Interferon inducible X-linked gene CXorf21 may contribute to sexual dimorphism in Systemic Lupus Erythematosus.
Christopher A OdhamsAmy L RobertsSusan K VesterCarolina S T DuarteCharlie T BealesAnna Katharina SimonSonja LindingerSamuel J DaffernAntonino ZitoLingyan ChenLeonardo L JonesLora BotevaDavid L MorrisKerrin S SmallMichelle M A FernandoDeborah S Cunninghame GrahamTimothy J VysePublished in: Nature communications (2019)
Systemic lupus erythematosus (SLE) is an autoimmune disease, characterised by increased expression of type I interferon (IFN)-regulated genes and a striking sex imbalance towards females. Through combined genetic, in silico, in vitro, and ex vivo approaches, we define CXorf21, a gene of hitherto unknown function, which escapes X-chromosome inactivation, as a candidate underlying the Xp21.2 SLE association. We demonstrate that CXorf21 is an IFN-response gene and that the sexual dimorphism in expression is magnified by immunological challenge. Fine-mapping reveals a single haplotype as a potential causal cis-eQTL for CXorf21. We propose that expression is amplified through modification of promoter and 3'-UTR chromatin interactions. Finally, we show that the CXORF21 protein colocalises with TLR7, a pathway implicated in SLE pathogenesis. Our study reveals modulation in gene expression affected by the combination of two hallmarks of SLE: CXorf21 expression increases in a both an IFN-inducible and sex-specific manner.
Keyphrases
- systemic lupus erythematosus
- poor prognosis
- genome wide
- gene expression
- disease activity
- dendritic cells
- copy number
- immune response
- dna methylation
- binding protein
- mental health
- rheumatoid arthritis
- genome wide identification
- inflammatory response
- dna damage
- oxidative stress
- small molecule
- risk assessment
- amino acid
- molecular dynamics simulations
- high density
- mass spectrometry
- human health