Systemic lupus erythematosus and rheumatoid arthritis

There was a north to south gradient in allele frequency in Sweden, however, the 
number of patients from southern Sweden was quite small, which could explain 
the relatively high allele frequency of 1858T in the control group. There was an 
increased frequency of renal disorder in patients carrying the risk allele 
compared with patients homozygous for the major allele (Table 13).
It was shown in paper II that the 
PD-1.3A
allele was associated with renal 
disorder as was the case for the 
PTPN22
1858T allele. A combined analysis of 
the two risk alleles was performed in patients with renal disorder (n = 142) and 
compared to those without either allele and to controls. The strongest 
association was between individuals negative for both 
PTPN22
1858T and 
PD-
1.3A
compared with the control group (P = 0.000008) (Table 14). This 
suggested a strong protective effect of the non-risk alleles. The test for 
independence was more significantly associated in the 
PTPN22
positive and 
PDCD1
negative group (P = 0.004) than in the 
PDCD1
positive and 
PTPN22
negative group (P = 0.0710) when patients with renal disorder were compared 
with patients without renal disorder. This suggests that 
PTPN22
1858T confers 
a stronger risk for renal disorder than 
PD-1.3A
and that they may be 
independently associated (Table 14). There was some degree of interaction, 
although weak, and was based on only 9 individuals (P = 0.02) (Table 14). 
Table 14.
PTPN22
1858T and 
PD-1.3A
are independent genetic susceptibility factors in SLE. 
PDCD1 +ve = positive for 
PD-1.3A
; PTPN22 +ve = positive for 
PTPN22
1858T; PDCD1 -ve = 
negative for 
PD-1.3A
; PTPN22 -ve = negative for 
PTPN22
1858T. 

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