α-Enolase–binding peptide enhances drug delivery efficiency and therapeutic efficacy against colorectal cancer

Wu, Chien‐Hsun; Kuo, Yi-Huei; Hong, Ruey‐Long; Wu, Han‐Chung

doi:10.1126/scitranslmed.aaa9391

Cited by 53 publications

(47 citation statements)

References 41 publications

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“…Also, peptides clear rapidly for reduced background and less biodistribution in non-target tissues30. Peptides have less potential for immunogenicity than antibodies, which allows for repetitive use31. We used Cy5.5, a NIR fluorophore, to label the peptide to maximize imaging depth, avoid hemoglobin absorption, reduce tissue scattering, and minimize autofluorescence background32.…”

Section: Discussionmentioning

confidence: 99%

Visualizing epithelial expression of EGFR in vivo with distal scanning side-viewing confocal endomicroscope

Duan

Zhou

et al. 2016

Sci Rep

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Confocal endomicroscopy is an emerging imaging technology that has recently been introduced into the clinic to instantaneously collect “optical biopsies” in vivo with histology-like quality. Here, we demonstrate a fast scanner located in the distal end of a side-viewing instrument using a compact lens assembly with numerical aperture of 0.5 to achieve a working distance of 100 μm and field-of-view of 300 × 400 μm2. The microelectromechanical systems (MEMS) mirror was designed based on the principle of parametric resonance and images at 5 frames per second. The instrument has a 4.2 mm outer diameter and 3 cm rigid length, and can pass through the biopsy channel of a medical endoscope. We achieved real time optical sections of NIR fluorescence with 0.87 μm lateral resolution, and were able to visualize in vivo binding of a Cy5.5-labeled peptide specific for EGFR to the cell surface of pre-cancerous colonocytes within the epithelium of dysplastic crypts in mouse colon. By performing targeted imaging with endomicroscopy, we can visualize molecular expression patterns in vivo that provide a biological basis for disease detection.

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Section: Discussionmentioning

confidence: 99%

Visualizing epithelial expression of EGFR in vivo with distal scanning side-viewing confocal endomicroscope

Duan

Zhou

et al. 2016

Sci Rep

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“…It can be performed in vitro against various types of cells, including cultured cell lines, primary cells isolated from animal models or human patients, or processed cells (fixed cells, activated cells etc.). Within the past ten years, several studies have focused on the in vitro biopanning of phage displayed peptide libraries using various cancer cell types [86][87][88][89][90] to identify cell-specific ligands [91].…”

Section: Selection Of Cell-specific Peptidesmentioning

confidence: 99%

“…Wu and co-workers aimed to overcome the problems outlined above by using biotinylated peptides to directly bind intact cells, and subsequent fixation of ligandreceptor complexes by cross-linking with 3,3′-dithiobis[sulfosuccinimidyl propionate] (DTSSP). After affinity trapping and LC-MS/MS analysis, the unknown target protein on the plasma membrane of the cells could be identified [89]. It is important to note that advances in peptide identification and subsequent receptor identification can lead to the discovery of important cellular targets that were previously unknown.…”

Section: Selection Of Cell-specific Peptidesmentioning

confidence: 99%

“…5). Remote loading methods, such as the ammonium sulfate method [110] and the pH gradient method [111], can encapsulate weak bases, such as doxorubicin or vinorelbine, into the liposomes with more than 95 % efficiency [89]. Schedule-dependent drugs, such as vinca alkaloids and topotecan, are reasonable candidates for liposomal delivery because of their effectiveness at enhancing the exposure time of cancer cells to therapeutic drug levels.…”

Section: Phage Circulation Elution and Amplificationmentioning

confidence: 99%

“…Increased IFP contributes to decreased transcapillary transport in tumors, which reduces uptake of drugs. This approach sidesteps the problem of high tumor IFP [89,113,114] and improves treatment effectiveness, thereby reducing incomplete tumor response, rapid disease relapse, and development of drug resistance due to suboptimal doses, which are often seen when using conventional chemotherapies.…”

Section: Phage Circulation Elution and Amplificationmentioning

confidence: 99%

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Advancement and applications of peptide phage display technology in biomedical science

et al. 2016

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Combinatorial phage library is a powerful research tool for high-throughput screening of protein interactions. Of all available molecular display techniques, phage display has proven to be the most popular approach. Screening phage-displayed random peptide libraries is an effective means of identifying peptides that can bind target molecules and regulate their function. Phage-displayed peptide libraries can be used for (i) B-cell and T-cell epitope mapping, (ii) selection of bioactive peptides bound to receptors or proteins, disease-specific antigen mimics, peptides bound to non-protein targets, cell-specific peptides, or organ-specific peptides, and (iii) development of peptide-mediated drug delivery systems and other applications. Targeting peptides identified using phage display technology may be useful for basic research and translational medicine. In this review article, we summarize the latest technological advancements in the application of phage-displayed peptide libraries to applied biomedical sciences.

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Peptide Targeting Methods

Patil

et al. 2019

Handbook of in Vivo Chemistry in Mice

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α-Enolase–binding peptide enhances drug delivery efficiency and therapeutic efficacy against colorectal cancer

Cited by 53 publications

References 41 publications

Visualizing epithelial expression of EGFR in vivo with distal scanning side-viewing confocal endomicroscope

Visualizing epithelial expression of EGFR in vivo with distal scanning side-viewing confocal endomicroscope

Advancement and applications of peptide phage display technology in biomedical science

Peptide Targeting Methods

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