Solid phase synthesis in the development of magnetic resonance imaging probes

Connah, Liam; Angelovski, Goran

doi:10.1039/d0qo00921k

Cited by 6 publications

(5 citation statements)

References 138 publications

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“…As shown in Figure a, six different peptoid sequences ( Pep-1 – Pep-6 ) with different numbers and chemistries of ligands were synthesized. Npy, Nqn, and Do3a were selected as ligands because they are known to coordinate transitional metal cations. ,, The Co 2+ cation was selected because of a notable enhancement in the activity of PTE when native Zn 2+ was substituted by Co 2+ . The catalytic activities of Co 2+ -containing peptoid nanomembranes made from Pep-1 to Pep-6 were tested in NEM buffer (pH 10) at room temperature.…”

Section: Resultsmentioning

confidence: 99%

Designed Metal-Containing Peptoid Membranes as Enzyme Mimetics for Catalytic Organophosphate Degradation

Trinh,

Jian,

Jin

et al. 2023

ACS Appl. Mater. Interfaces

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The detoxification of lethal organophosphate (OP) residues in the environment is crucial to prevent human exposure and protect modern society. Despite serving as excellent catalysts for OP degradation, natural enzymes require costly preparation and readily deactivate upon exposure to environmental conditions. Herein, we designed and prepared a series of phosphotriesterase mimics based on stable, self-assembled peptoid membranes to overcome these limitations of the enzymes and effectively catalyze the hydrolysis of dimethyl p-nitrophenyl phosphate (DMNP)�a nerve agent simulant. By covalently attaching metal-binding ligands to peptoid N-termini, we attained enzyme mimetics in the form of surface-functionalized crystalline nanomembranes. These nanomembranes display a precisely controlled arrangement of coordinated metal ions, which resemble the active sites found in phosphotriesterases to promote DMNP hydrolysis. Moreover, using these highly programmable peptoid nanomembranes allows for tuning the local chemical environment of the coordinated metal ion to achieve enhanced hydrolysis activity. Among the crystalline membranes that are active for DMNP degradation, those assembled from peptoids containing bis-quinoline ligands with an adjacent phenyl side chain showed the highest hydrolytic activity with a 219-fold rate acceleration over the background, demonstrating the important role of the hydrophobic environment in proximity to the active sites. Furthermore, these membranes exhibited remarkable stability and were able to retain their catalytic activity after heating to 60 °C and after multiple uses. This work provides insights into the principal features to construct a new class of biomimetic materials with high catalytic efficiency, cost-effectiveness, and reusability applied in nerve agent detoxification.

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Section: Resultsmentioning

confidence: 99%

Designed Metal-Containing Peptoid Membranes as Enzyme Mimetics for Catalytic Organophosphate Degradation

Trinh,

Jian,

Jin

et al. 2023

ACS Appl. Mater. Interfaces

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“…3 A variety of peptides have been fabricated in a combinatorial fashion to explore biochemical mechanisms, 10,11 develop new functional materials, 12,13 and create artificial enzymes. 14,15 To further improve bioactivity, bioavailability, and structural diversity, many unnatural inorganic residues-including metal clusters, [16][17][18] polyhedral oligomeric silsesquioxane (POSS), 19 and oligonuclear transition metal coordination complexes 18,20,21 -have been incorporated as non-canonical amino acids into peptide sequences through manual synthesis. This is important since such compounds can serve as spectroscopic or photo-affinity probes for bioassays, [18][19][20] cancer diagnoses, 16,17 and cancer-targeted therapy.…”

Section: Introductionmentioning

confidence: 99%

“…14,15 To further improve bioactivity, bioavailability, and structural diversity, many unnatural inorganic residues-including metal clusters, [16][17][18] polyhedral oligomeric silsesquioxane (POSS), 19 and oligonuclear transition metal coordination complexes 18,20,21 -have been incorporated as non-canonical amino acids into peptide sequences through manual synthesis. This is important since such compounds can serve as spectroscopic or photo-affinity probes for bioassays, [18][19][20] cancer diagnoses, 16,17 and cancer-targeted therapy. 21,22 However, there is a lack of configurability regarding charge density, redox activity, and the introduction of radical new structures and coordination systems.…”

Section: Introductionmentioning

confidence: 99%

Robotic synthesis of peptides containing metal-oxide-based amino acids

She¹,

Bell²,

Zheng³

et al. 2022

Chem

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“…37 Solid-phase synthesis has been advantageously used for the development of complex and specific MRI probes. 48 Success of the strategy depends on accumulation of the vector−contrastophore conjugate on the cell surface or inside the cell and therefore on its access to tumor cells, its affinity for the receptor, and the concentration of the receptor. If internalized, the intracellular trafficking pathway taken by the conjugates might have an effect because its trapping in a sub-cellular vesicle/endosome/ lysosome can quench the expected relaxation rate gain 49,50 and/or lead to the release of free toxic gadolinium.…”

Section: ■ Introductionmentioning

confidence: 99%

“…This goal may be pursued using nanoparticles, polymers, dendrimers, liposomes, or microemulsion-conjugating multiple contrastophores to the targeting moiety − and/or taking advantage of receptor-mediated internalization to accumulate the targeted contrastophores . Solid-phase synthesis has been advantageously used for the development of complex and specific MRI probes . Success of the strategy depends on accumulation of the vector–contrastophore conjugate on the cell surface or inside the cell and therefore on its access to tumor cells, its affinity for the receptor, and the concentration of the receptor.…”

Section: Introductionmentioning

confidence: 99%

High-Relaxivity Molecular MRI Contrast Agent to Target Gb3-Expressing Cancer Cells

et al. 2022

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Targeted contrast agents (CAs) can improve magnetic resonance imaging (MRI) for accurate cancer diagnosis. In this work, we used the Shiga toxin B-subunit (STxB) as a targeting agent, which binds to Gb3, a glycosphingolipid highly overexpressed on the surface of tumor cells. We developed STxB-targeted MRI probes from cyclic peptide scaffolds functionalized with six to nine monoamide DO3A[Gd(III)] chelates. The influence of structural constraints on the longitudinal relaxivity (r 1) of the CAs has been studied. The cyclic peptide carrying nine monoamide DO3A[Gd(III)] exhibited a r 1 per compound of 32 and 93 mM–1s–1 at 9.4 and 1.5 T, respectively. Its conjugation to the pentameric STxB protein led to a 70 kDa compound with a higher r 1 of 150 and 475 mM–1 s–1 at 9.4 and 1.5 T, respectively. Specific accumulation and cellular distribution of this conjugate in Gb3-expressing cancer cells were demonstrated using immunofluorescence microscopy and quantified by an inductively coupled plasma–mass spectrometry dosage of Gd(III). Such an agent should enable the in vivo detection by MRI of tumors expressing Gb3 receptors.

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Solid phase synthesis in the development of magnetic resonance imaging probes

Abstract: We review the use of the solid phase synthesis methodology for the preparation of diverse and potent MRI probes.

Cited by 6 publications

References 138 publications

Designed Metal-Containing Peptoid Membranes as Enzyme Mimetics for Catalytic Organophosphate Degradation

Designed Metal-Containing Peptoid Membranes as Enzyme Mimetics for Catalytic Organophosphate Degradation

Robotic synthesis of peptides containing metal-oxide-based amino acids

High-Relaxivity Molecular MRI Contrast Agent to Target Gb3-Expressing Cancer Cells

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