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Nanoscale Colocalization of NK Cell Activating and Inhibitory Receptors Controls Signal Integration
by
Dyson, Julian
, Henriques, Ricardo
, Tomaz, David
, Pereira, Pedro Matos
, Gould, Keith
, Guerra, Nadia
in
Animals
/ Carrier Proteins - metabolism
/ CD4 antigen
/ Cell growth
/ Flow cytometry
/ Fluorescence resonance energy transfer
/ FRET
/ H-2 Antigens
/ Histocompatibility Antigen H-2D - metabolism
/ Hypotheses
/ Immunology
/ Integration
/ Killer Cells, Natural
/ Kinases
/ Lectins, C-Type - metabolism
/ Ligands
/ Ly49A
/ Major histocompatibility complex
/ Mice
/ nanoscale colocalization
/ Natural killer cells
/ NIH 3T3 Cells
/ NK Cell Lectin-Like Receptor Subfamily A - metabolism
/ NK Cell Lectin-Like Receptor Subfamily K - metabolism
/ NK cell receptors and ligands
/ NK cell signaling
/ NKG2 antigen
/ NKG2D
/ Phosphatase
/ Proteins
/ Receptors, Natural Killer Cell - metabolism
/ Receptors, NK Cell Lectin-Like - metabolism
2022
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Nanoscale Colocalization of NK Cell Activating and Inhibitory Receptors Controls Signal Integration
by
Dyson, Julian
, Henriques, Ricardo
, Tomaz, David
, Pereira, Pedro Matos
, Gould, Keith
, Guerra, Nadia
in
Animals
/ Carrier Proteins - metabolism
/ CD4 antigen
/ Cell growth
/ Flow cytometry
/ Fluorescence resonance energy transfer
/ FRET
/ H-2 Antigens
/ Histocompatibility Antigen H-2D - metabolism
/ Hypotheses
/ Immunology
/ Integration
/ Killer Cells, Natural
/ Kinases
/ Lectins, C-Type - metabolism
/ Ligands
/ Ly49A
/ Major histocompatibility complex
/ Mice
/ nanoscale colocalization
/ Natural killer cells
/ NIH 3T3 Cells
/ NK Cell Lectin-Like Receptor Subfamily A - metabolism
/ NK Cell Lectin-Like Receptor Subfamily K - metabolism
/ NK cell receptors and ligands
/ NK cell signaling
/ NKG2 antigen
/ NKG2D
/ Phosphatase
/ Proteins
/ Receptors, Natural Killer Cell - metabolism
/ Receptors, NK Cell Lectin-Like - metabolism
2022
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Nanoscale Colocalization of NK Cell Activating and Inhibitory Receptors Controls Signal Integration
by
Dyson, Julian
, Henriques, Ricardo
, Tomaz, David
, Pereira, Pedro Matos
, Gould, Keith
, Guerra, Nadia
in
Animals
/ Carrier Proteins - metabolism
/ CD4 antigen
/ Cell growth
/ Flow cytometry
/ Fluorescence resonance energy transfer
/ FRET
/ H-2 Antigens
/ Histocompatibility Antigen H-2D - metabolism
/ Hypotheses
/ Immunology
/ Integration
/ Killer Cells, Natural
/ Kinases
/ Lectins, C-Type - metabolism
/ Ligands
/ Ly49A
/ Major histocompatibility complex
/ Mice
/ nanoscale colocalization
/ Natural killer cells
/ NIH 3T3 Cells
/ NK Cell Lectin-Like Receptor Subfamily A - metabolism
/ NK Cell Lectin-Like Receptor Subfamily K - metabolism
/ NK cell receptors and ligands
/ NK cell signaling
/ NKG2 antigen
/ NKG2D
/ Phosphatase
/ Proteins
/ Receptors, Natural Killer Cell - metabolism
/ Receptors, NK Cell Lectin-Like - metabolism
2022
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Nanoscale Colocalization of NK Cell Activating and Inhibitory Receptors Controls Signal Integration
Journal Article
Nanoscale Colocalization of NK Cell Activating and Inhibitory Receptors Controls Signal Integration
2022
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Overview
Natural killer (NK) cell responses depend on the balance of signals from inhibitory and activating receptors. However, how the integration of antagonistic signals occurs upon NK cell–target cell interaction is not fully understood. Here we provide evidence that NK cell inhibition
via
the inhibitory receptor Ly49A is dependent on its relative colocalization at the nanometer scale with the activating receptor NKG2D upon immune synapse (IS) formation. NKG2D and Ly49A signal integration and colocalization were studied using NKG2D-GFP and Ly49A-RFP-expressing primary NK cells, forming ISs with NIH3T3 target cells, with or without the expression of single-chain trimer (SCT) H2-Dd and an extended form of SCT H2-Dd-CD4 MHC-I molecules. Nanoscale colocalization was assessed by Förster resonance energy transfer between NKG2D-GFP and Ly49A-RFP and measured for each synapse. In the presence of their respective cognate ligands, NKG2D and Ly49A colocalize at the nanometer scale, leading to NK cell inhibition. However, increasing the size of the Ly49A ligand reduced the nanoscale colocalization with NKG2D, consequently impairing Ly49A-mediated inhibition. Thus, our data shows that NK cell signal integration is critically dependent on the dimensions of NK cell ligand–receptor pairs by affecting their relative nanometer-scale colocalization at the IS. Our results together suggest that the balance of NK cell signals and NK cell responses is determined by the relative nanoscale colocalization of activating and inhibitory receptors in the immune synapse.
Publisher
Frontiers Media SA,Frontiers Media S.A
Subject
/ Carrier Proteins - metabolism
/ Fluorescence resonance energy transfer
/ FRET
/ Histocompatibility Antigen H-2D - metabolism
/ Kinases
/ Lectins, C-Type - metabolism
/ Ligands
/ Ly49A
/ Major histocompatibility complex
/ Mice
/ NK Cell Lectin-Like Receptor Subfamily A - metabolism
/ NK Cell Lectin-Like Receptor Subfamily K - metabolism
/ NK cell receptors and ligands
/ NKG2D
/ Proteins
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