Rho kinase proteins display aberrant upregulation in vascular tumors and contribute to vascular tumor growth

Clarissa N Amaya; Dianne C Mitchell; Brad A Bryan

doi:10.1186/s12885-017-3470-7

Rho kinase proteins display aberrant upregulation in vascular tumors and contribute to vascular tumor growth

BMC Cancer. 2017 Jul 14;17(1):485. doi: 10.1186/s12885-017-3470-7.

Authors

Clarissa N Amaya¹, Dianne C Mitchell², Brad A Bryan^{3

4}

Affiliations

¹ Department of Biomedical Sciences, Texas Tech University Health Sciences Center, Paul L. Foster School of Medicine, Center of Excellence in Cancer Research, 5001 El Paso Drive, MSB1 Room 2111, El Paso, TX, 79905, USA.
² Minerva Genetics, 5130 Gateway Blvd East, Suite 315, El Paso, TX, 79905, USA.
³ Department of Biomedical Sciences, Texas Tech University Health Sciences Center, Paul L. Foster School of Medicine, Center of Excellence in Cancer Research, 5001 El Paso Drive, MSB1 Room 2111, El Paso, TX, 79905, USA. brad.bryan@ttuhsc.edu.
⁴ Minerva Genetics, 5130 Gateway Blvd East, Suite 315, El Paso, TX, 79905, USA. brad.bryan@ttuhsc.edu.

Abstract

Background: The serine/threonine protein kinases ROCK1 and 2 are key RhoA-mediated regulators of cell shape and cytoskeletal dynamics. These proteins perform multiple functions in vascular endothelial cell physiology and are attractive targets for cancer therapy based on their roles as oncogenes and metastatic promoters. Given their critical functions in both of these processes, we hypothesized that molecular targeting of ROCK proteins would be exceedingly effective against vascular tumors such as hemangiomas and angiosarcomas, which are neoplasms composed of aberrant endothelial cells.

Methods: In this study, we compared ROCK1 and 2 protein expression in a large panel of benign and malignant vascular tumors to that of normal vasculature. We then utilized shRNA technology to knockdown the expression of ROCK1 and 2 in SVR tumor-forming vascular cells, and evaluated tumor size and proliferation rate in a xenograft model. Finally, we employed proteomics and metabolomics to assess how knockdown of the ROCK paralogs induced alterations in protein expression/phosphorylation and metabolite concentrations in the xenograft tumors.

Results: Our findings revealed that ROCK1 was overexpressed in malignant vascular tumors such as hemangioendotheliomas and angiosarcomas, and ROCK2 was overexpressed in both benign and malignant vascular tumors including hemangiomas, hemangioendotheliomas, hemangiopericytomas, and angiosarcomas. shRNA-mediated knockdown of ROCK2, but not ROCK1, in xenograft vascular tumors significantly reduced tumor size and proliferative index compared to control tumors. Proteomics and metabolomics analysis of the xenograft tumors revealed both overlapping as well as unique roles for the ROCK paralogs in regulating signal transduction and metabolite concentrations.

Conclusions: Collectively, these data indicate that ROCK proteins are overexpressed in diverse vascular tumors and suggest that specific targeting of ROCK2 proteins may show efficacy against malignant vascular tumors.

Keywords: Angiosarcoma; Hemangioendothelioma; Hemangioma; Hemangiopericytoma; Rho kinase; Rock; Vascular sarcoma; shRNA.

MeSH terms

Animals
Endothelial Cells / metabolism
Endothelial Cells / pathology
Gene Expression Regulation, Neoplastic
Humans
Mice
Neoplasms / genetics*
Neoplasms / pathology
RNA, Small Interfering / genetics
Signal Transduction / genetics
Transcriptional Activation / genetics
Vascular Neoplasms / classification
Vascular Neoplasms / genetics*
Vascular Neoplasms / pathology
Xenograft Model Antitumor Assays
rho-Associated Kinases / genetics*

Substances

RNA, Small Interfering
ROCK1 protein, human
ROCK2 protein, human
rho-Associated Kinases

Grants and funding

R15 HL098931/HL/NHLBI NIH HHS/United States