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1 stimulated with OVA (assay for induction of delayed hypersensitivity).
2 ir recipients failed to display RPE-specific delayed hypersensitivity.
3 owed the capacity to suppress donor-specific delayed hypersensitivity.
4 roinflammatory Th1 cells in a mouse model of delayed hypersensitivity.
5 nship including onset patterns suggestive of delayed hypersensitivity, alongside consistent HSV featu
6 red the HLA loci in 98 Spanish patients with delayed hypersensitivity and 315 with immediate hypersen
10 . into naive recipients induced allospecific delayed hypersensitivity and elicited delayed hypersensi
11 e recipients were evaluated for RPE-specific delayed hypersensitivity and examined clinically and his
12 a2 induce immune deviation in vivo (impaired delayed hypersensitivity and IgG2a Ab production) when i
13 these types of grafts display donor-specific delayed hypersensitivity and in vitro proliferating prim
14 1 is functionally relevant in the genesis of delayed hypersensitivity and may be a useful therapeutic
15 f IFN-gamma, induce macrophage cytotoxicity, delayed hypersensitivity, and enhanced cellular immunity
18 geneic mice elicited an intense RPE-specific delayed hypersensitivity associated with a vehement cell
19 binding proteins inhibit local expression of delayed hypersensitivity by a T-cell fibronectin-depende
20 stered therapeutically to animals undergoing delayed hypersensitivity can almost completely abolish T
21 genotyped the MHC region in 24 patients with delayed hypersensitivity compared with 20 patients with
22 fragments were evaluated for donor-specific delayed hypersensitivity (DH) and ACAID, and fragment-co
23 recipients were evaluated for acquisition of delayed hypersensitivity (DH) and cytotoxic T cells (Tc)
24 opulations of regulatory T cells that impair delayed hypersensitivity (DH) by two different mechanism
27 ologically and acquisition of donor-specific delayed hypersensitivity (DH) was assessed at selected i
29 nduces an Ag-specific impairment of systemic delayed hypersensitivity (DH), termed anterior chamber a
35 ear pinnae of normal BALB/c mice (assay for delayed hypersensitivity expression) or coinjected with
36 lar immune privilege, prevents Th1-dependent delayed hypersensitivity from developing in response to
37 ure TGFbeta and suppressed the expression of delayed hypersensitivity in a local adoptive transfer as
39 ulatory T cells that suppressed RPE-specific delayed hypersensitivity in naive syngeneic recipients.
42 we show that using a rat model of cutaneous delayed hypersensitivity, MCP-1 expression correlates sp
44 histochemical findings suggest a mixed-type, delayed hypersensitivity reaction as the mechanism of in
47 ction rate is high, and it was produced by a delayed hypersensitivity reaction with a Th2 response.
52 d in EPA and DHA suppressed antigen-specific delayed hypersensitivity reactions and mitogen-induced p
56 dies report a very low incidence of acute or delayed hypersensitivity reactions to the antivenom.
61 taneously in two doses 2 weeks apart, evoked delayed hypersensitivity responses in a concentration-de
63 method for inducing tolerance in humoral and delayed hypersensitivity responses which is associated w
64 atients) and healthy control subjects with a delayed hypersensitivity skin test response to M. avium
65 ripheral T-cell function, as measured by the delayed hypersensitivity skin test to tuberculin, and an
67 ere was a strong inverse association between delayed hypersensitivity to Mycobacterium tuberculosis a
68 icantly associated with an increased risk of delayed hypersensitivity to penicillins (OR, 1.7; 95% CI
69 :02 alleles in the risk management of severe delayed hypersensitivity to penicillins should be evalua
70 ns and aztreonam in subjects with documented delayed hypersensitivity to penicillins who especially r