Target‐Selective Drug Delivery through Liposomes Labeled with Oligobranched Neurotensin Peptides

Falciani, Chiara; Accardo, Antonella; Brunetti, Jlenia; Tesauro, Diego; Lelli, Barbara; Pini, Alessandro; Bracci, Luisa; Morelli, Giancarlo

doi:10.1002/cmdc.201000463

Cited by 44 publications

(62 citation statements)

References 30 publications

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“…38,39 Previous studies have described the influence of PEG loading on targeting properties in vivo; 7 therefore, it was decided to investigate this behavior in vitro with RLPs carrying varying amounts of PEG. In vitro binding to isolated α v β 3 integrin receptors revealed the highest binding when no PEG building block was used ( Figure 3) and binding decreased with higher PEG loading of the RLPs.…”

Section: Discussionmentioning

confidence: 99%

Influence of PEGylation and RGD loading on the targeting properties of radiolabeled liposomal nanoparticles

Rangger¹,

Helbok²,

Guggenberg³

et al. 2012

IJN

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Purpose: Liposomes have been proposed to be a means of selectively targeting cancer sites for diagnostic and therapeutic applications. The focus of this work was the evaluation of radiolabeled PEGylated liposomes derivatized with varying amounts of a cyclic arginyl-glycyl-aspartic acid (RGD) peptide. RGD peptides are known to bind to α v β 3 integrin receptors overexpressed during tumor-induced angiogenesis. Methods: Several liposomal nanoparticles carrying the RGD peptide targeting sequence (RLPs) were synthesized using a combination of 1-palmitoyl-2-oleoyl-sn-glycero-3-phosphocholine, cholesterol, diethylenetriaminepentaacetic acid-derivatized lipids for radiolabeling, a polyethylene glycol (PEG) building block, and a lipid-based RGD building block. Relative amounts of RGD and PEG building blocks were varied. In vitro binding affinities were determined using isolated α v β 3 integrin receptors incubated with different concentrations of RLPs in competition with iodine-125-labeled cyclo-(-RGDyV-). Binding of the indium-111-labeled RLPs was also evaluated. Biodistribution and micro single photon emission computed tomography/computed tomography imaging studies were performed in nude mice using different tumor xenograft models. Results: RLPs were labeled with indium-111 with high radiochemical yields. In vitro binding studies of RLPs with different RGD/PEG loading revealed good binding to isolated receptors, which was dependent on the extent of RGD and PEG loading. Binding increased with higher RGD loading, whereas reduced binding was found with higher PEG loading. Biodistribution showed increased circulating time for PEGylated RLPs, but no dependence on RGD loading. Both biodistribution and micro single photon emission computed tomography/computed tomography imaging studies revealed low, nonspecific tumor uptake values. Conclusion: In this study, RLPs for targeting angiogenesis were described. Even though good binding to α v β 3 integrin receptors was found in vitro, the balance between PEGylation and RGD loading clearly requires optimization to achieve targeting in vivo. These data form the basis for future development and provide a platform for the investigation of multimodal approaches.

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Section: Discussionmentioning

confidence: 99%

Influence of PEGylation and RGD loading on the targeting properties of radiolabeled liposomal nanoparticles

Rangger¹,

Helbok²,

Guggenberg³

et al. 2012

IJN

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“…[16][17][18] Recently, some evidence that these properties are also maintained when the peptide is bounded on the external liposomal surface have been demonstrated. 19,20 Liposomes were chosen as the vector since they can accommodate large quantities of relevant therapeutic drugs in their lumen. Moreover, the addition of a large amount of the amphiphilic gadolinium complex (C18) 2 DTPA(Gd) to the liposomal formulation allows its use a potential contrast agent for magnetic resonance imaging (MRI).…”

Section: Ringhieri Et Almentioning

confidence: 99%

Liposomes derivatized with multimeric copies of KCCYSL peptide as targeting agents for HER-2-overexpressing tumor cells

Ringhieri¹,

Mannucci²,

Conti³

et al. 2017

IJN

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Mixed liposomes, obtained by coaggregation of 1,2-dioleoyl-sn-glycero-3-phosphocholine and of the synthetic monomer containing a gadolinium complex ([C18]2DTPA[Gd]) have been prepared. Liposomes externally decorated with KCCYSL (P6.1 peptide) sequence in its monomeric, dimeric, and tetrameric forms are studied as target-selective delivery systems toward cancer cells overexpressing human epidermal growth factor receptor-2 (HER-2) receptors. Derivatization of liposomal surface with targeting peptides is achieved using the postmodification method: the alkyne-peptide derivative Pra-KCCYSL reacts, through click chemistry procedures, with a synthetic surfactant modified with 1, 2, or 4 azido moieties previously inserted in liposome formulation. Preliminary in vitro data on MDA-MB-231 and BT-474 cells indicated that liposomes functionalized with P6.1 peptide in its tetrameric form had better binding to and uptake into BT-474 cells compared to liposomes decorated with monomeric or dimeric versions of the P6.1 peptide. BT-474 cells treated with liposomes functionalized with the tetrameric form of P6.1 showed high degree of liposome uptake, which was comparable with the uptake of anti-HER-2 antibodies such as Herceptin. Moreover, magnetic MRI experiments have demonstrated the potential of liposomes to act as MRI contrast agents

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“…108 Functionalization with neurotensin peptides significantly improved the ability of liposomes to deliver chemotherapeutics into CRC cells and resulted in a four fold increase in cytotoxicity. 109 Her2 and VEGFR are overexpressed in many cancer types including gastric cancer 110 and CRC. 111 Anti-Her2 and anti-VEGFR immunoliposomes provide a novel tool for safe and efficient immnochemotherapy of Her2 or VEGFR positive GI cancers.…”

Section: Active Targeting Liposomesmentioning

confidence: 99%

Application of liposomes in drug development – focus on gastroenterological targets

Zhang¹,

Wang²,

Mao³

et al. 2013

IJN

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Over the past decade, liposomes became a focal point in developing drug delivery systems. New liposomes, with novel lipid molecules or conjugates, and new formulations opened possibilities for safely and efficiently treating many diseases including cancers. New types of liposomes can prolong circulation time or specifically deliver drugs to therapeutic targets. This article concentrates on current developments in liposome based drug delivery systems for treating diseases of the gastrointestinal tract. We will review different types and uses of liposomes in the development of therapeutics for gastrointestinal diseases including inflammatory bowel diseases and colorectal cancer.

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Target‐Selective Drug Delivery through Liposomes Labeled with Oligobranched Neurotensin Peptides

Cited by 44 publications

References 30 publications

Influence of PEGylation and RGD loading on the targeting properties of radiolabeled liposomal nanoparticles

Influence of PEGylation and RGD loading on the targeting properties of radiolabeled liposomal nanoparticles

Liposomes derivatized with multimeric copies of KCCYSL peptide as targeting agents for HER-2-overexpressing tumor cells

Application of liposomes in drug development – focus on gastroenterological targets

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Target‐Selective Drug Delivery through Liposomes Labeled with Oligobranched Neurotensin Peptides

Cited by 44 publications

References 30 publications

Influence of PEGylation and RGD loading on the targeting properties of radiolabeled liposomal nanoparticles

Influence of PEGylation and RGD loading on the targeting properties of radiolabeled liposomal nanoparticles

Liposomes derivatized with multimeric copies of KCCYSL peptide as targeting agents for HER-2-overexpressing tumor cells

Application of liposomes in drug development &ndash; focus on gastroenterological targets

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Application of liposomes in drug development – focus on gastroenterological targets