Antigen-Engaged B Cells Undergo Chemotaxis toward the T Zone and Form Motile Conjugates with Helper T Cells

Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon microscopy of intact lymph nodes, we show that upon exposure to antigen, B cells migrate with directional preference toward the B-zone-T-zone boun...

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Vydáno v:PLoS biology Ročník 3; číslo 6; s. e150
Hlavní autoři: Okada, Takaharu, Miller, Mark J, Parker, Ian, Krummel, Matthew F, Neighbors, Margaret, Hartley, Suzanne B, O'Garra, Anne, Cahalan, Michael D, Cyster, Jason G
Médium: Journal Article
Jazyk:angličtina
Vydáno: United States Public Library of Science 01.06.2005
Public Library of Science (PLoS)
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ISSN:1545-7885, 1544-9173, 1545-7885
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Abstract Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon microscopy of intact lymph nodes, we show that upon exposure to antigen, B cells migrate with directional preference toward the B-zone-T-zone boundary in a CCR7-dependent manner, through a region that exhibits a CCR7-ligand gradient. Initially the B cells show reduced motility, but after 1 d, motility is increased to approximately 9 microm/min. Antigen-engaged B cells pair with antigen-specific helper T cells for 10 to more than 60 min, whereas non-antigen-specific interactions last less than 10 min. B cell-T cell conjugates are highly dynamic and migrate extensively, being led by B cells. B cells occasionally contact more than one T cell, whereas T cells are strictly monogamous in their interactions. These findings provide evidence of lymphocyte chemotaxis in vivo, and they begin to define the spatiotemporal cellular dynamics associated with T cell-dependent antibody responses.
AbstractList Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon microscopy of intact lymph nodes, we show that upon exposure to antigen, B cells migrate with directional preference toward the B-zone-T-zone boundary in a CCR7-dependent manner, through a region that exhibits a CCR7-ligand gradient. Initially the B cells show reduced motility, but after 1 d, motility is increased to approximately 9 μm/min. Antigen-engaged B cells pair with antigen-specific helper T cells for 10 to more than 60 min, whereas non-antigen-specific interactions last less than 10 min. B cell-T cell conjugates are highly dynamic and migrate extensively, being led by B cells. B cells occasionally contact more than one T cell, whereas T cells are strictly monogamous in their interactions. These findings provide evidence of lymphocyte chemotaxis in vivo, and they begin to define the spatiotemporal cellular dynamics associated with T cell-dependent antibody responses.
Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon microscopy of intact lymph nodes, we show that upon exposure to antigen, B cells migrate with directional preference toward the B-zone-T-zone boundary in a CCR7-dependent manner, through a region that exhibits a CCR7-ligand gradient. Initially the B cells show reduced motility, but after 1 d, motility is increased to approximately 9 microm/min. Antigen-engaged B cells pair with antigen-specific helper T cells for 10 to more than 60 min, whereas non-antigen-specific interactions last less than 10 min. B cell-T cell conjugates are highly dynamic and migrate extensively, being led by B cells. B cells occasionally contact more than one T cell, whereas T cells are strictly monogamous in their interactions. These findings provide evidence of lymphocyte chemotaxis in vivo, and they begin to define the spatiotemporal cellular dynamics associated with T cell-dependent antibody responses.Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon microscopy of intact lymph nodes, we show that upon exposure to antigen, B cells migrate with directional preference toward the B-zone-T-zone boundary in a CCR7-dependent manner, through a region that exhibits a CCR7-ligand gradient. Initially the B cells show reduced motility, but after 1 d, motility is increased to approximately 9 microm/min. Antigen-engaged B cells pair with antigen-specific helper T cells for 10 to more than 60 min, whereas non-antigen-specific interactions last less than 10 min. B cell-T cell conjugates are highly dynamic and migrate extensively, being led by B cells. B cells occasionally contact more than one T cell, whereas T cells are strictly monogamous in their interactions. These findings provide evidence of lymphocyte chemotaxis in vivo, and they begin to define the spatiotemporal cellular dynamics associated with T cell-dependent antibody responses.
Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon microscopy of intact lymph nodes, we show that upon exposure to antigen, B cells migrate with directional preference toward the B-zone-T-zone boundary in a CCR7-dependent manner, through a region that exhibits a CCR7-ligand gradient. Initially the B cells show reduced motility, but after 1 d, motility is increased to approximately 9 microm/min. Antigen-engaged B cells pair with antigen-specific helper T cells for 10 to more than 60 min, whereas non-antigen-specific interactions last less than 10 min. B cell-T cell conjugates are highly dynamic and migrate extensively, being led by B cells. B cells occasionally contact more than one T cell, whereas T cells are strictly monogamous in their interactions. These findings provide evidence of lymphocyte chemotaxis in vivo, and they begin to define the spatiotemporal cellular dynamics associated with T cell-dependent antibody responses.
Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon microscopy of intact lymph nodes, we show that upon exposure to antigen, B cells migrate with directional preference toward the B-zone-T-zone boundary in a CCR7-dependent manner, through a region that exhibits a CCR7-ligand gradient. Initially the B cells show reduced motility, but after 1 d, motility is increased to approximately 9 [mu]m/min. Antigen-engaged B cells pair with antigen-specific helper T cells for 10 to more than 60 min, whereas non-antigen-specific interactions last less than 10 min. B cell-T cell conjugates are highly dynamic and migrate extensively, being led by B cells. B cells occasionally contact more than one T cell, whereas T cells are strictly monogamous in their interactions. These findings provide evidence of lymphocyte chemotaxis in vivo, and they begin to define the spatiotemporal cellular dynamics associated with T cell-dependent antibody responses.
Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon microscopy of intact lymph nodes, we show that upon exposure to antigen, B cells migrate with directional preference toward the B-zone–T-zone boundary in a CCR7-dependent manner, through a region that exhibits a CCR7-ligand gradient. Initially the B cells show reduced motility, but after 1 d, motility is increased to approximately 9 μm/min. Antigen-engaged B cells pair with antigen-specific helper T cells for 10 to more than 60 min, whereas non-antigen-specific interactions last less than 10 min. B cell–T cell conjugates are highly dynamic and migrate extensively, being led by B cells. B cells occasionally contact more than one T cell, whereas T cells are strictly monogamous in their interactions. These findings provide evidence of lymphocyte chemotaxis in vivo, and they begin to define the spatiotemporal cellular dynamics associated with T cell–dependent antibody responses. Interactions between B and T cells in intact lymph nodes are monitored with two-photon laser scanning microscopy.
  Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon microscopy of intact lymph nodes, we show that upon exposure to antigen, B cells migrate with directional preference toward the B-zone-T-zone boundary in a CCR7-dependent manner, through a region that exhibits a CCR7-ligand gradient. Initially the B cells show reduced motility, but after 1 d, motility is increased to approximately 9 μm/min. Antigen-engaged B cells pair with antigen-specific helper T cells for 10 to more than 60 min, whereas non-antigen-specific interactions last less than 10 min. B cell-T cell conjugates are highly dynamic and migrate extensively, being led by B cells. B cells occasionally contact more than one T cell, whereas T cells are strictly monogamous in their interactions. These findings provide evidence of lymphocyte chemotaxis in vivo, and they begin to define the spatiotemporal cellular dynamics associated with T cell-dependent antibody responses.
Author Okada, Takaharu
Hartley, Suzanne B
Neighbors, Margaret
Miller, Mark J
O'Garra, Anne
Cahalan, Michael D
Cyster, Jason G
Parker, Ian
Krummel, Matthew F
AuthorAffiliation 1 Howard Hughes Medical Institute and Department of Microbiology and Immunology, University of California San Francisco, California United States of America
4 Department of Pathology, University of California San Francisco, California United States of America
5 Department of Immunobiology, DNAX Research Institute Palo Alto, California United States of America
University of Minnesota United States of America
3 Department of Neurobiology and Behavior, University of California Irvine, California United States of America
2 Department of Physiology and Biophysics, University of California Irvine, California United States of America
AuthorAffiliation_xml – name: 4 Department of Pathology, University of California San Francisco, California United States of America
– name: 5 Department of Immunobiology, DNAX Research Institute Palo Alto, California United States of America
– name: 3 Department of Neurobiology and Behavior, University of California Irvine, California United States of America
– name: 1 Howard Hughes Medical Institute and Department of Microbiology and Immunology, University of California San Francisco, California United States of America
– name: 2 Department of Physiology and Biophysics, University of California Irvine, California United States of America
– name: University of Minnesota United States of America
Author_xml – sequence: 1
  givenname: Takaharu
  surname: Okada
  fullname: Okada, Takaharu
– sequence: 2
  givenname: Mark J
  surname: Miller
  fullname: Miller, Mark J
– sequence: 3
  givenname: Ian
  surname: Parker
  fullname: Parker, Ian
– sequence: 4
  givenname: Matthew F
  surname: Krummel
  fullname: Krummel, Matthew F
– sequence: 5
  givenname: Margaret
  surname: Neighbors
  fullname: Neighbors, Margaret
– sequence: 6
  givenname: Suzanne B
  surname: Hartley
  fullname: Hartley, Suzanne B
– sequence: 7
  givenname: Anne
  surname: O'Garra
  fullname: O'Garra, Anne
– sequence: 8
  givenname: Michael D
  surname: Cahalan
  fullname: Cahalan, Michael D
– sequence: 9
  givenname: Jason G
  surname: Cyster
  fullname: Cyster, Jason G
BackLink https://www.ncbi.nlm.nih.gov/pubmed/15857154$$D View this record in MEDLINE/PubMed
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Copyright 2005 Okada et al. This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited. Citation: Okada T, Miller MJ, Parker I, Krummel MF, Neighbors M, et al. (2005) Antigen-Engaged B Cells Undergo Chemotaxis toward the T Zone and Form Motile Conjugates with Helper T Cells. PLoS Biol 3(6): e150. doi:10.1371/journal.pbio.0030150
Copyright: © 2005 Okada et al. 2005
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Keywords Chemotaxis, Leukocyte
Ovalbumin
Humans
Receptors, CCR7
B-Lymphocytes
Cell Communication
T-Lymphocytes, Helper-Inducer
Receptors, Chemokine
Language English
License This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
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Snippet Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon...
  Interactions between B and T cells are essential for most antibody responses, but the dynamics of these interactions are poorly understood. By two-photon...
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SubjectTerms B-Lymphocytes - immunology
Cell Communication - immunology
Chemotaxis, Leukocyte - immunology
Humans
Immune system
Immunology
Lymph nodes
Lymphocytes
Mus (Mouse)
Ovalbumin - immunology
Proteins
Receptors, CCR7
Receptors, Chemokine - immunology
T cell receptors
T-Lymphocytes, Helper-Inducer - immunology
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Title Antigen-Engaged B Cells Undergo Chemotaxis toward the T Zone and Form Motile Conjugates with Helper T Cells
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