Zhang, Xiaoying; Jin, Tao; Shi, Na; Yao, Linbo; Yang, Xinmin; Han, Chenxia; Wen, Li; Du, Dan; Szatmary, Peter; Mukherjee, Rajarshi; Liu, Tingting; Xia, Qing; Criddle, David N.; Huang, Wei; Chvanov, Michael; Sutton, Robert

doi:10.3389/fphys.2018.01922

Results

Title: Mechanisms of Pancreatic Injury Induced by Basic Amino Acids Differ Between L -Arginine, L -Ornithine, and L -Histidine.
Authors: Zhang, Xiaoying; Jin, Tao; Shi, Na; Yao, Linbo; Yang, Xinmin; Han, Chenxia; Wen, Li; Du, Dan; Szatmary, Peter; Mukherjee, Rajarshi; Liu, Tingting; Xia, Qing; Criddle, David N.; Huang, Wei; Chvanov, Michael; Sutton, Robert
Abstract: Pancreatic acinar cells require high rates of amino acid uptake for digestive enzyme synthesis, but excessive concentrations can trigger acute pancreatitis (AP) by mechanisms that are not well understood. We have used three basic natural amino acids L-arginine, L-ornithine, and L-histidine to determine mechanisms of amino acid-induced pancreatic injury and whether these are common to all three amino acids. Caffeine markedly inhibited necrotic cell death pathway activation in isolated pancreatic acinar cells induced by L-arginine, but not L-ornithine, whereas caffeine accelerated L-histidine-induced cell death. Both necroptosis inhibitors of RIPK1 and RIPK3 and a necroptosis activator/apoptosis inhibitor z-VAD increased cell death caused by L-histidine, but not L-arginine or L-ornithine. Cyclophilin D knock-out (Ppif-/-) significantly attenuated cell death induced by L-histidine, but not L-arginine, or L-ornithine. Allosteric modulators of calcium-sensing receptor (CaSR) and G-protein coupled receptor class C group 6 member A (GPRC6A) had inhibitory effects on cell death induced by L-arginine but not L-ornithine or L-histidine. We developed a novel amino acid-induced AP murine model with high doses of L-histidine and confirmed AP severity was significantly reduced in Ppif-/- vs. wild type mice. In L-arginine-induced AP neither Ppif-/-, caffeine, or allosteric modulators of CaSR or GPRC6A reduced pancreatic damage, even though CaSR inhibition with NPS-2143 significantly reduced pancreatic and systemic injury in caerulein-induced AP. These findings demonstrate marked differences in the mechanisms of pancreatic injury induced by different basic amino acids and suggest the lack of effect of treatments on L-arginine-induced AP may be due to conversion to L-ornithine in the urea cycle.
Subjects: PANCREATIC injuries; AMINO acids; CELL death; CAFFEINE; PANCREATIC diseases
Publication: Frontiers in Physiology, 2019, pN.PAG
ISSN: 1664-042X
Publication type: Academic Journal
DOI: 10.3389/fphys.2018.01922

Mechanisms of Pancreatic Injury Induced by Basic Amino Acids Differ Between L -Arginine, L -Ornithine, and L -Histidine.

Zhang, Xiaoying; Jin, Tao; Shi, Na; Yao, Linbo; Yang, Xinmin; Han, Chenxia; Wen, Li; Du, Dan; Szatmary, Peter; Mukherjee, Rajarshi; Liu, Tingting; Xia, Qing; Criddle, David N.; Huang, Wei; Chvanov, Michael; Sutton, Robert

PANCREATIC injuries; AMINO acids; CELL death; CAFFEINE; PANCREATIC diseases

Frontiers in Physiology, 2019, pN.PAG

1664-042X

Academic Journal

10.3389/fphys.2018.01922