Systemic lupus erythematosus and rheumatoid arthritis

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7. Genetics of SLE and RA
A strong genetic component is involved in the aetiology of SLE. The disease
concordance rate is 2-5% for dizygotic twins compared with 24-58% for
- 25 -

monozygotic twins.
4
There is also familial clustering with an
λ
s
,
i.e.
an
increased risk of disease in siblings of patients with SLE compared with that of
the general population,
of approximately 20.
97
As for SLE, there are strong
genetic components contributing to the susceptibility for RA. The disease
concordance rate for dizygotic twins in RA is 3.6% whereas it is 15% for
monozygotic twins.
5
There is a familial clustering of RA with a
λ
s
estimated to
be between 2 and 17.
98
Common for both SLE and RA, as well as for other autoimmune disorders, is a
strong genetic contribution from the human leukocyte antigen (
HLA
) region on
chromosome 6p21.1-21.3. The
HLA
region contains over 200 genes and is the
most polymorphic region of the genome. The
HLA
genes are divided into the
class I region (
HLA
A
,
B
and
C
), the class II region (
HLA DR
,
DQ
and
DP
) and
the class III region, which contains a variety of genes for immunologically
active products,
i.e.
, tumour necrosis factor (
TNF
) and the complement
components
C2
and
C4
(Figure 8).
Figure 8.
Gene map of the human leukocyte antigen (HLA) region on chromosome 6. Adapted
from Mehra
et al.
99
SLE has been associated with haplotypes of the class II genes, mainly
DRB1*1501/DQB1*0602
,
DRB1*0301/DQB1*0201
and
DRB1*0801/DQB1*0402
in Caucasians.
100
In RA,
HLA
class II haplotypes have
also been associated with disease, especially
DRB1*0101, *0401, *0405,
and
*0408
, also known as the shared epitope (
HLA-SE
) alleles because of a shared
common sequence.
101
Linkage studies have successfully identified causative
loci in monogenic diseases but they have not been as successful in identifying
candidate genes in SLE and RA. The problem with linkage studies in complex
diseases has been that the identified susceptibility loci have been too large and
contained a vast number of potential candidate genes. A number of established
candidate genes, for example
IRF5
in SLE, have not been included in
previously reported linkage regions. For SLE and RA, the main advances in the
hunt for candidate genes have been made by association studies and in

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