Substrate tubular

This is a combined organic-inorganic membrane that comprises a macropor-ous a-alumina substrate (tubular or multichannel), an intermediate mesopor-ous inorganic titanium oxide layer (thickness 1 pm) and a microporous Nafion polymer top-layer (thickness less than 0.1 pm). The overall performance and... 

We find that the tubes are placed almost horizontally on the substrate. Irregular nanostructures were also formed, as displayed in the images. However, the high occurrence of tubes clearly shows that carbon prefers to condense to tubular structures, as opposed to other nanostructures, under our preparation conditions. 

The co-administration of drugs which inhibit the transporters involved in renal tubular secretion can reduce the urinaty excretion of drugs which are substrates of the transporter, leading to elevated plasma concentrations of the drugs. For example, probenecid increases the plasma concentration and the duration of effect of penicillin by inhibiting its renal tubular secretion. It also elevates the plasma concentration of methotrexate by the same mechanism, provoking its toxic effects. 

Figure 5.28 Schematic of the experimental set-up. Water/ethylene glycol/SDS reservoir (a) high-pressure liquid pumps (b) catalyst/ substrate HPLC injection valve with 200 pi sample loop (c) hydrogen supply, equipped with mass flow controller (d) micro mixer (e) heating jacket (f) tubular glass or quartz reactor (g) back-pressure regulator (h) [64],...

The CES family of proteins is characterized by the ability to hydrolyze a wide variety of aromatic and aliphatic substrates containing ester, thioester, and amide bonds (Heymann 1980, 1982). Cauxin is a member of the CES family, and is secreted from the proximal straight tubular cells into the urine in a species-, sex-, and age-dependent manner. Therefore, we postulated that cauxin was involved in an enzymatic reaction in cat urine and the products made by the reaction should vary with species, sex, and age. Based on this hypothesis, we searched for physiological substrates and products of cauxin in cat urine and identified 2-amino-7-hydroxy-5,5-dimethyl-4-thiaheptanoic acid, also known as felinine. 

It is contended that the renal slice technique measures primarily basolateral uptake of substrates or nephrotoxins, based on histological evidence of collapsed tubular lumens. This results in the inaccessibility of brush-border surfaces for reabsorptive transport (Burg and Orloff, 1969 Cohen and Kamm, 1976). This observation limits the ability of this model to accurately reflect reactions to nephrotoxins that occur as the result of brush-border accumulation of an injurious agent. Ultrastructurally, a number of alterations, particularly in the plasma membrane and mitochondrial compartments, have been shown to occur over a 2-h incubation period (Martel-Pelletier et al., 1977). This deterioration in morphology is very likely a consequence of the insufficient diffusion of oxygen, metabolic substrates, and waste products in the innermost regions of the kidney slice (Cohen and Kamm, 1976). Such factors also limit the use of slices in studying renal metabolism and transport functions. 

FIG. 26. Scanning electron micrographs (A) the template-synthesized gold tubule ensemble obtained after dissolution of the polyester template membrane (B) as per A, but after CVD synthesis of TiSj outer tubes on the Au inner tubes. These tubular microstructures contained 0.86 mg of TiS2 cm of substrate A1 surface area (C) as per B, but with a larger quantity (2.04 mg cm ) of TiSj (D) CVD TiSj film. 

Fig. 4 Setup for continuous-flow asymmetric hydrovinylation using an IL/SCCO2 biphasic system. Liquid and gaseous substrates are mixed with the SCCO2 stream before entering the tubular reactor unit and bubbled through the catalyst-containing IL using a capillary. The CO2 flow leaves the reactor on top and the product is collected in a cold trap after controlled expansion to ambient pressure...

A model of such structures has been proposed that captures transport phenomena of both substrates and redox cosubstrate species within a composite biocatalytic electrode.The model is based on macrohomo-geneous and thin-film theories for porous electrodes and accounts for Michaelis—Menton enzyme kinetics and one-dimensional diffusion of multiple species through a porous structure defined as a mesh of tubular fibers. In addition to the solid and aqueous phases, the model also allows for the presence of a gas phase (of uniformly contiguous morphology), as shown in Figure 11, allowing the treatment of high-rate gas-phase reactant transport into the electrode. 

The proximal tubular cell plays a major role in the elimination of both inorganic and organic substrates. The ceUs have two distinct membrane domains. The basolateral membrane is in contact with the blood, and the apical brush-border membrane lines the tubular lumen. 

Alternatively, the pro-drug may be a substrate for brush-border enzymes of the proximal tubular cell, resulting in release of the active drug in the tubular lumen and subsequent reabsorption at distal sites or elimination in the urine. 

Apart from glomerular filtration (B), drugs present in blood may pass into urine by active secretion. Certain cations and anions are secreted by the epithelium of the proximal tubules into the tubular fluid via special, energyconsuming transport systems. These transport systems have a limited capacity. When several substrates are present simultaneously, competition for the carrier may occur (see p. 268). 

The loop diuretics must be present in the tubular fluid before they can become effective. Because of their extensive binding to plasma proteins, filtration across the glomerular capillaries is restricted. Like the thiazides, however, the loop diuretics are weak organic acids that are substrates for the organic acid secretory system in the proximal tubule. A consequence of this active secretion is that the presence of other organic acids or certain forms of renal disease may impair the therapeutic usefulness of the loop diuretics. 

Memantine is not a major substrate for hepatic cytochrome P450 isoenzymes and has not been shown to significantly inhibit or induce these enzymes. However, memantine is partially excreted by renal tubular secretion. Thus, concomitant use of other medications that use the same renal system (i.e., triampterene, hydrochlorothiazide, digoxin, cimetidine, ranitidine, metformin, and quinidine) may affect plasma levels of both drugs (Namenda 2005). Memantine should not be used in combination with other NMDA receptor antagonists, such as amantadine or dextromethorphan, because these combinations have not been formally studied. The clearance of memantine can be reduced when the urine is alkalinized, such as with the concomitant use of sodium bicarbonate or carbonic anhy-... 

---