Chronic encephalomyelitis virus exhibits cellular tropism and evades pDCs by binding to sialylated integrins as the cell surface receptors

Theiler's murine encephalomyelitis virus (TMEV) causes a chronic demyelinating disease similar to multiple sclerosis in mice. Although sialic acids have been shown to be essential for TMEV attachment to the host, the surface receptor has not been identified. While type I interferons play a pivo...

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Veröffentlicht in:	European journal of immunology 2023-10, Vol.53 (10), p.e2350452-n/a
Hauptverfasser:	Takeda, Kazuya, Kaifu, Tomonori, Michihata, Ryunosuke, Kinugawa, Naotaka, Fujioka, Atushi, Tateno, Ayaka, Toshima, Kaoru, Kanoh, Hirotaka, Inamori, Kei‐Ichiro, Kamijo, Keiju, Himeda, Toshiki, Ohara, Yoshiro, Inokuchi, Jin‐Ichi, Nakamura, Akira
Format:	Artikel
Sprache:	eng
Schlagworte:	Cell membranes Cell surface Cell surface receptors Cytoplasm Demyelinating diseases Demyelination Dendritic cells Encephalomyelitis Integrin Integrins Multiple sclerosis pDC Sialic acid Sialic acids TMEV Tropism Virus attachment Viruses
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creator	Takeda, Kazuya Kaifu, Tomonori Michihata, Ryunosuke Kinugawa, Naotaka Fujioka, Atushi Tateno, Ayaka Toshima, Kaoru Kanoh, Hirotaka Inamori, Kei‐Ichiro Kamijo, Keiju Himeda, Toshiki Ohara, Yoshiro Inokuchi, Jin‐Ichi Nakamura, Akira
description	Theiler's murine encephalomyelitis virus (TMEV) causes a chronic demyelinating disease similar to multiple sclerosis in mice. Although sialic acids have been shown to be essential for TMEV attachment to the host, the surface receptor has not been identified. While type I interferons play a pivotal role in the elimination of the chronic infectious Daniel (DA) strain, the role of plasmacytoid dendritic cells (pDCs) is controversial. We herein found that TMEV binds to conventional DCs but not to pDCs. A glycomics analysis showed that the sialylated N‐glycan fractions were lower in pDCs than in conventional DCs, indicating that pDCs are not susceptible to TMEV infection due to the low levels of sialic acid. TMEV capsid proteins contain an integrin recognition motif, and dot blot assays showed that the integrin proteins bind to TMEV and that the viral binding was reduced in the desialylated αXβ2. αXβ2 protein suppressed TMEV replication in vivo, and TMEV co‐localized with integrin αM at the cell membrane and TLR 3 in the cytoplasm, suggesting that αM serves as the viral attachment and entry. These results show that the chronic encephalomyelitis virus utilizes sialylated integrins as cell surface receptors, leading to cellular tropism to evade pDC activation. TMEV binds to the open form αI‐domain containing integrins that undergo sialic acid (NeuAc) modifications on DCs. In contrast, because pDCs have reduced sialic acid modifications, integrins are not sialylated and TMEV evades recognition by pDCs.
doi_str_mv	10.1002/eji.202350452
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Although sialic acids have been shown to be essential for TMEV attachment to the host, the surface receptor has not been identified. While type I interferons play a pivotal role in the elimination of the chronic infectious Daniel (DA) strain, the role of plasmacytoid dendritic cells (pDCs) is controversial. We herein found that TMEV binds to conventional DCs but not to pDCs. A glycomics analysis showed that the sialylated N‐glycan fractions were lower in pDCs than in conventional DCs, indicating that pDCs are not susceptible to TMEV infection due to the low levels of sialic acid. TMEV capsid proteins contain an integrin recognition motif, and dot blot assays showed that the integrin proteins bind to TMEV and that the viral binding was reduced in the desialylated αXβ2. αXβ2 protein suppressed TMEV replication in vivo, and TMEV co‐localized with integrin αM at the cell membrane and TLR 3 in the cytoplasm, suggesting that αM serves as the viral attachment and entry. These results show that the chronic encephalomyelitis virus utilizes sialylated integrins as cell surface receptors, leading to cellular tropism to evade pDC activation. TMEV binds to the open form αI‐domain containing integrins that undergo sialic acid (NeuAc) modifications on DCs. 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Although sialic acids have been shown to be essential for TMEV attachment to the host, the surface receptor has not been identified. While type I interferons play a pivotal role in the elimination of the chronic infectious Daniel (DA) strain, the role of plasmacytoid dendritic cells (pDCs) is controversial. We herein found that TMEV binds to conventional DCs but not to pDCs. A glycomics analysis showed that the sialylated N‐glycan fractions were lower in pDCs than in conventional DCs, indicating that pDCs are not susceptible to TMEV infection due to the low levels of sialic acid. TMEV capsid proteins contain an integrin recognition motif, and dot blot assays showed that the integrin proteins bind to TMEV and that the viral binding was reduced in the desialylated αXβ2. αXβ2 protein suppressed TMEV replication in vivo, and TMEV co‐localized with integrin αM at the cell membrane and TLR 3 in the cytoplasm, suggesting that αM serves as the viral attachment and entry. These results show that the chronic encephalomyelitis virus utilizes sialylated integrins as cell surface receptors, leading to cellular tropism to evade pDC activation. TMEV binds to the open form αI‐domain containing integrins that undergo sialic acid (NeuAc) modifications on DCs. In contrast, because pDCs have reduced sialic acid modifications, integrins are not sialylated and TMEV evades recognition by pDCs.</description><subject>Cell membranes</subject><subject>Cell surface</subject><subject>Cell surface receptors</subject><subject>Cytoplasm</subject><subject>Demyelinating diseases</subject><subject>Demyelination</subject><subject>Dendritic cells</subject><subject>Encephalomyelitis</subject><subject>Integrin</subject><subject>Integrins</subject><subject>Multiple sclerosis</subject><subject>pDC</subject><subject>Sialic acid</subject><subject>Sialic acids</subject><subject>TMEV</subject><subject>Tropism</subject><subject>Virus attachment</subject><subject>Viruses</subject><issn>0014-2980</issn><issn>1521-4141</issn><fulltext>true</fulltext><rsrctype>article</rsrctype><creationdate>2023</creationdate><recordtype>article</recordtype><recordid>eNp9kTtvFDEURi0EIkugpEWWaGgm-DGeR4mWAEGRaKAeeezrrFee8eDrCcxf4FfjsCEFBXLh5ujcTzqEvOTsgjMm3sLRXwgmpGK1Eo_IjivBq5rX_DHZMcbrSvQdOyPPEI-Msb5R_VNyJlvVlFfvyK_9IcXZGwqzgeWgQ5w2CD57pLc-rUjh58GPPiM1EMIadKI5xcXjRPVsKdxqC0iX93uk40ZHP1s_39AcKXodtqAzWOrnDDfJz0g10nyAPyqKa3LaAE1QDueY8Dl54nRAeHH_n5NvHy6_7j9V118-Xu3fXVemZlJVinWt5a1oVGscs6OWTvWMSSu4Noa31jZdo51pjZEN9E5LcLWwrnN1I4zu5Tl5c_IuKX5fAfMwebybpGeIKw6iU0xyXqQFff0Peoxrmsu6QrVdz8sgXqjqRJkUERO4YUl-0mkbOBvuIg0l0vAQqfCv7q3rOIF9oP9WKYA4AT98gO3_tuHy85VSnZK_Abugntw</recordid><startdate>202310</startdate><enddate>202310</enddate><creator>Takeda, Kazuya</creator><creator>Kaifu, Tomonori</creator><creator>Michihata, Ryunosuke</creator><creator>Kinugawa, Naotaka</creator><creator>Fujioka, Atushi</creator><creator>Tateno, Ayaka</creator><creator>Toshima, Kaoru</creator><creator>Kanoh, Hirotaka</creator><creator>Inamori, Kei‐Ichiro</creator><creator>Kamijo, Keiju</creator><creator>Himeda, Toshiki</creator><creator>Ohara, Yoshiro</creator><creator>Inokuchi, Jin‐Ichi</creator><creator>Nakamura, Akira</creator><general>Wiley Subscription Services, Inc</general><scope>NPM</scope><scope>AAYXX</scope><scope>CITATION</scope><scope>7QP</scope><scope>7T5</scope><scope>7TK</scope><scope>7TM</scope><scope>8FD</scope><scope>FR3</scope><scope>H94</scope><scope>K9.</scope><scope>M7N</scope><scope>P64</scope><scope>RC3</scope><scope>7X8</scope><orcidid>https://orcid.org/0000-0003-3798-7964</orcidid></search><sort><creationdate>202310</creationdate><title>Chronic encephalomyelitis virus exhibits cellular tropism and evades pDCs by binding to sialylated integrins as the cell surface receptors</title><author>Takeda, Kazuya ; 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Although sialic acids have been shown to be essential for TMEV attachment to the host, the surface receptor has not been identified. While type I interferons play a pivotal role in the elimination of the chronic infectious Daniel (DA) strain, the role of plasmacytoid dendritic cells (pDCs) is controversial. We herein found that TMEV binds to conventional DCs but not to pDCs. A glycomics analysis showed that the sialylated N‐glycan fractions were lower in pDCs than in conventional DCs, indicating that pDCs are not susceptible to TMEV infection due to the low levels of sialic acid. TMEV capsid proteins contain an integrin recognition motif, and dot blot assays showed that the integrin proteins bind to TMEV and that the viral binding was reduced in the desialylated αXβ2. αXβ2 protein suppressed TMEV replication in vivo, and TMEV co‐localized with integrin αM at the cell membrane and TLR 3 in the cytoplasm, suggesting that αM serves as the viral attachment and entry. These results show that the chronic encephalomyelitis virus utilizes sialylated integrins as cell surface receptors, leading to cellular tropism to evade pDC activation. TMEV binds to the open form αI‐domain containing integrins that undergo sialic acid (NeuAc) modifications on DCs. In contrast, because pDCs have reduced sialic acid modifications, integrins are not sialylated and TMEV evades recognition by pDCs.</abstract><cop>Germany</cop><pub>Wiley Subscription Services, Inc</pub><pmid>37565654</pmid><doi>10.1002/eji.202350452</doi><tpages>14</tpages><orcidid>https://orcid.org/0000-0003-3798-7964</orcidid><oa>free_for_read</oa></addata></record>
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subjects	Cell membranes Cell surface Cell surface receptors Cytoplasm Demyelinating diseases Demyelination Dendritic cells Encephalomyelitis Integrin Integrins Multiple sclerosis pDC Sialic acid Sialic acids TMEV Tropism Virus attachment Viruses
title	Chronic encephalomyelitis virus exhibits cellular tropism and evades pDCs by binding to sialylated integrins as the cell surface receptors
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