Your search keyword '"Microbial Collagenase pharmacology"' showing total 15 results

1. Zone-specific inducibility of cytochrome P450 2B1/2 is retained in isolated perivenous hepatocytes.

Author

Bars RG, Bell DR, Elcombe CR, Oinonen T, Jalava T, and Lindros KO

Subjects

Animals, Base Sequence, Blotting, Western, Cells, Cultured, Cytochrome P-450 Enzyme System genetics, Enzyme Induction, Immunohistochemistry, Isoenzymes genetics, Liver blood supply, Liver cytology, Male, Microbial Collagenase pharmacology, Molecular Sequence Data, Phenobarbital pharmacology, RNA, Messenger biosynthesis, RNA, Messenger genetics, Rats, Transcription, Genetic drug effects, Transcription, Genetic genetics, Veins, Cytochrome P-450 Enzyme System biosynthesis, Isoenzymes biosynthesis, Liver enzymology

Abstract

The expression and induction of the cytochrome P450 2B1/2 isoenzyme is heterogeneous, exhibiting a regional pattern in the intact liver and a varied response to phenobarbital in isolated cultured hepatocytes. We report that P450 2B1/2 immunostaining of hepatocytes isolated from the perivenous liver region and cultured in the presence of phenobarbital is much stronger than that of cells identically treated but isolated from the periportal region. P450 2B1 mRNA, quantified by a sensitive and specific RNAase protection assay, is also preferentially induced in perivenous hepatocytes, demonstrating that the difference in induced expression is at the pretranslational level. Our results suggest that perivenous and periportal hepatocytes are differentially imprinted to retain regiospecific factors governing their inducibility after isolation.

Published

1992

2. Metalloproteinase digestion of cartilage proteoglycan. Pattern of cleavage by stromelysin and susceptibility to collagenase.

Author

Hughes C, Murphy G, and Hardingham TE

Subjects

Animals, Cartilage drug effects, Cartilage enzymology, Chondroitin Sulfates pharmacology, Culture Media, Humans, Hydrolysis, Matrix Metalloproteinase 3, Proteoglycans chemistry, Rabbits, Swine, Cartilage chemistry, Metalloendopeptidases pharmacology, Microbial Collagenase pharmacology, Proteoglycans metabolism

Abstract

The action of purified rabbit bone stromelysin was investigated on proteoglycan aggregates from pig laryngeal cartilage. The enzyme caused a rapid fall in viscosity of proteoglycan aggregate solution (6 mg/ml), and the products of a partial digest (60% loss of relative viscosity) and a complete digest (95% loss of relative viscosity) were characterized. Analysis by gel chromatography on Sepharose 2B under associative conditions showed that 95% of the glycosaminoglycans in the complete digest were in small-sized fragments, whereas most of the hyaluronan-binding G1 domain and link protein remained intact and bound to hyaluronan. In contrast, there was extensive digestion of the G2 domain which resulted in 76% loss in its detection by immunoassay. Analysis of the partial digest also showed considerable loss (40%) of detection of the G2 domain, but the glycosaminoglycan-rich fragments were much larger than in the complete digest. There was also much less cleavage to create small fragments containing the G1 domain. This was evident on SDS/PAGE analysis where a 58 kDa G1 domain fragment was abundant in the complete digest, but was only present in small amounts in the partial digest. There was also only very limited conversion of link protein from a 44 kDa form to a 40 kDa form. The digestion of proteoglycan aggregate (6 mg/ml) by stromelysin was unaffected by the addition of a high concentration of extra chondroitin sulphate chains (14 mg/ml), and the digestion of proteoglycan monomer showed that the G1 domain was resistant to stromelysin digestion even when not bound to hyaluronan and link protein. The results show that stromelysin degrades the proteoglycan protein core with major cleavages close to, but not within, the G1 domain, and extensive cleavage in other regions. Experiments with purified collagenase, a metalloproteinase structurally related to stromelysin, showed that it too cleaved proteoglycan at several sites within the glycosaminoglycan-rich region of the core protein. Metalloproteinase attack on proteoglycan thus not only occurs with stromelysin but also with collagenase.

Published

1991

3. Formation of two species of nascent proteochondroitin in separate loci of a microsomal preparation from chick-embryo epiphyseal cartilage.

Author

Sugumaran G and Silbert JE

Subjects

Animals, Chick Embryo, Chondroitin Lyases pharmacology, Chondroitin Sulfate Proteoglycans chemistry, Chondroitin Sulfates chemistry, Microbial Collagenase pharmacology, Microsomes metabolism, Molecular Weight, Polyethylene Glycols pharmacology, Cartilage metabolism, Chondroitin Sulfate Proteoglycans metabolism, Chondroitin Sulfates metabolism

Abstract

The potential relationship of an intact membrane organization to the synthesis of chondroitin was examined before and after modification of a chick-embryo cartilage microsomal system with the non-ionic detergent Triton X-100. Incubations with labelled UDP-GlcA and UDP-GalNAc indicated that Triton X-100 had little effect on the amount of chondroitin synthesized to form one species of large proteochondroitin (Type I). However, Triton X-100 had a marked stimulatory effect on the formation of another smaller species of proteochondroitin (Type II). Presence of this detergent during chondroitin polymerization also resulted in chains that were slightly smaller. Neither of the two proteochondroitin species were collagenase-sensitive, nor did they contain dermatan-like regions. Thus in these respects they were unlike the small proteochondroitins (PG-Lb or PG-Lt) that have been found in chick-embryo cartilage. They also differed greatly in size from these small proteoglycans as well as from the large aggregatable proteochondroitin (PG-H) from the same source. Synthesis of the larger (Type I) proteochondroitin species was not affected by prior treatment of the microsomes with chondroitin ABC lyase at concentrations sufficient for elimination of synthesis of most of the smaller (Type II) proteochondroitin species. Use of chondroitin ABC lyase subsequent to synthesis of the chondroitin also resulted in preferential degradation of the smaller species. Thus there were differences in formation and limitation in access of the chondroitin ABC lyase to the two species, consistent with other differences described previously. These results indicate that there are separate loci within the microsomal membranes for synthesis of the two species.

Published

1991

4. Renal glycerol metabolism and the distribution of glycerol kinase in rabbit nephron.

Author

Wirthensohn G, Vandewalle A, and Guder WG

Subjects

Animals, Dihydroxyacetone metabolism, Female, Freezing, In Vitro Techniques, Kidney Tubules drug effects, Kidney Tubules enzymology, Microbial Collagenase pharmacology, Rabbits, Substrate Specificity, Tissue Distribution, Glycerol metabolism, Glycerol Kinase metabolism, Kidney Tubules metabolism, Phosphotransferases metabolism

Abstract

Glycerol and dihydroxyacetone are metabolized by rabbit kidney-cortex tubules, isolated by collagenase treatment. Half-maximal concentrations of both substrates were determined with regard to uptake rates and product formations. Maximal uptake rates were 643 and 329 mumol/h per g of protein for dihydroxyacetone and glycerol respectively. Glucose and lactate were found as major metabolic products. Glycerol kinase, the enzyme catalysing the first step in renal glycerol and dihydroxyacetone metabolism, was measured radiochemically as described by Newsholme, Robinson & Taylor [(1967) Biochim, Biophys. Acta 132, 338-346] and adapted for studies of the localization of this enzyme along the different structures of rabbit nephron. The results show that glycerol kinase is located exclusively in the proximal segments, i.e. the proximal convoluted tubules and the pars recta, but is negligible in the other structures studied. The activities were close to the maximal dihydroxyacetone uptake rates measured in tubule suspensions.

Published

1981

5. Biosynthesis and release of glycoproteins by human skin fibroblasts in culture.

Author

Sear CH, Grant ME, and Jackson DS

Subjects

Ascorbic Acid pharmacology, Cells, Cultured, Cysteine metabolism, Fibroblasts metabolism, Fucose metabolism, Humans, Macromolecular Substances, Microbial Collagenase pharmacology, Molecular Weight, Glycoproteins biosynthesis, Skin metabolism

Abstract

1. Confluent human skin fibroblasts maintained in a chemically defined medium incorporate l-[1-(3)H]fucose in a linear manner with time into non-diffusible macromolecules for up to 48h. Chromatographic analysis demonstrated that virtually all the macromolecule-associated (3)H was present as [(3)H]fucose. 2. Equilibrium CsCl-density-gradient centrifugation established that [(3)H]fucose-labelled macromolecules released into the medium were predominantly glycoproteins. Confirmation of this finding was provided by molecular-size analyses of the [(3)H]fucose-labelled material before and after trypsin digestion. 3. The [(3)H]fucose-labelled glycoproteins released into fibroblast culture medium were analysed by gel-filtration chromatography and sodium dodecyl sulphate/polyacrylamide-gel electrophoresis. These techniques demonstrated that the major fucosylated glycoprotein had an apparent mol.wt. of 230000-250000; several minor labelled species were also detected. 4. Dual-labelling experiments with [(3)H]fucose and (14)C-labelled amino acids indicated that the major fucosylated glycoprotein was synthesized de novo by cultured fibroblasts. The non-collagenous nature of this glycoprotein was established by three independent methods. 5. Gel-filtration analysis before and after reduction with dithiothreitol showed that the major glycoprotein occurs as a disulphide-bonded dimer when analysed under denaturing conditions. Further experiments demonstrated that this glycoprotein was the predominant labelled species released into the medium when fibroblasts were incubated with [(35)S]cysteine. 6. The relationship between the major fucosylated glycoprotein and a glycoprotein, or group of glycoproteins, variously known as fibronectin, LETS protein, cell-surface protein etc., is discussed.

Published

1977

6. Degradation of glomerular basement membrane by purified mammalian metalloproteinases.

Author

Baricos WH, Murphy G, Zhou YW, Nguyen HH, and Shah SV

Subjects

Animals, Basement Membrane drug effects, Cattle, Chromatography, Gel, Gelatinases, Hydrogen-Ion Concentration, Matrix Metalloproteinase 3, Microbial Collagenase pharmacology, Kidney Glomerulus drug effects, Metalloendopeptidases pharmacology, Pepsin A pharmacology

Abstract

Neutral metalloproteinases degrade components of the extracellular matrix, including collagen types I-V, fibronectin, laminin and proteoglycan. However, their ability to degrade intact glomerular basement membrane (GBM) has not previously been investigated. Incubation of [3H]GBM (50,000 c.p.m.; pH 7.5; 24 h at 37 degrees C) with purified gelatinase or stromelysin (2 units) resulted in significant GBM degradation: gelatinase, 46 +/- 2.2; stromelysin, 59 +/- 5.8 (means +/- S.E.M.; percentage release of non-sedimentable radioactivity; n = 4). In contrast, 2 units of collagenase released only 5.6 +/- 0.52% (n = 3) of the [3H]GBM radioactivity compared with 2.0 +/- 0.15% (n = 7) released from [3H]GBM incubated alone. Sephadex G-200 gel chromatography of supernatants obtained from incubations of [3H]GBM with either gelatinase or stromelysin confirmed the ability of these enzymes to degrade GBM and revealed both high-(800,000) and relatively low-(less than 20,000) Mr degradation products for both enzymes. GBM degradation by gelatinase and stromelysin was dose-dependent (range 0.02-2.0 units), near maximal between pH 6.0 and 8.6, and was completely inhibited (greater than 95%) by 2 mM-o-phenanthroline. Collagenase (2 units) did not enhance the degradation of GBM by either gelatinase (0.02 or 0.2 unit) or stromelysin (0.02 or 0.2 unit). Our results indicate that metalloproteinase-mediated GBM degradation by neutrophils and glomeruli may be attributable to gelatinase (neutrophils) and/or stromelysin (glomeruli) and suggest an important role for these proteinases in glomerular pathophysiology.

Published

1988

7. Extracellular-matrix synthesis by skeletal muscle in culture. Major secreted collagenous proteins of clonal myoblasts.

Author

Beach RL, Rao JS, and Festoff BW

Subjects

Animals, Cell Line, Chemical Precipitation, Collagen immunology, Electrophoresis, Polyacrylamide Gel, Extracellular Space metabolism, Macromolecular Substances, Mercaptoethanol pharmacology, Mice, Microbial Collagenase pharmacology, Muscle Proteins immunology, Muscles cytology, Pepsin A pharmacology, Peptide Fragments analysis, Collagen metabolism, Muscle Proteins metabolism

Abstract

We have previously shown that G8-1, a murine clonal skeletal-muscle cell line, produces a substrate-attached extracellular matrix [Beach, Burton, Hendricks & Festoff (1982) J. Biol. Chem. 257, 11437-11442]. To examine further the expression of extracellular-matrix proteins by muscle cells, we have analysed the collagenous proteins secreted by G8-1 myoblasts. We have found that collagens and/or procollagens, corresponding to genetic types I, III and IV (and possibly V), are produced and secreted by G8-1 myoblasts. The major secreted collagenous polypeptides were identified as alpha 1 type I and its precursors by using pulse-chase studies, pepsin and collagenase digestions and CNBr fragmentation. The presence of lesser amounts of the other collagens was determined by immunoprecipitation. These results demonstrate that clonal skeletal-muscle cells, in the absence of fibroblasts and an exogenous collagen substrate, are able to synthesize and secrete several extracellular-matrix collagenous proteins in proportions similar to those which are commonly found in muscle tissue and mixed cultures of muscle cells and fibroblasts.

Published

1985

8. The nature of the microfibrillar glycoproteins of elastic fibres. A biosynthetic study.

Author

Sear CH, Grant ME, and Jackson DS

Subjects

Animals, Ascorbic Acid pharmacology, Cattle, Cells, Cultured, Chromatography, Gel, Cytoskeleton metabolism, Elastic Tissue drug effects, Electrophoresis, Polyacrylamide Gel, Fibronectins biosynthesis, Glycoproteins metabolism, Hydroxylysine analysis, Hydroxyproline analysis, Microbial Collagenase pharmacology, Elastic Tissue metabolism, Glycoproteins biosynthesis

Abstract

1. Cell cultures propagated from foetal bovine ligamentum nuchae synthesized and secreted two glycoproteins, designated MFP I and MFP II, that are closely related to elastic-fibre microfibrils. Glycoproteins MFP I (apparent mol.wt. 150 000) and MFP II (apparent mol.wt. 300 000) were metabolically labelled, separated from other culture-medium components by immunoprecipitation with a specific anti-(microfibrillar protein) serum, and analysed by sodium dodecyl sulphate/polyacrylamide-gel electrophoresis and sodium dodecyl sulphate/gel-filtration chromatography. 2. Ligament cells also synthesized and secreted fibronectin, but salt-fractionation and immunoprecipitation studies with a specific anti-(cold-insoluble globulin) serum established that neither glycoprotein MFP I nor glycoprotein MFP II was related to fibronectin. 3. The secretion of glycoprotein MFP I, but not that of glycoprotein MFP II, was enhanced by the addition of ascorbate to the culture medium. 4. Ascorbate-supplemented ligament cells incorporated [3H]proline into glycoprotein MFP I, and 36% of the nondiffusible proline residues were hydroxylated, exclusively as 4-hydroxy[3H]proline. Less than 1% of the total proline residues in [3H]proline-labelled glycoprotein MFP II were hydroxylated. 5. Ascorbate-supplemented cells incorporated [14C]lysine into glycoprotein MFP I and 30% of the non-diffusible lysine residues were hydroxylated. 6. Newly secreted glycoprotein MFP I was digested by highly purified bacterial collagenase to yield polypeptide fragments of apparent mol.wts. 50 000 and 30 000. Glycoprotein MFP II was not digested by bacterial collagenase. 7. The results suggest that elastic-fibre microfibrils are composed of a novel collagenous glycoprotein MFP I in association, as yet undefined, with a non-collagenous glycoprotein MFP II.

Published

1981

9. Complete loss of heparin-releasable triacylglycerol lipase activity after collagenase treatment of the rat liver.

Author

Thomas J, Debeer LJ, and Mannaerts GP

Subjects

Animals, Heparin pharmacology, In Vitro Techniques, Liver enzymology, Male, Rats, Lipase antagonists & inhibitors, Liver drug effects, Microbial Collagenase pharmacology

Abstract

Lipolytic activity at pH 8.5-9.5 was lowered by approx. 80% in homogenates from livers perfused with collagenase or heparin. No heparin-releasable lipase activity was detected in hepatocytes isolated by collagenase treatment. It is concluded that crude collagenase completely inactivates the plasma-membrane-bound heparin-releasable lipase.

Published

1978

10. The structure of the hepatic insulin receptor and insulin binding.

Author

Haynes FJ, Helmerhorst E, and Yip CC

Subjects

Animals, Cell Membrane drug effects, Cell Membrane metabolism, Electrophoresis, Polyacrylamide Gel, In Vitro Techniques, Kinetics, Liver drug effects, Male, Microbial Collagenase pharmacology, Pancreatic Elastase pharmacology, Rats, Rats, Inbred Strains, Receptor, Insulin drug effects, Insulin metabolism, Liver metabolism, Receptor, Insulin metabolism

Abstract

Hepatocytes or hepatic plasma membranes were photoaffinity-labelled with radioiodinated N epsilon B29-monoazidobenzoyl-insulin. Analysis of the samples by SDS/polyacrylamide-gel electrophoresis and autoradiography revealed the insulin receptor as a predominant band of 450 kDa. When hepatic plasma membranes were first treated with clostridial collagenase and then photolabelled, the insulin receptor appeared as a predominant band of 360 kDa. This effect of collagenase treatment on the insulin receptor was due to Ca2+-dependent heat-labile proteinases contaminating the preparation of collagenase, and it could be mimicked by elastase. The decrease in size of the insulin receptor to 360 kDa resulted from the loss of a receptor component that was inaccessible to photolabelling. In contrast, the size of the insulin receptor of intact cells was not affected by collagenase treatment. This suggests that the site sensitive to proteolysis was located on the cytoplasmic side of the plasma membrane. In hepatic plasma membranes that were treated with collagenase or elastase, and contained the 360 kDa form of the insulin receptor, the binding affinity for insulin was increased by up to 2-fold. These findings support the concept that a component which is either a part of, or closely associated with, the insulin receptor may regulate its affinity for insulin.

Published

1986

11. Differences in the metabolism of very-low-density lipoproteins by isolated beating-heart cells and the isolated perfused rat heart. Evidence for collagenase-released extracellular lipoprotein lipase.

Author

Rajaram OV, Clark MG, and Barter PJ

Subjects

Animals, Extracellular Space enzymology, Heart drug effects, In Vitro Techniques, Lipolysis, Lipoprotein Lipase antagonists & inhibitors, Male, Myocardium cytology, Palmitates metabolism, Perfusion, Rats, Lipoprotein Lipase metabolism, Lipoproteins, VLDL metabolism, Microbial Collagenase pharmacology, Myocardium metabolism

Abstract

1. The metabolism of VLD lipoproteins (very-low-density lipoproteins) was studied in intact isolated beating-heart cells and isolated perfused rat heart from starved animals by using [14C]triacylglycerol fatty acid-labelled VLD lipoprotein prepared from rats previously injected with [1-14C]palmitate. 2. 14C-labelled VLD lipoprotein was metabolized by the isolated perfused heart, but was only minimally metabolized by the heart cells unless an exogenous source of lipoprotein lipase was added. 3. Measurements of lipoprotein lipase at pH 7.4 with the natural substrate 14C-labelled VLD lipoprotein indicated that during collagenase perfusion of the heart the enzyme was released into the perfusate, the activity released being proportional to the concentration of collagenase used. Lipoprotein lipase activity in homogenates of hearts that had been perfused with collagenase showed a corresponding loss of activity. 4. At high perfusate concentrations of collagenase, inactivation of the released lipoprotein lipase occurred. 5. Lipoprotein lipase activity was largely undetectable in the homogenate of the isolated heart cells. 6. It is concluded that the lipoprotein lipase responsible for the hydrolysis of VLD lipoprotein triacylglycerol is predominantly located externally to the heart muscle cells and that its release can be facilitated by perfusion of the heart with bacterial collagenase.

Published

1980

12. Studies on the assembly of the rat lens capsule. Biosynthesis and partial characterization of the collagenous components.

Author

Heathcote G, Sear CH, and Grant ME

Subjects

Aminopropionitrile pharmacology, Animals, Basement Membrane metabolism, Chromatography, Gel, Electrophoresis, Polyacrylamide Gel, Hydroxyproline biosynthesis, In Vitro Techniques, Male, Microbial Collagenase pharmacology, Molecular Weight, Morphogenesis, Proline metabolism, Rats, Collagen biosynthesis, Lens, Crystalline metabolism, Peptide Biosynthesis

Abstract

1. Isolated rat lens capsules synthesized hydroxy[3H]proline-containing polypeptides when incubated with [3H]proline. 2. The collagenous polypeptides synthesized during a 2 h incubation were analyzed by both gel-filtration chromatography and sodium dodecyl sulphate/polyacrylamide-gel electrophoresis and shown to have an apparent mol.wt. of approx. 180,000. 3. No evidence was obtained for conversion of these polypeptides into a lower-molecular-weight species in experiments where capsules were labelled for 2 h and chased with non-radioactive proline for up to 22 h. However, a time-dependent incorporation of the 180,000-mol.wt. species into a larger collagenous component was observed and this could be prevented by the inclusion of beta-aminopropionitrile in the incubation medium. 4. The radioactive components synthesized by the capsules correspond to subunits of the intact lens capsule and the direct incorporation of the polypeptide of mol.wt. 180,000 into deoxycholate-insoluble basement membrane was demonstrated.

Published

1978

13. A method for the study of bone mucosubstances by using collagenase.

Author

Oldroyd D and Herring GM

Subjects

Chondroitin analysis, Chromatography, Edetic Acid pharmacology, Electrophoresis, In Vitro Techniques, Neuraminic Acids analysis, Bone and Bones analysis, Microbial Collagenase pharmacology, Mucoproteins analysis

Published

1967

14. The characterization of rat kidney plasma membranes prepared by zonal centrifugation.

Author

Price RG, Taylor DG, and Robinson D

Subjects

Acid Phosphatase analysis, Alkaline Phosphatase analysis, Animals, Catalase analysis, Centrifugation, Zonal, Electron Transport Complex IV analysis, Kidney Cortex cytology, Methods, Microbial Collagenase pharmacology, Microscopy, Electron, Nucleotidases analysis, Rats, Cell Membrane enzymology, Kidney cytology

Abstract

1. Plasma membranes were isolated from a 10000g-min pellet prepared from a renal cortical homogenate in 20mm-NaHCO(3) by isopycnic centrifugation in a linear sucrose gradient in an ;A'-type zonal rotor. 2. The preparation was characterized by electron microscopy, and alkaline phosphatase, 5'-nucleotidase, l-leucine beta-naphthylamidase and l-leucine p-nitroanilidase activities were found to be selectively associated with the renal plasma membrane. 3. The preparation had a high degree of purity, as indicated by the presence of low activities of marker enzymes associated with subcellular organelles. A preliminary chemical analysis indicated that the chemical composition resembled that of plasma membranes of other tissues. 4. Plasma membranes were also prepared from tubular fragments and their enzyme contents were found to be similar to those of plasma membranes prepared from cortical homogenates. 5. l-Leucine beta-naphthylamidase, l-leucine p-nitroanilidase and 5'-nucleotidase were not enriched to the same extent as alkaline phosphatase in the preparation of plasma membranes from tubular fragments. A possible explanation for this finding is discussed.

Published

1972

15. Clearing-factor lipase in adipose tissue. Distinction of different states of the enzyme and the possible role of the fat cell in the maintenance of tissue activity.

Author

Cunningham VJ and Robinson DS

Subjects

Adipose Tissue cytology, Adipose Tissue drug effects, Adipose Tissue metabolism, Animals, Culture Media, Dactinomycin pharmacology, Depression, Chemical, Diet, Drug Stability, Epididymis, Fatty Acids, Nonesterified metabolism, In Vitro Techniques, Male, Methods, Rats, Starvation enzymology, Time Factors, Adipose Tissue enzymology, Lipoprotein Lipase metabolism, Microbial Collagenase pharmacology

Abstract

1. Incubation of intact epididymal adipose tissue from fed rats at 37 degrees in an albumin solution at pH7.4 in vitro results in rapid loss of clearing-factor lipase activity until a low activity, stable to prolonged incubation, is attained. The clearing-factor lipase activity of intact tissue from starved rats, which is initially much less than that of tissue from fed rats, is mainly stable to incubation at 37 degrees . 2. Much of the clearing-factor lipase activity of intact epididymal adipose tissue from fed rats is inactivated by collagenase. The enzyme activity of intact tissue from starved rats is not inactivated by collagenase. 3. The clearing-factor lipase activity of fat cells isolated from the epididymal adipose tissue of fed rats is stable to prolonged incubation at 37 degrees . It represents only a small proportion of the total activity of the intact tissue. In starved rats, the isolated fat cells contain a much higher proportion of the activity of the intact tissue. Their activity is also stable at 37 degrees . 4. Incubation of isolated fat cells in a serum-based medium leads to a progressive rise in clearing-factor lipase activity. Actinomycin increases the extent of this rise in activity. No rise in clearing-factor lipase activity occurs when stromal-vascular cells isolated from epididymal adipose tissue are incubated in the medium. 5. The findings indicate that less than 20% of the activity of intact adipose tissue from fed rats is retained when fat cells are isolated from the tissue by collagenase treatment. The activity that is lost could be that which normally functions in the uptake of triglyceride fatty acids by the tissue.

Published

1969