Autocrine Canonical Wnt Signaling Primes Noncanonical Signaling through ROR1 in Metastatic Castration-Resistant Prostate Cancer

Ma, Fen; Arai, Seiji; Wang, Keshan; Calagua, Carla; Yuan, Amanda R; Poluben, Larysa; Gu, Zhongkai; Russo, Joshua W.; Einstein, David J.; Ye, Huihui; He, Meng Xiao; Liu, Yu; Allen, Eliezer Van; Sowalsky, Adam G.; Bhasin, Manoj; Yuan, Xin; Balk, Steven P.

doi:10.1158/0008-5472.can-21-1807

Cited by 19 publications

(17 citation statements)

References 54 publications

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“…Other classical tumorigenic pathways, such as Wnt signaling pathway (KEGG:04310, adjusted p-value = 3.48e-4) and TGF-beta signaling pathway (KEGG:04350, adjusted p-value = 3.30e-5) appear also enriched. In this regard, recent studies analyzed the involvement of Wnt signaling in the proliferation of prostate cancer cells (Ma et al 2022; Wei et al 2022), as well as the involvement and TGF-beta signaling (Natani et al 2022; Xi et al 2022).…”

Section: Resultsmentioning

confidence: 99%

The PENGUIN approach to reconstruct protein interactions at enhancer-promoter regions and its application to prostate cancer

Armaos

Serra

Núñez-Carpintero

et al. 2022

Preprint

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DNA-binding proteins (DBPs) and in particular transcription factors interact with enhancers and their target genes through enhancer-promoter (E-P) interactions. Technological advancements such as chromosome conformation capture allow to identify E-P interactions, but the protein networks involved have not yet been characterized. Most importantly, the role of nuclear protein networks in human diseases has been so far poorly investigated. Prostate cancer (PrCa) heritability is associated with variations in enhancers that affect specific gene expression. Here, we introduce a novel approach, called Promoter-ENhancer-GUided Interaction Networks (PENGUIN), to identify protein-protein interactions (PPI) in E-P interactions and apply it to our PrCa dataset. PENGUIN integrates chromatin interactions between a promoter and its enhancers defined by high-coverage H3K27ac-HiChIP data, with a tissue-specific PPI network inferred from DNA-binding motifs and refined with gene expression. Among a total of 4,314 E-P networks, PENGUIN performed unsupervised clustering. We functionally validated this clustering procedure by searching for enrichments of specific biological features. We first validated PENGUIN structural classification of E-P networks by showing a clear differential enrichment of the architectural protein CTCF. Next, and directly related to our PrCa case study, we observed that one of our 8 main clusters, containing 273 promoters, is particularly enriched for PrCA associated single nucleotide polymorphisms (SNPs) and oncogenes. Our approach proposes a mechanistic explanation for 208 PrCa SNPs falling either inside the binding sites of DNA-binding proteins (DBPs) or within genes encoding for intermediate proteins bridging E-P contacts. PENGUIN not only confirmed the relevance of key regulators in PrCa, but also identified new candidates for intervention, opening up new directions to identify molecular targets for disease treatment.

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Section: Resultsmentioning

confidence: 99%

The PENGUIN approach to reconstruct protein interactions at enhancer-promoter regions and its application to prostate cancer

Armaos

Serra

Núñez-Carpintero

et al. 2022

Preprint

View full text Add to dashboard Cite

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“…Previous studies have shown that WNT-pathway activation is associated with higher Gleason grades and PSA levels [ 13 ]. In addition, aberrant activation of the WNT pathway is causative to multiple cancer progression, which may be caused by mutations of pathway components or dyshomeostasis of autocrine/paracrine signaling [ 31 , 34 , 35 ]. Among them, functional mutations in WNT pathway components have been demonstrated to be important for progression and NHT resistance in mCRPC patients.…”

Section: Discussionmentioning

confidence: 99%

“…In other word, upstream components of the pathway may be responsible for the high frequency of WNT signal activation besides somatic mutations. Emerging evidence show WNT3A [ 37 , 38 ], WNT16B [ 39 ] and WNT5A [ 34 ] are essential in PCA for its initial, development, progression and therapy resistance, which may be autocrine or paracrine from stroma. In this study, higher WNT3A was detected in HOXB3 + tumors and was associated with higher tumor grade and stage.…”

Section: Discussionmentioning

confidence: 99%

HOXB3 drives WNT-activation associated progression in castration-resistant prostate cancer

et al. 2023

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Enabled resistance or innate insensitiveness to antiandrogen are lethal for castration-resistant prostate cancer (CRPC). Unfortunately, there seems to be little can be done to overcome the antiandrogen resistance because of the largely unknown mechanisms. In prospective cohort study, we found that HOXB3 protein level was an independent risk factor of PSA progression and death in patients with metastatic CRPC. In vivo, upregulated HOXB3 contributed to CRPC xenografts progression and abiraterone resistance. To uncover the mechanism of HOXB3 driving tumor progression, we performed RNA-sequencing in HOXB3 negative (HOXB3-) and HOXB3 high (HOXB3 + ) staining CRPC tumors and determined that HOXB3 activation was associated with the expression of WNT3A and enriched WNT pathway genes. Furthermore, extra WNT3A and APC deficiency led HOXB3 to be isolated from destruction-complex, translocated to nuclei, and then transcriptionally regulated multiple WNT pathway genes. What’s more, we also observed that the suppression of HOXB3 could reduce cell proliferation in APC-downregulated CRPC cells and sensitize APC-deficient CRPC xenografts to abiraterone again. Together, our data indicated that HOXB3 served as a downstream transcription factor of WNT pathway and defined a subgroup of CRPC resistant to antiandrogen which would benefit from HOXB3-targeted therapy.

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“…Recent work has shown that Wnt/β-catenin signaling not only promotes stem cell maintenance and invasive ability in mCRPC but also potentiates noncanonical Wnt5a -ROR1 signaling [ 255 ]. The non-canonical Wnt co-receptor ROR1 is elevated in several hematological and solid malignancies, particularly chemo-refractory disease [ 255 , 256 , 257 , 258 , 259 ]. Furthermore, the anti-ROR1 blocking antibody cirmtuzumab has shown efficacy in chronic lymphocytic leukemia (CLL) and mantle cell lymphoma (MCL) trials [ 247 ].…”

Section: Targeting the Wnt Cascade To Treat Prostate Cancermentioning

confidence: 99%

Exploring the Wnt Pathway as a Therapeutic Target for Prostate Cancer

et al. 2022

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Aberrant activation of the Wnt pathway is emerging as a frequent event during prostate cancer that can facilitate tumor formation, progression, and therapeutic resistance. Recent discoveries indicate that targeting the Wnt pathway to treat prostate cancer may be efficacious. However, the functional consequence of activating the Wnt pathway during the different stages of prostate cancer progression remains unclear. Preclinical work investigating the efficacy of targeting Wnt signaling for the treatment of prostate cancer, both in primary and metastatic lesions, and improving our molecular understanding of treatment responses is crucial to identifying effective treatment strategies and biomarkers that help guide treatment decisions and improve patient care. In this review, we outline the type of genetic alterations that lead to activated Wnt signaling in prostate cancer, highlight the range of laboratory models used to study the role of Wnt genetic drivers in prostate cancer, and discuss new mechanistic insights into how the Wnt cascade facilitates prostate cancer growth, metastasis, and drug resistance.

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Autocrine Canonical Wnt Signaling Primes Noncanonical Signaling through ROR1 in Metastatic Castration-Resistant Prostate Cancer

Cited by 19 publications

References 54 publications

The PENGUIN approach to reconstruct protein interactions at enhancer-promoter regions and its application to prostate cancer

The PENGUIN approach to reconstruct protein interactions at enhancer-promoter regions and its application to prostate cancer

HOXB3 drives WNT-activation associated progression in castration-resistant prostate cancer

Exploring the Wnt Pathway as a Therapeutic Target for Prostate Cancer

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