Toward the development of a novel non-RGD cyclic peptide drug conjugate for treatment of human metastatic melanoma

Redko, Boris; Segal, Tamar; Tobi, Dror; Luboshits, Galia; Ashur‐Fabian, Osnat; Pinhasov, Albert; Gerlitz, Gabi; Gellerman, Gary

doi:10.18632/oncotarget.12748

Cited by 31 publications

(28 citation statements)

References 51 publications

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“…Recently, a new non-RGD cyclic peptide called ALOS4 (cyclo-(CSSAGSLFC)) was found to bind to overexpressed integrin α V β 3 in malignant melanoma cells (Figure 1; Table 1) [37]. ALOS4 peptide has been similarly explored as a tumor targeting peptide due to its binding affinity for α V β 3 integrin.…”

Section: B Cell Adhesion Peptidesmentioning

confidence: 99%

“…ALOS4 peptide has been similarly explored as a tumor targeting peptide due to its binding affinity for α V β 3 integrin. The binding site for ALOS4 on α V β 3 integrin is different from the binding site of RGD peptide [37]. However, this peptide can be used as an alternative method of delivering cytotoxic drug to cancer cells overexpressing α V β 3 integrin.…”

Section: B Cell Adhesion Peptidesmentioning

confidence: 99%

“…ALOS4 was conjugated to fluorescein isothiocyanate (FITC) via a γ-aminobutyric acid (GABA) linker, to make FITC-GABA-ALOS4 [37]. This molecule was engulfed by WM-266-4 melanoma cells via binding to upregulated α V β 3 integrins, as detected by FACScan [37]. The high deposition of FITC-GABA-ALOS4 was found at the tumor xenograft of WM-266-4 melanoma cells in nude mice, indicating tumor targeting by ALOS4 peptide.…”

Section: Cell Adhesion Peptide-drug Conjugates (Pdc)mentioning

confidence: 99%

“…The results showed that CPT-GABA-ALOS4 killed WM-266-4 cells in a dose-dependent manner to as much as 70% at 10 μM. In contrast, it only killed 30% of non-malignant HEK-293 with the same dose [37]. Because non-malignant HEK-293 do not overexpress α V β 3 integrin on their cell surfaces, the results suggest that selectivity of ALOS constructs for WM-266-4 over HEK-293 cells are due to the overexpression of α V β 3 integrins on WM-266-4 cells.…”

Section: Cell Adhesion Peptide-drug Conjugates (Pdc)mentioning

confidence: 99%

“…In addition, the free CPT and two other cytotoxic drugs consistently killed considerable percentages of cell-populations in both WM-266-4 and non-malignant HEK-293. This study presents a promising non-RGD targeting peptide for the enhancement of chemo-stability and effective tumor-specific delivery of cytotoxic drugs [37]. …”

Section: Cell Adhesion Peptide-drug Conjugates (Pdc)mentioning

confidence: 99%

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Conjugates of Cell Adhesion Peptides for Therapeutics and Diagnostics Against Cancer and Autoimmune Diseases

Moral

Siahaan

2018

CTMC

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Overexpressed cell-surface receptors are hallmarks of many disease states and are often used as markers for targeting diseased cells over healthy counterparts. Cell adhesion peptides, which are often derived from interacting regions of these receptor-ligand proteins, mimic surfaces of intact proteins and, thus, have been studied as targeting agents for various payloads to certain cell targets for cancers and autoimmune diseases. Because many cytotoxic agents in the free form are often harmful to healthy cells, the use of cell adhesion peptides in targeting their delivery to diseased cells has been studied to potentially reduce required effective doses and associated harmful side-effects. In this review, multiple cell adhesion peptides from extracellular matrix and ICAM proteins were used to selectively direct drug payloads, signal-inhibitor peptides, and diagnostic molecules, to diseased cells over normal counterparts. RGD constructs have been used to improve the selectivity and efficacy of diagnostic and drug-peptide conjugates against cancer cells. From this precedent, novel conjugates of antigenic and cell adhesion peptides, called bifunctional peptide inhibitors (BPIs), have been designed to selectively regulate immune cells and suppress harmful inflammatory responses in autoimmune diseases. Similar peptide conjugations with imaging agents have delivered promising diagnostic methods in animal models of rheumatoid arthritis. BPIs have also been shown to generate immune tolerance and suppress autoimmune diseases in animal models of type-1 diabetes, rheumatoid arthritis, and multiple sclerosis. Collectively, these studies show the potential of cell adhesion peptides in improving the delivery of drugs and diagnostic agents to diseased cells in clinical settings.

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Section: B Cell Adhesion Peptidesmentioning

confidence: 99%

Section: B Cell Adhesion Peptidesmentioning

confidence: 99%

Section: Cell Adhesion Peptide-drug Conjugates (Pdc)mentioning

confidence: 99%

Section: Cell Adhesion Peptide-drug Conjugates (Pdc)mentioning

confidence: 99%

Section: Cell Adhesion Peptide-drug Conjugates (Pdc)mentioning

confidence: 99%

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Conjugates of Cell Adhesion Peptides for Therapeutics and Diagnostics Against Cancer and Autoimmune Diseases

Moral

Siahaan

2018

CTMC

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Peptide Targeting Methods

Patil

et al. 2019

Handbook of in Vivo Chemistry in Mice

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Targeted Therapy against Metastatic Melanoma Based on Self‐Assembled Metal‐Phenolic Nanocomplexes Comprised of Green Tea Catechin

et al. 2019

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The targeted therapy of metastatic melanoma is an important yet challenging goal that has received only limited attention to date. Herein, green tea polyphenols, (–)‐epigallocatechin‐3‐gallate (EGCG), and lanthanide metal ions (Sm 3+ ) are used as building blocks to engineer self‐assembled Sm III ‐EGCG nanocomplexes with synergistically enhanced tumor inhibitory properties. These nanocomplexes have negligible systemic toxic effects on healthy cells but cause a significant reduction in the viability of melanoma cells by efficiently regulating their metabolic pathways. Moreover, the wound‐induced migration of melanoma cells can be efficiently inhibited by Sm III ‐EGCG, which is a key criterion for metastatic melanoma therapy. In a mouse melanoma tumor model, Sm III ‐EGCG is directly compared with a clinical anticancer drug, 5‐fluorouracil and shows remarkable tumor inhibition. Moreover, the targeted therapy of Sm III ‐EGCG is shown to prevent metastatic lung melanoma from spreading to main organs with no adverse side effects on the body weight or organs. These in vivo results demonstrate significant advantages of Sm III ‐EGCG over its clinical counterpart. The results suggest that these green tea‐based, self‐assembled nanocomplexes possess all of the key traits of a clinically promising candidate to address the challenges associated with the treatment of advanced stage metastatic melanoma.

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Toward the development of a novel non-RGD cyclic peptide drug conjugate for treatment of human metastatic melanoma

Cited by 31 publications

References 51 publications

Conjugates of Cell Adhesion Peptides for Therapeutics and Diagnostics Against Cancer and Autoimmune Diseases

Conjugates of Cell Adhesion Peptides for Therapeutics and Diagnostics Against Cancer and Autoimmune Diseases

Peptide Targeting Methods

Targeted Therapy against Metastatic Melanoma Based on Self‐Assembled Metal‐Phenolic Nanocomplexes Comprised of Green Tea Catechin

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