A positive cytokine/chemokine feedback loop establishes plasmacytoid DC–driven autoimmune pancreatitis in IgG4-related disease
Akane Hara, Tomohiro Watanabe, Kosuke Minaga, Tomoe Yoshikawa, Masayuki Kurimoto, Ikue Sekai, Yasuhiro Masuta, Ryutaro Takada, Yasuo Otsuka, Ken Kamata, Shiki Takamura, Masatoshi Kudo, Warren Strober
Akane Hara, Tomohiro Watanabe, Kosuke Minaga, Tomoe Yoshikawa, Masayuki Kurimoto, Ikue Sekai, Yasuhiro Masuta, Ryutaro Takada, Yasuo Otsuka, Ken Kamata, Shiki Takamura, Masatoshi Kudo, Warren Strober
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Research Article Gastroenterology

A positive cytokine/chemokine feedback loop establishes plasmacytoid DC–driven autoimmune pancreatitis in IgG4-related disease

Abstract

The pathogenesis of the murine model of autoimmune pancreatitis associated with IgG4-related disease (AIP/IgG4-RD) induced by administration of polyinosinic-polycytidylic acid (poly[I:C]) is incompletely understood. While it is known that murine and human AIP/IgG4-RD is driven by plasmacytoid dendritic cells (pDCs) producing IFN-α, the origin of these cells and their relation to effector T cells is not known. Here, we show that murine AIP was initiated by TLR3-bearing conventional DCs in the uninflamed pancreas whose activation by the TLR3 ligand poly(I:C) caused IFN-α, CXCL9, and CXCL10 secretion. This, in turn, induced pancreatic recruitment of CXCR3+ T cells and these T cells, via their secretion of CCL25, facilitated migration of pDCs bearing CCR9 into the pancreas. This established a feedback loop anchored by the now dominant pDC production of IFN-α and the continued CXCR3+ T cell facilitation of pDC migration. Remarkably, the interaction between CXCR3+ T cells and pDCs also existed at the functional level since this interaction enhanced the production of CCL25 and IFN-α by CXCR3+ T cells and pDCs, respectively. Evidence presented here that a similar disease mechanism was present in human AIP/IgG4-RD creates new avenues of disease treatment.

Authors

Akane Hara, Tomohiro Watanabe, Kosuke Minaga, Tomoe Yoshikawa, Masayuki Kurimoto, Ikue Sekai, Yasuhiro Masuta, Ryutaro Takada, Yasuo Otsuka, Ken Kamata, Shiki Takamura, Masatoshi Kudo, Warren Strober

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Figure 1

Blockade of TLR3 by inhibitors prevents the development of experimental autoimmune pancreatitis.

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Blockade of TLR3 by inhibitors prevents the development of experimental ...
MRL/MpJ mice were administered poly(I:C) by intraperitoneal injection twice a week for a total of 16 times to induce experimental autoimmune pancreatitis (AIP). Each poly(I:C) injection was preceded by intraperitoneal injection of saline (PBS, n = 4) or TLR3/dsRNA binding inhibitor (1 mg, n = 4). After sacrifice at 3 hours following the final set of injections, pancreases were removed and analyzed as indicated. (A and B) Hematoxylin and eosin staining of the pancreatic tissues and pathological scores of induced AIP in the 2 groups. Original magnification, ×400. (C) Percentages of plasmacytoid DCs (pDCs), CD3+ T cells, CD11b+ myeloid cells, and CD11c+ DCs within pancreatic mononuclear cells, as determined by flow cytometric analyses. pDCs were defined as PDCA-1+B220lo cells. Left panels: Representative cytometric analysis. Right panels: Bar graphs of cumulative results. (D) Concentrations of IFN-α, IL-33, CXCL9, and CXCL10 in protein extracts of pancreatic tissues from mice without and with TLR3 inhibitor administration, as determined by ELISA. Each dot corresponds to the value in 1 mouse. Statistical analyses were performed using an unpaired, 2-tailed Student’s t test. Results are expressed as mean ± SEM. **P < 0.01.