首页> 外文期刊>American Journal of Surgical Pathology >Extranodal NK/T-cell lymphoma, nasal type, includes cases of natural killer cell and αβ, γδ, and αβ/γδ T-cell origin: A comprehensive clinicopathologic and phenotypic study
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Extranodal NK/T-cell lymphoma, nasal type, includes cases of natural killer cell and αβ, γδ, and αβ/γδ T-cell origin: A comprehensive clinicopathologic and phenotypic study

机译:鼻外结节性NK / T细胞淋巴瘤,包括自然杀伤细胞和αβ,γδ和αβ/γδT细胞来源的病例:全面的临床病理和表型研究

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Extranodal NK/T-cell lymphoma (ENKTL), nasal type, may be of NK or T-cell origin; however, the proportion of T-ENKTLs and whether they are of αβ or γδ type remains uncertain. To elucidate the cell of origin and detailed phenotype of ENKTL and assess any clinicopathologic associations, 67 cases of ENKTL from Thailand were investigated, together with 5 γδ enteropathy-associated T-cell lymphomas (EATLs) for comparison. In all, 70% of the ENKTL were T-cell receptor (TCR) β,γ and, in cases tested, δ negative (presumptive NK origin); 5% were TCR γδ, 3% were TCR αβ, 1% were TCR αβ/γδ, and 21% were indeterminate. Out of 17 presumptive NK-ENKTLs tested, 3 had clonal TCR rearrangements. All cases were EBV and TIA-1; >85% were positive for CD3, CD2, granzyme B, pSTAT3, and Lsk/MATK; and all were CD16. Presumptive NK-ENKTLs had significantly more frequent CD56 (83% vs. 33%) and CXCL13 (59% vs. 0%) but less frequent PD-1 (0% vs. 40%) compared with T-ENKTLs. Of the NK-ENKTLs, 38% were Oct-2 compared with 0% of T-ENKTLs, and 54% were IRF4/MUM1 compared with 20% of T-ENKTLs. Only αβ T-ENKTLs were CD5. Intestinal ENKTLs were EBV and had significantly more frequent CD30, pSTAT3, and IRF4/MUM1 expression but less frequent CD16 compared with γδ EATL. Significant adverse prognostic indicators included a primary non-upper aerodigestive tract site, high stage, bone marrow involvement, International Prognostic Index = 2, lack of radiotherapy, Ki67 >40%, and CD25 expression. The upper aerodigestive tract ENKTLs of T-cell origin compared with those of presumptive NK origin showed a trend for better survival. Thus, at least 11% of evaluable ENKTLs are of T-cell origin. Although T-ENKTLs have phenotypic and some possible clinical differences, they share many similarities with ENKTLs that lack TCR expression and are distinct from intestinal γδ EATL.
机译:鼻外型结外NK / T细胞淋巴瘤(ENKTL)可能是NK或T细胞起源的;然而,T-ENKTLs的比例以及它们是αβ型还是γδ型仍然不确定。为了阐明ENKTL的起源细胞和详细的表型并评估任何临床病理学关联,对泰国的67例ENKTL病例以及5种与γδ肠病相关的T细胞淋巴瘤(EATL)进行了比较。总共,ENKTL的70%为T细胞受体(TCR)β,γ,在测试的情况下为δ阴性(推测为NK起源); TCRγδ占5%,TCRαβ占3%,TCRαβ/γδ占1%,不确定的占21%。在测试的17种推测性NK-ENKTL中,有3种具有克隆的TCR重排。所有病例均为EBV和TIA-1; > 85%的CD3,CD2,颗粒酶B,pSTAT3和Lsk / MATK阳性;都是CD16推定的NK-ENKTL与T-ENKTL相比,其CD56(83%vs. 33%)和CXCL13(59%vs. 0%)的发生率明显更高,但PD-1的发生率较低(0%对40%)。在NK-ENKTL中,Oct-2为38%,而T-ENKTL为0%,IRF4 / MUM1为54%,而T-ENKTL为20%。只有αβT-ENKTL是CD5。肠内ENKTLs为EBV,与γδEATL相比,其CD30,pSTAT3和IRF4 / MUM1的表达明显更高,而CD16的表达则更低。重要的不良预后指标包括原发性非上消化道部位,高分​​期,骨髓受累,国际预后指数= 2,缺乏放疗,Ki67> 40%和CD25表达。与推测的NK起源的相比,T细胞起源的上消化道ENKTL显示出更好的生存趋势。因此,至少11%的可评估ENKTL是T细胞起源的。尽管T-ENKTL具有表型和某些可能的临床差异,但它们与缺乏TCR表达且不同于肠道γδEATL的ENKTL具有许多相似之处。

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