Human Mitochondrial Thymidine Kinase Is Selectively Inhibited by 3′-Thiourea Derivatives of β-Thymidine: Identification of Residues Crucial for Both Inhibition and Catalytic Activity

Balzarini, Jan; Daele, Ineke Van; Negri, Ana; Solaroli, Nicola; Karlsson, Anna; Liekens, Sandra; Gago, Federico; Calenbergh, Serge Van

doi:10.1124/mol.108.053785

Cited by 12 publications

(25 citation statements)

References 40 publications

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“…It is also interesting to note that 14a and 14b, both containing a BVDU moiety in place of the thymine, are only marginally more potent than 8c and 8f, respectively, an observation that is in line with the facts that (i) the Km value of BVDU when used as a substrate for Dm-DNK is only ~4-fold lower than that of AZT, 25 (ii) the nucleobase-binding site in Dm-DNK and human TK2 are highly comparable, and (iii) AZT and BVDU binding to Dm-DNK show similar characteristics, as inferred from comparison of PDB structures 2JJ8 and 2VQS. Finally, our finding that a 5'-O-trityl substituent renders the inhibitors in the present series inactive is also consistent with the proposed binding mode in so far as the 5'-hydroxyl is used, as described above and reported previously for thiourea-derived inhibitors, 11 to anchor the inhibitor in the substrate binding site through hydrogen bonding interactions with the catalytically important Arg134 and Glu81.…”

Section: +supporting

confidence: 92%

3′-[4-Aryl-(1,2,3-triazol-1-yl)]-3′-deoxythymidine Analogues as Potent and Selective Inhibitors of Human Mitochondrial Thymidine Kinase

Poecke

Negri²,

Gago³

et al. 2010

J. Med. Chem.

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Abbreviations: TK: thymidine kinase; HSV: herpes simplex virus; VZV, varicella zoster virus; Dm: Drosophila melanogaster; dNK: deoxynucleoside kinase; dThd: thymidine; AZT: azidothymidine. 2Abstr act In an effort to increase the potency and selectivity of earlier identified substrate-based inhibitors of mitochondrial thymidine kinase 2 (TK-2), we now describe the synthesis of new thymidine analogues containing a 4-or 5-substituted 1,2,3-triazol-1-yl substituent at the 3'-position of the 2'-deoxyribofuranosyl ring. These analogues were prepared by Cu-and Ru-catalysed cycloadditions of 3'-azido-3'-deoxythymidine and the appropriate alkynes, which produced the 1,4-and 1,5-triazoles, respectively. Selected analogues showed nanomolar inhibitory activity for TK-2, while virtually not affecting the TK-1 counterpart. Enzyme kinetics indicated a competitive and uncompetitive inhibition profile against thymidine and the co-substrate ATP, respectively. This behavior is rationalized by suggesting that the inhibitors occupy the substrate-binding site in a TK-2-ATP complex that maintains the enzyme's active site in a closed conformation through the stabilization of a small lid domain.

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Section: +supporting

confidence: 92%

3′-[4-Aryl-(1,2,3-triazol-1-yl)]-3′-deoxythymidine Analogues as Potent and Selective Inhibitors of Human Mitochondrial Thymidine Kinase

Poecke

Negri²,

Gago³

et al. 2010

J. Med. Chem.

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“…Since our last report in 2008 [29], the research on TK2 inhibitors has been headed mainly by Van Calenbergh and collaborators who reported in 2009 a series of 3´-substituted thymidine derivatives as potent and selective inhibitors of human TK2 (Fig. 6) [40]. Originally designed and evaluated as inhibitors of Mycobacterium tuberculosis thymidylate kinase (TMPKmt) [41], the 3´-thiourea-dThd derivatives 24-31( Fig.…”

Section: Chemical Structures Of Tk2 Inhibitors: From Nucleosides To Amentioning

confidence: 99%

“…Thus it may be concluded that the acyclic nucleoside inhibitors occupy the thymidine binding site of TK2 only when the cosubstrate ATP is already bound to the enzyme. As regards the 3´-substituted nucleosides, the kinetic properties of compounds 30 [40] and 38 [42] have also been investigated against TK2. When tested against variable concentrations of dThd, these inhibitors inhibited TK2 in a purely competitive fashion with considerable low K i values of 0.054 and 0.012 μM, respectively.…”

Section: Kinetic Analysis Of Tk2 Inhibitors and Biological Studiesmentioning

confidence: 99%

Recent Advances in Thymidine Kinase 2 (TK2) Inhibitors and New Perspectives for Potential Applications

Priego

Karlsson²,

Gago³

et al. 2012

CPD

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Thymidine kinase 2 (TK2), encoded on chromosome 16q22 of the human genome, is a deoxynucleoside kinase (dNK) that catalyzes the phosphorylation of the pyrimidine deoxynucleosides 2'-deoxythymidine (dThd), 2'-deoxyuridine (dUrd) and 2'- deoxycytidine (dCyd) to the corresponding deoxynucleoside 5'-monophosphate derivatives. In contrast to the S-phase-specific thymidine kinase 1 (TK1), TK2 is constitutively expressed in the mitochondria and plays an important role in providing dNTPs for the replication and maintenance of mitochondrial DNA (mtDNA). The severe mitochondrial DNA depletion syndrome (MDS) has been associated with mutations in TK2, resulting in mtDNA depletion, isolated skeletal myopathy, and death of the individual at an early stage of life. Some antiviral nucleoside analogs, such as 3'-azido-dThd (AZT) that is targeting the human immunodeficiency virus (HIV)-encoded reverse transcriptase, are substrates for TK2 and it has been proposed that the mitochondrial toxicity observed after prolonged treatment with such drugs could be due to their interaction with TK2. Therefore, the design of specific TK2 inhibitors may be useful to investigate the role of TK2 in the maintenance and homeostasis of mitochondrial dNTP pools and its contribution to the mitochondrial toxicity of several antiviral and anticancer drugs. Since 2000, several potent and selective TK2 inhibitors have been described. Besides bringing together previously reported inhibitors, special attention will be paid in this review to the new families of TK2 inhibitors more recently described, together with modeling studies and biological assays. Moreover, the last section will be focused on several recent investigations that suggest that depletion of mtDNA can take place both in tumorigenesis and during cancer treatment with certain nucleoside analogues.

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“…21 Moreover, 5′-thiourea α-thymidine derivatives were completely inactive against human thymidine kinase 1 and only showed weak inhibition of human mitochondrial nucleoside kinase TK-2. 22,23 …”

Section: Introductionmentioning

confidence: 99%

Synthesis and Evaluation of α-Thymidine Analogues as Novel Antimalarials

et al. 2012

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Plasmodium falciparum thymidylate kinase (PfTMPK) is a key enzyme in pyrimidine nucleotide biosynthesis. 3-Trifluoromethyl-4-chloro-phenyl-urea-α-thymidine has been reported as an inhibitor of Mycobacterium tuberculosis TMPK (MtTMPK). Starting from this point, we designed, synthesized and evaluated a number of thymidine analogues as antimalarials. Both 5′-urea-α- and β-thymidine derivatives were moderate inhibitors of PfTMPK and furthermore showed moderate inhibition of parasite growth. The structure of several enzyme–inhibitor complexes provides a basis for improved inhibitor design. However, we found that certain 5′-urea-α-thymidine analogues had antimalarial activity where inhibition of PfTMPK is not the major mode of action. Optimization of this series resulted in a compound with potent antimalarial activity (EC50 = 28 nM; CC50 = 29 μM).

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Human Mitochondrial Thymidine Kinase Is Selectively Inhibited by 3′-Thiourea Derivatives of β-Thymidine: Identification of Residues Crucial for Both Inhibition and Catalytic Activity

Cited by 12 publications

References 40 publications

3′-[4-Aryl-(1,2,3-triazol-1-yl)]-3′-deoxythymidine Analogues as Potent and Selective Inhibitors of Human Mitochondrial Thymidine Kinase

3′-[4-Aryl-(1,2,3-triazol-1-yl)]-3′-deoxythymidine Analogues as Potent and Selective Inhibitors of Human Mitochondrial Thymidine Kinase

Recent Advances in Thymidine Kinase 2 (TK2) Inhibitors and New Perspectives for Potential Applications

Synthesis and Evaluation of α-Thymidine Analogues as Novel Antimalarials

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