Implementation of the recommended immunohistochemistry algorithm for classification of peripheral T-cell lymphoma, not otherwise specified into the prognostically significant GATA3 and TBX21 subtypes

IF 2.2 4区 医学 Q3 HEMATOLOGY
Surabhi Jain, Aijaz Ahmad, Ambreen Jan, Ajay Gogia, Mukul Aggarwal, Ganesh Kumar Viswanathan, Trisha Mandal, Atul Sharma, Ranjit Sahoo, Mehar Chand Sharma, Sameer Bakhshi, Lalit Kumar, Saumyaranjan Mallick
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Abstract

Introduction

Current molecular research has shown the several oncogenic pathways that give rise to the peripheral T-cell lymphoma, not otherwise defined (PTCL, NOS) subtypes, which alter prognosis and might have predictive value. This study was conducted to assess the immunohistochemistry (IHC) algorithm by Amador et al for the subtyping of PTCL, NOS and determine its applicability in relation to the clinicopathological profile.

Methods

This study included 43 patients with PTCL, NOS diagnosis. Following the use of IHC for the transcription factors GATA3, TBX21, CCR4, and CXCR3, two pathologists subtyped the samples. Comprehensive clinicopathological correlation was carried out.

Results

Applying the algorithm of Amador et al., cases were classified into GATA3 (20), TBX21 (15), and unclassified (8) subtypes. No significant association with clinical parameters of subtypes or CD4/ CD8 positivity was observed. Although a higher proportion of cases in the TBX21 subgroup showed a polymorphic population compared with the GATA3 subgroup, which had a monomorphic population, no significant p-value (0.111) was observed. Two Lennert lymphomas were classified into the GATA3 subgroup. Multivariate analysis showed no significant difference in overall survival (p-value = 0.105) and progression-free survival (p-value = 0.0509) between IHC-defined subtypes; trends indicate that overall survival and progression-free survival are worse in the GATA3 subgroup.

Conclusion

Although the algorithm is reproducible, a proportion of cases remains unclassifiable and may require additional investigation and gene expression profiling. The GATA3 subgroup was found to have a monomorphic population with a poor overall prognosis and thus requires a larger sample size for validation.

采用推荐的免疫组化算法,将外周 T 细胞淋巴瘤(未另作规定)分为对预后有重要意义的 GATA3 和 TBX21 亚型。
导言:目前的分子研究表明,有几种致癌途径可导致未另作定义的外周T细胞淋巴瘤(PTCL,NOS)亚型,这些亚型可改变预后并可能具有预测价值。本研究旨在评估 Amador 等人提出的用于 PTCL NOS 亚型划分的免疫组化(IHC)算法,并确定该算法与临床病理特征的相关性:本研究共纳入 43 名确诊为 PTCL(NOS)的患者。两名病理学家对样本进行了转录因子 GATA3、TBX21、CCR4 和 CXCR3 的 IHC 分型。结果:应用 Amador 等人的算法,病例被分为 GATA3(20 例)、TBX21(15 例)和未分类(8 例)亚型。未观察到亚型与临床参数或 CD4/ CD8 阳性有明显关联。虽然 TBX21 亚组中出现多形性群体的病例比例高于 GATA3 亚组(后者为单形性群体),但未观察到明显的 p 值(0.111)。两个 Lennert 淋巴瘤被归入 GATA3 亚组。多变量分析显示,IHC定义的亚型之间的总生存期(p值=0.105)和无进展生存期(p值=0.0509)无显著差异;趋势表明,GATA3亚组的总生存期和无进展生存期较差:尽管该算法具有可重复性,但仍有一部分病例无法分类,可能需要进行更多的调查和基因表达谱分析。研究发现,GATA3 亚组的病例为单型,总体预后较差,因此需要更大的样本量进行验证。
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来源期刊
CiteScore
4.50
自引率
6.70%
发文量
211
审稿时长
6-12 weeks
期刊介绍: The International Journal of Laboratory Hematology provides a forum for the communication of new developments, research topics and the practice of laboratory haematology. The journal publishes invited reviews, full length original articles, and correspondence. The International Journal of Laboratory Hematology is the official journal of the International Society for Laboratory Hematology, which addresses the following sub-disciplines: cellular analysis, flow cytometry, haemostasis and thrombosis, molecular diagnostics, haematology informatics, haemoglobinopathies, point of care testing, standards and guidelines. The journal was launched in 2006 as the successor to Clinical and Laboratory Hematology, which was first published in 1979. An active and positive editorial policy ensures that work of a high scientific standard is reported, in order to bridge the gap between practical and academic aspects of laboratory haematology.
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