Initial In Vitro and In Vivo Evaluation of a Novel CCK2R Targeting Peptide Analog Labeled with Lutetium-177

Hörmann, Anton Amadeus; Klingler, Maximilian; Rezaeianpour, Maliheh; Hörmann, Nikolas; Gust, Ronald; Shahhosseini, Soraya; Guggenberg, Elisabeth von

doi:10.3390/molecules25194585

Cited by 12 publications

(17 citation statements)

References 41 publications

(70 reference statements)

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“…Therefore, truncated analogues of CP04 1 have also been investigated, including the peptide MG11 2 that lacks all N-terminal glutamic acid residues. This shortened peptide displayed significantly reduced renal uptake and retention, spurring additional refinements of the core MG11 2 structure to further reduce kidney uptake and enhance tumor targeting (Erba et al 2018;Grob et al 2020;Hörmann et al 2020;Klingler et al 2019;Maximilian et al 2020;Uprimny et al 2020).…”

Section: Introductionmentioning

confidence: 98%

Investigation of Fluorine-18 Labelled Peptides for Binding to Cholecystokinin-2 Receptors with High Affinity

Khan

Corlett

Hutton

et al. 2021

Int J Pept Res Ther

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Many cancers of neuroendocrine origin overexpress cholecystokinin-2 receptors (CCK-2R) including medullary thyroid cancer, small cell lung cancer and other lung carcinoids. Fluorine-18 labelled peptides targeting CCK-2R enable direct visualization and quantification of this receptor in vivo using positron emission tomography imaging. CP04 1 and MG11 2 are two previously described truncated peptides derived from the native CCK-2R hormone ligand, gastrin. The N-terminus of the MG11 2 octopeptide was chemically modified with various fluorine containing aromatic (4-fluorobenzoate), heterocyclic (6-fluoronicotinate) and aliphatic (2-fluoropropionate) moieties. To assess the impact these modifications had on CCK-2R binding, ligand-binding assays were conducted using A431 cells overexpressing human CCK-2R. MG11 2 modified by 4-fluorobenzoate (FB-MG11 3) demonstrated the highest binding affinity (0.20 nM) followed by MG11 2 modified by 6-fluoronicotinate (FNic-MG11 4; 0.74 nM) and 2-fluoropropionate (FP-MG11 5; 1.80 nM), respectively. Whilst indirect labelling of MG11 2 using fluorine-18 labelled activated esters of fluorobenzoate and 6-fluoronicotinate was unsuccessful, direct fluorine-18 labelling at the N-terminus modified with 6-nitronicotinate afforded a 47.6% radiochemical yield of [18F]FNic-MG11. Unfortunately, [18F]FNic-MG11 4 was chemically unstable, decomposing slowly through defluorination, thereby impeding any further work with this radiotracer.

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Section: Introductionmentioning

confidence: 98%

Investigation of Fluorine-18 Labelled Peptides for Binding to Cholecystokinin-2 Receptors with High Affinity

Khan

Corlett

Hutton

et al. 2021

Int J Pept Res Ther

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“…Among three different peptide derivatives with proline substitution studied, DOTA-MGS8 radiolabeled with indium-111 and lutetium-177 showed the most promising advantages in terms of enhanced tumor uptake with concomitant low kidney uptake [ 16 ]. A stabilizing effect against enzymatic degradation in vivo could be observed, as demonstrated by the absence of the metabolites with cleavage at position DGlu-Pro, Pro-Tyr and Tyr-Gly in the blood and urine of mice intravenously injected with [ 177 Lu]Lu-DOTA-MGS8 [ 29 ]. Thus, a considerable reduction of the enzymatic degradation compared to [ 111 In]In-DOTA-MG11 could be achieved [ 11 , 24 ].…”

Section: Discussionmentioning

confidence: 99%

Automated Synthesis of 68Ga-Labeled DOTA-MGS8 and Preclinical Characterization of Cholecystokinin-2 Receptor Targeting

et al. 2022

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The new minigastrin analog DOTA-MGS8 targeting the cholecystokinin-2 receptor (CCK2R) used in this study displays the combination of two site-specific modifications within the C-terminal receptor binding sequence together with an additional N-terminal amino acid substitution preventing fast metabolic degradation. Within this study, the preparation of 68Ga-labeled DOTA-MGS8 was validated using an automated synthesis module, describing the specifications and analytical methods for quality control for possible clinical use. In addition, preclinical studies were carried out to characterize the targeting potential. [68Ga]Ga-DOTA-MGS8 showed a high receptor-specific cell internalization into AR42J rat pancreatic cells (~40%) with physiological expression of rat CCK2R as well as A431-CCK2R cells transfected to stably express human CCK2R (~47%). A favorable biodistribution profile was observed in BALB/c nude mice xenografted with A431-CCK2R cells and mock-transfected A431 cells as control. The high tumor uptake of ~27% IA/g together with low background activity and limited uptake in non-target tissue confirms the potential for high-sensitivity positron emission tomography of stabilized MG analogs in patients with MTC and other CCK2R-related malignancies.

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“…44 A common site of initial metabolic breakdown in CP04based peptides has been identified at Asp 12 −Phe 13 . 53,56 Journal of Medicinal Chemistry Therefore, we prepared one last peptide in this study with Nmethylated Nal 13 to investigate if that has any influence on the in vivo characteristics. N-methylation of Phe 13 has been shown to reduce binding affinity toward CCK-2R.…”

Section: ■ Discussionmentioning

confidence: 99%

A New Turn in Peptide-Based Imaging Agents: Foldamers Afford Improved Theranostics Targeting Cholecystokinin-2 Receptor-Positive Cancer

et al. 2021

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Proteins adopt unique folded secondary and tertiary structures that are responsible for their remarkable biological properties. This structural complexity is key in designing efficacious peptides that can mimic the three-dimensional structure needed for biological function. In this study, we employ different chemical strategies to induce and stabilize a β-hairpin fold of peptides targeting cholecystokinin-2 receptors for theranostic application (combination of a targeted therapeutic and a diagnostic companion). The newly developed peptides exhibited enhanced folding capacity as demonstrated by circular dichroism (CD) spectroscopy, ion-mobility spectrometry–mass spectrometry, and two-dimensional (2D) NMR experiments. Enhanced folding characteristics of the peptides led to increased biological potency, affording four optimal Ga-68 labeled radiotracers ([68Ga]Ga-4b, [68Ga]Ga-11b–13b) targeting CCK-2R. In particular, [68Ga]Ga-12b and [68Ga]Ga-13b presented improved metabolic stability, enhanced cell internalization, and up to 6 fold increase in tumor uptake. These peptides hold great promise as next-generation theranostic radiopharmaceuticals.

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Initial In Vitro and In Vivo Evaluation of a Novel CCK2R Targeting Peptide Analog Labeled with Lutetium-177

Cited by 12 publications

References 41 publications

Investigation of Fluorine-18 Labelled Peptides for Binding to Cholecystokinin-2 Receptors with High Affinity

Investigation of Fluorine-18 Labelled Peptides for Binding to Cholecystokinin-2 Receptors with High Affinity

Automated Synthesis of 68Ga-Labeled DOTA-MGS8 and Preclinical Characterization of Cholecystokinin-2 Receptor Targeting

A New Turn in Peptide-Based Imaging Agents: Foldamers Afford Improved Theranostics Targeting Cholecystokinin-2 Receptor-Positive Cancer

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