Peptide‐labeled supramolecular aggregates as selective doxorubicin carriers for delivery to tumor cells

Salsano

Morisco

et al. 2012

IJN

Self Cite

Objectives: Drug delivery systems consisting of liposomes displaying a cell surface receptor-targeting peptide are being developed to specifically deliver chemotherapeutic drugs to tumors overexpressing a target receptor. This study addresses novel liposome composition approaches to specifically target tissues overexpressing bombesin (BN) receptors. Methods: A new amphiphilic peptide derivative (MonY-BN) containing the BN(7-14) peptide, the DTPA (diethylenetriaminepentaacetate) chelating agent, a hydrophobic moiety with two C 18 alkyl chains, and polyethylene glycol spacers, has been synthesized by solid-phase methods. Liposomes have been generated by co-aggregation of MonY-BN with 1,2-distearoyl-sn-glycero-3-phosphocholine (DSPC). The structural and biological properties of these new target-selective drug-delivery systems have been characterized. Results: Liposomes with a DSPC/MonY-BN (97/3 molar ratio) composition showed a diameter of 145.5 ± 31.5 nm and a polydispersity index of 0.20 ± 0.05. High doxorubicin (Dox) loading was obtained with the remote pH gradient method using citrate as the inner buffer. Specific binding to PC-3 cells of DSPC/MonY-BN liposomes was obtained (2.7% ± 0.3%, at 37°C), compared with peptide-free DSPC liposomes (1.4% ± 0.2% at 37°C). Incubation of cells with DSPC/ MonY-BN/Dox showed significantly lower cell survival compared with DSPC/Dox-treated cells, in the presence of 100 ng/mL and 300 ng/mL drug amounts, in cytotoxicity experiments. Intravenous treatment of PC-3 xenograft-bearing mice with DSPC/MonY-BN/Dox at 10 mg/kg Dox dose produced higher tumour growth inhibition (60%) compared with nonspecific DSPC/ Dox liposomes (36%) relative to control animals. Conclusion:The structural and loading properties of DSPC/MonY-BN liposomes along with the observed in-vitro and in-vivo activity are encouraging for further development of this approach for target-specific cancer chemotherapy.

Section: Introductionmentioning

confidence: 99%

Peptide-modified liposomes for selective targeting of bombesin receptors overexpressed by cancer cells: a potential theranostic agent

Salsano

Morisco

et al. 2012

IJN

Self Cite

“…(C18) 2 DOTA/(C18) 2 L5CCK8 (90/10) liposomes showed comparable results. 59 Very recently, the same authors described new BN-conjugated nanosystems for theranostic purposes. 60 The liposomes are based on the co-aggregation of a DSPC phospholipid with MonY-BN, a new synthetic amphiphilic monomer ( Figure 2) containing a 7-14-Bombesin peptide fragment, DTPA chelating agent, hydrophobic moiety with two C18 alkyl chains, and PEG spacers.…”

Section: Naposomesmentioning

confidence: 98%

Peptide-based targeting strategies for simultaneous imaging and therapy with nanovectors

Tesauro

Morelli

2013

Polym J

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Over recent years, multifunctional compounds that combine diagnostic and therapeutic modalities using one unified material\ud have been developed and designated as theranostics. These compounds provide the chance to develop individually designed\ud therapies against various diseases to accomplish personalized medicine. In this review, theranostic agents based on nanovectors\ud (liposomes, naposomes, micelles, polymeric micelles and micelles built around a solid core) externally modified with targeting\ud peptides able to simultaneously carry a drug and a contrast agent are described, demonstrating that peptide-modified nanovectors can selectively carry a drug to target cells with an imaging probe co-incorporated into the nanovector to monitor therapy

“…Two liposomes decorated with CCK8 peptide and loaded with DOX have been developed for the targeting of the cholecystokinin subtype receptors A (or CCK1‐R) and B (or CCK2‐R) . CCK1‐R has been found to be overexpressed in gastroenteropancreatic neuroendocrine tumors, meningiomas and in certain neuroblastomas; whereas CCK2‐R has been found to be overexpressed in stromal ovarian cancers, medullary thyroid cancers, astrocytomas and small‐cell lung cancers .…”

Section: Gpcr Receptorsmentioning

confidence: 99%

Review peptide‐targeted liposomes for selective drug delivery: Advantages and problematic issues

Morelli

2015

Biopolymers

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We describe the use of bioactive peptides to drive liposomal drugs on target receptors overexpressed in cancer cells. A detailed description for several targeting liposomes derivatized with different peptides and thus able to target relevant receptors for cancer therapy is reported. Even if the development of peptide-targeted liposomes represents a great advance in the use of liposomal drugs for cancer therapy, many critical issues are still unsolved in the development of these innovative drug delivery systems. Advantages and drawbacks of the peptide-mediated active targeting are discussed.