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Visualization of melanoma tumor with lectin-conjugated rare-earth doped fluoride nanocrystals

AIM: To develop specific fluorescent markers for melanoma tumor visualization, which would provide high selectivity and reversible binding pattern, by the use of carbohydrate-recognizing proteins, lectins, combined with the physical ability for imaging deep in the living tissues by utilizing red and...

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Autores principales: Dumych, Tetiana, Lutsyk, Maxym, Banski, Mateusz, Yashchenko, Antonina, Sojka, Bartlomiej, Horbay, Rostyslav, Lutsyk, Alexander, Stoika, Rostyslav, Misiewicz, Jan, Podhorodecki, Artur, Bilyy, Rostyslav
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Croatian Medical Schools 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4049210/
https://www.ncbi.nlm.nih.gov/pubmed/24891277
http://dx.doi.org/10.3325/cmj.2014.55.186
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author Dumych, Tetiana
Lutsyk, Maxym
Banski, Mateusz
Yashchenko, Antonina
Sojka, Bartlomiej
Horbay, Rostyslav
Lutsyk, Alexander
Stoika, Rostyslav
Misiewicz, Jan
Podhorodecki, Artur
Bilyy, Rostyslav
author_facet Dumych, Tetiana
Lutsyk, Maxym
Banski, Mateusz
Yashchenko, Antonina
Sojka, Bartlomiej
Horbay, Rostyslav
Lutsyk, Alexander
Stoika, Rostyslav
Misiewicz, Jan
Podhorodecki, Artur
Bilyy, Rostyslav
author_sort Dumych, Tetiana
collection PubMed
description AIM: To develop specific fluorescent markers for melanoma tumor visualization, which would provide high selectivity and reversible binding pattern, by the use of carbohydrate-recognizing proteins, lectins, combined with the physical ability for imaging deep in the living tissues by utilizing red and near infrared fluorescent properties of specific rare-earth doped nanocrystals (NC). METHODS: B10F16 melanoma cells were inoculated to C57BL/6 mice for inducing experimental melanoma tumor. Tumors were removed and analyzed by lectin-histochemistry using LABA, PFA, PNA, HPA, SNA, GNA, and NPL lectins and stained with hematoxylin and eosin. NPL lectin was conjugated to fluorescent NaGdF(4):Eu(3+)-COOH nanoparticles (5 nm) via zero length cross-linking reaction, and the conjugates were purified from unbound substances and then used for further visualization of histological samples. Fluorescent microscopy was used to visualize NPL-NaGdF(4):Eu(3+) with the fluorescent emission at 600-720 nm range. RESULTS: NPL lectin selectively recognized regions of undifferentiated melanoblasts surrounding neoangiogenic foci inside melanoma tumor, PNA lectin recognized differentiated melanoblasts, and LCA and WGA were bound to tumor stroma regions. NPL-NaGdF(4):Eu(3+) conjugated NC were efficiently detecting newly formed regions of melanoma tumor, confirmed by fluorescent microscopy in visible and near infrared mode. These conjugates possessed high photostability and were compatible with convenient xylene-based mounting systems and preserved intensive fluorescent signal at samples storage for at least 6 months. CONCLUSION: NPL lectin-NaGdF(4):Eu(3+) conjugated NC permitted distinct identification of contours of the melanoma tissue on histological sections using red excitation at 590-610 nm and near infrared emission of 700-720 nm. These data are of potential practical significance for development of glycans-conjugated nanoparticles to be used for in vivo visualization of melanoma tumor.
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spelling pubmed-40492102014-06-12 Visualization of melanoma tumor with lectin-conjugated rare-earth doped fluoride nanocrystals Dumych, Tetiana Lutsyk, Maxym Banski, Mateusz Yashchenko, Antonina Sojka, Bartlomiej Horbay, Rostyslav Lutsyk, Alexander Stoika, Rostyslav Misiewicz, Jan Podhorodecki, Artur Bilyy, Rostyslav Croat Med J Central and Eastern European Biomedical Bridges AIM: To develop specific fluorescent markers for melanoma tumor visualization, which would provide high selectivity and reversible binding pattern, by the use of carbohydrate-recognizing proteins, lectins, combined with the physical ability for imaging deep in the living tissues by utilizing red and near infrared fluorescent properties of specific rare-earth doped nanocrystals (NC). METHODS: B10F16 melanoma cells were inoculated to C57BL/6 mice for inducing experimental melanoma tumor. Tumors were removed and analyzed by lectin-histochemistry using LABA, PFA, PNA, HPA, SNA, GNA, and NPL lectins and stained with hematoxylin and eosin. NPL lectin was conjugated to fluorescent NaGdF(4):Eu(3+)-COOH nanoparticles (5 nm) via zero length cross-linking reaction, and the conjugates were purified from unbound substances and then used for further visualization of histological samples. Fluorescent microscopy was used to visualize NPL-NaGdF(4):Eu(3+) with the fluorescent emission at 600-720 nm range. RESULTS: NPL lectin selectively recognized regions of undifferentiated melanoblasts surrounding neoangiogenic foci inside melanoma tumor, PNA lectin recognized differentiated melanoblasts, and LCA and WGA were bound to tumor stroma regions. NPL-NaGdF(4):Eu(3+) conjugated NC were efficiently detecting newly formed regions of melanoma tumor, confirmed by fluorescent microscopy in visible and near infrared mode. These conjugates possessed high photostability and were compatible with convenient xylene-based mounting systems and preserved intensive fluorescent signal at samples storage for at least 6 months. CONCLUSION: NPL lectin-NaGdF(4):Eu(3+) conjugated NC permitted distinct identification of contours of the melanoma tissue on histological sections using red excitation at 590-610 nm and near infrared emission of 700-720 nm. These data are of potential practical significance for development of glycans-conjugated nanoparticles to be used for in vivo visualization of melanoma tumor. Croatian Medical Schools 2014-06 /pmc/articles/PMC4049210/ /pubmed/24891277 http://dx.doi.org/10.3325/cmj.2014.55.186 Text en Copyright © 2014 by the Croatian Medical Journal. All rights reserved. http://creativecommons.org/licenses/by/2.5/ This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Central and Eastern European Biomedical Bridges
Dumych, Tetiana
Lutsyk, Maxym
Banski, Mateusz
Yashchenko, Antonina
Sojka, Bartlomiej
Horbay, Rostyslav
Lutsyk, Alexander
Stoika, Rostyslav
Misiewicz, Jan
Podhorodecki, Artur
Bilyy, Rostyslav
Visualization of melanoma tumor with lectin-conjugated rare-earth doped fluoride nanocrystals
title Visualization of melanoma tumor with lectin-conjugated rare-earth doped fluoride nanocrystals
title_full Visualization of melanoma tumor with lectin-conjugated rare-earth doped fluoride nanocrystals
title_fullStr Visualization of melanoma tumor with lectin-conjugated rare-earth doped fluoride nanocrystals
title_full_unstemmed Visualization of melanoma tumor with lectin-conjugated rare-earth doped fluoride nanocrystals
title_short Visualization of melanoma tumor with lectin-conjugated rare-earth doped fluoride nanocrystals
title_sort visualization of melanoma tumor with lectin-conjugated rare-earth doped fluoride nanocrystals
topic Central and Eastern European Biomedical Bridges
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4049210/
https://www.ncbi.nlm.nih.gov/pubmed/24891277
http://dx.doi.org/10.3325/cmj.2014.55.186
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