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Query: UNIPROT:P15088 (
mast cell
)
14,925
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Mast cell-mediated responses are likely to be regulated by the cross talk between activatory and inhibitory signals. We have screened human cord blood mast cells for recently characterized inhibitory receptors expressed on NK cells. We found that
IRp60
, an Ig superfamily member, is expressed on human mast cells. On NK cells,
IRp60
cross-linking leads to the inhibition of cytotoxic activity vs target cells in vitro.
IRp60
is constitutively expressed on mast cells but is down-regulated in vitro by the eosinophil proteins major basic protein and eosinophil-derived neurotoxin. An immune complex-mediated cross-linking of
IRp60
led to inhibition of IgE-induced degranulation and stem cell factor-mediated survival via a mechanism involving tyrosine phosphorylation, phosphatase recruitment, and termination of cellular calcium influx. To evaluate the role of
IRp60
in regulation of allergic responses in vivo, a murine model of allergic peritonitis was used in which the murine homolog of
IRp60
, LMIR1, was neutralized in BALB/c mice by mAbs. This neutralization led to a significantly augmented release of inflammatory mediators and eosinophilic infiltration. These data demonstrate a novel pathway for the regulation of human
mast cell
function and allergic responses, indicating
IRp60
as a candidate target for future treatment of allergic and
mast cell
-associated diseases.
...
PMID:The inhibitory receptor IRp60 (CD300a) is expressed and functional on human mast cells. 1633 35
The inhibitory myeloid immunoglobulin receptor CD300a (
IRp60
) has been shown to downregulate
mast cell
and eosinophil activities, thereby serving as a potential target for inhibiting allergic effector cell input in allergy. Our aims were to study the expression and functional properties of this receptor in purified human basophils, cells that crucially contribute to Th2-type immunity and allergy. Basophils homogeneously expressed CD300a as well as the inhibitory receptor CD200R on their cell surface, and these expressions increased after anti-IgE stimulation. IgE-mediated basophil degranulation was also significantly inhibited by crosslinking of either CD200R or CD300a (by 90% and 50%, respectively). Inhibitory SHIP-1 phosphorylations were also induced by CD200R and CD300a, although they were not noticeably increased by IgE-dependent activation. We conclude that both CD200R and CD300a play a role in reducing IgE-mediated basophil function and may crucially govern the known differential activities of these cells in vivo.
...
PMID:Expressions and inhibitory functions of CD300a receptors on purified human basophils. 2316 58
