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Clinical Trial
. 2019 Nov;28(13):1524-1533.
doi: 10.1177/0961203319885447. Epub 2019 Oct 29.

Type I interferon gene signature test-low and -high patients with systemic lupus erythematosus have distinct gene expression signatures

P Z Brohawn  1 K Streicher  1 B W Higgs  1 C Morehouse  1 H Liu  1 G Illei  1 K Ranade  1
Affiliations
Clinical Trial

Type I interferon gene signature test-low and -high patients with systemic lupus erythematosus have distinct gene expression signatures

P Z Brohawn et al. Lupus. 2019 Nov.

Abstract

Objectives: Type I interferon (IFN) is implicated in systemic lupus erythematosus (SLE) pathogenesis. We aimed to identify type I IFN signaling-dependent and -independent molecular pathways in a large population of patients with SLE.

Methods: Baseline blood samples from adult patients with moderate to severe SLE from two Phase IIb studies (NCT01438489, n = 265; NCT01283139, n = 416) were profiled using whole transcriptome array analyses. Type I IFN gene signature (IFNGS) test status (high or low) was determined using a validated qualitative polymerase chain reaction-based test. IFN-type-specific signatures were developed by stimulating healthy blood with IFN-β, IFN-γ, IFN-λ, IFN-ω, or pooled IFN-α. These, and multiple literature-derived cell type and cytokine pathway signatures, were evaluated in individual and pooled study populations. A Fisher's exact test was used for associations, adjusted for false discovery rate.

Results: Whole blood samples from IFNGS test-high patients were enriched versus IFNGS test-low patients for CD40L signaling (Q < 0.001), CXC cytokine (Q < 0.001), TLR8-mediated monocyte activation (Q < 0.001), IgG (Q < 0.001), major histocompatibility complex class I (Q < 0.001), and plasma cell (Q < 0.001) gene expression signatures. IFNGS test-low patients had significant enrichment of eosinophil (Q < 0.001), IFN-γ-specific (Q = 0.005), and T-cell or B-cell (Q < 0.001) signatures. Similar enrichment profiles were demonstrated in patients with primary Sjögren's syndrome, systemic sclerosis, and dermatomyositis.

Conclusions: IFNGS test-high patients overexpressed many gene signatures associated with SLE pathogenesis compared with IFNGS test-low patients, reflecting broad immune activation. These results provide new insights into the molecular heterogeneity underlying SLE pathogenesis, highlighting shared mechanisms beyond type I IFN, across several autoimmune diseases.

Trial registration: Clinicaltrials.gov: NCT01438489 and NCT01283139.

Keywords: Anifrolumab; disease pathogenesis; systemic lupus erythematosus; transcriptomics; type I IFN.

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