Your search keyword '"Smitha Kizhake"' showing total 23 results

1. Characterization of Promiscuous Binding of Phosphor Ligands to Breast-Cancer-Gene 1 (BRCA1) C-Terminal (BRCT): Molecular Dynamics, Free Energy, Entropy and Inhibitor Design.

Author

Wanli You, Yu-Ming M Huang, Smitha Kizhake, Amarnath Natarajan, and Chia-En A Chang

Subjects

Biology (General), QH301-705.5

Abstract

Inhibition of the protein-protein interaction (PPI) mediated by breast-cancer-gene 1 C-terminal (BRCT) is an attractive strategy to sensitize breast and ovarian cancers to chemotherapeutic agents that induce DNA damage. Such inhibitors could also be used for studies to understand the role of this PPI in DNA damage response. However, design of BRCT inhibitors is challenging because of the inherent flexibility associated with this domain. Several studies identified short phosphopeptides as tight BRCT binders. Here we investigated the thermodynamic properties of 18 phosphopeptides or peptide with phosphate mimic and three compounds with phosphate groups binding to BRCT to understand promiscuous molecular recognition and guide inhibitor design. We performed molecular dynamics (MD) simulations to investigate the interactions between inhibitors and BRCT and their dynamic behavior in the free and bound states. MD simulations revealed the key role of loops in altering the shape and size of the binding site to fit various ligands. The mining minima (M2) method was used for calculating binding free energy to explore the driving forces and the fine balance between configuration entropy loss and enthalpy gain. We designed a rigidified ligand, which showed unfavorable experimental binding affinity due to weakened enthalpy. This was because it lacked the ability to rearrange itself upon binding. Investigation of another phosphate group containing compound, C1, suggested that the entropy loss can be reduced by preventing significant narrowing of the energy well and introducing multiple new compound conformations in the bound states. From our computations, we designed an analog of C1 that introduced new intermolecular interactions to strengthen attractions while maintaining small entropic penalty. This study shows that flexible compounds do not always encounter larger entropy penalty, compared with other more rigid binders, and highlights a new strategy for inhibitor design.

Published

2016

2. Stapling proteins in the RELA complex inhibits TNFα-induced nuclear translocation of RELA

Author

Tom Huxford, Dragana Lagundžin, Nicholas T. Woods, Sandeep Rana, Smit Kour, Amarnath Natarajan, Smitha Kizhake, David Klinkebiel, and Jayapal Reddy Mallareddy

Subjects

Chemistry, chemistry.chemical_compound, Chemistry (miscellaneous), Protein subunit, Dimer, Tumor necrosis factor alpha, Biochemistry, Genetics and Molecular Biology (miscellaneous), Molecular Biology, Biochemistry, Nuclear translocation, Cell biology

Abstract

Tumor necrosis factor (TNF) α-induced nuclear translocation of the NF-κB subunit RELA has been implicated in several pathological conditions. Here we report the discovery of a spirocyclic dimer (SpiD7) that covalently modifies RELA to inhibit TNFα-induced nuclear translocation. This is a previously unexplored strategy to inhibit TNFα-induced NF-κB activation., Discovery of a spirocyclic dimer (SpiD7) that covalently modifies RELA to generate stable high molecular weight complexes. SpiD7 inhibits TNFα-induced nuclear translocation of RELA resulting in the blockade of NF-kB gene transcription, through a previously unexplored modality.

Published

2022

3. Computational and experimental studies of the interaction between phospho-peptides and the C-terminal domain of BRCA1.

Author

Victor M. Anisimov, Arturas Ziemys, Smitha Kizhake, Ziyan Yuan, Amarnath Natarajan, and Claudio N. Cavasotto

Published

2011

4. Small-molecule IKKβ activation modulator (IKAM) targets MAP3K1 and inhibits pancreatic tumor growth

Author

John Victor Napoleon, Satish Sagar, Sydney P. Kubica, Lidia Boghean, Smit Kour, Hannah M. King, Yogesh A. Sonawane, Ayrianne J. Crawford, Nagsen Gautam, Smitha Kizhake, Pawel A. Bialk, Eric Kmiec, Jayapal Reddy Mallareddy, Prathamesh P. Patil, Sandeep Rana, Sarbjit Singh, Janani Prahlad, Paul M. Grandgenett, Gloria E. O. Borgstahl, Gargi Ghosal, Yazen Alnouti, Michael A. Hollingsworth, Prakash Radhakrishnan, and Amarnath Natarajan

Subjects

Pancreatic Neoplasms, Multidisciplinary, Humans, MAP Kinase Kinase Kinase 1, Protein Serine-Threonine Kinases, I-kappa B Kinase

Abstract

Activation of inhibitor of nuclear factor NF-κB kinase subunit-β (IKKβ), characterized by phosphorylation of activation loop serine residues 177 and 181, has been implicated in the early onset of cancer. On the other hand, tissue-specific IKKβ knockout in Kras mutation-driven mouse models stalled the disease in the precancerous stage. In this study, we used cell line models, tumor growth studies, and patient samples to assess the role of IKKβ and its activation in cancer. We also conducted a hit-to-lead optimization study that led to the identification of 39-100 as a selective mitogen-activated protein kinase kinase kinase (MAP3K) 1 inhibitor. We show that IKKβ is not required for growth of Kras mutant pancreatic cancer (PC) cells but is critical for PC tumor growth in mice. We also observed elevated basal levels of activated IKKβ in PC cell lines, PC patient-derived tumors, and liver metastases, implicating it in disease onset and progression. Optimization of an ATP noncompetitive IKKβ inhibitor resulted in the identification of 39-100, an orally bioavailable inhibitor with improved potency and pharmacokinetic properties. The compound 39-100 did not inhibit IKKβ but inhibited the IKKβ kinase MAP3K1 with low-micromolar potency. MAP3K1-mediated IKKβ phosphorylation was inhibited by 39-100, thus we termed it IKKβ activation modulator (IKAM) 1. In PC models, IKAM-1 reduced activated IKKβ levels, inhibited tumor growth, and reduced metastasis. Our findings suggests that MAP3K1-mediated IKKβ activation contributes to KRAS mutation-associated PC growth and IKAM-1 is a viable pretherapeutic lead that targets this pathway.

Published

2022

5. CDK5 Inhibitor Downregulates Mcl-1 and Sensitizes Pancreatic Cancer Cell Lines to Navitoclax

Author

Xu Luo, Michael A. Hollingsworth, Carter J. Barger, Smit Kour, Ayrianne J. Crawford, Smitha Kizhake, Jacob I. Contreras, Hannah M. King, Amarnath Natarajan, Caroline M. Robb, Mourad Bendjennat, Sandeep Rana, and Yogesh A. Sonawane

Subjects

0301 basic medicine, Cell Survival, Small Molecule Libraries, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cyclin-dependent kinase, Cell Line, Tumor, Humans, Protein Kinase Inhibitors, Cell Proliferation, Pharmacology, Sulfonamides, Gene knockdown, Aniline Compounds, Navitoclax, Dose-Response Relationship, Drug, biology, Cell growth, Chemistry, Kinase, Cyclin-dependent kinase 2, Cyclin-Dependent Kinase 5, Drug Synergism, Articles, 3. Good health, Gene Expression Regulation, Neoplastic, Pancreatic Neoplasms, 030104 developmental biology, Apoptosis, Cell culture, Cancer research, biology.protein, Myeloid Cell Leukemia Sequence 1 Protein, Pyrazoles, Molecular Medicine, 030217 neurology & neurosurgery, HeLa Cells

Abstract

Developing small molecules that indirectly regulate Mcl-1 function has attracted a lot of attention in recent years. Here, we report the discovery of an aminopyrazole, 2-([1,1′-biphenyl]-4-yl)-N-(5-cyclobutyl-1H-pyrazol-3-yl)acetamide (analog 24), which selectively inhibited cyclin-dependent kinase (CDK) 5 over CDK2 in cancer cell lines. We also show that analog 24 reduced Mcl-1 levels in a concentration-dependent manner in cancer cell lines. Using a panel of doxycycline inducible cell lines, we show that CDK5 inhibitor 24 selectively modulates Mcl-1 function while the CDK4/6 inhibitor 6-acetyl-8-cyclopentyl-5-methyl-2-(5-(piperazin-1-yl)pyridin-2-ylamino)pyrido[2,3-day]pyrimidin-7(8H)-one does not. Previous studies using RNA interference and CRISPR showed that concurrent elimination of Bcl-xL and Mcl-1 resulted in induction of apoptosis. In pancreatic cancer cell lines, we show that either CDK5 knockdown or expression of a dominant negative CDK5 when combined with Bcl2 inhibitor results in synergistic induction of apoptosis. Moreover, concurrent pharmacological perturbation of Mcl-1 and Bcl-xL in pancreatic cancer cell lines using a CDK5 inhibitor analog 24 that reduced Mcl-1 levels and 4-(4-{[2-(4-chlorophenyl)-5,5-dimethyl-1-cyclohexen-1-yl]methyl}-1-piperazinyl)-N-[(4-{[(2R)-4-(4-morpholinyl)-1-(phenylsulfanyl)-2-butanyl]amino}-3-[(trifluoromethyl)sulfonyl]phenyl)sulfonyl] benzamide (navitoclax), a Bcl-2/Bcl-xL/Bcl-w inhibitor, resulted in synergistic inhibition of cell growth and induction of apoptosis. In conclusion, we demonstrate targeting CDK5 will sensitize pancreatic cancers to Bcl-2 inhibitors. SIGNIFICANCE STATEMENT Mcl-1 is stabilized by CDK5-mediated phosphorylation in pancreatic ductal adenocarcinoma, resulting in the deregulation of the apoptotic pathway. Thus, genetic or pharmacological targeting of CDK5 sensitizes pancreatic cancers to Bcl-2 inhibitors, such as navitoclax.

Published

2019

6. Selective degradation of CDK6 by a palbociclib based PROTAC

Author

Smitha Kizhake, Smit Kour, Muhammad Zahid, Hannah M. King, Mourad Bendjennat, Amarnath Natarajan, and Sandeep Rana

Subjects

Models, Molecular, Pyridines, Clinical Biochemistry, Pharmaceutical Science, Palbociclib, 01 natural sciences, Biochemistry, Article, Piperazines, Structure-Activity Relationship, Drug Discovery, Humans, Binding site, Protein Kinase Inhibitors, Molecular Biology, chemistry.chemical_classification, Dose-Response Relationship, Drug, Molecular Structure, biology, 010405 organic chemistry, Kinase, Organic Chemistry, Cyclin-Dependent Kinase 6, 0104 chemical sciences, Cell biology, 010404 medicinal & biomolecular chemistry, Enzyme, chemistry, Selective degradation, Proteolysis, biology.protein, Molecular Medicine, Cyclin-dependent kinase 6, Function (biology)

Abstract

Development of selective kinase inhibitors that target the ATP binding site continues to be a challenge largely due to similar binding pockets. Palbociclib is a cyclin-dependent kinase inhibitor that targets the ATP binding site of CDK4 and CDK6 with similar potency. The enzymatic function associated with the kinase can be effectively probed using kinase inhibitors however the kinase-independent functions cannot. Herein, we report a palbociclib based PROTAC that selectively degrades CDK6 while sparing the homolog CDK4. We used competition studies to characterize the binding and mechanism of CDK6 degradation.

Published

2019

7. Structure activity relationship (SAR) study identifies a quinoxaline urea analog that modulates IKKβ phosphorylation for pancreatic cancer therapy

Author

Jayapal Reddy Mallareddy, Edward L. Ezell, Jacob I. Contreras, Smitha Kizhake, Yogesh A. Sonawane, Sandeep Rana, John Victor Napoleon, Christabelle Rajesh, Prakash Radhakrishnan, Sarbjit Singh, Satish Sagar, Amarnath Natarajan, and Jered C. Garrison

Subjects

Antineoplastic Agents, 01 natural sciences, Article, 03 medical and health sciences, Mice, Structure-Activity Relationship, Pancreatic tumor, Pancreatic cancer, Cell Line, Tumor, Quinoxalines, Drug Discovery, Genetic model, medicine, Structure–activity relationship, Animals, Humans, Urea, Phosphorylation, Protein Kinase Inhibitors, 030304 developmental biology, Cell Proliferation, Pharmacology, 0303 health sciences, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Kinase, Chemistry, Organic Chemistry, General Medicine, medicine.disease, Gemcitabine, 0104 chemical sciences, I-kappa B Kinase, Pancreatic Neoplasms, Cancer research, Tumor necrosis factor alpha, Drug Screening Assays, Antitumor, medicine.drug

Abstract

Genetic models validated Inhibitor of nuclear factor (NF) kappa B kinase beta (IKKβ) as a therapeutic target for KRAS mutation associated pancreatic cancer. Phosphorylation of the activation loop serine residue (S(177), S(181)) IKKβ is a key event that drives tumor necrosis factor (TNF) α induced NF-κB mediated gene expression. Here we conducted structure activity relationship (SAR) study to improve potency and oral bioavailability of a quinoxaline analog 13–197 that was previously reported as an NFκB inhibitor for pancreatic cancer therapy. The SAR led to the identification of a novel quinoxaline urea analog 84 that reduced the levels of p-IKKβ in dose- and time-dependent studies. When compared to 13–197, analog 84 was ~2.5-fold more potent in TNFα-induced NFκB inhibition and ~4-fold more potent in inhibiting pancreatic cancer cell growth. Analog 84 exhibited ~4.3-fold greater exposure (AUC(0−)∞) resulting in ~5.7-fold increase in oral bioavailability (%F) when compared to 13–197. Importantly, oral administration of 84 by itself and in combination of gemcitabine reduced p-IKKβ levels and inhibited pancreatic tumor growth in a xenograft model.

Published

2021

8. Small molecule binding to Inhibitor of nuclear factor kappa-B kinase subunit beta in an ATP non-competitive manner

Author

Smitha Kizhake, Michel M. Ouellette, Nicholas Y. Palermo, Sandeep Rana, Sarbjit Singh, John Victor Napoleon, Mourad Bendjennat, Vikas Kumar, Amarnath Natarajan, and Tom Huxford

Subjects

Protein subunit, Allosteric regulation, Regulator, Catalysis, Article, Small Molecule Libraries, 03 medical and health sciences, 0302 clinical medicine, Adenosine Triphosphate, Ubiquitin, Materials Chemistry, Humans, Binding site, Beta (finance), Protein Kinase Inhibitors, 030304 developmental biology, 0303 health sciences, Binding Sites, biology, Dose-Response Relationship, Drug, Molecular Structure, Kinase, Chemistry, Metals and Alloys, General Chemistry, Surfaces, Coatings and Films, Electronic, Optical and Magnetic Materials, Cell biology, I-kappa B Kinase, 030220 oncology & carcinogenesis, Ceramics and Composites, biology.protein, Small molecule binding

Abstract

Inhibitor of nuclear factor kappa-B kinase subunit beta (IKKβ) is a key regulator of the cannonical NF-κB pathway. IKKβ has been validated as a drug target for pathological conditions, which include chronic inflammatory diseases and cancer. Pharmacological studies revealed that chronic administration of ATP-competitive IKKβ inhibitors resulted in unexpected toxicity. We previously reported the discovery of 13-197 as a non-toxic IKKβ inhibitor that reduced tumor growth. Here, we show that 13-197 inhibits IKKβ in a ATP non-competitive manner and an allosteric pocket at the interface of the kinase and ubiquitin like domains was identified as the potential binding site.

Published

2021

9. Dimers of isatin derived α-methylene-γ-butyrolactone as potent anti-cancer agents

Author

Sandeep Rana, Smit Kour, Smitha Kizhake, Hannah M. King, Jayapal Reddy Mallareddy, Adam J. Case, Tom Huxford, and Amarnath Natarajan

Subjects

Isatin, Organic Chemistry, Clinical Biochemistry, NF-kappa B, Transcription Factor RelA, Pharmaceutical Science, Antineoplastic Agents, Protein Serine-Threonine Kinases, Biochemistry, Article, I-kappa B Kinase, 4-Butyrolactone, Cell Line, Tumor, Drug Discovery, Molecular Medicine, Phosphorylation, Molecular Biology

Abstract

The IKK-NFκB complex is a key signaling node that facilitates activation of gene expression in response to extracellular signals. The kinase IKKβ and the transcription factor RELA have been targeted by covalent modifiers that bind to surface exposed cysteine residues. A common feature in well characterized covalent modifiers of RELA and IKKβ is the Michael acceptor containing α-methylene-γ-butyrolactone functionality. Through synthesis and evaluation of a focused set of α-methylene-γ-butyrolactone containing spirocyclic dimers (SpiDs) we identified SpiD3 as an anticancer agent with low nanomolar potency. Using cell-free and cell-based studies we show that SpiD3 is a covalent modifier that generates stable RELA containing high molecular weight complexes. SpiD3 inhibits TNFα-induced IκBα phosphorylation resulting in the blockade of RELA nuclear translocation. SpiD3 induces apoptosis, inhibits colony formation and migration of cancer cells. The NCI-60 cell line screen revealed that SpiD3 potently inhibits growth of leukemia cell lines, making it a suitable pre-therapeutic lead for hematological malignancies.

Published

2022

10. Spirocyclic dimer SpiD7 activates the unfolded protein response to selectively inhibit growth and induce apoptosis of cancer cells

Author

Smit Kour, Sandeep Rana, Sydney P. Kubica, Smitha Kizhake, Mudassier Ahmad, Catalina Muñoz-Trujillo, David Klinkebiel, Sarbjit Singh, Jayapal Reddy Mallareddy, Surabhi Chandra, Nicholas T. Woods, Adam R. Karpf, and Amarnath Natarajan

Subjects

Cell Line, Tumor, Carcinoma, Drug Discovery, Eukaryotic Initiation Factor-2, Unfolded Protein Response, Humans, Apoptosis, Cell Biology, Endoplasmic Reticulum, Endoplasmic Reticulum Stress, Molecular Biology, Biochemistry

Abstract

The unfolded protein response (UPR) is an adaptation mechanism activated to resolve transient accumulation of unfolded/misfolded proteins in the endoplasmic reticulum. Failure to resolve the transient accumulation of such proteins results in UPR-mediated programmed cell death. Loss of tumor suppressor gene or oncogene addiction in cancer cells can result in sustained higher basal UPR levels; however, it is not clear if these higher basal UPR levels in cancer cells can be exploited as a therapeutic strategy. We hypothesized that covalent modification of surface-exposed cysteine (SEC) residues could simulate unfolded/misfolded proteins to activate the UPR, and that higher basal UPR levels in cancer cells would provide the necessary therapeutic window. To test this hypothesis, here we synthesized analogs that can covalently modify multiple SEC residues and evaluated them as UPR activators. We identified a spirocyclic dimer, SpiD7, and evaluated its effects on UPR activation signals, that is, XBP1 splicing, phosphorylation of eIF2α, and a decrease in ATF 6 levels, in normal and cancer cells, which were further confirmed by RNA-Seq analyses. We found that SpiD7 selectively induced caspase-mediated apoptosis in cancer cells, whereas normal cells exhibited robust XBP1 splicing, indicating adaptation to stress. Furthermore, SpiD7 inhibited the growth of high-grade serous carcinoma cell lines ~3-15-fold more potently than immortalized fallopian tube epithelial (paired normal control) cells and reduced clonogenic growth of high-grade serous carcinoma cell lines. Our results suggest that induction of the UPR by covalent modification of SEC residues represents a cancer cell vulnerability and can be exploited to discover novel therapeutics.

Published

2022

11. Symbiotic Prodrugs (SymProDs) Dual Targeting of NFkappaB and CDK

Author

Yogesh A. Sonawane, Smitha Kizhake, Smit Kour, Amarnath Natarajan, Jacob I. Contreras, Muhammad Zahid, Sandeep Rana, Caroline M. Robb, and Adam R. Karpf

Subjects

Drug, Pyridines, media_common.quotation_subject, Antineoplastic Agents, Apoptosis, Pharmacology, 01 natural sciences, Biochemistry, Article, Piperazines, chemistry.chemical_compound, Structure-Activity Relationship, 4-Butyrolactone, Piperidines, Cyclin-dependent kinase, Cell Line, Tumor, Drug Discovery, Humans, Prodrugs, Molecular Targeted Therapy, Amines, Protein Kinase Inhibitors, media_common, Cell Proliferation, Ovarian Neoplasms, biology, 010405 organic chemistry, Kinase, Organic Chemistry, NF-kappa B, Biological activity, Prodrug, In vitro, Cyclin-Dependent Kinases, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, chemistry, Cell culture, biology.protein, Molecular Medicine, Pyrazoles, Female, Growth inhibition, Drug Screening Assays, Antitumor, Sesquiterpenes, Signal Transduction

Abstract

The release of an active drug from the prodrug generates a pro-fragment that typically has no biological activity and could result in adverse effects. By combining two drugs, wherein each drug acts as a pro-fragment of the other drug will eliminate the pro-fragment in the prodrug. As they are prodrugs of each other and are symbiotic, we termed these as symbiotic prodrugs (SymProDs). To test this idea, we generated SymProDs using NFκB inhibitors that contain the reactive α-methylene-γ-butyrolactone moiety and CDK inhibitors with solvent exposed secondary nitrogen atoms. We show that secondary amine prodrugs of α-methylene-γ-butyrolactone containing NFκB inhibitors undergo slow release over a 72 hr period. Using an alkyne-tagged secondary amine prodrug of α-methylene-γ-butyrolactone containing NFκB inhibitor, we demonstrate target engagement. The NFκB-CDK SymProDs were ~20- to 200-fold less active against the corresponding CDK inhibitors in in vitro CDK kinase assays. Growth inhibition studies in a panel of ovarian cancer cell lines revealed potency trends of the SymProDs mirrored those of the single treatments suggesting their dissociation in cells. In conclusion, our results suggest that SymProDs offer a productive path forward for advancing compounds with reactive functionality and can be used as dual targeting agents.

Published

2020

12. Chemical Genetic Screens Identify Kinase Inhibitor Combinations that Target Anti-Apoptotic Proteins for Cancer Therapy

Author

Michael A. Hollingsworth, Jared Baxter, Sandeep Rana, Caroline M. Robb, Yogesh A. Sonawane, Smit Kour, Ayrianne J. Crawford, Xu Luo, Smitha Kizhake, Jacob I. Contreras, Amarnath Natarajan, and Hannah M. King

Subjects

0301 basic medicine, Cell, Caspase 3, Biochemistry, Article, 03 medical and health sciences, 0302 clinical medicine, Cyclin-dependent kinase, Cell Line, Tumor, Neoplasms, medicine, Humans, Protein Kinase Inhibitors, PI3K/AKT/mTOR pathway, biology, Chemistry, Kinase, General Medicine, High-Throughput Screening Assays, 030104 developmental biology, medicine.anatomical_structure, Proto-Oncogene Proteins c-bcl-2, Cell culture, Apoptosis, Doxycycline, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Molecular Medicine, Drug Therapy, Combination, Apoptosis Regulatory Proteins, Genetic screen

Abstract

The study presented here provides a framework for the discovery of unique inhibitor combinations that target the apoptosis network for cancer therapy. A pair of doxycycline (Dox) -inducible cell lines that specifically report on the ability of an inhibitor to induce apoptosis either by targeting the Mcl-1 arm or the Bcl-2/Bcl-xL/Bcl-w arm were used. Cell-based assays were optimized for high throughput screening (HTS) with caspase 3/7 as a read out. HTS with a 355-member kinase inhibitor library and the panel of Dox-inducible cell lines revealed that cyclin dependent kinase (CDK) inhibitors induced apoptosis by targeting the Mcl-1 arm whereas PI3K inhibitors induced apoptosis by targeting the Bcl-2/Bcl-xL/Bcl-w arm. Validation studies identified unique combinations that synergistically inhibited growth and induced apoptosis in a panel of cancer cell lines. Since these inhibitors have been or are currently in clinical trials as single agents, the combinations can be rapidly translated to the clinics.

Published

2018

13. Characterization of CDK(5) inhibitor, 20-223 (aka CP668863) for colorectal cancer therapy

Author

Jing Wang, Carter J. Barger, Smitha Kizhake, Smit Kour, Michael A. Hollingsworth, Rhishikesh Thakare, Sanjib Chowdhury, Jennifer D. Black, Beth K. Neilsen, Sandeep Rana, Caroline M. Robb, Yogesh A. Sonawane, Michael G. Brattain, Ekta Agarwal, Amarnath Natarajan, Jacob I. Contreras, and Margaret A. Taylor

Subjects

0301 basic medicine, Cell cycle checkpoint, biology, Kinase, business.industry, Cyclin-dependent kinase 5, Cyclin-dependent kinase 2, Correction, Cell cycle, cyclin-dependent kinase (CDK), colorectal cancer (CRC), CDK inhibitor, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, Cyclin-dependent kinase, 030220 oncology & carcinogenesis, biology.protein, Cancer research, Medicine, Kinase activity, business, Research Paper

Abstract

Colorectal cancer (CRC) remains one of the leading causes of cancer related deaths in the United States. Currently, there are limited therapeutic options for patients suffering from CRC, none of which focus on the cell signaling mechanisms controlled by the popular kinase family, cyclin dependent kinases (CDKs). Here we evaluate a Pfizer developed compound, CP668863, that inhibits cyclin-dependent kinase 5 (CDK5) in neurodegenerative disorders. CDK5 has been implicated in a number of cancers, most recently as an oncogene in colorectal cancers. Our lab synthesized and characterized CP668863 - now called 20-223. In our established colorectal cancer xenograft model, 20-223 reduced tumor growth and tumor weight indicating its value as a potential anti-CRC agent. We subjected 20-223 to a series of cell-free and cell-based studies to understand the mechanism of its anti-tumor effects. In our hands, in vitro 20-223 is most potent against CDK2 and CDK5. The clinically used CDK inhibitor AT7519 and 20-223 share the aminopyrazole core and we used it to benchmark the 20-223 potency. In CDK5 and CDK2 kinase assays, 20-223 was ∼3.5-fold and ∼65.3-fold more potent than known clinically used CDK inhibitor, AT7519, respectively. Cell-based studies examining phosphorylation of downstream substrates revealed 20-223 inhibits the kinase activity of CDK5 and CDK2 in multiple CRC cell lines. Consistent with CDK5 inhibition, 20-223 inhibited migration of CRC cells in a wound-healing assay. Profiling a panel of CRC cell lines for growth inhibitory effects showed that 20-223 has nanomolar potency across multiple CRC cell lines and was on an average >2-fold more potent than AT7519. Cell cycle analyses in CRC cells revealed that 20-223 phenocopied the effects associated with AT7519. Collectively, these findings suggest that 20-223 exerts anti-tumor effects against CRC by targeting CDK 2/5 and inducing cell cycle arrest. Our studies also indicate that 20-223 is a suitable lead compound for colorectal cancer therapy.

Published

2017

14. Aminopyrazole based CDK9 PROTAC sensitizes pancreatic cancer cells to venetoclax

Author

Hannah M. King, Edward L. Ezell, Smitha Kizhake, Muhammad Zahid, Sydney P. Kubica, Michael J. Naldrett, Jayapal Reddy Mallareddy, Amarnath Natarajan, Henry C.-H. Law, Sophie Alvarez, Nicholas T. Woods, and Sandeep Rana

Subjects

Clinical Biochemistry, Pharmaceutical Science, Antineoplastic Agents, 01 natural sciences, Biochemistry, Article, Structure-Activity Relationship, chemistry.chemical_compound, Cyclin-dependent kinase, Drug Discovery, Humans, Kinome, Protein Kinase Inhibitors, Molecular Biology, Cell Proliferation, Sulfonamides, Dose-Response Relationship, Drug, Molecular Structure, biology, 010405 organic chemistry, Venetoclax, Kinase, Organic Chemistry, Proteolysis targeting chimera, Bridged Bicyclo Compounds, Heterocyclic, Cyclin-Dependent Kinase 9, 0104 chemical sciences, Pancreatic Neoplasms, 010404 medicinal & biomolecular chemistry, chemistry, Proteolysis, Cancer research, biology.protein, Pyrazoles, Molecular Medicine, Oncogene MYC, Cyclin-dependent kinase 9, Drug Screening Assays, Antitumor, Growth inhibition

Abstract

Cyclin-dependent kinase 9 (CDK9) is a member of the cyclin-dependent kinase (CDK) family which is involved in transcriptional regulation of several genes, including the oncogene Myc, and is a validated target for pancreatic cancer. Here we report the development of an aminopyrazole based proteolysis targeting chimera (PROTAC 2) that selectively degrades CDK9 (DC50 = 158 ± 6 nM). Mass spectrometry-based kinome profiling shows PROTAC 2 selectively degrades CDK9 in MiaPaCa2 cells and sensitizes them to Venetoclax mediated growth inhibition.

Published

2021

15. Synthesis of aminopyrazole analogs and their evaluation as CDK inhibitors for cancer therapy

Author

Smitha Kizhake, Sandeep Rana, Margaret A. Taylor, Amarnath Natarajan, Yogesh A. Sonawane, and Muhammad Zahid

Subjects

0301 basic medicine, Clinical Biochemistry, Cancer therapy, Pharmaceutical Science, Biochemistry, Article, 03 medical and health sciences, chemistry.chemical_compound, Structure-Activity Relationship, Cyclin-dependent kinase, Cell Line, Tumor, Drug Discovery, Humans, Molecular Biology, Protein Kinase Inhibitors, Amination, Cell Proliferation, biology, Chemistry, Cyclin-dependent kinase 5, Organic Chemistry, Cyclin-dependent kinase 2, Cyclin-Dependent Kinase 2, Cyclin-Dependent Kinase 5, Molecular Docking Simulation, Pancreatic Neoplasms, 030104 developmental biology, biology.protein, Molecular Medicine, Pyrazoles, Growth inhibition, Hinge region, Carcinoma, Pancreatic Ductal

Abstract

We synthesized a library of aminopyrazole analogs to systematically explore the hydrophobic pocket adjacent to the hinge region and the solvent exposed region of cyclin dependent kinases. Structure-activity relationship studies identified an optimal substitution for the hydrophobic pocket and analog 24 as a potent and selective CDK2/5 inhibitor.

Published

2018

16. Characterization of Promiscuous Binding of Phosphor Ligands to Breast-Cancer-Gene 1 (BRCA1) C-Terminal (BRCT): Molecular Dynamics, Free Energy, Entropy and Inhibitor Design

Author

Chia-en A. Chang, Amarnath Natarajan, Smitha Kizhake, Wanli You, and Yu ming M. Huang

Subjects

Phosphopeptides, 0301 basic medicine, Entropy, Ligands, Physical Chemistry, Biochemistry, 01 natural sciences, Molecular dynamics, Enthalpy, Biochemical Simulations, lcsh:QH301-705.5, Free Energy, Ecology, BRCA1 Protein, Chemistry, Hydrogen bond, Physics, Chemical Reactions, Classical Mechanics, Ligand (biochemistry), Computational Theory and Mathematics, Modeling and Simulation, Physical Sciences, Thermodynamics, Research Article, Protein Binding, DNA damage, Configuration entropy, Solvation, Antineoplastic Agents, Molecular Dynamics Simulation, 010402 general chemistry, Vibration, Phosphates, 03 medical and health sciences, Cellular and Molecular Neuroscience, Molecular recognition, Genetics, Humans, Binding site, Molecular Biology, Ecology, Evolution, Behavior and Systematics, Chemical Bonding, Chemical Compounds, Biology and Life Sciences, Computational Biology, Hydrogen Bonding, 0104 chemical sciences, 030104 developmental biology, lcsh:Biology (General), Biophysics

Abstract

Inhibition of the protein-protein interaction (PPI) mediated by breast-cancer-gene 1 C-terminal (BRCT) is an attractive strategy to sensitize breast and ovarian cancers to chemotherapeutic agents that induce DNA damage. Such inhibitors could also be used for studies to understand the role of this PPI in DNA damage response. However, design of BRCT inhibitors is challenging because of the inherent flexibility associated with this domain. Several studies identified short phosphopeptides as tight BRCT binders. Here we investigated the thermodynamic properties of 18 phosphopeptides or peptide with phosphate mimic and three compounds with phosphate groups binding to BRCT to understand promiscuous molecular recognition and guide inhibitor design. We performed molecular dynamics (MD) simulations to investigate the interactions between inhibitors and BRCT and their dynamic behavior in the free and bound states. MD simulations revealed the key role of loops in altering the shape and size of the binding site to fit various ligands. The mining minima (M2) method was used for calculating binding free energy to explore the driving forces and the fine balance between configuration entropy loss and enthalpy gain. We designed a rigidified ligand, which showed unfavorable experimental binding affinity due to weakened enthalpy. This was because it lacked the ability to rearrange itself upon binding. Investigation of another phosphate group containing compound, C1, suggested that the entropy loss can be reduced by preventing significant narrowing of the energy well and introducing multiple new compound conformations in the bound states. From our computations, we designed an analog of C1 that introduced new intermolecular interactions to strengthen attractions while maintaining small entropic penalty. This study shows that flexible compounds do not always encounter larger entropy penalty, compared with other more rigid binders, and highlights a new strategy for inhibitor design., Author Summary Promiscuous proteins are commonly observed in biological systems, such as modular domains that recognize phosphopeptides during signal transduction. The use of phosphopeptides and compounds with phosphate groups as inhibitors to protein–protein interactions have attracted increasing interest for years. By using atomistic molecular dynamics simulations, we are able to perform detailed analyses of the dihedral space to explore protein fluctuation upon ligand binding to better understand promiscuous molecular recognition. Free energy calculation can further provide insights into the mechanism of binding, including both enthalpic and entropic contributions for molecular recognition, which assist in inhibitor design. Our calculation results show that pre-rigidifying a ligand is not always advantageous, suggesting the challenge in retaining optimized intermolecular interactions in pre-rigidified ligand. Instead, certain flexible ligands with multiple binding conformations can reduce entropic penalty, and therefore improves binding affinity. According to our computations, we can introduce new intermolecular interactions to flexible ligand to strengthen attractions while maintaining small entropic penalty by retaining its plasticity in the bound conformation. The study might cast light on a new general strategy for designing inhibitors targeting promiscuous modular domains and protein–protein interactions.

Published

2016

17. Isatin Derived Spirocyclic Analogues with α-Methylene-γ-butyrolactone as Anticancer Agents: A Structure-Activity Relationship Study

Author

Prakash Radhakrishnan, Adnan R. Munkarah, Jacob I. Contreras, Rajkumar N. Rajule, Tian Zhou, Calvin Tebbe, Elizabeth C. Blowers, Sandeep Rana, Smitha Kizhake, Amarnath Natarajan, Jamie L. Arnst, and Ramandeep Rattan

Subjects

Isatin, Stereochemistry, α methylene γ butyrolactone, Antineoplastic Agents, 010402 general chemistry, 01 natural sciences, Article, chemistry.chemical_compound, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, medicine, Potency, Structure–activity relationship, Humans, Tumor growth, Spiro Compounds, Cell Proliferation, Dose-Response Relationship, Drug, Molecular Structure, 010405 organic chemistry, Tumor Necrosis Factor-alpha, NF-kappa B, medicine.disease, Combinatorial chemistry, 0104 chemical sciences, chemistry, Cancer cell, Molecular Medicine, Drug Screening Assays, Antitumor, Ovarian cancer

Abstract

Design, synthesis, and evaluation of α-methylene-γ-butyrolactone analogues and their evaluation as anticancer agents is described. SAR identified a spirocyclic analogue 19 that inhibited TNFα-induced NF-κB activity, cancer cell growth and tumor growth in an ovarian cancer model. A second iteration of synthesis and screening identified 29 which inhibited cancer cell growth with low-μM potency. Our data suggest that an isatin-derived spirocyclic α-methylene-γ-butyrolactone is a suitable core for optimization to identify novel anticancer agents.

Published

2016

18. Computational and experimental studies of the interaction between phospho-peptides and the C-terminal domain of BRCA1

Author

Arturas Ziemys, Ziyan Yuan, Smitha Kizhake, Victor M. Anisimov, Claudio N. Cavasotto, and Amarnath Natarajan

Subjects

Phosphopeptides, Stereochemistry, Amino Acid Motifs, Peptide, Plasma protein binding, Molecular Dynamics Simulation, Article, Molecular dynamics, Protein structure, Drug Discovery, Humans, Physical and Theoretical Chemistry, Binding site, chemistry.chemical_classification, Binding Sites, BRCA1 Protein, C-terminus, Interaction energy, Ligand (biochemistry), Protein Structure, Tertiary, Computer Science Applications, Crystallography, chemistry, Mutation, Thermodynamics, Protein Binding

Abstract

The C-terminal domain of BRCA1 (BRCT) is involved in the DNA repair pathway by recognizing the pSXXF motif in interacting proteins. It has been reported that short peptides containing this motif bind to BRCA1(BRCT) in the micromolar range with high specificity. In this work, the binding of pSXXF peptides has been studied computationally and experimentally in order to characterize their interaction with BRCA1(BRCT). Elucidation of the contacts that drive the protein-ligand interactions is critical for the development of high affinity small-molecule BRCA1 inhibitors. Molecular dynamics simulations revealed the key role of threonine at the peptide P+2 position in providing structural rigidity to the ligand in the bound state. The mutation at P+1 had minor effects. Peptide extension at the N-terminal position with the naphthyl amino acid exhibited a modest increase in binding affinity, what could be explained by the dispersion interaction of the naphthyl side-chain with a hydrophobic patch. Three in silico end-point methods were considered for the calculation of binding free energy. The Molecular Mechanics Poisson-Boltzmann Surface Area (MM/PB-SA) and the Solvated Interaction Energy (SIE) gave reasonable agreement with experimental data, exhibiting a Pearlman predictive index of 0.71 and 0.78, respectively. The MM-Quantum Mechanics-Surface Area (MM-QMSA) method yielded improved results, which was characterized by a Pearlman index of 0.78. The correlation coefficients were 0.59, 0.61 and 0.69, respectively. The ability to apply a QM level of theory within an end-point binding free energy protocol may provide a way for a consistent improvement of accuracy in computer-aided drug design.

Published

2011

19. Exploiting the P-1 Pocket of BRCT Domains Toward a Structure Guided Inhibitor Design

Author

Ziyan Yuan, Smitha Kizhake, Eric A. Kumar, Stephen J. Campbell, Amarnath Natarajan, Nicholas Y. Palermo, and J. N. Mark Glover

Subjects

chemistry.chemical_classification, DNA damage, DNA repair, Organic Chemistry, Peptide, Biology, Biochemistry, MDC1, Cell biology, Crystallography, chemistry, Drug Discovery, Phosphorylation, Binding site, Phosphorylated proteins, Gene

Abstract

Breast cancer gene 1 carboxy terminus (BRCT) domains are found in a number of proteins that are important for DNA damage response (DDR). The BRCT domains bind phosphorylated proteins, and these protein–protein interactions are essential for DDR and DNA repair. High affinity domain specific inhibitors are needed to facilitate the dissection of the protein–protein interactions in the DDR signaling. The BRCT domains of BRCA1 bind phosphorylated protein through a pSXXF consensus recognition motif. We identified a hydrophobic pocket at the P-1 position of the pSXXF binding site. Here we conducted a structure-guided synthesis of peptide analogues with hydrophobic functional groups at the P-1 position. Evaluation of these led to the identification of a peptide mimic 15 with a inhibitory constant (Ki) of 40 nM for BRCT(BRCA1). Analysis of the TopBP1 and MDC1 BRCT domains suggests a similar approach is viable to design high affinity inhibitors.

Published

2011

20. Structural characterization of BRCT–tetrapeptide binding interactions

Author

Prem Raj B. Joseph, Smitha Kizhake, Krishna Rajarathnam, Amarnath Natarajan, Ziyan Yuan, Eric A. Kumar, and G. L. Lokesh

Subjects

Protein Conformation, Stereochemistry, Amino Acid Motifs, Biophysics, Plasma protein binding, Biochemistry, Article, Conserved sequence, Protein structure, Humans, skin and connective tissue diseases, Nuclear Magnetic Resonance, Biomolecular, Molecular Biology, Binding affinities, Oligopeptide, Tetrapeptide, BRCA1 Protein, Chemistry, Cell Biology, Nuclear magnetic resonance spectroscopy, DNA Repair Pathway, Drug Design, Thermodynamics, Oligopeptides, Protein Binding

Abstract

BRCT(BRCA1) plays a major role in DNA repair pathway, and does so by recognizing the conserved sequence pSXXF in its target proteins. Remarkably, tetrapeptides containing pSXXF motif bind with high specificity and micromolar affinity. Here, we have characterized the binding interactions of pSXXF tetrapeptides using NMR spectroscopy and calorimetry. We show that BRCT is dynamic and becomes structured on binding, that pSer and Phe residues dictate overall binding, and that the binding affinities of the tetrapeptides are intimately linked to structural and dynamic changes both in the BRCT(BRCA1) and tetrapeptides. These results provide critical insights for designing high-affinity BRCT(BRCA1) inhibitors.

Published

2010

21. The paradox of conformational constraint in the design of Cbl(TKB)-binding peptides

Author

Amarnath Natarajan, Gloria E. O. Borgstahl, Qianyi Chen, Chia-en A. Chang, Myungshim Kang, Eric A. Kumar, Smitha Kizhake, and Carol Kolar

Subjects

Models, Molecular, Stereochemistry, Molecular Conformation, Peptide, Molecular Dynamics Simulation, Ligands, 01 natural sciences, Pentapeptide repeat, Article, 03 medical and health sciences, Amino Acid Sequence, Proto-Oncogene Proteins c-cbl, Binding site, Peptide sequence, 030304 developmental biology, Polyproline helix, chemistry.chemical_classification, 0303 health sciences, Multidisciplinary, Binding Sites, 010405 organic chemistry, Hydrogen bond, Chemistry, Hydrogen Bonding, 0104 chemical sciences, Amino acid, Molecular Docking Simulation, Kinetics, Biochemistry, Helix, Peptides, Protein Binding

Abstract

Solving the crystal structure of Cbl(TKB) in complex with a pentapeptide, pYTPEP, revealed that the PEP region adopted a poly-L-proline type II (PPII) helix. An unnatural amino acid termed a proline-templated glutamic acid (ptE) that constrained both the backbone and sidechain to the bound conformation was synthesized and incorporated into the pYTPXP peptide. We estimated imposing structural constraints onto the backbone and sidechain of the peptide and preorganize it to the bound conformation in solution will yield nearly an order of magnitude improvement in activity. NMR studies confirmed that the ptE-containing peptide adopts the PPII conformation, however, competitive binding studies showed an order of magnitude loss of activity. Given the emphasis that is placed on imposing structural constraints, we provide an example to support the contrary. These results point to conformational flexibility at the interface, which have implications in the design of potent Cbl(TKB)-binding peptides.

Published

2013

22. Peptide truncation leads to a twist and an unusual increase in affinity for casitas B-lineage lymphoma tyrosine kinase binding domain

Author

Nicholas Y. Palermo, Smitha Kizhake, G. L. Lokesh, Gulzar Ahmad, Hamid Band, Gloria E. O. Borgstahl, Lin Dong, Ziyan Yuan, Amarnath Natarajan, Carol Kolar, and Eric A. Kumar

Subjects

chemistry.chemical_classification, Models, Molecular, Oligopeptide, Binding Sites, Chemistry, fungi, Peptide, Plasma protein binding, Oncogene Protein v-cbl, Protein-Tyrosine Kinases, Pentapeptide repeat, Article, Structure-Activity Relationship, Biochemistry, Peptide Library, Drug Discovery, Molecular Medicine, Structure–activity relationship, Thermodynamics, Binding site, Peptide library, Oligopeptides, Protein Binding

Abstract

We describe truncation and SAR studies to identify a pentapeptide that binds Cbl tyrosine kinase binding domain with a higher affinity than the parental peptide. The pentapeptide has an alternative binding mode that allows occupancy of a previously uncharacterized groove. A peptide library was used to map the binding site and define the interface landscape. Our results suggest that the pentapeptide is an ideal starting point for the development of inhibitors against Cbl driven diseases.

Published

2012

23. Structure-activity relationship studies to probe the phosphoprotein binding site on the carboxy terminal domains of the breast cancer susceptibility gene 1

Author

Smitha Kizhake, Eric A. Kumar, Ziyan Yuan, and Amarnath Natarajan

Subjects

Models, Molecular, Oligopeptide, Binding Sites, Chemistry, Peptidomimetic, DNA damage, BRCA1 Protein, Biological activity, Phosphoprotein binding, Calorimetry, Phosphoproteins, Small molecule, Article, Protein Structure, Tertiary, Structure-Activity Relationship, Biochemistry, Drug Discovery, Molecular Medicine, Structure–activity relationship, Thermodynamics, Binding site, Oligopeptides

Abstract

The carboxy terminal BRCT domains of the breast cancer susceptibility gene 1 (BRCA1) bind to a plethora of phosphorylated proteins through a pSXXF consensus recognition motif. BRCT-protein binding regulates key cellular functions such as lipogenesis, cell-cycle checkpoint control and DNA damage response. Identification of the minimal binding sequence and defining the key interactions responsible for biological activity are critical steps in the peptidomimetic design process. Here, we report a systematic structure activity relationship study that maps the BRCT(BRCA1)-pSXXF binding interface. The study has led to the identification of peptides with nanomolar binding affinities comparable to the previously reported 13-mer peptides. The results also provide a clear description of the pSXXF-BRCT interface, which is essential for developing small molecule inhibitors via the peptidomimetic approach.

Published

2011