The Localisation of Sorbitol Pathway Activity in the Rat Renal Cortex and Its Relationship to the Pathogenesis of the Renal Complications of Diabetes Mellitus

Hutton, JC; Schofield, PJ; Jd, Williams; Hollows, FC

doi:10.1038/icb.1975.5

Cited by 15 publications

(3 citation statements)

References 8 publications

(12 reference statements)

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“…Speculatively, the urea-myo-inositol may act as a house keeping counteracting system while the other two may invoke only on cellular demands (e.g., extreme stresses) because the existing levels of myo-inositol may not be sufficient enough to take care of the whole proteome stability under high hypertonic conditions (e.g., anti-diuretic condition) in the kidney. Interestingly, almost all reports on the osmotic content of the kidney cells were derived from the measurements under high hypertonic conditions [64], [65], [66], [67], [68]. It is, therefore, important to estimate osmotically active solute in the kidney cells under hypotonic conditions or diuresis.…”

Section: Discussionmentioning

confidence: 99%

Testing the Ability of Non-Methylamine Osmolytes Present in Kidney Cells to Counteract the Deleterious Effects of Urea on Structure, Stability and Function of Proteins

et al. 2013

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Human kidney cells are under constant urea stress due to its urine concentrating mechanism. It is believed that the deleterious effect of urea is counteracted by methylamine osmolytes (glycine betaine and glycerophosphocholine) present in kidney cells. A question arises: Do the stabilizing osmolytes, non-methylamines (myo-inositol, sorbitol and taurine) present in the kidney cells also counteract the deleterious effects of urea? To answer this question, we have measured structure, thermodynamic stability (ΔG D o) and functional activity parameters (K m and k cat) of different model proteins in the presence of various concentrations of urea and each non-methylamine osmolyte alone and in combination. We observed that (i) for each protein myo-inositol provides perfect counteraction at 1∶2 ([myo-inositol]:[urea]) ratio, (ii) any concentration of sorbitol fails to refold urea denatured proteins if it is six times less than that of urea, and (iii) taurine regulates perfect counteraction in a protein specific manner; 1.5∶2.0, 1.2∶2.0 and 1.0∶2.0 ([taurine]:[urea]) ratios for RNase-A, lysozyme and α-lactalbumin, respectively.

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Section: Discussionmentioning

confidence: 99%

Testing the Ability of Non-Methylamine Osmolytes Present in Kidney Cells to Counteract the Deleterious Effects of Urea on Structure, Stability and Function of Proteins

et al. 2013

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“…6-Fluoro-3,4-dihydro-2Ff-l-benzopyran-4-carboxylic Acid Phenylmethyl Ester (7). A solution of 9 (50.0 g, 0.25 mol) in saturated aqueous NaHC03 (200 mL) was added to a solution of benzyl bromide (42.8 g, 0.25 mol) in Ch2Cl2 (200 mL) containing benzyltributylammonium chloride (78.2 g, 0.25 mol) and stirred overnight at room temperature.…”

Section: Methodsmentioning

confidence: 99%

A highly specific aldose reductase inhibitor, ethyl 1-benzyl-3-hydroxy-2(5H)-oxopyrrole-4-carboxylate and its congeners

Mylari

Beyer²,

Siegel³

1991

J. Med. Chem.

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Ethyl 1-benzyl-3-hydroxy-2(5H)-oxopyrrole-4-carboxylate (1, EBPC) is a potent and specific inhibitor of aldose reductase. It was greater than 4000X more potent in its inhibition of rat lens aldose reductase than the closely related rat or pig kidney aldehyde reductase, thus making it the most selective inhibitor of a NADPH-dependent carbonyl reductase identified to date. In agreement with this observation, it was found to be a highly potent inhibitor of aldose reductase from rat sciatic nerve with greater than 98% inhibition at 1 microM, but it was practically devoid of activity against aldehyde reductases from rat liver and brain. Inhibition of aldose reductase was mixed type for glyceraldehyde (Ki = 8.0 x 10(-8) M) and noncompetitive for NADPH (Ki = 1.70 x 10(-8) M). Its potential as an in vitro tool to quantitate monomeric aldo/keto reductase activities in crude tissue extracts is presented. Structure-activity relationships emerging from synthetic modifications of EBPC are discussed. Several modifications were found to be active in vitro against aldose reductase from human placenta and in vivo in a rat model of diabetic complications, but none was more potent than EBPC.

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“…C ells in the medulla of the kidney contain high concentrations of glycerophosphoiylcholine (GVC), 1 -2 inositol, 2^ sorbitol, 4 and betaine. 5 All four compounds are intermediates in important biochemical pathways, but that is not the reason there is so much of them in these particular cells.…”

mentioning

confidence: 99%

Importance of organic osmolytes for osmoregulation by renal medullary cells.

García-Peréz

Burg

1990

Hypertension

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The cells in the renal medulla protect themselves from the extracellular hypertonicity in that region of the kidney by accumulating large amounts of sorbitol, inositol, grycerophosphorylcholine, and betaine. The system is uniquely active in this part of the body, but it represents a throwback to primitive mechanisms by which cells in virtually all organisms, including bacteria, yeasts, plants, and lower animals counteract water stress. In this brief review, we summarize how these "compatible organic osmolytes" help the renal medullary cells to survive, the mechanisms by which the organic osmolytes are accumulated, and how the accumulation is controlled to adjust for changing extracellular NaCl and urea concentrations. The compatible organic osmolytes are all intermediates in important biochemical pathways, and although the medical consequences are not yet fully worked out, it is already apparent that inappropriate accumulation of these solutes has major pathophysiological consequences. (Hypertension 1990;16:595-602)

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The Localisation of Sorbitol Pathway Activity in the Rat Renal Cortex and Its Relationship to the Pathogenesis of the Renal Complications of Diabetes Mellitus

Cited by 15 publications

References 8 publications

Testing the Ability of Non-Methylamine Osmolytes Present in Kidney Cells to Counteract the Deleterious Effects of Urea on Structure, Stability and Function of Proteins

Testing the Ability of Non-Methylamine Osmolytes Present in Kidney Cells to Counteract the Deleterious Effects of Urea on Structure, Stability and Function of Proteins

A highly specific aldose reductase inhibitor, ethyl 1-benzyl-3-hydroxy-2(5H)-oxopyrrole-4-carboxylate and its congeners

Importance of organic osmolytes for osmoregulation by renal medullary cells.

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