β2-adrenoreceptor Signaling Increases Therapy Resistance in Prostate Cancer by Upregulating MCL1.
Sazzad HassanAshok K PullikuthKyle C NelsonAnabel FloresYelena KarpovaDaniele BaizSinan ZhuGuangchao SuiYue HuangYoung A ChoiRalph D'AgostinoAshok HemalUrs von HolzenWaldemar DebinskiGeorge KulikPublished in: Molecular cancer research : MCR (2020)
There is accumulating evidence that continuous activation of the sympathetic nervous system due to psychosocial stress increases resistance to therapy and accelerates tumor growth via β2-adrenoreceptor signaling (ADRB2). However, the effector mechanisms appear to be specific to tumor type. Here we show that activation of ADRB2 by epinephrine, increased in response to immobilization stress, delays the loss of MCL1 apoptosis regulator (MCL1) protein expression induced by cytotoxic drugs in prostate cancer cells; and thus, increases resistance of prostate cancer xenografts to cytotoxic therapies. The effect of epinephrine on MCL1 protein depended on protein kinase A (PKA) activity, but was independent from androgen receptor expression. Furthermore, elevated blood epinephrine levels correlated positively with an increased MCL1 protein expression in human prostate biopsies. In summary, we demonstrate that stress triggers an androgen-independent antiapoptotic signaling via the ADRB2/PKA/MCL1 pathway in prostate cancer cells. IMPLICATIONS: Presented results justify clinical studies of ADRB2 blockers as therapeutics and of MCL1 protein expression as potential biomarker predicting efficacy of apoptosis-targeting drugs in prostate cancer.
Keyphrases
- prostate cancer
- radical prostatectomy
- oxidative stress
- endothelial cells
- endoplasmic reticulum stress
- cell death
- cell cycle arrest
- mental health
- stress induced
- transcription factor
- stem cells
- regulatory t cells
- dendritic cells
- signaling pathway
- angiotensin ii
- binding protein
- immune response
- smoking cessation
- drug induced
- angiotensin converting enzyme