Association of PSORS1C3, CARD14 and TLR4 genotypes and haplotypes with psoriasis susceptibility
Psoriasis is a common chronic, immune-mediated inflammatory disease of the skin. PSORS1C3 is a non-protein coding gene, of which the RNA transcript is found in psoriatic patients. CARD14 is mainly expressed in epidermal keratinocytes. TLR4 is a transmembrane protein to recognize microbial antigens....
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Veröffentlicht in: | Genetics and molecular biology 2022-01, Vol.45 (4), p.e20220099-e20220099 |
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Zusammenfassung: | Psoriasis is a common chronic, immune-mediated inflammatory disease of the skin.
PSORS1C3
is a non-protein coding gene, of which the RNA transcript is found in psoriatic patients. CARD14 is mainly expressed in epidermal keratinocytes. TLR4 is a transmembrane protein to recognize microbial antigens. Our study aimed to assess the relationship among
PSORS1C3, CARD14
and
TLR4
polymorphisms, inflammatory expression and psoriasis susceptibility. To the end, 71 patients with psoriasis and 46 healthy individuals with the well-characterized clinical profiles were enrolled. Gene polymorphisms were determined by Sanger DNA sequencing and secretion of cytokines by ELISA. As a result, genetic analysis of
PSORS1C3
gene identified nine SNPs and three haplotype blocks. Sequencing of the
CARD14
gene determined eight SNPs and one haplotype block. Sequencing of
TLR4
gene identified nine SNPs, in which a SNP rs1018673641 was found to exert deleterious effect. The linkage disequilibrium analysis showed that seven variants in
PSORS1C3
gene and three SNPs in
CARD14
gene were in tightly linked. More importantly, a significant association between IL-6 level and rs1018673641 AT genotype in
TLR4
gene was detected in psoriatic patients. In conclusion, the
PSORS1C3, CARD14
and
TLR4
polymorphisms and haplotypes may be correlated with risk of suffering psoriasis and the IL-6-mediated chronic inflammation in psoriasis could be partially regulated by the
TLR4
functional variant. |
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ISSN: | 1415-4757 1678-4685 1678-4685 |
DOI: | 10.1590/1678-4685-gmb-2022-0099 |