Automated PGP9.5 immunofluorescence staining: a valuable tool in the assessment of small fiber neuropathy?

BACKGROUND: In this study we explored the possibility of automating the PGP9.5 immunofluorescence staining assay for the diagnosis of small fiber neuropathy using skin punch biopsies. The laboratory developed test (LDT) was subjected to a validation strategy as required by good laboratory practice g...

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Autores principales: Van Acker, Nathalie, Ragé, Michael, Sluydts, Ellen, Knaapen, Michiel W. M., De Bie, Martine, Timmers, Maarten, Fransen, Erik, Duymelinck, Carla, De Schepper, Stefanie, Anand, Praveen, Meert, Theo, Plaghki, Léon, Cras, Patrick
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioMed Central 2016
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4878004/
https://www.ncbi.nlm.nih.gov/pubmed/27215701
http://dx.doi.org/10.1186/s13104-016-2085-4
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author Van Acker, Nathalie
Ragé, Michael
Sluydts, Ellen
Knaapen, Michiel W. M.
De Bie, Martine
Timmers, Maarten
Fransen, Erik
Duymelinck, Carla
De Schepper, Stefanie
Anand, Praveen
Meert, Theo
Plaghki, Léon
Cras, Patrick
author_facet Van Acker, Nathalie
Ragé, Michael
Sluydts, Ellen
Knaapen, Michiel W. M.
De Bie, Martine
Timmers, Maarten
Fransen, Erik
Duymelinck, Carla
De Schepper, Stefanie
Anand, Praveen
Meert, Theo
Plaghki, Léon
Cras, Patrick
author_sort Van Acker, Nathalie
collection PubMed
description BACKGROUND: In this study we explored the possibility of automating the PGP9.5 immunofluorescence staining assay for the diagnosis of small fiber neuropathy using skin punch biopsies. The laboratory developed test (LDT) was subjected to a validation strategy as required by good laboratory practice guidelines and compared to the well-established gold standard method approved by the European Federation of Neurological Societies (EFNS). To facilitate automation, the use of thinner sections. (16 µm) was evaluated. Biopsies from previously published studies were used. The aim was to evaluate the diagnostic performance of the LDT compared to the gold standard. We focused on technical aspects to reach high-quality standardization of the PGP9.5 assay and finally evaluate its potential for use in large scale batch testing. RESULTS: We first studied linear nerve fiber densities in skin of healthy volunteers to establish reference ranges, and compared our LDT using the modifications to the EFNS counting rule to the gold standard in visualizing and quantifying the epidermal nerve fiber network. As the LDT requires the use of 16 µm tissue sections, a higher incidence of intra-epidermal nerve fiber fragments and a lower incidence of secondary branches were detected. Nevertheless, the LDT showed excellent concordance with the gold standard method. Next, the diagnostic performance and yield of the LDT were explored and challenged to the gold standard using skin punch biopsies of capsaicin treated subjects, and patients with diabetic polyneuropathy. The LDT reached good agreement with the gold standard in identifying small fiber neuropathy. The reduction of section thickness from 50 to 16 µm resulted in a significantly lower visualization of the three-dimensional epidermal nerve fiber network, as expected. However, the diagnostic performance of the LDT was adequate as characterized by a sensitivity and specificity of 80 and 64 %, respectively. CONCLUSIONS: This study, designed as a proof of principle, indicated that the LDT is an accurate, robust and automated assay, which adequately and reliably identifies patients presenting with small fiber neuropathy, and therefore has potential for use in large scale clinical studies.
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spelling pubmed-48780042016-05-25 Automated PGP9.5 immunofluorescence staining: a valuable tool in the assessment of small fiber neuropathy? Van Acker, Nathalie Ragé, Michael Sluydts, Ellen Knaapen, Michiel W. M. De Bie, Martine Timmers, Maarten Fransen, Erik Duymelinck, Carla De Schepper, Stefanie Anand, Praveen Meert, Theo Plaghki, Léon Cras, Patrick BMC Res Notes Research Article BACKGROUND: In this study we explored the possibility of automating the PGP9.5 immunofluorescence staining assay for the diagnosis of small fiber neuropathy using skin punch biopsies. The laboratory developed test (LDT) was subjected to a validation strategy as required by good laboratory practice guidelines and compared to the well-established gold standard method approved by the European Federation of Neurological Societies (EFNS). To facilitate automation, the use of thinner sections. (16 µm) was evaluated. Biopsies from previously published studies were used. The aim was to evaluate the diagnostic performance of the LDT compared to the gold standard. We focused on technical aspects to reach high-quality standardization of the PGP9.5 assay and finally evaluate its potential for use in large scale batch testing. RESULTS: We first studied linear nerve fiber densities in skin of healthy volunteers to establish reference ranges, and compared our LDT using the modifications to the EFNS counting rule to the gold standard in visualizing and quantifying the epidermal nerve fiber network. As the LDT requires the use of 16 µm tissue sections, a higher incidence of intra-epidermal nerve fiber fragments and a lower incidence of secondary branches were detected. Nevertheless, the LDT showed excellent concordance with the gold standard method. Next, the diagnostic performance and yield of the LDT were explored and challenged to the gold standard using skin punch biopsies of capsaicin treated subjects, and patients with diabetic polyneuropathy. The LDT reached good agreement with the gold standard in identifying small fiber neuropathy. The reduction of section thickness from 50 to 16 µm resulted in a significantly lower visualization of the three-dimensional epidermal nerve fiber network, as expected. However, the diagnostic performance of the LDT was adequate as characterized by a sensitivity and specificity of 80 and 64 %, respectively. CONCLUSIONS: This study, designed as a proof of principle, indicated that the LDT is an accurate, robust and automated assay, which adequately and reliably identifies patients presenting with small fiber neuropathy, and therefore has potential for use in large scale clinical studies. BioMed Central 2016-05-23 /pmc/articles/PMC4878004/ /pubmed/27215701 http://dx.doi.org/10.1186/s13104-016-2085-4 Text en © The Author(s). 2016 Open AccessThis article is distributed under the terms of the Creative Commons Attribution 4.0 International License (http://creativecommons.org/licenses/by/4.0/), which permits unrestricted use, distribution, and reproduction in any medium, provided you give appropriate credit to the original author(s) and the source, provide a link to the Creative Commons license, and indicate if changes were made. The Creative Commons Public Domain Dedication waiver (http://creativecommons.org/publicdomain/zero/1.0/) applies to the data made available in this article, unless otherwise stated.
spellingShingle Research Article
Van Acker, Nathalie
Ragé, Michael
Sluydts, Ellen
Knaapen, Michiel W. M.
De Bie, Martine
Timmers, Maarten
Fransen, Erik
Duymelinck, Carla
De Schepper, Stefanie
Anand, Praveen
Meert, Theo
Plaghki, Léon
Cras, Patrick
Automated PGP9.5 immunofluorescence staining: a valuable tool in the assessment of small fiber neuropathy?
title Automated PGP9.5 immunofluorescence staining: a valuable tool in the assessment of small fiber neuropathy?
title_full Automated PGP9.5 immunofluorescence staining: a valuable tool in the assessment of small fiber neuropathy?
title_fullStr Automated PGP9.5 immunofluorescence staining: a valuable tool in the assessment of small fiber neuropathy?
title_full_unstemmed Automated PGP9.5 immunofluorescence staining: a valuable tool in the assessment of small fiber neuropathy?
title_short Automated PGP9.5 immunofluorescence staining: a valuable tool in the assessment of small fiber neuropathy?
title_sort automated pgp9.5 immunofluorescence staining: a valuable tool in the assessment of small fiber neuropathy?
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4878004/
https://www.ncbi.nlm.nih.gov/pubmed/27215701
http://dx.doi.org/10.1186/s13104-016-2085-4
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