Systemic Lupus Erythematosus (SLE)

Biomarkers for systemic lupus erythematosus (SLE)

Systemic lupus erythematosus (SLE) is a complex and heterogeneous autoimmune disease marked by episodic flares, multi-organ involvement, and progressive tissue damage driven by both immune activation and impaired resolution. Despite advances in serological testing, conventional biomarkers often fail to reflect the dynamic tissue-level changes occurring during disease progression.

Moreover, they offer limited ability to distinguish between distinct organ-specific manifestations, making treatment decisions and response monitoring challenging in clinical practice.There is a growing need for biomarkers that can capture disease activity at the tissue level, support endotyping, and enable precision medicine approaches in SLE.

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Biomarkers for systemic lupus erythematosus (SLE)

Nordic ProteinFingerPrint Technology™ offers a way to monitor extracellular matrix (ECM) turnover—an essential component of chronic inflammation and fibrotic progression in lupus.

Our biomarkers enable quantification of tissue degradation, formation, and resolution in affected organs such as kidneys, lungs, and skin.

By capturing this tissue-level remodeling, our biomarkers provide deeper biological insight into disease activity and endotypes, with the potential to guide treatment selection and predict response.

Browse our list of SLE biomarkers

Serum markers of fibrosis and basement membrane turnover are elevated in SLE and LN

Measuring biomarkers of ECM turnover provides a non-invasive means to assess disease activity and underlying tissue pathology. NordicPRO-C3™ indicates type III collagen formation and active fibrogenesis. LG1M reflects laminin degradation, signaling basement membrane disruption from inflammatory protease activity.

C4M quantifies type IV collagen degradation and indicates basement membrane remodeling and tissue injury. TUM (tumstatin), a matrikine released during type IV collagen degradation, serves as a marker of vascular ECM remodeling and endothelial dysfunction. Together, these biomarkers capture distinct but complementary aspects of SLE pathology, including fibrosis, basement membrane turnover, and vascular involvement.

Figure 1. ECM turnover biomarkers are elevated in SLE compared to healthy controls.

In lupus nephritis (LN), specific ECM biomarkers can provide insights into renal tissue remodeling and disease progression. NordicPRO-C6™ reflects the formation of type VI collagen, which is particularly enriched in the renal interstitium. Elevated levels of nordicPRO-C6™ suggest ongoing interstitial fibrogenesis, a key process associated with chronic kidney damage and a predictor of progression in LN.TUM is relevant in LN due to its association with basement membrane remodeling and its potential link to glomerular injury and vascular dysfunction. Together, these markers can help identify active fibrotic and vascular processes in the kidney, supporting their use in monitoring LN disease activity and progression.

Figure 2. Urinary ECM-turnover biomarkers are elevated in LN

Browse our list of SLE biomarkers

About systemic lupus erythematosus (SLE)

  • SLE is a chronic autoimmune disease characterized by widespread inflammation and damage across multiple organ systems. SLE is highly heterogeneous, with clinical manifestations ranging from mild cutaneous symptoms to severe organ-threatening complications involving the kidneys, lungs, heart, and central nervous system.

    The hallmark of SLE is immune system dysregulation, where the body produces autoantibodies targeting nuclear, cytoplasmic, and cell surface antigens. These immune complexes deposit in tissues and trigger a sustained inflammatory response, leading to tissue damage. The unpredictable nature of disease flares and remission cycles adds complexity to disease management and increases the risk of cumulative organ damage over time.

  • Clinically, SLE presents with a wide spectrum of symptoms, including fatigue, joint pain, skin rashes, photosensitivity, and serositis. Severe cases may involve nephritis, pulmonary involvement, cardiovascular complications, and neuropsychiatric manifestations. Disease progression and organ involvement vary significantly between individuals, contributing to the overall challenge of diagnosis and treatment.

  • Management of SLE aims to control inflammation, prevent flares, and protect organs from damage. Treatment strategies often include corticosteroids, antimalarials, immunosuppressive agents, and targeted biologic therapies. Early diagnosis, regular monitoring, and individualized treatment approaches are critical for improving long-term outcomes and quality of life for patients living with SLE.

  • Biomarkers provide valuable insight into the biological processes driving disease activity in SLE. They offer a non-invasive way to track tissue damage, inflammation, and fibrotic progression—especially when traditional biomarkers fall short in capturing disease heterogeneity or predicting flares.

  • Unlike conventional tests, these biomarkers directly measure tissue remodeling processes, enabling more accurate disease activity assessment, patient endotyping, and evaluation of treatment responses—all essential for advancing precision medicine in SLE.

    In lupus nephritis, biomarkers like NordicPRO-C6™ and TUM help detect interstitial fibrosis and glomerular injury. Measuring these markers in serum or urine provides a non-invasive tool to monitor disease activity, guide treatment, and predict long-term kidney outcomes.

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