NMDA receptors as a possible component of store-operated Ca^sup 2+^ entry in human T-lymphocytes

NMDA receptors as a possible component of store-operated Ca^sup 2+^ entry in human T-lymphocytes

Elevation of intracellular Ca^sup 2+^ in T-lymphocytes as a consequence of T cell antigen receptor activation triggers transcriptional programs resulting in effector cytokine secretion and immune response coordination. Increase of Ca^sup 2+^ concentration in T-lymphocytes follows both the Ins(1,4,5)...

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Veröffentlicht in:Biochemistry (Moscow) 2011-11, Vol.76 (11), p.1220
Hauptverfasser: Zainullina, L F, Yamidanov, R S, Vakhitov, V A, Vakhitova, Yu V
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Antigens
Biochemistry
Cytokines
Immune response
Immunology
Lymphocytes
Neurotransmitters
T cell receptors
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container_issue 11
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container_title Biochemistry (Moscow)
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creator Zainullina, L F
Yamidanov, R S
Vakhitov, V A
Vakhitova, Yu V
description Elevation of intracellular Ca^sup 2+^ in T-lymphocytes as a consequence of T cell antigen receptor activation triggers transcriptional programs resulting in effector cytokine secretion and immune response coordination. Increase of Ca^sup 2+^ concentration in T-lymphocytes follows both the Ins(1,4,5)P^sub 3^-dependent release from an intracellular store and subsequent influx from extracellular milieu. Flow cytometry and the fluorescent dye Fluo-4AM have been used to demonstrate that noncompetitive NMDA receptor antagonist (+)-MK801 inhibits Ca^sup 2+^ influx in T cells induced by thapsigargin. Combination of thapsigargin and (+)-MK801 with following incubation does not affect Ca^sup 2+^ mobilization from intracellular stores, while decreased Ca^sup 2+^ entry was observed. Overall data indicate that the ion channel blocker (+)-MK801 is able to inhibit the Ca^sup 2+^ influx and confirm our suggestion about involvement of NMDA receptor in the store-operated Ca^sup 2+^ entry mechanisms in human T-lymphocytes. To identify the signal transduction pathways associated with NMDA receptors in mitogen-stimulated T-lymphocytes, the cells were incubated with (+)-MK801, then activity of key phosphorylated protein kinases of MAP-activated (pERK1/2, pSAPK/JNK, p-p38), Ca^sup 2+^-dependent (pCaMKII), PI3/Akt-dependent (pGSK-3β), and PKC-activated (pPKC[theta]) pathways were detected. The data we obtained demonstrate that (+)-MK801 treatment leads to more prominent decrease in Ras-activated protein kinases pERK1/2 and Rac-activated proteins p-p38 and pSAPK/JNK, as compared to DAG-dependent pPKC[theta] and Ca^sup 2+^-dependent pCaMKII. These results show that NMDA receptors are mainly involved in regulation of Ras/Rac-dependent signaling in T-lymphocytes.[PUBLICATION ABSTRACT]
doi_str_mv 10.1134/S0006297911110034
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To identify the signal transduction pathways associated with NMDA receptors in mitogen-stimulated T-lymphocytes, the cells were incubated with (+)-MK801, then activity of key phosphorylated protein kinases of MAP-activated (pERK1/2, pSAPK/JNK, p-p38), Ca^sup 2+^-dependent (pCaMKII), PI3/Akt-dependent (pGSK-3β), and PKC-activated (pPKC[theta]) pathways were detected. The data we obtained demonstrate that (+)-MK801 treatment leads to more prominent decrease in Ras-activated protein kinases pERK1/2 and Rac-activated proteins p-p38 and pSAPK/JNK, as compared to DAG-dependent pPKC[theta] and Ca^sup 2+^-dependent pCaMKII. 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subjects Antigens
Biochemistry
Cytokines
Immune response
Immunology
Lymphocytes
Neurotransmitters
T cell receptors
title NMDA receptors as a possible component of store-operated Ca^sup 2+^ entry in human T-lymphocytes
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