Literature DB >> 17645706

Lymphoid cell proliferation in renal transplants: biologic and diagnostic implications.

Hulya Akgun1, Ayhan Ozcan, Mini Chirala, Jim Zhai, Steven S Shen, Wadi N Suki, Luan D Truong.   

Abstract

It is unclear whether alloreaction develops in peripheral lymphoid organs and effector cells being recruited to the target organs, or the entire process of alloreaction can happen within the transplanted kidneys. Interstitial inflammatory cell (IIC) proliferation was evaluated by MIB-1 antigen immunostain and the rate expressed as positive cells/1000 cells. This rate was higher in acute cell-mediated rejection (ACR) (25.7, n = 14) compared with normal kidney (0.4, n = 8), acute tubular necrosis (1.2, n = 8), chronic allograft nephropathy (CAN, 2.4, n = 20), and native kidneys with diverse diseases (9.2, n = 63); but was comparable to that in CAN with significant IIC (20.6, n = 16). 10.1% and 8.3% of T lymphocytes underwent proliferation in ACR with or without CAN, whereas only rare B lymphocytes or macrophages showed this change (<1.2%), regardless of diagnostic categories. All biopsies diagnosed as ACR in conjunction with a high rate of MIB-1 + IIC and 9/12 biopsies with CAN and significant IIC in which ACR was diagnosed due to a high rate of MIB-1 + IIC, responded to anti-rejection therapy. Proliferation of IIC involves predominantly T lymphocytes. These observations provide support for the concept of in situ alloimmunization, and facilitate the diagnosis of ACR.

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Year:  2007        PMID: 17645706     DOI: 10.1111/j.1399-0012.2007.00670.x

Source DB:  PubMed          Journal:  Clin Transplant        ISSN: 0902-0063            Impact factor:   2.863


  1 in total

1.  Dynamic expression of Qa-2 during acute graft rejection.

Authors:  Nan Lu; Chuanxin Wang; Xiaojing Yang; Shengmei Zhao; Xiangdong Li; Xiaoli Li; Hong Jiang; Jinbo Feng; Yi Zhang; Xiong Zou
Journal:  Mol Med       Date:  2010-11-12       Impact factor: 6.354

  1 in total

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