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作为靶向碳酸酐酶 IX 的探针的 Tc-羟肟酸配合物的研制。

Development of the Tc-Hydroxamamide Complex as a Probe Targeting Carbonic Anhydrase IX.

机构信息

Department of Patho-Functional Bioanalysis, Graduate School of Pharmaceutical Sciences , Kyoto University , 46-29 Yoshida Shimoadachi-cho, Sakyo-ku , Kyoto 606-8501 , Japan.

出版信息

Mol Pharm. 2019 Apr 1;16(4):1489-1497. doi: 10.1021/acs.molpharmaceut.8b01120. Epub 2019 Mar 20.

DOI:10.1021/acs.molpharmaceut.8b01120
PMID:30892905
Abstract

Carbonic anhydrase IX (CA-IX) is regarded as a favorable target for in vivo imaging because of its specific expression in hypoxic regions of tumors. Hypoxia assists tumor propagation and growth and is resistant to chemotherapy and radiotherapy. Here, we designed and synthesized [Tc]hydroxamamide ([Tc]Ham) and [Tc]methyl-substituted-hydroxamamide ([Tc]MHam) complexes including a bivalent CA-IX ligand, sulfonamide (SA), and ureidosulfonamide (UR). In a cell binding assay, [Tc]Ham complexes with bivalent SA ([Tc]SAB2A and [Tc]SAB2B) and UR ([Tc]URB2A and [Tc]URB2B) showed significantly greater uptake into CA-IX high-expressing (HT-29) cells than that into CA-IX low-expressing cells. Since the binding affinity of [Tc]URB2A and [Tc]URB2B for CA-IX was significantly higher than that of [Tc]SAB2A and [Tc]SAB2B, we additionally synthesized [Tc]MURB2 (a [Tc]MHam complex with bivalent UR) and evaluated the CA-IX-specific binding affinity of [Tc]URB2A, [Tc]URB2B, and [Tc]MURB2. Their uptake into HT-29 cells was reduced by the addition of a CA inhibitor, acetazolamide, suggesting their CA-IX-specific binding affinity. A biodistribution study in HT-29 tumor-bearing mice was carried out using [Tc]URB2A and [Tc]MURB2 with the highest specificity for HT-29 cells. [Tc]URB2A showed moderate tumor uptake and reduction by coinjection with acetazolamide; however, the tumor/blood ratio was insufficient for in vivo imaging. These results provided key information for the design of novel Ham-based imaging probes targeting CA-IX.

摘要

碳酸酐酶 IX(CA-IX)因其在肿瘤缺氧区域的特异性表达而被认为是体内成像的有利靶标。缺氧有助于肿瘤的繁殖和生长,并且对化疗和放疗具有抗性。在这里,我们设计并合成了包含双价 CA-IX 配体磺酰胺(SA)和脲磺酰胺(UR)的 [Tc] 羟酰胺([Tc]Ham)和 [Tc] 甲基取代羟酰胺([Tc]MHam)复合物。在细胞结合测定中,具有双价 SA([Tc]SAB2A 和 [Tc]SAB2B)和 UR([Tc]URB2A 和 [Tc]URB2B)的 [Tc]Ham 复合物对 CA-IX 高表达(HT-29)细胞的摄取明显大于 CA-IX 低表达细胞。由于 [Tc]URB2A 和 [Tc]URB2B 与 CA-IX 的结合亲和力明显高于 [Tc]SAB2A 和 [Tc]SAB2B,我们还合成了 [Tc]MURB2(一种具有双价 UR 的 [Tc]MHam 复合物),并评估了 [Tc]URB2A、[Tc]URB2B 和 [Tc]MURB2 的 CA-IX 特异性结合亲和力。它们对 HT-29 细胞的摄取被 CA 抑制剂乙酰唑胺的加入所减少,表明它们具有 CA-IX 特异性结合亲和力。用对 HT-29 细胞具有最高特异性的 [Tc]URB2A 和 [Tc]MURB2 进行 HT-29 荷瘤小鼠的生物分布研究。[Tc]URB2A 显示出中等的肿瘤摄取,并通过与乙酰唑胺共注射而减少;然而,肿瘤/血液比对于体内成像不足。这些结果为设计针对 CA-IX 的新型 Ham 基成像探针提供了关键信息。

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