Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: UNIPROT:P06126 (
CD1a
)
2,221
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
A subset of Pts develops dysfunctional MO to inflammatory DC differentiation and immunosuppression.
MDDC
, a newly described DC subset, is pivotal in initiating antibacterial responses. Endogenous proteins are known to alter MO to
MDDC
differentiation. In particular, trauma-elevated TSP-1, a protein that is known to affect MO functions, could trigger
MDDC
differentiation defects. We hypothesized that TSP-1-deranged differentiation of inflammatory
CD1a
(+)
MDDC
would negatively alter activation of immune functions, thereby increasing the risk of postinjury infections. Post-trauma increased TSP-1 levels in patients' plasma and MO correlated with two distinct
MDDC
differentiation dysfunctions: the previously described decreased
CD1a
(+)DC yields but also, development of an immunoincompetent
CD1a
(+)
MDDC
. The Pts' development of Dysf DC correlated to increased infectious complications. TSP-1 triggered its inhibitory receptor, CD47, activating an inhibitory phosphatase, SHP-1. Increased pSHP-1, decreased antigen processing, and depressed T cell stimulation characterized Pt Dysf DC. TSP-1 mimics added during Cnt
MDDC
differentiation depressed
CD1a
(+)DC yields but more importantly, also induced defective
CD1a
(+)
MDDC
, reproducing Pts'
MDDC
differentiation dysfunctions. CD47 triggering during Cnt
MDDC
differentiation increased SHP-1 activation, inhibiting IL-4-induced STAT-6 activation (critical for
CD1a
(+)
MDDC
differentiation). SHP-1 inhibition during
MDDC
differentiation in the presence of TSP-1 mimics restored pSTAT-6 levels and
CD1a
(+)
MDDC
immunogenicity. Thus, postinjury-elevated TSP-1 can decrease
CD1a
(+)DC yields but more critically, also induces SHP-1 hyperactivity, deviating
MDDC
differentiation to defective
CD1a
(+) inflammatory MDDCs by inhibiting STAT-6.
...
PMID:Elevated postinjury thrombospondin 1-CD47 triggering aids differentiation of patients' defective inflammatory CD1a+dendritic cells. 2500 59
