2016

DOI: 10.6061/clinics/2016(08)05

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Treatment of patients with aortic atherosclerotic disease with paclitaxel-associated lipid nanoparticles

Afonso Akio Shiozaki

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,

Aleksandra Tiemi Morikawa

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et al.

Abstract: OBJECTIVE:The toxicity of anti-cancer chemotherapeutic agents can be reduced by associating these compounds, such as the anti-proliferative agent paclitaxel, with a cholesterol-rich nanoemulsion (LDE) that mimics the lipid composition of low-density lipoprotein (LDL). When injected into circulation, the LDE concentrates the carried drugs in neoplastic tissues and atherosclerotic lesions. In rabbits, atherosclerotic lesion size was reduced by 65% following LDE-paclitaxel treatment. The current study aimed to te… Show more

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Nanoparticle-mediated Drug Delivery For Restenosis Preventio3

Nanopartícula Lipídica Artificial (Lde)1

Controle (N=9) Lde-dtx (N=9)1

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Cited by 38 publications

(28 citation statements)

References 22 publications

(29 reference statements)

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“…These qualities are determined by the nanoparticle size ( Walkey et al, 2012 ; Tan et al, 2013 ), surface properties ( Walkey et al, 2012 ), particle geometry ( Tan et al, 2013 ), shear stress and flow rate in the blood vessel ( Klingberg et al, 2015 ), and drug release kinetics ( Panyam and Labhasetwar, 2004 ). Many different materials have been used for fabricating drug-eluting nanoparticles, including synthetic polymers [reviewed in ( Wang et al, 2016 )], lipoproteins [reviewed in ( Damiano et al, 2013 ; Harisa and Alanazi, 2014 )], lipids ( Shiozaki et al, 2016 ), and metals ( Weakley et al, 2011 ). Different materials and design criteria may be needed depending on the type of drug to be released, and the intended target of the nanoparticle.…”

Section: Nanoparticle-mediated Drug Delivery For Restenosis Preventiomentioning

confidence: 99%

“…Intravenously injected lipid nanoparticles loaded with the drug carmustine successfully decreased lesion area by reducing SMC proliferation, secretion of inflammatory factors, and macrophage burden in rabbits ( Daminelli et al, 2016 ). Shiozaki et al (2016) recently published a pilot clinical study where cholesterol-rich non-protein nano-emulsion (LDE) particles, which resemble low-density lipoproteins, were loaded with paclitaxel oleate. When delivered systemically via intravenous injection, the nanoparticles were able to reduce total plaque in patients, though the difference was not significant ( Shiozaki et al, 2016 ).…”

Section: Nanoparticle-mediated Drug Delivery For Restenosis Preventiomentioning

confidence: 99%

“… Shiozaki et al (2016) recently published a pilot clinical study where cholesterol-rich non-protein nano-emulsion (LDE) particles, which resemble low-density lipoproteins, were loaded with paclitaxel oleate. When delivered systemically via intravenous injection, the nanoparticles were able to reduce total plaque in patients, though the difference was not significant ( Shiozaki et al, 2016 ).…”

Section: Nanoparticle-mediated Drug Delivery For Restenosis Preventiomentioning

confidence: 99%

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Targeted Delivery of Bioactive Molecules for Vascular Intervention and Tissue Engineering

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²

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³

et al. 2018

Front. Pharmacol.

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Cardiovascular diseases are the leading cause of death in the United States. Treatment often requires surgical interventions to re-open occluded vessels, bypass severe occlusions, or stabilize aneurysms. Despite the short-term success of such interventions, many ultimately fail due to thrombosis or restenosis (following stent placement), or incomplete healing (such as after aneurysm coil placement). Bioactive molecules capable of modulating host tissue responses and preventing these complications have been identified, but systemic delivery is often harmful or ineffective. This review discusses the use of localized bioactive molecule delivery methods to enhance the long-term success of vascular interventions, such as drug-eluting stents and aneurysm coils, as well as nanoparticles for targeted molecule delivery. Vascular grafts in particular have poor patency in small diameter, high flow applications, such as coronary artery bypass grafting (CABG). Grafts fabricated from a variety of approaches may benefit from bioactive molecule incorporation to improve patency. Tissue engineering is an especially promising approach for vascular graft fabrication that may be conducive to incorporation of drugs or growth factors. Overall, localized and targeted delivery of bioactive molecules has shown promise for improving the outcomes of vascular interventions, with technologies such as drug-eluting stents showing excellent clinical success. However, many targeted vascular drug delivery systems have yet to reach the clinic. There is still a need to better optimize bioactive molecule release kinetics and identify synergistic biomolecule combinations before the clinical impact of these technologies can be realized.

“…These qualities are determined by the nanoparticle size ( Walkey et al, 2012 ; Tan et al, 2013 ), surface properties ( Walkey et al, 2012 ), particle geometry ( Tan et al, 2013 ), shear stress and flow rate in the blood vessel ( Klingberg et al, 2015 ), and drug release kinetics ( Panyam and Labhasetwar, 2004 ). Many different materials have been used for fabricating drug-eluting nanoparticles, including synthetic polymers [reviewed in ( Wang et al, 2016 )], lipoproteins [reviewed in ( Damiano et al, 2013 ; Harisa and Alanazi, 2014 )], lipids ( Shiozaki et al, 2016 ), and metals ( Weakley et al, 2011 ). Different materials and design criteria may be needed depending on the type of drug to be released, and the intended target of the nanoparticle.…”

Section: Nanoparticle-mediated Drug Delivery For Restenosis Preventiomentioning

confidence: 99%

“…Intravenously injected lipid nanoparticles loaded with the drug carmustine successfully decreased lesion area by reducing SMC proliferation, secretion of inflammatory factors, and macrophage burden in rabbits ( Daminelli et al, 2016 ). Shiozaki et al (2016) recently published a pilot clinical study where cholesterol-rich non-protein nano-emulsion (LDE) particles, which resemble low-density lipoproteins, were loaded with paclitaxel oleate. When delivered systemically via intravenous injection, the nanoparticles were able to reduce total plaque in patients, though the difference was not significant ( Shiozaki et al, 2016 ).…”

Section: Nanoparticle-mediated Drug Delivery For Restenosis Preventiomentioning

confidence: 99%

“… Shiozaki et al (2016) recently published a pilot clinical study where cholesterol-rich non-protein nano-emulsion (LDE) particles, which resemble low-density lipoproteins, were loaded with paclitaxel oleate. When delivered systemically via intravenous injection, the nanoparticles were able to reduce total plaque in patients, though the difference was not significant ( Shiozaki et al, 2016 ).…”

Section: Nanoparticle-mediated Drug Delivery For Restenosis Preventiomentioning

confidence: 99%

See 1 more Smart Citation

Targeted Delivery of Bioactive Molecules for Vascular Intervention and Tissue Engineering

¹

,

²

,

³

et al. 2018

Front. Pharmacol.

View full text Add to dashboard Cite

Cardiovascular diseases are the leading cause of death in the United States. Treatment often requires surgical interventions to re-open occluded vessels, bypass severe occlusions, or stabilize aneurysms. Despite the short-term success of such interventions, many ultimately fail due to thrombosis or restenosis (following stent placement), or incomplete healing (such as after aneurysm coil placement). Bioactive molecules capable of modulating host tissue responses and preventing these complications have been identified, but systemic delivery is often harmful or ineffective. This review discusses the use of localized bioactive molecule delivery methods to enhance the long-term success of vascular interventions, such as drug-eluting stents and aneurysm coils, as well as nanoparticles for targeted molecule delivery. Vascular grafts in particular have poor patency in small diameter, high flow applications, such as coronary artery bypass grafting (CABG). Grafts fabricated from a variety of approaches may benefit from bioactive molecule incorporation to improve patency. Tissue engineering is an especially promising approach for vascular graft fabrication that may be conducive to incorporation of drugs or growth factors. Overall, localized and targeted delivery of bioactive molecules has shown promise for improving the outcomes of vascular interventions, with technologies such as drug-eluting stents showing excellent clinical success. However, many targeted vascular drug delivery systems have yet to reach the clinic. There is still a need to better optimize bioactive molecule release kinetics and identify synergistic biomolecule combinations before the clinical impact of these technologies can be realized.

“…Em trabalhos subsequentes, foi demonstrado que outro quimioterápico associado à LDE, o etoposídeo, também reduziu as lesões ateroscleróticas em coelhos em 85% (Tavares et al, 2011). Em pacientes com doença arterial coronária e aterosclerose, também foi observado que a LDE é captada por segmentos arteriais e reduziu as lesões ateroscleróticas (Couto et al, 2003;Shiozaki et al, 2016).…”

Section: Nanopartícula Lipídica Artificial (Lde)unclassified

Efeito do tratamento crônico do metotrexato associado à nanoemulsão de LDE no remodelamento cardíaco por infarto do miocárdio em ratos Wistar

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Agradecimentos"Há pessoas que nos falam e nem as escutamos; há pessoas que nos ferem e nem cicatrizes deixam, mas há pessoas que simplesmente aparecem em nossa vida e nos marcam para sempre." Cecília Meireles Ao meu orientador, Prof. Dr. Raul Cavalcante Maranhão, pela oportunidade em realizar os meus sonhos e por acreditar em mim.A todos os funcionários do Laboratório de Metabolismo de Lípides do Incor, principalmente, Dra. Fátima e Dra. Priscila, pelo suporte na realização deste trabalho e pelos momentos de descontração durante o tão apreciado café.À Dra Maria Carolina Guido, pela contribuição durante o trabalho. A todos os companheiros de pós-graduação do Laboratório deMetabolismo de Lípides pelo suporte e amizade.À Neusa Rodrigues Dini e todas as funcionárias da secretaria de pós-graduação, pelo apoio em tornar esse sonho possível. À Profa. Dra. Vera Maria Cury Salemi, pela realização e análise dos ecocardiogramas.Ao Dr. Marcelo Dantas Tavares de Melo, pela análise dos ecocardiogramas. Aos funcionários do Serviço de Apoio à Pesquisa e ExperimentaçãoAnimal do Incor, pela assistência e cuidado com os animais. À CAPES (Coordenação de Aperfeiçoamento de Pessoal de NívelSuperior), pela bolsa de doutorado e de doutorado-sanduíche realizado na Boston University, possibilitando a publicação de um artigo.À minha irmã Ariane, pelo carinho, cuidado e por ser o meu pilar em momentos difíceis. Acute myocardial infarction (AMI) is the main cause of worldwide mortality. Normalização adotadaAMI is accompanied by cardiac remodeling, characterized by genetic, molecular and cellular alterations, with consequent changes in the size, shape and function of the heart, resulting in ventricular dysfunction and heart failure. Experimental and clinical evidence indicate that prevention or treatment of cardiac remodeling benefits the ventricular function. LDE is a lipid nanoparticle with a structure similar to low density lipoprotein (LDL). LDE

“…A associação do paclitaxel à LDE praticamente elimina a toxicidade clínica e laboratorial desta droga, como demonstrado em animais experimentais e em estudos com pacientes com cânceres avançados. A viabilidade e segurança do tratamento com esta formulação também foi comprovada em um estudo piloto envolvendo pacientes com ateromas aórticos (Maranhão et al, 2008;Shiozaki et al, 2016;Graziani et al, 2017).…”

Section: Controle (N=9) Lde-dtx (N=9)unclassified

Uso de nanopartícula lipídica como veículo do quimioterápico docetaxel no tratamento da aterosclerose induzida em coelhos

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Meneghini C.B. Use of lipid core nanoparticle as a vehicle of the chemotherapeutic docetaxel in the treatment of atherosclerosis induced in rabbits [thesis]. São Paulo: "Faculdade de Medicina, Universidade de São Paulo"; 2018. Considered as a new strategy of targeting drugs to injured tissues, LDE, a lipid core nanoparticle concentrates on inflammatory sites with high cell proliferation rates, as atherosclerotic lesions, and it is used as a vehicle for drugs in experimental models and in humans. Docetaxel (DTX), an antiproliferative chemotherapeutic agent has not been explored yet in the treatment of atherosclerosis. New Zealand white male rabbits were fed with 1% cholesterol diet throughout the 8-week experimental period to induce atherosclerosis. After 4 weeks, the animals were treated weekly with LDE-DTX (n=9) at a dose of 1mg/kg i.p. or only with LDE (Control group, n=9). We evaluated feed intake, lipid, hematological, and weight profiles during the protocol at baseline, 4 weeks and post-treatment. After euthanasia was performed morphological analysis and Western blot of the aorta. As expected, total cholesterol increased 42-fold in both groups comparing baseline to post-treatment. There was a decrease in red blood cells number in both groups but it is probably not treatment-related. There was no hepatic and renal treatment-related toxicity.

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