Prognostic gene expression and microRNA profiling signatures and genetic alterations in primary testicular diffuse large B-cell lymphoma

Wenyu Shi; Zijun Y. Xu-Monette; Youchao Jia; Alexandar Tzankov; Heounjeong Go; Ling Li; Maurilio Ponzoni; Yafei Wang; Qiongli Zhai; Anamarija M. Perry; Shi Wang; Xiaoxiao Wang; April Chiu; Mina L. Xu; Carlo Visco; Karen Dybkaer; Henry Withers; Mark Long; Alyssa F. Yuan; Yi Miao; Everardo Macias; Dehong Wu; Wen Shuai; Bangchen Wang; Jianyong Li; Govind Bhagat; Youli Zu; Zenggang Pan; William Choi; Santiago Montes-Moreno; Weina Chen; J. Han van Krieken; Michael B. Møller; Xinfang Yu; Benjamin M. Parsons; Shanxiang Zhang; Eric D. Hsi; Aliyah R. Sohani; Jeremy S. Abramson; Andrés J.M. Ferreri; Bing Xu; Yong Li; Ken H. Young

doi:10.1038/s41408-025-01323-8

Prognostic gene expression and microRNA profiling signatures and genetic alterations in primary testicular diffuse large B-cell lymphoma

Wenyu Shi, Zijun Y. Xu-Monette, Youchao Jia, Alexandar Tzankov, Heounjeong Go, Ling Li, Maurilio Ponzoni, Yafei Wang, Qiongli Zhai, Anamarija M. Perry, Shi Wang, Xiaoxiao Wang, April Chiu, Mina L. Xu, Carlo Visco, Karen Dybkaer, Henry Withers, Mark Long, Alyssa F. Yuan, Yi MiaoEverardo Macias, Dehong Wu, Wen Shuai, Bangchen Wang, Jianyong Li, Govind Bhagat, Youli Zu, Zenggang Pan, William Choi, Santiago Montes-Moreno, Weina Chen, J. Han van Krieken, Michael B. Møller, Xinfang Yu, Benjamin M. Parsons, Shanxiang Zhang, Eric D. Hsi, Aliyah R. Sohani, Jeremy S. Abramson, Andrés J.M. Ferreri, Bing Xu, Yong Li, Ken H. Young

Research output: Contribution to journal › Article › peer-review

Abstract

Primary testicular (PT) diffuse large B-cell lymphoma (DLBCL) is a rare and aggressive lymphoma with distinct clinical and molecular characteristics. To identify prognostic biomarkers in PT-DLBCL, in this study we analyzed DNA and RNA samples of PT-DLBCL tumors from 206 patients using next-generation sequencing platforms and assays. Genetic alteration analysis found that multiple chromosomal copy number variations (CNVs), TP53 transcript mutations with high variant allele frequency, and MCD subtype had significantly adverse prognostic effects, whereas elevated microsatellite instability had a significantly favorable prognostic effect in PT-DLBCL. Targeted RNA-seq analysis identified a PTL gene expression signature by comparing PT-DLBCL with systemic DLBCL and revealed the heterogeneity within PT-DLBCL by unsupervised clustering, which classified PT-DLBCLs into a testicular lymphoma tumor (TLT) subtype and a microenvironment (ME) subtype. The TLT subtype featured upregulation of genes functioning in DNA damage response, DNA repair, chromatin remodeling, the cell cycle, and the nucleus, and was associated with significantly poorer patient survival and higher frequencies of MYD88 mutations, multiple CNVs, MCD subtype, bulk tumors, and elderly patients in the PT-DLBCL cohort. In contrast, the ME subtype distinctively featured upregulation of various signaling pathway genes involving the tumor microenvironment and downregulation of BTK and B-cell receptor signaling genes, and was associated with significantly better clinical outcome than the TLT subtype of PT-DLBCL independently of CNVs, MCD and MYD88 mutation and than systemic DLBCL. Moreover, genomic microRNA profiling analysis identified a PTL microRNA signature significantly differentially expressed between PT-DLBCL and systemic DLBCL patients and within the PT-DLBCL cohort, and PT-DLBCL patients with higher expression of 16 PTL microRNAs (14 are testicular tissue-specific) had significantly better survival. In summary, this study revealed the molecular heterogeneity in genetic abnormalities and expression profiles of coding genes and microRNAs within the PT-DLBCL entity, and identified significant prognostic biomarkers and PTL signatures. (Figure presented.)

Original language	English (US)
Article number	123
Journal	Blood Cancer Journal
Volume	15
Issue number	1
DOIs	https://doi.org/10.1038/s41408-025-01323-8
State	Published - Dec 2025

ASJC Scopus subject areas

Hematology
Oncology

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10.1038/s41408-025-01323-8

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Shi, W., Xu-Monette, Z. Y., Jia, Y., Tzankov, A., Go, H., Li, L., Ponzoni, M., Wang, Y., Zhai, Q., Perry, A. M., Wang, S., Wang, X., Chiu, A., Xu, M. L., Visco, C., Dybkaer, K., Withers, H., Long, M., Yuan, A. F., ... Young, K. H. (2025). Prognostic gene expression and microRNA profiling signatures and genetic alterations in primary testicular diffuse large B-cell lymphoma. Blood Cancer Journal, 15(1), Article 123. https://doi.org/10.1038/s41408-025-01323-8

Shi, W, Xu-Monette, ZY, Jia, Y, Tzankov, A, Go, H, Li, L, Ponzoni, M, Wang, Y, Zhai, Q, Perry, AM, Wang, S, Wang, X, Chiu, A, Xu, ML, Visco, C, Dybkaer, K, Withers, H, Long, M, Yuan, AF, Miao, Y, Macias, E, Wu, D, Shuai, W, Wang, B, Li, J, Bhagat, G, Zu, Y, Pan, Z, Choi, W, Montes-Moreno, S, Chen, W, Krieken, JHV, Møller, MB, Yu, X, Parsons, BM, Zhang, S, Hsi, ED, Sohani, AR, Abramson, JS, Ferreri, AJM, Xu, B, Li, Y & Young, KH 2025, 'Prognostic gene expression and microRNA profiling signatures and genetic alterations in primary testicular diffuse large B-cell lymphoma', Blood Cancer Journal, vol. 15, no. 1, 123. https://doi.org/10.1038/s41408-025-01323-8

@article{cdc283baf51c43ddbee1d43f862bbc82,

title = "Prognostic gene expression and microRNA profiling signatures and genetic alterations in primary testicular diffuse large B-cell lymphoma",

abstract = "Primary testicular (PT) diffuse large B-cell lymphoma (DLBCL) is a rare and aggressive lymphoma with distinct clinical and molecular characteristics. To identify prognostic biomarkers in PT-DLBCL, in this study we analyzed DNA and RNA samples of PT-DLBCL tumors from 206 patients using next-generation sequencing platforms and assays. Genetic alteration analysis found that multiple chromosomal copy number variations (CNVs), TP53 transcript mutations with high variant allele frequency, and MCD subtype had significantly adverse prognostic effects, whereas elevated microsatellite instability had a significantly favorable prognostic effect in PT-DLBCL. Targeted RNA-seq analysis identified a PTL gene expression signature by comparing PT-DLBCL with systemic DLBCL and revealed the heterogeneity within PT-DLBCL by unsupervised clustering, which classified PT-DLBCLs into a testicular lymphoma tumor (TLT) subtype and a microenvironment (ME) subtype. The TLT subtype featured upregulation of genes functioning in DNA damage response, DNA repair, chromatin remodeling, the cell cycle, and the nucleus, and was associated with significantly poorer patient survival and higher frequencies of MYD88 mutations, multiple CNVs, MCD subtype, bulk tumors, and elderly patients in the PT-DLBCL cohort. In contrast, the ME subtype distinctively featured upregulation of various signaling pathway genes involving the tumor microenvironment and downregulation of BTK and B-cell receptor signaling genes, and was associated with significantly better clinical outcome than the TLT subtype of PT-DLBCL independently of CNVs, MCD and MYD88 mutation and than systemic DLBCL. Moreover, genomic microRNA profiling analysis identified a PTL microRNA signature significantly differentially expressed between PT-DLBCL and systemic DLBCL patients and within the PT-DLBCL cohort, and PT-DLBCL patients with higher expression of 16 PTL microRNAs (14 are testicular tissue-specific) had significantly better survival. In summary, this study revealed the molecular heterogeneity in genetic abnormalities and expression profiles of coding genes and microRNAs within the PT-DLBCL entity, and identified significant prognostic biomarkers and PTL signatures. (Figure presented.)",

author = "Wenyu Shi and Xu-Monette, \{Zijun Y.\} and Youchao Jia and Alexandar Tzankov and Heounjeong Go and Ling Li and Maurilio Ponzoni and Yafei Wang and Qiongli Zhai and Perry, \{Anamarija M.\} and Shi Wang and Xiaoxiao Wang and April Chiu and Xu, \{Mina L.\} and Carlo Visco and Karen Dybkaer and Henry Withers and Mark Long and Yuan, \{Alyssa F.\} and Yi Miao and Everardo Macias and Dehong Wu and Wen Shuai and Bangchen Wang and Jianyong Li and Govind Bhagat and Youli Zu and Zenggang Pan and William Choi and Santiago Montes-Moreno and Weina Chen and Krieken, \{J. Han van\} and M{\o}ller, \{Michael B.\} and Xinfang Yu and Parsons, \{Benjamin M.\} and Shanxiang Zhang and Hsi, \{Eric D.\} and Sohani, \{Aliyah R.\} and Abramson, \{Jeremy S.\} and Ferreri, \{Andr{\'e}s J.M.\} and Bing Xu and Yong Li and Young, \{Ken H.\}",

note = "Publisher Copyright: {\textcopyright} The Author(s) 2025.",

year = "2025",

month = dec,

doi = "10.1038/s41408-025-01323-8",

language = "English (US)",

volume = "15",

journal = "Blood Cancer Journal",

issn = "2044-5385",

publisher = "Springer Nature",

number = "1",

}

TY - JOUR

T1 - Prognostic gene expression and microRNA profiling signatures and genetic alterations in primary testicular diffuse large B-cell lymphoma

AU - Shi, Wenyu

AU - Xu-Monette, Zijun Y.

AU - Jia, Youchao

AU - Tzankov, Alexandar

AU - Go, Heounjeong

AU - Li, Ling

AU - Ponzoni, Maurilio

AU - Wang, Yafei

AU - Zhai, Qiongli

AU - Perry, Anamarija M.

AU - Wang, Shi

AU - Wang, Xiaoxiao

AU - Chiu, April

AU - Xu, Mina L.

AU - Visco, Carlo

AU - Dybkaer, Karen

AU - Withers, Henry

AU - Long, Mark

AU - Yuan, Alyssa F.

AU - Miao, Yi

AU - Macias, Everardo

AU - Wu, Dehong

AU - Shuai, Wen

AU - Wang, Bangchen

AU - Li, Jianyong

AU - Bhagat, Govind

AU - Zu, Youli

AU - Pan, Zenggang

AU - Choi, William

AU - Montes-Moreno, Santiago

AU - Chen, Weina

AU - Krieken, J. Han van

AU - Møller, Michael B.

AU - Yu, Xinfang

AU - Parsons, Benjamin M.

AU - Zhang, Shanxiang

AU - Hsi, Eric D.

AU - Sohani, Aliyah R.

AU - Abramson, Jeremy S.

AU - Ferreri, Andrés J.M.

AU - Xu, Bing

AU - Li, Yong

AU - Young, Ken H.

PY - 2025/12

Y1 - 2025/12

N2 - Primary testicular (PT) diffuse large B-cell lymphoma (DLBCL) is a rare and aggressive lymphoma with distinct clinical and molecular characteristics. To identify prognostic biomarkers in PT-DLBCL, in this study we analyzed DNA and RNA samples of PT-DLBCL tumors from 206 patients using next-generation sequencing platforms and assays. Genetic alteration analysis found that multiple chromosomal copy number variations (CNVs), TP53 transcript mutations with high variant allele frequency, and MCD subtype had significantly adverse prognostic effects, whereas elevated microsatellite instability had a significantly favorable prognostic effect in PT-DLBCL. Targeted RNA-seq analysis identified a PTL gene expression signature by comparing PT-DLBCL with systemic DLBCL and revealed the heterogeneity within PT-DLBCL by unsupervised clustering, which classified PT-DLBCLs into a testicular lymphoma tumor (TLT) subtype and a microenvironment (ME) subtype. The TLT subtype featured upregulation of genes functioning in DNA damage response, DNA repair, chromatin remodeling, the cell cycle, and the nucleus, and was associated with significantly poorer patient survival and higher frequencies of MYD88 mutations, multiple CNVs, MCD subtype, bulk tumors, and elderly patients in the PT-DLBCL cohort. In contrast, the ME subtype distinctively featured upregulation of various signaling pathway genes involving the tumor microenvironment and downregulation of BTK and B-cell receptor signaling genes, and was associated with significantly better clinical outcome than the TLT subtype of PT-DLBCL independently of CNVs, MCD and MYD88 mutation and than systemic DLBCL. Moreover, genomic microRNA profiling analysis identified a PTL microRNA signature significantly differentially expressed between PT-DLBCL and systemic DLBCL patients and within the PT-DLBCL cohort, and PT-DLBCL patients with higher expression of 16 PTL microRNAs (14 are testicular tissue-specific) had significantly better survival. In summary, this study revealed the molecular heterogeneity in genetic abnormalities and expression profiles of coding genes and microRNAs within the PT-DLBCL entity, and identified significant prognostic biomarkers and PTL signatures. (Figure presented.)

AB - Primary testicular (PT) diffuse large B-cell lymphoma (DLBCL) is a rare and aggressive lymphoma with distinct clinical and molecular characteristics. To identify prognostic biomarkers in PT-DLBCL, in this study we analyzed DNA and RNA samples of PT-DLBCL tumors from 206 patients using next-generation sequencing platforms and assays. Genetic alteration analysis found that multiple chromosomal copy number variations (CNVs), TP53 transcript mutations with high variant allele frequency, and MCD subtype had significantly adverse prognostic effects, whereas elevated microsatellite instability had a significantly favorable prognostic effect in PT-DLBCL. Targeted RNA-seq analysis identified a PTL gene expression signature by comparing PT-DLBCL with systemic DLBCL and revealed the heterogeneity within PT-DLBCL by unsupervised clustering, which classified PT-DLBCLs into a testicular lymphoma tumor (TLT) subtype and a microenvironment (ME) subtype. The TLT subtype featured upregulation of genes functioning in DNA damage response, DNA repair, chromatin remodeling, the cell cycle, and the nucleus, and was associated with significantly poorer patient survival and higher frequencies of MYD88 mutations, multiple CNVs, MCD subtype, bulk tumors, and elderly patients in the PT-DLBCL cohort. In contrast, the ME subtype distinctively featured upregulation of various signaling pathway genes involving the tumor microenvironment and downregulation of BTK and B-cell receptor signaling genes, and was associated with significantly better clinical outcome than the TLT subtype of PT-DLBCL independently of CNVs, MCD and MYD88 mutation and than systemic DLBCL. Moreover, genomic microRNA profiling analysis identified a PTL microRNA signature significantly differentially expressed between PT-DLBCL and systemic DLBCL patients and within the PT-DLBCL cohort, and PT-DLBCL patients with higher expression of 16 PTL microRNAs (14 are testicular tissue-specific) had significantly better survival. In summary, this study revealed the molecular heterogeneity in genetic abnormalities and expression profiles of coding genes and microRNAs within the PT-DLBCL entity, and identified significant prognostic biomarkers and PTL signatures. (Figure presented.)

UR - https://www.scopus.com/pages/publications/105011058018

UR - https://www.scopus.com/inward/citedby.url?scp=105011058018&partnerID=8YFLogxK

U2 - 10.1038/s41408-025-01323-8

DO - 10.1038/s41408-025-01323-8

M3 - Article

C2 - 40675955

AN - SCOPUS:105011058018

SN - 2044-5385

VL - 15

JO - Blood Cancer Journal

JF - Blood Cancer Journal

IS - 1

M1 - 123

ER -

Prognostic gene expression and microRNA profiling signatures and genetic alterations in primary testicular diffuse large B-cell lymphoma

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