Journal:  Clin Exp Immunol       Date:  2018-02-02       Impact factor: 4.330

5.  IL-23 is required for long-term control of Mycobacterium tuberculosis and B cell follicle formation in the infected lung.

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Journal:  J Immunol       Date:  2011-10-14       Impact factor: 5.422

Review 6.  Effector mechanisms of rejection.

Authors:  Aurélie Moreau; Emilie Varey; Ignacio Anegon; Maria-Cristina Cuturi
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Review 7.  Current concept for tertiary lymphoid structures in urothelial carcinoma of the bladder: a literature review and our experience.

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8.  NK cell and Th17 responses are differentially induced in murine cytomegalovirus infected renal allografts and vary according to recipient virus dose and strain.

Authors:  Mao Li; Srinivasa Rao Boddeda; Bo Chen; Qiang Zeng; Trenton R Schoeb; Victoria M Velazquez; Masako Shimamura
Journal:  Am J Transplant       Date:  2018-05-07       Impact factor: 8.086

9.  Lymphoid-Like Structures with Distinct B Cell Areas in Kidney Allografts are not Predictive for Graft Rejection. A Non-human Primate Study.

Authors:  Margreet Jonker; Jacqueline A M Wubben; Bert A 't Hart; Krista G Haanstra
Journal:  Inflammation       Date:  2015-12       Impact factor: 4.092

10.  Immune responses elicited in tertiary lymphoid tissues display distinctive features.

Authors:  Olivier Thaunat; Stéphanie Graff-Dubois; Sophie Brouard; Chantal Gautreau; Aditi Varthaman; Nicole Fabien; Anne-Christine Field; Liliane Louedec; Jianping Dai; Etienne Joly; Emmanuel Morelon; Jean-Paul Soulillou; Jean-Baptiste Michel; Antonino Nicoletti
Journal:  PLoS One       Date:  2010-06-30       Impact factor: 3.240

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