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F 标记的聚乙二醇化 Sansalvamide A 十肽的开发和临床前评价用于胰腺癌中 HSP90 状态的无创评估。

Development and Preclinical Evaluation of F-Labeled PEGylated Sansalvamide A Decapeptide for Noninvasive Evaluation of Hsp90 Status in Pancreas Cancer.

机构信息

Department of Nuclear Medicine, The First Hospital of Lanzhou University, Lanzhou 730000, China.

Molecular Imaging Center, Department of Radiology, Keck School of Medicine, University of Southern California, Los Angeles 90033, United States.

出版信息

Mol Pharm. 2024 Oct 7;21(10):5238-5246. doi: 10.1021/acs.molpharmaceut.4c00643. Epub 2024 Sep 24.

DOI:10.1021/acs.molpharmaceut.4c00643
PMID:39316366
Abstract

Heat shock protein 90 (Hsp90) is a promising target for cancer therapy and imaging. Accurate detection of Hsp90 levels in tumors via noninvasive PET imaging might be beneficial for management. To achieve this, the precursor compound Dimer-Sansalvamide A (Dimer-San A) was PEGylated and modified by conjugating it with the bifunctional chelator 1,4,7-triazacyclononane-1,4,7-triacetic acid (NOTA). The F-labeled PEGylated Dimer-SanA decapeptide (F-PEGylated San A) was completed within 30 min using a two-step process. stability and specificity were assessed, including competition studies with the Hsp90 inhibitor 17-allylamino-17-demethoxygeldanamycin (17-AAG). MicroPET imaging was performed on PL45 tumor-bearing mice to evaluate probe accumulation and tumor-to-muscle ratios. Biodistribution studies determined the route of excretion. The probe resulted in a radiochemical yield of 23.11% with a purity exceeding 95%. , F-PEGylated San A exhibited high stability and selectively accumulated in Hsp90-positive PL45 cells, with binding effectively blocked by the Hsp90 inhibitor 17AAG, confirming its specificity. MicroPET imaging of PL45 tumor-bearing mice showed significant probe accumulation in tumor tissues at 1 and 2 h postinjection (4.06 ± 0.30 and 3.72 ± 0.61%ID/g, respectively), with optimal tumor-to-muscle ratios observed at 2 h postinjection (6.09 ± 1.92). While F-PEGylated San A demonstrates enhanced water solubility, as indicated by increased kidney uptake relative to liver accumulation. The study successfully incorporated PEG units to create the novel probe F-PEGylated San A targeting to Hsp90 without affecting its targeting capability, aimed at improving the pharmacokinetics and PET imaging of Hsp90 expression noninvasively.

摘要

热休克蛋白 90(Hsp90)是癌症治疗和成像的有前途的靶点。通过非侵入性的 PET 成像准确检测肿瘤中的 Hsp90 水平可能有助于管理。为了实现这一目标,前体化合物二聚体-Sansalvamide A(Dimer-San A)被聚乙二醇化并通过与双功能螯合剂 1,4,7-三氮杂环壬烷-1,4,7-三乙酸(NOTA)缀合进行修饰。F-标记的聚乙二醇化 Dimer-SanA 十肽(F-PEGylated San A)在 30 分钟内通过两步法完成。评估了稳定性和特异性,包括与 Hsp90 抑制剂 17-烯丙基-17-去甲氧基格尔德霉素(17-AAG)的竞争研究。对携带 PL45 肿瘤的小鼠进行 MicroPET 成像,以评估探针的积累和肿瘤与肌肉的比值。生物分布研究确定了排泄途径。探针的放射化学产率为 23.11%,纯度超过 95%。F-PEGylated San A 表现出高稳定性,并选择性地积聚在 Hsp90 阳性的 PL45 细胞中,Hsp90 抑制剂 17AAG 有效阻断了结合,证实了其特异性。携带 PL45 肿瘤的小鼠的 MicroPET 成像显示,在注射后 1 和 2 小时,探针在肿瘤组织中显著积累(分别为 4.06±0.30 和 3.72±0.61%ID/g),在注射后 2 小时观察到最佳的肿瘤与肌肉比值(6.09±1.92)。虽然 F-PEGylated San A 表现出更高的水溶性,这表明与肝脏积累相比,肾脏摄取增加。该研究成功地将 PEG 单元整合到新型探针 F-PEGylated San A 中,以针对 Hsp90,而不影响其靶向能力,旨在改善 Hsp90 表达的药代动力学和 PET 成像的非侵入性。

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