Pirfenidone increases IL-10 and improves acute pancreatitis in multiple clinically relevant murine models
Ejas Palathingal Bava, John George, Mohammad Tarique, Srikanth Iyer, Preeti Sahay, Beatriz Gomez Aguilar, Dujon B. Edwards, Bhuwan Giri, Vrishketan Sethi, Tejeshwar Jain, Prateek Sharma, Utpreksha Vaish, Harrys K. C. Jacob, Anthony Ferrantella, Craig L. Maynard, Ashok K. Saluja, Rajinder K. Dawra, Vikas Dudeja
Ejas Palathingal Bava, John George, Mohammad Tarique, Srikanth Iyer, Preeti Sahay, Beatriz Gomez Aguilar, Dujon B. Edwards, Bhuwan Giri, Vrishketan Sethi, Tejeshwar Jain, Prateek Sharma, Utpreksha Vaish, Harrys K. C. Jacob, Anthony Ferrantella, Craig L. Maynard, Ashok K. Saluja, Rajinder K. Dawra, Vikas Dudeja
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Research Article Gastroenterology Inflammation

Pirfenidone increases IL-10 and improves acute pancreatitis in multiple clinically relevant murine models

Abstract

Despite decades of research, there is no specific therapy for acute pancreatitis (AP). In the current study, we have evaluated the efficacy of pirfenidone, an antiinflammatory and antifibrotic agent that is approved by the FDA for treatment of idiopathic pulmonary fibrosis (IPF), in ameliorating local and systemic injury in AP. Our results suggest that treatment with pirfenidone in therapeutic settings (e.g., after initiation of injury), even when administered at the peak of injury, reduces severity of local and systemic injury and inflammation in multiple models of AP. In vitro evaluation suggests that pirfenidone decreases cytokine release from acini and macrophages and disrupts acinar-macrophage crosstalk. Therapeutic pirfenidone treatment increases IL-10 secretion from macrophages preceding changes in histology and modulates the immune phenotype of inflammatory cells with decreased levels of inflammatory cytokines. Antibody-mediated IL-10 depletion, use of IL-10–KO mice, and macrophage depletion experiments confirmed the role of IL-10 and macrophages in its mechanism of action, as pirfenidone was unable to reduce severity of AP in these scenarios. Since pirfenidone is FDA approved for IPF, a trial evaluating the efficacy of pirfenidone in patients with moderate to severe AP can be initiated expeditiously.

Authors

Ejas Palathingal Bava, John George, Mohammad Tarique, Srikanth Iyer, Preeti Sahay, Beatriz Gomez Aguilar, Dujon B. Edwards, Bhuwan Giri, Vrishketan Sethi, Tejeshwar Jain, Prateek Sharma, Utpreksha Vaish, Harrys K. C. Jacob, Anthony Ferrantella, Craig L. Maynard, Ashok K. Saluja, Rajinder K. Dawra, Vikas Dudeja

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Figure 9

Therapeutic pirfenidone does not reduce proinflammatory cytokines in the absence of IL-10 in the L-arginine model.

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Therapeutic pirfenidone does not reduce proinflammatory cytokines in the...
(AJ) Quantification of the mRNA levels of TNF-α, IL-6, IL-12α, iNOS, IL-23, IFN-γ, TGF-β2, MMP-9, COX-2, and NLRP3 demonstrates that pirfenidone is unable to reduce their levels in the presence of IL-10 neutralization. (K and L) Multi-Analyte Flow Assay for cytokines TNF-α and IL-17 in serum is in agreement with the notion that pirfenidone is not able to reduce their levels in the presence of IL-10 neutralization. Pirf., pirfenidone; IL-10 Ab, IL-10 neutralizing antibody. Data represent mean ± SEM and n =5 in each group. *P < 0.05 by Kruskal-Wallis test (Dunn’s multiple-comparison test).