A20 inhibits post-angioplasty restenosis by blocking macrophage trafficking and decreasing adventitial neovascularization

Damrauer, Scott M.; Fisher, Mark D.; Wada, Hiromi; Siracuse, Jeffrey J.; Silva, Cleide G. da; Moon, Karam; Csizmadia, Eva; Maccariello, Elizabeth; Patel, Virendra I.; Studer, Peter; Essayagh, Sanah; Aird, William C.; Daniel, Soizic; Ferran, Christiane

doi:10.1016/j.atherosclerosis.2010.03.029

Cited by 26 publications

(26 citation statements)

References 29 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…A very small percentage of these cells is Ki67 positive (f, arrowhead). (Scale bar 50 µm, magnification ×400) late-stage NH (Damrauer et al 2010). The total number of macrophages in the intima has been found to correlate with the degree of stenosis and was very high in our samples even at 6 months after implantation as shown by KiM1P/ CD68 positivity (Figs.…”

Section: Discussionmentioning

confidence: 70%

“…The role of chronic inflammation, however, remains unclear, but is not supported by our results. Early infiltrates of CD8-positive T helper cells might be the mainspring, whereas other studies favor VSMC-monocyte interaction (Damrauer et al 2010;Johnson et al 2000;Miller et al 1993). The absence of prominent immune cell infiltrates, but sweepingly the presence of monocytes at least at later points of time, might explain the relative ineffectiveness of immunosuppressive drugs in order to prolong bypass patency further emphasized by the unique morphology of allogen and autologous bypass material (Carpenter and Tomaszewski 1998).…”

Section: Discussionmentioning

confidence: 95%

See 1 more Smart Citation

Neointimal hyperplasia in allogeneic and autologous venous grafts is not different in nature

Albert

Hartmann

Wagner

et al. 2015

Histochem Cell Biol

View full text Add to dashboard Cite

Neointimal hyperplasia, transplant rejection and thus immunogenicity of allografts are possible reasons for poorer patency rates in cryopreserved venous allografts for peripheral bypass surgery in comparison with autologous venous grafts. To expand the limited knowledge from human allografts, we histologically investigated allogeneic and autologous venous grafts in arterial location. Specimens of allogeneic and autologous venous graft stenosis, harvested 6 months after bypass implantation, were immunohistochemically characterized. Examination of the lesions showed a uniform morphological pattern. A continuous endothelial layer, tissue fibrosis and a thickened neointima with monocytes and dedifferentiated vascular smooth muscle cells were seen in both conduits with very low cell turnover and the absence of acute and chronic inflammation. Neoangiogenesis with CD34-positive endothelium was abundant in the vessel media. The morphological patterns of allogeneic and autologous neointima formation are similar. Consequently, neointimal hyperplasia in venous grafts may reflect a uniform physiological host response of non-immunological factors with the reasons for poorer clinical outcome of cryopreserved allografts yet to be elucidated.

show abstract

Section: Discussionmentioning

confidence: 70%

Section: Discussionmentioning

confidence: 95%

Neointimal hyperplasia in allogeneic and autologous venous grafts is not different in nature

Albert

Hartmann

Wagner

et al. 2015

Histochem Cell Biol

View full text Add to dashboard Cite

show abstract

“…Those stem from its potent antiinflammatory function in EC and SMC through inhibition of NF-B activation (8,9). They also rely on its NF-B-independent anti-apoptotic, anti-oxidative, and immunomodulatory functions in EC (10 -12) and anti-proliferative and pro-apoptotic (only neointimal SMC) functions in SMC (9,(13)(14)(15). However, the impact of A20 on pro-atherogenic IFN␥ signaling in EC and SMC had never been explored.…”

Section: Ifn␥ Typically Secreted By Th1 and Natural Killer (Nk)mentioning

confidence: 99%

A20 Regulates Atherogenic Interferon (IFN)-γ Signaling in Vascular Cells by Modulating Basal IFNβ Levels

Moll

Lee

Minussi

et al. 2014

Journal of Biological Chemistry

Self Cite

View full text Add to dashboard Cite

Background: IFN␥ signaling is a major culprit in occlusive vascular disease. Results: The anti-inflammatory protein A20 negatively regulates IFN␥ signaling in vascular cells in vitro and in vivo. Conclusion: A20 impacts IFN␥ signaling by modulating basal IFN␤ and downstream STAT1 expression. Significance: This novel function of A20 supports its promise as a therapeutic target and prognostic marker for atherosclerotic disease.

show abstract

“…Heightened NF-κB activation in SMC is also involved in their phenotypic switch from contractile to synthetic and proliferative(44–46). Inhibiting SMC proliferation is therefore a sound therapeutic strategy to counteract TA, and we had convincingly reported that overexpression of A20 inhibits SMC proliferation both in vitro(9), and in rodent models of IH, including TA(5, 9, 16, 47, 48). Conversely, our data indicate that A20 knockdown in allografts associates with a significant increase in the proliferation rate of SMC.…”

Section: Discussionmentioning

confidence: 99%

“…For immunohistochemistry (IHC) analysis, frozen sections were incubated with antibodies to VCAM-1, ICAM-1, CD4, CD8 (BD Biosciences, San Jose, CA), NK cells (R&D Systems Inc. Minneapolis, MN) and Ki-67 (ThermoFisher, Tewksubury, MA) followed by biotinylated secondary antibodies (Vector, Burlingame, CA)(16). Adventitial CD4, CD8, and NK positive cells were scored by cell counting using Image J, and expressed as cell number per vessel section.…”

Section: Methodsmentioning

confidence: 99%

A20 Haploinsufficiency Aggravates Transplant Arteriosclerosis in Mouse Vascular Allografts

et al. 2016

Self Cite

View full text Add to dashboard Cite

Background Inflammation is central to the pathogenesis of transplant arteriosclerosis (TA). We questioned whether physiologic levels of anti-inflammatory A20 influence TA severity. Methods We performed major histocompatibility complex (MHC) mismatched aorta to carotid artery interposition grafts, using wild type (WT) or A20 heterozygote (HET) C57BL/6 (H-2b) donors and BALB/c (H-2d) recipients, and conversely BALB/c donors and WT/HET recipients. We analyzed aortic allografts by histology, immunohistochemistry, immunofluorescence, and gene profiling (qPCR). We validated select in vivo A20 targets in human and mouse smooth muscle cell (SMC) cultures. Results We noted significantly greater intimal hyperplasia in HET vs. WT allografts, indicating aggravated TA. Inadequate upregulation of A20 in HET allografts after transplantation was associated with excessive NF-κB activation, gauged by higher levels of IκBα, p65, VCAM-1, ICAM-1, CXCL10, CCL2, TNF, and IL-6 (mostly localized to SMC). Correspondingly, cytokine-induced upregulation of TNF and IL-6 in human and mouse SMC cultures inversely correlated with A20 expression. Aggravated TA in HET vs. WT allografts correlated with increased intimal SMC proliferation, and a higher number of infiltrating IFNγ+ and Granzyme B+ CD4+ T cells and natural killer cells, and lower number of FoxP3+ regulatory T cells. A20 haploinsufficiency in allograft recipients did not influence TA. Conclusions A20 haploinsufficiency in vascular allografts aggravates lesions of TA by exacerbating inflammation, SMC proliferation, and infiltration of pathogenic T cells. A20 single nucleotide polymorphisms (SNPs) associating with lower A20 expression or function in donors of vascularized allografts may inform risk and severity of TA, highlighting the clinical implications of our findings.

show abstract

A20 inhibits post-angioplasty restenosis by blocking macrophage trafficking and decreasing adventitial neovascularization

Cited by 26 publications

References 29 publications

Neointimal hyperplasia in allogeneic and autologous venous grafts is not different in nature

Neointimal hyperplasia in allogeneic and autologous venous grafts is not different in nature

A20 Regulates Atherogenic Interferon (IFN)-γ Signaling in Vascular Cells by Modulating Basal IFNβ Levels

A20 Haploinsufficiency Aggravates Transplant Arteriosclerosis in Mouse Vascular Allografts

Contact Info

Product

Resources

About