Céline Dubuis scite author profile

tissues, except at a very low concentration (0.044 ng/mg) in the liver, suggesting a very low risk 50 of systemic toxicity of locally delivered ATV. Additionally, the ex vivo data showed that ATV in 51 solution permeates through isolated human saphenous veins and thus is a good candidate for 52 perivascular delivery. 53Our data demonstrate that a local biphasic ATV release on the mice ligated carotid 54 efficiently prevents the development of IH without apparent toxicity. 55 56

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Atorvastatin-Loaded Hydrogel Affects the Smooth Muscle Cells of Human Veins

Dubuis

May

Alonso

et al. 2013

J Pharmacol Exp Ther

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Intimal hyperplasia (IH) is the major cause of stenosis of vein grafts. Drugs such as statins prevent stenosis, but their systemic administration has limited effects. We developed a hyaluronic acid hydrogel matrix, which ensures a controlled release of atorvastatin (ATV) at the site of injury. The release kinetics demonstrated that 100% of ATV was released over 10 hours, independent of the loading concentration of the hydrogel. We investigated the effects of such a delivery on primary vascular smooth muscle cells isolated from human veins. ATV decreased the proliferation, migration, and passage of human smooth muscle cells (HSMCs) across a matrix barrier in a similar dose-dependent (5-10 mM) and time-dependent manner (24-72 hours), whether the drug was directly added to the culture medium or released from the hydrogel. Expression analysis of genes known to be involved in the development of IH demonstrated that the transcripts of both the gap junction protein connexin43 (Cx43) and plasminogen activator inhibitor-1 (PAI-1) were decreased after a 24-48-hour exposure to the hydrogel loaded with ATV, whereas the transcripts of the heme oxygenase (HO-1) and the inhibitor of tissue plasminogen activator were increased. At the protein level, Cx43, PAI-1, and metalloproteinase-9 expression were decreased, whereas HO-1 was upregulated in the presence of ATV. The data demonstrate that ATV released from a hydrogel has effects on HSMCs similar to the drug being freely dissolved in the environment.

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Céline Dubuis

Hydrogen sulfide-releasing peptide hydrogel limits the development of intimal hyperplasia in human vein segments

Connexin37 reduces smooth muscle cell proliferation and intimal hyperplasia in a mouse model of carotid artery ligation

The use of external mesh reinforcement to reduce intimal hyperplasia and preserve the structure of human saphenous veins

Perivascular sustained release of atorvastatin from a hydrogel-microparticle delivery system decreases intimal hyperplasia

Atorvastatin-Loaded Hydrogel Affects the Smooth Muscle Cells of Human Veins

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