Partial purification and characterization of selected enzymes of bovine nitrogen metabolism : comparison of the Nguni and Hereford breeds

Mathomu, Lutendo Michael

11 1900

Ruminant animals consuming low N-diet have been reported to have increased urea reabsorption with the Nguni being categorized as N-recycling ruminant. The enzymes associated with N-cycling are hypothesized to contribute to survival of the Nguni in harsh conditions. Enzymes responsible for such a function needed to be characterized in order to determine their effect in the functioning of the Nguni as opposed to Hereford breed. Crude enzymes from both breeds were separated from most or some contaminants by sephadex G-25, DEAE sephacel, and different affinity column chromatography. CPS and GDH were successfully purified and characterized by LC-MS/MS and further analysed by ProteinPilot™, blasted and matched >95% with those of Bos Taurus. Comparison of characterized enzymes and those which failed to ionise such as ARG, GS and GA was done using kinetics and graphs annotating specific activities. Partial purification and characterization was in part achieved. / Life and Consumer Sciences / M. Sc. (Life Sciences)

Cattle breeds

Purification

Characterization

Nitrogen metabolism

Arginase

Carbamoyl phosphate synthetase

Glutamine synthetase

Glutamate dehydrogenase

Glutaminase

Chromatography

Rate of maximal velocity

Enzyme activity

Kinetics

636.208521

Nguni cattle -- Feeding and feeds

Nitrogen -- Metabolism

Hereford cattle -- Feeding and feeds

A Global Kinase and Phosphatase Interaction Network in the Budding Yeast Reveals Novel Effectors of the Target of Rapamycin (TOR) Pathway

Sharom, Jeffrey Roslan

31 August 2011

In the budding yeast Saccharomyces cerevisiae, the evolutionarily conserved Target of Rapamycin (TOR) signaling network regulates cell growth in accordance with nutrient and stress conditions. In this work, I present evidence that the TOR complex 1 (TORC1)-interacting proteins Nnk1, Fmp48, Mks1, and Sch9 link TOR to various facets of nitrogen metabolism and mitochondrial function. The Nnk1 kinase controlled nitrogen catabolite repression-sensitive gene expression via Ure2 and Gln3, and physically interacted with the NAD+-linked glutamate dehydrogenase Gdh2 that catalyzes deamination of glutamate to alpha-ketoglutarate and ammonia. In turn, Gdh2 modulated rapamycin sensitivity, was phosphorylated in Nnk1 immune complexes in vitro, and was relocalized to a discrete cytoplasmic focus in response to NNK1 overexpression or respiratory growth. The Fmp48 kinase regulated respiratory function and mitochondrial morphology, while Mks1 linked TORC1 to the mitochondria-to-nucleus retrograde signaling pathway. The Sch9 kinase appeared to act as both an upstream regulator and downstream sensor of mitochondrial function. Loss of Sch9 conferred a respiratory growth defect, a defect in mitochondrial DNA transmission, lower mitochondrial membrane potential, and decreased levels of reactive oxygen species. Conversely, loss of mitochondrial DNA caused loss of Sch9 enrichment at the vacuolar membrane, loss of Sch9 phospho-isoforms, and small cell size suggestive of reduced Sch9 activity. Sch9 also exhibited dynamic relocalization in response to stress, including enrichment at mitochondria under conditions that have previously been shown to induce apoptosis in yeast. Taken together, this work reveals intimate connections between TORC1, nitrogen metabolism, and mitochondrial function, and has implications for the role of TOR in regulating aging, cancer, and other human diseases.

Target of Rapamycin

budding yeast

Saccharomyces cerevisiae

yeast

kinase

phosphatase

protein-protein interactions

TOR

nutrients

growth

rapamycin

signaling

network

metabolism

nitrogen catabolite repression

retrograde response

glutamate dehydrogenase

glutamine

glutamate

alpha-ketoglutarate

cell size

aging

lifespan

mitochondria

uncoupled respiration

petite

reactive oxygen species

free radical theory of aging

apoptosis

cancer

glutaminolysis

TORC1

Nnk1

Fmp48

Mks1

Sch9

Gdh2

Ure2

ribosomal protein S6 kinase

S6K

cell biology

molecular biology

0307

0379

0369

0410

0306

A Global Kinase and Phosphatase Interaction Network in the Budding Yeast Reveals Novel Effectors of the Target of Rapamycin (TOR) Pathway

Sharom, Jeffrey Roslan

31 August 2011

In the budding yeast Saccharomyces cerevisiae, the evolutionarily conserved Target of Rapamycin (TOR) signaling network regulates cell growth in accordance with nutrient and stress conditions. In this work, I present evidence that the TOR complex 1 (TORC1)-interacting proteins Nnk1, Fmp48, Mks1, and Sch9 link TOR to various facets of nitrogen metabolism and mitochondrial function. The Nnk1 kinase controlled nitrogen catabolite repression-sensitive gene expression via Ure2 and Gln3, and physically interacted with the NAD+-linked glutamate dehydrogenase Gdh2 that catalyzes deamination of glutamate to alpha-ketoglutarate and ammonia. In turn, Gdh2 modulated rapamycin sensitivity, was phosphorylated in Nnk1 immune complexes in vitro, and was relocalized to a discrete cytoplasmic focus in response to NNK1 overexpression or respiratory growth. The Fmp48 kinase regulated respiratory function and mitochondrial morphology, while Mks1 linked TORC1 to the mitochondria-to-nucleus retrograde signaling pathway. The Sch9 kinase appeared to act as both an upstream regulator and downstream sensor of mitochondrial function. Loss of Sch9 conferred a respiratory growth defect, a defect in mitochondrial DNA transmission, lower mitochondrial membrane potential, and decreased levels of reactive oxygen species. Conversely, loss of mitochondrial DNA caused loss of Sch9 enrichment at the vacuolar membrane, loss of Sch9 phospho-isoforms, and small cell size suggestive of reduced Sch9 activity. Sch9 also exhibited dynamic relocalization in response to stress, including enrichment at mitochondria under conditions that have previously been shown to induce apoptosis in yeast. Taken together, this work reveals intimate connections between TORC1, nitrogen metabolism, and mitochondrial function, and has implications for the role of TOR in regulating aging, cancer, and other human diseases.

Target of Rapamycin

budding yeast

Saccharomyces cerevisiae

yeast

kinase

phosphatase

protein-protein interactions

TOR

nutrients

growth

rapamycin

signaling

network

metabolism

nitrogen catabolite repression

retrograde response

glutamate dehydrogenase

glutamine

glutamate

alpha-ketoglutarate

cell size

aging

lifespan

mitochondria

uncoupled respiration

petite

reactive oxygen species

free radical theory of aging

apoptosis

cancer

glutaminolysis

TORC1

Nnk1

Fmp48

Mks1

Sch9

Gdh2

Ure2

ribosomal protein S6 kinase

S6K

cell biology

molecular biology

0307

0379

0369

0410

0306