Discovery of Indoline-Based, Natural-Product-like Compounds as Probes of Focal Adhesion Kinase Signaling Pathways

Poondra, Rajamohan R.; Kumar, Niti; Bijian, Krikor; Prakesch, Michaël; Campágna-Slater, Valérie; Reayi, Ayub; Reddy, P. Thirupathi; Choudhry, Asna; Barnes, Michael; Leek, Donald M.; Daroszewska, Malgosia; Lougheed, Caroline; Xu, Bin; Schapira, Matthieu; Alaoui‐Jamali, Moulay A.; Arya, Prabhat

doi:10.1021/cc8001525

Cited by 20 publications

(4 citation statements)

References 26 publications

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“…Protein interactions crucially mediate many signaling pathways controlling cellular proliferation and apoptosis; blocking such interactions in an intracellular compartment holds great therapeutic potential for the development of anti-cancer drugs [1, 2]. Small molecules, however, have difficulty targeting these interactions because of the nature of the protein interface, which is normally extensive, shallow and hydrophobic [3]. Moreover, antibody therapeutics, albeit popular candidates because of advantages including high affinity and specificity, also demonstrate serious disadvantages, such as unfavorable immunogenicity, low drug penetration and hypersensitivity reactions [4].…”

Section: Introductionmentioning

confidence: 99%

Nanoparticle delivery of a peptide targeting EGFR signaling

Kim

Huang

2012

Journal of Controlled Release

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EGFR serves as an important therapeutic target because of its over-expression in many cancers. In this study, we investigated a peptide-based therapy aimed at blocking intracellular protein-protein interactions during EGFR signaling and evaluated a targetable lipid carrier system that can deliver peptides to intracellular targets in human cancer cells. EEEEpYFELV (EV), a nonapeptide mimicking the Y845 site of EGFR which is responsible for STAT5b phosphorylation, was designed to block EGFR downstream signaling. EV was loaded onto LPH nanoparticles that are comprised of a membrane/core structure including a surface-grafted polyethylene glycol (PEG) used to evade the reticuloendothelial system (RES) and anisamide (AA) for targeting the sigma receptor over-expressed in H460 human lung cancer cells. EV formulated with PEGylated and targeted LPH (LPH-PEG-AA) was taken up by the tumor cells and trafficked to the cytoplasm with high efficiency. Using this approach, EV acted as a dominant negative inhibitor of STAT5b phosphorylation, arrested cell proliferation, and induced massive apoptosis. Intravenous administration of EV loaded in LPH-PEG-AA led to efficient EV peptide delivery to the tumor in a xenograft mouse model, and multiple injections inhibited tumor growth in a dose-dependent manner. Our findings offer proof-of-concept for an intracellular peptide-mediated cancer therapy that is delivered by carefully designed nanoparticles.

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Section: Introductionmentioning

confidence: 99%

Nanoparticle delivery of a peptide targeting EGFR signaling

Kim

Huang

2012

Journal of Controlled Release

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“…The precise cellular mechanisms underlying the effects of adhesion ligand presentation are being intensely investigated and are speculated to result, at least in part, from modulation of adhesion contacts and clustering of cellular receptor that in turn modulate the cytoskeleton and intrinsic cell signaling pathways (Chen et al , 1997; Geiger et al , 2001; Comisar et al , 2006; Discher et al , 2009). Interestingly, as there is better understanding of the biological basis of these material’s biophysical interactions at the nanoscale, the material composition itself can be designed to serve as an extrinsic cue to trigger specific signal transduction pathways, as demonstrated by direct induction of focal adhesion kinase signaling in a recent report (Poondra et al , 2009). In vivo , mechanically tailored material systems, both natural and synthetic, have demonstrated efficacy in aiding regeneration of cardiac muscle (van Amerongen et al , 2006; Valarmathi et al , 2010) and PDL (Moioli et al , 2008), as well as modulating scar tissue formation (Agrawal et al , 2010).…”

Section: Soluble Cues – Regulated Presentation Of Biomoleculesmentioning

confidence: 99%

At the edge of translation – materials to program cells for directed differentiation

Arany

Mooney²

2010

Oral Diseases

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The rapid advancement in basic biology knowledge, especially in the stem cell field, has created new opportunities to develop biomaterials capable of orchestrating the behavior of transplanted and host cells. Based on our current understanding of cellular differentiation, a conceptual framework for the use of materials to program cells in situ is presented, namely a domino vs a switchboard model, to highlight the use of single vs multiple cues in a controlled manner to modulate biological processes. Further, specific design principles of material systems to present soluble and insoluble cues that are capable of recruiting, programming and deploying host cells for various applications are presented. The evolution of biomaterials from simple inert substances used to fill defects, to the recent development of sophisticated material systems capable of programming cells in situ is providing a platform to translate our understanding of basic biological mechanisms to clinical care.Oral Diseases (2011) 17, 241-251

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“…Small molecules usually have difficulties in precisely targeting protein interactions for the reasons that protein interfaces are normally extensive, shallow, and hydrophobic in nature [80]. Therapeutics based on antibodies which show high affinities and specificities to tumors still have disadvantages such as unfavorable immunogenicity, low drug penetration, and undesired hypersensitivity reactions [81].…”

Section: Introductionmentioning

confidence: 99%

Peptide-Based Nanostructures for Cancer Diagnosis and Therapy

An¹,

Gilani²,

Liang³

2014

CMC

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Peptide-based nanoparticles (pep-NPs) are emerging as promising imaging and therapeutic agents against cancer due to their biocompatibility and tunability. Optimized design of the peptide sequence and moderate conjugation of the sequence with extraneous molecules are crucial to the performance of the inherent properties of pep-NPs such as nanostructure formation and ability of drug delivery. Meanwhile, the peptide sequences based on natural/unnatural amino acids could be utilized for designing nanostructures susceptive/resistant to specific enzymes. Herein, we firstly summarize the basic peptide structures to provide a whole image of pep-NPs. Subsequently, the diagnostic strategies based on different imaging modalities and recent therapeutic applications of pep-NPs for cancer are reviewed.

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Discovery of Indoline-Based, Natural-Product-like Compounds as Probes of Focal Adhesion Kinase Signaling Pathways

Cited by 20 publications

References 26 publications

Nanoparticle delivery of a peptide targeting EGFR signaling

Nanoparticle delivery of a peptide targeting EGFR signaling

At the edge of translation – materials to program cells for directed differentiation

Peptide-Based Nanostructures for Cancer Diagnosis and Therapy

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