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The receptor BLT1 is essential on neutrophils in a mouse model of mucous membrane pemphigoid
Tabea Bremer, Sripriya Murthy, Sabrina Patzelt, Paul Schilf, Mareike Neumann, Sina Gonther, Jasper Pruessmann, Wiebke Pruessmann, Enno Schmidt, Thomas Rülicke, Christian D. Sadik
Tabea Bremer, Sripriya Murthy, Sabrina Patzelt, Paul Schilf, Mareike Neumann, Sina Gonther, Jasper Pruessmann, Wiebke Pruessmann, Enno Schmidt, Thomas Rülicke, Christian D. Sadik
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Research Article Dermatology

The receptor BLT1 is essential on neutrophils in a mouse model of mucous membrane pemphigoid

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Abstract

Mucous membrane pemphigoid (MMP) is a mucocutaneous autoimmune blistering disease affecting diverse mucous membranes and the skin with inflammatory blisters and erosions. The pathogenesis of MMP is only poorly understood, but inflammation in MMP is triggered by specific binding of autoantibodies directed to different proteins of the dermal-epidermal/-epithelial junction, subsequently leading to the influx of inflammatory cells, particularly neutrophils, into the dermis. Using the anti-laminin 332 antibody transfer model of MMP, we addressed the molecular mechanisms of neutrophil infiltration and its significance for the eruption of mucocutaneous lesions. Mice deficient in 5-lipoxygenase (Alox5–/–) or in the leukotriene B4 (LTB4) receptor BLT1 (Ltb4r1–/–) were resistant to skin inflammation and exhibited substantially fewer mucosal lesions, with deficiency in either gene compromising the recruitment of neutrophils to the lesion. Furthermore, neutrophil-specific genetic deficiency in Ltb4r1 similarly protected from MMP. Hence, BLT1 was required on neutrophils, and neutrophil recruitment was indispensable for the eruption of lesions in MMP. In line with these findings, the BLT1 inhibitor CP-105,606 ameliorated MMP dose-dependently. Collectively, our results highlight neutrophils and LTB4/BLT1 as key drivers of inflammation in MMP and as promising therapeutic targets.

Authors

Tabea Bremer, Sripriya Murthy, Sabrina Patzelt, Paul Schilf, Mareike Neumann, Sina Gonther, Jasper Pruessmann, Wiebke Pruessmann, Enno Schmidt, Thomas Rülicke, Christian D. Sadik

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Figure 5

Neutrophil-specific Ltb4r1–/– (Ltb4r1ΔPMN) mice are protected from mucocutaneous lesions in the MMP model.

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Neutrophil-specific Ltb4r1–/– (Ltb4r1ΔPMN) mice are protected from mucoc...
(A) Ltb4r1/Hprt1 mRNA levels in bone marrow leukocytes, neutrophils, and neutrophil-depleted leukocytes. (B) Chemotaxis of neutrophils toward LTB4. (C) The total body surface (%) affected by lesions (n = 7 male and 7 female mice/group). (D) Representative clinical presentation and (E) histopathology and immunopathology of the skin on day 16 with (a) H&E staining of lesional skin, arrows indicate dermal epidermal clefts; (b) immunofluorescence stainings for Ly-6G in the dermis of inflamed skin, arrows indicate Ly-6G+ cells; (c) direct immunofluorescence staining for IgG, arrows indicate the IgG depositions at the dermal-epidermal junction; and (d) immunofluorescence staining for C3, arrows indicate C3 depositions at the dermal-epidermal junction. (F) Contingency table of wild-type and Ltb4r1ΔPMN mice with and without oropharyngeal lesions. (G) Severity of mucosal lesions in those mice developing lesions (n = 6–11 mice/group). (H) Representative endoscopic pictures of mucosal surfaces. Arrows indicate inflammatory lesions. (I) Contingency table of wild-type and Ltb4r1ΔPMN mice with and without conjunctival lesions (n = 7 male and 6–7 female mice/group). (J) Severity of conjunctivitis in those mice with mucosal inflammation (n = 6–14). (K) Representative H&E stainings of the conjunctiva. Arrows indicate dermal-epidermal clefts, and scale bars equal 50 μm. Data merged from 2 independent experiments are presented as mean ± SEM. Each dot in A, B, G, and J represents a mouse. Results in A–C were compared by 2-way ANOVA and Holm-Šídák post hoc test and in G and J by Mann-Whitney test. *P < 0.05; **P < 0.01; ***P < 0.01; ****P < 0.0001 for the comparisons indicated. The results in G and I were analyzed by χ2 test. In both, the groups significantly differed with P < 0.01.

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