Anti-JNK2 peptide-siRNA nanostructures improve plaque endothelium and reduce thrombotic risk in atherosclerotic mice

被引：16

作者：

Pan, Hua ^{[1
]}

Palekar, Rohun U. ^{[2
]}

Hou, Kirk K. ^{[3
]}

Bacon, John ^{[2
]}

Yan, Huimin ^{[3
]}

Springer, Luke E. ^{[3
]}

Akk, Antonina ^{[3
]}

Yang, Lihua ^{[3
]}

Miller, Mark J. ^{[3
]}

Pham, Christine T. N. ^{[3
]}

Schlesinger, Paul H. ^{[3
]}

Wickline, Samuel A. ^{[1
]}

机构：

[1] Univ S Florida, USF Hlth Heart Inst, Morsani Coll Med, Dept Cardiovasc Sci,USF Hlth, 12901 Bruce B Downs Blvd MDC36, Tampa, FL 33612 USA

[2] Washington Univ, Dept Med, St Louis, MO USA

[3] Washington Univ, Dept Biomed Engn, St Louis, MO USA

来源：

INTERNATIONAL JOURNAL OF NANOMEDICINE | 2018年 / 13卷

基金：

美国国家卫生研究院;

关键词：

siRNA; JNK2; peptide nanoparticles; perfluorocarbon nanoparticles; macrophages; atherosclerosis; plaque; ApoE(-/-) mice; thrombosis; endothelium; erosions; scavenger receptors; NF-KAPPA-B; LOW-DENSITY-LIPOPROTEIN; MELITTIN-DERIVED PEPTIDES; COLONY-STIMULATING FACTOR; HUMAN CORONARY-ARTERIES; E-DEFICIENT MICE; PATHOPHYSIOLOGICAL SIGNIFICANCE; PERFLUOROCARBON NANOPARTICLES; INTIMAL NEOVASCULARIZATION; MACROPHAGE ACCUMULATION;

D O I：

10.2147/IJN.S168556

中图分类号：

TB3 [工程材料学];

学科分类号：

0805 ; 080502 ;

摘要：

Background: A direct and independent role of inflammation in atherothrombosis was recently highlighted by the Canakinumab Antiinflammatory Thrombosis Outcome Study (CANTOS) trial, showing the benefit of inhibiting signaling molecules, eg, interleukins. Accordingly, we sought to devise a flexible platform for preventing the inflammatory drivers at their source to preserve plaque endothelium and mitigate procoagulant risk. Methods: p5RHH-siRNA nanoparticles were formulated through self-assembly processes. The therapeutic efficacy of p5RHH-JNK2 siRNA nanoparticles was evaluated both in vitro and in vivo. Results: Because JNK2 is critical to macrophage uptake of oxidized lipids through scavenger receptors that engender expression of myriad inflammatory molecules, we designed an RNA-silencing approach based on peptide-siRNA nanoparticles (p5RHH-siRNA) that localize to atherosclerotic plaques exhibiting disrupted endothelial barriers to achieve control of JNK2 expression by macrophages. After seven doses of p5RHH-JNK2 siRNA nanoparticles over 3.5 weeks in ApoE(-/-) mice on a Western diet, both JNK2 mRNA and protein levels were significantly decreased by 26% (P=0.044) and 42% (P=0.042), respectively. Plaque-macrophage populations were markedly depleted and NF kappa B and STAT3-signaling pathways inhibited by 47% (P<0.001) and 46% (P=0.004), respectively. Endothelial barrier integrity was restored (2.6-fold reduced permeability to circulating 200 nm nanoparticles in vivo, P=0.003) and thrombotic risk attenuated (200% increased clotting times to carotid artery injury, P=0.02), despite blood-cholesterol levels persistently exceeding 1,000 mg/dL. No adaptive or innate immunoresponses toward the nanoparticles were observed, and blood tests after the completion of treatment confirmed the largely nontoxic nature of this approach. Conclusion: The ability to formulate these nanostructures rapidly and easily interchange or multiplex their oligonucleotide content represents a promising approach for controlling deleterious signaling events locally in advanced atherosclerosis.

引用

页码：5187 / 5205

页数：19