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DRH1 – a novel blood-based HPV tumour marker

BACKGROUND: To date, no studies have successfully shown that a highly specific, blood-based tumour marker to detect clinically relevant HPV-induced disease could be used for screening, monitoring therapy response or early detection of recurrence. This study aims to assess the clinical performance of...

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Autores principales: Weiland, Thomas, Eckert, Alexander, Tomazic, Peter Valentin, Wolf, Axel, Pondorfer, Prisca, Vasicek, Sarah, Graupp, Matthias, Holzmeister, Clemens, Moser, Ulrich, Andrianakis, Alexandros, Kangler, Georg, Kiss, Peter, Brcic, Luka, Kappler, Matthias, Wickenhauser, Claudia, Haak, Anja, Krüger, Maximilian, Al-Nawas, Bilal, Blatt, Sebastian, Brockmeyer, Norbert, Skaletz-Rorowski, Adriane, Potthoff, Anja, French, Lars E., Charnowski, Sara, Reinholz, Markus, Kaufmann, Andreas M., Thies, Sarah, Lambrecht, Hans-Georg, Seliger, Barbara, Wild, Dominik C., Thurnher, Dietmar
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2020
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7300133/
https://www.ncbi.nlm.nih.gov/pubmed/32535546
http://dx.doi.org/10.1016/j.ebiom.2020.102804
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author Weiland, Thomas
Eckert, Alexander
Tomazic, Peter Valentin
Wolf, Axel
Pondorfer, Prisca
Vasicek, Sarah
Graupp, Matthias
Holzmeister, Clemens
Moser, Ulrich
Andrianakis, Alexandros
Kangler, Georg
Kiss, Peter
Brcic, Luka
Kappler, Matthias
Wickenhauser, Claudia
Haak, Anja
Krüger, Maximilian
Al-Nawas, Bilal
Blatt, Sebastian
Brockmeyer, Norbert
Skaletz-Rorowski, Adriane
Potthoff, Anja
French, Lars E.
Charnowski, Sara
Reinholz, Markus
Kaufmann, Andreas M.
Thies, Sarah
Lambrecht, Hans-Georg
Seliger, Barbara
Wild, Dominik C.
Thurnher, Dietmar
author_facet Weiland, Thomas
Eckert, Alexander
Tomazic, Peter Valentin
Wolf, Axel
Pondorfer, Prisca
Vasicek, Sarah
Graupp, Matthias
Holzmeister, Clemens
Moser, Ulrich
Andrianakis, Alexandros
Kangler, Georg
Kiss, Peter
Brcic, Luka
Kappler, Matthias
Wickenhauser, Claudia
Haak, Anja
Krüger, Maximilian
Al-Nawas, Bilal
Blatt, Sebastian
Brockmeyer, Norbert
Skaletz-Rorowski, Adriane
Potthoff, Anja
French, Lars E.
Charnowski, Sara
Reinholz, Markus
Kaufmann, Andreas M.
Thies, Sarah
Lambrecht, Hans-Georg
Seliger, Barbara
Wild, Dominik C.
Thurnher, Dietmar
author_sort Weiland, Thomas
collection PubMed
description BACKGROUND: To date, no studies have successfully shown that a highly specific, blood-based tumour marker to detect clinically relevant HPV-induced disease could be used for screening, monitoring therapy response or early detection of recurrence. This study aims to assess the clinical performance of a newly developed HPV16-L1 DRH1 epitope-specific serological assay. METHODS: In a multi-centre study sera of 1486 patients (301 Head and Neck Squamous Cell Carcinoma (HNSCC) patients, 12 HIV+ anal cancer patients, 80 HIV-positive patients, 29 Gardasil-9-vaccinees, 1064 healthy controls) were tested for human HPV16-L1 DRH1 antibodies. Analytical specificity was determined using WHO reference-sera for HPV16/18 and 29 pre- and post-immune sera of Gardasil-9-vaccinees. Tumour-tissue was immunochemically stained for HPV-L1-capsidprotein-expression. FINDINGS: The DRH1-competitive-serological-assay showed a sensitivity of 95% (95% CI, 77(.)2–99(.)9%) for HPV16-driven HNSCC, and 90% (95% CI, 55(.)5–99(.)7%) for HPV16-induced anal cancer in HIV-positives. Overall diagnostic specificity was 99(.)46% for men and 99(.)29% for women ≥ 30 years. After vaccination, antibody level increased from average 364 ng/ml to 37,500 ng/ml. During post-therapy-monitoring, HNSCC patients showing an antibody decrease in the range of 30–100% lived disease free over a period of up to 26 months. The increase of antibodies from 2750 to 12,000 ng/ml mirrored recurrent disease. We can also show that the L1-capsidprotein is expressed in HPV16-DNA positive tumour-tissue. INTERPRETATION: HPV16-L1 DRH1 epitope-specific antibodies are linked to HPV16-induced malignant disease. As post-treatment biomarker, the assay allows independent post-therapy monitoring as well as early diagnosis of tumour recurrence. An AUC of 0(.)96 indicates high sensitivity and specificity for early detection of HPV16-induced disease. FUNDING: The manufacturer provided assays free of charge.
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spelling pubmed-73001332020-06-22 DRH1 – a novel blood-based HPV tumour marker Weiland, Thomas Eckert, Alexander Tomazic, Peter Valentin Wolf, Axel Pondorfer, Prisca Vasicek, Sarah Graupp, Matthias Holzmeister, Clemens Moser, Ulrich Andrianakis, Alexandros Kangler, Georg Kiss, Peter Brcic, Luka Kappler, Matthias Wickenhauser, Claudia Haak, Anja Krüger, Maximilian Al-Nawas, Bilal Blatt, Sebastian Brockmeyer, Norbert Skaletz-Rorowski, Adriane Potthoff, Anja French, Lars E. Charnowski, Sara Reinholz, Markus Kaufmann, Andreas M. Thies, Sarah Lambrecht, Hans-Georg Seliger, Barbara Wild, Dominik C. Thurnher, Dietmar EBioMedicine Research paper BACKGROUND: To date, no studies have successfully shown that a highly specific, blood-based tumour marker to detect clinically relevant HPV-induced disease could be used for screening, monitoring therapy response or early detection of recurrence. This study aims to assess the clinical performance of a newly developed HPV16-L1 DRH1 epitope-specific serological assay. METHODS: In a multi-centre study sera of 1486 patients (301 Head and Neck Squamous Cell Carcinoma (HNSCC) patients, 12 HIV+ anal cancer patients, 80 HIV-positive patients, 29 Gardasil-9-vaccinees, 1064 healthy controls) were tested for human HPV16-L1 DRH1 antibodies. Analytical specificity was determined using WHO reference-sera for HPV16/18 and 29 pre- and post-immune sera of Gardasil-9-vaccinees. Tumour-tissue was immunochemically stained for HPV-L1-capsidprotein-expression. FINDINGS: The DRH1-competitive-serological-assay showed a sensitivity of 95% (95% CI, 77(.)2–99(.)9%) for HPV16-driven HNSCC, and 90% (95% CI, 55(.)5–99(.)7%) for HPV16-induced anal cancer in HIV-positives. Overall diagnostic specificity was 99(.)46% for men and 99(.)29% for women ≥ 30 years. After vaccination, antibody level increased from average 364 ng/ml to 37,500 ng/ml. During post-therapy-monitoring, HNSCC patients showing an antibody decrease in the range of 30–100% lived disease free over a period of up to 26 months. The increase of antibodies from 2750 to 12,000 ng/ml mirrored recurrent disease. We can also show that the L1-capsidprotein is expressed in HPV16-DNA positive tumour-tissue. INTERPRETATION: HPV16-L1 DRH1 epitope-specific antibodies are linked to HPV16-induced malignant disease. As post-treatment biomarker, the assay allows independent post-therapy monitoring as well as early diagnosis of tumour recurrence. An AUC of 0(.)96 indicates high sensitivity and specificity for early detection of HPV16-induced disease. FUNDING: The manufacturer provided assays free of charge. Elsevier 2020-06-11 /pmc/articles/PMC7300133/ /pubmed/32535546 http://dx.doi.org/10.1016/j.ebiom.2020.102804 Text en © 2020 The Author(s) http://creativecommons.org/licenses/by-nc-nd/4.0/ This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Research paper
Weiland, Thomas
Eckert, Alexander
Tomazic, Peter Valentin
Wolf, Axel
Pondorfer, Prisca
Vasicek, Sarah
Graupp, Matthias
Holzmeister, Clemens
Moser, Ulrich
Andrianakis, Alexandros
Kangler, Georg
Kiss, Peter
Brcic, Luka
Kappler, Matthias
Wickenhauser, Claudia
Haak, Anja
Krüger, Maximilian
Al-Nawas, Bilal
Blatt, Sebastian
Brockmeyer, Norbert
Skaletz-Rorowski, Adriane
Potthoff, Anja
French, Lars E.
Charnowski, Sara
Reinholz, Markus
Kaufmann, Andreas M.
Thies, Sarah
Lambrecht, Hans-Georg
Seliger, Barbara
Wild, Dominik C.
Thurnher, Dietmar
DRH1 – a novel blood-based HPV tumour marker
title DRH1 – a novel blood-based HPV tumour marker
title_full DRH1 – a novel blood-based HPV tumour marker
title_fullStr DRH1 – a novel blood-based HPV tumour marker
title_full_unstemmed DRH1 – a novel blood-based HPV tumour marker
title_short DRH1 – a novel blood-based HPV tumour marker
title_sort drh1 – a novel blood-based hpv tumour marker
topic Research paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7300133/
https://www.ncbi.nlm.nih.gov/pubmed/32535546
http://dx.doi.org/10.1016/j.ebiom.2020.102804
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