Targeting IL-6 by both passive or active immunization strategies prevents bleomycin-induced skin fibrosis

Lucille Desallais; Jérôme Avouac; Maxime Fréchet; Muriel Elhai; Rojo Ratsimandresy; Matthieu Montes; Hadley Mouhsine; Hervé Do; Jean François Zagury; Yannick Allanore

doi:10.1186/ar4672

Targeting IL-6 by both passive or active immunization strategies prevents bleomycin-induced skin fibrosis

Lucille Desallais, Jérôme Avouac^*, Maxime Fréchet, Muriel Elhai, Rojo Ratsimandresy, Matthieu Montes, Hadley Mouhsine, Hervé Do, Jean François Zagury, Yannick Allanore

^*Corresponding author for this work

Medicine, Rheumatology Division

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

63 Scopus citations

Abstract

Introduction: Interleukin-6 (IL-6) is a pleiotropic cytokine for which preliminary data have suggested that it might contribute to systemic sclerosis (SSc). Our aims were to investigate, firstly, IL-6 expression in patients with SSc and, secondly, the efficacy of both passive and active immunization against IL-6 to reduce skin fibrosis in complementary mouse models of SSc.Methods: Human serum levels and skin expression of IL-6 were determined by enzyme-linked immunosorbent assay and immunohistochemistry, respectively. We first evaluated the antifibrotic properties of the monoclonal anti-IL-6R antibody, MR16-1, in the bleomycin-induced dermal fibrosis mouse model, reflecting early and inflammatory stages of SSc. Then, we assessed the efficacy of MR16-1 in tight skin-1 (Tsk-1) mice, an inflammation-independent model of skin fibrosis. Additionally, we have developed an innovative strategy using an anti-IL-6 peptide-based active immunization. Infiltrating leukocytes, T cells, and B cells were quantified, and IL-6 levels were measured in the serum and lesional skin of mice after passive or active immunization.Results: Serum and skin levels of IL-6 were significantly increased in patients with early SSc. Treatment with MR16-1 led in the bleomycin mouse model to a 25% (P = 0.02) and 30% (P = 0.007) reduction of dermal thickness and hydroxyproline content, respectively. MR16-1 demonstrated no efficacy in Tsk-1 mice. Thereafter, mice were immunized against a small peptide derived from murine IL-6 and this strategy led in the bleomycin model to a 20% (P = 0.02) and 25% (P = 0.005) decrease of dermal thickness and hydroxyproline content, respectively. Passive and active immunization led to decreased T-cell infiltration in the lesional skin of mice challenged with bleomycin. Upon bleomycin injections, serum and skin IL-6 levels were increased after treatment with MR16-1 and were significantly reduced after anti-IL-6 active immunization.Conclusions: Our results support the relevance of targeting IL-6 in patients with early SSc since IL-6 is overexpressed in early stages of the disease. Targeting IL-6 by both passive and active immunization strategies prevented the development of bleomycin-induced dermal fibrosis in mice. Our results highlight the therapeutic potential of active immunization against IL-6, which is a seductive alternative to passive immunization.

Original language	English (US)
Article number	R157
Journal	Arthritis Research and Therapy
Volume	16
Issue number	4
DOIs	https://doi.org/10.1186/ar4672
State	Published - Jul 24 2014

ASJC Scopus subject areas

Rheumatology
Immunology and Allergy
Immunology

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This output contributes to the following UN Sustainable Development Goals (SDGs)

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10.1186/ar4672

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@article{1f57a950201c4e5ea26e075459213caa,

title = "Targeting IL-6 by both passive or active immunization strategies prevents bleomycin-induced skin fibrosis",

abstract = "Introduction: Interleukin-6 (IL-6) is a pleiotropic cytokine for which preliminary data have suggested that it might contribute to systemic sclerosis (SSc). Our aims were to investigate, firstly, IL-6 expression in patients with SSc and, secondly, the efficacy of both passive and active immunization against IL-6 to reduce skin fibrosis in complementary mouse models of SSc.Methods: Human serum levels and skin expression of IL-6 were determined by enzyme-linked immunosorbent assay and immunohistochemistry, respectively. We first evaluated the antifibrotic properties of the monoclonal anti-IL-6R antibody, MR16-1, in the bleomycin-induced dermal fibrosis mouse model, reflecting early and inflammatory stages of SSc. Then, we assessed the efficacy of MR16-1 in tight skin-1 (Tsk-1) mice, an inflammation-independent model of skin fibrosis. Additionally, we have developed an innovative strategy using an anti-IL-6 peptide-based active immunization. Infiltrating leukocytes, T cells, and B cells were quantified, and IL-6 levels were measured in the serum and lesional skin of mice after passive or active immunization.Results: Serum and skin levels of IL-6 were significantly increased in patients with early SSc. Treatment with MR16-1 led in the bleomycin mouse model to a 25% (P = 0.02) and 30% (P = 0.007) reduction of dermal thickness and hydroxyproline content, respectively. MR16-1 demonstrated no efficacy in Tsk-1 mice. Thereafter, mice were immunized against a small peptide derived from murine IL-6 and this strategy led in the bleomycin model to a 20% (P = 0.02) and 25% (P = 0.005) decrease of dermal thickness and hydroxyproline content, respectively. Passive and active immunization led to decreased T-cell infiltration in the lesional skin of mice challenged with bleomycin. Upon bleomycin injections, serum and skin IL-6 levels were increased after treatment with MR16-1 and were significantly reduced after anti-IL-6 active immunization.Conclusions: Our results support the relevance of targeting IL-6 in patients with early SSc since IL-6 is overexpressed in early stages of the disease. Targeting IL-6 by both passive and active immunization strategies prevented the development of bleomycin-induced dermal fibrosis in mice. Our results highlight the therapeutic potential of active immunization against IL-6, which is a seductive alternative to passive immunization.",

author = "Lucille Desallais and J{\'e}r{\^o}me Avouac and Maxime Fr{\'e}chet and Muriel Elhai and Rojo Ratsimandresy and Matthieu Montes and Hadley Mouhsine and Herv{\'e} Do and Zagury, {Jean Fran{\c c}ois} and Yannick Allanore",

note = "Funding Information: We acknowledge for their assistance the Plateformes d{\textquoteright}Immuno-biologie (M. Andrieu), de Morphologie / Histologie (M. Favier) et d{\textquoteright}imagerie cellulaire (P. Bourdoncle) de l{\textquoteright}institut Cochin, Paris, France and Prof. C. Chaussain, EA2496, Universit{\'e} Paris Descartes, Facult{\'e} de Chirurgie Dentaire, Montrouge, France. LD was funded by a fellowship from Direction G{\'e}n{\'e}rale de l{\textquoteright}Armement, and the work was funded in part by Conservatoire National des Arts et M{\'e}tiers. Funding Information: YA has received honorarium and research grants from Roche (Basel, Switzerland), Pfizer (New York, NY, USA), and Sanofi (Paris, France). JA has received research grants and honorarium from Actelion (Allschwil, Switzerland) and Pfizer. The other authors declare that they have no competing interests. Publisher Copyright: {\textcopyright} 2014 Desallais et al.; licensee BioMed Central Ltd.",

year = "2014",

month = jul,

day = "24",

doi = "10.1186/ar4672",

language = "English (US)",

volume = "16",

journal = "Arthritis Research and Therapy",

issn = "1478-6354",

publisher = "BioMed Central",

number = "4",

}

TY - JOUR

T1 - Targeting IL-6 by both passive or active immunization strategies prevents bleomycin-induced skin fibrosis

AU - Desallais, Lucille

AU - Avouac, Jérôme

AU - Fréchet, Maxime

AU - Elhai, Muriel

AU - Ratsimandresy, Rojo

AU - Montes, Matthieu

AU - Mouhsine, Hadley

AU - Do, Hervé

AU - Zagury, Jean François

AU - Allanore, Yannick

N1 - Funding Information: We acknowledge for their assistance the Plateformes d’Immuno-biologie (M. Andrieu), de Morphologie / Histologie (M. Favier) et d’imagerie cellulaire (P. Bourdoncle) de l’institut Cochin, Paris, France and Prof. C. Chaussain, EA2496, Université Paris Descartes, Faculté de Chirurgie Dentaire, Montrouge, France. LD was funded by a fellowship from Direction Générale de l’Armement, and the work was funded in part by Conservatoire National des Arts et Métiers. Funding Information: YA has received honorarium and research grants from Roche (Basel, Switzerland), Pfizer (New York, NY, USA), and Sanofi (Paris, France). JA has received research grants and honorarium from Actelion (Allschwil, Switzerland) and Pfizer. The other authors declare that they have no competing interests. Publisher Copyright: © 2014 Desallais et al.; licensee BioMed Central Ltd.

PY - 2014/7/24

Y1 - 2014/7/24

N2 - Introduction: Interleukin-6 (IL-6) is a pleiotropic cytokine for which preliminary data have suggested that it might contribute to systemic sclerosis (SSc). Our aims were to investigate, firstly, IL-6 expression in patients with SSc and, secondly, the efficacy of both passive and active immunization against IL-6 to reduce skin fibrosis in complementary mouse models of SSc.Methods: Human serum levels and skin expression of IL-6 were determined by enzyme-linked immunosorbent assay and immunohistochemistry, respectively. We first evaluated the antifibrotic properties of the monoclonal anti-IL-6R antibody, MR16-1, in the bleomycin-induced dermal fibrosis mouse model, reflecting early and inflammatory stages of SSc. Then, we assessed the efficacy of MR16-1 in tight skin-1 (Tsk-1) mice, an inflammation-independent model of skin fibrosis. Additionally, we have developed an innovative strategy using an anti-IL-6 peptide-based active immunization. Infiltrating leukocytes, T cells, and B cells were quantified, and IL-6 levels were measured in the serum and lesional skin of mice after passive or active immunization.Results: Serum and skin levels of IL-6 were significantly increased in patients with early SSc. Treatment with MR16-1 led in the bleomycin mouse model to a 25% (P = 0.02) and 30% (P = 0.007) reduction of dermal thickness and hydroxyproline content, respectively. MR16-1 demonstrated no efficacy in Tsk-1 mice. Thereafter, mice were immunized against a small peptide derived from murine IL-6 and this strategy led in the bleomycin model to a 20% (P = 0.02) and 25% (P = 0.005) decrease of dermal thickness and hydroxyproline content, respectively. Passive and active immunization led to decreased T-cell infiltration in the lesional skin of mice challenged with bleomycin. Upon bleomycin injections, serum and skin IL-6 levels were increased after treatment with MR16-1 and were significantly reduced after anti-IL-6 active immunization.Conclusions: Our results support the relevance of targeting IL-6 in patients with early SSc since IL-6 is overexpressed in early stages of the disease. Targeting IL-6 by both passive and active immunization strategies prevented the development of bleomycin-induced dermal fibrosis in mice. Our results highlight the therapeutic potential of active immunization against IL-6, which is a seductive alternative to passive immunization.

AB - Introduction: Interleukin-6 (IL-6) is a pleiotropic cytokine for which preliminary data have suggested that it might contribute to systemic sclerosis (SSc). Our aims were to investigate, firstly, IL-6 expression in patients with SSc and, secondly, the efficacy of both passive and active immunization against IL-6 to reduce skin fibrosis in complementary mouse models of SSc.Methods: Human serum levels and skin expression of IL-6 were determined by enzyme-linked immunosorbent assay and immunohistochemistry, respectively. We first evaluated the antifibrotic properties of the monoclonal anti-IL-6R antibody, MR16-1, in the bleomycin-induced dermal fibrosis mouse model, reflecting early and inflammatory stages of SSc. Then, we assessed the efficacy of MR16-1 in tight skin-1 (Tsk-1) mice, an inflammation-independent model of skin fibrosis. Additionally, we have developed an innovative strategy using an anti-IL-6 peptide-based active immunization. Infiltrating leukocytes, T cells, and B cells were quantified, and IL-6 levels were measured in the serum and lesional skin of mice after passive or active immunization.Results: Serum and skin levels of IL-6 were significantly increased in patients with early SSc. Treatment with MR16-1 led in the bleomycin mouse model to a 25% (P = 0.02) and 30% (P = 0.007) reduction of dermal thickness and hydroxyproline content, respectively. MR16-1 demonstrated no efficacy in Tsk-1 mice. Thereafter, mice were immunized against a small peptide derived from murine IL-6 and this strategy led in the bleomycin model to a 20% (P = 0.02) and 25% (P = 0.005) decrease of dermal thickness and hydroxyproline content, respectively. Passive and active immunization led to decreased T-cell infiltration in the lesional skin of mice challenged with bleomycin. Upon bleomycin injections, serum and skin IL-6 levels were increased after treatment with MR16-1 and were significantly reduced after anti-IL-6 active immunization.Conclusions: Our results support the relevance of targeting IL-6 in patients with early SSc since IL-6 is overexpressed in early stages of the disease. Targeting IL-6 by both passive and active immunization strategies prevented the development of bleomycin-induced dermal fibrosis in mice. Our results highlight the therapeutic potential of active immunization against IL-6, which is a seductive alternative to passive immunization.

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Targeting IL-6 by both passive or active immunization strategies prevents bleomycin-induced skin fibrosis

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