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1 hesitis, axial joint disease, and persistent oligoarthritis.
2 established linkage of the locus to juvenile oligoarthritis.
3 TNFalpha in the etiopathogenesis of juvenile oligoarthritis.
4 B1 was also observed in female patients with oligoarthritis.
5 ps of persistent oligoarthritis and extended oligoarthritis.
6 irmed as independent susceptibility loci for oligoarthritis.
7 , and DRB1 in UK Caucasian JIA patients with oligoarthritis.
8 locus is linked and associated with juvenile oligoarthritis.
9 ypes containing this haplotype with extended oligoarthritis.
10 ly acquired ReA and 31 with undifferentiated oligoarthritis.
11 ers clinical course but usually manifests as oligoarthritis.
12 tients recruited to the study, 266 (53%) had oligoarthritis.
13 rse clinical course but usually manifests as oligoarthritis.
14 ways was evident in patients with persistent oligoarthritis.
15 es from 15 patients (8 with undifferentiated oligoarthritis, 3 with ReA, 1 with rheumatoid arthritis,
16 ad Reiter's syndrome, 7 had undifferentiated oligoarthritis, 4 had undifferentiated monarthritis, 6 h
17 -related arthritis [ERA], 42 with persistent oligoarthritis, 45 with rheumatoid factor [RF]-negative
19 0 days), developed acute and severe mono- or oligoarthritis almost exclusively in the limb closest to
20 remission is disease category, particularly oligoarthritis, although a few additional clinical predi
22 Linkage to HLA-A and HLA-DRB1 was seen in oligoarthritis and in the International League of Associ
23 ogical examinations revealed severe poly- or oligoarthritis and moderate to severe cortical hyperplas
25 sociation of multiple TNF SNPs with juvenile oligoarthritis and to construct and analyze SNP-tagged T
26 o establish linkage of HLA-A and HLA-DRB1 in oligoarthritis and to show that the 2 loci contribute in
27 ation of dactylitis of a toe, heel pain, and oligoarthritis appears to be strongly suggestive of psor
28 teroids are an effective treatment for early oligoarthritis, but there is still a high level of long-
30 e associations between HLA loci and juvenile oligoarthritis have previously been documented, evidence
33 umented, evidence for linkage of HLA loci in oligoarthritis in UK Caucasians with juvenile idiopathic
35 8 patients with either ReA, undifferentiated oligoarthritis, or other forms of arthritis, and from 24
36 ted States, intermittent or chronic mono- or oligoarthritis, particularly affecting the knee, is the
38 of non-systemic phenotypes of JIA, including oligoarthritis, polyarthritis, enthesitis-related arthri
39 compared with those from the ERA, persistent oligoarthritis, RF-negative polyarthritis, and systemic
41 ents with polyarticular course JIA (extended oligoarthritis, rheumatoid factor-positive or rheumatoid
45 umbers were higher in patients with extended oligoarthritis, the more severe subtype of JIA, as compa
47 were more common in southeast Asia, whereas oligoarthritis was more prevalent in southern Europe (13
49 , rheumatoid arthritis, and undifferentiated oligoarthritis, was assayed by polymerase chain reaction
51 ling subgroups of JIA, systemic and extended oligoarthritis, were underrepresented in that study.
52 of unselected patients with undifferentiated oligoarthritis, which further supports the hypothesis th