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Literature DB >> 32426057

Targeting Dysfunctional Vascular Endothelial Cells Using Immunoliposomes Under Flow Conditions.

Mahsa Kheradmandi¹, Ian Ackers^2,3, Monica M Burdick^1,3, Ramiro Malgor^2,3, Amir M Farnoud^1,3.

Abstract

INTRODUCTION: Atherosclerosis (ATH), the build up of fat in the arteries, is a principal cause of heart attack and stroke. Drug instability and lack of target specificity are major drawbacks of current clinical therapeutics. These undesirable effects can be eliminated by site-specific drug delivery. The endothelial surface over ATH lesions has been shown to overexpress vascular cell adhesion molecule1 (VCAM1), which can be used for targeted therapy.
METHODS: Here, we report the synthesis, characterization, and development of anti VCAM1-functionalized liposomes to target cells overexpressing VCAM1 under static and flow conditions. Liposomes were composed of dioleoyl-phosphatidylcholine, sphingomyelin, cholesterol, and distearoyl-phosphatidylethanolamine-polyethylene glycol-cyanur (31.67:31.67:31.67:5 mol%). VCAM1 expression in endothelial cells was induced by lipopolysaccharide (LPS) treatment.
RESULTS: Characterization study revealed that liposomes were negatively charged (- 7.7 ± 2.6 mV) with an average diameter of 201.3 ± 3.3 nm. Liposomes showed no toxicity toward THP-1 derived macrophages and endothelial cells. Liposomes were able to target both fixed and non-fixed endothelial cells, in vitro, with significantly higher localization observed in non-fixed conditions. To mimic biological and physiologically-relevant conditions, liposome targeting was also examined under flow (4 dyn/cm2) with or without erythrocytes (40% v/v hematocrit). Liposomes were able to target LPS-treated endothelial cells under dynamic culture, in the presence or absence of erythrocytes, although targeting efficiency was five-fold lower in flow compared to static conditions.
CONCLUSIONS: This liposomal delivery system showed a significant improvement in localization on dysfunctional endothelium after surface functionalization. We conclude that VCAM1-functionalized liposomes can target and potentially deliver therapeutic compounds to ATH regions. © Biomedical Engineering Society 2020.

Entities: Chemical

Keywords: Atherosclerosis; Cell adhesion molecules; Drug delivery; Endothelium; Nanomedicine

Year: 2020 PMID： 32426057 PMCID： PMC7225235 DOI： 10.1007/s12195-020-00616-1

Source DB: PubMed Journal: Cell Mol Bioeng ISSN： 1865-5025 Impact factor: 2.321

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References

44 in total

1. Immobilized platelets support human colon carcinoma cell tethering, rolling, and firm adhesion under dynamic flow conditions.

Authors: O J McCarty; S A Mousa; P F Bray; K Konstantopoulos
Journal: Blood Date: 2000-09-01 Impact factor: 22.113

2. Influence of Red Blood Cells on Nanoparticle Targeted Delivery in Microcirculation.

Authors: Jifu Tan; Antony Thomas; Yaling Liu
Journal: Soft Matter Date: 2011-12-22 Impact factor: 3.679

3. Effect of flow on endothelial endocytosis of nanocarriers targeted to ICAM-1.

Authors: Tridib Bhowmick; Erik Berk; Xiumin Cui; Vladimir R Muzykantov; Silvia Muro
Journal: J Control Release Date: 2011-09-16 Impact factor: 9.776

4. Heart Disease and Stroke Statistics-2019 Update: A Report From the American Heart Association.

Authors: Emelia J Benjamin; Paul Muntner; Alvaro Alonso; Marcio S Bittencourt; Clifton W Callaway; April P Carson; Alanna M Chamberlain; Alexander R Chang; Susan Cheng; Sandeep R Das; Francesca N Delling; Luc Djousse; Mitchell S V Elkind; Jane F Ferguson; Myriam Fornage; Lori Chaffin Jordan; Sadiya S Khan; Brett M Kissela; Kristen L Knutson; Tak W Kwan; Daniel T Lackland; Tené T Lewis; Judith H Lichtman; Chris T Longenecker; Matthew Shane Loop; Pamela L Lutsey; Seth S Martin; Kunihiro Matsushita; Andrew E Moran; Michael E Mussolino; Martin O'Flaherty; Ambarish Pandey; Amanda M Perak; Wayne D Rosamond; Gregory A Roth; Uchechukwu K A Sampson; Gary M Satou; Emily B Schroeder; Svati H Shah; Nicole L Spartano; Andrew Stokes; David L Tirschwell; Connie W Tsao; Mintu P Turakhia; Lisa B VanWagner; John T Wilkins; Sally S Wong; Salim S Virani
Journal: Circulation Date: 2019-03-05 Impact factor: 29.690

5. Endothelial alpha(v)beta3 integrin-targeted fumagillin nanoparticles inhibit angiogenesis in atherosclerosis.

Authors: Patrick M Winter; Anne M Neubauer; Shelton D Caruthers; Thomas D Harris; J David Robertson; Todd A Williams; Anne H Schmieder; Grace Hu; John S Allen; Elizabeth K Lacy; Huiying Zhang; Samuel A Wickline; Gregory M Lanza
Journal: Arterioscler Thromb Vasc Biol Date: 2006-07-06 Impact factor: 8.311

Targeting Dysfunctional Vascular Endothelial Cells Using Immunoliposomes Under Flow Conditions.

1. Immobilized platelets support human colon carcinoma cell tethering, rolling, and firm adhesion under dynamic flow conditions.

2. Influence of Red Blood Cells on Nanoparticle Targeted Delivery in Microcirculation.

3. Effect of flow on endothelial endocytosis of nanocarriers targeted to ICAM-1.

4. Heart Disease and Stroke Statistics-2019 Update: A Report From the American Heart Association.

5. Endothelial alpha(v)beta3 integrin-targeted fumagillin nanoparticles inhibit angiogenesis in atherosclerosis.

6. Targetability of novel immunoliposomes prepared by a new antibody conjugation technique.

7. VCAM-1 directed immunoliposomes selectively target tumor vasculature in vivo.

8. Chitosan oligosaccharide (COS) inhibits LPS-induced inflammatory effects in RAW 264.7 macrophage cells.

Review 9. Immune and inflammatory mechanisms of atherosclerosis (*).

10. ICAM-1 regulates macrophage polarization by suppressing MCP-1 expression via miR-124 upregulation.