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Electroporation-based proteome sampling ex vivo enables the detection of brain melanoma protein signatures in a location proximate to visible tumor margins

A major concern in tissue biopsies with a needle is missing the most lethal clone of a tumor, leading to a false negative result. This concern is well justified, since needle-based biopsies gather tissue information limited to needle size. In this work, we show that molecular harvesting with electro...

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Autores principales: Genish, Ilai, Gabay, Batel, Ruban, Angela, Goldshmit, Yona, Singh, Amrita, Wise, Julia, Levkov, Klimentiy, Shalom, Avshalom, Vitkin, Edward, Yakhini, Zohar, Golberg, Alexander
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9119512/
https://www.ncbi.nlm.nih.gov/pubmed/35588133
http://dx.doi.org/10.1371/journal.pone.0265866
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author Genish, Ilai
Gabay, Batel
Ruban, Angela
Goldshmit, Yona
Singh, Amrita
Wise, Julia
Levkov, Klimentiy
Shalom, Avshalom
Vitkin, Edward
Yakhini, Zohar
Golberg, Alexander
author_facet Genish, Ilai
Gabay, Batel
Ruban, Angela
Goldshmit, Yona
Singh, Amrita
Wise, Julia
Levkov, Klimentiy
Shalom, Avshalom
Vitkin, Edward
Yakhini, Zohar
Golberg, Alexander
author_sort Genish, Ilai
collection PubMed
description A major concern in tissue biopsies with a needle is missing the most lethal clone of a tumor, leading to a false negative result. This concern is well justified, since needle-based biopsies gather tissue information limited to needle size. In this work, we show that molecular harvesting with electroporation, e-biopsy, could increase the sampled tissue volume in comparison to tissue sampling by a needle alone. Suggested by numerical models of electric fields distribution, the increased sampled volume is achieved by electroporation-driven permeabilization of cellular membranes in the tissue around the sampling needle. We show that proteomic profiles, sampled by e-biopsy from the brain tissue, ex vivo, at 0.5mm distance outside the visible margins of mice brain melanoma metastasis, have protein patterns similar to melanoma tumor center and different from the healthy brain tissue. In addition, we show that e-biopsy probed proteome signature differentiates between melanoma tumor center and healthy brain in mice. This study suggests that e-biopsy could provide a novel tool for a minimally invasive sampling of molecules in tissue in larger volumes than achieved with traditional needle biopsies.
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spelling pubmed-91195122022-05-20 Electroporation-based proteome sampling ex vivo enables the detection of brain melanoma protein signatures in a location proximate to visible tumor margins Genish, Ilai Gabay, Batel Ruban, Angela Goldshmit, Yona Singh, Amrita Wise, Julia Levkov, Klimentiy Shalom, Avshalom Vitkin, Edward Yakhini, Zohar Golberg, Alexander PLoS One Research Article A major concern in tissue biopsies with a needle is missing the most lethal clone of a tumor, leading to a false negative result. This concern is well justified, since needle-based biopsies gather tissue information limited to needle size. In this work, we show that molecular harvesting with electroporation, e-biopsy, could increase the sampled tissue volume in comparison to tissue sampling by a needle alone. Suggested by numerical models of electric fields distribution, the increased sampled volume is achieved by electroporation-driven permeabilization of cellular membranes in the tissue around the sampling needle. We show that proteomic profiles, sampled by e-biopsy from the brain tissue, ex vivo, at 0.5mm distance outside the visible margins of mice brain melanoma metastasis, have protein patterns similar to melanoma tumor center and different from the healthy brain tissue. In addition, we show that e-biopsy probed proteome signature differentiates between melanoma tumor center and healthy brain in mice. This study suggests that e-biopsy could provide a novel tool for a minimally invasive sampling of molecules in tissue in larger volumes than achieved with traditional needle biopsies. Public Library of Science 2022-05-19 /pmc/articles/PMC9119512/ /pubmed/35588133 http://dx.doi.org/10.1371/journal.pone.0265866 Text en © 2022 Genish et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Article
Genish, Ilai
Gabay, Batel
Ruban, Angela
Goldshmit, Yona
Singh, Amrita
Wise, Julia
Levkov, Klimentiy
Shalom, Avshalom
Vitkin, Edward
Yakhini, Zohar
Golberg, Alexander
Electroporation-based proteome sampling ex vivo enables the detection of brain melanoma protein signatures in a location proximate to visible tumor margins
title Electroporation-based proteome sampling ex vivo enables the detection of brain melanoma protein signatures in a location proximate to visible tumor margins
title_full Electroporation-based proteome sampling ex vivo enables the detection of brain melanoma protein signatures in a location proximate to visible tumor margins
title_fullStr Electroporation-based proteome sampling ex vivo enables the detection of brain melanoma protein signatures in a location proximate to visible tumor margins
title_full_unstemmed Electroporation-based proteome sampling ex vivo enables the detection of brain melanoma protein signatures in a location proximate to visible tumor margins
title_short Electroporation-based proteome sampling ex vivo enables the detection of brain melanoma protein signatures in a location proximate to visible tumor margins
title_sort electroporation-based proteome sampling ex vivo enables the detection of brain melanoma protein signatures in a location proximate to visible tumor margins
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9119512/
https://www.ncbi.nlm.nih.gov/pubmed/35588133
http://dx.doi.org/10.1371/journal.pone.0265866
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