Skip to main content

Knockdown of PRKAR1A, the Gene Responsible for Carney Complex, Interferes With Differentiation in Osteoblastic Cells

Publication ,  Journal Article
Zhang, M; Manchanda, PK; Wu, D; Wang, Q; Kirschner, LS
Published in: Molecular Endocrinology
March 1, 2014

PRKAR1A is the gene encoding the type 1A regulatory subunit of protein kinase A, and it is the cause of the inherited human tumor syndrome Carney complex. Data from our laboratory has demonstrated that Prkar1a loss causes tumors in multiple cell lineages, including neural crest cells and osteoblasts. We have proposed that one mechanism by which tumorigenesis occurs is through the failure of terminal differentiation. In the present study, we directly test the effects of Prkar1a reduction on osteogenic differentiation in mouse and human cells in vitro. We found that Prkar1a levels noticeably increased during osteoblastic differentiation, indicating a positive correlation between the expression of Prkar1a and osteogenic potential. To validate this hypothesis, we generated stable Prkar1a knockdown in both mouse and human cells. These cells displayed significantly suppressed bone nodule formation and decreased expression of osteoblast markers such as osteocalcin and osteopontin. These observations imply that the antiosteogenic effect of Prkar1a ablation is not species or cell line specific. Furthermore, because Runt-related transcription factor-2 (Runx2) is a key mediator of osteoblast differentiation, we reasoned that the function of this transcription factor may be inhibited by Prkar1a knockdown. Chromatin immunoprecipitation and luciferase assays demonstrated that Prkar1a ablation repressed DNA binding and function of Runx2 at its target genes. Additionally, we determined that this effect is likely due to reductions in the Runx2-cooperating transcription factors forkhead box O1 and activating transcription factor 4. Taken together, this study provides direct evidence that ablation of Prkar1a interferes with signaling pathways necessary for osteoblast differentiation.

Duke Scholars

Published In

Molecular Endocrinology

DOI

EISSN

1944-9917

ISSN

0888-8809

Publication Date

March 1, 2014

Volume

28

Issue

3

Start / End Page

295 / 307

Publisher

The Endocrine Society

Related Subject Headings

  • Endocrinology & Metabolism
  • 3205 Medical biochemistry and metabolomics
  • 3102 Bioinformatics and computational biology
  • 11 Medical and Health Sciences
  • 07 Agricultural and Veterinary Sciences
  • 06 Biological Sciences
 

Citation

APA
Chicago
ICMJE
MLA
NLM
Zhang, M., Manchanda, P. K., Wu, D., Wang, Q., & Kirschner, L. S. (2014). Knockdown of PRKAR1A, the Gene Responsible for Carney Complex, Interferes With Differentiation in Osteoblastic Cells. Molecular Endocrinology, 28(3), 295–307. https://doi.org/10.1210/me.2013-1152
Zhang, Mei, Parmeet K. Manchanda, Dayong Wu, Qianben Wang, and Lawrence S. Kirschner. “Knockdown of PRKAR1A, the Gene Responsible for Carney Complex, Interferes With Differentiation in Osteoblastic Cells.” Molecular Endocrinology 28, no. 3 (March 1, 2014): 295–307. https://doi.org/10.1210/me.2013-1152.
Zhang M, Manchanda PK, Wu D, Wang Q, Kirschner LS. Knockdown of PRKAR1A, the Gene Responsible for Carney Complex, Interferes With Differentiation in Osteoblastic Cells. Molecular Endocrinology. 2014 Mar 1;28(3):295–307.
Zhang, Mei, et al. “Knockdown of PRKAR1A, the Gene Responsible for Carney Complex, Interferes With Differentiation in Osteoblastic Cells.” Molecular Endocrinology, vol. 28, no. 3, The Endocrine Society, Mar. 2014, pp. 295–307. Crossref, doi:10.1210/me.2013-1152.
Zhang M, Manchanda PK, Wu D, Wang Q, Kirschner LS. Knockdown of PRKAR1A, the Gene Responsible for Carney Complex, Interferes With Differentiation in Osteoblastic Cells. Molecular Endocrinology. The Endocrine Society; 2014 Mar 1;28(3):295–307.

Published In

Molecular Endocrinology

DOI

EISSN

1944-9917

ISSN

0888-8809

Publication Date

March 1, 2014

Volume

28

Issue

3

Start / End Page

295 / 307

Publisher

The Endocrine Society

Related Subject Headings

  • Endocrinology & Metabolism
  • 3205 Medical biochemistry and metabolomics
  • 3102 Bioinformatics and computational biology
  • 11 Medical and Health Sciences
  • 07 Agricultural and Veterinary Sciences
  • 06 Biological Sciences