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vedolizumab PubMed monitoring Monitoring

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Evidence Scanner:
vedolizumab PubMed monitoring
Abstracts analysis summary

🫀 Vedolizumab shines in early Crohn's disease: LOVE-CD phase 4 results

🧪 What was studied — Phase 4 open-label cohort (n=260; 86 early, 174 late Crohn's, 22 centres, Europe). Patients with moderate-severe Crohn’s received IV vedolizumab for 1 year. Comparison: early (<2 years, biologic-naive) vs late (>2 years, prior anti-TNF) disease. Endpoints: dual clinical (CDAI ≤150) and endoscopic (SES-CD <4) remission at weeks 26 & 52; safety.

📈 Key results — Clinical+endoscopic remission achieved in 31.4% (27/86) early vs. 8.6% (15/174) late CD (diff 22.8%, 95% CI 12.6-33.7). Serious adverse events substantially less frequent in early disease (3.5% vs 26.4%), with lower infections, surgery, and malignancy.

📍 What this changes in practice


  • Initiate vedolizumab early in biologic-naive Crohn’s for best remission outcomes.
  • Expect fewer complications and superior safety in early-stage patients.
  • Practical for moderate-severe, ulcerative cases with short disease duration.

🔗 Source — PubMed | DOI

🫀 US real-world data: Very low TB risk for vedolizumab & other advanced therapies in IBD

🔥 Main in 3 points


  • Tuberculosis rates on vedolizumab, anti-TNFs, and ustekinumab all <40/100,000 person-years
  • No significant difference between drug classes (HR 1.16, 95% CI 0.41–3.31)
  • Low TB incidence with all agents in US clinical practice

🧪 Context — US registry study (n=20,705 IBD patients on advanced therapies, 2014–2022). Incidence and comparative risk of TB after biologic/JAK therapy launch.

📍 Practical significance —


  • Baseline TB screening remains essential, but overall risk is minimal in low-incidence areas.
  • Vedolizumab and other advanced therapies can be safely prescribed without extra TB concern in the US.

🔗 Source — PubMed | DOI

🫀 Genotype-guided IBD management: IL10 variant linked to biologic success

🔥 Main in 3 points


  • IL10 rs1800896 variant independently predicts higher remission rates with biologic therapy (aOR = 4.15, 95% CI: 1.49-11.56)
  • Genotyping key cytokine SNVs can help individualise IBD therapy
  • No such links found for TNFA, TGFB, or IL6 SNVs

🧪 Context — Italian cohort (n=197, CD/UC patients; prospective, 12-months follow-up) on biologics; outcome biochemical remission at 1 year.

📍 Practical significance —


  • Consider genetic profiling for patients starting biologics—IL10 rs1800896 status may help predict remission odds and tailor therapy decisions.

🔗 Source — PubMed | DOI
Medical Advisers's Group
MAG | Medical Adviser’s Group, France
Contact:
mdwrt.com
+33 6 32 14 87 09
yakov@mdwrt.com
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