Volatile Phases Derived from Serum, DC, or MLC Culture Supernatants to Deduce a VOC-Based Diagnostic Profiling Strategy for Leukemic Diseases

Volatile organic compounds (VOCs) reflect the metabolism in healthy and pathological conditions, and can be collected easily in a noninvasive manner. They are directly measured using electronical nose (eNose), and may qualify as a systemic tool to monitor biomarkers related to disease. Myeloid leuke...

Descripción completa

Detalles Bibliográficos
Autores principales: Baudrexler, Tobias, Boeselt, Tobias, Li, Lin, Bohlscheid, Sophia, Boas, Ursel, Schmid, Christoph, Rank, Andreas, Schmohl, Jörg, Koczulla, Rembert, Schmetzer, Helga Maria
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2023
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10296614/
https://www.ncbi.nlm.nih.gov/pubmed/37371569
http://dx.doi.org/10.3390/biom13060989
_version_ 1785063691741298688
author Baudrexler, Tobias
Boeselt, Tobias
Li, Lin
Bohlscheid, Sophia
Boas, Ursel
Schmid, Christoph
Rank, Andreas
Schmohl, Jörg
Koczulla, Rembert
Schmetzer, Helga Maria
author_facet Baudrexler, Tobias
Boeselt, Tobias
Li, Lin
Bohlscheid, Sophia
Boas, Ursel
Schmid, Christoph
Rank, Andreas
Schmohl, Jörg
Koczulla, Rembert
Schmetzer, Helga Maria
author_sort Baudrexler, Tobias
collection PubMed
description Volatile organic compounds (VOCs) reflect the metabolism in healthy and pathological conditions, and can be collected easily in a noninvasive manner. They are directly measured using electronical nose (eNose), and may qualify as a systemic tool to monitor biomarkers related to disease. Myeloid leukemic blasts can be transformed into leukemia-derived dendritic cells (DC(leu)) able to improve (anti-leukemic) immune responses. To profile immunological changes in healthy and acute myeloid leukemic (AML) patients’ ex vivo cell cultures, we correlated the cell biological data with the profiles of cell culture supernatant-derived VOCs. DC/DC(leu) from leukemic or healthy whole blood (WB) were generated without (Control) or with immunomodulatory Kit M (Granulocyte macrophage-colony-stimulating-factor (GM-CSF) + prostaglandin E(1) (PGE(1))) in dendritic cell cultures (DC culture). Kit-pretreated/not pretreated WB was used to stimulate T cell-enriched immunoreactive cells in mixed lymphocyte cultures (MLC culture). Leukemia-specific adaptive and innate immune cells were detected with a degranulation assay (Deg) and an intracellular cytokine assay (InCyt). Anti-leukemic cytotoxicity was explored with a cytotoxicity fluorolysis assay (CTX). VOCs collected from serum or DC- and MLC culture supernatants (with vs. without Kit M pretreatment and before vs. after culture) were measured using eNose. Compared to the Control (without treatment), Kit M-pretreated leukemic and healthy WB gave rise to higher frequencies of mature (leukemia-derived) DC subtypes of activated and (memory) T cells after MLC. Moreover, antigen (leukemia)-specific cells of several lines (innate and adaptive immunity cells) were induced, giving rise to blast-lysing cells. The eNose could significantly distinguish between healthy and leukemic patients’ serum, DC and MLC culture supernatant-derived volatile phases and could significantly separate several supernatant (with vs. without Kit M treatment, cultured vs. uncultured)-derived VOCs within subgroups (healthy DC or leukemic DC, or healthy MLC or leukemic MLC supernatants). Interestingly, the eNose could indicate a Kit M- and culture-associated effect. The eNose may be a prospective option for the deduction of a VOC-based profiling strategy using serum or cell culture supernatants and could be a useful diagnostic tool to recognize or qualify AML disease.
format Online
Article
Text
id pubmed-10296614
institution National Center for Biotechnology Information
language English
publishDate 2023
publisher MDPI
record_format MEDLINE/PubMed
spelling pubmed-102966142023-06-28 Volatile Phases Derived from Serum, DC, or MLC Culture Supernatants to Deduce a VOC-Based Diagnostic Profiling Strategy for Leukemic Diseases Baudrexler, Tobias Boeselt, Tobias Li, Lin Bohlscheid, Sophia Boas, Ursel Schmid, Christoph Rank, Andreas Schmohl, Jörg Koczulla, Rembert Schmetzer, Helga Maria Biomolecules Article Volatile organic compounds (VOCs) reflect the metabolism in healthy and pathological conditions, and can be collected easily in a noninvasive manner. They are directly measured using electronical nose (eNose), and may qualify as a systemic tool to monitor biomarkers related to disease. Myeloid leukemic blasts can be transformed into leukemia-derived dendritic cells (DC(leu)) able to improve (anti-leukemic) immune responses. To profile immunological changes in healthy and acute myeloid leukemic (AML) patients’ ex vivo cell cultures, we correlated the cell biological data with the profiles of cell culture supernatant-derived VOCs. DC/DC(leu) from leukemic or healthy whole blood (WB) were generated without (Control) or with immunomodulatory Kit M (Granulocyte macrophage-colony-stimulating-factor (GM-CSF) + prostaglandin E(1) (PGE(1))) in dendritic cell cultures (DC culture). Kit-pretreated/not pretreated WB was used to stimulate T cell-enriched immunoreactive cells in mixed lymphocyte cultures (MLC culture). Leukemia-specific adaptive and innate immune cells were detected with a degranulation assay (Deg) and an intracellular cytokine assay (InCyt). Anti-leukemic cytotoxicity was explored with a cytotoxicity fluorolysis assay (CTX). VOCs collected from serum or DC- and MLC culture supernatants (with vs. without Kit M pretreatment and before vs. after culture) were measured using eNose. Compared to the Control (without treatment), Kit M-pretreated leukemic and healthy WB gave rise to higher frequencies of mature (leukemia-derived) DC subtypes of activated and (memory) T cells after MLC. Moreover, antigen (leukemia)-specific cells of several lines (innate and adaptive immunity cells) were induced, giving rise to blast-lysing cells. The eNose could significantly distinguish between healthy and leukemic patients’ serum, DC and MLC culture supernatant-derived volatile phases and could significantly separate several supernatant (with vs. without Kit M treatment, cultured vs. uncultured)-derived VOCs within subgroups (healthy DC or leukemic DC, or healthy MLC or leukemic MLC supernatants). Interestingly, the eNose could indicate a Kit M- and culture-associated effect. The eNose may be a prospective option for the deduction of a VOC-based profiling strategy using serum or cell culture supernatants and could be a useful diagnostic tool to recognize or qualify AML disease. MDPI 2023-06-14 /pmc/articles/PMC10296614/ /pubmed/37371569 http://dx.doi.org/10.3390/biom13060989 Text en © 2023 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Baudrexler, Tobias
Boeselt, Tobias
Li, Lin
Bohlscheid, Sophia
Boas, Ursel
Schmid, Christoph
Rank, Andreas
Schmohl, Jörg
Koczulla, Rembert
Schmetzer, Helga Maria
Volatile Phases Derived from Serum, DC, or MLC Culture Supernatants to Deduce a VOC-Based Diagnostic Profiling Strategy for Leukemic Diseases
title Volatile Phases Derived from Serum, DC, or MLC Culture Supernatants to Deduce a VOC-Based Diagnostic Profiling Strategy for Leukemic Diseases
title_full Volatile Phases Derived from Serum, DC, or MLC Culture Supernatants to Deduce a VOC-Based Diagnostic Profiling Strategy for Leukemic Diseases
title_fullStr Volatile Phases Derived from Serum, DC, or MLC Culture Supernatants to Deduce a VOC-Based Diagnostic Profiling Strategy for Leukemic Diseases
title_full_unstemmed Volatile Phases Derived from Serum, DC, or MLC Culture Supernatants to Deduce a VOC-Based Diagnostic Profiling Strategy for Leukemic Diseases
title_short Volatile Phases Derived from Serum, DC, or MLC Culture Supernatants to Deduce a VOC-Based Diagnostic Profiling Strategy for Leukemic Diseases
title_sort volatile phases derived from serum, dc, or mlc culture supernatants to deduce a voc-based diagnostic profiling strategy for leukemic diseases
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10296614/
https://www.ncbi.nlm.nih.gov/pubmed/37371569
http://dx.doi.org/10.3390/biom13060989
work_keys_str_mv AT baudrexlertobias volatilephasesderivedfromserumdcormlcculturesupernatantstodeduceavocbaseddiagnosticprofilingstrategyforleukemicdiseases
AT boeselttobias volatilephasesderivedfromserumdcormlcculturesupernatantstodeduceavocbaseddiagnosticprofilingstrategyforleukemicdiseases
AT lilin volatilephasesderivedfromserumdcormlcculturesupernatantstodeduceavocbaseddiagnosticprofilingstrategyforleukemicdiseases
AT bohlscheidsophia volatilephasesderivedfromserumdcormlcculturesupernatantstodeduceavocbaseddiagnosticprofilingstrategyforleukemicdiseases
AT boasursel volatilephasesderivedfromserumdcormlcculturesupernatantstodeduceavocbaseddiagnosticprofilingstrategyforleukemicdiseases
AT schmidchristoph volatilephasesderivedfromserumdcormlcculturesupernatantstodeduceavocbaseddiagnosticprofilingstrategyforleukemicdiseases
AT rankandreas volatilephasesderivedfromserumdcormlcculturesupernatantstodeduceavocbaseddiagnosticprofilingstrategyforleukemicdiseases
AT schmohljorg volatilephasesderivedfromserumdcormlcculturesupernatantstodeduceavocbaseddiagnosticprofilingstrategyforleukemicdiseases
AT koczullarembert volatilephasesderivedfromserumdcormlcculturesupernatantstodeduceavocbaseddiagnosticprofilingstrategyforleukemicdiseases
AT schmetzerhelgamaria volatilephasesderivedfromserumdcormlcculturesupernatantstodeduceavocbaseddiagnosticprofilingstrategyforleukemicdiseases

Ejemplares similares