Biphasic regulation by bile acids of dermal fibroblast proliferation through regulation of cAMP production and COX-2 expression level

Jian, Meng; Ceryak, Susan; Aratsu, Zaheer; Jones, L.; Epstein, Lauren; Bouscarel, Bernard

doi:10.1152/ajpcell.00011.2006

Cited by 16 publications

(6 citation statements)

References 56 publications

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“…Extrapolation of data from cancer studies (40)(41)(42)(43)(44)(45) suggested the possibility that a CDCA-Wnt/␤-catenin or a CDCA-COX2-Wnt/␤-catenin pathway might function in the healthy intestinal epithelium and drive AMPP synthesis. Expression of Ptgs2 (Cox2) in the ileum was in fact upregulated by CDCA feeding (Fig.…”

Section: Resultsmentioning

confidence: 99%

Bile Acid Administration Elicits an Intestinal Antimicrobial Program and Reduces the Bacterial Burden in Two Mouse Models of Enteric Infection

et al. 2017

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In addition to their chemical antimicrobial nature, bile acids are thought to have other functions in the homeostatic control of gastrointestinal immunity. However, those functions have remained largely undefined. In this work, we used ileal explants and mouse models of bile acid administration to investigate the role of bile acids in the regulation of the intestinal antimicrobial response. Mice fed on a diet supplemented with 0.1% chenodeoxycholic acid (CDCA) showed an upregulated expression of Paneth cell ␣-defensins as well as an increased synthesis of the type-C lectins Reg3b and Reg3g by the ileal epithelium. CDCA acted on several epithelial cell types, by a mechanism independent from farnesoid X receptor (FXR) and not involving STAT3 or ␤-catenin activation. CDCA feeding did not change the relative abundance of major commensal bacterial groups of the ileum, as shown by 16S analyses. However, administration of CDCA increased the expression of ileal Muc2 and induced a change in the composition of the mucosal immune cell repertoire, decreasing the proportion of Ly6G ϩ and CD68 ϩ cells, while increasing the relative amount of IgG ϩ B cells. Oral administration of CDCA to mice attenuated infections with the bile-resistant pathogens Salmonella enterica serovar Typhimurium and Citrobacter rodentium, promoting lower systemic colonization and faster bacteria clearance, respectively. Our results demonstrate that bile acid signaling in the ileum triggers an antimicrobial program that can be potentially used as a therapeutic option against intestinal bacterial infections.

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Section: Resultsmentioning

confidence: 99%

Bile Acid Administration Elicits an Intestinal Antimicrobial Program and Reduces the Bacterial Burden in Two Mouse Models of Enteric Infection

et al. 2017

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“…Activation of adenylate cyclase by bile acids increases cellular cAMP in many cells (21)(22)(23); however, whether this occurs in hepatocytes is unknown. Because taurocholate-accelerated canalicular network formation is adenylate cyclase-dependent ( Fig.…”

Section: Resultsmentioning

confidence: 99%

Bile acid stimulates hepatocyte polarization through a cAMP-Epac-MEK-LKB1-AMPK pathway

Wakabayashi

Lippincott‐Schwartz

et al. 2011

Proc. Natl. Acad. Sci. U.S.A.

124

115

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This study describes a unique function of taurocholate in bile canalicular formation involving signaling through a cAMP-Epac-MEK-Rap1-LKB1-AMPK pathway. In rat hepatocyte sandwich cultures, polarization was manifested by sequential progression of bile canaliculi from small structures to a fully branched network. Taurocholate accelerated canalicular network formation and concomitantly increased cAMP, which were prevented by adenyl cyclase inhibitor. The cAMP-dependent PKA inhibitor did not prevent the taurocholate effect. In contrast, activation of Epac, another cAMP downstream kinase, accelerated canalicular network formation similar to the effect of taurocholate. Inhibition of Epac downstream targets, Rap1 and MEK, blocked the taurocholate effect. Taurocholate rapidly activated MEK, LKB1, and AMPK, which were prevented by inhibition of adenyl cyclase or MEK. Our previous study showed that activated-LKB1 and AMPK participate in canalicular network formation. Linkage between bile acid synthesis, hepatocyte polarization, and regulation of energy metabolism is likely important in normal hepatocyte development and disease.primary hepatocytes | occludin | P-glycoprotein H epatocytes, the major epithelial cells in the liver, are polarized. Tight junction proteins, including occludin, claudin, and ZO-1, seal the canalicular lumen, thereby separating apical and basolateral membrane domains and forming the bile canaliculus (1). Polarization is essential for biliary secretion. The mechanisms of polarization are complex and include cytoskeletal, tight junctional, and intracellular trafficking components (2-5). Loss of polarity causes bile secretory failure (cholestasis) and liver damage (6).Bile acids are synthesized from cholesterol in hepatocytes, secreted by ABCB11 (Bsep) into the bile canaliculus, and then mostly absorbed into the enterohepatic circulation (7). The major bile acids in mammals are tauro or glycine conjugates of cholic, deoxycholic, and chenodeoxycholic acids (8). In addition to their traditional function in emulsification of dietary fat (8), recent studies reveal that bile acids function as signaling molecules (9), which increase calcium mobilization (10) and cellular cAMP (9); translocate and activate protein kinase C (11), nuclear farnesoid X receptor (FXR), and pregnane X receptors (PXR) (7, 9); activate PI3K/AKT/glycogen synthase kinase 3 (GSK3) (12); and enhance liver regeneration (13).During embryonic development, early fetal hepatocytes are not polarized (14-16). In fetal mice and rats, infrequent small canaliculi are present, but do not attain an adult appearance until several days postpartum (17). Bile acid synthesis, turnover, and secretion are sparse in fetal liver, and rapidly increase postnatally (18,19), concomitant with hepatocyte polarization and development of a branched canalicular network. Based on these events, we postulated that bile acids may regulate hepatocyte polarization and canalicular formation. Using collagen sandwich cultures of rat primary hepatocytes, we confirmed this hy...

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“…In contrast, we found that dermal fibroblasts are less sensitive to the antimitogenic effect of PGE 2 than gingival fibroblasts. Prostaglandin E 2 inhibits proliferation of many cell types, including fibroblasts from various sources (7)(8)(9)(10)(11)(12)(13)(14)(15)(16)(17)(18), and in several of these cells it was shown to operate via the EP 2 receptor and cAMP generation (10,12,14,(16)(17)(18). Like GFs (48), DFs express all four EP receptors (49) and, since PGE 2 causes cAMP production in DFs (50), it is reasonably safe to assume that EP 2 also mediates the inhibitory effect of PGE 2 on DF proliferation.…”

Section: Discussionmentioning

confidence: 99%

“…However, exaggerated local production of PGs due to trauma or infection of the wound may interfere with proper cutaneous healing. In addition to its recognized role in the inflammation per se , PGE 2 has documented antiproliferative effects on gingival (7–10) and dermal fibroblasts (11,12) as well as on fibroblasts from other sources [tendon (13), lung (14), embryonic (15) and liver (16)] and on other cell types, such as gastric carcinoma cells (17) and arterial smooth muscle cells (18). Interestingly, there are no solid data on whether PGE 2 affects the proliferation of gingival epithelial cells (keratinocytes).…”

mentioning

confidence: 99%

Differential effects of prostaglandin E2 and enamel matrix derivative on the proliferation of human gingival and dermal fibroblasts and gingival keratinocytes

Weinberg

Topaz

Dard

et al. 2010

Journal of Periodontal Research

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Biphasic regulation by bile acids of dermal fibroblast proliferation through regulation of cAMP production and COX-2 expression level

Cited by 16 publications

References 56 publications

Bile Acid Administration Elicits an Intestinal Antimicrobial Program and Reduces the Bacterial Burden in Two Mouse Models of Enteric Infection

Bile Acid Administration Elicits an Intestinal Antimicrobial Program and Reduces the Bacterial Burden in Two Mouse Models of Enteric Infection

Bile acid stimulates hepatocyte polarization through a cAMP-Epac-MEK-LKB1-AMPK pathway

Differential effects of prostaglandin E2 and enamel matrix derivative on the proliferation of human gingival and dermal fibroblasts and gingival keratinocytes

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