Matricellular protein CCN3 mitigates abdominal aortic aneurysm
Chao Zhang, … , Domenick A. Prosdocimo, Zhiyong Lin
Chao Zhang, … , Domenick A. Prosdocimo, Zhiyong Lin
Published March 14, 2016
Citation Information: J Clin Invest. 2016;126(4):1282-1299. https://doi.org/10.1172/JCI82337.
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Research Article Vascular biology

Matricellular protein CCN3 mitigates abdominal aortic aneurysm

Abstract

Abdominal aortic aneurysm (AAA) is a major cause of morbidity and mortality; however, the mechanisms that are involved in disease initiation and progression are incompletely understood. Extracellular matrix proteins play an integral role in modulating vascular homeostasis in health and disease. Here, we determined that the expression of the matricellular protein CCN3 is strongly reduced in rodent AAA models, including angiotensin II–induced AAA and elastase perfusion–stimulated AAA. CCN3 levels were also reduced in human AAA biopsies compared with those in controls. In murine models of induced AAA, germline deletion of Ccn3 resulted in severe phenotypes characterized by elastin fragmentation, vessel dilation, vascular inflammation, dissection, heightened ROS generation, and smooth muscle cell loss. Conversely, overexpression of CCN3 mitigated both elastase- and angiotensin II–induced AAA formation in mice. BM transplantation experiments suggested that the AAA phenotype of CCN3-deficient mice is intrinsic to the vasculature, as AAA was not exacerbated in WT animals that received CCN3-deficient BM and WT BM did not reduce AAA severity in CCN3-deficient mice. Genetic and pharmacological approaches implicated the ERK1/2 pathway as a critical regulator of CCN3-dependent AAA development. Together, these results demonstrate that CCN3 is a nodal regulator in AAA biology and identify CCN3 as a potential therapeutic target for vascular disease.

Authors

Chao Zhang, Dustin van der Voort, Hong Shi, Rongli Zhang, Yulan Qing, Shuichi Hiraoka, Minoru Takemoto, Koutaro Yokote, Joseph V. Moxon, Paul Norman, Laure Rittié, Helena Kuivaniemi, G. Brandon Atkins, Stanton L. Gerson, Guo-Ping Shi, Jonathan Golledge, Nianguo Dong, Bernard Perbal, Domenick A. Prosdocimo, Zhiyong Lin

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Figure 7

ERK1/2 activation by Ang II is increased in CCN3-deficient aorta.

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ERK1/2 activation by Ang II is increased in CCN3-deficient aorta. (A) Im...
(A) Immunohistochemistry assessment of ERK1/2 activation in CCN3-deficient aortae in response to Ang II treatment (7 days and 4 weeks). Representative images are shown on the left; results are quantified on the right. n = 3–5 per group. Scale bars: 100 μm. (B) Western blot of phospho-ERK1/2 in aortae following saline or Ang II treatment (4 weeks). n = 4 for saline group; n = 6–8 for Ang II group. (C) Western blot of phospho-ERK1/2 and phospho-MEK1/2 in aortae following saline or Ang II treatment (7 days). n = 4 for saline group, n = 6–8 for Ang II group. (D) Western blot of phospho-ERK1/2 and phospho-MEK1/2 in aortic SMCs following Ang II (30 minutes) treatment. n = 3 for WT, n = 4 for KO. T-ERK1/2, total ERK1/2; T-MEK1/2, total MEK1/2. Two-way ANOVA followed by Bonferroni’s post-hoc correction was used.