Novel Peptide Conjugates for Tumor-Specific Chemotherapy

柔红霉素 化学 阿霉素 细胞毒性 神经母细胞瘤 结合 受体 神经肽Y受体 细胞培养 生物化学 化疗 体外 生物 神经肽 免疫学 白血病 数学分析 遗传学 数学
作者
Michael Langer,Felix Kratz,Barbara Rothen‐Rutishauser,Heidi Wunderli‐Allenspach,Annette G. Beck‐Sickinger
出处
期刊:Journal of Medicinal Chemistry [American Chemical Society]
卷期号:44 (9): 1341-1348 被引量:93
标识
DOI:10.1021/jm001065f
摘要

One of the major problems in cancer chemotherapy are the severe side effects that limit the dose of the anticancer drugs because of their unselectivity for tumor versus normal cells. In the present work, we show that coupling of anthracyclines to peptides is a promising approach to obtain selectivity. The peptide−drug conjugate was designed to bind to specific receptors expressed on the tumor cells with subsequent internalization of the ligand−receptor complex. Neuropeptide Y (NPY), a 36-amino acid peptide of the pancreatic polypeptide family, was chosen as model peptide because NPY receptors are overexpressed in a number of neuroblastoma tumors and the thereof derived cell lines. Daunorubicin and doxorubicin, two widely used antineoplastic agents in tumor therapy, were covalently linked to NPY via two spacers that differ in stability: an acid-sensitive hydrazone bond at the 13-keto position of daunorubicin and a stable amide bond at the 3‘-amino position of daunorubicin and doxorubicin. Receptor binding of these three conjugates ([C15]-NPY-Dauno-HYD, [C15]-NPY-Dauno-MBS, and [C15]-NPY-Doxo-MBS) was determined at the human neuroblastoma cell line SK-N-MC, which selectively expresses the NPY Y1 receptor subtype, and cytotoxic activity was evaluated using a XTT-based colorimetric cellular cytotoxicity assay. The different conjugates were able to bind to the receptor with affinities ranging from 25 to 51 nM, but only the compound containing the acid-sensitive bond ([C15]-NPY-Dauno-HYD) showed cytotoxic activity comparable to the free daunorubicin. This cytotoxicity is Y1 receptor-mediated as shown in blocking studies with BIBP 3226, because tumor cells that do not express NPY receptors were sensitive to free daunorubicin, but not to the peptide−drug conjugate. The intracellular distribution was investigated by confocal laser scanning microscopy. We found evidence that the active conjugate [C15]-NPY-Dauno-HYD releases daunorubicin, which is localized close to the nucleus, whereas the inactive conjugate [C15]-NPY-Dauno-MBS is distributed distantly from the nucleus and does not seem to release the drug within the cell.
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