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Query: UMLS:C0003864 (
arthritis
)
69,039
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Histocompatibility antigens were determined in 60 patients with psoriatic arthritis. The patients were divided into clinical subgroups according to axial or peripheral joint involvement, disease severity based on number of peripheral joints involved, and the presence or absence of bone erosions. The total group showed a significant increase in frequency of HLA-A1, B17, B27, and
DR7
when compared with a control population. The subgroup with spondylitis had a significant increase in frequency of HLA-B27 when compared with patients with peripheral
arthritis
(p less than 0.001). The subgroup with peripheral
arthritis
alone had a higher frequency of HLA-
DR7
than the control group (p less than 0.001). There were also significant associations between HLA-
DR7
and chronic severe disease (p less than 0.001) and between HLA-DR4 and the presence of erosions (p less than 0.05).
...
PMID:Psoriatic arthritis: clinical subgroups and histocompatibility antigens. 357 82
Fifty one patients with ankylosing spondylitis (AS) were typed for HLA-A, B, C, DR, and DQ antigens. The antigen frequencies were compared with those of a normal population and with a B27 positive control group. All but one of the patients with AS were HLA-B27 positive. A positive linkage disequilibrium between Cw1, Cw2, DR1, and the B27 antigen was observed. Patients with AS showed a significant increase in DQw2 antigen compared with the B27 positive control group. No differences in antigenic frequencies were observed in patients having peripheral
arthritis
and patients with only axial involvement. Seven out of nine patients (78%) with an erosive peripheral
arthritis
were
DR7
positive, suggesting that
DR7
or genes closely linked could be related with a more aggressive peripheral joint involvement in patients with AS.
...
PMID:HLA class II antigens (DR, DQ loci) and peripheral arthritis in ankylosing spondylitis. 366 36
HLA antigen frequencies were studied in 158 patients with psoriatic arthritis, and compared to those of 101 patients with uncomplicated psoriasis and 243 healthy controls. The HLA antigens B16, B17, B27, B39 and Cw6 were associated with psoriatic arthritis. No associations between DR antigens and psoriatic arthritis were demonstrated. However, the subset of patients with rheumatoid-like
arthritis
demonstrated an increase in DR4. Uncomplicated psoriasis patients had higher frequencies of B17, Cw6 and
DR7
than patients with psoriatic arthritis, while B7 and B27 correlated with development of
arthritis
. HLA-B27, Cw2 and DRw52 were associated with back involvement, whereas B38 and B39 were associated with polyarthritis. HLA-B7, B13 and
DR7
correlated with milder disease in patients with psoriatic arthritis.
...
PMID:HLA antigens in psoriatic arthritis. 373 81
HLA phenotypes were determined in 50 patients with psoriasis alone and in 50 patients with psoriasis and psoriatic arthritis. Positive associations were found in both groups with B13, B17, B37, Cw6, and
DR7
, and in addition with C4A6. Higher relative risks were found in respect to the patients with psoriasis alone compared with those with
arthritis
, and this suggests the involvement of additional genetic factors predisposing to peripheral
arthritis
. In patients with psoriasis only, the presence of Cw6 was associated with a significantly earlier age of onset.
...
PMID:HLA antigens in psoriasis and psoriatic arthritis. 386 77
Fifty-nine patients with HLA-B27 positive ankylosing spondylitis were HLA genotyped to look for immunogenetic differences between patients with associated peripheral
arthritis
and those with disease limited to the axial skeleton. An association was found between the peripheral arthropathy and 2 antigens, HLA-A11 and HLA-
DR7
at the p less than 0.05 level. Complementation between these 2 alleles and HLA-B27 occurred in both the cis and trans positions. Four patients with peripheral
arthritis
had a rare HLA-B27 haplotype (HLA-B27, HLA-
DR7
) which was not found in the group with axial disease alone.
...
PMID:Complementation with HLA-A and HLA-D locus alleles in ankylosing spondylitis with peripheral arthritis. 387 37
The HLA genetic region was studied in 51 patients with systemic onset juvenile rheumatoid arthritis: 35 with childhood onset and 16 with adult onset (adult Still's disease). HLA genotypes were established by including family members, 261 of whom were also typed in the study. The most marked difference between patients and controls involved the HLA-DR4 gene, which occurred with a frequency of 0.348 in the childhood onset patients and 0.170 in the controls (chi 2 = 8.97, P = 0.0028, adjusted P = 0.017). In contrast, the adult onset patients showed a marginal increase in HLA-
DR7
, but were similar to controls with respect to HLA-DR4. HLA-Bw35 was increased in children with systemic onset disease, in accordance with earlier findings. The results suggest that patients with systemic onset juvenile rheumatoid arthritis have complex HLA associations which are different in childhood onset and adult onset disease.
Arthritis
Rheum 1985 Feb
PMID:HLA gene frequencies in children and adults with systemic onset juvenile rheumatoid arthritis. 397 Jul 30
The responses of synovial lymphocytes to Chlamydia/Ureaplasma and to enteric antigens were studied in 31 patients with
arthritis
confined to knee joints, 15 patients with sexually-transmitted Reiter's syndrome, 9 with enteric Reiter's syndrome, and 24 with rheumatoid arthritis. The frequency of HLA antigens was studied in 28 patients with knee joint
arthritis
; this group was characterized by elevated frequencies of HLA-A2 and DR1. A subgroup of 8 responders to Chlamydia/Ureaplasma was characterized by an increase of HLA-Bw44 and
DR7
or 8, while a subgroup of 8 responders to enteric antigens was characterized by increases of HLA-A1 and DR5. The frequency of HLA-B27 in the groups responding to antigens was 25-30%, less than half the frequency in patients with Reiter's syndrome.
Arthritis
Rheum 1984 Oct
PMID:Arthritis confined to knee joints. Synovial lymphocyte responses to microbial antigens correlate with distribution of HLA. 648 96
Patients with ankylosing spondylitis, psoriatic arthritis, and psoriasis alone were typed for HLA A, B, Cw, and DR antigens, and the antigen frequencies were compared with those in a normal control population and in patients with rheumatoid arthritis. Patients with psoriasis had a significantly raised frequency of Cw6. Those with
arthritis
in addition to their psoriasis also had raised frequencies of B27 and
DR7
. Patients with ankylosing spondylitis were characterised by the expected high frequency of HLA B27. Again, those with peripheral
arthritis
had a higher B27 and
DR7
frequency than those without. DR3 is associated with the development of erosions in psoriatic arthritis.
...
PMID:Histocompatibility antigens in psoriasis, psoriatic arthropathy, and ankylosing spondylitis. 657 72
Measurement of serum rheumatoid factor (RF) by conventional methods in patients with rheumatoid arthritis (RA) has repeatedly identified a subpopulation of patients without detectable RF. Previous investigators have consistently confirmed the association of HLA-DR4 with seropositive RA, but studies of seronegative RA have been limited and contradictory. We studied 140 randomly selected patients from Alabama, all of whom had either classic or definite RA, and we were able to complete HLA typing for 110 of these individuals. Eighty were consistently seropositive (on at least 2 separate occasions) and 30 were consistently seronegative (on at least 3 separate determinations). There was no statistically significant difference between the seronegative RA patients and 123 control subjects in the distribution of DR antigens. In seropositive RA, there was a significant increase in DR4 (P less than 0.001; relative risk = 8.02; attributable risk = 49.2%) and a significant decrease in DR3 (P less than 0.001; relative risk = 0.14) and
DR7
(0.01 greater than P greater than 0.001; relative risk = 0.33). The clinical data also distinguished between seropositive RA and seronegative RA; subcutaneous nodules (37.5%) and vasculitis (6.3%) were present only in seropositive RA. DR4 positively did not correlate with any of the clinical variables measured in the seropositive RA group. In contrast, DR4 in the seronegative RA group was associated with more destructive disease. The data suggest that seronegative RA represents a disease entity clinically and immunogenetically distinct from seropositive RA. Moreover, our results indicate that DR4 may be a previously undisclosed marker for disease severity in seronegative RA.
Arthritis
Rheum 1982 May
PMID:Seronegative rheumatoid arthritis. A distinct immunogenetic disease? 695 76
Whether a genetic predisposition to develop the antiphospholipid syndrome (APS) and to produce anticardiolipin antibodies (aCL) and lupus anticoagulant (LAC) exists has been addressed by family studies and by population studies on primary APS and on aCL in diseases other than primary APS. Various studies suggest a familial occurrence of aCL and LAC, with or without clinical evidence of APS. This familial tendency could be genetically determined, because APS, aCL, and LAC occur in families carrying haplotypes which contain HLA-DR4, -
DR7
, and -DRw53. Population studies on primary APS also indicate that HLA genes have a role in conferring susceptibility to develop primary APS. Again, DR4,
DR7
, and DRw53 are the relevant loci. Population studies on aCL in diseases other than primary APS indicate that aCL are associated with DR4,
DR7
, and DRw53, at least when they are found in patients with systemic lupus erythematosus. Because HLA-DR4, -
DR7
, and -DRw53 are in linkage disequilibrium, the genetic association of aCL could be with DRw53 and, depending on the regional frequency of DR4 or
DR7
, it could be linked with either DR4 or
DR7
. HLA-DR4 seems to be more important in Anglo-Saxons, whereas
DR7
emerges in populations of Latin origin. In this report we review our studies and the pertinent literature in this field.
Semin
Arthritis
Rheum 1996 Jun
PMID:The immunogenetics of the antiphospholipid syndrome, anticardiolipin antibodies, and lupus anticoagulant. 879 13
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