Interleukin 17 drives vascular inflammation, endothelial dysfunction, and arterial hypertension in psoriasis-like skin disease.

نویسندگان

  • Susanne Karbach
  • Andrew L Croxford
  • Matthias Oelze
  • Rebecca Schüler
  • Daniel Minwegen
  • Joanna Wegner
  • Lija Koukes
  • Nir Yogev
  • Alexei Nikolaev
  • Sonja Reißig
  • Alexander Ullmann
  • Maike Knorr
  • Maximilian Waldner
  • Markus F Neurath
  • Huige Li
  • Zhixiong Wu
  • Christoph Brochhausen
  • Jürgen Scheller
  • Stefan Rose-John
  • Carolin Piotrowski
  • Ingo Bechmann
  • Markus Radsak
  • Philipp Wild
  • Andreas Daiber
  • Esther von Stebut
  • Philip Wenzel
  • Ari Waisman
  • Thomas Münzel
چکیده

OBJECTIVE Interleukin (IL)-17A is regarded as an important cytokine to drive psoriasis, an inflammatory skin disease marked by increased cardiovascular mortality. We aimed to test the hypothesis that overproduction of IL-17A in the skin leading to dermal inflammation may systemically cause vascular dysfunction in psoriasis-like skin disease. APPROACH AND RESULTS Conditional overexpression of IL-17A in keratinocytes caused severe psoriasis-like skin inflammation in mice (K14-IL-17A(ind/+) mice), associated with increased reactive oxygen species formation and circulating CD11b(+) inflammatory leukocytes in blood, with endothelial dysfunction, increased systolic blood pressure, left ventricular hypertrophy, and reduced survival compared with controls. In K14-IL-17A(ind/+) mice, immunohistochemistry and flow cytometry revealed increased vascular production of the nitric oxide/superoxide reaction product peroxynitrite and infiltration of the vasculature with myeloperoxidase(+)CD11b(+)GR1(+)F4/80(-) cells accompanied by increased expression of the inducible nitric oxide synthase and the nicotinamide dinucleotide phosphate (NADPH) oxidase, nox2. Neutrophil depletion by anti-GR-1 antibody injections reduced oxidative stress in blood and vessels. Neutralization of tumor necrosis factor-α and IL-6 (both downstream of IL-17A) reduced skin lesions, attenuated oxidative stress in heart and blood, and partially improved endothelial dysfunction in K14-IL-17A(ind/+) mice. CONCLUSIONS Dermal overexpression of IL-17A induces systemic endothelial dysfunction, vascular oxidative stress, arterial hypertension, and increases mortality mainly driven by myeloperoxidase(+)CD11b(+)GR1(+)F4/80(-) inflammatory cells. Depletion of the GR-1(+) immune cells or neutralization of IL-17A downstream cytokines by biologicals attenuates the vascular phenotype in K14-IL-17A(ind/+) mice.

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عنوان ژورنال:
  • Arteriosclerosis, thrombosis, and vascular biology

دوره 34 12  شماره 

صفحات  -

تاریخ انتشار 2014