Slp1 and Slp2-a Localize to the Plasma Membrane of CTL and Contribute to Secretion from the Immunological Synapse

Rab27a is required for polarized secretion of lysosomes from cytotoxic T lymphocytes (CTLs) at the immunological synapse. A series of Rab27a-interacting proteins have been identified; however, only Munc13-4 has been found to be expressed in CTL. In this study, we screened for expression of the synap...

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Autores principales: Holt, Oliver, Kanno, Eiko, Bossi, Giovanna, Booth, Sarah, Daniele, Tiziana, Santoro, Alessandra, Arico, Maurizio, Saegusa, Chika, Fukuda, Mitsunori, Griffiths, Gillian M
Formato: Texto
Lenguaje:English
Publicado: Blackwell Publishing Ltd 2008
Materias:
Original Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2329822/
https://www.ncbi.nlm.nih.gov/pubmed/18266782
http://dx.doi.org/10.1111/j.1600-0854.2008.00714.x
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author Holt, Oliver
Kanno, Eiko
Bossi, Giovanna
Booth, Sarah
Daniele, Tiziana
Santoro, Alessandra
Arico, Maurizio
Saegusa, Chika
Fukuda, Mitsunori
Griffiths, Gillian M
author_facet Holt, Oliver
Kanno, Eiko
Bossi, Giovanna
Booth, Sarah
Daniele, Tiziana
Santoro, Alessandra
Arico, Maurizio
Saegusa, Chika
Fukuda, Mitsunori
Griffiths, Gillian M
author_sort Holt, Oliver
collection PubMed
description Rab27a is required for polarized secretion of lysosomes from cytotoxic T lymphocytes (CTLs) at the immunological synapse. A series of Rab27a-interacting proteins have been identified; however, only Munc13-4 has been found to be expressed in CTL. In this study, we screened for expression of the synaptotagmin-like proteins (Slps): Slp1/JFC1, Slp2-a/exophilin4, Slp3-a, Slp4/granuphilin, Slp5 and rabphilin in CTL. We found that both Slp1 and Slp2-a are expressed in CTL. Isoforms of Slp2-a in CTL showed variation of the linker region but conserved the C2A and C2B and Slp homology (SHD) domains. Both Slp1 and Slp2-a interact with Rab27a in CTL, and Slp2-a, but not Slp1, is rapidly degraded when Rab27a is absent. Slp2-a contains PEST-like sequences within its linker region, which render it susceptible to degradation. Both Slp1 and Slp2-a localize predominantly to the plasma membrane of both human and mouse CTLs, and we show that Slp2-a can focus tightly at the immunological synapse formed with a target cell. Individual knockouts of either Slp2-a or Slp1 fail to impair CTL-mediated killing of targets; however, overexpression of a dominant-negative construct consisting of the SHD of Slp2-a, which is 56% identical to that of Slp1, reduces target cell death, suggesting that both Slp1 and Slp2-a contribute to secretory lysosome exocytosis from CTL. These results suggest that both Slp1 and Slp2-a may form part of a docking complex, capturing secretory lysosomes at the immunological synapse.
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spelling pubmed-23298222008-04-30 Slp1 and Slp2-a Localize to the Plasma Membrane of CTL and Contribute to Secretion from the Immunological Synapse Holt, Oliver Kanno, Eiko Bossi, Giovanna Booth, Sarah Daniele, Tiziana Santoro, Alessandra Arico, Maurizio Saegusa, Chika Fukuda, Mitsunori Griffiths, Gillian M Traffic Original Articles Rab27a is required for polarized secretion of lysosomes from cytotoxic T lymphocytes (CTLs) at the immunological synapse. A series of Rab27a-interacting proteins have been identified; however, only Munc13-4 has been found to be expressed in CTL. In this study, we screened for expression of the synaptotagmin-like proteins (Slps): Slp1/JFC1, Slp2-a/exophilin4, Slp3-a, Slp4/granuphilin, Slp5 and rabphilin in CTL. We found that both Slp1 and Slp2-a are expressed in CTL. Isoforms of Slp2-a in CTL showed variation of the linker region but conserved the C2A and C2B and Slp homology (SHD) domains. Both Slp1 and Slp2-a interact with Rab27a in CTL, and Slp2-a, but not Slp1, is rapidly degraded when Rab27a is absent. Slp2-a contains PEST-like sequences within its linker region, which render it susceptible to degradation. Both Slp1 and Slp2-a localize predominantly to the plasma membrane of both human and mouse CTLs, and we show that Slp2-a can focus tightly at the immunological synapse formed with a target cell. Individual knockouts of either Slp2-a or Slp1 fail to impair CTL-mediated killing of targets; however, overexpression of a dominant-negative construct consisting of the SHD of Slp2-a, which is 56% identical to that of Slp1, reduces target cell death, suggesting that both Slp1 and Slp2-a contribute to secretory lysosome exocytosis from CTL. These results suggest that both Slp1 and Slp2-a may form part of a docking complex, capturing secretory lysosomes at the immunological synapse. Blackwell Publishing Ltd 2008-04-01 2008-02-11 /pmc/articles/PMC2329822/ /pubmed/18266782 http://dx.doi.org/10.1111/j.1600-0854.2008.00714.x Text en © 2008 The Authors Journal compilation © 2008 Blackwell Publishing Ltd https://creativecommons.org/licenses/by/2.5/ Re-use of this article is permitted in accordance with the Creative Commons Deed, Attribution 2.5, which does not permit commercial exploitation.
spellingShingle Original Articles
Holt, Oliver
Kanno, Eiko
Bossi, Giovanna
Booth, Sarah
Daniele, Tiziana
Santoro, Alessandra
Arico, Maurizio
Saegusa, Chika
Fukuda, Mitsunori
Griffiths, Gillian M
Slp1 and Slp2-a Localize to the Plasma Membrane of CTL and Contribute to Secretion from the Immunological Synapse
title Slp1 and Slp2-a Localize to the Plasma Membrane of CTL and Contribute to Secretion from the Immunological Synapse
title_full Slp1 and Slp2-a Localize to the Plasma Membrane of CTL and Contribute to Secretion from the Immunological Synapse
title_fullStr Slp1 and Slp2-a Localize to the Plasma Membrane of CTL and Contribute to Secretion from the Immunological Synapse
title_full_unstemmed Slp1 and Slp2-a Localize to the Plasma Membrane of CTL and Contribute to Secretion from the Immunological Synapse
title_short Slp1 and Slp2-a Localize to the Plasma Membrane of CTL and Contribute to Secretion from the Immunological Synapse
title_sort slp1 and slp2-a localize to the plasma membrane of ctl and contribute to secretion from the immunological synapse
topic Original Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2329822/
https://www.ncbi.nlm.nih.gov/pubmed/18266782
http://dx.doi.org/10.1111/j.1600-0854.2008.00714.x
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