Journal article
The β2-adrenergic receptor is a molecular switch for neuroendocrine transdifferentiation of prostate cancer cells
- Abstract:
- The incidence of treatment-related neuroendocrine (NE) prostate cancer (t-NEPC) is rising as more potent drugs targeting the androgen signaling axis are clinically implemented. Neuroendocrine transdifferentiation (NEtD), an putative initial step in t-NEPC development, is induced by androgen deprivation therapy (ADT) or anti-androgens, and by activation of the β2-adrenergic receptor (ADRB2) in prostate cancer cell lines. Thus, understanding whether ADRB2 is involved in ADT-initiated NEtD may assist in developing treatment strategies that can prevent or reverse t-NEPC emergence, thereby prolonging therapeutic responses. Here we found that in primary, treatment-naïve prostate cancers, ADRB2 mRNA was positively correlated with expression of luminal differentiation markers, and ADRB2 protein levels were inversely correlated with Gleason grade. ADRB2 mRNA was upregulated in metastatic prostate cancer, and progressively downregulated during androgen deprivation therapy (ADT) and t-NEPC emergence. In androgen-deprivated medium, high ADRB2 was required for LNCaP cells to undergo NEtD, measured as increased neurite outgrowth and expression of neuron differentiation and NE genes. ADRB2 overexpression induced an NE-like morphology in both AR positive and -negative prostate cancer cell lines. ADRB2 downregulation in LNCaP cells increased canonical Wnt signaling, and GSK3α/β inhibition reduced the expression of neuron differentiation and NE genes. In LNCaP xenografts, more pronounced castration-induced NEtD was observed in tumors derived from high than low-ADRB2 cells. In conclusion, high ADRB2 expression is required for ADT-induced NEtD, characterized by ADRB2 downregulation and t-NEPC emergence. Implications: This data suggest a potential application of β-blockers to prevent cancer cells committed to a neuroendocrine lineage from evolving into t-NEPC.
- Publication status:
- Published
- Peer review status:
- Peer reviewed
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- Files:
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-
(Preview, Accepted manuscript, pdf, 4.9MB, Terms of use)
-
- Publisher copy:
- 10.1158/1541-7786.mcr-18-0605
Authors
- Publisher:
- American Association of Cancer Research
- Journal:
- Molecular Cancer Research More from this journal
- Volume:
- 17
- Issue:
- 11
- Pages:
- 2154-2168
- Publication date:
- 2019-08-08
- Acceptance date:
- 2019-07-10
- DOI:
- EISSN:
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1557-3125
- ISSN:
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1541-7786
- Pmid:
-
31395667
- Language:
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English
- Keywords:
- Pubs id:
-
pubs:1041741
- UUID:
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uuid:f1d0a133-6c4f-4757-b6f7-8c140b68f3f2
- Local pid:
-
pubs:1041741
- Source identifiers:
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1041741
- Deposit date:
-
2019-08-10
Terms of use
- Copyright holder:
- AACR
- Copyright date:
- 2019
- Rights statement:
- © 2019 American Association for Cancer Research.
- Notes:
- This is the accepted manuscript version of the article. The final version is available from AACR Publication at: http://dx.doi.org/10.1158/1541-7786.mcr-18-0605
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