Oncotarget

Research Papers:

Dissecting the functional differences and clinical features of R-spondin family members in metastatic prostate cancer

Aiden Deacon, Ava Gustafson, Allison Makovec, Ella Boytim, Gabriella von Dohlen, David Moline, Elin Kairies, Sam Kellen, Khalid Ishani, Megan L. Ludwig, Emily John, Alexis Anike, Hai Dang Nguyen, Scott M. Dehm, Justin M. Drake, Emmanuel S. Antonarakis and Justin Hwang _

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Oncotarget. 2025; 16:606-620. https://doi.org/10.18632/oncotarget.28758

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Abstract

Aiden Deacon1,4, Ava Gustafson1,4, Allison Makovec1,4, Ella Boytim1,4, Gabriella von Dohlen1,4, David Moline1,4, Elin Kairies2, Sam Kellen1,4, Khalid Ishani1,4, Megan L. Ludwig3, Emily John1,4, Alexis Anike1,4, Hai Dang Nguyen3,4, Scott M. Dehm1,4, Justin M. Drake1,3, Emmanuel S. Antonarakis1,4 and Justin Hwang1,4

1 Department of Medicine, University of Minnesota-Twin Cities, Minneapolis, MN 55455, USA

2 Cornell College, Mount Vernon, IA 52314, USA

3 Department of Pharmacology, University of Minnesota- Twin Cities, Minneapolis, MN 55455, USA

4 Masonic Cancer Center, University of Minnesota-Twin Cities, Minneapolis, MN 55455, USA

Correspondence to:

Justin Hwang, email: [email protected]

Keywords: RSPO2; prostate cancer; Wnt signaling; genomics; therapeutics

Received: March 18, 2025     Accepted: July 16, 2025     Published: July 25, 2025

Copyright: © 2025 Deacon et al. This is an open access article distributed under the terms of the Creative Commons Attribution License (CC BY 4.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.

ABSTRACT

This study investigates the R-spondin family of genes (RSPO1/2/3/4), a group of secreted proteins that act as Wnt regulators, and their subsequent role in advanced prostate cancer (PC). When evaluating transcriptomic data from primary and metastatic PC patients, we found that alterations in RSPO2 were more prevalent than in other RSPO family members or Wnt-regulating genes APC and CTNNB1. Further, we found that RSPO2 alterations in PCs were significantly associated with worse disease-free survival. Through our in silico modeling, RSPO2 exhibited strong positive associations with genes regulating epithelial-mesenchymal transition (EMT) and double-negative prostate cancer (DNPC), but had negative correlations with androgen receptor (AR) and AR-associated genes. Furthermore, 3D modeling of RSPO2 revealed structural differences between itself and other RSPOs. In cell lines, RSPO2 overexpression caused up-regulation of EMT pathways, including EMT-regulatory transcription factors ZEB1, ZEB2, and TWIST1. Conversely, this was not observed when CTNNB1 was overexpressed in the same models. These findings highlight that, in PC, RSPO2 functions as a unique member of the R-spondin family by promoting genes and signaling pathways associated with aggressive PC, and RSPO2 amplifications are associated with poor outcomes in PC patients.


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