Development and evaluation of a new modular nanotransporter for drug delivery into nuclei of pathological cells expressing folate receptors

Slastnikova, Tatiana A.; Rosenkranz, Andrey A.; Khramtsov, Yuri V.; Karyagina, Tatiana S; Ovechko, Sergey A; Соболев, А. С.

doi:10.2147/dddt.s127270

Cited by 26 publications

(34 citation statements)

References 43 publications

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“…As 111 In Auger electrons have extremely short ranges, their cytotoxicity was highest when they were localized in the nucleus (Li et al, 2015;Slastnikova et al, 2017a). Thus, we measured the ability of 111 In-NOTA-MNT to accumulate in the nuclei.…”

Section: Resultsmentioning

confidence: 99%

“…Labeling MNT With 111 In Using p-SCN-Bn-NOTA MNT C-EGF , MNT N-affibody , and MNT N-EGF were labeled in accordance with a previously published protocol (Slastnikova et al, 2017a). MNT were incubated with 10-fold molar excess of the bifunctional p-SCN-Bn-NOTA chelator in conjugation carbonate buffer at pH 8.6 (Hens et al, 2009) for 20 h at room temperature with final concentrations of MNT ≥1.5 mg/ml.…”

Section: Interactions Of the Mnt With A/b Importins Evaluated By Thermentioning

confidence: 99%

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Targeted Delivery of 111In Into the Nuclei of EGFR Overexpressing Cells via Modular Nanotransporters With Anti-EGFR Affibody

et al. 2020

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Since cell nucleus is one of the most vulnerable compartments, the maximum therapeutic effect from a variety of locally acting agents, such as photosensitizers, alfa-emitters, Auger electron emitters, will be expected when they get there. Therefore, the targeted delivery of these agents into the nuclei of target tumor cells is necessary for their anticancer effects and minimization of side effects. Modular nanotransporters (MNT) are artificial polypeptides comprising several predefined modules that recognize target cell, launching their subsequent internalization, escape from endosomes, and transport the drug load to the nucleus. This technology significantly enhances the cytotoxicity of locally acting drugs in vitro and in vivo. Epidermal growth factor receptors (EGFR) are useful molecular targets as they are overexpressed in glioblastoma, head-and-neck cancer, bladder cancer, and other malignancies. Here, we examined the possibility of using internalizable anti-EGFR affibody as an EGFR-targeting MNT module for drug transport into the cancer cell nuclei. It binds to both murine and human EGFR facilitating preclinical studies. We showed that MNT with affibody on the N-terminus (MNT N-affibody ) effectively delivered the Auger electron emitter 111 In to target cell nuclei and had pronounced cytotoxic efficacy against EGFR-overexpressing human A431 epidermoid carcinoma cells. Using EGFR-expressing human adenocarcinoma MCF-7 cells, we demonstrated that in contrast to MNT with N-terminal epidermal growth factor (EGF), MNT N-affibody and MNT with EGF on the C-terminus did not stimulate cancer cell proliferation.

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Section: Resultsmentioning

confidence: 99%

Section: Interactions Of the Mnt With A/b Importins Evaluated By Thermentioning

confidence: 99%

Targeted Delivery of 111In Into the Nuclei of EGFR Overexpressing Cells via Modular Nanotransporters With Anti-EGFR Affibody

et al. 2020

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“…They showed superior uptake and cytotoxicity over 67 Ga-hEGF, which was attributed to improved nuclear retention. This MNT has been used with various other ligand modules (melanocortin receptor and folate receptor ligands) and radionuclides ( 111 In, 125 I) ( Slastnikova et al, 2012 , 2017a , b ), and has recently been reviewed by Sobolev (2018) .…”

Section: Subcellular Targets For Radionuclide Therapymentioning

confidence: 99%

Subcellular Targeting of Theranostic Radionuclides

et al. 2018

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The last decade has seen rapid growth in the use of theranostic radionuclides for the treatment and imaging of a wide range of cancers. Radionuclide therapy and imaging rely on a radiolabeled vector to specifically target cancer cells. Radionuclides that emit β particles have thus far dominated the field of targeted radionuclide therapy (TRT), mainly because the longer range (μm–mm track length) of these particles offsets the heterogeneous expression of the molecular target. Shorter range (nm–μm track length) α- and Auger electron (AE)-emitting radionuclides on the other hand provide high ionization densities at the site of decay which could overcome much of the toxicity associated with β-emitters. Given that there is a growing body of evidence that other sensitive sites besides the DNA, such as the cell membrane and mitochondria, could be critical targets in TRT, improved techniques in detecting the subcellular distribution of these radionuclides are necessary, especially since many β-emitting radionuclides also emit AE. The successful development of TRT agents capable of homing to targets with subcellular precision demands the parallel development of quantitative assays for evaluation of spatial distribution of radionuclides in the nm–μm range. In this review, the status of research directed at subcellular targeting of radionuclide theranostics and the methods for imaging and quantification of radionuclide localization at the nanoscale are described.

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“…Following intratumoral administration of folate-MNT- 111 In, normal tissues showed low radioactivity, which was mostly limited to liver and kidney (Slastnikova et al, 2017b). Intratumoral (B16F1 melanoma, C57BL/6J mice) retention of intratumorally injected 111 In-DTox-HMP-NLS-MSH was even better: 3.7 days as fitted to a single exponential.…”

Section: Modular Nanotransporters: In Vivo Delivery Of Auger Electronmentioning

confidence: 99%

Modular Nanotransporters for Nuclear-Targeted Delivery of Auger Electron Emitters

Соболев

2018

Front. Pharmacol.

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This review describes artificial modular nanotransporters (MNTs) delivering their cargos into target cells and then into the nuclei – the most vulnerable cell compartment for most anticancer agents and especially for radionuclides emitting short-range particles. The MNT strategy uses natural subcellular transport processes inherent in practically all cells including cancer cells. The MNTs use these processes just as a passenger who purchased tickets for a multiple-transfer trip making use of different kinds of public transport to reach the desired destination. The MNTs are fusion polypeptides consisting of several parts, replaceable modules, accomplishing binding to a specific receptor on the cell and subsequent internalization, endosomal escape and transport into the cell nucleus. Radionuclides emitting short-range particles, like Auger electron emitters, acquire cell specificity and significantly higher cytotoxicity both in vitro and in vivo when delivered by the MNTs into the nuclei of cancer cells. MNT modules are interchangeable, allowing replacement of receptor recognition modules, which permits their use for different types of cancer cells and, as a cocktail of several MNTs, for targeting several tumor-specific molecules for personalized medicine.

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Development and evaluation of a new modular nanotransporter for drug delivery into nuclei of pathological cells expressing folate receptors

Cited by 26 publications

References 43 publications

Targeted Delivery of 111In Into the Nuclei of EGFR Overexpressing Cells via Modular Nanotransporters With Anti-EGFR Affibody

Targeted Delivery of 111In Into the Nuclei of EGFR Overexpressing Cells via Modular Nanotransporters With Anti-EGFR Affibody

Subcellular Targeting of Theranostic Radionuclides

Modular Nanotransporters for Nuclear-Targeted Delivery of Auger Electron Emitters

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