Background/Objetive: Long non-coding RNAs (lncRNAs) regulate immune signaling pathways, including interferon (IFN)-mediated responses implicated in antiphospholipid syndrome (APS). The IFN-inducible lncRNA NRIR (AC017076.5) exhibits context-dependent regulatory functions and has been associated with modulation of STAT1/STAT2 activation in human monocytes. Its expression profile in APS remains unexplored. Method: In this cross-sectional exploratory study, NRIR expression was quantified by reverse transcription-quantitative PCR in CD14-enriched peripheral blood monocytes from APS patients and age-and sex-matched healthy controls. Relative expression was calculated using the 2 -Ct method with GAPDH as endogenous control. Subgroup analyses compared obstetric APS (OAPS) and non-obstetric APS (NOAPS). Complementary in silico protein-protein interaction and pathway enrichment analyses contextualized NRIR within IFN-related networks. Results: NRIR expression was significantly reduced in APS compared with controls. OAPS patients exhibited less pronounced downregulation than NOAPS, showing an intermediate expression pattern. Network analysis identified a STAT1-centered IFN-enriched module related to antiviral and type I IFN signaling, with NRIR positioned peripherally. Functional inferences remain hypothesis-generating due to sample size and absence of direct IFN measurements. Conclusion:NRIR is downregulated in peripheral monocytes from APS patients, with phenotype-dependent differences.Further mechanistic and IFN-integrated studies are required.
Guzmán-Martín et al. (Mon,) studied this question.
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