The Biosynthesis of Bovine Submaxillary Mucin

Lawford, G. Ross; Schachter, Harry

doi:10.3138/9781442631649-030

Cited by 18 publications

(25 citation statements)

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“…The results described are supported by the findings of other workers, in particular O'Brien Canady, Hall & Neufeld (1966) with respect to the occurrence of sialic acid-deficient glycoproteins in liver microsomes, and Lawford & Schachter (1966) with respect to the subcellular localization of components involved in the biosynthesis of glycoproteins.…”

Section: Resultssupporting

confidence: 87%

“…The results obtained support the view that precursors of components of serum fraction I that contain at least some N-acetylglucosamine residues are present within vesicles enclosed by rough-surfaced endoplasmic reticulum, and that components bearing completed prosthetic groups are found within vesicles present in the smooth-membrane microsome subfraction. The results can be explained by a process in which polypeptide chains, possibly bearing initial N-acetylglucosamine residues (Lawford & Schachter, 1966), pass from ribosomes into the cisternae of the rough-surfaced endoplasmic reticulum (Redman & Sabatini, 1966), and while they are present successively in the rough-surfaced and smooth-surfaced endoplasmic reticulum (Peters, 1962) acquire sugar residues (e.g. Molnar, Robinson & Winzler, 1965;Sarcione, Bohne & Leahy, 1964).…”

Section: Resultsmentioning

confidence: 99%

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Studies on the nature of microsome-bound substances involved in the biosynthesis of acidic glycoproteins of guinea-pig serum

Simkin

Jamieson

1968

Biochemical Journal

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1. In further studies on the biosynthesis of components of fraction I, an acidic glycoprotein-containing fraction from guinea-pig serum, an investigation was made of the substances bound to liver microsomes that had earlier been implicated to participate in the synthesis of components of fraction I present in serum. These substances were normally liberated by ultrasonic vibrations. Antisera to subfractions of fraction I were used for characterization. 2. At pH8.6, most of the microsome-bound substances showed electrophoretic mobilities lower than components of fraction I but similar to components of sialic acid-free fraction I. 3. The sialic acid/protein ratios of immune precipitates formed by microsome extracts were similar to those of precipitates formed by sialic acid-free fraction I. 4. On chromatography on Sephadex G-150, most of the microsomal substances were eluted at an essentially similar volume to the main components of fraction I. 5. It was concluded that most of the microsome-bound substances lack sialic acid residues, and, as appreciable degradation of completed molecules is unlikely, these substances appear to be precursors of serum glycoprotein molecules with incomplete prosthetic groups. 6. Evidence was obtained on the submicrosomal localization of incomplete and complete serum glycoprotein molecules.

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Section: Resultssupporting

confidence: 87%

Section: Resultsmentioning

confidence: 99%

Studies on the nature of microsome-bound substances involved in the biosynthesis of acidic glycoproteins of guinea-pig serum

Simkin

Jamieson

1968

Biochemical Journal

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“…4 and 6). This could be explained either by the presence of bound polyribosomes in the nuclear fraction, which have been shown to be active for incorporation of leucine and glucosamine into protein (21) or by contamination of nuclear material with components of the microsome fraction, since labelling of lines formed by extracts of nuclear material was eliminated by extensive washing prior to extraction with Lubrol-W. In all experiments, lines given by extracts of kidney, spleen, and liver cell sap were not radioactive even although the lines were fairly intense, particularly in the case of liver cell sap.…”

Section: Zmm~nodi#usioa Studies On the Biosynthesis Ofmentioning

confidence: 95%

Studies on Acute Phase Proteins of Rat Serum. III. Site of Synthesis of Albumin and α₁-Acid Glycoprotein and the Contents of These Proteins in Liver Microsome Fractions from Rats Suffering from Induced Inflammation

Jamieson¹,

Ashton²

1973

Can. J. Biochem.

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Following injection of L-ieucine-3H or D-glucosamine-14C to normal rats or rats suffering from inflammation for 12 h there was a delay of 10–15 min before label appeared in albumin and α1-acid glycoprotein in serum; thereafter, there were rapid increases in specific radioactivities. The specific radioactivity of L-leucine-3H in albumin in serum from normal and experimental animals was not significantly different; however, there was a more rapid increase in specific radioactivities of both labelled compounds in α1-acid glycoprotein isolated from serum from experimental animals. Immunological techniques coupled with radioautography indicated that the microsome fraction of liver was the subcellular site of synthesis of albumin and of carbohydrate and polypeptide moieties of α1-acid glycoprotein in normal and experimental animals. The contents of albumin and α1-acid glycoprotein in liver microsome fractions from normal and experimental animals were determined by application of the quantitative precipitin technique to Lubrol-W extracts of microsome material. Little change in content of albumin associated with microsome material was found as a result of inflammation; however, there was a significant increase in the content of α1-acid glycoprotein in microsome material from experimental animals, reaching a maximum at 8–12 h after inflammation. On the basis of these latter results, it is suggested (1) that there is a fairly rapid stimulation of synthesis of α1-acid glycoprotein by liver in response to inflammation and (2) that the increased content of α1-acid glycoprotein associated with microsome material at short times of exposure to inflammatory agent is responsible for the increased content of this protein found in serum at longer times of exposure to inflammatory agent.

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“…€ cleolos, que desaparecer en los estadios posteriores en q los núcleos se hacen más picnóticos (1). El contenido de ^ue en los primeros estadios corresponde al de células di-< i ploides (17), comienza a disminuir con la maduración (célu las hipodiploid.es), y se hace ni^Lo luego de la extrusión del núcleo (18), durante el pasaje de eritroblasto ortocromático a reticulocito (19). Si analizamos la evolución de la síntesis de proteínas durante el curso de la maduración eritroblástica, se puede observar que la formación de la mayor parte de las ri síntesis, tiene lugar esos precursores en proteínas totales por bonucleoproteínas necesarias para esa en los estadios tempranos (19).…”

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“…El contenido de ^ue en los primeros estadios corresponde al de células di-< i ploides (17), comienza a disminuir con la maduración (célu las hipodiploid.es), y se hace ni^Lo luego de la extrusión del núcleo (18), durante el pasaje de eritroblasto ortocromático a reticulocito (19). Si analizamos la evolución de la síntesis de proteínas durante el curso de la maduración eritroblástica, se puede observar que la formación de la mayor parte de las ri síntesis, tiene lugar esos precursores en proteínas totales por bonucleoproteínas necesarias para esa en los estadios tempranos (19). Desde adelante, la actividad de síntesis de volumen de células se mantiene a un nivel constante (17), * pero en la transformaciones ios eritroblastos basófilos a policromatófilos, se especializa y vuelca abrupta y uasi ejt cluyentemente hacia la producción de hemoglobina (Kr) (30) (31), y continúa así hasta el estadio de reticulociitosde resultas de esta polarización del aparatp de sfntesie de > >« proteínas y la falta de recambio de hemoglobina se produce la acumulación de ésta llevándola a constituir el 95$ (6) del peso seco de los eritrocitos maduros.…”

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Estudios sobre la síntesis de proteínas en células de médula ósea

Grau¹

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En este trabajo se estudia el aparato de síntesis de proteínas en el citoplasma de células eritroblásticas de médula ósea de conejos, y se demuestra la presencia de estructuras polirribosómicas y su actividad ”in vivo” e ”in vitro” en la síntesis de proteínas. La actividad de ribonucleasas en los extractos acelulares de este tejido dificultó estas observaciones, que solamente pudieron llevarse a cabo mediante el empleo del inhibidor de ribonucleasas presente en homogenados de hígado.

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The Biosynthesis of Bovine Submaxillary Mucin

Cited by 18 publications

References 0 publications

Studies on the nature of microsome-bound substances involved in the biosynthesis of acidic glycoproteins of guinea-pig serum

Studies on the nature of microsome-bound substances involved in the biosynthesis of acidic glycoproteins of guinea-pig serum

Studies on Acute Phase Proteins of Rat Serum. III. Site of Synthesis of Albumin and α₁-Acid Glycoprotein and the Contents of These Proteins in Liver Microsome Fractions from Rats Suffering from Induced Inflammation

Estudios sobre la síntesis de proteínas en células de médula ósea

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The Biosynthesis of Bovine Submaxillary Mucin

Cited by 18 publications

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Studies on the nature of microsome-bound substances involved in the biosynthesis of acidic glycoproteins of guinea-pig serum

Studies on the nature of microsome-bound substances involved in the biosynthesis of acidic glycoproteins of guinea-pig serum

Studies on Acute Phase Proteins of Rat Serum. III. Site of Synthesis of Albumin and α1-Acid Glycoprotein and the Contents of These Proteins in Liver Microsome Fractions from Rats Suffering from Induced Inflammation

Estudios sobre la síntesis de proteínas en células de médula ósea

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Studies on Acute Phase Proteins of Rat Serum. III. Site of Synthesis of Albumin and α₁-Acid Glycoprotein and the Contents of These Proteins in Liver Microsome Fractions from Rats Suffering from Induced Inflammation