Clinicopathological comparison between PTCL‐TBX21 and PTCL‐GATA3 in Japanese patients

Author:

Shimasaki Yasumasa12,Miyoshi Hiroaki1ORCID,Kawamoto Keisuke13,Yoshida Noriaki14,Mishina Tatsuzo15,Nakashima Kazutaka1,Imamoto Teppei16,Sugio Takeshi7,Yanagida Eriko1,Kato Takeharu8,Yamada Kyohei1,Takeuchi Mai1,Suzuki Takaharu3,Moritsubo Mayuko1ORCID,Furuta Takuya1,Imaizumi Yoshitaka8ORCID,Takizawa Jun3,Kato Koji7,Suzumiya Junji9,Suzuki Ritsuro2,Ohshima Koichi1

Affiliation:

1. Department of Pathology, School of Medicine Kurume University Kurume Japan

2. Department of Hematology Shimane University Hospital Izumo Japan

3. Department of Hematology, Endocrinology, and Metabolism, Faculty of Medicine Niigata University Niigata Japan

4. Department of Clinical Studies Radiation Effects Research Foundation Hiroshima Japan

5. Department of Hematology Chiba University Hospital Chiba Japan

6. Department of Surgical Pathology Hokkaido University Hospital Sapporo Japan

7. Department of Medicine and Biosystemic Science, Graduate School of Medical Sciences Kyushu University Fukuoka Japan

8. Department of Hematology, Atomic Bomb Disease and Hibakusha Medicine Unit Nagasaki University Graduate School of Biomedical Sciences Nagasaki Japan

9. Department of Hematology Kohga Hospital Yaizu Japan

Abstract

AbstractAimPeripheral T‐cell lymphoma not otherwise specified (PTCL‐NOS) is a heterogeneous disease that can be classified into the PTCL‐TBX21 and PTCL‐GATA3 subtypes.MethodsIn this study, we compared the clinicopathological features of PTCL‐NOS in a Japanese cohort, classified using an IHC algorithm.ResultsOne hundred patients with PTCL‐NOS were categorized as having PTCL‐TBX21 (n = 55), PTCL‐GATA3 (n = 24), or PTCL‐unclassified (n = 21). When comparing PTCL‐TBX21 and PTCL‐GATA3, PTCL‐TBX21 showed significantly lower CD4 positivity (p = 0.047), lower counts of high endothelial venules (p = 0.032), and a tendency for a better response to initial treatment (p = 0.088). Gene expression analysis using the nCounter system showed higher expression of tumor immunity‐related genes, such as PD‐L1, LAG3, and IDO1, in PTCL‐TBX21 than in PTCL‐GATA3. PTCL‐GATA3 had significantly worse overall survival (OS) than those with PTCL‐TBX21 (p = 0.047), although a similar tendency was observed for progression‐free survival (PFS) (p = 0.064). PTCL‐GATA3 was a prognostic factor for OS in univariate analysis (HR 2.02; 95% CI, 1.09–3.77; p = 0.027), although multivariate analysis did not show significance (HR 2.07; 95% CI, 0.93–4.61; p = 0.074). In the PFS analysis, PTCL‐GATA3 was an independent prognostic factor by univariate analysis (HR 1.96; 95% CI, 1.08–3.56; p = 0.027) and multivariate analysis (HR 2.34; 95% CI, 1.07–5.11; p = 0.032).ConclusionThe classification of PTCL‐NOS into PTCL‐TBX21 and PTCL‐GATA3 is useful for predicting the prognosis of Japanese patients and stratifying the administration of tumor immune checkpoint inhibitors in clinical practice.

Publisher

Wiley

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