“Nucleotide pyrophosphatase/phosphodiesterase”的意思、由来-开放百科全书

The catalytic site of NPP consists of a two-metal-ion (bimetallo) Zn²⁺ catalytic core. These Zn²⁺ catalytic components are thought to stabilize the transition state of the NPP phosphoryl transfer reaction.^[7]

Mechanism

Overview

NPP catalyses the nucleophilic substitution of one ester bond on a phosphodiester substrate. It has a nucleoside binding pocket that excludes phospholipid substrates from the active site.^[8] A threonine nucleophile has been identified through site-directed mutagenesis,^[9]^[10]^[11] and the reaction inverts the stereochemistry of the phosphorus center.^[12] The sequence of bond breakage and formation has yet to be resolved.

Ongoing Investigation

Three extreme possibilities have been proposed for the mechanism of NPP-catalyzed phosphoryl transfer. They are distinguished by the sequence in which bonds to phosphorus are made and broken. Though this phenomenon is subtle, it is important for understanding the physiological roles of AP superfamily enzymes, and also to molecular dynamic modeling.

Extreme mechanistic scenarios:1) A two-step "dissociative" (elimination-addition or D_N + A_N) mechanism that proceeds via a trigonal metaphosphate intermediate.^[13] This mechanism is represented by the red dashed lines in the figure at right.

2) A two-step "associative" (addition-elimination or A_N + D_N) mechanism that proceeds via a pentavalent phosphorane intermediate.^[13] This is represented by the blue dashed lines in the figure at right.

3) A one-step fully synchronous mechanism analogous to S_N2 substitution. Bond formation and breakage occur simultaneously and at the same rate. This is represented by the black dashed line in the figure at right.

The above three cases represent archetypes for the reaction mechanism, and the actual mechanism probably falls somewhere in between them.^[13]^[14] The red and blue dotted lines in Fig. 2a represent more realistic "concerted" mechanisms in which addition and elimination overlap, but are not fully synchronous. The difference in initial rates of the two steps implies different charge distribution in the transition state (TS).

When the addition step occurs more quickly than elimination (an A_ND_N mechanism),^[13] more positive charge develops on the nucleophile, and the transition state is said to be "tight."^[6]^[14] Conversely, if elimination occurs more quickly than addition (D_NA_N), the transition state is considered "loose."

López-Canut et al. modeled substitution of a phosphodiester substrate using a hybrid quantum mechanics/molecular mechanics model.^[14] Notably, the model predicted an A_ND_N concerted mechanism in aqueous solution, but a D_NA_N mechanism in the active site of Xac NPP.

Promiscuity

Although NPP primarily catalyzes phosphodiester hydrolysis, the enzyme will also catalyze the hydrolysis of phosphate monoesters, though to a much smaller extent. NPP preferentially hydrolyzes phosphate diesters over monoesters by factors of 10²-10⁶, depending on the identity of the diester substrate. This ability to catalyze a reaction with a secondary substrate is known as enzyme promiscuity,^[6] and may have played a role in NPP’s evolutionary history.^[15]

NPP’s promiscuity enables the enzyme to share substrates with alkaline phosphatase (AP), another member of the alkaline phosphate superfamily. Alkaline phosphatase primarily hydrolyzes phosphate monoester bonds, but it shows some promiscuity towards hydrolyzing phosphate diester bonds, making it a sort of opposite to NPP. The active sites of these two enzymes show marked similarities, namely in the presence of nearly superimposable Zn²⁺ bimetallo catalytic centers. In addition to the bimetallo core, AP also has an Mg²⁺ ion in its active site.^[6]

Biological function

NPPs have been implicated in several biological processes, including bone mineralization, purine nucleotide and insulin signaling, and cell differentiation and motility. They are generally regulated at the transcriptional level.^[12]

Mammalian Isoforms

Nucleotide pyrophosphatase/phosphodiesterase I

The pyrophosphate produced by NPP1 in bone cells is thought to serve as both a phosphate source for calcium phosphate deposition and as an inhibitory modulator of calcification.^[17] NPP1 appears to be important for maintaining pyrophosphate/phosphate balance. Overactivity of the enzyme is associated with chondrocalcinosis, while deficiency correlates to pathological calcification.^[5]

NPP1 inhibits the insulin receptor in vitro. In 2005, overexpression of the isoform was implicated in insulin resistance in mice.^[18] It has been linked to insulin resistance and Type 2 diabetes in humans.^[12]

NPP2

NPP2, known in humans as autotaxin, acts primarily in cell motility pathways. With its active site functioning, NPP2 promotes cellular migration at picomolar concentrations.^[12] Soluble splice variants of NPP2 are thought to be important to cancer metastasis, and also show angiogenic properties in tumors.^[5]

NPP3

NPP3 is probably a major contributor to nucleotide metabolism in the intestine and liver.^[12]

The liver releases ATP and ADP into the bile to regulate bile secretion.^[20] It subsequently reclaims adenosine via a pathway that probably contains NPP3.^[21]

Evolution

NPP belongs to the alkaline phosphatase superfamily, which is a group of evolutionarily related enzymes that catalyze phosphoryl and sulfuryl transfer reactions. This group includes phosphomonoesterases, phosphodiesterases, phosphoglycerate mutases, phosphophenomutases, and sulfatases.^[22]

References

1. ^Enzyme Promiscuity, Evolution, and Phosphoryl Transfer. Herschlag Lab. Stanford University, Retrieved 1 March 2012.
2. ^{{Cite journal| last = Terkeltaub| first = Robert| date = 2006-06-01| title = Physiologic and pathologic functions of the NPP nucleotide pyrophosphatase/phosphodiesterase family focusing on NPP1 in calcification| journal = Purinergic Signalling| language = en| volume = 2| issue = 2| pages = 371–377| doi = 10.1007/s11302-005-5304-3| issn = 1573-9538| pmc = 2254483| pmid = 18404477}}
3. ^Pham, Truc Chi T.; Wanjala, Irene; Howard, Angela; Parrill, Abby L.; Baker, Daniel L. "Insights into the structure and function of lipid preferring Nucleotide PyrophosphotasePhosphodiesterase isoforms" 2011
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Structure