Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:4.2.2.7 (
heparinase
)
1,270
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
A protein kinase capable of phosphorylating basic fibroblast growth factor (FGF) can be localized on the outer cell surface of human hepatoma cells (SK-Hep cells). The addition of [gamma-32P]ATP, but not H3(32)PO4, results in a rapid (less than 10 min) incorporation of 32P into exogenously added basic FGF. The reaction is time and concentration dependent (apparent Km, 170 nM) and is stimulated by the addition of
cAMP
(EC50, 0.5 microM), but not the phorbol ester 12-O-tetradecanoyl-phorbol-13-acetate. There is also no tyrosine protein kinase detected on the cell surface. The inhibition of basic FGF binding to its low and/or high affinity sites decreases the phosphorylation of basic FGF by the ecto-protein kinase. Accordingly, pretreatment of cells with
heparinase
for 30 min or coincubation with heparin (0.1-10 micrograms/ml) decreases phosphorylation in a dose-dependent manner. Furthermore, the addition of a nonphosphorylatable peptide analog of basic FGF ([Val112] basic FGF-(106-146)NH2) that can compete with basic FGF binding to cells prevents the phosphorylation of basic FGF. Together, these observations suggest that 1) exogenous basic FGF must associate with its low and/or high affinity binding sites to be phosphorylated, and 2) the kinase is
cAMP
dependent and associated with the outer cell surface, and support the hypothesis that phosphorylation may regulate the activity and/or bioavailability of the growth factor.
...
PMID:Phosphorylation of basic fibroblast growth factor by a protein kinase associated with the outer surface of a target cell. 165 31
The development and survival of spinal motor neurons depends upon muscle-derived trophic factors. Some circumstantial evidence suggested to us that the regulatory subunit of cyclic adenosine 3':5'-monophosphate-dependent protein kinase (cAMP-dPK)-type II might be involved in neuritic outgrowth from spinal neurons. In the present study, we tested a commercial preparation of
cAMP
-dPK for neurite-promoting activity. Commercial
cAMP
-dPK-type II from skeletal and cardiac muscles elicited a significant neurite outgrowth from cultured embryonic chicken neurons when the enzyme preparation was bound to polylysine-coated substrata; type I
cAMP
-dPK from skeletal muscle was ineffective. Neither
cAMP
-dPK-type I nor -type II had a significant effect on the survival of spinal neurons in culture. Type II
cAMP
-dPK also stimulated neurite outgrowth from chicken cerebral hemisphere neurons, dorsal root ganglionic neurons, ciliary ganglionic neurons, and rat sympathetic ganglionic neurons in culture. The neurite-promoting activity appears to reside in a contaminant of the preparation since neither the purified regulatory nor catalytic subunits of
cAMP
-dPK-type II had an effect on neurite outgrowth per se from cultured neurons and since neurite-promoting activity did not correlate with [3H]
cAMP
binding or
cAMP
-dependent kinase activity. The neurite-promoting protein was then partially purified from commercial
cAMP
-dPK-type II by gel filtration on Sephadex G-200 followed by ion-exchange chromatography on DE-52 cellulose. Sodium dodecyl sulfate gel electrophoresis of the active protein peak revealed a major protein band (MW 50 kDa) and several minor bands (e.g., MW 200 kDa, 52 kDa, 45 kDa). Also, immunoblot analysis and immunoprecipitation revealed that the partially purified neurite-promoting protein was distinct from laminin, heparan sulfate proteoglycan, nerve growth factor, neural cell adhesion molecule, and fibronectin. Furthermore, the neurite-promoting activity was not diminished by treatment with
heparinase
nor was it bound to heparin conjugated to Sepharose. Our results demonstrate that a protein unrelated to laminin or its associated macromolecules and which copurifies with the type II
cAMP
-dPK of striated muscle stimulates neurite outgrowth from neurons of the central and peripheral nervous systems.
...
PMID:A muscle-derived substrate-bound factor that promotes neurite outgrowth from neurons of the central and peripheral nervous systems. 283 49
We have investigated the effect of soluble or extracellular-matrix (ECM) -bound heparin in conjunction with various second messenger pathways on cell proliferation and tissue-specific gene expression in primary cultures of hepatocytes. None of the combinations of heparin and second messenger stimulators or inhibitors had an effect on hepatocyte proliferation. Soluble heparin enhanced albumin expression in hepatocytes. Activation of protein kinase C, as well as an increase in intracellular
cAMP
, abolished this increase in albumin expression in the presence of heparin. When hepatocytes were plated on hepatocyte-derived ECM, containing highly sulfated heparan sulfate chains, activation of protein kinase C and an increase in intracellular
cAMP
strongly reduced albumin expression in hepatocytes. When heparan sulfate chains were removed from the ECM by
heparinase
treatment, activation of protein kinase C and increased
cAMP
were less inhibitory for albumin expression in hepatocytes. Inhibition of tyrosine kinases did not affect the induction of albumin mRNA by heparin. We conclude that heparin induces albumin expression in hepatocytes and activation of protein kinase C or increased intracellular
cAMP
antagonize this effect. ECM-bound heparan sulfates do not act in the same manner as soluble heparin.
...
PMID:Synergies of heparin and second messengers pathways involved in tissue-specific gene expression in hepatocytes. 1134 47
