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Query: EC:3.1.4.3 (
phospholipase C
)
18,461
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Adaptor proteins have important functions in coupling stimulation through immunoreceptors with downstream events. The adaptor linker for activation of B cells (LAB)/
non-T cell activation linker
(
NTAL
) is expressed in various immune cell types and has a similar domain structure as linker for activation of T cells (LAT). In this study we generated a LAB transgenic mouse to compare the functional differences between LAB and LAT. A LAB transgene expressed in LAT-deficient T cells was able to restore T cell development. However, these mice developed severe organomegaly with disorganized lymphoid tissues. Lymphocytes from these transgenic mice were hyperactivated, and T cells produced large amounts of type II cytokines. In addition, these activities appeared to be uncoupled from the TCR. An examination of the signaling capabilities of these T cells revealed that LAB resembled a LAT molecule unable to bind
phospholipase C
-gamma1.
...
PMID:Linker for activation of B cells: a functional equivalent of a mutant linker for activation of T cells deficient in phospholipase C-gamma1 binding. 1515 99
Engagement of the Fcepsilon receptor I (FcepsilonRI) on mast cells and basophils initiates signaling pathways leading to degranulation. Early activation events include tyrosine phosphorylation of two transmembrane adaptor proteins, linker for activation of T cells (LAT) and
non-T cell activation linker
(
NTAL
; also called LAB; a product of Wbscr5 gene). Previous studies showed that the secretory response was partially inhibited in bone marrow-derived mast cells (BMMCs) from LAT-deficient mice. To clarify the role of
NTAL
in mast cell degranulation, we compared FcepsilonRI-mediated signaling events in BMMCs from
NTAL
-deficient and wild-type mice. Although
NTAL
is structurally similar to LAT, antigen-mediated degranulation responses were unexpectedly increased in
NTAL
-deficient mast cells. The earliest event affected was enhanced tyrosine phosphorylation of LAT in antigen-activated cells. This was accompanied by enhanced tyrosine phosphorylation and enzymatic activity of
phospholipase C
gamma1 and
phospholipase C
gamma2, resulting in elevated levels of inositol 1,4,5-trisphosphate and free intracellular Ca2+.
NTAL
-deficient BMMCs also exhibited an enhanced activity of phosphatidylinositol 3-OH kinase and Src homology 2 domain-containing protein tyrosine phosphatase-2. Although both LAT and
NTAL
are considered to be localized in membrane rafts, immunogold electron microscopy on isolated membrane sheets demonstrated their independent clustering. The combined data show that
NTAL
is functionally and topographically different from LAT.
...
PMID:Negative regulation of mast cell signaling and function by the adaptor LAB/NTAL. 1547 48
SLP-65 and the linker for activation of T cells (LAT) are central adaptor proteins that link the activated pre-BCR to downstream events in pre-B cells. Recently, a new transmembrane adaptor called
NTAL
/LAB/LAT2 (hereafter called
NTAL
for
non-T cell activation linker
) with striking functional and structural similarity to LAT has been identified in B cells. In this study, we compare the function of
NTAL
and LAT in pre-BCR signaling and show that, in contrast to LAT,
NTAL
does not induce pre-BCR down-regulation, calcium flux, or pre-B cell differentiation. To test whether differences between
NTAL
-mediated and LAT-mediated signaling are caused by the missing
phospholipase C
(
PLC
)-gamma binding motif in
NTAL
, we inserted the
PLC
-gamma1/2 binding motif of LAT into
NTAL
. This insertion rendered
NTAL
capable of activating pre-BCR down-regulation and calcium flux. Unexpectedly however, the ability of
NTAL
to induce calcium flux was not sufficient to promote pre-B cell differentiation, suggesting that the
PLC
-gamma binding motif has only partial effects on
NTAL
-mediated pre-BCR signaling. By generating chimeric swap mutants, we identified the N terminus of
NTAL
as an inhibitory domain that prevents pre-B cell differentiation while allowing pre-BCR down-regulation and receptor-mediated calcium flux. Our data suggest that, in addition to the missing
PLC
-gamma1/2 binding motif, the N terminus is responsible for the functional differences between
NTAL
and LAT in pre-B cells.
...
PMID:The N terminus of the non-T cell activation linker (NTAL) confers inhibitory effects on pre-B cell differentiation. 1727 39
