Neuroprotection by endogenous and exogenous PACAP following stroke

Chen, Yun; Samal, Babru; Hamelink, Carol; Xiang, Charlie; Chen, Yong; Chen, Mei; Vaudry, David; Brownstein, Michael J.; Hallenbeck, John M.; Eiden, Lee E.

doi:10.1016/j.regpep.2006.06.016

Cited by 104 publications

(116 citation statements)

References 78 publications

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“…Numerous studies have shown that it plays a crucial role not only during secretion and motility but in immunity and inflammation processes (Azuma et al 2008;Arranz et al 2008;Gomariz et al 2006). Increasing evidence suggests that PACAP-38 has protective effects in I/R models, like in global and focal cerebral ischemia, retinal ischemia, kidney warm ischemia model, cultured cardiomyocytes, and in small bowel transplantation (Atlasz et al 2007;Chen et al 2006;Ohtaki et al 2008;Racz et al 2008;Riera et al 2001;Shioda et al 1998Shioda et al , 2006Reglodi et al 2004;Ferencz et al 2009a). However, there is no data on the effect of endogenous PACAP-38 against warm mesenteric ischemia.…”

Section: Introductionmentioning

confidence: 99%

Comparison of Intestinal Warm Ischemic Injury in PACAP Knockout and Wild-Type Mice

et al. 2010

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Pituitary adenylate cyclase-activating polypeptide (PACAP) is present in the gastrointestinal tract and plays a central role in the intestinal physiology, mainly in the secretion and motility. The aim of our study was to compare the ischemic injury in wild-type and PACAP-38 knockout mice following warm mesenteric small bowel ischemia. Warm ischemia groups were designed with occlusion of superior mesenteric artery for 1, 3, and 6 h in wild-type (n = 10 in each group) and PACAP-38 knockout (n=10 in each group) mice. Small bowel biopsies were collected after laparotomy (control) and at the end of the ischemia periods. To determine oxidative stress parameters, malondialdehyde (MDA), reduced glutathione (GSH), and superoxide dismutase (SOD) were measured. Tissue damage was analyzed by qualitative and quantitative methods on hematoxylin/eosin-stained sections. In PACAP-38 knockout animals, tissue MDA increased significantly after 3 and 6 h ischemia (133.97 ± 6,2; 141.86 ± 5,8) compared to sham-operated (100.92±3,6) and compared to wild-type results (112.8±2,1; 118.4±1.03 μmol/g, p< 0.05). Meanwhile, tissue concentration of GSH and activity of SOD decreased significantly in knockout mice compared to wild-type form (GSH, 795.97±10.4; 665.1±8,8 vs. 893.23±μmol/g; SOD, 94.4±1.4; 81.2±3.9 vs. 208.09± 3,7 IU/g). Qualitative and quantitative histological results showed destruction of the mucous, submucous layers, and crypts in knockout mice compared to wild-type tissues. These processes correlated with the warm ischemia periods. Our present results propose an important protective effect of endogenous PACAP-38 against intestinal warm ischemia, which provides basis for further investigation to elucidate the mechanism of this protective effect.

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Section: Introductionmentioning

confidence: 99%

Comparison of Intestinal Warm Ischemic Injury in PACAP Knockout and Wild-Type Mice

et al. 2010

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“…A significant literature also implicates cAMP in a broad range of neuronal differentiation responses, including neuritogenesis, survival, regeneration, repair, and expression of genes encoding neuron-specific proteins, such as neurotransmitter biosynthetic enzymes, neuropeptides, receptors, and ion channels (Qiu et al, 2002), although the effects of first messengers that regulate cAMP generation in differentiating neurons have not been studied as extensively as receptor tyrosine kinase-stimulating neurotrophins such as NGF. The neuropeptide PACAP has garnered significant interest in this regard, because PACAP is neuritogenic upon exposure to PC12 cells (Deutsch and Sun, 1992), enhances neuronal survival of cerebellar granule cells (Kienlen Campard et al, 1997) and PC12 cells (Tanaka et al, 1996), and is neuroprotective after ischemic injury to the brain (Reglodi et al, 2000;Chen et al, 2006;Ohtaki et al, 2006). PACAP signaling in PC12 cells leading to neuritogenesis is distinct from that of NGF.…”

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confidence: 99%

A cAMP-Dependent, Protein Kinase A-Independent Signaling Pathway Mediating Neuritogenesis through Egr1 in PC12 Cells

Ravni¹,

Vaudry²,

Gerdin³

et al. 2008

Mol Pharmacol

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The neurotrophic peptide PACAP (pituitary adenylate cyclaseactivating polypeptide) elevates cAMP in PC12 cells. Forskolin and dibutyryl cAMP mimic PACAP's neuritogenic and cell morphological effects, suggesting that they are driven by cAMP. Comparison of microarray expression profiles after exposure of PC12 cells to either forskolin, dibutyryl cAMP, or PACAP revealed a small group of cAMP-dependent target genes. Neuritogenesis induced by all three agents is protein kinase A (PKA)-independent [not blocked by N- [2-(4-bromocinnamylamino)ethyl]-5-isoquinoline (H89)] and extracellular signal-regulated kinase (ERK)-dependent [blocked by 1,4-diamino-2,3-dicyano-1,4-bis(methylthio) butadiene (U0126)], and therefore cAMP-dependent target genes potentially mediating neuritogenesis were selected for further analysis based on the pharmacological profile of their induction by PACAP (i.e., mimicking that of neuritogenesis). Small interfering RNA (siRNA) targeting one of these genes, Egr1, blocked PACAPinduced neuritogenesis, and siRNA targeting another, Vil2, blocked a component of the cell size increase elicited by PACAP. Neither siRNA blocked PACAP's PKA-dependent antiproliferative effects. PACAP signaling to neuritogenesis was also impaired by dominant-negative Rap1 expression but was not affected by inhibition of protein kinase C (PKC), indicating a G-protein-coupled receptor-mediated differentiation pathway distinct from the one activated by receptor tyrosine kinase ligands such as nerve growth factor (NGF), that involves both Rap1 and PKC. We have thus identified a cAMP-dependent, PKA-independent pathway proceeding through ERK that functions to up-regulate the transcription of two genes, Egr1 and Vil2, required for PACAP-dependent neuritogenesis and increased cell size, respectively. Dominant-negative Rap1 expression impairs both PACAP-induced neuritogenesis and Egr1 activation by PACAP, suggesting that cAMP elevation and ERK activation by PACAP are linked through Rap1.Neurotrophic factors activating receptor tyrosine kinases, such as nerve growth factor (NGF), promote neurite extension through a cAMP-independent signaling pathway involving Ras, PKC, and ERK (Ginty et al., 1991;Vaudry et al., 2002b), although other effects of NGF, such as induction of sodium channel expression, do require cAMP (Ginty et al., 1992;Yao et al., 1998). A significant literature also implicates cAMP in a broad range of neuronal differentiation responses, including neuritogenesis, survival, regeneration, repair, and expression of genes encoding neuron-specific proteins, such as neurotransmitter biosynthetic enzymes, neuropeptides, receptors, and ion channels (Qiu et al., 2002),

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“…4(B)]. Whereas the IC50 for VIP(1 -7)/GRF (8)(9)(10)(11)(12)(13)(14)(15)(16)(17)(18)(19)(20)(21)(22)(23)(24)(25)(26)(27), an established human VPAC1-specific agonist, at human VPAC2 was over 20 mM. These results showed that DBAYL could competitively displace […”

Section: Dbay L Selectively Binding To Vpac2 Receptormentioning

confidence: 99%

“…VPAC1 and VPAC2 receptors exhibit similar high affinity for PACAP38, PACAP27, and VIP [5]. PACAP is widely distributed in the brain and peripheral organs, notably in the endocrine pancreas, gonads, respiratory, and urogenital tracts, which has been shown to have effects on many pathological states including Parkinson's disease [6], diabetes [7,8], ischemia [9], traumatic injury [10], immunological disorders [11,12], myeloma kidney injury, and so on [13]. Most of these neuroprotective actions of PACAP are mediated through the selective PAC1 receptor whereas the effects on peripheral organs often involve VPAC1 or VPAC2 receptor.…”

Section: Introductionmentioning

confidence: 99%

A new recombinant pituitary adenylate cyclase-activating peptide-derived peptide efficiently promotes glucose uptake and glucose-dependent insulin secretion

Ma¹,

Luo²,

Xu³

et al. 2012

ABBS

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The recombinant peptide, DBAYL, a promising therapeutic peptide for type 2 diabetes, is a new, potent, and highly selective agonist for VPAC2 generated through sitedirected mutagenesis based on sequence alignments of pituitary adenylate cyclase-activating peptide (PACAP), vasoactive intestinal peptide (VIP), and related analogs. The recombinant DBAYL was used to evaluate its effect and mechanism in blood glucose metabolism and utilization. As much as 28.9 mg recombinant DBAYL peptide with purity over 98% can be obtained from 1 l of LuriaBertani medium culture by the method established in this study and the prepared DBAYL with four mutations (N10Q, V18L, N29Q, and M added to the N-terminal) were much more stable than BAY55-9837. The half-life of recombinant DBAYL was about 25 folds compared with that of BAY55-9837 in vitro. The bioactivity assay of DBAYL showed that it displaced [ 125 I]PACAP38 and [ 125 I]VIP from VPAC2 with a half-maximal inhibitory concentration of 48.4 + + + + + 6.9 and 47.1 + + + + + 4.9 nM, respectively, which were significantly lower than that of BAY55-9837, one established VPAC2 agonists. DBAYL enhances the cAMP accumulation in CHO cells expressing human VPAC2 with a half-maximal stimulatory concentration (EC 50 ) of 0.68 nM, whereas the receptor potency of DBAYL at human VPAC1 (EC 50 of 737 nM) was only 1/1083 of that at human VPAC2, and DBAYL had no activity toward human PAC1 receptor. Western blot analysis of the key proteins of insulin receptor signaling pathway: insulin receptor substrate 1 (IRS-1) and glucose transporter 4 (GLUT4) indicated that the DBAYL could significantly induce the insulin-stimulated IRS-1 and GLUT4 expression more efficiently than BAY55-9837 and VIP in adipocytes. Compared with BAY55-9837 and PACAP38, the recombinant peptide DBAYL can more efficiently promote insulin release and decrease plasma glucose level in Institute of Cancer Research (ICR) mice. These results suggested that DBAYL could efficiently improve glucose uptake and glucose-dependent insulin secretion by VPAC2-mediated effect.

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Neuroprotection by endogenous and exogenous PACAP following stroke

Cited by 104 publications

References 78 publications

Comparison of Intestinal Warm Ischemic Injury in PACAP Knockout and Wild-Type Mice

Comparison of Intestinal Warm Ischemic Injury in PACAP Knockout and Wild-Type Mice

A cAMP-Dependent, Protein Kinase A-Independent Signaling Pathway Mediating Neuritogenesis through Egr1 in PC12 Cells

A new recombinant pituitary adenylate cyclase-activating peptide-derived peptide efficiently promotes glucose uptake and glucose-dependent insulin secretion

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