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肿瘤特异性蛋白人半乳糖凝集素-1与抗癌药物相互作用。

Tumor-specific protein human galectin-1 interacts with anticancer agents.

作者信息

D'Auria Sabato, Petrova Lidia, John Constance, Russev George, Varriale Antonio, Bogoeva Vanya

机构信息

Laboratory for Molecular Sensing, Institute of Protein Biochemistry, CNR, Via P. Castellino, 111, 80131 Naples, Italy.

出版信息

Mol Biosyst. 2009 Nov;5(11):1331-6. doi: 10.1039/b905921k. Epub 2009 Aug 18.

DOI:10.1039/b905921k
PMID:19823749
Abstract

The present work shows a novel binding activity of the tumor specific lectin--recombinant human galectin-1 (hGal-1)--to three porphyrin compounds: (1) Zn-porphyrin (ZnTPPS); (2) Mn-porphyrin and (3) Au-porphyrin. These compounds are widely applied in the photodynamic therapy of cancer (PDT). Our data indicate that hGal-1, similar to some plant lectins, a bacterial lectin from Pseudomonas aeruginosa and an animal lectin from Helix pomatia, possesses dual functions binding to both carbohydrate and non-carbohydrate ligands. The interaction of ZnTPPS with hGal-1 was studied by the specific fluorescence emission of the porphyrin. The protein binding properties to Mn/Au-porphyrins and adenine were measured by intrinsic protein fluorescence quenching. The values determined for the apparent dissociation constants (K(D)) of 0.6-1.5 microM are similar to the K(D) for complexes of concanavalin A and porphyrin, and are indicative of the high affinity of hGal-1 for these porphyrins. In addition, the analysis of the hyperbolic binding curves obtained suggests the presence of one hGal-1 binding site for porphyrins or adenine. Additionally, we found that hGal-1 interacts with the fluorescent probe 2-(p-toluidinyl)naphthalene sulfonic acid (TNS), that was used to identify the hydrophobic regions within hGal-1. Homodimeric hGal-1 has more than one class of binding site for TNS as revealed by the sigmoidal shape of the fluorescence titration curve. hGal-1 can be characterized as a porphyrin-binding protein based on its interactions with the Zn/Mn- and Au-porphyrins, and this indicates that hGal-1 may have potential as a delivery molecule to target systems (e.g., tumor cells) with possible application in photodynamic therapy.

摘要

目前的研究表明,肿瘤特异性凝集素——重组人半乳糖凝集素-1(hGal-1)——对三种卟啉化合物具有新型结合活性:(1)锌卟啉(ZnTPPS);(2)锰卟啉;(3)金卟啉。这些化合物广泛应用于癌症的光动力疗法(PDT)。我们的数据表明,hGal-1与一些植物凝集素、铜绿假单胞菌的一种细菌凝集素以及苹果螺的一种动物凝集素类似,具有与碳水化合物和非碳水化合物配体结合的双重功能。通过卟啉的特异性荧光发射研究了ZnTPPS与hGal-1的相互作用。通过蛋白质固有荧光猝灭测量了蛋白质与锰/金卟啉和腺嘌呤的结合特性。测定的表观解离常数(K(D))值为0.6 - 1.5微摩尔,与伴刀豆球蛋白A和卟啉复合物的K(D)相似,表明hGal-1对这些卟啉具有高亲和力。此外,对所得双曲线结合曲线的分析表明,存在一个hGal-1与卟啉或腺嘌呤的结合位点。此外,我们发现hGal-1与用于识别hGal-1内疏水区域的荧光探针2-(对甲苯氨基)萘磺酸(TNS)相互作用。荧光滴定曲线的S形表明,同型二聚体hGal-1对TNS有不止一类结合位点。基于hGal-1与锌/锰和金卟啉的相互作用,它可被表征为一种卟啉结合蛋白,这表明hGal-1可能具有作为靶向系统(如肿瘤细胞)的递送分子的潜力,并可能应用于光动力疗法。

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