Your search keyword '"Zheleva DI"' showing total 13 results

1. Discovery and characterization of 2-anilino-4- (thiazol-5-yl)pyrimidine transcriptional CDK inhibitors as anticancer agents.

Author

Wang S, Griffiths G, Midgley CA, Barnett AL, Cooper M, Grabarek J, Ingram L, Jackson W, Kontopidis G, McClue SJ, McInnes C, McLachlan J, Meades C, Mezna M, Stuart I, Thomas MP, Zheleva DI, Lane DP, Jackson RC, Glover DM, Blake DG, and Fischer PM

Subjects

Animals, Antineoplastic Agents therapeutic use, Apoptosis, Binding Sites, Cell Line, Tumor, Computer Simulation, Cyclin-Dependent Kinases genetics, Cyclin-Dependent Kinases metabolism, Disease Models, Animal, Drug Evaluation, Preclinical, Humans, Leukemia drug therapy, Mice, Protein Kinase Inhibitors therapeutic use, Pyrimidines therapeutic use, Transcription, Genetic drug effects, Tumor Suppressor Protein p53 metabolism, Antineoplastic Agents chemistry, Cyclin-Dependent Kinases antagonists & inhibitors, Protein Kinase Inhibitors chemistry, Pyrimidines chemistry

Abstract

The main difficulty in the development of ATP antagonist kinase inhibitors is target specificity, since the ATP-binding motif is present in many proteins. We introduce a strategy that has allowed us to identify compounds from a kinase inhibitor library that block the cyclin-dependent kinases responsible for regulating transcription, i.e., CDK7 and especially CDK9. The screening cascade employs cellular phenotypic assays based on mitotic index and nuclear p53 protein accumulation. This permitted us to classify compounds into transcriptional, cell cycle, and mitotic inhibitor groups. We describe the characterization of the transcriptional inhibitor class in terms of kinase inhibition profile, cellular mode of action, and selectivity for transformed cells. A structural selectivity rationale was used to optimize potency and biopharmaceutical properties and led to the development of a transcriptional inhibitor, 3,4-dimethyl-5-[2-(4-piperazin-1-yl-phenylamino)-pyrimidin-4-yl]-3H-thiazol-2-one, with anticancer activity in animal models., (Copyright © 2010 Elsevier Ltd. All rights reserved.)

Published

2010

2. Discovery of N-phenyl-4-(thiazol-5-yl)pyrimidin-2-amine aurora kinase inhibitors.

Author

Wang S, Midgley CA, Scaërou F, Grabarek JB, Griffiths G, Jackson W, Kontopidis G, McClue SJ, McInnes C, Meades C, Mezna M, Plater A, Stuart I, Thomas MP, Wood G, Clarke RG, Blake DG, Zheleva DI, Lane DP, Jackson RC, Glover DM, and Fischer PM

Subjects

Adenosine Triphosphate metabolism, Animals, Aurora Kinase A, Aurora Kinases, Binding, Competitive, Cell Line, Tumor, Cell Proliferation drug effects, Humans, Inhibitory Concentration 50, Mice, Mitosis drug effects, Models, Molecular, Protein Conformation, Protein Kinase Inhibitors chemistry, Protein Kinase Inhibitors pharmacokinetics, Protein Serine-Threonine Kinases chemistry, Protein Serine-Threonine Kinases metabolism, Pyrimidines chemistry, Pyrimidines metabolism, Pyrimidines pharmacokinetics, Substrate Specificity, Thiazoles chemistry, Thiazoles metabolism, Thiazoles pharmacokinetics, Xenograft Model Antitumor Assays, Drug Discovery methods, Protein Kinase Inhibitors pharmacology, Protein Serine-Threonine Kinases antagonists & inhibitors, Pyrimidines pharmacology, Thiazoles pharmacology

Abstract

Through cell-based screening of our kinase-directed compound collection, we discovered that a subset of N-phenyl-4-(thiazol-5-yl)pyrimidin-2-amines were potent cytotoxic agents against cancer cell lines, suppressed mitotic histone H3 phosphorylation, and caused aberrant mitotic phenotypes. It was subsequently established that these compounds were in fact potent inhibitors of aurora A and B kinases. It was shown that potency and selectivity of aurora kinase inhibition correlated with the presence of a substituent at the aniline para-position in these compounds. The anticancer effects of lead compound 4-methyl-5-(2-(4-morpholinophenylamino)pyrimidin-4-yl)thiazol-2-amine (18; K(i) values of 8.0 and 9.2 nM for aurora A and B, respectively) were shown to emanate from cell death following mitotic failure and increased polyploidy as a consequence of cellular inhibition of aurora A and B kinases. Preliminary in vivo assessment showed that compound 18 was orally bioavailable and possessed anticancer activity. Compound 18 (CYC116) is currently undergoing phase I clinical evaluation in cancer patients.

Published

2010

3. Design, synthesis, and evaluation of 2-methyl- and 2-amino-N-aryl-4,5-dihydrothiazolo[4,5-h]quinazolin-8-amines as ring-constrained 2-anilino-4-(thiazol-5-yl)pyrimidine cyclin-dependent kinase inhibitors.

Author

McIntyre NA, McInnes C, Griffiths G, Barnett AL, Kontopidis G, Slawin AM, Jackson W, Thomas M, Zheleva DI, Wang S, Blake DG, Westwood NJ, and Fischer PM

Subjects

Aminoquinolines chemical synthesis, Antineoplastic Agents chemical synthesis, Antineoplastic Agents chemistry, Antineoplastic Agents pharmacology, Blotting, Western, Cell Line, Tumor, Cell Proliferation drug effects, Crystallography, X-Ray, Cyclin-Dependent Kinases chemistry, Cyclin-Dependent Kinases metabolism, Humans, Inhibitory Concentration 50, Magnetic Resonance Spectroscopy, Models, Molecular, Protein Kinase Inhibitors chemical synthesis, Protein Kinase Inhibitors pharmacology, Structure-Activity Relationship, Thiazoles chemical synthesis, Aminoquinolines chemistry, Aminoquinolines pharmacology, Cyclin-Dependent Kinases antagonists & inhibitors, Protein Kinase Inhibitors chemistry, Thiazoles chemistry, Thiazoles pharmacology

Abstract

Following the recent discovery and development of 2-anilino-4-(thiazol-5-yl)pyrimidine cyclin dependent kinase (CDK) inhibitors, a program was initiated to evaluate related ring-constrained analogues, specifically, 2-methyl- and 2-amino-N-aryl-4,5-dihydrothiazolo[4,5-h]quinazolin-8-amines for inhibition of CDKs. Here we report the rational design, synthesis, structure-activity relationships (SARs), and cellular mode-of-action profile of these second generation CDK inhibitors. Many of the analogues from this chemical series inhibit CDKs with very low nanomolar K(i) values. The most potent compound reported in this study inhibits CDK2 with an IC(50) of 0.7 nM ([ATP] = 100 microM). Furthermore, an X-ray crystal structure of 2-methyl-N-(3-(nitro)phenyl)-4,5-dihydrothiazolo[4,5-h]quinazolin-8-amine (11g), a representative from the chemical series in complex with cyclin A-CDK2, is reported, confirming the design rationale and expected binding mode within the CDK2 ATP binding pocket.

Published

2010

4. Structural and biochemical studies of human proliferating cell nuclear antigen complexes provide a rationale for cyclin association and inhibitor design.

Author

Kontopidis G, Wu SY, Zheleva DI, Taylor P, McInnes C, Lane DP, Fischer PM, and Walkinshaw MD

Subjects

Amino Acid Sequence, Crystallography, X-Ray, Cyclin-Dependent Kinase Inhibitor p21, Humans, Macromolecular Substances, Models, Molecular, Molecular Sequence Data, Peptides chemistry, Peptides genetics, Peptides metabolism, Sequence Alignment, Cell Cycle Proteins antagonists & inhibitors, Cell Cycle Proteins chemistry, Cell Cycle Proteins genetics, Cell Cycle Proteins metabolism, Cyclin-Dependent Kinases chemistry, Cyclin-Dependent Kinases metabolism, Cyclins chemistry, Cyclins metabolism, Proliferating Cell Nuclear Antigen chemistry, Proliferating Cell Nuclear Antigen genetics, Proliferating Cell Nuclear Antigen metabolism, Protein Structure, Quaternary

Abstract

The interactions between the tumor suppressor protein p21WAF1 and the cyclin-dependent kinase (CDK) complexes and with proliferating cell nuclear antigen (PCNA) regulate and coordinate the processes of cell-cycle progression and DNA replication. We present the x-ray crystal structure of PCNA complexed with a 16-mer peptide related to p21 that binds with a Kd of 100 nM. Two additional crystal structures of native PCNA provide previously undescribed structures of uncomplexed human PCNA and show that significant changes on ligand binding include rigidification of a number of flexible regions on the surface of PCNA. In the competitive binding experiments described here, we show that a 20-mer sequence from p21 can be associated simultaneously with PCNA and CDK/cyclin complexes. A structural model for this quaternary complex is presented in which the C-terminal sequence of p21 acts like double-sided tape and docks to both the PCNA and cyclin molecules. The quaternary complex shows little direct interaction between PCNA and cyclin, giving p21 the role of an adaptor molecule. Taken together, the biochemical and structural results delineate a druggable inhibitor site on the surface of PCNA that may be exploited in the design of peptidomimetics, which will act independently of cyclin-groove inhibitors.

Published

2005

5. Insights into cyclin groove recognition: complex crystal structures and inhibitor design through ligand exchange.

Author

Kontopidis G, Andrews MJ, McInnes C, Cowan A, Powers H, Innes L, Plater A, Griffiths G, Paterson D, Zheleva DI, Lane DP, Green S, Walkinshaw MD, and Fischer PM

Subjects

Amino Acid Motifs, Binding Sites, CDC2-CDC28 Kinases antagonists & inhibitors, CDC2-CDC28 Kinases chemistry, Crystallography, X-Ray, Cyclin A antagonists & inhibitors, Cyclin A chemistry, Cyclin-Dependent Kinase 2, Cyclin-Dependent Kinase Inhibitor p21, Humans, Ligands, Models, Molecular, Peptides chemistry, Protein Binding, Protein Conformation, Protein Structure, Secondary, Structure-Activity Relationship, Cyclins chemistry

Abstract

Inhibition of CDK2/CA (cyclin-dependent kinase 2/cyclin A complex) activity through blocking of the substrate recognition site in the cyclin A subunit has been demonstrated to be an effective method for inducing apoptosis in tumor cells. We have used the cyclin binding motif (CBM) present in the tumor suppressor proteins p21(WAF1) and p27(KIP1) as a template to optimize the minimal sequence necessary for CDK2/CA inhibition. A series of peptides were prepared, containing nonnatural amino acids, which possess nano- to micromolar CDK2-inhibitory activity. Here we present X-ray structures of the protein complex CDK2/CA, together with the cyclin groove-bound peptides H-Ala-Ala-Abu-Arg-Ser-Leu-Ile-(p-F-Phe)-NH(2) (peptide 1), H-Arg-Arg-Leu-Ile-Phe-NH(2) (peptide 2), Ac-Arg-Arg-Leu-Asn-(m-Cl-Phe)-NH(2) (peptide 3), H-Arg-Arg-Leu-Asn-(p-F-Phe)-NH(2) (peptide 4), and H-Cit-Cit-Leu-Ile-(p-F-Phe)-NH(2) (peptide 5). Some of the peptide complexes presented here were obtained through the novel technique of ligand exchange within protein crystals. This method may find general application for obtaining complex structures of proteins with surface-bound ligands.

Published

2003

6. The p53-Mdm2 pathway: targets for the development of new anticancer therapeutics.

Author

Zheleva DI, Lane DP, and Fischer PM

Subjects

Antineoplastic Agents chemistry, Genetic Therapy, Humans, Neoplasms metabolism, Neoplasms pathology, Protein Binding drug effects, Proto-Oncogene Proteins genetics, Proto-Oncogene Proteins c-mdm2, Tumor Suppressor Protein p53 chemistry, Tumor Suppressor Protein p53 genetics, Antineoplastic Agents pharmacology, Drug Design, Neoplasms drug therapy, Nuclear Proteins, Proto-Oncogene Proteins antagonists & inhibitors, Proto-Oncogene Proteins metabolism, Tumor Suppressor Protein p53 antagonists & inhibitors, Tumor Suppressor Protein p53 metabolism

Abstract

The tumour suppressor p53 is at the centre of a network of regulatory pathways that guard over the continued integrity of the living cell and its progeny after exposure to different forms of stress, particularly those capable of inducing DNA damage. Tumour cells very frequently circumvent this control by disabling the function of p53, or other proteins in the p53 network, through mutation. Here we review the different therapeutic strategies that have been adopted to exploit common neoplastic aberrations in the p53 pathways. We emphasise in particular those approaches where modulation with pharmaceutical agents has already shown some promise, including pharmacological rescue of mutant p53, modulation of the protein-protein interaction between p53 and one of its negative regulators, Mdm2, as well as interference with downstream targets.

Published

2003

7. Discovery of a novel family of CDK inhibitors with the program LIDAEUS: structural basis for ligand-induced disordering of the activation loop.

Author

Wu SY, McNae I, Kontopidis G, McClue SJ, McInnes C, Stewart KJ, Wang S, Zheleva DI, Marriage H, Lane DP, Taylor P, Fischer PM, and Walkinshaw MD

Subjects

Adenosine Triphosphate metabolism, Binding Sites, Cell Line, Tumor, Crystallography, X-Ray, Cyclin-Dependent Kinases chemistry, Cyclin-Dependent Kinases metabolism, Databases, Protein, Humans, Hydrogen Bonding, Ligands, Macromolecular Substances, Models, Molecular, Molecular Structure, Protein Binding, Pyridines chemistry, Pyridines metabolism, Cyclin-Dependent Kinases antagonists & inhibitors, Enzyme Inhibitors chemistry, Enzyme Inhibitors metabolism, Protein Structure, Secondary, Software

Abstract

A family of 4-heteroaryl-2-amino-pyrimidine CDK2 inhibitor lead compounds was discovered with the new database-mining program LIDAEUS through in silico screening. Four compounds with IC(50) values ranging from 17 to 0.9 microM were selected for X-ray crystal analysis. Two distinct binding modes are observed, one of which resembles the hydrogen bonding pattern of bound ATP. In the second binding mode, the ligands trigger a conformational change in the activation T loop by inducing movement of Lys(33) and Asp(145) side chains. The family of molecules discovered provides an excellent starting point for the design and synthesis of tight binding inhibitors, which may lead to a new class of antiproliferative drugs.

Published

2003

8. Peptidomimetic design of CDK inhibitors targeting the recruitment site of the cyclin subunit.

Author

McInnes C, Andrews MJ, Zheleva DI, Lane DP, and Fischer PM

Subjects

Animals, Antineoplastic Agents pharmacology, Binding Sites, Cell Cycle Proteins chemistry, Cyclin-Dependent Kinase Inhibitor p21, Cyclin-Dependent Kinase Inhibitor p27, Cyclins chemistry, Enzyme Inhibitors chemistry, Enzyme Inhibitors pharmacology, Enzyme Inhibitors therapeutic use, Humans, Models, Molecular, Peptides chemistry, Peptides pharmacology, Structure-Activity Relationship, Tumor Suppressor Proteins chemistry, Antineoplastic Agents chemistry, Cyclin-Dependent Kinases antagonists & inhibitors, Peptides therapeutic use

Abstract

The recognition of cyclin-dependent kinase (CDK)/cyclin complexes by various cell-cycle regulatory proteins, including certain tumour suppressors and transcription factors, occurs at least in part through a protein-protein interaction with a binding groove on the cyclin subunit. Since CDK function is generally deregulated in tumour cells, blocking of this recruitment site prevents recognition and subsequent phosphorylation of CDK substrates and offers a therapeutic approach towards restoration of checkpoint control in transformed cells. Here we discuss the finding that peptides derived from such cyclin-interacting proteins, and rendered permeable through conjugation to cellular delivery vectors, can apparently induce tumour cells to undergo apoptosis selectively. We review the current status of 3D-structural information available on cyclin-peptide interactions and we summarise our extensive peptide structure-activity relationship studies in light of this information. We also show how a combination of molecular modelling and introduction into synthetic peptides of peptidomimetic elements, such as non-natural amino acid residues and conformational constraints, is being used hopefully to arrive at drug candidates capable of modulating CDK function in a selective mechanism-based approach rather than through ATP antagonism.

Published

2003

9. Highly potent p21(WAF1)-derived peptide inhibitors of CDK-mediated pRb phosphorylation: delineation and structural insight into their interactions with cyclin A.

Author

Zheleva DI, McInnes C, Gavine AL, Zhelev NZ, Fischer PM, and Lane DP

Subjects

Amino Acid Motifs genetics, Amino Acid Motifs physiology, Cyclin-Dependent Kinase Inhibitor p21, Cyclins metabolism, Histones metabolism, Humans, Peptides genetics, Phosphorylation, Structure-Activity Relationship, Cyclin A metabolism, Cyclin-Dependent Kinases antagonists & inhibitors, Cyclins genetics, Peptides metabolism, Retinoblastoma Protein metabolism

Abstract

The tumour suppressor protein p21(WAF1) plays a central role in regulating eukaryotic cell-cycle progression. Through its association with G1- and S-phase CDK complexes it regulates activation of the retinoblastoma protein (pRb) and E2F transcription factors. Recognition of CDK/cyclin complexes by p21 occurs, at least in part, through a protein-protein interaction with a binding groove on the cyclin subunit. The same groove has been shown to be involved in the recruitment of macromolecular CDK substrates, including pRb and E2F. Blocking of this recruitment site therefore prevents recognition and subsequent phosphorylation of CDK substrates and offers a therapeutic approach towards restoration of p21-like tumour suppression. Starting from the C-terminal cyclin-binding domain of p21 we have identified the minimal and optimized bioactive (152)HAKRRLIF(159) peptide sequence with respect to CDK protein kinase inhibition where pRb is the substrate. The phosphorylation of histone H1, however, which does not contain a recognizable cyclin-binding motif, was unaffected. Detailed structure-activity relationship investigations revealed that the determinants within this sequence are residues Arg(155), Leu(157) and Phe(159) and more completely define the composition of the cyclin-binding motif. A marked increase in potency was obtained upon replacement of the native Ser(153) with an Ala residue in the context of short synthetic peptide inhibitors and significantly, this mutation resulted in comparable affinity with CDK2/cyclin A as does the full-length recombinant p21 (which has CDK2 and cyclin A binding sites). Peptides derived from various proteins known to interact with cyclins were compared for potency and selectivity. A molecular model of the complex between the cyclin groove and the HAKRRLIF peptide was constructed. This model accounts for the observed peptide structure-activity relationships, including the potency enhancement of the LIF sequence occupying the hydrophobic pocket. Furthermore, it provides generic insights into molecular interactions governing cyclin groove recognition and lays the foundation for the development of peptidomimetic inhibitors of CDKs.

Published

2002

10. Peptide inhibitors of CDK2-cyclin A that target the cyclin recruitment-site: structural variants of the C-terminal Phe.

Author

Atkinson GE, Cowan A, McInnes C, Zheleva DI, Fischer PM, and Chan WC

Subjects

Amino Acid Sequence, Chromatography, High Pressure Liquid, Cyclin A chemistry, Cyclin-Dependent Kinase 2, Cyclin-Dependent Kinases chemistry, Enzyme Inhibitors chemistry, Models, Molecular, Peptides chemistry, Protein Serine-Threonine Kinases chemistry, CDC2-CDC28 Kinases, Cyclin A antagonists & inhibitors, Cyclin-Dependent Kinases antagonists & inhibitors, Enzyme Inhibitors pharmacology, Peptides pharmacology, Protein Serine-Threonine Kinases antagonists & inhibitors

Abstract

A focused series of octapeptides based on the lead compound H-His-Ala-Lys-Arg-Arg-Leu-Ile-Phe-NH(2) 1, in which the C-terminal phenylalanine residue was replaced by alpha and/or beta-modified variants, was synthesized using solid-phase chemistry. Both the L-threo-beta-hydroxy-phenylalanine (beta-phenylserine, Pse) and (2S)-phenylalaninol derivatives, as competitive binders at the cyclin-recruitment site, displayed potent inhibitory activity towards the CDK2-cyclin A complex. Unexpectedly, the D-threo-Pse derivatives also showed inhibitory activity.

Published

2002

11. Liquid-phase peptide synthesis on polyethylene glycol (PEG) supports using strategies based on the 9-fluorenylmethoxycarbonyl amino protecting group: application of PEGylated peptides in biochemical assays.

Author

Fischer PM and Zheleva DI

Subjects

Chromatography, High Pressure Liquid, Amino Acids chemistry, Fluorenes chemistry, Peptides chemical synthesis, Polyethylene Glycols

Abstract

Stepwise synthetic assembly of polypeptide chains reversibly linked to polyethylene glycol represents a hybrid between traditional solution and solid-phase chemistries and combines the inherent advantages of both approaches. The technical simplicity and scalability of the liquid-phase peptide synthesis method renders it particularly attractive for multiple parallel syntheses, combinatorial approaches and the large-scale preparation of peptides. The versatile protection strategy based on the N alpha-fluorenylmethoxycarbonyl group commonly used in solid-phase peptide synthesis was adapted to the liquid-phase approach. Fluoride ions were used rather than the conventional organic base piperidine for the repetitive amino-deprotection step. Using a range of acid- and base-labile linkers between the polymer and the peptide, it was shown that free and fully side-chain protected peptides can be obtained using our version of the liquid-phase peptide synthesis method. Protocols for simultaneous multiple syntheses requiring a minimum of equipment are presented and the use of polyethylene glycol-bound peptides in biochemical binding and functional assay systems is demonstrated.

Published

2002

12. Use of peptides from p21 (Waf1/Cip1) to investigate PCNA function in Xenopus egg extracts.

Author

Mattock H, Jares P, Zheleva DI, Lane DP, Warbrick E, and Blow JJ

Subjects

Animals, Antimalarials pharmacology, Blotting, Western, Chloroquine pharmacology, Cyclin-Dependent Kinase Inhibitor p21, Cyclins chemistry, Cyclins genetics, DNA Replication physiology, DNA-Directed DNA Polymerase genetics, DNA-Directed DNA Polymerase metabolism, Enzyme Inhibitors chemistry, Female, Humans, Male, Oocytes drug effects, Oocytes physiology, Peptides chemistry, Peptides metabolism, Proliferating Cell Nuclear Antigen pharmacology, Protein Structure, Tertiary, Recombinant Proteins metabolism, Spermatozoa cytology, Spermatozoa physiology, Tissue Extracts chemistry, Tissue Extracts metabolism, Xenopus laevis, Chromatin physiology, Cyclins metabolism, DNA Replication drug effects, Enzyme Inhibitors metabolism, Proliferating Cell Nuclear Antigen physiology

Abstract

Cell-free systems derived from unfertilized Xenopus eggs have been particularly informative in the study of the regulation and biochemistry of DNA replication. We have developed a Xenopus-based system to analyze proliferating cell nuclear antigen (PCNA)-specific effects on the functional properties of egg extracts. To do this, we have coupled peptides derived from p21 (Waf1/Cip1) to beads and used these to deplete PCNA from Xenopus egg extracts. The effect on various aspects of DNA replication can be analyzed after the readdition of PCNA and other purified proteins. Using this system, we have shown that replication of single-stranded M13 DNA is entirely dependent upon PCNA. By adding exogenous T7 DNA polymerase to PCNA-depleted extracts, we have uncoupled processive DNA replication from PCNA activity and so created an experimental system to analyze the dependence of postreplicative processes on PCNA function. We have shown that successful chromatin assembly is specifically dependent on PCNA. However, systems for analyzing the far more complex mechanisms required for the replication of nuclear double-stranded DNA have proved so far to be refractory to specific PCNA depletion., (Copyright 2001 Academic Press.)

Published

2001

13. A quantitative study of the in vitro binding of the C-terminal domain of p21 to PCNA: affinity, stoichiometry, and thermodynamics.

Author

Zheleva DI, Zhelev NZ, Fischer PM, Duff SV, Warbrick E, Blake DG, and Lane DP

Subjects

Amino Acid Sequence, Binding Sites, Cyclin-Dependent Kinase Inhibitor p21, Cyclins chemistry, Fluorescein, Molecular Sequence Data, Thermodynamics, Cyclins metabolism, Proliferating Cell Nuclear Antigen metabolism

Abstract

Proliferating cell nuclear antigen (PCNA) plays an essential role in DNA replication, repair, and control of cell proliferation, and its activity can be modulated by interaction with p21(Waf1/Cip1) [Cox, L. S., (1997) Trends Cell Biol. 7, 493-497]. This protein-protein interaction provides a particularly good model target for designing therapeutic agents to treat proliferative disorders such as cancer. In this study, the formation of complexes between PCNA and peptides derived from the C-terminus of p21 has been investigated at the molecular level and quantified using a competitive PCNA binding assay and isothermal titration calorimetry (ITC). The affinity constant for the interaction between p21 (141-160) peptide and PCNA has been determined to be 1.14 x 10(7) M(-)(1), corresponding to a K(d) of 87.7 nM. Measurement of the interaction of truncation and substitution analogues based on the p21 (141-160) sequence with PCNA revealed that the N-terminal part (residues 141-152) of the above peptide is the minimum recognition motif, required for PCNA binding. Truncation of the C-terminal region p21 (153-160), though, inhibited significantly the ability of the peptides to compete with the full-length p21 (141-160) for binding to PCNA. Alanine mutation of Met 147 or Asp 149 completely abolished or significantly decreased, respectively, the level of the PCNA binding and the inhibition of SV40 DNA replication. Comparison of the data obtained by the competitive PCNA binding assay and the ITC measurements demonstrated the usefulness of this assay for screening for compounds that could modulate the PCNA-p21 interaction. Using this assay, we have screened rationally designed peptides for binding to PCNA and interruption of the PCNA-p21 (141-160) complex. As a result of this screening, we have identified a 16-residue peptide (consensus motif 1 peptide) with the following sequence: SAVLQKKITDYFHPKK. Consensus motif 1 peptide and p21 (141-160) have similar affinities for binding PCNA and abilities to inhibit in vitro replication of DNA originated from SV40. Such peptides could prove useful in assessing p21-mimetic strategies for cancer treatment.

Published

2000