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Target Concepts:
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Query: UMLS:C0033036 (
APC
)
10,214
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Astrocytes are nonprofessional APCs that may participate in Ag presentation and activation of pathogenic CD4+ T cells involved in central nervous system (CNS) inflammatory diseases. Using immortalized pure astrocytes as a complement to the study of primary astrocytes, we investigated whether these astrocytes express elements involved in the class II endocytic pathway and if they are capable of processing native myelin basic protein (MBP), a step that could be necessary for initiating or perpetuating T cell recognition of this self-Ag in vivo. Upon IFN-gamma-stimulation, primary and immortalized astrocytes up-regulate
class II transactivator
(
CIITA
), invariant chain (Ii) (p31 and p41), H-2Ma, and H-2Mb. Analysis of
CIITA
cDNA sequences demonstrated that
CIITA
transcription in astrocytes is directed by a promoter (type IV) that mediates IFN-gamma-inducible
CIITA
expression and encodes a
CIITA
protein that differs in its N-terminal sequence from
CIITA
reported in professional
APC
. Comparing live and fixed
APC
for Ag presentation, we show that Ag processing by
APC
is required for presentation of native MBP to autopathogenic T cells specific for the major MBP epitope, Acl-11. We have observed that primary astrocytes and some, but not all, astrocyte lines in the absence of contaminating microglia are capable of processing and presenting native MBP, suggesting that there may be heterogeneity. Our study provides definitive evidence that astrocytes are capable of processing CNS autoantigen, indicating that astrocytes have potential for processing and presentation of CNS autoantigen to proinflammatory T cells in CNS autoimmune disease.
...
PMID:Astrocytes express elements of the class II endocytic pathway and process central nervous system autoantigen for presentation to encephalitogenic T cells. 983 77
Infections by human CMV are controlled by cellular immune responses. Professional
APC
such as monocytes and macrophages can be infected in vivo and are considered as a reservoir of virus. However, CMV-specific CD4(+) responses against infected
APC
have not been reported. To develop a model of CD4-infected
APC
interaction, we have transfected the U373MG astrocytoma cell line with the
class II transactivator
(
CIITA
). Confocal microscopy experiments showed that U373MG-
CIITA
cells expressed markers characteristic of
APC
. Functional assays demonstrated that infected U373MG-
CIITA
APC
processed and presented both exogenous and endogenously neosynthesized nuclear immediate early (IE) protein 1 through the MHC class II pathway. More importantly, endogenous presentation of IE1 by infected
APC
lead to efficient control of CMV infection as revealed by decreased viral titer. Thus, these results describe the endogenous presentation of a nuclear viral protein by the MHC class II pathway and suggest that IE1-specific CD4(+) T cells may play an important role in CMV infection by directly acting against infected
APC
.
...
PMID:Infection of APC by human cytomegalovirus controlled through recognition of endogenous nuclear immediate early protein 1 by specific CD4(+) T lymphocytes. 1213 51
The role of the
MHC class II transactivator
(
CIITA
) in Ag presentation by astrocytes and susceptibility to experimental autoimmune encephalomyelitis (EAE) was examined using
CIITA
-deficient mice and newly created transgenic mice that used the glial fibrillary acidic protein promoter to target
CIITA
expression in astrocytes.
CIITA
was required for class II expression on astrocytes. Like class II-deficient mice,
CIITA
-deficient mice were resistant to EAE by immunization with CNS autoantigen, although T cells from immunized
CIITA
-deficient, but not class II-deficient, mice proliferated and secreted Th1 cytokines.
CIITA
-deficient splenic
APC
presented encephalitogenic peptide to purified wild-type encephalitogenic CD4(+) T cells, indicating that
CIITA
-independent mechanisms can be used for class II-restricted Ag presentation in lymphoid tissue.
CIITA
-deficient mice were also resistant to EAE by adoptive transfer of encephalitogenic class II-restricted CD4(+) Th1 cells, indicating that
CIITA
-dependent class II expression was required for CNS Ag presentation. Despite constitutive
CIITA
-driven class II expression on astrocytes in vivo, glial fibrillary acidic protein-
CIITA
transgenic mice were no more susceptible to EAE than controls.
CIITA
-transfected astrocytes presented peptide Ag, but in contrast to IFN-gamma-activated astrocytes, they could not process and present native Ag.
CIITA
-transfected astrocytes did not express cathepsin S without IFN-gamma activation, indicating that
CIITA
does not regulate other elements that may be required for Ag processing by astrocytes. Although our results demonstrate that
CIITA
-directed class II expression is required for EAE induction,
CIITA
-directed class II expression by astrocytes does not appear to increase EAE susceptibility. These results do not support the role of astrocytes as
APC
for class II-restricted Ag presentation during the induction phase of EAE.
...
PMID:The role of the MHC class II transactivator in class II expression and antigen presentation by astrocytes and in susceptibility to central nervous system autoimmune disease. 1247 Nov 3
This study focused on synthesis of MHC class II glycoproteins (MHCII) by rat CD4(+) T-helper cells. During activation in Con A and IL-2, purified rat splenic CD4(+) T cells expressed abundant surface MHCII together with transcripts for I-A alpha/beta, invariant chain, and the type III and type IV
MHC class II transactivator
(
CIITA
). Activated thymic CD8(+)CD4(-) and CD8(+)CD4(+) T cells exhibited essentially the same phenotype. MHCII synthesis by CD4(+) T cells enabled presentation of myelin basic protein (MBP) to antigen-specific responders. T cell expression of MHCII was due to direct biosynthesis rather than adsorption from professional
APC
; indeed, T cell-mediated expression of MHCII was optimal in the absence of professional
APC
. Despite periodic reactivation with Con A during 3-4 weeks of culture, CD4(+) T cells repressed MHCII synthesis and reverted to a MHCII(-) phenotype. These short-term lines resembled established lines of MBP-specific T cells in that mitogenic activation elicited extensive blastogenesis without MHCII synthesis. Activation-dependent synthesis of MHCII however was partially restored in lines of mitogen-stimulated T cells when the cultures were reconstituted with irradiated splenic
APC
. These data indicate that most naive rat CD4(+) T cells exhibit activation-dependent synthesis of MHCII whereas continuously propagated T cells require an
APC
-derived signal to support MHCII synthesis.
...
PMID:MHC class II biosynthesis by activated rat CD4+ T cells: development of repression in vitro and modulation by APC-derived signals. 1554 17
Experimental autoimmune myocarditis (EAM) in rats is a T-cell-mediated disorder and has been shown to involve immune imbalance. The aim of this study was to examine the immunomodulatory effects of 3-hydroxy-3-methyl-glutaryl coenzyme A reductase inhibitor, atorvastatin, on the expression of MHC class II molecules in the myocardium of rats with EAM, and to examine its therapeutic potential for EAM. EAM was induced in Lewis rats by injection of porcine cardiac myosin. High-dosage (10 mg/kg per day) or low-dosage (1 mg/kg per day) atorvastatin or vehicle was given orally for 3 weeks. On day 21 after immunization, echocardiography was carried out and the severity of myocarditis was evaluated by histopathological investigations. Immunohistochemistry techniques were used to examine the expression of MHC class II molecules in the myocardium. Type I, III and IV
class II transactivator
(
CIITA
) promoter transcription was evaluated by reverse transcription-PCR. Cardiomyocytes were isolated and the expression of MHC class II molecules by them was detected using cytometry. Serum Th1/Th2 cytokines were examined on day 21 by ELISA. Cardiac function was improved in the two atorvastatin-treated groups compared with the untreated one. In atorvastatin groups, the histopathological severity of myocarditis was attenuated and the expression of MHC class II molecules on the 'nonprofessional'
APC
, the cardiomyocytes, was reduced. mRNA level of type IV
CIITA
promoter was downregulated in the statin-treated groups in a dosage-dependent manner, but levels of type I and III
CIITA
mRNA did not differ between the groups statistically. Levels of IFN-gamma and IL-2 increased, whereas levels of IL-4 and IL-10 decreased, in immunized rats from day three through day 21. Atorvastatin reversed these trends in the treated groups. Atorvastatin improves cardiac function and histopathology of the myocardium in EAM by inducing Th2-biased immune responses, and thus 3-hydroxy-3-methyl-glutaryl coenzyme A reductase blockade may be a promising new strategy for the treatment of cardiac autoimmune impairments. The underlying mechanisms may be related to downregulation of MHC class II Ag expression due to silencing of the
CIITA
mRNA transcription.
...
PMID:Immunoregulatory effects of atorvastatin on experimental autoimmune myocarditis in Lewis rats. 1650 27
