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整合素αvβ3靶向的聚酰胺-胺(PAMAM)树枝状大分子的合成、表征及生物学评价

Synthesis, characterization, and biological evaluation of integrin alphavbeta3-targeted PAMAM dendrimers.

作者信息

Boswell C Andrew, Eck Peter K, Regino Celeste A S, Bernardo Marcelino, Wong Karen J, Milenic Diane E, Choyke Peter L, Brechbiel Martin W

机构信息

Radioimmune & Inorganic Chemistry Section, Radiation Oncology Branch, National Cancer Institute, National Institutes of Health, Bethesda, Maryland 20892-1088, USA.

出版信息

Mol Pharm. 2008 Jul-Aug;5(4):527-39. doi: 10.1021/mp800022a. Epub 2008 Jun 7.

Abstract

Ligand size and valency strongly influence the receptor uptake and clearance of tumor angiogenesis imaging agents. The structures of successful imaging agents exhibit a high degree of variability, encompassing small monovalent arginine-glycine-aspartic acid (RGD)-containing peptides, multivalent RGD-oligomers, and a monoclonal antibody against integrin alpha-v-beta-3 (alpha-v-beta-3). We have pursued a nanoscale approach to imaging of angiogenesis using rationally designed polyamidoamine (PAMAM) dendrimers covalently adorned with RGD-cyclopeptides. An orthogonal oxime-ligation strategy was applied to chemoselectively effect conjugation of the PAMAM dendrimers with RGD-cyclopeptides for targeting alpha vbeta 3. Fluorescent dyes for optical imaging and chelates for gadolinium-based magnetic resonance (MR) imaging were subsequently appended to create robust multimodal macromolecular imaging agents. Fluorescence microscopy revealed selective binding of the resulting RGD peptide-bearing dendrimer with empty chelates to alpha-v-beta-3-expressing cells, but somewhat reduced selectivity was observed following Gd(III) complexation. The expected incomplete saturation of chelates with Gd(III) ions permitted radiometal complexation, and an in vivo tissue distribution of the resulting agent in M21 melanoma tumor-bearing mice showed mostly renal and reticuloendothelial accumulation, with the tumor:blood ratio peaking (3.30+/-0.03) at 2 h postinjection.

摘要

配体大小和化合价对肿瘤血管生成显像剂的受体摄取和清除有强烈影响。成功的显像剂结构具有高度变异性,包括含一价精氨酸-甘氨酸-天冬氨酸(RGD)的小分子肽、多价RGD寡聚物以及抗整合素α-v-β-3(α-v-β-3)单克隆抗体。我们采用纳米级方法,利用经合理设计的、共价连接有RGD环肽的聚酰胺-胺(PAMAM)树枝状大分子对血管生成进行成像。应用正交肟连接策略实现PAMAM树枝状大分子与RGD环肽的化学选择性偶联,以靶向α vβ 3。随后添加用于光学成像的荧光染料和用于钆基磁共振(MR)成像的螯合物,以制备强大的多模态大分子显像剂。荧光显微镜显示,所得带有RGD肽的空螯合树枝状大分子与表达α-v-β-3的细胞有选择性结合,但在钆(III)络合后观察到选择性有所降低。钆(III)离子对螯合物的预期不完全饱和允许放射性金属络合,所得显像剂在荷M21黑色素瘤肿瘤小鼠体内的组织分布显示,主要在肾脏和网状内皮系统蓄积,肿瘤与血液的比值在注射后2小时达到峰值(3.30±0.03)。

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