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Aberrant immunoarchitecture distinguishes hyperplastic germinal centres in pattern 1 angioimmunoblastic T-cell lymphoma from reactive follicles

机译:异常的免疫体系结构将模式1血管免疫母细胞T细胞淋巴瘤中的增生生发中心与反应性卵泡区分开

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摘要

We compare 30 biopsies each of Pattern 1 angioimmunoblastic T-cell lymphoma (AITL1) and reactive lymphoid hyperplasia (RLH) by immunohistology, in-situ hybridization for Epstein-Barr virus-encoded RNA and T-cell receptor- (TRG)-clonality. AITL1 cases, more often than RLH controls, were older [median ages 61 (range 23-79) vs 46 (range 11-59) years, p<10(-4)], non-Chinese [16/30 (53%) vs 8/28 (29%), p=0.035], presented nodally [29/30 (97%) vs 23/30 (77%), p=0.024], showed: pan-T cell antigen attenuation [25/29 (86%) vs 5/21 (24%), p=1.0x10(-5)], CD4 predominance [25/28 (89%) vs 12/23 (52%), p=3.4x10(-3)], interfollicular lymphoid CD10-positivity [16/30 (53%) vs 1/29 (3%), p=1.5x10(-5)], TRG clonality [16/28 (57%) vs 1/20 (5%), p=1.4x10(-4)], higher maximum number of Epstein-Barr virus-encoded RNA+nuclei per 0.5-mm high-power field [median 6 (range 0-70) vs 1 (range 0-40), p=0.012] and interfollicular Ki-67 proliferation fraction [median 40% (range 10-80%) vs 20% (range 5-40), p<10(-4)], whereas their germinal centres (GCs) more often showed attenuation of CD10 [30/30 (100%) vs 11/29 (38%), p=5.3x10(-8)] and CD57 [18/25 (72%) vs 4/22 (18%), p=2.4x10(-4)] (respectively). GC-predominant PD-1 and ICOS immunoreactivity were more often seen in RLH [20/22 and 9/19 controls (91% and 47%)] than AITL1 [9/25 and 3/19 cases (36% and 16%), p=1.0x10(-4) and 0.033, respectively]. Significant independent predictors against AITL1 were: solid GC CD10 immunoreactivity {p=0.023, odds ratio (OR) for AITL1 0.01 [95% confidence interval (CI): 0.0002-0.529]}; lower interfollicular proliferation fraction [p=0.047, OR for AITL1 1.1 (95% CI: 1.001-1.209) per % rise in Ki-67]; younger presenting age [p=0.028, OR for AITL1 1.136 (95% CI: 1.014-1.272) per year older]. Hence, GCs and perifollicular zones in AITL1 are distinct from those in RLH. Copyright (c) 2013 John Wiley & Sons, Ltd.
机译:我们通过免疫组织学,针对爱泼斯坦-巴尔病毒编码的RNA和T细胞受体-(TRG)-克隆的原位杂交,比较了30个活检样本中的每个模式1血管免疫母细胞性T细胞淋巴瘤(AITL1)和反应性淋巴样增生(RLH)。 AITL1病例比RLH对照多,年龄较大[中位年龄61岁(23-79岁)vs 46岁(11-59岁),p <10(-4)],非中国人[16/30(53% )相对于8/28(29%),p = 0.035],结节呈现[29/30(97%)vs 23/30(77%),p = 0.024],显示:pan-T细胞抗原减毒[25 / 29(86%)vs 5/21(24%),p = 1.0x10(-5)],CD4优势[25/28(89%)vs 12/23(52%),p = 3.4x10(-3) )],小泡间淋巴样CD10阳性[16/30(53%)vs 1/29(3%),p = 1.5x10(-5)],TRG克隆性[16/28(57%)vs 1/20( 5%),p = 1.4x10(-4)],每个0.5毫米高倍视野的最大爱泼斯坦-巴尔病毒编码RNA +核的最大数目[中位数6(范围0-70)与1(范围0- 40),p = 0.012]和小泡间Ki-67增殖率[中位数40%(范围10-80%)对20%(范围5-40),p <10(-4)),而它们的生发中心(GCs) )更经常显示CD10的衰减[30/30(100%)vs 11/29(38%),p = 5.3x10(-8)]和CD57 [18/25(72%)vs 4/22(18%) ),分别为p = 2.4x10(-4)]。与AITL1相比,RLH [20/22和9/19对照(91%和47%)]中更常见以GC为主的PD-1和ICOS免疫反应[9/25和3/19例(36%和16%) ,分别为p = 1.0x10(-4)和0.033]。针对AITL1的重要独立预测因子是:固体GC CD10免疫反应性{p = 0.023,AITL1的优势比(OR)0.01 [95%置信区间(CI):0.0002-0.529]};较低的小泡间增生分数[p = 0.047,或Ki-67中每增加1%的AITL1 1.1(95%CI:1.001-1.209)];呈现年龄[p = 0.028,或AITL1 1.136(95%CI:1.014-1.272)/年长]。因此,AITL1中的GC和滤泡周围区域与RLH中的不同。版权所有(c)2013 John Wiley&Sons,Ltd.

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