4.6 Article

Antiangiogenic Synergism of Integrin-Targeted Fumagillin Nanoparticles and Atorvastatin in Atherosclerosis

Journal

JACC-CARDIOVASCULAR IMAGING
Volume 1, Issue 5, Pages 624-634

Publisher

ELSEVIER SCIENCE INC
DOI: 10.1016/j.jcmg.2008.06.003

Keywords

angiogenesis; molecular imaging; fumagillin; nanoparticle

Funding

  1. NCI NIH HHS [U54 CA136398, N01-CO-27031-16, U54 CA119342, U54 CA136398-010003, U54 CA119342-01, U54 CA119342-040001, CA-119342, N01-CO-37007] Funding Source: Medline
  2. NHLBI NIH HHS [R01 HL073646, HL-73646, R01 HL078631-04, HL-78631, R01 HL078631-03, R01 HL073646-01A1, R01 HL078631-01, R01 HL078631, R01 HL078631-02] Funding Source: Medline
  3. NIAID NIH HHS [N01CO37007] Funding Source: Medline
  4. NIBIB NIH HHS [R01 EB001704-01, EB-01704, R01 EB001704-04, R01 EB001704] Funding Source: Medline
  5. NINDS NIH HHS [R01 NS059302-01, R01 NS059302, R01 NS059302-02] Funding Source: Medline
  6. NATIONAL CANCER INSTITUTE [U54CA136398, U54CA119342] Funding Source: NIH RePORTER
  7. NATIONAL HEART, LUNG, AND BLOOD INSTITUTE [R01HL078631, R01HL073646] Funding Source: NIH RePORTER
  8. NATIONAL INSTITUTE OF BIOMEDICAL IMAGING AND BIOENGINEERING [R01EB001704] Funding Source: NIH RePORTER
  9. NATIONAL INSTITUTE OF NEUROLOGICAL DISORDERS AND STROKE [R01NS059302] Funding Source: NIH RePORTER

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OBJECTIVES Studies were performed to develop a prolonged antiangiogenesis therapy regimen based on theranostic alpha(nu)beta(3)-targeted nanoparticles. BACKGROUND Antiangiogenesis therapy may normalize atherosclerotic plaque vasculature and promote plaque stabilization. alpha(nu)beta(3)-targeted paramagnetic nanoparticles can quantify atherosclerotic angiogenesis and incorporate fumagillin to elicit acute antiangiogenic effects. METHODS In the first experiment, hyperlipidemic rabbits received alpha(nu)beta(3)-targeted fumagillin nanoparticles (0, 30, or 90 mu g/kg) with either a continued high fat diet or conversion to standard chow. The antiangiogenic response was followed for 4 weeks by cardiac magnetic resonance (CMR) molecular imaging with alpha(nu)beta(3)-targeted paramagnetic nanoparticles. In a second 8-week study, atherosclerotic rabbits received atorvastatin (0 or 44 mg/kg diet) alone or with alpha(nu)beta(3)-targeted fumagillin nanoparticles (only week 0 vs. weeks 0 and 4), and angiogenesis was monitored with CMR molecular imaging. Histology was performed to determine the location of bound nanoparticles and to correlate the level of CMR enhancement with the density of angiogenic vessels. RESULTS The alpha(nu)beta(3)-targeted fumagillin nanoparticles reduced the neovascular signal by 50% to 75% at 1 week and maintained this effect for 3 weeks regardless of diet and drug dose. In the second study, atherosclerotic rabbits receiving statin alone had no antineovascular benefit over 8 weeks. The alpha(nu)beta(3)-targeted fumagillin nanoparticles decreased aortic angiogenesis for 3 weeks as in study 1, and readministration on week 4 reproduced the 3-week antineovascular response with no carry-over benefit. However, atorvastatin and 2 doses of alpha(nu)beta(3)-targeted fumagillin nanoparticles (0 and 4 weeks) achieved marked and sustainable antiangiogenesis. Microscopic studies corroborated the high correlation between CMR signal and neovessel counts and confirmed that the alpha(nu)beta(3)-targeted nanoparticles were constrained to the vasculature of the aortic adventia. CONCLUSIONS The CMR molecular imaging with alpha(nu)beta(3)-targeted paramagnetic nanoparticles demonstrated that the acute antiangiogenic effects of alpha(nu)beta(3)-targeted fumagillin nanoparticles could be prolonged when combined with atorvastatin, representing a potential strategy to evaluate antiangiogenic treatment and plaque stability. (J Am Coll Cardiol Img 2008; 1: 624-34) c 2008 by the American College of Cardiology Foundation

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