A thermally targeted c-Myc inhibitory polypeptide inhibits breast tumor growth

Bidwell, Gene L.; Perkins, Eddie; Raucher, Dražen

doi:10.1016/j.canlet.2011.12.042

Cited by 58 publications

(67 citation statements)

References 25 publications

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“…The delivery of the H1 peptide by Bac-ELP was shown to effectively reduce tumor burden in mammary pad breast tumors, following intraperitoneal administration [85], and also demonstrated increased tumor accumulation and prolonged survival in a model of rat glioma, following intravenous administration [86]. In both applications, four cycles of tumor heating and cooling enhanced local tumor accumulation of temperature-sensitive CPP-ELPs and improved therapeutic response, as compared to tumors that were not heated.…”

Section: Hyperthermia-targeted Drug Carriersmentioning

confidence: 99%

Applications of elastin-like polypeptides in drug delivery

MacEwan

Chilkoti

2014

Journal of Controlled Release

211

236

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Elastin-like polypeptides (ELPs) are biopolymers inspired by human elastin. Their lower critical solution temperature phase transition behavior and biocompatibility make them useful materials for stimulus-responsive applications in biological environments. Due to their genetically encoded design and recombinant synthesis, the sequence and size of ELPs can be exactly defined. These design parameters control the structure and function of the ELP with a precision that is unmatched by synthetic polymers. Due to these attributes, ELPs have been used extensively for drug delivery in a variety of different embodiments—as soluble macromolecular carriers, self-assembled nanoparticles, cross-linked microparticles, or thermally coacervated depots. These ELP systems have been used to deliver biologic therapeutics, radionuclides, and small molecule drugs to a variety of anatomical sites for the treatment of diseases including cancer, type 2 diabetes, osteoarthritis, and neuroinflammation.

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Section: Hyperthermia-targeted Drug Carriersmentioning

confidence: 99%

Applications of elastin-like polypeptides in drug delivery

MacEwan

Chilkoti

2014

Journal of Controlled Release

211

236

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“…Furthermore, in an in vivo study that used both a CPP-ELP conjugate and applied local hyperthermia, intratumoral drug accumulation was doubled in comparison to the group without hyperthermia, leading to enhanced antitumor efficacy and possibly suggesting a discriminated toxic response between heated and nonheated tissues [66]. This research group then developed an ELP loaded with an anticancer molecule, the p21 Waf1/Cip1 inhibitory peptide (ELP-p21) [67].…”

Section: Reviewmentioning

confidence: 99%

Cell-penetrating peptides: strategies for anticancer treatment

Raucher

Ryu

2015

Trends in Molecular Medicine

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200

159

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“…Elastin-like polypeptide (ELP) is a synthetic protein made of repeated units of a 5 amino acid motif, and it has been applied as a drug carrier in several preclinical disease models. [6][7][8][9][10][11] ELP is advantageous as a drug delivery vector because it is nonimmunogenic, is easily purified by taking advantage of its unique property of thermally triggered aggregation, [12][13][14] and is amenable to fusion with small molecule, peptide, or protein-based therapeutic agents (reviewed in Raucher et al 15 ). ELP is produced recombinantly, and its coding sequence is easily modified for fusion of targeting or cell-penetrating peptides (CPPs) and with therapeutic proteins, peptides, or drug conjugation sites using basic molecular biology protocols.…”

Section: Introductionmentioning

confidence: 99%

Corneal Penetrating Elastin-Like Polypeptide Carriers

George

et al. 2016

Journal of Ocular Pharmacology and Therapeutics

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Purpose: Elastin-like polypeptide (ELP) is a bioengineered protein widely applied as a drug carrier due to its biocompatibility and amenability to modification with cell-penetrating peptides (CPPs) and therapeutic agents. The purpose of this study was to determine whether topically applied ELP or CPP-fused ELPs penetrate the corneal barrier. Methods: In vitro binding and cytotoxicity to human corneal epithelial (HCE) cells were determined for ELP or CPP-ELPs. Corneal binding, clearance, and penetration were assessed in a rabbit model following topical application of the fluorescently labeled proteins by quantitative fluorescence imaging and histology. Results: ELP bound to HCE cells in vitro, and binding/uptake was enhanced 2-to 3-fold by the addition of CPPs. When applied topically to rabbit eyes, ELP accumulated in the cornea at levels 7.4-fold higher than did an equivalent dose of immunoglobulin G. Both ELP and a CPP-ELP penetrated the corneal epithelium and were detectable in the stroma. Addition of CPPs to ELP, however, did not significantly enhance corneal uptake or penetration in vivo relative to ELP alone. The polypeptides cleared from the cornea over a period of 20-30 min after application, after which cornea levels reached a steady state of 15-30 mg/mL for up to 3 h. Conclusions: The ELP drug carrier can penetrate the corneal epithelium and accumulate in the stroma. Given its amenability for fusion to multiple types of therapeutic agents, ELP has the potential to serve as a drug carrier for topical ocular applications.

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A thermally targeted c-Myc inhibitory polypeptide inhibits breast tumor growth

Cited by 58 publications

References 25 publications

Applications of elastin-like polypeptides in drug delivery

Applications of elastin-like polypeptides in drug delivery

Cell-penetrating peptides: strategies for anticancer treatment

Corneal Penetrating Elastin-Like Polypeptide Carriers

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