Copy Number Analysis of 9p24.1 in Classic Hodgkin Lymphoma Arising in Immune Deficiency/Dysregulation-Reference-Cited by-同舟云学术

Copy Number Analysis of 9p24.1 in Classic Hodgkin Lymphoma Arising in Immune Deficiency/Dysregulation

Published:2024-03-27 Issue:7 Volume:16 Page:1298
ISSN:2072-6694
Container-title:Cancers
language:en
Short-container-title:Cancers

Author:

Ohsawa Kumiko¹²,Momose Shuji²,Nishikori Asami¹^ORCID,Nishimura Midori Filiz¹^ORCID,Gion Yuka³^ORCID,Sawada Keisuke²^ORCID,Higashi Morihiro²^ORCID,Tokuhira Michihide⁴,Tamaru Jun-ichi²⁵,Sato Yasuharu¹^ORCID

Affiliation:

1. Department of Molecular Hematopathology, Okayama University Graduate School of Health Sciences, Okayama 700-8558, Japan

2. Department of Pathology, Saitama Medical Center, Saitama Medical University, Saitama 350-8550, Japan

3. Department of Medical Technology, Faculty of Health Sciences, Ehime Prefectural University of Health Sciences, Tobe 791-2101, Japan

4. Department of Hematology, Japan Community Health Care Organization Saitama Medical Center, Saitama 330-0074, Japan

5. PCL Japan, Pathology and Cytology Center, Saitama 331-9530, Japan

Abstract

A subset of patients with rheumatoid arthritis receiving methotrexate develop immune deficiencies and dysregulation-associated lymphoproliferative disorders. Patients with these disorders often exhibit spontaneous regression after MTX withdrawal; however, chemotherapeutic intervention is frequently required in patients with classic Hodgkin lymphoma arising in immune deficiency/dysregulation. In this study, we examined PD-L1 expression levels and 9p24.1 copy number alterations in 27 patients with classic Hodgkin lymphoma arising from immune deficiency/dysregulation. All patients demonstrated PD-L1 protein expression and harbored 9p24.1 copy number alterations on the tumor cells. When comparing clinicopathological data and associations with 9p24.1 copy number features, the copy gain group showed a significantly higher incidence of extranodal lesions and clinical stages than the amplification group. Notably, all cases in the amplification group had latency type II, while 6/8 (75%) in the copy gain group had latency type II, and 2/8 (25%) had latency type I. Thus, a subset of the copy-gain group demonstrated more extensive extranodal lesions and higher clinical stages. This finding speculates the presence of a genetically distinct subgroup within the group of patients who develop immune deficiencies and dysregulation-associated lymphoproliferative disorders, which may explain certain characteristic features.

Publisher

MDPI AG

Link

https://www.mdpi.com/2072-6694/16/7/1298/pdf

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