Piezo1-mediated stellate cell activation causes pressure-induced pancreatic fibrosis in mice
Sandip M. Swain, Joelle M-J Romac, Steven R. Vigna, Rodger A. Liddle
Sandip M. Swain, Joelle M-J Romac, Steven R. Vigna, Rodger A. Liddle
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Research Article Gastroenterology

Piezo1-mediated stellate cell activation causes pressure-induced pancreatic fibrosis in mice

Abstract

Pancreatic fibrosis is a complication of chronic pancreatitis and is a prominent feature of pancreatic cancer. Pancreatic fibrosis is commonly observed in patients with prolonged pancreatic duct obstruction, which elevates intrapancreatic pressure. We show here that increased pancreatic duct pressure causes fibrosis and describes the mechanism by which pressure increases deposition of extracellular matrix proteins and fibrosis. We found that pancreatic stellate cells (PSCs), the source of the extracellular matrix proteins in fibrosis, express the mechanically activated ion channel Piezo1. By increasing intracellular calcium, mechanical stress or the Piezo1 agonist Yoda1-activated PSCs manifest by loss of perinuclear fat droplets and increased TGF-β1, fibronectin, and type I collagen expression. These effects were blocked by the Piezo1 inhibitor GsMTx4 and absent in PSCs from mice with conditional genetic deletion of Piezo1 in stellate cells, as was pancreatic duct ligation–induced fibrosis. Although TRPV4 has been proposed to have direct mechanosensing properties, we discovered that PSCs from Trpv4-KO mice were protected against Yoda1-triggered activation. Moreover, mice devoid of TRPV4 were protected from pancreatic duct ligation–induced fibrosis. Thus, high pressure within the pancreas stimulates Piezo1 channel opening, and subsequent activation of TRPV4 leads to stellate cell activation and pressure-induced chronic pancreatitis and fibrosis.

Authors

Sandip M. Swain, Joelle M-J Romac, Steven R. Vigna, Rodger A. Liddle

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Figure 7

TRPV4-KO mice were protected from pancreatic duct ligation–induced fibrosis.

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TRPV4-KO mice were protected from pancreatic duct ligation–induced fibro...
(A and D) DIC and Bodipy 493/503–stained images of PSCs from TRPV4-KO mice 24 hours after Yoda1 (25 μM). (B and C) Mean cell area and Feret’s diameter (max) of PSCs 24 hours after Yoda1 (25 μM) (from 3 experiments with 20 cells each). (E) Loss of fat droplets in PSCs following Yoda1 (25 μM) (from 3 experiments and > 100 cells). (F and G) Quantification of collagen type I and fibronectin immunostaining in PSCs from TRPV4-KO mice 4 days after Yoda1 (25 μM). (H and I) Representative images of collagen type I and fibronectin staining for the data shown in F and G. (JM) Pancreatic duct ligation (PDL) at the tail region of the pancreas induced chronic pancreatitis and fibrosis in WT and TRPV4-KO mice. Eight days after PDL, chronic pancreatitis and fibrosis parameters of the tail region included (J) H&E staining, (K) H&E score, (L) Masson’s trichrome staining, and (M) area of WT and TRPV4-KO mice (n = 5). Statistical comparisons were made using 2-tailed Student’s t test. ***P ≤ 0.001. Scale bar: 100 μm.