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定义人类肾移植中 T 细胞介导排斥反应的典型形式。

Defining the canonical form of T-cell-mediated rejection in human kidney transplants.

机构信息

Alberta Transplant Applied Genomics Centre, Division of Nephrology and Transplant Immunology, Department of Medicine.

Department of Laboratory Medicine and Pathology, University of Alberta, Edmonton, AB, Canada.

出版信息

Am J Transplant. 2010 Apr;10(4):810-820. doi: 10.1111/j.1600-6143.2009.03007.x. Epub 2010 Feb 3.

Abstract

Banff defines T-cell-mediated rejection (TCMR) using nonspecific lesions and arbitrary cutoffs, with no external gold standard. We reexamined features of TCMR using exclusively molecular definition independent of histopathology. The definition was derived from mouse kidney transplants with fully developed TCMR, and is based on high expression of transcripts reflecting IFNG effects and alternative macrophage activation. In 234 human kidney transplant biopsies for cause phenotyped by microarrays, we identified 26 biopsies meeting these criteria. After excluding three biopsies with unrelated diseases, all 23 biopsies had typical Banff lesions of TCMR (inflammation, tubulitis), with v lesions in 10/23. Banff histopathology diagnosed 18 as TCMR, 1 as mixed and 4 as borderline. Despite marked changes in transcriptome indicating tissue injury and dedifferentiation, all kidneys with molecularly defined TCMR, even with v lesions or late rejection, demonstrated excellent recovery of function at 6 months with no graft loss (mean follow-up 2.5 years). Thus TCMR defined exclusively by molecules manifests TCMR-related lesions and function impairment, but good recovery and survival, even with late rejection or arteritis. This combination of pathologic, clinical and molecular features constitutes the typical or canonical T-cell-mediated rejection.

摘要

班夫定义 T 细胞介导的排斥反应(TCMR)使用非特异性病变和任意截止值,没有外部金标准。我们使用完全独立于组织病理学的分子定义重新检查了 TCMR 的特征。该定义源自具有完全发展的 TCMR 的小鼠肾脏移植,基于反映 IFNG 效应和替代巨噬细胞激活的高表达转录物。在 234 例因表型而异的人类肾脏移植活检中,我们通过微阵列鉴定了 26 例符合这些标准的活检。排除了 3 例具有无关疾病的活检后,所有 23 例活检均具有典型的 TCMR(炎症、肾小管炎)Banff 病变,其中 10/23 例有 v 病变。Banff 组织病理学诊断 18 例为 TCMR,1 例为混合性,4 例为边界性。尽管转录组有明显变化表明组织损伤和去分化,但所有分子定义的 TCMR 肾脏,即使有 v 病变或晚期排斥反应,在 6 个月时功能恢复良好,无移植物丢失(平均随访 2.5 年)。因此,仅通过分子定义的 TCMR 表现出 TCMR 相关的病变和功能障碍,但具有良好的恢复和存活率,即使有晚期排斥反应或动脉炎。这种病理、临床和分子特征的组合构成了典型或经典的 T 细胞介导的排斥反应。

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