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Anti-Inflammatory Actions of Soluble Ninjurin-1 Ameliorate Atherosclerosis.
Jeon, Sejin; Kim, Tae Kyeong; Jeong, Se-Jin; Jung, In-Hyuk; Kim, Nayoung; Lee, Mi-Ni; Sonn, Seong-Keun; Seo, Seungwoon; Jin, Jing; Kweon, Hyae Yon; Kim, Sinai; Shim, Dahee; Park, Young Mi; Lee, Sang-Hak; Kim, Kyu-Won; Cybulsky, Myron I; Shim, Hyunbo; Roh, Tae-Young; Park, Woong-Yang; Lee, Hae-Ock; Choi, Jae-Hoon; Park, Sung Ho; Oh, Goo Taeg.
Afiliação
  • Jeon S; Immune and Vascular Cell Network Research Center, National Creative Initiatives, Department of Life Sciences (S.J., T.K.K., M.-N.L., S.-K.S., S.S., J.J., H.Y.K., S.K., G.T.O.), Ewha Womans University, Seoul, Korea.
  • Kim TK; Immune and Vascular Cell Network Research Center, National Creative Initiatives, Department of Life Sciences (S.J., T.K.K., M.-N.L., S.-K.S., S.S., J.J., H.Y.K., S.K., G.T.O.), Ewha Womans University, Seoul, Korea.
  • Jeong SJ; Cardiovascular Division, Department of Medicine, Washington University School of Medicine, St. Louis, MO (S.-J.J., I.-H.J.).
  • Jung IH; Cardiovascular Division, Department of Medicine, Washington University School of Medicine, St. Louis, MO (S.-J.J., I.-H.J.).
  • Kim N; Samsung Genome Institute, Samsung Medical Center, Seoul, Korea (N.K., W.-Y.P., H.-O.L.).
  • Lee MN; Department of Molecular Cell Biology, Sungkyunkwan University School of Medicine, Suwon, Korea (N.K., W.-Y.P., H.-O.L.).
  • Sonn SK; Immune and Vascular Cell Network Research Center, National Creative Initiatives, Department of Life Sciences (S.J., T.K.K., M.-N.L., S.-K.S., S.S., J.J., H.Y.K., S.K., G.T.O.), Ewha Womans University, Seoul, Korea.
  • Seo S; Immune and Vascular Cell Network Research Center, National Creative Initiatives, Department of Life Sciences (S.J., T.K.K., M.-N.L., S.-K.S., S.S., J.J., H.Y.K., S.K., G.T.O.), Ewha Womans University, Seoul, Korea.
  • Jin J; Immune and Vascular Cell Network Research Center, National Creative Initiatives, Department of Life Sciences (S.J., T.K.K., M.-N.L., S.-K.S., S.S., J.J., H.Y.K., S.K., G.T.O.), Ewha Womans University, Seoul, Korea.
  • Kweon HY; Immune and Vascular Cell Network Research Center, National Creative Initiatives, Department of Life Sciences (S.J., T.K.K., M.-N.L., S.-K.S., S.S., J.J., H.Y.K., S.K., G.T.O.), Ewha Womans University, Seoul, Korea.
  • Kim S; Immune and Vascular Cell Network Research Center, National Creative Initiatives, Department of Life Sciences (S.J., T.K.K., M.-N.L., S.-K.S., S.S., J.J., H.Y.K., S.K., G.T.O.), Ewha Womans University, Seoul, Korea.
  • Shim D; Immune and Vascular Cell Network Research Center, National Creative Initiatives, Department of Life Sciences (S.J., T.K.K., M.-N.L., S.-K.S., S.S., J.J., H.Y.K., S.K., G.T.O.), Ewha Womans University, Seoul, Korea.
  • Park YM; Department of Life Science, College of Natural Sciences, Research Institute for Natural Sciences, Hanyang University, Seoul, Korea (D.S., J.-H.C.).
  • Lee SH; Department of Molecular Medicine, Ewha Womans University School of Medicine, Seoul, Korea (Y.M.P.).
  • Kim KW; Division of Cardiology, Department of Internal Medicine, Yonsei University College of Medicine, Seoul, Korea (S.-H.L.).
  • Cybulsky MI; College of Pharmacy, Seoul National University, Seoul, Korea (K.-W.K.).
  • Shim H; Toronto General Hospital Research Institute, University Health Network, and Department of Laboratory Medicine and Pathobiology, University of Toronto, ON, Canada (M.I.C.).
  • Roh TY; Departments of Bioinspired Science and Life Science (H.S.), Ewha Womans University, Seoul, Korea.
  • Park WY; Department of Life Sciences, Pohang University of Science and Technology (POSTECH), Pohang, Korea (T.-Y.R.).
  • Lee HO; Samsung Genome Institute, Samsung Medical Center, Seoul, Korea (N.K., W.-Y.P., H.-O.L.).
  • Choi JH; Department of Molecular Cell Biology, Sungkyunkwan University School of Medicine, Suwon, Korea (N.K., W.-Y.P., H.-O.L.).
  • Park SH; Samsung Genome Institute, Samsung Medical Center, Seoul, Korea (N.K., W.-Y.P., H.-O.L.).
  • Oh GT; Department of Molecular Cell Biology, Sungkyunkwan University School of Medicine, Suwon, Korea (N.K., W.-Y.P., H.-O.L.).
Circulation ; 142(18): 1736-1751, 2020 11 03.
Article em En | MEDLINE | ID: mdl-32883094
ABSTRACT

BACKGROUND:

Macrophages produce many inflammation-associated molecules, released by matrix metalloproteinases, such as adhesion molecules, and cytokines, as well, which play a crucial role in atherosclerosis. In this context, we investigated the relationship between Ninjurin-1 (Ninj1 [nerve injury-induced protein]), a novel matrix metalloproteinase 9 substrate, expression, and atherosclerosis progression.

METHODS:

Ninj1 expression and atherosclerosis progression were assessed in atherosclerotic aortic tissue and serum samples from patients with coronary artery disease and healthy controls, and atheroprone apolipoprotein e-deficient (Apoe-/-) and wild-type mice, as well. Apoe-/- mice lacking systemic Ninj1 expression (Ninj1-/-Apoe-/-) were generated to assess the functional effects of Ninj1. Bone marrow transplantation was also used to generate low-density lipoprotein receptor-deficient (Ldlr-/-) mice that lack Ninj1 specifically in bone marrow-derived cells. Mice were fed a Western diet for 5 to 23 weeks, and atherosclerotic lesions were investigated. The anti-inflammatory role of Ninj1 was verified by treating macrophages and mice with the peptides Ninj11-56 (ML56) and Ninj126-37 (PN12), which mimic the soluble form of Ninj1 (sNinj1).

RESULTS:

Our in vivo results conclusively showed a correlation between Ninj1 expression in aortic macrophages and the extent of human and mouse atherosclerotic lesions. Ninj1-deficient macrophages promoted proinflammatory gene expression by activating mitogen-activated protein kinase and inhibiting the phosphoinositide 3-kinase/Akt signaling pathway. Whole-body and bone marrow-specific Ninj1 deficiencies significantly increased monocyte recruitment and macrophage accumulation in atherosclerotic lesions through elevated macrophage-mediated inflammation. Macrophage Ninj1 was directly cleaved by matrix metalloproteinase 9 to generate a soluble form that exhibited antiatherosclerotic effects, as assessed in vitro and in vivo. Treatment with the sNinj1-mimetic peptides, ML56 and PN12, reduced proinflammatory gene expression in human and mouse classically activated macrophages, thereby attenuating monocyte transendothelial migration. Moreover, continuous administration of mPN12 alleviated atherosclerosis by inhibiting the enhanced monocyte recruitment and inflammation characteristics of this disorder in mice, regardless of the presence of Ninj1.

CONCLUSIONS:

Ninj1 is a novel matrix metalloproteinase 9 substrate in macrophages, and sNinj1 is a secreted atheroprotective protein that regulates macrophage inflammation and monocyte recruitment in atherosclerosis. Moreover, sNinj1-mediated anti-inflammatory effects are conserved in human macrophages and likely contribute to human atherosclerosis.
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Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Transdução de Sinais / Moléculas de Adesão Celular Neuronais / Aterosclerose / Peptidomiméticos / Macrófagos / Anti-Inflamatórios / Fatores de Crescimento Neural Limite: Animals Idioma: En Revista: Circulation Ano de publicação: 2020 Tipo de documento: Article
Texto completo
Imprimir
XML
PubMed Links
Buscar no Google

Texto completo: 1 Coleções: 01-internacional Base de dados: MEDLINE Assunto principal: Transdução de Sinais / Moléculas de Adesão Celular Neuronais / Aterosclerose / Peptidomiméticos / Macrófagos / Anti-Inflamatórios / Fatores de Crescimento Neural Limite: Animals Idioma: En Revista: Circulation Ano de publicação: 2020 Tipo de documento: Article