Journal article

Loss of Prkar1a leads to Bcl-2 family protein induction and cachexia in mice

L Gangoda, M Doerflinger, R Srivastava, N Narayan, LE Edgington, J Orian, C Hawkins, LA O'Reilly, H Gu, M Bogyo, P Ekert, A Strasser, H Puthalakath

Cell Death and Differentiation | Published : 2014

DOI: 10.1038/cdd.2014.98

Abstract

Loss of function mutations in the Prkar1a gene are the cause of most cases of Carney complex disorder. Defects in Prkar1a are thought to cause hyper-activation of PKA signalling, which drives neoplastic transformation, and Prkar1a is therefore considered to be a tumour suppressor. Here we show that loss of Prkar1a in genetically modified mice caused transcriptional activation of several proapoptotic Bcl-2 family members and thereby caused cell death. Interestingly, combined loss of Bim and Prkar1a increased colony formation of fibroblasts in culture and promoted their growth as tumours in immune-deficient mice. Apart from inducing apoptosis, systemic deletion of Prkar1a caused cachexia with ..

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Grants

Awarded by National Cancer Institute

Funding Acknowledgements

We thank Anissa Jabbour, Liam O'Connor, Liz Milla, Philippe Bouillet, Ann Lin and Claretta D'Souza for reagents and advice and the LARTF staff for the care and maintenance of mice. LG is supported by CRC-BT and HP is supported by ARC Future Fellowship (FT0990683) and by ARC project grant (DP110100417). CH is supported by an ARC Future Fellowship (FT0991464).

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Keywords

Life Sciences & Biomedicine
3211 Oncology and Carcinogenesis
Rare Diseases
Cancer
Cardiac Myxomas
31 Biological Sciences
Mutations
Regulatory Subunit
Carney Complex
2.1 Biological and Endogenous Factors
Apoptotic Responses
Activation
Differentiation
Science & Technology
Cell Biology
3101 Biochemistry and Cell Biology
Tumors
Mediated Phosphorylation
Kinase-A Pka
Genetics
32 Biomedical and Clinical Sciences
Biochemistry & Molecular Biology