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Query: UNIPROT:P01275 (
glucagon
)
26,492
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The possible relationship between changes in islet cell mass and in
islet neogenesis-associated protein
(
INGAP
)-cell mass induced by sucrose administration to normal hamsters was investigated. Normal hamsters were given sucrose (10% in drinking water) for 5 (S8) or 21 (S24) weeks and compared with control (C) fed hamsters. Serum glucose and insulin levels were measured and quantitative immunocytochemistry of the endocrine pancreas was performed. Serum glucose levels were comparable among the groups, while insulin levels were higher in S hamsters. There was a significant increase in beta-cell mass (P<0.02) and in beta-cell 5-bromo-2'-deoxyuridine index (P<0.01), and a significant decrease in islet volume (P<0.01) only in S8 vs C8 hamsters. Cytokeratin (CK)-labelled cells were detected only in S8 hamsters.
INGAP
-positive cell mass was significantly larger only in S8 vs C8 hamsters. Endocrine
INGAP
-positive cells were located at the islet periphery ( approximately 96%), spread within the exocrine pancreas ( approximately 3%), and in ductal cells (<1%) in all groups.
INGAP
positivity and
glucagon
co-localization varied according to topographic location and type of treatment. In C8 hamsters, 49.1+/-6. 9% cells were
INGAP
- and
glucagon
-positive in the islets, while this percentage decreased by almost half in endocrine extra-insular and ductal cells. In S8 animals, co-expression increased in endocrine extra-insular cells to 36.3+/-9.5%, with similar figures in the islets, decreasing to 19.7+/-6.9% in ductal cells.
INGAP
-positive cells located at the islet periphery also co-expressed CK. In conclusion, a significant increase of
INGAP
-positive cell mass was only observed at 8 weeks when neogenesis was present, suggesting that this peptide might participate in the control of islet neogenesis. Thus,
INGAP
could be a potentially useful tool to treat conditions in which there is a decrease in beta-cell mass.
...
PMID:Possible relationship between changes in islet neogenesis and islet neogenesis-associated protein-positive cell mass induced by sucrose administration to normal hamsters. 1082 57
The aim of this work was to study the possible relationship between pancreatic duodenal homeobox-1 (Pdx-1) and
islet neogenesis-associated protein
(
INGAP
) during induced islet neogenesis. Pregnant hamsters were fed with (S) and without (C) sucrose, and glycemia, insulin secretion in vitro, and pancreas immunomorphometric parameters were measured in their 7-day-old offspring. S offspring had significantly lower glycemic levels than C animals. Insulin release in response to increasing glucose concentrations in the incubation medium (2-16 mM glucose) did not increase in pancreata from either C or S offspring. However, pancreata from S offspring released more insulin than those from C animals. In S offspring, beta-cell mass, beta-cell replication rate and islet neogenesis increased significantly, with a simultaneous decrease in beta-cell apoptotic rate.
INGAP
- and Pdx-1-positive cell mass also increased in the islets and among acinar and duct cells. We found two subpopulations of Pdx-1 cells:
INGAP
-positive and
INGAP
-negative. Pdx-1/
INGAP
-positive cells did not stain with insulin,
glucagon
, somatostatin, pancreatic polypeptide, or neurogenin 3 antibodies. The increment of Pdx-1/
INGAP
-positive cells represented the major contribution to the Pdx-1 cell mass increase. Such increments varied among pancreas subsectors: ductal>insular>extrainsular. Our results suggested that
INGAP
participates in the regulation of islet neogenesis, and Pdx-1/
INGAP
-positive cells represent a new stem cell subpopulation at an early stage of development, highly activateable in neogenesis.
...
PMID:Pancreatic duodenal homeobox-1 and islet neogenesis-associated protein: a possible combined marker of activateable pancreatic cell precursors. 1274 13
The Reg-related protein family member
INGAP
(
islet neogenesis-associated protein
) is a pleiotropic factor enhancing islet neogenesis, neurite growth, beta-cell protection, and beta-cell function. Using an antibody to the N-termini of
INGAP
, we have identified that immunoreactivity to
INGAP
localized to the pancreatic endocrine cells in mouse.
INGAP
- and insulin-immunoreactive cells are mutually exclusive, with
INGAP
-immunoreactive cells being preserved after streptozotocin-mediated destruction of beta-cells.
Glucagon
- and
INGAP
-immunoreactive cells colocalize, although respective antigen expression occurs in different intracellular locations. These data suggest that
INGAP
-immunoreactive cells include alpha-cells; however, detection of single
INGAP
-immunoreactive/
glucagon
-negative cells indicates that this may not be exclusive. In addition to mouse, detection of islet endocrine cells that were
INGAP
immunoreactive/
glucagon
immunoreactive/insulin negative was also observed in islets from human, monkey, and rat. These findings reveal that
INGAP
and/or related group 3 Reg proteins have a conserved expression in the pancreatic islet.
...
PMID:Pancreatic islet immunoreactivity to the Reg protein INGAP. 1799 66
We evaluated the effect of
islet neogenesis-associated protein
pentadecapeptide (INGAP-PP) upon islet beta- and non-beta cell differentiation from mouse embryonic stem (mES) cells. ES-D3 cell lines were cultured following Lumelsky's protocol with or without
INGAP
-PP (5 microg/ml) at different stages. Gene expression was quantified using qPCR. mES cells were fixed and immunostained using anti insulin-, somatostatin-,
glucagon
-, Pdx-1-, Ngn-3-, Nkx-6.1 and PGP9.5 specific antibodies. PCNA was used to measure replication rate. Bcl(2) (immunostaining) and caspase-3 (enzyme activity and gene expression) were determined as apoptosis markers.
INGAP
-PP increased IAPP, Glut-2, Kir-6.2, SUR-1 and insulin gene expression, and the percentage of insulin-immunostained cells. Conversely,
INGAP
-PP reduced significantly
glucagon
and somatostatin gene expression and immunopositivity. While nestin gene expression was not affected, there was a significant reduction in the percentage of PGP9.5-immunostained cells. Pdx-1 gene expression increased by 115% in
INGAP
-PP treated cells, as well as the percentage of Pdx-1, Ngn-3 and Nkx-6.1 immunopositive cells. Neither caspase-3 (expression and activity) nor Bcl(2) positively immunostained cells were affected by
INGAP
-PP. Accordingly,
INGAP
-PP would promote stem cell differentiation into a beta-like cell phenotype, simultaneously decreasing its differentiation toward non-beta-cell precursors. Therefore,
INGAP
-PP would be potentially useful to obtain beta-cells from stem cells for replacement therapy.
...
PMID:Selective effect of INGAP-PP upon mouse embryonic stem cell differentiation toward islet cells. 1915 49
