Carnosine quenches the reactive carbonyl acrolein in the central nervous system and attenuates autoimmune neuroinflammation

Jan Spaas; Wouter M. A. Franssen; Charly Keytsman; Laura Blancquaert; Tim Vanmierlo; Jeroen Bogie; Bieke Broux; Niels Hellings; Jack van Horssen; Dheeraj Kumar Posa; David Hoetker; Shahid P. Baba; Wim Derave; Bert O. Eijnde

doi:https://doi.org/10.1186/s12974-021-02306-9

Carnosine quenches the reactive carbonyl acrolein in the central nervous system and attenuates autoimmune neuroinflammation

Jan Spaas, Wouter M. A. Franssen, Charly Keytsman, Laura Blancquaert, Tim Vanmierlo, Jeroen Bogie, Bieke Broux, Niels Hellings, Jack van Horssen, Dheeraj Kumar Posa, David Hoetker, Shahid P. Baba, Wim Derave, Bert O. Eijnde

Research output: Contribution to journal › Article › Academic › peer-review

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Abstract

Background: Multiple sclerosis (MS) is a chronic autoimmune disease driven by sustained inflammation in the central nervous system. One of the pathological hallmarks of MS is extensive free radical production. However, the subsequent generation, potential pathological role, and detoxification of different lipid peroxidation-derived reactive carbonyl species during neuroinflammation are unclear, as are the therapeutic benefits of carbonyl quenchers. Here, we investigated the reactive carbonyl acrolein and (the therapeutic effect of) acrolein quenching by carnosine during neuroinflammation. Methods: The abundance and localization of acrolein was investigated in inflammatory lesions of MS patients and experimental autoimmune encephalomyelitis (EAE) mice. In addition, we analysed carnosine levels and acrolein quenching by endogenous and exogenous carnosine in EAE. Finally, the therapeutic effect of exogenous carnosine was assessed in vivo (EAE) and in vitro (primary mouse microglia, macrophages, astrocytes). Results: Acrolein was substantially increased in inflammatory lesions of MS patients and EAE mice. Levels of the dipeptide carnosine (β-alanyl-l-histidine), an endogenous carbonyl quencher particularly reactive towards acrolein, and the carnosine-acrolein adduct (carnosine-propanal) were ~ twofold lower within EAE spinal cord tissue. Oral carnosine treatment augmented spinal cord carnosine levels (up to > tenfold), increased carnosine-acrolein quenching, reduced acrolein-protein adduct formation, suppressed inflammatory activity, and alleviated clinical disease severity in EAE. In vivo and in vitro studies indicate that pro-inflammatory microglia/macrophages generate acrolein, which can be efficiently quenched by increasing carnosine availability, resulting in suppressed inflammatory activity. Other properties of carnosine (antioxidant, nitric oxide scavenging) may also contribute to the therapeutic effects. Conclusions: Our results identify carbonyl (particularly acrolein) quenching by carnosine as a therapeutic strategy to counter inflammation and macromolecular damage in MS.

Original language	English
Article number	255
Journal	Journal of neuroinflammation
Volume	18
Issue number	1
DOIs	https://doi.org/10.1186/s12974-021-02306-9
Publication status	Published - 1 Dec 2021

Keywords

Acrolein
Carnosine
Multiple sclerosis
Neuroinflammation
Oxidative stress
Reactive carbonyl

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https://doi.org/10.1186/s12974-021-02306-9

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Spaas, J., Franssen, W. M. A., Keytsman, C., Blancquaert, L., Vanmierlo, T., Bogie, J., Broux, B., Hellings, N., van Horssen, J., Posa, D. K., Hoetker, D., Baba, S. P., Derave, W., & Eijnde, B. O. (2021). Carnosine quenches the reactive carbonyl acrolein in the central nervous system and attenuates autoimmune neuroinflammation. Journal of neuroinflammation, 18(1), Article 255. https://doi.org/10.1186/s12974-021-02306-9

@article{b4166508680c4a0b8e5fa2f27e4ccb41,

title = "Carnosine quenches the reactive carbonyl acrolein in the central nervous system and attenuates autoimmune neuroinflammation",

abstract = "Background: Multiple sclerosis (MS) is a chronic autoimmune disease driven by sustained inflammation in the central nervous system. One of the pathological hallmarks of MS is extensive free radical production. However, the subsequent generation, potential pathological role, and detoxification of different lipid peroxidation-derived reactive carbonyl species during neuroinflammation are unclear, as are the therapeutic benefits of carbonyl quenchers. Here, we investigated the reactive carbonyl acrolein and (the therapeutic effect of) acrolein quenching by carnosine during neuroinflammation. Methods: The abundance and localization of acrolein was investigated in inflammatory lesions of MS patients and experimental autoimmune encephalomyelitis (EAE) mice. In addition, we analysed carnosine levels and acrolein quenching by endogenous and exogenous carnosine in EAE. Finally, the therapeutic effect of exogenous carnosine was assessed in vivo (EAE) and in vitro (primary mouse microglia, macrophages, astrocytes). Results: Acrolein was substantially increased in inflammatory lesions of MS patients and EAE mice. Levels of the dipeptide carnosine (β-alanyl-l-histidine), an endogenous carbonyl quencher particularly reactive towards acrolein, and the carnosine-acrolein adduct (carnosine-propanal) were ~ twofold lower within EAE spinal cord tissue. Oral carnosine treatment augmented spinal cord carnosine levels (up to > tenfold), increased carnosine-acrolein quenching, reduced acrolein-protein adduct formation, suppressed inflammatory activity, and alleviated clinical disease severity in EAE. In vivo and in vitro studies indicate that pro-inflammatory microglia/macrophages generate acrolein, which can be efficiently quenched by increasing carnosine availability, resulting in suppressed inflammatory activity. Other properties of carnosine (antioxidant, nitric oxide scavenging) may also contribute to the therapeutic effects. Conclusions: Our results identify carbonyl (particularly acrolein) quenching by carnosine as a therapeutic strategy to counter inflammation and macromolecular damage in MS.",

keywords = "Acrolein, Carnosine, Multiple sclerosis, Neuroinflammation, Oxidative stress, Reactive carbonyl",

author = "Jan Spaas and Franssen, {Wouter M. A.} and Charly Keytsman and Laura Blancquaert and Tim Vanmierlo and Jeroen Bogie and Bieke Broux and Niels Hellings and {van Horssen}, Jack and Posa, {Dheeraj Kumar} and David Hoetker and Baba, {Shahid P.} and Wim Derave and Eijnde, {Bert O.}",

note = "Funding Information: This research was funded by the Special Research Fund (BOF, Hasselt University, Belgium) and Research Foundation Flanders (FWO Vlaanderen, Belgium; 1138520N). Funding Information: We sincerely thank prof. dr. Aruni Bhatnagar from the University of Louisville, Diabetes and Obesity Center for his hospitality and useful advice. We are grateful to Flamma (Flamma Group, Chignolo d?Isola, Bergamo, Italy) for providing L-carnosine and L-anserine, and K. Wauterickx (Hasselt University) for assistance with immunohistochemistry on human brain samples. Figure 7 a was created in BioRender. Publisher Copyright: {\textcopyright} 2021, The Author(s).",

year = "2021",

month = dec,

day = "1",

doi = "https://doi.org/10.1186/s12974-021-02306-9",

language = "English",

volume = "18",

journal = "Journal of neuroinflammation",

issn = "1742-2094",

publisher = "BioMed Central",

number = "1",

}

Spaas, J, Franssen, WMA, Keytsman, C, Blancquaert, L, Vanmierlo, T, Bogie, J, Broux, B, Hellings, N, van Horssen, J, Posa, DK, Hoetker, D, Baba, SP, Derave, W & Eijnde, BO 2021, 'Carnosine quenches the reactive carbonyl acrolein in the central nervous system and attenuates autoimmune neuroinflammation', Journal of neuroinflammation, vol. 18, no. 1, 255. https://doi.org/10.1186/s12974-021-02306-9

TY - JOUR

T1 - Carnosine quenches the reactive carbonyl acrolein in the central nervous system and attenuates autoimmune neuroinflammation

AU - Spaas, Jan

AU - Franssen, Wouter M. A.

AU - Keytsman, Charly

AU - Blancquaert, Laura

AU - Vanmierlo, Tim

AU - Bogie, Jeroen

AU - Broux, Bieke

AU - Hellings, Niels

AU - van Horssen, Jack

AU - Posa, Dheeraj Kumar

AU - Hoetker, David

AU - Baba, Shahid P.

AU - Derave, Wim

AU - Eijnde, Bert O.

N1 - Funding Information: This research was funded by the Special Research Fund (BOF, Hasselt University, Belgium) and Research Foundation Flanders (FWO Vlaanderen, Belgium; 1138520N). Funding Information: We sincerely thank prof. dr. Aruni Bhatnagar from the University of Louisville, Diabetes and Obesity Center for his hospitality and useful advice. We are grateful to Flamma (Flamma Group, Chignolo d?Isola, Bergamo, Italy) for providing L-carnosine and L-anserine, and K. Wauterickx (Hasselt University) for assistance with immunohistochemistry on human brain samples. Figure 7 a was created in BioRender. Publisher Copyright: © 2021, The Author(s).

PY - 2021/12/1

Y1 - 2021/12/1

N2 - Background: Multiple sclerosis (MS) is a chronic autoimmune disease driven by sustained inflammation in the central nervous system. One of the pathological hallmarks of MS is extensive free radical production. However, the subsequent generation, potential pathological role, and detoxification of different lipid peroxidation-derived reactive carbonyl species during neuroinflammation are unclear, as are the therapeutic benefits of carbonyl quenchers. Here, we investigated the reactive carbonyl acrolein and (the therapeutic effect of) acrolein quenching by carnosine during neuroinflammation. Methods: The abundance and localization of acrolein was investigated in inflammatory lesions of MS patients and experimental autoimmune encephalomyelitis (EAE) mice. In addition, we analysed carnosine levels and acrolein quenching by endogenous and exogenous carnosine in EAE. Finally, the therapeutic effect of exogenous carnosine was assessed in vivo (EAE) and in vitro (primary mouse microglia, macrophages, astrocytes). Results: Acrolein was substantially increased in inflammatory lesions of MS patients and EAE mice. Levels of the dipeptide carnosine (β-alanyl-l-histidine), an endogenous carbonyl quencher particularly reactive towards acrolein, and the carnosine-acrolein adduct (carnosine-propanal) were ~ twofold lower within EAE spinal cord tissue. Oral carnosine treatment augmented spinal cord carnosine levels (up to > tenfold), increased carnosine-acrolein quenching, reduced acrolein-protein adduct formation, suppressed inflammatory activity, and alleviated clinical disease severity in EAE. In vivo and in vitro studies indicate that pro-inflammatory microglia/macrophages generate acrolein, which can be efficiently quenched by increasing carnosine availability, resulting in suppressed inflammatory activity. Other properties of carnosine (antioxidant, nitric oxide scavenging) may also contribute to the therapeutic effects. Conclusions: Our results identify carbonyl (particularly acrolein) quenching by carnosine as a therapeutic strategy to counter inflammation and macromolecular damage in MS.

AB - Background: Multiple sclerosis (MS) is a chronic autoimmune disease driven by sustained inflammation in the central nervous system. One of the pathological hallmarks of MS is extensive free radical production. However, the subsequent generation, potential pathological role, and detoxification of different lipid peroxidation-derived reactive carbonyl species during neuroinflammation are unclear, as are the therapeutic benefits of carbonyl quenchers. Here, we investigated the reactive carbonyl acrolein and (the therapeutic effect of) acrolein quenching by carnosine during neuroinflammation. Methods: The abundance and localization of acrolein was investigated in inflammatory lesions of MS patients and experimental autoimmune encephalomyelitis (EAE) mice. In addition, we analysed carnosine levels and acrolein quenching by endogenous and exogenous carnosine in EAE. Finally, the therapeutic effect of exogenous carnosine was assessed in vivo (EAE) and in vitro (primary mouse microglia, macrophages, astrocytes). Results: Acrolein was substantially increased in inflammatory lesions of MS patients and EAE mice. Levels of the dipeptide carnosine (β-alanyl-l-histidine), an endogenous carbonyl quencher particularly reactive towards acrolein, and the carnosine-acrolein adduct (carnosine-propanal) were ~ twofold lower within EAE spinal cord tissue. Oral carnosine treatment augmented spinal cord carnosine levels (up to > tenfold), increased carnosine-acrolein quenching, reduced acrolein-protein adduct formation, suppressed inflammatory activity, and alleviated clinical disease severity in EAE. In vivo and in vitro studies indicate that pro-inflammatory microglia/macrophages generate acrolein, which can be efficiently quenched by increasing carnosine availability, resulting in suppressed inflammatory activity. Other properties of carnosine (antioxidant, nitric oxide scavenging) may also contribute to the therapeutic effects. Conclusions: Our results identify carbonyl (particularly acrolein) quenching by carnosine as a therapeutic strategy to counter inflammation and macromolecular damage in MS.

KW - Acrolein

KW - Carnosine

KW - Multiple sclerosis

KW - Neuroinflammation

KW - Oxidative stress

KW - Reactive carbonyl

UR - http://www.scopus.com/inward/record.url?scp=85118759302&partnerID=8YFLogxK

U2 - https://doi.org/10.1186/s12974-021-02306-9

DO - https://doi.org/10.1186/s12974-021-02306-9

M3 - Article

C2 - 34740381

SN - 1742-2094

VL - 18

JO - Journal of neuroinflammation

JF - Journal of neuroinflammation

IS - 1

M1 - 255

ER -

Carnosine quenches the reactive carbonyl acrolein in the central nervous system and attenuates autoimmune neuroinflammation

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Keywords

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