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In vitro binding evaluation of 177Lu-AMBA, a novel 177Lu-labeled GRP-R agonist for systemic radiotherapy in human tissues

机译:177 Lu-AMBA(新型 177 Lu标记的GRP-R激动剂)在人体组织中的体外结合评价

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Members of the gastrin-releasing peptide (GRP) family and its analogs bombesin (BBN) have been implicated in the biology of several human cancers including prostate, breast, colon and lung. To date, three mammalian GRP/BBN receptor subtypes have been cloned and characterized: the neuromedin B receptor (NMBR), the GRP receptor (GRPR) and the BBN-receptor subtype 3 (BB3). The fourth BBN receptor subtype, BB4, has only been identified in amphibian and at present no mammalian equivalent of this receptor has been described. GRPR analogs have been used as carriers to deliver drugs, radionuclides and cytotoxins to target various cancer types that are GRPR positive. We investigated the in vitro binding properties of 177Lu-AMBA, a novel radiolabelled BBN analog currently undergoing clinical trial as systemic radiotherapy for hormone refractory prostate cancer (HRPC) patients. Pharmacological analyses of the 177Lu-AMBA was determined using in vitro binding studies using membrane target system containing specific receptor subtypes. We investigated the distribution of binding sites for 177Lu-AMBA by receptor autoradiography on human neoplastic and non-neoplastic tissues. Pharmacological characterizations of 177Lu-AMBA shows, high affinity towards NMB and GRP receptors, while little or no affinity towards BB3 receptor. Among the 40 different types of non-neoplastic tissues tested seven of them showed limited but specific binding of 177Lu-AMBA. Fourteen of 17 primary prostate cancers, six of 13 primary breast cancers expressed binding sites for 177Lu-AMBA. Furthermore, no apparent differences in 177Lu-AMBA-binding sites expression were observed between matched pairs (primary vs. secondary) of prostate and breast cancer tissues. These data represent the molecular basis for clinical applications of 177Lu-AMBA for diagnosis and treatment of GRP-R and NMB-R positive tumors.
机译:胃泌素释放肽(GRP)家族的成员及其类似物蛙皮素(BBN)已与包括前列腺癌,乳腺癌,结肠癌和肺癌在内的几种人类癌症有关。迄今为止,已经克隆并表征了三种哺乳动物GRP / BBN受体亚型:神经调节素B受体(NMBR),GRP受体(GRPR)和BBN受体亚型3(BB 3 )。仅在两栖动物中鉴定出第四种BBN受体亚型BB 4 ,目前尚未描述该受体的哺乳动物等效物。 GRPR类似物已用作载体,以递送药物,放射性核素和细胞毒素,以靶向多种GRPR阳性的癌症。我们研究了 177 Lu-AMBA的体外结合特性,这是一种新型的放射性标记的BBN类似物,目前正在接受临床试验作为激素难治性前列腺癌(HRPC)患者的全身放疗。 177 Lu-AMBA的药理学分析是使用包含特定受体亚型的膜靶系统通过体外结合研究确定的。我们通过受体放射自显影技术研究了人类肿瘤和非肿瘤组织上 177 Lu-AMBA结合位点的分布。 177 Lu-AMBA的药理特性表明,它对NMB和GRP受体的亲和力很高,而对BB 3 受体的亲和力很小或没有。在测试的40种不同类型的非肿瘤组织中,有7种显示出 177 Lu-AMBA的结合有限但特异性。在17种原发性前列腺癌中,有14种在13种原发性乳腺癌中有6种表达了 177 Lu-AMBA的结合位点。此外,在前列腺和乳腺癌组织的匹配对(原发与继发)之间未观察到 177 Lu-AMBA结合位点表达的明显差异。这些数据代表了 177 Lu-AMBA在GRP-R和NMB-R阳性肿瘤的诊断和治疗中的临床应用的分子基础。

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