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1 ble in most cell types due to the paucity of endogenous antigen.
2 of Ii and DM and will preferentially present endogenous antigen.
3 he TAP complex for efficient presentation of endogenous antigen.
4 (NAbs) have been associated with exposure to endogenous antigens.
5 ng MAIT cells to sample both endocytosed and endogenous antigens.
6 les that display peptides from exogenous and endogenous antigens.
7 he stimulation of CD4+ T-cell responses from endogenous antigens.
8 processing and presentation of exogenous and endogenous antigen and are largely maturationally synchr
9 face antigen presentation of transfected and endogenous antigens and enhance cytotoxic T-cell respons
10  by compatibility with 28 antibodies to both endogenous antigens and transgenic reporters like GFP.
11 s) induce GrB(+)CD8(+) T cells by presenting endogenous antigens and using the 4-1BBL/4-1BB axis.
12 unogen and the immunogenicity of the related endogenous antigen are important in determining the spec
13                               However, other endogenous antigens are processed by cytoplasmic proteas
14  cells into lymphopenic mice that express an endogenous antigen as a systemic, secreted protein resul
15  in naive mice antigen-specific CTLs against endogenous antigens as well as exogenous peptides, but n
16       Class I MHC protein primarily presents endogenous antigen but also may present exogenous antige
17 imulating cellular immunity, presentation of endogenous antigens by dendritic cells transfected with
18 ity was also dispensable for presentation of endogenous antigens by MHC-I via the classical pathway.
19              The failure of T134K to present endogenous antigen can be overcome by using an ER target
20 lytic effector function and the finding that endogenous antigens can enter the HLA class II processin
21 ntigen uptake or presentation, the source of endogenous antigen, costimulatory molecules or peptides
22 nant populations that efficiently recognized endogenous antigen demonstrated lower intrinsic avidity
23                 T cells that respond to this endogenous antigen develop into effector cells that caus
24 t can effectively prime T cells specific for endogenous antigens expressed by poorly immunogenic tumo
25  and drugs or viral infections and, perhaps, endogenous antigens generated by genetically altered bon
26               Expression of HLA class II and endogenous antigen, however, does not always correlate w
27 ulated expression of H2 molecules presenting endogenous antigen in the peritoneal mesothelium and ves
28  model system to study the immunogenicity of endogenous antigens in adult animals.
29  alpha-galactosylceramide (alpha-galcer) and endogenous antigens in mouse splenic and bone marrow-der
30             Of the 10 clones, 3 responded to endogenous antigens in rat islets.
31 e of mature PDCs in priming CD8 responses to endogenous antigens, in addition to their previously rep
32 ass II-restricted surveillance of long-lived endogenous antigens including nuclear proteins relevant
33 antigenic epitopes derived from exogenous or endogenous antigens is altered in PA28-/- mice.
34 C cytoskeleton of the sizes and densities of endogenous antigen-loaded CD1d nanoclusters.
35 levant antigen-specific CTLs that recognized endogenous antigen-major histocompatibility complex comp
36  an absolute requirement for presentation of endogenous antigen on Ld or for induction of virus-speci
37  protein A-luciferase (SPA-luc) was bound to endogenous antigens on primary human bronchial epithelia
38     We hypothesized that constantly degraded endogenous antigen only accumulates upon inhibition of a
39 ent and specific T-cell response against the endogenous antigen or self-antigen still remains a major
40                    Enhanced autophagy boosts endogenous antigen presentation by MHC II and allows hos
41      In this study, we define a mechanism of endogenous antigen presentation by MR1 to MAIT cells.
42 vaccine cells present tumor peptides via the endogenous antigen presentation pathway to activate CD4(
43  antigen processing, utilizing the classical endogenous antigen presentation pathway.
44 egy for systematically learning the rules of endogenous antigen presentation.
45 otein involved in the MHC class I pathway of endogenous antigen presentation.
46 fer of cellular material from vaccine DCs to endogenous antigen presenting cells was visualized in ly
47  of antigen from antigen-specific B cells to endogenous antigen-presenting cells or by direct B-T cel
48                                     Finally, endogenous antigen-primed CD4(+) T cells responded equiv
49 st, the contribution of proteasome-dependent endogenous antigen processing to the global influenza CD
50                             Although several endogenous antigen-processing pathways have been reporte
51 resolution of recombination intermediates in endogenous antigen receptor loci.
52 AG2 C terminus in mediating rearrangement of endogenous antigen-receptor loci.
53       The ability of iNKT cells to recognize endogenous antigens represents a distinct immune recogni
54 has not yet been resolved if there is single endogenous antigen responsible for both positive selecti
55 bsets in the skin and monitor the effects on endogenous antigen-specific CD4(+) T- and B-cell respons
56  in substantial expansion and maintenance of endogenous antigen-specific CD8 T cells.
57 n activation and expansion of both donor and endogenous antigen-specific cells in a dose-dependent ma
58 tions; however, the inability to detect rare endogenous antigen-specific cells limits current underst
59 tramers to track and analyze a population of endogenous antigen-specific memory CD4 T cells exposed t
60  suppression by polyclonal T regs depends on endogenous antigen stimulation; this occurs in a locatio
61 cells (DCs) sample and process exogenous and endogenous antigens that can trigger an inflammatory nid
62 hi dendritic cells (DCs) efficiently present endogenous antigen to activate naive PLP139-151-specific
63  US6 transfected cells are unable to present endogenous antigen to cytotoxic T lymphocytes and are th
64 ged to lysine (T134K), are unable to present endogenous antigens to CTLs.
65  lack this transporter are unable to present endogenous antigens to CTLs.
66     Typically, MHC class I molecules present endogenous antigens to cytotoxic T lymphocytes (CTLs).
67 ighly immunogenic and preferentially present endogenous antigens, while tumors coexpressing class II
68     The autoimmunity appears to be driven by endogenous antigens, with little polyclonal B cell activ

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