Clinicopathological features of HCV-positive splenic diffuse large B cell lymphoma.


Journal

Annals of hematology
ISSN: 1432-0584
Titre abrégé: Ann Hematol
Pays: Germany
ID NLM: 9107334

Informations de publication

Date de publication:
May 2019
Historique:
received: 13 07 2018
accepted: 29 01 2019
pubmed: 8 2 2019
medline: 26 4 2019
entrez: 8 2 2019
Statut: ppublish

Résumé

The hepatitis C virus (HCV) is a single-stranded RNA virus which is thought to be involved in the onset of B cell lymphoma. HCV-positive diffuse large B cell lymphoma (DLBCL) has been reported to clinically manifest in extranodal lesions (e.g., in the liver, spleen, and stomach). Here, we investigated HCV-positive and -negative primary splenic DLBCL (p-spDLBCL) and non-primary splenic DLBCL (ordinary DLBCL). Furthermore, to examine HCV lymphomagenesis, RNA in situ hybridization (ISH), RT-PCR (reverse-transcription polymerase chain reaction), and NS3 immunostaining of HCV viral nonstructural proteins were performed. HCV-positive p-spDLBCL patients presented fewer B symptoms (asymptomatic) and better performance status, with elevated presence of splenic macronodular lesions and more germinal center B cell (GCB) sub-group cases than HCV-negative p-spDLBCL patients. However, HCV-positive ordinary DLBCL patients were found to have more non-GCB sub-group cases than HCV-negative ordinary DLBCL patients. HCV-positive DLBCL patients showed 20.6% (7/34) NS3 positivity, 16.7% (1/6) HCV-RNA in situ positivity, and 22.2% (2/9) detection of HCV-RNA in tumor tissue by RT-PCR. Splenic samples were found to have a higher frequency of HCV detection than lymph node samples, thus suggesting that HCV may be closely related to lymphomagenesis, especially in splenic lymphoma.

Identifiants

pubmed: 30729289
doi: 10.1007/s00277-019-03628-8
pii: 10.1007/s00277-019-03628-8
doi:

Substances chimiques

NS3 protein, hepatitis C virus 0
RNA, Viral 0
Viral Nonstructural Proteins 0

Types de publication

Clinical Trial Journal Article

Langues

eng

Sous-ensembles de citation

IM

Pagination

1197-1207

Auteurs

Joji Shimono (J)

Department of Pathology, Kurume University, School of Medicine, Asahimachi 67, Kurume, Fukuoka, 830-0011, Japan.
Department of Hematology, Hokkaido University Faculty of Medicine, Sapporo, Japan.

Hiroaki Miyoshi (H)

Department of Pathology, Kurume University, School of Medicine, Asahimachi 67, Kurume, Fukuoka, 830-0011, Japan. miyoshi_hiroaki@med.kurume-u.ac.jp.

Fumiko Arakawa (F)

Department of Pathology, Kurume University, School of Medicine, Asahimachi 67, Kurume, Fukuoka, 830-0011, Japan.

Kyohei Yamada (K)

Department of Pathology, Kurume University, School of Medicine, Asahimachi 67, Kurume, Fukuoka, 830-0011, Japan.

Takeshi Sugio (T)

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

Kohta Miyawaki (K)

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

Tetsuya Eto (T)

Department of Hematology, Hamanomachi Hospital, Fukuoka, Japan.

Takuto Miyagishima (T)

Department of Hematology, Kushiro Rosai Hospital, Kushiro, Japan.

Koji Kato (K)

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

Koji Nagafuji (K)

Department of Hematology, Kurume University, School of Medicine, Kurume, Japan.

Koichi Akashi (K)

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

Takanori Teshima (T)

Department of Hematology, Hokkaido University Faculty of Medicine, Sapporo, Japan.

Koichi Ohshima (K)

Department of Pathology, Kurume University, School of Medicine, Asahimachi 67, Kurume, Fukuoka, 830-0011, Japan.

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Classifications MeSH