| Literature DB >> 28692064 |
Guillermo de Cárcer1, Paulina Wachowicz1, Sara Martínez-Martínez2,3, Jorge Oller2,3, Nerea Méndez-Barbero2, Beatriz Escobar1, Alejandra González-Loyola1, Tohru Takaki4, Aicha El Bakkali1, Juan A Cámara5, Luis J Jiménez-Borreguero3,6, Xosé R Bustelo7,8, Marta Cañamero9, Francisca Mulero5, María de Los Ángeles Sevilla10,8, María Jose Montero10,8, Juan Miguel Redondo2,3, Marcos Malumbres1.
Abstract
Polo-like kinase 1 (PLK1), an essential regulator of cell division, is currently undergoing clinical evaluation as a target for cancer therapy. We report an unexpected function of Plk1 in sustaining cardiovascular homeostasis. Plk1 haploinsufficiency in mice did not induce obvious cell proliferation defects but did result in arterial structural alterations, which frequently led to aortic rupture and death. Specific ablation of Plk1 in vascular smooth muscle cells (VSMCs) led to reduced arterial elasticity, hypotension, and an impaired arterial response to angiotensin II in vivo. Mechanistically, we found that Plk1 regulated angiotensin II-dependent activation of RhoA and actomyosin dynamics in VSMCs in a mitosis-independent manner. This regulation depended on Plk1 kinase activity, and the administration of small-molecule Plk1 inhibitors to angiotensin II-treated mice led to reduced arterial fitness and an elevated risk of aneurysm and aortic rupture. We thus conclude that a partial reduction of Plk1 activity that does not block cell division can nevertheless impair aortic homeostasis. Our findings have potentially important implications for current approaches aimed at PLK1 inhibition for cancer therapy.Entities:
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Year: 2017 PMID: 28692064 DOI: 10.1038/nm.4364
Source DB: PubMed Journal: Nat Med ISSN: 1078-8956 Impact factor: 53.440