Structure of the gene encoding VGF, a nervous system-specific mRNA that is rapidly and selectively induced by nerve growth factor in PC12 cells.

Salton, Stephen R.J.; Fischberg, Daniel; Dong, Ke-Wen

doi:10.1128/mcb.11.5.2335

Cited by 125 publications

(115 citation statements)

References 109 publications

(150 reference statements)

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“…Surprisingly, however, the VGF mRNA in the NGF-embedded composite group showed a three-fold higher level of expression compared with the 50 ng/mL NGF group on day 2. Our results demonstrated that VGF mRNA levels were maximally induced to ~16-fold, which was in agreement with a previous report [22]. However, polarization can also lead to a rapid increase in VGF mRNA expression level by triggering calcium influx through voltage-gated calcium channels [22,23].…”

Section: Mrna Expression Levels Of Cell Differentiationrelated Genessupporting

confidence: 93%

“…Our results demonstrated that VGF mRNA levels were maximally induced to ~16-fold, which was in agreement with a previous report [22]. However, polarization can also lead to a rapid increase in VGF mRNA expression level by triggering calcium influx through voltage-gated calcium channels [22,23]. During the degradation of the composites, β-TCP elevates the calcium concentration in the culture medium, which is involved in mediating the growth and migratory direction of axons.…”

Section: Mrna Expression Levels Of Cell Differentiationrelated Genessupporting

confidence: 93%

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Degradable PRGD/PDLLA/β-TCP/NGF composites promote differentiation and regulate gene expression in rat pheochromocytoma cells

Qiu

Yan

et al. 2013

Chin. Sci. Bull.

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In this study, we synthesized degradable PRGD/PDLLA/-TCP/NGF composites to facilitate neuronal repair. To this end, we (1) examined the release of nerve growth factor (NGF) from the composites, (2) evaluated the differentiation status of the cells and (3) address how transcriptional activity may regulate the differentiation mechanism of these cells. NGF content was determined using enzyme-linked immunosorbent assay, while the cellular mRNA expression was examined by real-time PCR analysis. Our results indicated that NGF release was robust during the first 10 days and then stabilized at a lower level thereafter. Treatment of PC12 cells with the extract of the NGF-embedded composites induced the formation of neurites and, in some cases, net-like neurites. Analysis of the expression level of differentiation-related genes, such as TrkA, VGF, Rab1, GAP43 and β-tubulin II, were significantly up-regulated. These findings suggest that these composites might be a suitable delivery system for growth factors like NGF that can be used to facilitate neuronal repair after injury.nerve guidance conduit, nerve growth factor, neuronal repair, PC12 cells Citation:Qiu T, Yu C, Yan Q J, et al. Degradable PRGD/PDLLA/-TCP/NGF composites promote differentiation and regulate gene expression in rat pheochromocytoma cells.

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Section: Mrna Expression Levels Of Cell Differentiationrelated Genessupporting

confidence: 93%

Section: Mrna Expression Levels Of Cell Differentiationrelated Genessupporting

confidence: 93%

Degradable PRGD/PDLLA/β-TCP/NGF composites promote differentiation and regulate gene expression in rat pheochromocytoma cells

Qiu

Yan

et al. 2013

Chin. Sci. Bull.

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“…82,83 We failed to show association to any of the candidate genes according to the dichotomized clinical diagnosis of schizophrenia and schizophrenia spectrum disorders among 245 schizophrenia families, originating from the same geographical region as the families revealing the linkage to 7q21-32. With the markers used, we had fairly good coverage of the allelic diversity of the four studied genes.…”

Section: Association Of Reelin With Working Memorymentioning

confidence: 74%

Replication of linkage on chromosome 7q22 and association of the regional Reelin gene with working memory in schizophrenia families

et al. 2007

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Schizophrenia is a common and complex mental disorder. Hereditary factors are important for its etiology, but despite linkage signals reported to several chromosomal regions in different populations, final identification of predisposing genes has remained a challenge. Utilizing a large family-based schizophrenia study sample from Finland, we have identified several linked loci: 1q32.2-q42, 2q, 4q31, 5q and 7q22. In this study, an independent sample of 352 nuclear schizophrenia families (n = 1626) allowed replication of linkage on 7q21-32. In a sample of 245 nuclear families (n = 1074) originating from the same geographical region as the families revealing the linkage, SNP and microsatellite association analyses of the four regional candidate genes, GRM3, RELN, SEMA3A and VGF, revealed no significant association to the clinical diagnosis of schizophrenia. Instead, quantifiable trait component analyses with neuropsychological endophenotypes available from 186 nuclear families (n = 861) of the sample showed significant association to RELN variants for traits related to verbal (P = 0.000003) and visual working memory (P = 0.002), memory (P = 0.002) and executive functioning (P = 0.002). Trait-associated allele-positive subjects scored lower in the tests measuring working memory (P = 0.0004-0.0000000004), memory (P = 0.02-0.0001) and executive functioning (P = 0.001). Our findings suggest that allelic variants of RELN contribute to the endophenotypes of schizophrenia.

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“…A related series of constructs was made by truncating the full-length HA-tagged VGF using PCR primers to introduce termination codons following amino acids 177, 282, 367, 480, and 543 of rat VGF. The VGF:GFP constructs, which directly fuse VGF and GFP sequences in the vector pcDNA3 (Invitrogen) at the indicated sites, were created by PCR using pEGFP-N1 and the rat VGF cDNA (7,16) as templates. Sequences of all PCR-generated fragments were verified.…”

Section: Methodsmentioning

confidence: 99%

“…Secreted via the Regulated Release Pathway-VGF can be differentially processed, and the C terminus is rich in paired basic amino acids (7,9,16). Additionally, N-terminal signal peptide sequences and loop structures have been implicated in sorting, so two series of plasmids that contained either N-or C-terminal modifications were constructed.…”

Section: Vgf and Epitope-tagged Vgf Are Localized In Ldcvs Andmentioning

confidence: 99%

A Prohormone Convertase Cleavage Site within a Predicted α-Helix Mediates Sorting of the Neuronal and Endocrine Polypeptide VGF into the Regulated Secretory Pathway

Garcia

Han

Janssen

et al. 2005

Journal of Biological Chemistry

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Distinct intracellular pathways are involved in regulated and constitutive protein secretion from neuronal and endocrine cells, yet the peptide signals and molecular mechanisms responsible for targeting and retention of soluble proteins in secretory granules are incompletely understood. By using confocal microscopy and subcellular fractionation, we examined trafficking of the neuronal and endocrine peptide precursor VGF that is stored in large dense core vesicles and undergoes regulated secretion. VGF cofractionated with secretory vesicle membranes but was not detected in detergent-resistant lipid rafts. Deletional analysis using epitope-tagged VGF suggested that the C-terminal 73-amino acid fragment of VGF, containing two predicted ␣-helical loops and four potential prohormone convertase (PC) cleavage sites, was necessary and sufficient with an N-terminal signal peptide-containing domain, for large dense core vesicle sorting and regulated secretion from PC12 and INS-1 cells. Further transfection analysis identified the sorting sequence as a compact C-terminal ␣-helix and embedded 564 RRR 566PC cleavage site; mutation of the 564 RRR 566 PC site in VGF-(1-65): GFP:VGF-(545-617) blocked regulated secretion, whereas disruption of the ␣-helix had no effect. Mutation of the adjacent 567 HFHH 570 motif, a charged region that might enhance PC cleavage in acidic environments, also blocked regulated release. Finally, inhibition of PC cleavage in PC12 cells using the membrane-permeable synthetic peptide chloromethyl ketone (decanoyl-RVKR-CMK) blocked regulated secretion of VGF. Our studies define a critical RRR-containing C-terminal domain that targets VGF into the regulated pathway in neuronal PC12 and endocrine INS-1 cells, providing additional support for the proposed role that PCs and their cleavage sites play in regulated peptide secretion.Regulated secretion of polypeptides from neuronal and endocrine cells, which relies on packaging of proteins into the appropriate vesicle pools within the cell, is a critical control point for regulating peptide levels and ultimately function. Polypeptide motifs that target cell surface proteins to specific vesicle populations or to discrete locations within the cell, such as the basolateral or apical surface of a polarized epithelial cell, have been relatively well characterized (1). Protein domains that are responsible for targeting soluble proteins into the regulated release pathway appear to be more heterogeneous, and thus generalized sorting domains and consensus motifs have been more difficult to identify. Perhaps as a consequence, several models that explain targeting into the regulated secretory pathway by selective sorting and/or selective retention have been proposed (2-5). Following signal sequence-directed translocation into the lumen of the endoplasmic reticulum, segregation of proteins into the constitutive or regulated pathways is suspected to occur in the trans-Golgi network (TGN). 4 Constitutive secretory vesicles transit directly from the TGN to the plasma membran...

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Structure of the gene encoding VGF, a nervous system-specific mRNA that is rapidly and selectively induced by nerve growth factor in PC12 cells.

Cited by 125 publications

References 109 publications

Degradable PRGD/PDLLA/β-TCP/NGF composites promote differentiation and regulate gene expression in rat pheochromocytoma cells

Degradable PRGD/PDLLA/β-TCP/NGF composites promote differentiation and regulate gene expression in rat pheochromocytoma cells

Replication of linkage on chromosome 7q22 and association of the regional Reelin gene with working memory in schizophrenia families

A Prohormone Convertase Cleavage Site within a Predicted α-Helix Mediates Sorting of the Neuronal and Endocrine Polypeptide VGF into the Regulated Secretory Pathway

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