Hydroxynaphthaldehyde Phosphate Derivatives as Potent Covalent Schiff Base Inhibitors of Fructose-1,6-bisphosphate Aldolase

Dax, Chantal; Coincon, M.; Sygusch, J.; Blonski, Casimir

doi:10.1021/bi0477992

Cited by 18 publications

(28 citation statements)

References 52 publications

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“…Similarly to salicylic derivative 44 , the presence of the hydroxyl group ortho to the aldehyde in 46 proved to be essential in determining its mechanism of action (Schiff base formation). [161] Hexitol diphosphate, consisting in a diastereoisomeric mixture of glucitol bisphosphate ( 47 ) and mannitol bisphosphate ( 48 ), had been known a long time as a competitive inhibitor of class I muscle ALD ( K i ~1.2 μM). [162] More recently 47 and 48 were separately tested on rabbit muscle aldolase, and they both behaved as competitive inhibitors with K i values of 100 μM ( 47 ) and 7.3 μM ( 48 ).…”

Section: Glycolytic Effectors As Potential Targets In Cancer Therapymentioning

confidence: 99%

Anticancer Agents That Counteract Tumor Glycolysis

2012

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Can we consider cancer as a “metabolic disease”? Tumors are the result of a metabolic selection, forming tissues composed of heterogeneous cells that generally express an overactive metabolism as a common feature. In fact, cancer cells have to deal with increased needs for both energy and biosynthetic intermediates, in order to support their growth and invasiveness. However, their high proliferation rate often generates regions that are not sufficiently oxygenated. Therefore, their carbohydrate metabolism has to rely mostly on a glycolytic process that is uncoupled from oxidative phosphorylation. This metabolic switch, also known as the “Warburg Effect”, constitutes a fundamental adaptation of the tumor cells to a relatively hostile environment, and supports the evolution of aggressive and metastatic phenotypes. As a result, tumor glycolysis may constitute an attractive target for cancer therapy. This approach has often raised concerns that anti-glycolytic agents may cause serious side effects on normal cells. Actually, the key for a selective action against cancer cells can be found in their hyperbolic addiction to glycolysis, which may be exploited to generate new anti-cancer drugs showing minimal toxicity. In fact, there is growing evidence that supports many glycolytic enzymes and transporters as suitable candidate targets for cancer therapy. Herein we review some of the most relevant anti-glycolytic agents that have been investigated so far for the treatment of cancer.

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Section: Glycolytic Effectors As Potential Targets In Cancer Therapymentioning

confidence: 99%

Anticancer Agents That Counteract Tumor Glycolysis

2012

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“…This species, whose presence was confirmed by spiking the STS-catalyzed reaction with an authentic sample of independently synthesized 4-diFME1 [3] (Figure 3 F), is formed as an unstable intermediate and rapidly decomposes to give 4-FE1 ( Figure 3 F and G). Because aldehydes have been known to act as highly potent and sometimes almost irreversible enzyme inhibitors, [10] we reasoned that inactivation of STS by compound 4 might be mainly due to inhibition by 4-FE1. Indeed, incubation of STS with just 4-FE1 resulted in time and concentration-dependent inhibition of STS (Figure 4 A).…”

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“…[13] Although the site of STS modification by 4-FE1 has yet to be established, it is highly likely that it is forming a Schiff base with an active-site residue because it has been shown that certain aldehydes can function as almost irreversible enzyme inhibitors through the formation of stable Schiff base adducts with residues bearing side-chain amines. [10] Lys368 in the active site of STS is a strong candidate for Schiff base formation A C H T U N G T R E N N U N G because it is in close proximity to the 4-position of estrone, which has been modeled into the active site of STS. [14] It is possible that the formyl group of 2-FE1 cannot attain the correct geometry or is too far removed from Lys368 to form a stable Schiff base.…”

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Multiple Pathways for the Irreversible Inhibition of Steroid Sulfatase with Quinone Methide‐Generating Suicide Inhibitors

2009

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Unexpected inhibition: 2‐ and 4‐mono‐ and difluoromethyl estrone sulfate derivatives are suicide inhibitors of steroid sulfatase (STS). Kinetic studies suggest that inhibition by the monofluoro derivatives is a result of a quinone methide intermediate that reacts with active‐site nucleophiles, whereas the main inhibition pathway of the 4‐difluoromethyl derivative is a result of decomposition of the initial quinone methide to an aldehyde that acts as potent, almost irreversible inhibitor.magnified image

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“…Schistosome cells express FBPA that upon degradation give rise to similar antigenic peptides that are presented on the cell surface complexed with MHC class I molecules (MHC I), that greatly affects the antigenic peptide repertoire presented to cytotoxic T lymphocytes (Apcher et al 2010;Zervoudi et al 2013), and as a result cannot develops cytotoxic cellular responses contributing to immune evasion by schistosome cells. Unlike the other molecules of S. japonicum, such as protein arginine methyltransferase 1 and allergen-like protein 1, which could induce mouse bone marrow-derived dendritic cell (BMDC) to mature and therefore activate their immune response (Diao et al 2014), or induce a polarized Th2 immune response by increasing specific antibody significantly in S. japonicum-infected mice (Chen et al 2010), sjFBPA contains similar antigenic peptides with that of human FBPAs and may contribute to immune evasion of S. japonicum from their host, human being. This result would be confirmed by some animal experiment.…”

Section: Discussionmentioning

confidence: 99%

Cloning, expression, and partial characterization of FBPA from Schistosoma japonicum, a molecule on that the fluke may develop nutrition competition and immune evasion from human

Xie

Zhu

et al. 2015

Parasitol Res

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Carbohydrate metabolism is the most important physiological process for Schistosoma japonicum which resides in host. However, as a key glycolytic enzyme in carbohydrate metabolism, fructose-1,6-bisphosphate aldolase (FBPA), there is no study on its enzymatic kinetics and antigenic peptides. Here, we report the gene cloning, expression, purification, and kinetics of the FBPA from S. japonicum (sjFBPA). After cloning, sjFBPA gene was introduced into pET-28a and transformed BL21, and a soluble His6-sjFBPA was expressed and purified successfully at the expected molecular mass of ~45 kDa. We first reported that the diversities in IGS regions and the features of residues position 346 and 357-362 of sjFBPA may be conferred either through conformational changes influencing easily the active site from a distance and/or causing the C-terminal region to interact directly with the active site, which lead His6-sjFBPA to exhibit a higher specific activity of 197.43 units/mg and degrades FBP with a typical substrate inhibition model and a higher efficiency of k cat = 6261.3/s and K m = 0.061 μM than human aldolases, which might be the strategy that S. japonicum gaining energy and surviving in its environment with low concentration of carbohydrate, and benefitting to get more metabolic substances for parasites in nutrition competition with their host. sjFBPA exhibits a high similarity of 81.46 % with that of hosts, especially in antigenic peptide regions, and 14 of 15 antigenic peptides of sjFBPA were conserved to those of human aldolase A, B, and/or C with high identity (17, 16, or 16 antigenic peptides, respectively), which may result in a molecular mimicry of FBPA with that of host, and an immune evasion from their hosts. This work would supply an experimental base for using FBPA to prevent the schistosomiasis in the future.

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Hydroxynaphthaldehyde Phosphate Derivatives as Potent Covalent Schiff Base Inhibitors of Fructose-1,6-bisphosphate Aldolase

Cited by 18 publications

References 52 publications

Anticancer Agents That Counteract Tumor Glycolysis

Anticancer Agents That Counteract Tumor Glycolysis

Multiple Pathways for the Irreversible Inhibition of Steroid Sulfatase with Quinone Methide‐Generating Suicide Inhibitors

Cloning, expression, and partial characterization of FBPA from Schistosoma japonicum, a molecule on that the fluke may develop nutrition competition and immune evasion from human

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