寡聚苯乙炔修饰RM26的177Lu标记和细胞内化研究  被引量：1

作　　者：廖伟[1] 付华霞 李祥玉 阚文涛[1] 杨夏[1] 王静[1] 赵鹏[1] 卓连刚 杨宇川[1] 魏洪源[1] LIAO Wei;FU Huaxia;LI Xiangyu;KAN Wentao;YANG Xia;WANG Jing;ZHAO Peng;ZHUO Liangang;YANG Yuchuan;WEI Hongyuan(Institute of Nuclear Physics and Chemistry,China Academy of Engineering Physics,Mianyang 621900,China;Department of Nuclear Medicine,The Affiliated Hospital of Southwest Medical University,Luzhou 646000,China)

机构地区：[1]中国工程物理研究院核物理与化学研究所,四川绵阳621900 [2]西南医科大学附属医院核医学科,四川泸州646000

出　　处：《同位素》2022年第3期200-208,共9页Journal of Isotopes

基　　金：国家自然科学基金资助项目(21906155,21976167)。

摘　　要：促胃泌素多肽受体(gastrin-releasing peptide receptor,GRPR)在多种肿瘤细胞中过度表达,可以被GRPR拮抗剂靶向。高的细胞内化率有助于提高放射性治疗药物的治疗效果,减少给药剂量。激动剂的内化率优于拮抗剂,但是严重的副作用限制了激动剂的应用。将具有跨膜能力的寡聚苯乙炔(OPE)和GRPR拮抗剂RM26偶联,可以提高拮抗剂的内化能力。本研究合成了两种多功能化合物NOTA-OPE-1-RM26和NOTA-OPE-2-RM26,分别进行^(177)Lu标记,得到了高放化纯度的标记物。标记化合物^(177)Lu-NOTA-OPEs-RM26在生理盐水、高糖培养液、新生牛血清中稳定存在。体外稳定性实验表明,引入OPE-1少量增加了化合物的内化率,而引入OPE-2显著增加了化合物的内化率。此外,引入OPE并没有改变RM26的特异性结合能力。实验结果表明,引入跨膜基团提高拮抗剂药物细胞内化率可行。Gastrin releasing peptide receptor(GRPR)is overexpressed in various tumors,and these GRPR-positive tumors have successfully and widely been targeted with GRPR antagonists.To achieve a good therapeutic effectiveness and less radioactive dosage administration,high cellular internalization is required.The cellular internalization of agonists is better than that of antagonists,but the severe side effects of agonists restrict their applications.In this study,we hypothesized that introducing membrane penetrating oligo-phenylene-ethynylene(OPE)to GRPR antagonist RM26 could increase the cellular internalization of antagonists.Therefore,two multifunctional compounds NOTA-OPE-1-RM26 and NOTA-OPE-2-RM26 were synthesized and labelled with ^(177)Lu with high efficiency.The ^(177)Lu labelled compounds ^(177)Lu-NOTA-OPEs-RM26 were stable in saline,dulbecco’s modified eagle medium(DMEM)and newborn bovine serum.The in vitro experimental results indicated that the introduction of OPE-1 slightly increased the cellular internalization of the radiolabelled compounds while OPE-2 significantly increased the cellular internalization.In addition,the introduction of OPEs did not change the specific binding ability of RM26.The investigations indicated that introducing the OPE to increase the internalization was feasible.

关 键 词：^(177)Lu RM26多肽 寡聚苯乙炔 内化率 

分 类 号：TL923[核科学技术—核燃料循环与材料] R817.5[医药卫生—影像医学与核医学]