AI Article Synopsis

  • - PKA and PP1 are critical proteins in various signaling pathways and can be inhibited by DARPP-32; this study looked into their expression in over 1,100 breast cancer tumors to see how they relate to patient outcomes.
  • - Low levels of PKA protein were linked to poorer survival rates in breast cancer patients, especially among those with estrogen receptor-positive tumors, while PP1 expression did not show a similar association.
  • - Additionally, analysis of mRNA levels in a separate dataset revealed specific subunits of PKA and PP1 related to cancer survival, highlighting their potential roles in influencing breast cancer prognosis.

Article Abstract

Cyclic AMP-dependent protein kinase A (PKA) and protein phosphatase 1 (PP1) are proteins involved in numerous essential signalling pathways that modulate physiological and pathological functions. Both PP1 and PKA can be inhibited by dopamine- and cAMP-regulated phosphoprotein 32 kD (DARPP-32). Using immunohistochemistry, PKA and PP1 expression was determined in a large primary breast tumour cohort to evaluate associations between clinical outcome and clinicopathological criteria (n > 1100). In addition, mRNA expression of PKA and PP1 subunits was assessed in the METABRIC data set (n = 1980). Low protein expression of PKA was significantly associated with adverse survival of breast cancer patients; interestingly, this relationship was stronger in ER-positive breast cancer patients. PP1 protein expression was not associated with patient survival. PKA and PP1 subunit mRNA was also assessed; PPP1CA, PRKACG and PRKAR1B were associated with breast cancer-specific survival. In patients with high expression of DARPP-32, low expression of PP1 was associated with adverse survival when compared to high expression in the same group. PKA expression and PP1 expression are of significant interest in cancer as they are involved in a wide array of cellular processes, and these data indicate PKA and PP1 may play an important role in patient outcome.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8178272PMC
http://dx.doi.org/10.1111/jcmm.16447DOI Listing

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