T cell egress via lymphatic vessels is tuned by antigen encounter and limits tumor control
Antigen-specific CD8 + T cell accumulation in tumors is a prerequisite for effective immunotherapy, and yet the mechanisms of lymphocyte transit are not well defined. Here we show that tumor-associated lymphatic vessels control T cell exit from tumors via the chemokine CXCL12, and intratumoral antig...
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| Veröffentlicht in: | Nature immunology 2023-04, Vol.24 (4), p.664-675 |
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| creator | Steele, Maria M. Jaiswal, Abhinav Delclaux, Ines Dryg, Ian D. Murugan, Dhaarini Femel, Julia Son, Sunny du Bois, Haley Hill, Cameron Leachman, Sancy A. Chang, Young H. Coussens, Lisa M. Anandasabapathy, Niroshana Lund, Amanda W. |
| description | Antigen-specific CD8
+
T cell accumulation in tumors is a prerequisite for effective immunotherapy, and yet the mechanisms of lymphocyte transit are not well defined. Here we show that tumor-associated lymphatic vessels control T cell exit from tumors via the chemokine CXCL12, and intratumoral antigen encounter tunes CXCR4 expression by effector CD8
+
T cells. Only high-affinity antigen downregulates CXCR4 and upregulates the CXCL12 decoy receptor, ACKR3, thereby reducing CXCL12 sensitivity and promoting T cell retention. A diverse repertoire of functional tumor-specific CD8
+
T cells, therefore, exit the tumor, which limits the pool of CD8
+
T cells available to exert tumor control. CXCR4 inhibition or loss of lymphatic-specific CXCL12 boosts T cell retention and enhances tumor control. These data indicate that strategies to limit T cell egress might be an approach to boost the quantity and quality of intratumoral T cells and thereby response to immunotherapy.
Here, the authors show that CD8
+
T cells egress from tumors via lymphatic vessels in a CXCL12/CXCR4-dependent manner. High-affinity antigen encounter inhibits CXCR4 and increases retention, while no encounter or weak affinity directs T cell exit to limit local tumor control. |
| doi_str_mv | 10.1038/s41590-023-01443-y |
| format | Article |
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+
T cell accumulation in tumors is a prerequisite for effective immunotherapy, and yet the mechanisms of lymphocyte transit are not well defined. Here we show that tumor-associated lymphatic vessels control T cell exit from tumors via the chemokine CXCL12, and intratumoral antigen encounter tunes CXCR4 expression by effector CD8
+
T cells. Only high-affinity antigen downregulates CXCR4 and upregulates the CXCL12 decoy receptor, ACKR3, thereby reducing CXCL12 sensitivity and promoting T cell retention. A diverse repertoire of functional tumor-specific CD8
+
T cells, therefore, exit the tumor, which limits the pool of CD8
+
T cells available to exert tumor control. CXCR4 inhibition or loss of lymphatic-specific CXCL12 boosts T cell retention and enhances tumor control. These data indicate that strategies to limit T cell egress might be an approach to boost the quantity and quality of intratumoral T cells and thereby response to immunotherapy.
Here, the authors show that CD8
+
T cells egress from tumors via lymphatic vessels in a CXCL12/CXCR4-dependent manner. High-affinity antigen encounter inhibits CXCR4 and increases retention, while no encounter or weak affinity directs T cell exit to limit local tumor control.</description><identifier>ISSN: 1529-2908</identifier><identifier>EISSN: 1529-2916</identifier><identifier>DOI: 10.1038/s41590-023-01443-y</identifier><identifier>PMID: 36849745</identifier><language>eng</language><publisher>New York: Nature Publishing Group US</publisher><subject>631/250/1619/554/1834/1269 ; 631/250/251 ; 631/250/98 ; 631/67/580/1884 ; Affinity ; Antigens ; Biomedical and Life Sciences ; Biomedicine ; CD8 antigen ; CD8-Positive T-Lymphocytes ; Chemokines ; CXCL12 protein ; CXCR4 protein ; Effector cells ; Humans ; Immunology ; Immunotherapy ; Infectious Diseases ; Lymphatic system ; Lymphatic Vessels - metabolism ; Lymphocytes ; Lymphocytes T ; Neoplasms - pathology ; Neoplasms - therapy ; Receptors, CXCR4 - metabolism ; Retention ; Tumors</subject><ispartof>Nature immunology, 2023-04, Vol.24 (4), p.664-675</ispartof><rights>The Author(s), under exclusive licence to Springer Nature America, Inc. 2023. corrected publication 2023. Springer Nature or its licensor (e.g. a society or other partner) holds exclusive rights to this article under a publishing agreement with the author(s) or other rightsholder(s); author self-archiving of the accepted manuscript version of this article is solely governed by the terms of such publishing agreement and applicable law.</rights><rights>2023. The Author(s), under exclusive licence to Springer Nature America, Inc.</rights><lds50>peer_reviewed</lds50><woscitedreferencessubscribed>false</woscitedreferencessubscribed><citedby>FETCH-LOGICAL-c375t-7ba02ffee62d2ef6f806992fb188382ecefbd03263a1b7e5cca64389ca9492ae3</citedby><cites>FETCH-LOGICAL-c375t-7ba02ffee62d2ef6f806992fb188382ecefbd03263a1b7e5cca64389ca9492ae3</cites><orcidid>0000-0002-0254-316X ; 0000-0003-2389-1865 ; 0000-0001-7389-9983 ; 0000-0001-8764-1959</orcidid></display><links><openurl>$$Topenurl_article</openurl><openurlfulltext>$$Topenurlfull_article</openurlfulltext><thumbnail>$$Tsyndetics_thumb_exl</thumbnail><linktopdf>$$Uhttps://link.springer.com/content/pdf/10.1038/s41590-023-01443-y$$EPDF$$P50$$Gspringer$$H</linktopdf><linktohtml>$$Uhttps://link.springer.com/10.1038/s41590-023-01443-y$$EHTML$$P50$$Gspringer$$H</linktohtml><link.rule.ids>314,780,784,27922,27923,41486,42555,51317</link.rule.ids><backlink>$$Uhttps://www.ncbi.nlm.nih.gov/pubmed/36849745$$D View this record in MEDLINE/PubMed$$Hfree_for_read</backlink></links><search><creatorcontrib>Steele, Maria M.</creatorcontrib><creatorcontrib>Jaiswal, Abhinav</creatorcontrib><creatorcontrib>Delclaux, Ines</creatorcontrib><creatorcontrib>Dryg, Ian D.</creatorcontrib><creatorcontrib>Murugan, Dhaarini</creatorcontrib><creatorcontrib>Femel, Julia</creatorcontrib><creatorcontrib>Son, Sunny</creatorcontrib><creatorcontrib>du Bois, Haley</creatorcontrib><creatorcontrib>Hill, Cameron</creatorcontrib><creatorcontrib>Leachman, Sancy A.</creatorcontrib><creatorcontrib>Chang, Young H.</creatorcontrib><creatorcontrib>Coussens, Lisa M.</creatorcontrib><creatorcontrib>Anandasabapathy, Niroshana</creatorcontrib><creatorcontrib>Lund, Amanda W.</creatorcontrib><title>T cell egress via lymphatic vessels is tuned by antigen encounter and limits tumor control</title><title>Nature immunology</title><addtitle>Nat Immunol</addtitle><addtitle>Nat Immunol</addtitle><description>Antigen-specific CD8
+
T cell accumulation in tumors is a prerequisite for effective immunotherapy, and yet the mechanisms of lymphocyte transit are not well defined. Here we show that tumor-associated lymphatic vessels control T cell exit from tumors via the chemokine CXCL12, and intratumoral antigen encounter tunes CXCR4 expression by effector CD8
+
T cells. Only high-affinity antigen downregulates CXCR4 and upregulates the CXCL12 decoy receptor, ACKR3, thereby reducing CXCL12 sensitivity and promoting T cell retention. A diverse repertoire of functional tumor-specific CD8
+
T cells, therefore, exit the tumor, which limits the pool of CD8
+
T cells available to exert tumor control. CXCR4 inhibition or loss of lymphatic-specific CXCL12 boosts T cell retention and enhances tumor control. These data indicate that strategies to limit T cell egress might be an approach to boost the quantity and quality of intratumoral T cells and thereby response to immunotherapy.
Here, the authors show that CD8
+
T cells egress from tumors via lymphatic vessels in a CXCL12/CXCR4-dependent manner. High-affinity antigen encounter inhibits CXCR4 and increases retention, while no encounter or weak affinity directs T cell exit to limit local tumor control.</description><subject>631/250/1619/554/1834/1269</subject><subject>631/250/251</subject><subject>631/250/98</subject><subject>631/67/580/1884</subject><subject>Affinity</subject><subject>Antigens</subject><subject>Biomedical and Life Sciences</subject><subject>Biomedicine</subject><subject>CD8 antigen</subject><subject>CD8-Positive T-Lymphocytes</subject><subject>Chemokines</subject><subject>CXCL12 protein</subject><subject>CXCR4 protein</subject><subject>Effector cells</subject><subject>Humans</subject><subject>Immunology</subject><subject>Immunotherapy</subject><subject>Infectious Diseases</subject><subject>Lymphatic system</subject><subject>Lymphatic Vessels - metabolism</subject><subject>Lymphocytes</subject><subject>Lymphocytes T</subject><subject>Neoplasms - pathology</subject><subject>Neoplasms - therapy</subject><subject>Receptors, CXCR4 - 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metabolism</topic><topic>Lymphocytes</topic><topic>Lymphocytes T</topic><topic>Neoplasms - pathology</topic><topic>Neoplasms - therapy</topic><topic>Receptors, CXCR4 - metabolism</topic><topic>Retention</topic><topic>Tumors</topic><toplevel>peer_reviewed</toplevel><toplevel>online_resources</toplevel><creatorcontrib>Steele, Maria M.</creatorcontrib><creatorcontrib>Jaiswal, Abhinav</creatorcontrib><creatorcontrib>Delclaux, Ines</creatorcontrib><creatorcontrib>Dryg, Ian D.</creatorcontrib><creatorcontrib>Murugan, Dhaarini</creatorcontrib><creatorcontrib>Femel, Julia</creatorcontrib><creatorcontrib>Son, Sunny</creatorcontrib><creatorcontrib>du Bois, Haley</creatorcontrib><creatorcontrib>Hill, Cameron</creatorcontrib><creatorcontrib>Leachman, Sancy A.</creatorcontrib><creatorcontrib>Chang, Young H.</creatorcontrib><creatorcontrib>Coussens, Lisa M.</creatorcontrib><creatorcontrib>Anandasabapathy, Niroshana</creatorcontrib><creatorcontrib>Lund, Amanda W.</creatorcontrib><collection>Medline</collection><collection>MEDLINE</collection><collection>MEDLINE (Ovid)</collection><collection>MEDLINE</collection><collection>MEDLINE</collection><collection>PubMed</collection><collection>CrossRef</collection><collection>ProQuest Central (Corporate)</collection><collection>Calcium & Calcified Tissue Abstracts</collection><collection>Chemoreception Abstracts</collection><collection>Immunology Abstracts</collection><collection>Neurosciences Abstracts</collection><collection>Nucleic Acids Abstracts</collection><collection>Virology and AIDS Abstracts</collection><collection>Health & Medical Collection</collection><collection>ProQuest Central (purchase pre-March 2016)</collection><collection>Medical Database (Alumni Edition)</collection><collection>ProQuest Pharma Collection</collection><collection>Public Health Database</collection><collection>Technology Research Database</collection><collection>ProQuest SciTech Collection</collection><collection>ProQuest Natural Science Collection</collection><collection>Hospital Premium Collection</collection><collection>Hospital Premium Collection (Alumni Edition)</collection><collection>ProQuest Central (Alumni) (purchase pre-March 2016)</collection><collection>ProQuest Central (Alumni Edition)</collection><collection>ProQuest One Sustainability</collection><collection>ProQuest Central UK/Ireland</collection><collection>ProQuest Central Essentials</collection><collection>Biological Science Collection</collection><collection>ProQuest Central</collection><collection>Natural Science Collection (ProQuest)</collection><collection>ProQuest One Community College</collection><collection>ProQuest Central Korea</collection><collection>Engineering Research Database</collection><collection>Health Research Premium Collection</collection><collection>Health Research Premium Collection (Alumni)</collection><collection>ProQuest Central Student</collection><collection>AIDS and Cancer Research Abstracts</collection><collection>SciTech Premium Collection</collection><collection>ProQuest Health & Medical Complete (Alumni)</collection><collection>ProQuest Biological Science Collection</collection><collection>Health & Medical Collection (Alumni Edition)</collection><collection>Medical Database</collection><collection>Algology Mycology and Protozoology Abstracts (Microbiology C)</collection><collection>Biological Science Database</collection><collection>Biotechnology and BioEngineering Abstracts</collection><collection>ProQuest One Academic Eastern Edition (DO NOT USE)</collection><collection>ProQuest One Academic</collection><collection>ProQuest One Academic UKI Edition</collection><collection>Genetics Abstracts</collection><collection>MEDLINE - Academic</collection><jtitle>Nature immunology</jtitle></facets><delivery><delcategory>Remote Search Resource</delcategory><fulltext>fulltext</fulltext></delivery><addata><au>Steele, Maria M.</au><au>Jaiswal, Abhinav</au><au>Delclaux, Ines</au><au>Dryg, Ian D.</au><au>Murugan, Dhaarini</au><au>Femel, Julia</au><au>Son, Sunny</au><au>du Bois, Haley</au><au>Hill, Cameron</au><au>Leachman, Sancy A.</au><au>Chang, Young H.</au><au>Coussens, Lisa M.</au><au>Anandasabapathy, Niroshana</au><au>Lund, Amanda W.</au><format>journal</format><genre>article</genre><ristype>JOUR</ristype><atitle>T cell egress via lymphatic vessels is tuned by antigen encounter and limits tumor control</atitle><jtitle>Nature immunology</jtitle><stitle>Nat Immunol</stitle><addtitle>Nat Immunol</addtitle><date>2023-04-01</date><risdate>2023</risdate><volume>24</volume><issue>4</issue><spage>664</spage><epage>675</epage><pages>664-675</pages><issn>1529-2908</issn><eissn>1529-2916</eissn><abstract>Antigen-specific CD8
+
T cell accumulation in tumors is a prerequisite for effective immunotherapy, and yet the mechanisms of lymphocyte transit are not well defined. Here we show that tumor-associated lymphatic vessels control T cell exit from tumors via the chemokine CXCL12, and intratumoral antigen encounter tunes CXCR4 expression by effector CD8
+
T cells. Only high-affinity antigen downregulates CXCR4 and upregulates the CXCL12 decoy receptor, ACKR3, thereby reducing CXCL12 sensitivity and promoting T cell retention. A diverse repertoire of functional tumor-specific CD8
+
T cells, therefore, exit the tumor, which limits the pool of CD8
+
T cells available to exert tumor control. CXCR4 inhibition or loss of lymphatic-specific CXCL12 boosts T cell retention and enhances tumor control. These data indicate that strategies to limit T cell egress might be an approach to boost the quantity and quality of intratumoral T cells and thereby response to immunotherapy.
Here, the authors show that CD8
+
T cells egress from tumors via lymphatic vessels in a CXCL12/CXCR4-dependent manner. High-affinity antigen encounter inhibits CXCR4 and increases retention, while no encounter or weak affinity directs T cell exit to limit local tumor control.</abstract><cop>New York</cop><pub>Nature Publishing Group US</pub><pmid>36849745</pmid><doi>10.1038/s41590-023-01443-y</doi><tpages>12</tpages><orcidid>https://orcid.org/0000-0002-0254-316X</orcidid><orcidid>https://orcid.org/0000-0003-2389-1865</orcidid><orcidid>https://orcid.org/0000-0001-7389-9983</orcidid><orcidid>https://orcid.org/0000-0001-8764-1959</orcidid></addata></record> |
| fulltext | fulltext |
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| ispartof | Nature immunology, 2023-04, Vol.24 (4), p.664-675 |
| issn | 1529-2908 1529-2916 |
| language | eng |
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| source | MEDLINE; Nature; SpringerLink Journals - AutoHoldings |
| subjects | 631/250/1619/554/1834/1269 631/250/251 631/250/98 631/67/580/1884 Affinity Antigens Biomedical and Life Sciences Biomedicine CD8 antigen CD8-Positive T-Lymphocytes Chemokines CXCL12 protein CXCR4 protein Effector cells Humans Immunology Immunotherapy Infectious Diseases Lymphatic system Lymphatic Vessels - metabolism Lymphocytes Lymphocytes T Neoplasms - pathology Neoplasms - therapy Receptors, CXCR4 - metabolism Retention Tumors |
| title | T cell egress via lymphatic vessels is tuned by antigen encounter and limits tumor control |
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