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NADPH phosphate

ATP + [hydroxymethylglutaryl-CoA reductase (NADPH)] = ADP + [hydroxy-methylglutaryl-CoA reductase (NADPH)] phosphate (EC 1.1.1.34 hydroxy-methylglutaryl-CoA reductase (NADPH) is inactivated by the phosphorylation of the enzyme protein. Histones can also act as acceptors.)... [Pg.466]

MeSOTf acid methylsulfenyl triflate NADPH phosphate, oxidized form nicotinamide adenine dinucleotide... [Pg.1800]

Step 2 The ketone carbonyl of the acetoacetyl group is reduced to an alcohol function This reduction requires NADPH as a coenzyme (NADPH is the phosphate ester of NADH and reacts similarly to it)... [Pg.1076]

Indicators There are certain compounds that are suitable as indicators for sensitive and specific clinical analysis. Nicotinamide adenine dinucleotide (NAD) occurs in oxidized (NAD" ) and reduced (NADH) forms. Nicotinamide adenine dinucleotide phosphate (NADP) also has two states, NADP" and NADPH. NADH has a very high uv—vis absorption at 339 nm, extinction coefficient = 6300 (M cm) , but NAD" does not. Similarly, NADPH absorbs light very strongly whereas NADP" does not. [Pg.38]

Two or more linked enzyme reactions can lead to a change in the concentration of NADH or NADPH that is equivalent to the concentration of the original analyte. The reference glucose measurement using hexokinase [9001-51-8] and glucose-6-phosphate dehydrogenase [9001-40-5] is an example ... [Pg.38]

NADP = nicotinamide-adenine dinucleotide phosphate NADPH = reduced nicotinamide—adenine dinucleotide phosphate NDP = nucleoside... [Pg.19]

NAD" — see Nicotinamide adenine dinucleotide NADP" — see Nicotinamide adenine dinucleotide phosphate NADPH... [Pg.705]

Nicotinamide adenine dinucleotide phosphate reduced tetrasodium salt (reduced diphosphopyridine nucleotide phosphate sodium salt, NADPH) [2646-71-1] M 833.4, pK as for NADP. Mostly similar to NADH above. [Pg.552]

Nicotinamide is an essential part of two important coenzymes nicotinamide adenine dinucleotide (NAD ) and nicotinamide adenine dinucleotide phosphate (NADP ) (Figure 18.19). The reduced forms of these coenzymes are NADH and NADPH. The nieotinamide eoenzymes (also known as pyridine nucleotides) are electron carriers. They play vital roles in a variety of enzyme-catalyzed oxidation-reduction reactions. (NAD is an electron acceptor in oxidative (catabolic) pathways and NADPH is an electron donor in reductive (biosynthetic) pathways.) These reactions involve direct transfer of hydride anion either to NAD(P) or from NAD(P)H. The enzymes that facilitate such... [Pg.588]

Most of the enzymes mediating the reactions of the Calvin cycle also participate in either glycolysis (Chapter 19) or the pentose phosphate pathway (Chapter 23). The aim of the Calvin scheme is to account for hexose formation from 3-phosphoglycerate. In the course of this metabolic sequence, the NADPH and ATP produced in the light reactions are consumed, as indicated earlier in Equation (22.3). [Pg.733]

BOTH RIBOSE-5-P AND NADPH ARE NEEDED BY THE CELL In this case, the first four reactions of the pentose phosphate pathway predominate (Figure 23.37). N/VDPH is produced by the oxidative reactions of the pathway, and ribose-5-P is the principal product of carbon metabolism. As stated earlier, the net reaction for these processes is... [Pg.769]

MORE RIBOSE-5-P THAN NADPH IS NEEDED BY THE CELL Synthesis of ribose-5-P can be accomplished without production of N/VDPH if the oxidative steps of the pentose phosphate pathway are bypassed. The key to this route is the extrac-... [Pg.769]

FIGURE 23.37 Wlien biosynthetic demands dictate, the first four reactions of the pentose phosphate pathway predominate and the principal products are ribose-5-P and NADPH. [Pg.770]

MORE NADPH THAN RmOSE-5-P IS NEEDED BY THE CELL Large amounts of N/VDPH can be supplied for biosynthesis without concomitant production of ribose-5-P, if ribose-5-P produced in the pentose phosphate pathway is recycled to produce glycolytic intermediates. As shown in Figure 23.39, this alternative involves a complex interplay between the transketolase and transaldolase reac-... [Pg.770]

FIGURE 23.40 Both ATP and NADPH (as well as NADH) can be produced by this version of the pentose phosphate and glycolytic pathways. [Pg.772]

NADPH can be produced in the pentose phosphate pathway as well as by malic enzyme (Figure 25.1). Reducing equivalents (electrons) derived from glycolysis in the form of NADH can be transformed into NADPH by the combined action of malate dehydrogenase and malic enzyme ... [Pg.805]

How many of the 14 NADPH needed to form one palmitate (Eq. 25.1) can be made in this way The answer depends on the status of malate. Every citrate entering the cytosol produces one acetyl-CoA and one malate (Figure 25.1). Every malate oxidized by malic enzyme produces one NADPH, at the expense of a decarboxylation to pyruvate. Thus, when malate is oxidized, one NADPH is produced for every acetyl-CoA. Conversion of 8 acetyl-CoA units to one palmitate would then be accompanied by production of 8 NADPH. (The other 6 NADPH required [Eq. 25.1] would be provided by the pentose phosphate pathway.) On the other hand, for every malate returned to the mitochondria, one NADPH fewer is produced. [Pg.805]

In living organisms, aldehyde and ketone reductions are carried out by either of the coenzymes NADH (reduced nicotinamide adenine dinucleotide) or NADPH (reduced nicotinamide adenine dinucleotide phosphate). Although... [Pg.610]

The first step in the biological degradation of lysine is reductive animation with a-ketoglutarate to give saccharopine. Nicotinamide adenine dinucleotide phosphate (NADPH), a relative of NADH, is the reducing agent. Show the mechanism. [Pg.1059]

All NOS isoforms utilize L-arginine as the substrate, and molecular oxygen and reduced nicotinamide adenine dinucleotide phosphate (NADPH) as cosubstrates. Flavin adenine dinucleotide (FMN), flavin mononucleotide (FAD), and (6R)-5,6,7,8-tetrahydro-L-biopterin (BH4) are cofactors of the enzyme. All NOS isoforms contain heme and bind calmodulin. In nNOS and eNOS,... [Pg.862]

TPP-dependent enzymes are involved in oxidative decarboxylation of a-keto acids, making them available for energy metabolism. Transketolase is involved in the formation of NADPH and pentose in the pentose phosphate pathway. This reaction is important for several other synthetic pathways. It is furthermore assumed that the above-mentioned enzymes are involved in the function of neurotransmitters and nerve conduction, though the exact mechanisms remain unclear. [Pg.1288]

Ethanol is oxidized by alcohol dehydrogenase (in the presence of nicotinamide adenine dinucleotide [NAD]) or the microsomal ethanol oxidizing system (MEOS) (in the presence of reduced nicotinamide adenine dinucleotide phosphate [NADPH]). Acetaldehyde, the first product in ethanol oxidation, is metabolized to acetic acid by aldehyde dehydrogenase in the presence of NAD. Acetic acid is broken down through the citric acid cycle to carbon dioxide (CO2) and water (H2O). Impairment of the metabolism of acetaldehyde to acetic acid is the major mechanism of action of disulfiram for the treatment of alcoholism. [Pg.6]


See other pages where NADPH phosphate is mentioned: [Pg.466]    [Pg.467]    [Pg.469]    [Pg.469]    [Pg.469]    [Pg.469]    [Pg.466]    [Pg.467]    [Pg.469]    [Pg.469]    [Pg.469]    [Pg.469]    [Pg.176]    [Pg.274]    [Pg.298]    [Pg.28]    [Pg.39]    [Pg.40]    [Pg.39]    [Pg.40]    [Pg.712]    [Pg.733]    [Pg.736]    [Pg.809]    [Pg.1074]    [Pg.862]    [Pg.865]    [Pg.194]    [Pg.229]   


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