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Query: UNIPROT:Q00604 (
X-linked
)
16,883
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Bruton's tyrosine kinase
(
Btk
) is required for normal B cell development and signal transduction through cell surface molecules, and its defects lead to
X-linked
immune deficiency in mice and X-linked agammaglobulinemia in humans. In this report, we will describe the identification and characterization of a molecule, BAM11, which binds to the pleckstrin homology domain of
Btk
. A sequence homology search revealed that BAM11 has 89% homology, at the amino acid level, to human LTG19/ENL, that was originally identified as one of the fusion partners involved in chromosomal translocations of 11q23, MLL/ALL-1/HRX, in leukemia cells. Deletion mutants demonstrated that the region of BAM11 required for binding to
Btk
was localized between amino acid residues 240 and 256. Forced expression of a truncated form of BAM11 (amino acids 246-368) inhibited IL-5-induced proliferation by 50%, whereas forced expression of full-length BAM11 in Y16 cells did not affect the IL-5 responsiveness. We have also shown that BAM11 (amino acids 246-368) inhibited the kinase activity of
Btk
. These results suggest that the binding of BAM11 to
Btk
plays a regulatory role in the
Btk
signal transduction pathway. A cell fractionation study and analysis using EGFP-fused
Btk
protein demonstrated that a proportion of
Btk
is present within the nucleus.
...
PMID:Identification and characterization of a molecule, BAM11, that associates with the pleckstrin homology domain of mouse Btk. 1100 57
Mutations in the gene encoding
Bruton's tyrosine kinase
(
BTK
) interfere with B cell proliferation and lead to an
X-linked
immunodeficiency in mice characterized by reduced B cell numbers. Recent studies have established that
BTK
transmits signals from the B cell antigen receptor (BCR) to transcription factor NF-kappaB, which in turn reprograms a set of genes required for normal B cell growth. We now demonstrate that induction of NF-kappaB via this pathway requires the intermediate action of the -gamma2 isoform of phospholipase C (PLC-gamma2), a potential phosphorylation substrate of
BTK
. Specifically, pharmacologic agents that block the action of either PLC-gamma2 or its second messengers prevent BCR-induced activation of IkappaB kinase. Moreover, activation of NF-kappaB in response to BCR signaling is completely abolished in B cells deficient for PLC-gamma2. Taken together, these findings strongly suggest that PLC-gamma2 functions as an integral component of the
BTK
/NF-kappaB axis following BCR ligation. Interference with this NF-kappaB cascade may account for some of the B cell defects reported for plc-gamma2(-/-) mice, which develop an
X-linked
immunodeficiency-like phenotype.
...
PMID:Phospholipase C-gamma 2 couples Bruton's tyrosine kinase to the NF-kappaB signaling pathway in B lymphocytes. 1104 93
The cytoplasmic protein tyrosine kinase Tec has been proposed to have important functions in hematopoiesis and lymphocyte signal transduction. Here we show that Tec-deficient mice developed normally and had no major phenotypic alterations of the immune system. To reveal potential compensatory roles of other Tec kinases such as
Bruton's tyrosine kinase
(
Btk
), Tec/
Btk
double-deficient mice were generated. These mice exhibited a block at the B220(+)CD43(+) stage of B cell development and displayed a severe reduction of peripheral B cell numbers, particularly immunoglobulin (Ig)M(lo)IgD(hi) B cells. Although Tec/
Btk
(null) mice were able to form germinal centers, the response to T cell-dependent antigens was impaired. Thus, Tec and
Btk
together have an important role both during B cell development and in the generation and/or function of the peripheral B cell pool. The ability of Tec to compensate for
Btk
may also explain phenotypic differences in
X-linked
immunodeficiency (xid) mice compared with human X-linked agammaglobulinemia (XLA) patients.
...
PMID:Severe B cell deficiency in mice lacking the tec kinase family members Tec and Btk. 1110 3
Binding of the transcription factor Bright to Ig heavy chain loci after B cell activation is associated with increased heavy chain transcription. We now report that Bright coprecipitates with
Bruton's tyrosine kinase
(
Btk
), the defective enzyme in
X-linked
immunodeficiency disease (xid). Furthermore, we observed
Btk
in the nucleus of activated murine B cells, and mobility shift assays suggest that it is a component of the Bright DNA-binding complex. While BRIGHT protein was synthesized in activated spleen cells from xid mice, it did not bind DNA or associate stably with
Btk
. These data suggest that deficiencies in BRIGHT DNA-binding activity may contribute to the defects in Ig production seen in xid mice.
...
PMID:The transcription factor Bright associates with Bruton's tyrosine kinase, the defective protein in immunodeficiency disease. 1112 Aug 22
X-linked
immunodeficient (Xid) mice carry a
Bruton's tyrosine kinase
(
Btk
) mutation and exhibit a selective failure to produce antibodies against bacterial capsular polysaccharides. Studies in vitro point to a fundamental survival defect of Xid B cells after receptor cross-linking by thymus-independent type-2 (TI-2) antigen because B cells undergo apoptosis without proliferating. We describe results from a novel model, which we have used to investigate the impact of the Xid mutation on migration, proliferation and differentiation of B cells after polysaccharide immunization in vivo. Immunoglobulin knock-in mice, in which a large proportion of B cells express transgene-encoded receptors specific for (4-hydroxy-3-nitrophenyl)-acetyl (NP), were crossed with CBA/N mice. The male progeny contain NP-specific Xid B cells, while the female progeny contain NP-specific B cells with normal
Btk
. After immunization with the TI-2 antigen NP-Ficoll, NP-specific Xid B cells migrate to the T zones and proliferate. Despite transient up-regulation of blimp-1 and survival beyond the time when terminal differentiation is normally underway,
Btk
-defective B cells fail to differentiate to plasmablasts or germinal center cells. CD40 ligation partially restores their ability to form plasma cells in response to TI-2 antigen.
...
PMID:Tracking the response of Xid B cells in vivo: TI-2 antigen induces migration and proliferation but Btk is essential for terminal differentiation. 1146 91
Bruton's tyrosine kinase
(
Btk
) is required for human and mouse B cell development.
Btk
deficiency causes X-linked agammaglobulinemia (XLA) in humans and
X-linked
immunodeficiency in mice. Unlike Src proteins,
Btk
lacks a negative regulatory domain at the COOH terminus and may rely on cytoplasmic
Btk
-binding proteins to regulates its kinase activity by trans-inhibitor mechanisms. Consistent with this possibility, IBtk, which we identified as an inhibitor of
Btk
, bound to the PH domain of
Btk
. IBtk downregulated
Btk
kinase activity,
Btk
-mediated calcium mobilization and nuclear factor-kappaB-driven transcription. These results define a potential mechanism for the regulation of
Btk
function in B cells.
...
PMID:Direct inhibition of Bruton's tyrosine kinase by IBtk, a Btk-binding protein. 1157 40
Bright, or B cell regulator of immunoglobulin heavy chain transcription, is a B lymphocyte-specific protein first discovered for its ability to increase immunoglobulin transcription three- to sevenfold in antigen-activated B cells. It interacts with DNA through an ARID, or A/T-rich interaction domain, and is the only member of a previously undescribed family of DNA-binding proteins for which target genes have been identified. The mechanism(s) by which Bright facilitates transcription are unknown. Several proteins that associate with Bright may shed light upon its function. These include the nuclear matrix proteins sp100 and LYSp100B, and suggest that Bright may affect chromatin configuration and nuclear sublocalization. Furthermore,
Bruton's tyrosine kinase
is required for Bright binding activity, suggesting links between Bright, cell signaling cascades, and
X-linked
immunodeficiency disease.
...
PMID:The transcription factor, Bright, and immunoglobulin heavy chain expression. 1159 53
Mutations in
Bruton's tyrosine kinase
(
Btk
) result in X-linked agammaglobulinemia (XLA) in humans and
X-linked
immunodeficiency (xid) in mice. While targeted disruption of the protein kinase C-beta (PKCbeta) gene in mice results in an immunodeficiency similar to xid, the overall tyrosine phosphorylation of
Btk
is significantly enhanced in PKCbeta-deficient B cells. We provide direct evidence that PKCbeta acts as a feedback loop inhibitor of
Btk
activation. Inhibition of PKCbeta results in a dramatic increase in B-cell receptor (BCR)-mediated Ca2+ signaling. We identified a highly conserved PKCbeta serine phosphorylation site in a short linker within the Tec homology domain of
Btk
. Mutation of this phosphorylation site led to enhanced tyrosine phosphorylation and membrane association of
Btk
, and augmented BCR and FcepsilonRI-mediated signaling in B and mast cells, respectively. These findings provide a novel mechanism whereby reversible translocation of
Btk
/Tec kinases regulates the threshold for immunoreceptor signaling and thereby modulates lymphocyte activation.
...
PMID:PKCbeta modulates antigen receptor signaling via regulation of Btk membrane localization. 1159 12
Human X-linked agammaglobulinemia (XLA) and murine
X-linked
immune defect (XID) are both immunodeficiencies mediated by mutations in
Bruton's tyrosine kinase
(
Btk
), yet the developmental stage(s) affected remain controversial. To further refine the placement of the XID defect(s), we used bromodeoxyuridine labeling to determine turnover, production and transition rates of developing B cell subsets in normal, xid and xid mice expressing a human Bcl-2 transgene (xid/bcl-2). We find the xid mutation manifest at two stages of B cell development. The first is early, reducing pre-B cell production by restricting pro-B to pre-B cell transit. Surprisingly, this impairment is offset by increased survival of cells progressing from the pre- to immature B cell pool, suggesting that
Btk
-independent homeostatic mechanisms act to maintain this compartment. The second point of action is late, substantially reducing mature B cell production. Together, these findings reconcile apparent discrepancies in the developmental stage affected by the murine versus human lesions and suggest previously unappreciated homeostatic processes that act at the pre-B to immature B cell transition. Finally,
Btk
likely functions differently at these two checkpoints, since ectopic Bcl-2 expression fails to directly complement the early xid lesion, yet reverses the defect impeding final B cell maturation.
...
PMID:xid mice reveal the interplay of homeostasis and Bruton's tyrosine kinase-mediated selection at multiple stages of B cell development. 1171 91
Bruton's tyrosine kinase
(
Btk
), a member of the Tec family of protein-tyrosine kinases, has been shown to be crucial for B cell development, differentiation, and signaling. Mutations in the
Btk
gene lead to X-linked agammaglobulinemia in humans and
X-linked
immunodeficiency in mice. Using a co-transfection approach, we present evidence here that
Btk
interacts physically with caveolin-1, a 22-kDa integral membrane protein, which is the principal structural and regulatory component of caveolae membranes. In addition, we found that native Bmx, another member of the Tec family kinases, is associated with endogenous caveolin-1 in primary human umbilical vein endothelial cells. Second, in transient transfection assays, expression of caveolin-1 leads to a substantial reduction in the in vivo tyrosine phosphorylation of both
Btk
and its constitutively active form, E41K. Furthermore, a caveolin-1 scaffolding peptide (amino acids 82--101) functionally suppressed the autokinase activity of purified recombinant
Btk
protein. Third, we demonstrate that mouse splenic B-lymphocytes express substantial amounts of caveolin-1. Interestingly, caveolin-1 was found to be constitutively phosphorylated on tyrosine 14 in these cells. The expression of caveolin-1 in B-lymphocytes and its interaction with
Btk
may have implications not only for B cell activation and signaling, but also for antigen presentation.
...
PMID:Functional interaction of caveolin-1 with Bruton's tyrosine kinase and Bmx. 1175 85
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