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Small molecule targeted NIR dye conjugate for imaging LHRH receptor positive cancers

机译:小分子靶向NIR染料偶联物用于LHRH受体阳性癌症的成像

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摘要

Overexpression of Luteinizing Hormone Releasing Hormone Receptor (LHRH-R) in various cancers and restricted expression of the receptor in healthy cells qualifies it as a valuable cancer biomarker. Previously, LHRH-R targeted peptides have been utilized to deliver attached payloads to LHRH-R expressing cancers. We report here for the first time the utilization of a small molecule non-peptidic ligand (BOEPL) of LHRH-R to deliver attached payloads to LHRH-R positive tumors. For this purpose, we linked the BOEPL ligand to a near infrared dye via various linkers. In vitro, these conjugates demonstrated low nanomolar binding affinity and in vivo they exhibited receptor-mediated uptake specifically in tumor tissue. Moreover, tumor uptake could be blocked by administration of excess unlabeled conjugate, and time course experiments showed retention of the dye conjugate in the tumor up to 12 h post injection. Because uptake of BOEPL-targeted NIR dye conjugates by nonmalignant organs/tissues was negligible and since the transient presence of targeted NIR dye in the kidneys was a result of clearance mechanism, we suggest that a BOEPL-targeted NIR dye might constitute a useful agent for fluorescence-guided surgery of LHRH-R positive cancers. Moreover, our results also provide proof of concept that BOEPL can be successfully used to deliver attached payloads to LHRH-R positive tumors in vivo.
机译:黄体生成激素释放激素受体(LHRH-R)在各种癌症中的过表达以及受体在健康细胞中的受限表达使其成为有价值的癌症生物标志物。以前,LHRH-R靶向肽已用于向表达LHRH-R的癌症输送附着的有效载荷。我们在这里首次报告LHRH-R的小分子非肽配体(BOEPL)的利用,以将附着的有效载荷传递给LHRH-R阳性肿瘤。为此,我们通过各种接头将BOEPL配体连接至近红外染料。在体外,这些结合物表现出低的纳摩尔结合亲和力,在体内它们表现出受体介导的摄取,特别是在肿瘤组织中。此外,可以通过施用过量的未标记的缀合物来阻止肿瘤摄取,并且时程实验显示染料缀合物在注射后长达12小时内保留在肿瘤中。由于非恶性器官/组织对BOEPL靶向的NIR染料结合物的吸收可忽略不计,并且由于肾脏中靶向NIR染料的瞬时存在是清除机制的结果,因此我们建议以BOEPL靶向的NIR染料可能构成有用的药物LHRH-R阳性癌症的荧光引导手术。此外,我们的结果还提供了概念证明,BOEPL可成功用于将附着的有效载荷体内递送至LHRH-R阳性肿瘤。

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