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Clinical Cancer Research 2013-Jan

Targeted delivery of paclitaxel to EphA2-expressing cancer cells.

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Il collegamento viene salvato negli appunti
Si Wang
Roberta Noberini
John L Stebbins
Swadesh Das
Ziming Zhang
Bainan Wu
Sayantan Mitra
Sandrine Billet
Ana Fernandez
Neil A Bhowmick

Parole chiave

Astratto

OBJECTIVE

YSA is an EphA2-targeting peptide that effectively delivers anticancer agents to prostate cancer tumors. Here, we report on how we increased the drug-like properties of this delivery system.

METHODS

By introducing non-natural amino acids, we have designed two new EphA2 targeting peptides: YNH, where norleucine and homoserine replace the two methionine residues of YSA, and dYNH, where a D-tyrosine replaces the L-tyrosine at the first position of the YNH peptide. We describe the details of the synthesis of YNH and dYNH paclitaxel conjugates (YNH-PTX and dYNH-PTX) and their characterization in cells and in vivo.

RESULTS

dYNH-PTX showed improved stability in mouse serum and significantly reduced tumor size in a prostate cancer xenograft model and also reduced tumor vasculature in a syngeneic orthotopic allograft mouse model of renal cancer compared with vehicle or paclitaxel treatments.

CONCLUSIONS

This study reveals that targeting EphA2 with dYNH drug conjugates could represent an effective way to deliver anticancer agents to a variety of tumor types.

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