Identification of inflammatory mediators in patients with Crohn's disease unresponsive to anti-TNFα therapy

Leal, Raquel Franco; Planell, Núria; Kajekar, Radhika; Lozano, Juan José; Ordás, Íngrid; Dotti, Isabella; Esteller, Manel; Masamunt, Maria Carme; Parmar, H.; Ricart, Elena; Panés, Julián; Salas, Antonio

doi:10.1136/gutjnl-2013-306518

Cited by 124 publications

(90 citation statements)

References 41 publications

(31 reference statements)

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“…Interestingly, we found that expression of miR-301a was found to be markedly decreased in the inflamed mucosa of patients with CD from the remission and response groups after IFX induction therapy compared with that before IFX therapy, while no change in miR-301a expression was observed in the failure group (figure 2B, and see online supplementary figure S1A,C,D). Interestingly, a recent report has shown that some pro-inflammatory cytokines such as IL-6 were also downregulated even in patients with CD who did not respond to IFX therapy 29. Since we showed that in vitro stimulation with IL-6 was able to modestly induce miR-301a expression on CD4+ T cells, their findings suggest that IL-6 may be dispensable in miR-301a expression in vivo.…”

Section: Resultssupporting

confidence: 54%

“…Clinical remission was defined as a CDAI score of <150 points, and clinical response as a decrease in the CDAI score ≥70 points at the evaluation time point in comparison with the baseline index. The failure category included all the remaining patients, whose CDAI was not significantly changed or increased 20 28 29. Endoscopic response to IFX therapy was also assessed at week 12 after initial administration and endoscopic variables were scored according to the Simple Endoscopic Severity for CD (SES-CD) as described elsewhere 30 31.…”

Section: Methodsmentioning

confidence: 99%

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miR-301a promotes intestinal mucosal inflammation through induction of IL-17A and TNF-α in IBD

Shi

et al. 2015

Gut

135

103

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Section: Resultssupporting

confidence: 54%

Section: Methodsmentioning

confidence: 99%

miR-301a promotes intestinal mucosal inflammation through induction of IL-17A and TNF-α in IBD

Shi

et al. 2015

Gut

135

103

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“…However, in CD, Leal et al 16 showed by whole-genome transcriptional analysis in colonic mucosa that anti-TNF therapy downregulates a subset of inflammatory genes even in patients who do not achieve endoscopic remission.…”

Section: Discussionmentioning

confidence: 99%

Effect of vedolizumab (anti-α4β7-integrin) therapy on histological healing and mucosal gene expression in patients with UC

Arijs

Hertogh

Lemmens

et al. 2016

Gut

140

122

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Objective Lymphocyte recruitment to the inflamed gut is increased in UC. Inhibition of this cell trafficking by vedolizumab (VDZ) was successful in inducing and maintaining remission and in induction of endoscopic mucosal healing. There are no data on histological healing with VDZ. We studied histological changes following VDZ therapy and compared gene expression in patients with UC before and after therapy. Design Forty-one patients with UC from GEMINI I and LTS were studied before and at three time points (weeks 6/12/52) following VDZ therapy. Colonic biopsies were scored using the Geboes index and correlated with Mayo endoscopic subscore. Gene expression was analysed using Affymetrix gene arrays. Results Fifty-five per cent of patients achieving endoscopic healing (= Mayo endoscopic subscore 0-1) with VDZ at the studied time points also had histological healing (= Geboes grade 0-1). In most healers, some residual histological changes (eg, disturbed architecture and increased mononuclear cell infiltrate) were still observed, although this was less at week 52. VDZ restored expression of many inflammatory genes in patients with endoscopic healing only at week 52 and not before. In VDZ healers, the expression of many genes remained dysregulated at weeks 6/12/52 compared with controls. Conclusions VDZ induces histological healing in >50% of patients with endoscopic healing, with maximal effect at week 52. VDZ also restored, although incompletely, the colonic expression of many immunerelated genes in patients with UC achieving endoscopic healing at week 52. However, persistent histological and gene dysregulations did remain even in healers, suggesting that maintenance therapy will be necessary to control the intestinal inflammation. Trial registration numbers: NCT00783718 and NCT00790933; post-results.

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“…For this reason, optimize the dose is a strategy to regain response to the anti-TNF, as increase the dose (Infliximab -10mg/kg) or decrease the interval between infusions (Infliximab every 4 weeks and Adalimumab 40 mg weekly), before you consider replacing the biological (1) . The chance for another class of therapy is a stated strategy in cases of lack of response to therapy optimization and high levels of circulating antibodies against anti-TNF (1,25,32) . Although, there are no available testes for measure the drug level, neither the detection of antibodies anti-drugs in Brazil, the optimization has been done empirically.…”

Section: Biological Therapymentioning

confidence: 99%

THERAPIES FOR CROHN'S DISEASE: a clinical update

Sobrado

Leal

Sobrado

2016

Arq. Gastroenterol.

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Identification of inflammatory mediators in patients with Crohn's disease unresponsive to anti-TNFα therapy

Cited by 124 publications

References 41 publications

miR-301a promotes intestinal mucosal inflammation through induction of IL-17A and TNF-α in IBD

miR-301a promotes intestinal mucosal inflammation through induction of IL-17A and TNF-α in IBD

Effect of vedolizumab (anti-α4β7-integrin) therapy on histological healing and mucosal gene expression in patients with UC

THERAPIES FOR CROHN'S DISEASE: a clinical update

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