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IBD

REVIEWED BY
Bill Maish, MD
Clinical Content Consultant
Published
May 31, 2026
Last updated
May 30, 2026
Key takeaway:

Blood testing for IBD (Crohn's disease or ulcerative colitis) measures CRP, ESR, albumin, FAR, and CAR to quantify intestinal inflammation without invasive procedures. Healthy ranges include CRP under 3–5 mg/L, ESR under 20 mm/hr, and albumin 3.5–5.0 g/dL; elevated CAR and FAR with low albumin are associated with greater disease severity. Tracking these five markers together may help support assessment of disease trajectory and systemic impact.

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Table of contents

Inflammatory Bowel Disease and the Blood Markers That Track It

IBD biomarkers are measurable signals from your immune system and gut that reveal when and how much inflammation is present in Crohn’s disease or ulcerative colitis. They translate invisible intestinal activity into objective information your care team can track, reducing guesswork and complementing symptoms and scans. Blood tests reflect whole-body inflammation and its ripple effects: a liver-made alarm protein (C-reactive protein), the rate red cells settle when inflammation is active (erythrocyte sedimentation rate), shifts in white cells and platelets (leukocytes, thrombocytes), anemia and iron status (hemoglobin, ferritin), and nutrition status (albumin). Stool testing adds a gut-specific readout from neutrophils at the bowel wall (fecal calprotectin). Together, these markers help distinguish IBD from look-alike conditions, gauge disease activity, anticipate flares, guide treatment choice and dosing, and monitor healing—often reducing the need for urgent endoscopy. Biologically, they arise from three places: liver acute-phase responses, immune-cell products, and proteins leaking from an injured intestinal barrier. Watching their patterns over time shows whether inflammation is quieting or smoldering, enabling timely, targeted care that protects the bowel.

Why Bloodwork Matters in IBD

Blood tests for IBD track how active inflammation is—and how it’s affecting the whole body. Inflammatory signals don’t stay in the gut; they alter liver protein production, clotting balance, nutrition status, and immune tone. These biomarkers help distinguish a quiet bowel from a brewing flare, and reveal extra‑intestinal impact on energy, growth, and recovery.CRP is an acute‑phase protein that typically sits under 3 in health (many labs accept under 5–8). ESR in healthy adults is often under 20, trending higher with age and in women. Albumin, a liver‑made carrier protein, usually runs 3.5–5.0, with optimal health toward the middle‑to‑higher end. Ratios such as FAR (fibrinogen‑to‑albumin) and CAR (CRP‑to‑albumin) have no universal reference ranges, but lower values generally indicate low inflammatory burden.When CRP and ESR are low, it suggests mucosal inflammation is minimal and systemic cytokine signaling is quiet—people tend to feel clearer, with steadier energy and fewer fevers or night sweats. By contrast, low albumin often reflects protein loss from an inflamed gut, poor intake, or catabolism, and can show up as swelling, muscle loss, slow wound healing, and in children, slowed growth. Pregnancy physiologically lowers albumin and can raise CRP; ESR runs higher with age and in women, so context matters. Low FAR and CAR are reassuring; higher values point to more active inflammation and catabolic stress, often paralleling abdominal pain, diarrhea, bleeding, and weight loss.Big picture, these markers integrate immune activity with liver synthesis, vascular inflammation, and nutrition—systems that shape bone health, anemia risk, clotting tendency, and long‑term complications of IBD. Regular measurement helps map disease trajectory and whole‑body impact over time.

What Inflammatory Markers Show and What They Miss

Inflammatory Bowel Disease (IBD) blood testing provides a window into how inflammation is affecting your body’s core systems—immunity, metabolism, nutrient absorption, and even energy production. Chronic inflammation in IBD can disrupt these interconnected processes, impacting everything from cardiovascular health to cognitive function. At Superpower, we measure five key biomarkers: C-reactive protein (CRP), erythrocyte sedimentation rate (ESR), albumin, fibrinogen-to-albumin ratio (FAR), and CRP-to-albumin ratio (CAR).CRP and ESR are markers of systemic inflammation. CRP rises quickly in response to inflammation, while ESR reflects more gradual changes. Both are commonly elevated during IBD flares, signaling active immune system engagement. Albumin is a major blood protein produced by the liver; low levels can indicate inflammation, poor nutrition, or protein loss through the gut, all of which are concerns in IBD. FAR and CAR are calculated ratios that combine these markers, offering a more nuanced view of inflammation and protein status.When these biomarkers are within healthy ranges, it suggests that inflammation is controlled, the immune system is stable, and the body’s protein reserves are adequate—key factors for maintaining gut integrity and overall resilience in IBD. Shifts outside the expected range can signal increased disease activity or complications, reflecting how well your body is coping with the demands of chronic inflammation.Interpretation of these results depends on context. Factors like age, pregnancy, recent infections, other illnesses, medications, and even laboratory methods can influence these markers. Results should always be considered alongside your clinical history and symptoms.

FAQs

It’s a blood check that tracks whole-body inflammation and protein status to understand IBD activity. Superpower tests your blood for CRP, ESR, Albumin, and the inflammation-to-protein ratios CAR (CRP/Albumin) and FAR (Fibrinogen/Albumin). CRP rises quickly with active inflammation (acute-phase response). ESR changes more slowly and reflects red cell settling in inflammatory states. Albumin often falls when inflammation is persistent or when there’s protein loss or poor intake. CAR and FAR integrate inflammatory burden against protein reserves, sharpening the picture of disease activity.

It quantifies inflammatory burden and protein status so you can track disease activity, gauge flare severity, and monitor response to therapy. CRP and ESR capture systemic inflammation; Albumin reflects the body’s protein reserve and negative acute-phase response; CAR and FAR combine these signals to improve risk assessment. Together, these markers help distinguish active inflammation from remission, flag complications, and complement stool tests and imaging without replacing endoscopy when needed.

Yes. With Superpower, our team member can organize a professional blood draw in your home. Your sample is collected by venipuncture, processed by accredited labs, and your CRP, ESR, Albumin, CAR, and FAR results are reported to your dashboard. It’s convenient, controlled, and designed to minimize delays between collection and analysis.

Testing frequency tracks disease dynamics. During a flare, right after diagnosis, or when treatments change, testing is typically more frequent to confirm trend direction and treatment effect. In stable remission, periodic surveillance is common to confirm low inflammatory burden and adequate protein status. Trends over time are more informative than any single result, and timing should align with your clinician’s monitoring plan.

Any acute inflammation can raise CRP, ESR, CAR, and FAR, including infections, injuries, or recent surgery. Anemia, pregnancy, and age can elevate ESR independently. Albumin can fall with inflammation, liver disease, kidney protein loss, or dilution from overhydration; it can appear higher with dehydration. Obesity and smoking can raise CRP. Corticosteroids and biologics can suppress inflammatory markers even when symptoms are present.

No special preparation is required. These are non-fasting tests. Aim for your usual routine so results reflect your baseline physiology. Stay normally hydrated. Do not stop prescribed medicines unless your clinician has told you to. If you recently had an infection, surgery, or intense exercise, tell your care team because those can shift inflammatory markers.

References

  1. Mosli, M. H., Zou, G., Garg, S. K., Feagan, S. G., MacDonald, J. K., Chande, N., Sandborn, W. J., & Feagan, B. G. (2015). C-reactive protein, fecal calprotectin, and stool lactoferrin for detection of endoscopic activity in symptomatic inflammatory bowel disease patients: A systematic review and meta-analysis. The American Journal of Gastroenterology, 110(6), 802-819. https://doi.org/10.1038/ajg.2015.120
  2. Rubin, D. T., Ananthakrishnan, A. N., Siegel, C. A., Barnes, E. L., & Long, M. D. (2025). ACG clinical guideline update: Ulcerative colitis in adults. The American Journal of Gastroenterology, 120(6), 1187-1224. https://doi.org/10.14309/ajg.0000000000003463
  3. Lichtenstein, G. R., Loftus, E. V., Afzali, A., & Cohen, R. D. (2025). ACG clinical guideline: Management of Crohn's disease in adults. The American Journal of Gastroenterology, 120(6), 1225-1264. https://doi.org/10.14309/ajg.0000000000003465
  4. Vermeire, S., Van Assche, G., & Rutgeerts, P. (2004). C-reactive protein as a marker for inflammatory bowel disease. Inflammatory Bowel Diseases, 10(5), 661-665. https://doi.org/10.1097/00054725-200409000-00026
  5. National Institute of Diabetes and Digestive and Kidney Diseases. (2024). Crohn's disease. https://www.niddk.nih.gov/health-information/digestive-diseases/crohns-disease

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