Commensal bacteria regulate toll-like receptor 3-dependent inflammation after skin injury

Yuping Lai; Anna Di Nardo; Teruaki Nakatsuji; Anke Leichtle; Yan Yang; Anna L. Cogen; Zi Rong Wu; Lora V. Hooper; Richard R. Schmidt; Sonja Von Aulock; Katherine A. Radek; Chun Ming Huang; Allen F. Ryan; Richard L. Gallo

doi:10.1038/nm.2062

Commensal bacteria regulate toll-like receptor 3-dependent inflammation after skin injury

Yuping Lai, Anna Di Nardo, Teruaki Nakatsuji, Anke Leichtle, Yan Yang, Anna L. Cogen, Zi Rong Wu, Lora V. Hooper, Richard R. Schmidt, Sonja Von Aulock, Katherine A. Radek, Chun Ming Huang, Allen F. Ryan, Richard L. Gallo

Klinik für Hals-, Nasen- und Ohrenheilkunde, Phoniatrie und Pädaudiologie

683 Zitate (Scopus)

Abstract

The normal microflora of the skin includes staphylococcal species that will induce inflammation when present below the dermis but are tolerated on the epidermal surface without initiating inflammation. Here we reveal a previously unknown mechanism by which a product of staphylococci inhibits skin inflammation. This inhibition is mediated by staphylococcal lipoteichoic acid (LTA) and acts selectively on keratinocytes triggered through Toll-like receptor 3(TLR3). We show that TLR3 activation is required for normal inflammation after injury and that keratinocytes require TLR3 to respond to RNA from damaged cells with the release of inflammatory cytokines. Staphylococcal LTA inhibits both inflammatory cytokine release from keratinocytes and inflammation triggered by injury through a TLR2-dependent mechanism. To our knowledge, these findings show for the first time that the skin epithelium requires TLR3 for normal inflammation after wounding and that the microflora can modulate specific cutaneous inflammatory responses.

Originalsprache	Englisch
Zeitschrift	Nature Medicine
Jahrgang	15
Ausgabenummer	12
Seiten (von - bis)	1377-1382
Seitenumfang	6
ISSN	1078-8956
DOIs	https://doi.org/10.1038/nm.2062
Publikationsstatus	Veröffentlicht - 12.2009

Fördermittel

We thank A. Peschel for advice regarding blocking LTA activity by the antibody; E. Raz from the University of California–San Diego for providing a C57BL/6 Tlr3-deficient mouse breeding pair; V. Nizet and E. Tistiskov for helpful discussion; G. Cheng, B. Beutler, R. Modlin and E. Raz for critical reading and helpful advice; and D. Bird for histological sections. This work was supported by US National Institutes of Health grants R56AI083358, R01AR052728 and R01 AI052453 and a US Veterans Administration Merit Award to R.L.G. and US National Institutes of Health grants DC00129 and DC006279 to A.F.R.

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title = "Commensal bacteria regulate toll-like receptor 3-dependent inflammation after skin injury",

abstract = "The normal microflora of the skin includes staphylococcal species that will induce inflammation when present below the dermis but are tolerated on the epidermal surface without initiating inflammation. Here we reveal a previously unknown mechanism by which a product of staphylococci inhibits skin inflammation. This inhibition is mediated by staphylococcal lipoteichoic acid (LTA) and acts selectively on keratinocytes triggered through Toll-like receptor 3(TLR3). We show that TLR3 activation is required for normal inflammation after injury and that keratinocytes require TLR3 to respond to RNA from damaged cells with the release of inflammatory cytokines. Staphylococcal LTA inhibits both inflammatory cytokine release from keratinocytes and inflammation triggered by injury through a TLR2-dependent mechanism. To our knowledge, these findings show for the first time that the skin epithelium requires TLR3 for normal inflammation after wounding and that the microflora can modulate specific cutaneous inflammatory responses.",

author = "Yuping Lai and \{Di Nardo\}, Anna and Teruaki Nakatsuji and Anke Leichtle and Yan Yang and Cogen, \{Anna L.\} and Wu, \{Zi Rong\} and Hooper, \{Lora V.\} and Schmidt, \{Richard R.\} and \{Von Aulock\}, Sonja and Radek, \{Katherine A.\} and Huang, \{Chun Ming\} and Ryan, \{Allen F.\} and Gallo, \{Richard L.\}",

note = "Funding Information: We thank A. Peschel for advice regarding blocking LTA activity by the antibody; E. Raz from the University of California–San Diego for providing a C57BL/6 Tlr3-deficient mouse breeding pair; V. Nizet and E. Tistiskov for helpful discussion; G. Cheng, B. Beutler, R. Modlin and E. Raz for critical reading and helpful advice; and D. Bird for histological sections. This work was supported by US National Institutes of Health grants R56AI083358, R01AR052728 and R01 AI052453 and a US Veterans Administration Merit Award to R.L.G. and US National Institutes of Health grants DC00129 and DC006279 to A.F.R.",

year = "2009",

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doi = "10.1038/nm.2062",

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pages = "1377--1382",

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AU - Lai, Yuping

AU - Di Nardo, Anna

AU - Nakatsuji, Teruaki

AU - Leichtle, Anke

AU - Yang, Yan

AU - Cogen, Anna L.

AU - Wu, Zi Rong

AU - Hooper, Lora V.

AU - Schmidt, Richard R.

AU - Von Aulock, Sonja

AU - Radek, Katherine A.

AU - Huang, Chun Ming

AU - Ryan, Allen F.

AU - Gallo, Richard L.

N1 - Funding Information: We thank A. Peschel for advice regarding blocking LTA activity by the antibody; E. Raz from the University of California–San Diego for providing a C57BL/6 Tlr3-deficient mouse breeding pair; V. Nizet and E. Tistiskov for helpful discussion; G. Cheng, B. Beutler, R. Modlin and E. Raz for critical reading and helpful advice; and D. Bird for histological sections. This work was supported by US National Institutes of Health grants R56AI083358, R01AR052728 and R01 AI052453 and a US Veterans Administration Merit Award to R.L.G. and US National Institutes of Health grants DC00129 and DC006279 to A.F.R.

PY - 2009/12

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N2 - The normal microflora of the skin includes staphylococcal species that will induce inflammation when present below the dermis but are tolerated on the epidermal surface without initiating inflammation. Here we reveal a previously unknown mechanism by which a product of staphylococci inhibits skin inflammation. This inhibition is mediated by staphylococcal lipoteichoic acid (LTA) and acts selectively on keratinocytes triggered through Toll-like receptor 3(TLR3). We show that TLR3 activation is required for normal inflammation after injury and that keratinocytes require TLR3 to respond to RNA from damaged cells with the release of inflammatory cytokines. Staphylococcal LTA inhibits both inflammatory cytokine release from keratinocytes and inflammation triggered by injury through a TLR2-dependent mechanism. To our knowledge, these findings show for the first time that the skin epithelium requires TLR3 for normal inflammation after wounding and that the microflora can modulate specific cutaneous inflammatory responses.

AB - The normal microflora of the skin includes staphylococcal species that will induce inflammation when present below the dermis but are tolerated on the epidermal surface without initiating inflammation. Here we reveal a previously unknown mechanism by which a product of staphylococci inhibits skin inflammation. This inhibition is mediated by staphylococcal lipoteichoic acid (LTA) and acts selectively on keratinocytes triggered through Toll-like receptor 3(TLR3). We show that TLR3 activation is required for normal inflammation after injury and that keratinocytes require TLR3 to respond to RNA from damaged cells with the release of inflammatory cytokines. Staphylococcal LTA inhibits both inflammatory cytokine release from keratinocytes and inflammation triggered by injury through a TLR2-dependent mechanism. To our knowledge, these findings show for the first time that the skin epithelium requires TLR3 for normal inflammation after wounding and that the microflora can modulate specific cutaneous inflammatory responses.

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ER -

Commensal bacteria regulate toll-like receptor 3-dependent inflammation after skin injury

Abstract

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