Substance P treatment stimulates chemokine synthesis in pancreatic acinar cells via the activation of NF-{kappa}B

doi:10.1152/ajpgi.00177.2006

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Am J Physiol Gastrointest Liver Physiol 291: G1113-G1119, 2006. First published July 27, 2006; doi:10.1152/ajpgi.00177.2006
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Substance P treatment stimulates chemokine synthesis in pancreatic acinar cells via the activation of NF- ${kappa}$ B

Raina Devi Ramnath and Madhav Bhatia

Department of Pharmacology, National University of Singapore, Singapore

Submitted 28 April 2006 ; accepted in final form 23 July 2006

Acinar cell injury early in acute pancreatitis leads to a localinflammatory reaction and to the subsequent systemic inflammatoryresponse, which may result in multiple organ dysfunction anddeath. Inflammatory mediators, including chemokines and substanceP (SP), are known to play a crucial role in the pathogenesisof acute pancreatitis. It has been shown that pancreatic acinarcells produce the chemokine monocyte chemoattractant protein-1(MCP-1) in response to caerulein hyperstimulation, demonstratingthat acinar-derived MCP-1 is an early mediator of inflammationin acute pancreatitis. Similarly, SP levels in the pancreasand pancreatic acinar cell expression of neurokinin-1 receptor,the primary receptor for SP, are both increased during secretagogue-inducedexperimental pancreatitis. This study aims to examine the functionalconsequences of exposing mouse pancreatic acinar cells to SPand to determine whether it leads to proinflammatory signaling,such as production of chemokines. Exposure of mouse pancreaticacini to SP significantly increased synthesis of MCP-1, macrophageinflammatory protein-1 ${alpha}$ (MIP-1 ${alpha}$ ), as well as MIP-2. Furthermore,SP also increased NF- ${kappa}$ B activation. The stimulatory effect ofSP was specific to chemokine synthesis through the NF- ${kappa}$ B pathway,since the increase in chemokine production was completely attenuatedwhen pancreatic acini were pretreated with the selective NF- ${kappa}$ Binhibitor NF- ${kappa}$ B essential modulator-binding domain peptide. Thisstudy shows that SP-induced chemokine synthesis in mouse pancreaticacinar cells is NF- ${kappa}$ B dependent.

pancreatitis; monocyte chemoattractant protein-1; macrophage inflammatory protein-1 ${alpha}$ ; macrophage inflammatory protein-2; neurokinin-1 receptor

Address for reprint requests and other correspondence: M. Bhatia, Dept. of Pharmacology, National Univ. of Singapore, Yong Loo Lin School of Medicine, Bldg. MD2, 18 Medical Dr., Singapore 117597 (e-mail: mbhatia{at}nus.edu.sg)

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Substance P treatment stimulates chemokine synthesis in pancreatic acinar cells via the activation of NF-B

Substance P treatment stimulates chemokine synthesis in pancreatic acinar cells via the activation of NF- ${kappa}$ B