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首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >The Transcription Factor, T-bet, Primes Intestine Transplantation Rejection and Is Associated With Disrupted Mucosal Homeostasis
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The Transcription Factor, T-bet, Primes Intestine Transplantation Rejection and Is Associated With Disrupted Mucosal Homeostasis

机译:转录因子,T-bet,引发肠移植排斥反应,并与粘膜稳态破坏有关。

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Background. The transcription factor, t-bet, promotes inflammatory polarization and intestinal homing of many inflammatory cells. In previous studies, the t-bet and granulysin genes were upregulated in peripheral blood before and after intestine transplantation (ITx) rejection, but not during rejection, possibly because of sequestration in allograft mucosa. Mucosal sequestration of t-bet and granulysin may also explain the presence of inflammatory CD14+ monocyte-derived macrophages (MDM) and immunoglobulin G+ B-cell lineage cells, and loss of mature non-inflammatory CD138+ plasma cells in allograft mucosa during ITx rejection in these previous studies. Methodology. T-bet-stained and granulysin-stained cells, MDM and CD138+ plasma cells were evaluated with immunohistochemistry in serial biopsies from 17 children, in whom changes in MDM and CD138+ plasma cells were observed previously. Results. T-bet-positive mucosal cells were significantly higher in postperfusion (P = 0.035) and early posttransplant biopsies (P = 0.016) among rejectors, compared with nonrejectors. T-bet-positive cell counts per high-power field (hpf) were (a) positively correlated with MDM counts/hpf in postperfusion (Spearman r = 0.73; P = 0.01) and early posttransplant biopsies (r = 0.54, r = 0.046), and (b) negatively correlated with CD138+B-/pre-plasma cells in early posttransplant biopsies (r = 0.63, P = 0.038). T-bet expression in CD14+ monocytes, CD19+B cells, and several other leukocyte subsets was higher in random blood samples from two rejectors, compared with those from five normal human subjects and three nonrejectors. Scant granulysin-stained mucosal cells precluded additional evaluation of this cytotoxin and its role in ITx rejection. Significance. The transcription factor, t-bet, primes ITx rejection, and associates with disrupted homeostatic relationships between innate and adaptive immune cells in the allograft mucosa during rejection.
机译:背景。转录因子t-bet可促进许多炎症细胞的炎症极化和肠归巢。在先前的研究中,肠移植(ITx)排斥之前和之后,外周血中的t-bet和颗粒溶素基因上调,但在排斥过程中则没有,这可能是由于同种异体移植粘膜中的螯合。 t-bet和颗粒溶素的粘膜隔离也可能解释了炎症性CD14 +单核细胞衍生巨噬细胞(MDM)和免疫球蛋白G + B细胞谱系细胞的存在,以及同种异体移植粘膜中ITx排斥过程中成熟非炎性CD138 +浆细胞的丢失之前的学习。方法。用免疫组织化学方法对来自17名儿童的T-bet染色和颗粒溶素染色的细胞,MDM和CD138 +浆细胞进行了免疫组织化学评估,他们先前曾观察到MDM和CD138 +浆细胞的变化。结果。与非排斥者相比,在排斥者中,灌注后(P = 0.035)和移植后早期活检(P = 0.016),T-bet阳性粘膜细胞明显更高。每个高倍视野(hpf)的T-bet阳性细胞计数与(a)与灌注后(Spearman r = 0.73; P = 0.01)和早期移植后活检(r = 0.54,r = 0.046)的MDM计数/ hpf正相关。 ),以及(b)在早期移植后活检中与CD138 + B- /浆前细胞呈负相关(r = 0.63,P = 0.038)。与五个正常人类受试者和三个非排斥者相比,在两个排斥者的随机血液样本中,CD14 +单核细胞,CD19 + B细胞和其他几个白细胞亚群中的T-bet表达更高。缺乏颗粒溶素染色的粘膜细胞无法进一步评估这种细胞毒素及其在ITx排斥中的作用。意义。转录因子t-bet可引发ITx排斥反应,并与排斥过程中同种异体移植粘膜中先天免疫细胞和适应性免疫细胞之间的稳态平衡相关。

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