| Literature DB >> 27524614 |
Omary Chillo1, Eike Christian Kleinert1, Thomas Lautz1, Manuel Lasch1, Judith-Irina Pagel2, Yvonn Heun1, Kerstin Troidl3, Silvia Fischer4, Amelia Caballero-Martinez1, Annika Mauer5, Angela R M Kurz1, Gerald Assmann6, Markus Rehberg7, Sandip M Kanse8, Bernhard Nieswandt9, Barbara Walzog1, Christoph A Reichel10, Hanna Mannell1, Klaus T Preissner4, Elisabeth Deindl11.
Abstract
The body has the capacity to compensate for an occluded artery by creating a natural bypass upon increased fluid shear stress. How this mechanical force is translated into collateral artery growth (arteriogenesis) is unresolved. We show that extravasation of neutrophils mediated by the platelet receptor GPIbα and uPA results in Nox2-derived reactive oxygen radicals, which activate perivascular mast cells. These c-kit(+)/CXCR-4(+) cells stimulate arteriogenesis by recruiting additional neutrophils as well as growth-promoting monocytes and T cells. Additionally, mast cells may directly contribute to vascular remodeling and vascular cell proliferation through increased MMP activity and by supplying growth-promoting factors. Boosting mast cell recruitment and activation effectively promotes arteriogenesis, thereby protecting tissue from severe ischemic damage. We thus find that perivascular mast cells are central regulators of shear stress-induced arteriogenesis by orchestrating leukocyte function and growth factor/cytokine release, thus providing a therapeutic target for treatment of vascular occlusive diseases.Entities:
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Year: 2016 PMID: 27524614 DOI: 10.1016/j.celrep.2016.07.040
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423