Inhibition of signaling downstream of beta-2 adrenoceptor by propranolol in prostate cancer cells

Aljoharah Alaskar; Amaal Abdulraqeb Ali; Sazzad Hassan; Zakia Shinwari; Ayodele Alaiya; Urs von Holzen; Lance Miller; George Kulik

doi:10.1002/pros.24455

Inhibition of signaling downstream of beta-2 adrenoceptor by propranolol in prostate cancer cells

Prostate. 2023 Feb;83(3):237-245. doi: 10.1002/pros.24455. Epub 2022 Nov 14.

Authors

Aljoharah Alaskar¹, Amaal Abdulraqeb Ali¹, Sazzad Hassan², Zakia Shinwari³, Ayodele Alaiya³, Urs von Holzen^{2

4}, Lance Miller^{5

6}, George Kulik^{1

5

6}

Affiliations

¹ Department of Life Sciences and Life Sciences Program, Alfaisal University, Riyadh, Saudi Arabia.
² Indiana University School of Medicine-South Bend, South Bend, Indiana, USA.
³ Stem Cell & Tissue Re-Engineering Program, King Faisal Specialist Hospital and Research Centre, Riyadh, Saudi Arabia.
⁴ Goshen Center for Cancer Care, Goshen, Indiana, USA.
⁵ Department of Cancer Biology, Comprehensive Cancer Center, Winston-Salem, North Carolina, USA.
⁶ Department of Urology, Wake Forest University Health Sciences, Winston-Salem, North Carolina, USA.

Abstract

Background: There is accumulating evidence that propranolol, an antagonist of beta-1 and beta-2 adrenoreceptors, extends survival of patients with prostate cancer; yet it is not known whether propranolol inhibits beta-adrenergic signaling in prostate cancer cells, or systemic effects of propranolol play the leading role in slowing down cancer progression. Recently initiated clinical studies offer a possibility to test whether administration of propranolol inhibits signaling pathways in prostate tumors, however, there is limited information on the dynamics of signaling pathways activated downstream of beta-2 adrenoreceptors in prostate cancer cells and on the inactivation of these pathways upon propranolol administration.

Methods: Western blot analysis was used to test the effects of epinephrine and propranolol on activation of protein kinase (PKA) signaling in mouse prostates and PKA, extracellular signal-regulated kinase (ERK), and protein kinase B/AKT (AKT) signaling in prostate cancer cell lines.

Results: In prostate cancer cell lines epinephrine induced robust phosphorylation of PKA substrates pS133CREB and pS157VASP that was evident 2 min after treatments and lasted for 3-6 h. Epinephrine induced phosphorylation of AKT in PTEN-positive 22Rv1 cells, whereas changes of constitutive AKT phosphorylation were minimal in PTEN-negative PC3, C42, and LNCaP cells. A modest short-term increase of pERK in response to epinephrine was observed in all tested cell lines. Incubation of prostate cancer cells with 10-fold molar excess of propranolol for 30 min inhibited all downstream pathways activated by epinephrine. Subjecting mice to immobilization stress induced phosphorylation of S133CREB, whereas injection of propranolol at 1.5 mg/kg prevented the stress-induced phosphorylation.

Conclusions: The analysis of pS133CREB and pS157VASP allows measuring activation of PKA signaling downstream of beta-2 adrenoreceptors. Presented results on the ratio of propranolol/epinephrine and the time needed to inhibit signaling downstream of beta-2 adrenoreceptors will help to design clinical studies that examine the effects of propranolol on prostate tumors.

Keywords: PKA; beta-2 adrenoreceptors; epinephrine; propranolol; prostate cancer; stress.

Publication types

Research Support, N.I.H., Extramural
Research Support, Non-U.S. Gov't

MeSH terms

Animals
Epinephrine / metabolism
Epinephrine / pharmacology
Humans
Male
Mice
Phosphorylation
Propranolol* / metabolism
Propranolol* / pharmacology
Prostate / pathology
Prostatic Neoplasms* / pathology
Proto-Oncogene Proteins c-akt / metabolism

Substances

Propranolol
Proto-Oncogene Proteins c-akt
Epinephrine

Grants and funding

P30 CA012197/CA/NCI NIH HHS/United States