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Facilitated diffusion/transport system

Glucose cannot diffuse directly into cells, but enters by one of two transport mechanisms a Na+-independent, facilitated diffusion transport system or a Na+-monosaccharide co-transporter system. [Pg.95]

There are, however, various types of active transport systems, involving protein carriers and known as uniports, symports, and antiports as indicated in Figure 3.7. Thus, symports and antiports involve the transport of two different molecules in either the same or a different direction. Uniports are carrier proteins, which actively or passively (see section "Facilitated Diffusion") transport one molecule through the membrane. Active transport requires a source of energy, usually ATP, which is hydrolyzed by the carrier protein, or the cotransport of ions such as Na+ or H+ down their electrochemical gradients. The transport proteins usually seem to traverse the lipid bilayer and appear to function like membrane-bound enzymes. Thus, the protein carrier has a specific binding site for the solute or solutes to be transferred. For example, with the Na+/K+ ATPase antiport, the solute (Na+) binds to the carrier on one side of... [Pg.42]

Most known saturable transporters at the BBB are facilitated diffusion systems (Davson and Segal, 1996c). For example, GLUT-1, the transporter for glucose, is a facilitated diffusion transporter. If the level of glucose is artificially raised above that of serum (or if radioactive glucose is introduced into the CNS, but not the serum), efflux of glucose can be shown. [Pg.29]

Calcium is absorbed from the intestine by facilitated diffusion and active transport. In the former, Ca " moves from the mucosal to the serosal compartments along a concentration gradient. The active transport system requires a cation pump. In both processes, a calcium-binding protein (CaBP) is thought to be required for the transport. Synthesis of CaBP is activated by 1,25-DHCC. In the active transport, release of Ca " from the mucosal cell into... [Pg.376]

All of the transport systems examined thus far are relatively large proteins. Several small molecule toxins produced by microorganisms facilitate ion transport across membranes. Due to their relative simplicity, these molecules, the lonophore antibiotics, represent paradigms of the mobile carrier and pore or charmel models for membrane transport. Mobile carriers are molecules that form complexes with particular ions and diffuse freely across a lipid membrane (Figure 10.38). Pores or channels, on the other hand, adopt a fixed orientation in a membrane, creating a hole that permits the transmembrane movement of ions. These pores or channels may be formed from monomeric or (more often) multimeric structures in the membrane. [Pg.321]

In addition to the passive diffusional processes over lipid membranes or between cells, substances can be transferred through the lipid phase of biological membranes through specialized systems, i.e., active transport and facilitated diffusion. Until recently, the active transport component has been discussed only for nutrients or endogenous substances (e.g., amino acids, sugars, bile acids, small peptides), and seemed not to play any major role in the absorption of pharmaceuticals. However, sufficient evidence has now been gathered to recognize the involvement of transporters in the disposition of pharmaceuticals in the body [50, 127]. [Pg.113]

Diffusion medium properties for the PEFC system were most recently reviewed by Mathias et al. The primary purpose of a diffusion medium or gas diffusion layer (GDL) is to provide lateral current collection from the catalyst layer to the current collecting lands as well as uniform gas distribution to the catalyst layer through diffusion. It must also facilitate the transport of water out of the catalyst layer. The latter function is usually fulfilled by adding a coating of hydrophobic polymer such as poly(tet-rafluoroethylene) (PTFE) to the GDL. The hydrophobic polymer allows the excess water in the cathode catalyst layer to be expelled from the cell by gas flow in the channels, thereby alleviating flooding. It is known that the electric conductivity of GDL is... [Pg.492]

The resorption process is facilitated by the large inner surface of the intestine, with its brush-border cells. Lipophilic molecules penetrate the plasma membrane of the mucosal cells by simple diffusion, whereas polar molecules require transporters (facilitated diffusion see p. 218). In many cases, carrier-mediated cotransport with Na"" ions can be observed. In this case, the difference in the concentration of the sodium ions (high in the intestinal lumen and low in the mucosal cells) drives the import of nutrients against a concentration gradient (secondary active transport see p. 220). Failure of carrier systems in the gastrointestinal tract can result in diseases. [Pg.272]

Carrier-mediated passage of a molecular entity across a membrane (or other barrier). Facilitated transport follows saturation kinetics ie, the rate of transport at elevated concentrations of the transportable substrate reaches a maximum that reflects the concentration of carriers/transporters. In this respect, the kinetics resemble the Michaelis-Menten behavior of enzyme-catalyzed reactions. Facilitated diffusion systems are often stereo-specific, and they are subject to competitive inhibition. Facilitated transport systems are also distinguished from active transport systems which work against a concentration barrier and require a source of free energy. Simple diffusion often occurs in parallel to facilitated diffusion, and one must correct facilitated transport for the basal rate. This is usually evident when a plot of transport rate versus substrate concentration reaches a limiting nonzero rate at saturating substrate While the term passive transport has been used synonymously with facilitated transport, others have suggested that this term may be confused with or mistaken for simple diffusion. See Membrane Transport Kinetics... [Pg.278]

The Permease Systems of Bacteria. The best defined of these is the galactoside permease of E. coli. This transport system mediates the active accumulation of galactosides in the presence of metabolic energy and the facilitated diffusion of these compounds when the energy system is blocked (8). A specific galactoside-binding protein has been implicated, but it seems clear that the system is different from the phosphotransferase system described above since no covalent intermediates of... [Pg.275]

The various proposed components of the permease system are based upon the response of the transport system to genetic or environmental changes. The complex nature postulated for the intact permease system is necessary to account for the various observed phenomena such as facilitated diffusion, active concentration, facilitated efflux, exchange diffusion, and counter transport of one compound driven by the downhill efflux of a second (2). [Pg.276]


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See also in sourсe #XX -- [ Pg.423 , Pg.423 , Pg.424 , Pg.426 , Pg.427 , Pg.427 ]




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Diffusion facilitated

Diffusion systems

Diffusion transporters

Diffusive systems

Facilitated diffusion transport

Facilitated transport

Facilitated transporters

Facilitative diffusion

Facilitative transport

Facilitators

Facilitization

Systemic Transport

Transport diffusive

Transport systems

Transport systems/transporters

Transport systems/transporters facilitated diffusion

Transport systems/transporters facilitated diffusion

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