Preclinical Investigations to Explore the Difference between the Diastereomers [ 177 Lu]Lu-SibuDAB and [ 177 Lu]Lu-RibuDAB toward Prostate Cancer Therapy.

[ 177 Lu]Lu-Ibu-DAB-PSMA, a radioligand modified with ibuprofen as the albumin binder, showed higher accumulation in PSMA-positive tumors of mice than the clinically used [ 177 Lu]Lu-PSMA-617 but lower retention in non-targeted tissues than previously developed albumin-binding PSMA radioligands. The aim of this study was to investigate whether the stereochemistry of the incorporated ibuprofen affects the radioligand's in vitro and in vivo properties and to select the more favorable radioligand for further development. For this purpose, SibuDAB and RibuDAB containing ( S )- and ( R )-ibuprofen, respectively, were synthesized and labeled with lutetium-177. In vitro , the two isomers had similar properties; however, [ 177 Lu]Lu-SibuDAB showed increased binding to mouse and human plasma proteins (91 ± 1 and 88 ± 2%, respectively) compared to [ 177 Lu]Lu-RibuDAB (75 ± 2 and 79 ± 2%, respectively). In vivo , [ 177 Lu]Lu-SibuDAB was metabolically more stable than [ 177 Lu]Lu-RibuDAB with ∼90 vs ∼67% intact radioligand detected in the blood at 4 h post injection (p.i.). In line with the lower albumin-binding affinity, the blood clearance of [ 177 Lu]Lu-RibuDAB in mice was considerably faster [27% of injected activity (% IA), 1 h p.i.] than for [ 177 Lu]Lu-SibuDAB (50% IA, 1 h p.i.). Time-dependent biodistribution studies performed in tumor-bearing athymic nude mice showed high PSMA-specific tumor uptake for both isomers. A twofold increased area under the curve (AUC 0→8d ) of the blood retention was determined for [ 177 Lu]Lu-SibuDAB as compared to [ 177 Lu]Lu-RibuDAB, whereas the kidney AUC 0→8d value of [ 177 Lu]Lu-SibuDAB was only half as high as for [ 177 Lu]Lu-RibuDAB. As a result, a more favorable tumor-to-kidney AUC 0→8d ratio was obtained for [ 177 Lu]Lu-SibuDAB, which was also visualized on SPECT/CT images. Based on its improved kidney clearance and higher metabolic stability, [ 177 Lu]Lu-SibuDAB was selected as the more favorable radioligand. Therapy studies performed with [ 177 Lu]Lu-SibuDAB (5 MBq/mouse) demonstrated the anticipated therapeutic superiority over the current gold-standard [ 177 Lu]Lu-PSMA-617 (5 MBq/mouse). The significantly increased survival time of mice treated with [ 177 Lu]Lu-SibuDAB as compared to those injected with [ 177 Lu]Lu-PSMA-617 justifies further development of this novel radioligand toward clinical application.