Dapsone Suppresses Disease in Preclinical Murine Models of Pemphigoid Diseases

Sripriya Murthy; Paul Schilf; Sabrina Patzelt; Markus Thieme; Mareike Becker; Lasse Kröger; Tabea Bremer; Aleksandra Derenda-Hell; Lea Knebel; Francesca Fagiani; Saleh M. Ibrahim; Enno Schmidt; Detlef Zillikens; Christian D. Sadik

doi:10.1016/j.jid.2021.04.009

Dapsone Suppresses Disease in Preclinical Murine Models of Pemphigoid Diseases

Sripriya Murthy, Paul Schilf, Sabrina Patzelt, Markus Thieme, Mareike Becker, Lasse Kröger, Tabea Bremer, Aleksandra Derenda-Hell, Lea Knebel, Francesca Fagiani, Saleh M. Ibrahim, Enno Schmidt, Detlef Zillikens, Christian D. Sadik^*

^*Korrespondierende/r Autor/-in für diese Arbeit

28 Zitate (Scopus)

Abstract

Epidermolysis bullosa acquisita and mucous membrane pemphigoid are autoimmune blistering diseases characterized by mucocutaneous blisters elicited by an autoantibody-mediated immune response against specific proteins of the epidermal basement membrane. The antibiotic dapsone is frequently used to treat both diseases, but its therapeutic effectiveness is uncertain, and its mode of action in these diseases is largely unknown. We evaluated the effect of dapsone in antibody transfer mouse models of epidermolysis bullosa acquisita and mucous membrane pemphigoid, which do not allow the drawing of conclusions on clinical treatment regimens but can be instrumental to partially uncover the mode(s) of action of dapsone in these diseases. Dapsone significantly mitigated inflammation in both models, reducing the recruitment of neutrophils into the skin and disrupting their release of leukotriene B₄ (LTB₄) and ROS in response to immune complexes. LTB₄ has been implicated in numerous diseases, but effective LTB₄ inhibitors for clinical use are not available. Our findings indicate that the mode of action of dapsone in these models may be based on the inhibition of LTB₄ and ROS release from neutrophils. Moreover, they encourage testing the use of dapsone as an effective, albeit nonspecific, inhibitor of LTB₄ biosynthesis in other LTB₄-driven diseases.

Originalsprache	Englisch
Zeitschrift	Journal of Investigative Dermatology
Jahrgang	141
Ausgabenummer	11
Seiten (von - bis)	2587-2595.e2
ISSN	0022-202X
DOIs	https://doi.org/10.1016/j.jid.2021.04.009
Publikationsstatus	Veröffentlicht - 11.2021

Fördermittel

DZ received consultant’s honoraria from UCB, Almirall, and ArGEN-X; grants from Biotest, Euroimmun, and Fresenius; and speakers’ honoraria/travel support from Biotest, Fresenius, Miltenyi, Roche, Biogen, AbbVie, UCB, Janssen, and Novartis. The remaining authors state no conflict of interest. This research was supported by funding from the Deutsche Forschungsgemeinschaft for the Clinical Research Unit 303 Pemphigoid Diseases—Molecular Pathways and their Therapeutic Potential and for the Excellence Cluster (EXC) 2167 Precision Medicine in Chronic Inflammation. This research was supported by funding from the Deutsche Forschungsgemeinschaft for the Clinical Research Unit 303 Pemphigoid Diseases?Molecular Pathways and their Therapeutic Potential and for the Excellence Cluster (EXC) 2167 Precision Medicine in Chronic Inflammation. Conceptualization: CDS; Data Curation: CDS; Formal Analysis: SM, CDS; Funding Acquisition: CDS, DZ; Investigation: SM, PS, SP, MT, MB, TB, LKn, LKr, ADH, FF; Methodology: ES, SMI; Supervision: CDS; Writing - Original Draft Preparation: SM, CDS; Writing - Review and Editing: DZ, ES, SMI

UN SDGs

Dieser Output leistet einen Beitrag zu folgendem(n) Ziel(en) für nachhaltige Entwicklung

SDG 3 – Gesundheit und Wohlergehen

Strategische Forschungsbereiche und Zentren

Forschungsschwerpunkt: Infektion und Entzündung - Zentrum für Infektions- und Entzündungsforschung Lübeck (ZIEL)
Zentren: Center for Research on Inflammation of the Skin (CRIS)

DFG-Fachsystematik

2.21-05 Immunologie
2.22-19 Dermatologie

Dokumente

10.1016/j.jid.2021.04.009

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EXC 2167: Präzisionsmedizin für Chronische Entzündungserkrankungen (PMI)
Schreiber, S. (Sprecher*in), Baines, J. F. (Beteiligte*r Wissenschaftler*in), Bosch, T. C. G. (Beteiligte*r Wissenschaftler*in), Buyx, A. (Beteiligte*r Wissenschaftler*in), Erdmann, J. (Beteiligte*r Wissenschaftler*in), Franke, A. (Beteiligte*r Wissenschaftler*in), Huber, R. (Beteiligte*r Wissenschaftler*in), Klein, C. (Beteiligte*r Wissenschaftler*in), Köhl, J. (Beteiligte*r Wissenschaftler*in), König, I. R. (Beteiligte*r Wissenschaftler*in), Lange, C. (Beteiligte*r Wissenschaftler*in), Laudes, M. (Beteiligte*r Wissenschaftler*in), Lieb, W. (Beteiligte*r Wissenschaftler*in), Ludwig, R. (Beteiligte*r Wissenschaftler*in), Nebel, A. (Beteiligte*r Wissenschaftler*in), Niemann, S. (Sprecher*in), Rabe, K. F. (Beteiligte*r Wissenschaftler*in), Riemekasten, G. (Sprecher*in), Rose-John, S. (Beteiligte*r Wissenschaftler*in), Rosenstiel, P. C. (Beteiligte*r Wissenschaftler*in), Schulenburg, H. (Beteiligte*r Wissenschaftler*in), Schwarz, K. (Beteiligte*r Wissenschaftler*in), Traulsen, A. (Beteiligte*r Wissenschaftler*in), Weidinger, S. (Beteiligte*r Wissenschaftler*in) & Zillikens, D. (Beteiligte*r Wissenschaftler*in)
01.01.19 → 31.12.32
Projekt: DFG Verbundprojekte › Exzellenzcluster

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Murthy, S., Schilf, P., Patzelt, S., Thieme, M., Becker, M., Kröger, L., Bremer, T., Derenda-Hell, A., Knebel, L., Fagiani, F., Ibrahim, S. M., Schmidt, E., Zillikens, D., & Sadik, C. D. (2021). Dapsone Suppresses Disease in Preclinical Murine Models of Pemphigoid Diseases. Journal of Investigative Dermatology, 141(11), 2587-2595.e2. https://doi.org/10.1016/j.jid.2021.04.009

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title = "Dapsone Suppresses Disease in Preclinical Murine Models of Pemphigoid Diseases",

abstract = "Epidermolysis bullosa acquisita and mucous membrane pemphigoid are autoimmune blistering diseases characterized by mucocutaneous blisters elicited by an autoantibody-mediated immune response against specific proteins of the epidermal basement membrane. The antibiotic dapsone is frequently used to treat both diseases, but its therapeutic effectiveness is uncertain, and its mode of action in these diseases is largely unknown. We evaluated the effect of dapsone in antibody transfer mouse models of epidermolysis bullosa acquisita and mucous membrane pemphigoid, which do not allow the drawing of conclusions on clinical treatment regimens but can be instrumental to partially uncover the mode(s) of action of dapsone in these diseases. Dapsone significantly mitigated inflammation in both models, reducing the recruitment of neutrophils into the skin and disrupting their release of leukotriene B4 (LTB4) and ROS in response to immune complexes. LTB4 has been implicated in numerous diseases, but effective LTB4 inhibitors for clinical use are not available. Our findings indicate that the mode of action of dapsone in these models may be based on the inhibition of LTB4 and ROS release from neutrophils. Moreover, they encourage testing the use of dapsone as an effective, albeit nonspecific, inhibitor of LTB4 biosynthesis in other LTB4-driven diseases.",

author = "Sripriya Murthy and Paul Schilf and Sabrina Patzelt and Markus Thieme and Mareike Becker and Lasse Kr{\"o}ger and Tabea Bremer and Aleksandra Derenda-Hell and Lea Knebel and Francesca Fagiani and Ibrahim, \{Saleh M.\} and Enno Schmidt and Detlef Zillikens and Sadik, \{Christian D.\}",

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year = "2021",

month = nov,

doi = "10.1016/j.jid.2021.04.009",

language = "English",

volume = "141",

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Murthy, S , Schilf, P, Patzelt, S, Thieme, M, Becker, M, Kröger, L, Bremer, T, Derenda-Hell, A, Knebel, L, Fagiani, F, Ibrahim, SM, Schmidt, E, Zillikens, D & Sadik, CD 2021, 'Dapsone Suppresses Disease in Preclinical Murine Models of Pemphigoid Diseases', Journal of Investigative Dermatology, Jg. 141, Nr. 11, S. 2587-2595.e2. https://doi.org/10.1016/j.jid.2021.04.009

TY - JOUR

T1 - Dapsone Suppresses Disease in Preclinical Murine Models of Pemphigoid Diseases

AU - Murthy, Sripriya

AU - Schilf, Paul

AU - Patzelt, Sabrina

AU - Thieme, Markus

AU - Becker, Mareike

AU - Kröger, Lasse

AU - Bremer, Tabea

AU - Derenda-Hell, Aleksandra

AU - Knebel, Lea

AU - Fagiani, Francesca

AU - Ibrahim, Saleh M.

AU - Schmidt, Enno

AU - Zillikens, Detlef

AU - Sadik, Christian D.

PY - 2021/11

Y1 - 2021/11

N2 - Epidermolysis bullosa acquisita and mucous membrane pemphigoid are autoimmune blistering diseases characterized by mucocutaneous blisters elicited by an autoantibody-mediated immune response against specific proteins of the epidermal basement membrane. The antibiotic dapsone is frequently used to treat both diseases, but its therapeutic effectiveness is uncertain, and its mode of action in these diseases is largely unknown. We evaluated the effect of dapsone in antibody transfer mouse models of epidermolysis bullosa acquisita and mucous membrane pemphigoid, which do not allow the drawing of conclusions on clinical treatment regimens but can be instrumental to partially uncover the mode(s) of action of dapsone in these diseases. Dapsone significantly mitigated inflammation in both models, reducing the recruitment of neutrophils into the skin and disrupting their release of leukotriene B4 (LTB4) and ROS in response to immune complexes. LTB4 has been implicated in numerous diseases, but effective LTB4 inhibitors for clinical use are not available. Our findings indicate that the mode of action of dapsone in these models may be based on the inhibition of LTB4 and ROS release from neutrophils. Moreover, they encourage testing the use of dapsone as an effective, albeit nonspecific, inhibitor of LTB4 biosynthesis in other LTB4-driven diseases.

AB - Epidermolysis bullosa acquisita and mucous membrane pemphigoid are autoimmune blistering diseases characterized by mucocutaneous blisters elicited by an autoantibody-mediated immune response against specific proteins of the epidermal basement membrane. The antibiotic dapsone is frequently used to treat both diseases, but its therapeutic effectiveness is uncertain, and its mode of action in these diseases is largely unknown. We evaluated the effect of dapsone in antibody transfer mouse models of epidermolysis bullosa acquisita and mucous membrane pemphigoid, which do not allow the drawing of conclusions on clinical treatment regimens but can be instrumental to partially uncover the mode(s) of action of dapsone in these diseases. Dapsone significantly mitigated inflammation in both models, reducing the recruitment of neutrophils into the skin and disrupting their release of leukotriene B4 (LTB4) and ROS in response to immune complexes. LTB4 has been implicated in numerous diseases, but effective LTB4 inhibitors for clinical use are not available. Our findings indicate that the mode of action of dapsone in these models may be based on the inhibition of LTB4 and ROS release from neutrophils. Moreover, they encourage testing the use of dapsone as an effective, albeit nonspecific, inhibitor of LTB4 biosynthesis in other LTB4-driven diseases.

UR - https://www.scopus.com/pages/publications/85107943548

UR - https://www.mendeley.com/catalogue/fc654e29-7d6c-3b1c-97c6-0a520c14ccb0/

U2 - 10.1016/j.jid.2021.04.009

DO - 10.1016/j.jid.2021.04.009

M3 - Journal articles

C2 - 34033839

AN - SCOPUS:85107943548

SN - 0022-202X

VL - 141

SP - 2587-2595.e2

JO - Journal of Investigative Dermatology

JF - Journal of Investigative Dermatology

IS - 11

ER -

Dapsone Suppresses Disease in Preclinical Murine Models of Pemphigoid Diseases

Abstract

Fördermittel

UN SDGs

Strategische Forschungsbereiche und Zentren

DFG-Fachsystematik

Dokumente

Weitere Links

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Projekte

EXC 2167: Präzisionsmedizin für Chronische Entzündungserkrankungen (PMI)

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