{"database":"biostudies-literature","file_versions":[],"scores":null,"additional":{"omics_type":["Unknown"],"volume":["63(10)"],"submitter":["Wurzer A"],"pubmed_abstract":["The prostate-specific membrane antigen (PSMA)-targeted radiohybrid (rh) ligand [<sup>177</sup>Lu]Lu-rhPSMA-7.3 has recently been assessed in a pretherapeutic dosimetry study on prostate cancer patients. In comparison to [<sup>177</sup>Lu]Lu-PSMA I&T, application of [<sup>177</sup>Lu]Lu-rhPSMA-7.3 resulted in a significantly improved tumor dose but also higher kidney accumulation. Although rhPSMA-7.3 has been initially selected as the lead compound for diagnostic application based on the characterization of its gallium complex, a systematic comparison of the most promising <sup>177</sup>Lu-labeled rhPSMA ligands is still missing. Thus, this study aimed to identify the rhPSMA ligand with the most favorable pharmacokinetics for <sup>177</sup>Lu-radioligand therapy. <b>Methods:</b> The 4 isomers of [<sup>177</sup>Lu]Lu-rhPSMA-7 (namely [<sup>177</sup>Lu]Lu-rhPSMA-7.1, -7.2, -7.3, and -7.4), along with the novel radiohybrid ligands [<sup>177</sup>Lu]Lu-rhPSMA-10.1 and -10.2, were compared with the state-of-the-art compounds [<sup>177</sup>Lu]Lu-PSMA I&T and [<sup>177</sup>Lu]Lu-PSMA-617. The comparative evaluation comprised affinity studies (half-maximal inhibitory concentration) and internalization experiments on LNCaP cells, as well as lipophilicity measurements. In addition, we determined the apparent molecular weight (AMW) of each tracer as a parameter for human serum albumin (HSA) binding. Biodistribution studies and small-animal SPECT imaging were performed on LNCaP-tumor bearing mice at 24 h after injection. <b>Results:</b> <sup>177</sup>Lu labeling of the radiohybrids was performed according to the established procedures for the currently established PSMA-targeted ligands. All ligands showed potent binding to PSMA-expressing LNCaP cells, with affinities in the low nanomolar range and high internalization rates. Surprisingly, the most pronounced differences regarded the HSA-related AMW. Although [<sup>177</sup>Lu]Lu-rhPSMA-7 isomers demonstrated the highest AMW and thus strongest HSA interactions, [<sup>177</sup>Lu]Lu-rhPSMA-10.1 showed an AMW lower than for [<sup>177</sup>Lu]Lu-rhPSMA-7.3 but higher than for the <sup>177</sup>Lu-labeled references PSMA I&T and PSMA-617. In biodistribution studies, [<sup>177</sup>Lu]Lu-rhPSMA-10.1 exhibited the lowest kidney uptake and fastest excretion from the blood pool of all rhPSMA ligands while preserving a high tumor accumulation. <b>Conclusion:</b> Clinical investigation of [<sup>177</sup>Lu]Lu-rhPSMA-10.1 is highly warranted to determine whether the favorable pharmacokinetics observed in mice will also result in high tumor uptake and decreased absorbed dose to kidneys and other nontarget tissues in patients."],"journal":["Journal of nuclear medicine : official publication, Society of Nuclear Medicine"],"pagination":["1489-1495"],"full_dataset_link":["https://www.ebi.ac.uk/biostudies/studies/S-EPMC9536713"],"repository":["biostudies-literature"],"pubmed_title":["Synthesis and Preclinical Evaluation of <sup>177</sup>Lu-Labeled Radiohybrid PSMA Ligands for Endoradiotherapy of Prostate Cancer."],"pmcid":["PMC9536713"],"pubmed_authors":["Beck R","Fischer S","Weber W","D'Alessandria C","Wurzer A","Rose F","Kunert JP","Wester HJ","Felber V"],"additional_accession":[]},"is_claimable":false,"name":"Synthesis and Preclinical Evaluation of <sup>177</sup>Lu-Labeled Radiohybrid PSMA Ligands for Endoradiotherapy of Prostate Cancer.","description":"The prostate-specific membrane antigen (PSMA)-targeted radiohybrid (rh) ligand [<sup>177</sup>Lu]Lu-rhPSMA-7.3 has recently been assessed in a pretherapeutic dosimetry study on prostate cancer patients. In comparison to [<sup>177</sup>Lu]Lu-PSMA I&T, application of [<sup>177</sup>Lu]Lu-rhPSMA-7.3 resulted in a significantly improved tumor dose but also higher kidney accumulation. Although rhPSMA-7.3 has been initially selected as the lead compound for diagnostic application based on the characterization of its gallium complex, a systematic comparison of the most promising <sup>177</sup>Lu-labeled rhPSMA ligands is still missing. Thus, this study aimed to identify the rhPSMA ligand with the most favorable pharmacokinetics for <sup>177</sup>Lu-radioligand therapy. <b>Methods:</b> The 4 isomers of [<sup>177</sup>Lu]Lu-rhPSMA-7 (namely [<sup>177</sup>Lu]Lu-rhPSMA-7.1, -7.2, -7.3, and -7.4), along with the novel radiohybrid ligands [<sup>177</sup>Lu]Lu-rhPSMA-10.1 and -10.2, were compared with the state-of-the-art compounds [<sup>177</sup>Lu]Lu-PSMA I&T and [<sup>177</sup>Lu]Lu-PSMA-617. The comparative evaluation comprised affinity studies (half-maximal inhibitory concentration) and internalization experiments on LNCaP cells, as well as lipophilicity measurements. In addition, we determined the apparent molecular weight (AMW) of each tracer as a parameter for human serum albumin (HSA) binding. Biodistribution studies and small-animal SPECT imaging were performed on LNCaP-tumor bearing mice at 24 h after injection. <b>Results:</b> <sup>177</sup>Lu labeling of the radiohybrids was performed according to the established procedures for the currently established PSMA-targeted ligands. All ligands showed potent binding to PSMA-expressing LNCaP cells, with affinities in the low nanomolar range and high internalization rates. Surprisingly, the most pronounced differences regarded the HSA-related AMW. Although [<sup>177</sup>Lu]Lu-rhPSMA-7 isomers demonstrated the highest AMW and thus strongest HSA interactions, [<sup>177</sup>Lu]Lu-rhPSMA-10.1 showed an AMW lower than for [<sup>177</sup>Lu]Lu-rhPSMA-7.3 but higher than for the <sup>177</sup>Lu-labeled references PSMA I&T and PSMA-617. In biodistribution studies, [<sup>177</sup>Lu]Lu-rhPSMA-10.1 exhibited the lowest kidney uptake and fastest excretion from the blood pool of all rhPSMA ligands while preserving a high tumor accumulation. <b>Conclusion:</b> Clinical investigation of [<sup>177</sup>Lu]Lu-rhPSMA-10.1 is highly warranted to determine whether the favorable pharmacokinetics observed in mice will also result in high tumor uptake and decreased absorbed dose to kidneys and other nontarget tissues in patients.","dates":{"release":"2022-01-01T00:00:00Z","publication":"2022 Oct","modification":"2025-04-26T04:50:47.301Z","creation":"2025-04-06T11:13:36.377Z"},"accession":"S-EPMC9536713","cross_references":{"pubmed":["35086894"],"doi":["10.2967/jnumed.121.263371"]}}