Optimization of RGD-Containing Cyclic Peptides against αvβ3 Integrin

Wang, Yan; Xiao, Wenwu; Zhang, Yonghong; Meza, Leah; Tseng, Harry; Takada, Yoshikazu; Ames, James B.; Lam, Kit S.

doi:10.1158/1535-7163.mct-15-0544

Cited by 40 publications

(38 citation statements)

References 37 publications

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“…OBOC library can also be used for discovery of cell penetrating peptide ligands, but a cleavable linker and a reporting probe are needed in between the library compound and beads; (iv) OBOC combinatorial libraries are based on synthetic chemistry; therefore, it enables incorporation of D-amino acids, unnatural amino acids, many other organic building blocks, and investigation of cyclic, turned or branched peptides and secondary structures which can confer enhanced resistance to proteolytic degradation, a key requirement for clinical applications; (v) tumor-targeting ligands identified by OBOC library approach are not limited to peptides, but also N -methylated peptides [108], glycopeptides [109-111], peptide tertiary amides [112,113], peptidomimetics [114,115], and peptoids [116]; and (vi) the OBOC method can be used for rapid optimization of the initial lead compounds, whether they are native or identified from biological or synthetic peptide libraries. In OBOC method, each library compound is tethered to the solid support via a linker such as polyethylene glycol.…”

Section: Oboc Peptide Librarymentioning

confidence: 99%

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Tumor-targeting peptides from combinatorial libraries

Liu

Xiao

et al. 2017

Advanced Drug Delivery Reviews

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169

102

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Cancer is one of the major and leading causes of death worldwide. Two of the greatest challenges infighting cancer are early detection and effective treatments with no or minimum side effects. Widespread use of targeted therapies and molecular imaging in clinics requires high affinity, tumor-specific agents as effective targeting vehicles to deliver therapeutics and imaging probes to the primary or metastatic tumor sites. Combinatorial libraries such as phage-display and one-bead one-compound (OBOC) peptide libraries are powerful approaches in discovering tumor-targeting peptides. This review gives an overview of different combinatorial library technologies that have been used for the discovery of tumor-targeting peptides. Examples of tumor-targeting peptides identified from each combinatorial library method will be discussed. Published tumor-targeting peptide ligands and their applications will also be summarized by the combinatorial library methods and their corresponding binding receptors.

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Section: Oboc Peptide Librarymentioning

confidence: 99%

“…Further optimization of LXW7 led to development of LXW64 with sequence cGRGDd-nal1-c (where nal1 stands for D-1-naphthylalanine). LXW64 exhibits 6.6-fold more potent binding affinity against ανβ3-expressing U-87MG cell in vitro and better in vivo tumor targeting compared to LXW7 [108]. …”

Section: Oboc Peptide Librarymentioning

confidence: 99%

Tumor-targeting peptides from combinatorial libraries

Liu

Xiao

et al. 2017

Advanced Drug Delivery Reviews

Self Cite

169

102

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“…anticancer drugs by providing peptides with high affinity and specificity, and in addition they typically have low interaction with the immune system and good tumor and tissue penetration (19). In the targeted delivery of anticancer drugs into cancer tissue the ability to penetrate deep into the solid tumor tissue can potentially be a great challenge for the targeted therapeutic (3).…”

Section: Discussionmentioning

confidence: 99%

Tumor-penetrating peptide fused to a pro-apoptotic peptide facilitates effective gastric cancer therapy

Huang

Sha

et al. 2017

Oncology Reports

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KLA (sequence, KLAKLAKKLAKLAK) is a peptide which leads to programmed cell death by disrupting the mitochondrial membrane. However, low penetration in tumors greatly limits its application and efficacy. To develop a KLA-based cancer therapy, KLA-iRGD, a recombinant protein was constructed. It consists of the KLA peptide and iRGD (CRGDKGPDC), a tumor-homing peptide with high penetration into tumor tissue and cells. The conjugated KLA exhibits pro-apoptotic activity to prevent the growth of a tumor once it is inside the cell. Once KLA-iRGD is internalized in cultured tumor cells, via the activation of the receptor neuropilin-1, it spreads extensively throughout the mass of the tumor. The recombinant KLA-iRGD protein showed antitumor activity in vivo in mice and in vitro in tumor cell lines. Repeated treatment with KLA-iRGD greatly prevented tumor growth, resulting in a considerable reduction in tumor volume. According to our data, KLA-iRGD may serve as a potential anticancer agent with limited systemic toxicity and high selectivity for the treatment of MKN45 gastric cancer, which may lead to the enhancement of new targeted anticancer agents.

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“…The cyclic RGD (cRGD) peptides display higher activity than the linear RGD peptides due to a less flexible conformational structure that resists proteolysis [88,89]. To enhance the biological properties and pharmacokinetics of RGD peptides, including their affinity, various strategies have been used to modify the structure of RGD peptides, such as altering their structure [90] and the stereochemical configuration of the constituent amino acids [91], introducing other amino acids to flank the RGD sequence [92], and N-methylation [93,94]. The modification of NPs with RGD peptides could increase their binding affinity to specific integrins.…”

Section: Rgd-based Integrin-targeted Ligandsmentioning

confidence: 99%

Targeting Integrins in Cancer Nanomedicine: Applications in Cancer Diagnosis and Therapy

Opadele

Onodera

et al. 2019

Cancers

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Due to advancements in nanotechnology, the application of nanosized materials (nanomaterials) in cancer diagnostics and therapeutics has become a leading area in cancer research. The decoration of nanomaterial surfaces with biological ligands is a major strategy for directing the actions of nanomaterials specifically to cancer cells. These ligands can bind to specific receptors on the cell surface and enable nanomaterials to actively target cancer cells. Integrins are one of the cell surface receptors that regulate the communication between cells and their microenvironment. Several integrins are overexpressed in many types of cancer cells and the tumor microvasculature and function in the mediation of various cellular events. Therefore, the surface modification of nanomaterials with integrin-specific ligands not only increases their binding affinity to cancer cells but also enhances the cellular uptake of nanomaterials through the intracellular trafficking of integrins. Moreover, the integrin-specific ligands themselves interfere with cancer migration and invasion by interacting with integrins, and this finding provides a novel direction for new treatment approaches in cancer nanomedicine. This article reviews the integrin-specific ligands that have been used in cancer nanomedicine and provides an overview of the recent progress in cancer diagnostics and therapeutic strategies involving the use of integrin-targeted nanomaterials.

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Optimization of RGD-Containing Cyclic Peptides against αvβ3 Integrin

Cited by 40 publications

References 37 publications

Tumor-targeting peptides from combinatorial libraries

Tumor-targeting peptides from combinatorial libraries

Tumor-penetrating peptide fused to a pro-apoptotic peptide facilitates effective gastric cancer therapy

Targeting Integrins in Cancer Nanomedicine: Applications in Cancer Diagnosis and Therapy

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