Abstract
Cholecystokinin (CCK) and other pancreatic secretagogues have recently been shown to activate signaling kinase cascades in pancreatic acinar cells, leading to the activation of extracellular signal-regulated kinases and Jun N-terminal kinases. We now show the presence of a third kinase cascade activating p38 mitogen-activated protein (MAP) kinase in isolated rat pancreatic acini. CCK and osmotic stress induced by sorbitol activated p38 MAP kinase within minutes; their effects were dose-dependent, with maximal activation of 2.8- and 4.4-fold, respectively. The effects of carbachol and bombesin on p38 MAP kinase activity were similar to those of CCK, whereas phorbol ester, epidermal growth factor, and vasoactive intestinal polypeptide stimulated p38 MAP kinase by 2-fold or less. Both CCK and sorbitol also increased the tyrosyl phosphorylation of p38 MAP kinase. Using the specific inhibitor of p38 MAP kinase, SB 203580, we found that p38 MAP kinase activity was required for MAP kinase-activated protein kinase-2 activation in pancreatic acini. SB 203580 reduced the level of basal phosphorylation and blocked the increased phosphorylation of Hsp 27 after stimulation with either CCK or sorbitol. CCK treatment induced an initial rapid decrease in total F-actin content of acini, followed by an increase after 40 min. Preincubation with SB 203580 significantly inhibited these changes in F-actin content. Staining of the actin cytoskeleton with rhodamine-conjugated phalloidin and analysis by confocal fluorescence microscopy showed disruption of the actin cytoskeleton after 10 and 40 min of CCK stimulation. Pretreatment with SB 203580 reduced these changes. These findings demonstrate that the activation of p38 MAP kinase is involved not only in response to stress, but also in physiological signaling by gastrointestinal hormones such as CCK, where activation of Gq-coupled receptors stimulates a cascade in which p38 MAP kinase activates MAP kinase-activated protein kinase-2, resulting in Hsp 27 phosphorylation. Activation of p38 MAP kinase, most likely through phosphorylation of Hsp 27, plays a role in the organization of the actin cytoskeleton in pancreatic acini.
Highlights
CCK1 regulates a variety of pancreatic functions, including secretion of pancreatic enzymes (1), stimulation of pancreatic growth (2, 3), and synthesis of digestive enzymes (4)
We recently reported that treatment of isolated rat pancreatic acini with CCK activates ERKs and JNKs, as well as other upstream components of the mitogen-activated protein (MAP) kinase signaling cascade, including Ras and MEK1/MEK2 (6, 7, 47, 48)
We have demonstrated that CCK activates p38 MAP kinase and that this activation leads to activation of MAPKAP kinase-2, resulting in an increase in heat shock protein (Hsp) 27 phosphorylation
Summary
CCK1 regulates a variety of pancreatic functions, including secretion of pancreatic enzymes (1), stimulation of pancreatic growth (2, 3), and synthesis of digestive enzymes (4). When acini were stimulated with CCK for varying times, the immunoprecipitated p38 MAP kinase activity was increased by 1 min and reached a maximum after 10 min, when a 2.8 Ϯ 0.1-fold increase was observed (Fig. 2A).
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