Toll-Like Receptor 3 Mediates Aortic Stenosis Through a Conserved Mechanism of Calcification

Can Gollmann-Tepeköylü; Michael Graber; Jakob Hirsch; Sophia Mair; Andreas Naschberger; Leo Pölzl; Felix Nägele; Elke Kirchmair; Gerald Degenhart; Egon Demetz; Richard Hilbe; Hao Yu Chen; James C. Engert; Anna Böhm; Nadja Franz; Daniela Lobenwein; Daniela Lener; Christiane Fuchs; Anna Weihs; Sonja Töchterle; Georg F. Vogel; Victor Schweiger; Jonas Eder; Peter Pietschmann; Markus Seifert; Florian Kronenberg; Stefan Coassin; Michael Blumer; Hubert Hackl; Dirk Meyer; Gudrun Feuchtner; Rudolf Kirchmair; Jakob Troppmair; Markus Krane; Günther Weiss; Sotirios Tsimikas; George Thanassoulis; Michael Grimm; Bernhard Rupp; Lukas A. Huber; Shen Ying Zhang; Jean Laurent Casanova; Ivan Tancevski; Johannes Holfeld

doi:10.1161/CIRCULATIONAHA.122.063481

Toll-Like Receptor 3 Mediates Aortic Stenosis Through a Conserved Mechanism of Calcification

Can Gollmann-Tepeköylü, Michael Graber, Jakob Hirsch, Sophia Mair, Andreas Naschberger, Leo Pölzl, Felix Nägele, Elke Kirchmair, Gerald Degenhart, Egon Demetz, Richard Hilbe, Hao Yu Chen, James C. Engert, Anna Böhm, Nadja Franz, Daniela Lobenwein, Daniela Lener, Christiane Fuchs, Anna Weihs, Sonja TöchterleGeorg F. Vogel, Victor Schweiger, Jonas Eder, Peter Pietschmann, Markus Seifert, Florian Kronenberg, Stefan Coassin, Michael Blumer, Hubert Hackl, Dirk Meyer, Gudrun Feuchtner, Rudolf Kirchmair, Jakob Troppmair, Markus Krane, Günther Weiss, Sotirios Tsimikas, George Thanassoulis, Michael Grimm, Bernhard Rupp, Lukas A. Huber, Shen Ying Zhang, Jean Laurent Casanova, Ivan Tancevski, Johannes Holfeld

Clinic for Heart and Vascular Surgery

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

11 Scopus citations

Abstract

BACKGROUND: Calcific aortic valve disease (CAVD) is characterized by a phenotypic switch of valvular interstitial cells to bone-forming cells. Toll-like receptors (TLRs) are evolutionarily conserved pattern recognition receptors at the interface between innate immunity and tissue repair. Type I interferons (IFNs) are not only crucial for an adequate antiviral response but also implicated in bone formation. We hypothesized that the accumulation of endogenous TLR3 ligands in the valvular leaflets may promote the generation of osteoblast-like cells through enhanced type I IFN signaling. METHODS: Human valvular interstitial cells isolated from aortic valves were challenged with mechanical strain or synthetic TLR3 agonists and analyzed for bone formation, gene expression profiles, and IFN signaling pathways. Different inhibitors were used to delineate the engaged signaling pathways. Moreover, we screened a variety of potential lipids and proteoglycans known to accumulate in CAVD lesions as potential TLR3 ligands. Ligand-receptor interactions were characterized by in silico modeling and verified through immunoprecipitation experiments. Biglycan (Bgn), Tlr3, and IFNα/β receptor alpha chain (Ifnar1)–deficient mice and a specific zebrafish model were used to study the implication of the biglycan (BGN)-TLR3-IFN axis in both CAVD and bone formation in vivo. Two large-scale cohorts (GERA [Genetic Epidemiology Research on Adult Health and Aging], n=55 192 with 3469 aortic stenosis cases; UK Biobank, n=257 231 with 2213 aortic stenosis cases) were examined for genetic variation at genes implicated in BGN-TLR3-IFN signaling associating with CAVD in humans. RESULTS: Here, we identify TLR3 as a central molecular regulator of calcification in valvular interstitial cells and unravel BGN as a new endogenous agonist of TLR3. Posttranslational BGN maturation by xylosyltransferase 1 (XYLT1) is required for TLR3 activation. Moreover, BGN induces the transdifferentiation of valvular interstitial cells into bone-forming osteoblasts through the TLR3-dependent induction of type I IFNs. It is intriguing that Bgn^−/−, Tlr3^−/−, and Ifnar1^−/− mice are protected against CAVD and display impaired bone formation. Meta-analysis of 2 large-scale cohorts with >300 000 individuals reveals that genetic variation at loci relevant to the XYLT1–BGN–TLR3–interferon-α/β receptor alpha chain (IFNAR) 1 pathway is associated with CAVD in humans. CONCLUSIONS: This study identifies the BGN-TLR3-IFNAR1 axis as an evolutionarily conserved pathway governing calcification of the aortic valve and reveals a potential therapeutic target to prevent CAVD.

Original language	English
Pages (from-to)	1518-1533
Number of pages	16
Journal	Circulation
Volume	147
Issue number	20
DOIs	https://doi.org/10.1161/CIRCULATIONAHA.122.063481
State	Published - 16 May 2023

Keywords

Toll-like receptor 3
aortic valve disease
biglycan
extracellular matrix
osteogenesis
proteins

UN SDGs

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

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10.1161/CIRCULATIONAHA.122.063481

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Gollmann-Tepeköylü, C., Graber, M., Hirsch, J., Mair, S., Naschberger, A., Pölzl, L., Nägele, F., Kirchmair, E., Degenhart, G., Demetz, E., Hilbe, R., Chen, H. Y., Engert, J. C., Böhm, A., Franz, N., Lobenwein, D., Lener, D., Fuchs, C., Weihs, A., ... Holfeld, J. (2023). Toll-Like Receptor 3 Mediates Aortic Stenosis Through a Conserved Mechanism of Calcification. Circulation, 147(20), 1518-1533. https://doi.org/10.1161/CIRCULATIONAHA.122.063481

@article{ecee2571251246b4bb2ef6c1b0bd74ce,

title = "Toll-Like Receptor 3 Mediates Aortic Stenosis Through a Conserved Mechanism of Calcification",

abstract = "BACKGROUND: Calcific aortic valve disease (CAVD) is characterized by a phenotypic switch of valvular interstitial cells to bone-forming cells. Toll-like receptors (TLRs) are evolutionarily conserved pattern recognition receptors at the interface between innate immunity and tissue repair. Type I interferons (IFNs) are not only crucial for an adequate antiviral response but also implicated in bone formation. We hypothesized that the accumulation of endogenous TLR3 ligands in the valvular leaflets may promote the generation of osteoblast-like cells through enhanced type I IFN signaling. METHODS: Human valvular interstitial cells isolated from aortic valves were challenged with mechanical strain or synthetic TLR3 agonists and analyzed for bone formation, gene expression profiles, and IFN signaling pathways. Different inhibitors were used to delineate the engaged signaling pathways. Moreover, we screened a variety of potential lipids and proteoglycans known to accumulate in CAVD lesions as potential TLR3 ligands. Ligand-receptor interactions were characterized by in silico modeling and verified through immunoprecipitation experiments. Biglycan (Bgn), Tlr3, and IFNα/β receptor alpha chain (Ifnar1)–deficient mice and a specific zebrafish model were used to study the implication of the biglycan (BGN)-TLR3-IFN axis in both CAVD and bone formation in vivo. Two large-scale cohorts (GERA [Genetic Epidemiology Research on Adult Health and Aging], n=55 192 with 3469 aortic stenosis cases; UK Biobank, n=257 231 with 2213 aortic stenosis cases) were examined for genetic variation at genes implicated in BGN-TLR3-IFN signaling associating with CAVD in humans. RESULTS: Here, we identify TLR3 as a central molecular regulator of calcification in valvular interstitial cells and unravel BGN as a new endogenous agonist of TLR3. Posttranslational BGN maturation by xylosyltransferase 1 (XYLT1) is required for TLR3 activation. Moreover, BGN induces the transdifferentiation of valvular interstitial cells into bone-forming osteoblasts through the TLR3-dependent induction of type I IFNs. It is intriguing that Bgn−/−, Tlr3−/−, and Ifnar1−/− mice are protected against CAVD and display impaired bone formation. Meta-analysis of 2 large-scale cohorts with >300 000 individuals reveals that genetic variation at loci relevant to the XYLT1–BGN–TLR3–interferon-α/β receptor alpha chain (IFNAR) 1 pathway is associated with CAVD in humans. CONCLUSIONS: This study identifies the BGN-TLR3-IFNAR1 axis as an evolutionarily conserved pathway governing calcification of the aortic valve and reveals a potential therapeutic target to prevent CAVD.",

keywords = "Toll-like receptor 3, aortic valve disease, biglycan, extracellular matrix, osteogenesis, proteins",

author = "Can Gollmann-Tepek{\"o}yl{\"u} and Michael Graber and Jakob Hirsch and Sophia Mair and Andreas Naschberger and Leo P{\"o}lzl and Felix N{\"a}gele and Elke Kirchmair and Gerald Degenhart and Egon Demetz and Richard Hilbe and Chen, {Hao Yu} and Engert, {James C.} and Anna B{\"o}hm and Nadja Franz and Daniela Lobenwein and Daniela Lener and Christiane Fuchs and Anna Weihs and Sonja T{\"o}chterle and Vogel, {Georg F.} and Victor Schweiger and Jonas Eder and Peter Pietschmann and Markus Seifert and Florian Kronenberg and Stefan Coassin and Michael Blumer and Hubert Hackl and Dirk Meyer and Gudrun Feuchtner and Rudolf Kirchmair and Jakob Troppmair and Markus Krane and G{\"u}nther Weiss and Sotirios Tsimikas and George Thanassoulis and Michael Grimm and Bernhard Rupp and Huber, {Lukas A.} and Zhang, {Shen Ying} and Casanova, {Jean Laurent} and Ivan Tancevski and Johannes Holfeld",

note = "Publisher Copyright: {\textcopyright} 2023 American Heart Association, Inc.",

year = "2023",

month = may,

day = "16",

doi = "10.1161/CIRCULATIONAHA.122.063481",

language = "English",

volume = "147",

pages = "1518--1533",

journal = "Circulation",

issn = "0009-7322",

publisher = "Lippincott Williams and Wilkins",

number = "20",

}

Gollmann-Tepeköylü, C, Graber, M, Hirsch, J, Mair, S, Naschberger, A, Pölzl, L, Nägele, F, Kirchmair, E, Degenhart, G, Demetz, E, Hilbe, R, Chen, HY, Engert, JC, Böhm, A, Franz, N, Lobenwein, D, Lener, D, Fuchs, C, Weihs, A, Töchterle, S, Vogel, GF, Schweiger, V, Eder, J, Pietschmann, P, Seifert, M, Kronenberg, F, Coassin, S, Blumer, M, Hackl, H, Meyer, D, Feuchtner, G, Kirchmair, R, Troppmair, J, Krane, M, Weiss, G, Tsimikas, S, Thanassoulis, G, Grimm, M, Rupp, B, Huber, LA, Zhang, SY, Casanova, JL, Tancevski, I & Holfeld, J 2023, 'Toll-Like Receptor 3 Mediates Aortic Stenosis Through a Conserved Mechanism of Calcification', Circulation, vol. 147, no. 20, pp. 1518-1533. https://doi.org/10.1161/CIRCULATIONAHA.122.063481

TY - JOUR

T1 - Toll-Like Receptor 3 Mediates Aortic Stenosis Through a Conserved Mechanism of Calcification

AU - Gollmann-Tepeköylü, Can

AU - Graber, Michael

AU - Hirsch, Jakob

AU - Mair, Sophia

AU - Naschberger, Andreas

AU - Pölzl, Leo

AU - Nägele, Felix

AU - Kirchmair, Elke

AU - Degenhart, Gerald

AU - Demetz, Egon

AU - Hilbe, Richard

AU - Chen, Hao Yu

AU - Engert, James C.

AU - Böhm, Anna

AU - Franz, Nadja

AU - Lobenwein, Daniela

AU - Lener, Daniela

AU - Fuchs, Christiane

AU - Weihs, Anna

AU - Töchterle, Sonja

AU - Vogel, Georg F.

AU - Schweiger, Victor

AU - Eder, Jonas

AU - Pietschmann, Peter

AU - Seifert, Markus

AU - Kronenberg, Florian

AU - Coassin, Stefan

AU - Blumer, Michael

AU - Hackl, Hubert

AU - Meyer, Dirk

AU - Feuchtner, Gudrun

AU - Kirchmair, Rudolf

AU - Troppmair, Jakob

AU - Krane, Markus

AU - Weiss, Günther

AU - Tsimikas, Sotirios

AU - Thanassoulis, George

AU - Grimm, Michael

AU - Rupp, Bernhard

AU - Huber, Lukas A.

AU - Zhang, Shen Ying

AU - Casanova, Jean Laurent

AU - Tancevski, Ivan

AU - Holfeld, Johannes

PY - 2023/5/16

Y1 - 2023/5/16

N2 - BACKGROUND: Calcific aortic valve disease (CAVD) is characterized by a phenotypic switch of valvular interstitial cells to bone-forming cells. Toll-like receptors (TLRs) are evolutionarily conserved pattern recognition receptors at the interface between innate immunity and tissue repair. Type I interferons (IFNs) are not only crucial for an adequate antiviral response but also implicated in bone formation. We hypothesized that the accumulation of endogenous TLR3 ligands in the valvular leaflets may promote the generation of osteoblast-like cells through enhanced type I IFN signaling. METHODS: Human valvular interstitial cells isolated from aortic valves were challenged with mechanical strain or synthetic TLR3 agonists and analyzed for bone formation, gene expression profiles, and IFN signaling pathways. Different inhibitors were used to delineate the engaged signaling pathways. Moreover, we screened a variety of potential lipids and proteoglycans known to accumulate in CAVD lesions as potential TLR3 ligands. Ligand-receptor interactions were characterized by in silico modeling and verified through immunoprecipitation experiments. Biglycan (Bgn), Tlr3, and IFNα/β receptor alpha chain (Ifnar1)–deficient mice and a specific zebrafish model were used to study the implication of the biglycan (BGN)-TLR3-IFN axis in both CAVD and bone formation in vivo. Two large-scale cohorts (GERA [Genetic Epidemiology Research on Adult Health and Aging], n=55 192 with 3469 aortic stenosis cases; UK Biobank, n=257 231 with 2213 aortic stenosis cases) were examined for genetic variation at genes implicated in BGN-TLR3-IFN signaling associating with CAVD in humans. RESULTS: Here, we identify TLR3 as a central molecular regulator of calcification in valvular interstitial cells and unravel BGN as a new endogenous agonist of TLR3. Posttranslational BGN maturation by xylosyltransferase 1 (XYLT1) is required for TLR3 activation. Moreover, BGN induces the transdifferentiation of valvular interstitial cells into bone-forming osteoblasts through the TLR3-dependent induction of type I IFNs. It is intriguing that Bgn−/−, Tlr3−/−, and Ifnar1−/− mice are protected against CAVD and display impaired bone formation. Meta-analysis of 2 large-scale cohorts with >300 000 individuals reveals that genetic variation at loci relevant to the XYLT1–BGN–TLR3–interferon-α/β receptor alpha chain (IFNAR) 1 pathway is associated with CAVD in humans. CONCLUSIONS: This study identifies the BGN-TLR3-IFNAR1 axis as an evolutionarily conserved pathway governing calcification of the aortic valve and reveals a potential therapeutic target to prevent CAVD.

AB - BACKGROUND: Calcific aortic valve disease (CAVD) is characterized by a phenotypic switch of valvular interstitial cells to bone-forming cells. Toll-like receptors (TLRs) are evolutionarily conserved pattern recognition receptors at the interface between innate immunity and tissue repair. Type I interferons (IFNs) are not only crucial for an adequate antiviral response but also implicated in bone formation. We hypothesized that the accumulation of endogenous TLR3 ligands in the valvular leaflets may promote the generation of osteoblast-like cells through enhanced type I IFN signaling. METHODS: Human valvular interstitial cells isolated from aortic valves were challenged with mechanical strain or synthetic TLR3 agonists and analyzed for bone formation, gene expression profiles, and IFN signaling pathways. Different inhibitors were used to delineate the engaged signaling pathways. Moreover, we screened a variety of potential lipids and proteoglycans known to accumulate in CAVD lesions as potential TLR3 ligands. Ligand-receptor interactions were characterized by in silico modeling and verified through immunoprecipitation experiments. Biglycan (Bgn), Tlr3, and IFNα/β receptor alpha chain (Ifnar1)–deficient mice and a specific zebrafish model were used to study the implication of the biglycan (BGN)-TLR3-IFN axis in both CAVD and bone formation in vivo. Two large-scale cohorts (GERA [Genetic Epidemiology Research on Adult Health and Aging], n=55 192 with 3469 aortic stenosis cases; UK Biobank, n=257 231 with 2213 aortic stenosis cases) were examined for genetic variation at genes implicated in BGN-TLR3-IFN signaling associating with CAVD in humans. RESULTS: Here, we identify TLR3 as a central molecular regulator of calcification in valvular interstitial cells and unravel BGN as a new endogenous agonist of TLR3. Posttranslational BGN maturation by xylosyltransferase 1 (XYLT1) is required for TLR3 activation. Moreover, BGN induces the transdifferentiation of valvular interstitial cells into bone-forming osteoblasts through the TLR3-dependent induction of type I IFNs. It is intriguing that Bgn−/−, Tlr3−/−, and Ifnar1−/− mice are protected against CAVD and display impaired bone formation. Meta-analysis of 2 large-scale cohorts with >300 000 individuals reveals that genetic variation at loci relevant to the XYLT1–BGN–TLR3–interferon-α/β receptor alpha chain (IFNAR) 1 pathway is associated with CAVD in humans. CONCLUSIONS: This study identifies the BGN-TLR3-IFNAR1 axis as an evolutionarily conserved pathway governing calcification of the aortic valve and reveals a potential therapeutic target to prevent CAVD.

KW - Toll-like receptor 3

KW - aortic valve disease

KW - biglycan

KW - extracellular matrix

KW - osteogenesis

KW - proteins

UR - http://www.scopus.com/inward/record.url?scp=85159733142&partnerID=8YFLogxK

U2 - 10.1161/CIRCULATIONAHA.122.063481

DO - 10.1161/CIRCULATIONAHA.122.063481

M3 - Article

C2 - 37013819

AN - SCOPUS:85159733142

SN - 0009-7322

VL - 147

SP - 1518

EP - 1533

JO - Circulation

JF - Circulation

IS - 20

ER -

Toll-Like Receptor 3 Mediates Aortic Stenosis Through a Conserved Mechanism of Calcification

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Keywords

UN SDGs

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