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Albumin-Binding Lutetium-177-Labeled LLP2A Derivatives as Theranostics for Melanoma

Michael Pun, Fabio Gallazzi, Khanh‐Van Ho, Lisa Watkinson, Terry Carmack, Ejike Iweha, Longbo Li, Carolyn J. Anderson

2024Molecular Pharmaceutics12 citationsDOI

Abstract

Very late antigen-4 (VLA-4) is a transmembrane integrin protein that is highly expressed in aggressive forms of metastatic melanoma. A small-molecule peptidomimetic, LLP2A, was found to have a low pM affinity binding to VLA-4. Because LLP2A itself does not inhibit cancer cell proliferation and survival, it is an ideal candidate for the imaging and delivery of therapeutic payloads. An analog of [ 177 Lu]Lu-labeled-LLP2A was previously investigated as a therapeutic agent in melanoma tumor-bearing mice, resulting in only a modest improvement in tumor growth inhibition, likely due to rapid clearance of the agent from the tumor. To improve the pharmacokinetic profile, DOTAGA-PEG 4 -LLP2A with a 4-( p -iodophenyl)butyric acid (pIBA) albumin binding moiety was synthesized. We demonstrate the feasibility of this albumin binding strategy by comparing in vitro cell binding assays and in vivo biodistribution performance of [ 177 Lu]Lu-DOTAGA-PEG4-LLP2A ([ 177 Lu]Lu- 1 ) to the albumin binding [ 177 Lu]Lu-DOTAGA-pIBA-PEG 4 -LLP2A ([ 177 Lu]Lu- 2 ). In vitro cell binding assay results for [ 177 Lu]Lu- 1 and [ 177 Lu]Lu- 2 showed K d values of 0.40 ± 0.07 and 1.75 ± 0.40 nM, with similar B max values of 200 ± 6 and 315 ± 15 fmol/mg, respectively. In vivo biodistribution data for both tracers exhibited specific uptake in the tumor, spleen, thymus, and bone due to endogenous expression of VLA-4. Compound [ 177 Lu]Lu- 2 exhibited a much longer blood circulation time compared to [ 177 Lu]Lu- 1 . The tumor uptake for [ 177 Lu]Lu- 1 was highest at 1 h (∼15%ID/g) and that for [ 177 Lu]Lu- 2 was highest at 4 h (∼23%ID/g). Significant clearance of [ 177 Lu]Lu- 1 from the tumor occurs at 24 h (<5%ID/g) while[ 177 Lu]Lu- 2 is retained for greater than 96 h (∼10%ID/g). An efficacy study showed that melanoma tumor-bearing mice receiving compound [ 177 Lu]Lu- 2 given in two fractions (2 × 14.8 MBq, 14 days apart) had a greater median survival time than mice administered a single 29.6 MBq dose of compound [ 177 Lu]Lu- 1, while a single 29.6 MBq dose of [ 177 Lu]Lu- 2 imparted hematopoietic toxicity. The in vitro and in vivo data show addition of pIBA to [ 177 Lu]Lu-DOTAGA-PEG 4 -LLP2A slows blood clearance for a higher tumor uptake, and there is potential of [ 177 Lu]Lu- 2 as a theranostic in fractionated administered doses.

Topics & Concepts

LutetiumChemistryAlbuminMelanomaCancer researchRadiochemistryMedicinePharmacologyBiochemistryOrganic chemistryYttriumOxideMonoclonal and Polyclonal Antibodies ResearchNanoparticle-Based Drug DeliveryAdvanced biosensing and bioanalysis techniques
Albumin-Binding Lutetium-177-Labeled LLP2A Derivatives as Theranostics for Melanoma | Litcius