Your search keyword '"Jayapal Reddy Mallareddy"' showing total 36 results

1. Proteolysis targeting chimera (PROTAC)-driven antibody internalization of oncogenic cell surface receptors

Author

Ezequiel J. Tolosa, Lin Yang, Jennifer Ayers-Ringler, Shinichiro Suzuki, Jayapal Reddy Mallareddy, Janet Schaefer-Klein, Mitesh Borad, Farhad Kosari, Amarnath Natarajan, and Aaron S. Mansfield

Subjects

Biology (General), QH301-705.5

Abstract

Abstract Antibody-drug conjugates (ADCs) are increasingly used in clinic for multiple indications and may improve upon the activity of parental antibodies by delivering cytotoxic payloads into target cells. This activity is predicated upon internalization to release the cytotoxic payloads intracellularly. Since binding of ADCs to their cell surface targets does not guarantee their internalization, we hypothesize that proteolysis targeting chimeras (PROTACs) could improve the activity of ADCs through forced internalization. We show that PROTACs improve internalization of antibodies or their derivative antibody drug conjugates when both agents target the same oncogenic cell surface proteins (EGFR, HER2 or MET) by 1.4-1.9 fold in most models. PROTACs also significantly enhance cytotoxicity with HER2-targeting ADCs. These effects depend on dynamin and proteolysis. This application of PROTACs may impact the use of ADCs and provides a rationale to combine these agents in clinical trials.

Published

2024

2. The Novel Anti-Cancer Agent, SpiD3, Is Cytotoxic in CLL Cells Resistant to Ibrutinib or Venetoclax

Author

Alexandria P. Eiken, Elizabeth Schmitz, Erin M. Drengler, Audrey L. Smith, Sydney A. Skupa, Kabhilan Mohan, Sandeep Rana, Sarbjit Singh, Jayapal Reddy Mallareddy, Grinu Mathew, Amarnath Natarajan, and Dalia El-Gamal

Subjects

chronic lymphocytic leukemia (CLL), drug resistance, SpiD3, ibrutinib, venetoclax, unfolded protein response (UPR), Medicine

Abstract

Background: B-cell receptor (BCR) signaling is a central driver in chronic lymphocytic leukemia (CLL), along with the activation of pro-survival pathways (e.g., NF-κB) and aberrant anti-apoptotic mechanisms (e.g., BCL2) culminating to CLL cell survival and drug resistance. Front-line targeted therapies such as ibrutinib (BTK inhibitor) and venetoclax (BCL2 inhibitor) have radically improved CLL management. Yet, persisting CLL cells lead to relapse in ~20% of patients, signifying the unmet need of inhibitor-resistant refractory CLL. SpiD3 is a novel spirocyclic dimer of analog 19 that displays NF-κB inhibitory activity and preclinical anti-cancer properties. Recently, we have shown that SpiD3 inhibits CLL cell proliferation and induces cytotoxicity by promoting futile activation of the unfolded protein response (UPR) pathway and generation of reactive oxygen species (ROS), resulting in the inhibition of protein synthesis in CLL cells. Methods: We performed RNA-sequencing using CLL cells rendered resistant to ibrutinib and venetoclax to explore potential vulnerabilities in inhibitor-resistant and SpiD3-treated CLL cells. Results: The transcriptomic analysis of ibrutinib- or venetoclax-resistant CLL cell lines revealed ferroptosis, UPR signaling, and oxidative stress to be among the top pathways modulated by SpiD3 treatment. By examining SpiD3-induced protein aggregation, ROS production, and ferroptosis in inhibitor-resistant CLL cells, our findings demonstrate cytotoxicity following SpiD3 treatment in cell lines resistant to current front-line CLL therapeutics. Conclusions: Our results substantiate the development of SpiD3 as a novel therapeutic agent for relapsed/refractory CLL disease.

Published

2024

3. DHODH inhibition enhances the efficacy of immune checkpoint blockade by increasing cancer cell antigen presentation

Author

Nicholas J Mullen, Surendra K Shukla, Ravi Thakur, Sai Sundeep Kollala, Dezhen Wang, Nina Chaika, Juan F Santana, William R Miklavcic, Drew A LaBreck, Jayapal Reddy Mallareddy, David H Price, Amarnath Natarajan, Kamiya Mehla, David B Sykes, Michael A Hollingsworth, and Pankaj K Singh

Subjects

DHODH, MHC-I, P-TEFb, pyrimidine nucleotide, antigen presentation, Brequinar, Medicine, Science, Biology (General), QH301-705.5

Abstract

Pyrimidine nucleotide biosynthesis is a druggable metabolic dependency of cancer cells, and chemotherapy agents targeting pyrimidine metabolism are the backbone of treatment for many cancers. Dihydroorotate dehydrogenase (DHODH) is an essential enzyme in the de novo pyrimidine biosynthesis pathway that can be targeted by clinically approved inhibitors. However, despite robust preclinical anticancer efficacy, DHODH inhibitors have shown limited single-agent activity in phase 1 and 2 clinical trials. Therefore, novel combination therapy strategies are necessary to realize the potential of these drugs. To search for therapeutic vulnerabilities induced by DHODH inhibition, we examined gene expression changes in cancer cells treated with the potent and selective DHODH inhibitor brequinar (BQ). This revealed that BQ treatment causes upregulation of antigen presentation pathway genes and cell surface MHC class I expression. Mechanistic studies showed that this effect is (1) strictly dependent on pyrimidine nucleotide depletion, (2) independent of canonical antigen presentation pathway transcriptional regulators, and (3) mediated by RNA polymerase II elongation control by positive transcription elongation factor B (P-TEFb). Furthermore, BQ showed impressive single-agent efficacy in the immunocompetent B16F10 melanoma model, and combination treatment with BQ and dual immune checkpoint blockade (anti-CTLA-4 plus anti-PD-1) significantly prolonged mouse survival compared to either therapy alone. Our results have important implications for the clinical development of DHODH inhibitors and provide a rationale for combination therapy with BQ and immune checkpoint blockade.

Published

2024

4. Systemic Administration of a Brain Permeable Cdk5 Inhibitor Alters Neurobehavior

Author

Alan Umfress, Sarbjit Singh, Kevin J. Ryan, Ayanabha Chakraborti, Florian Plattner, Yogesh Sonawane, Jayapal Reddy Mallareddy, Edward P. Acosta, Amarnath Natarajan, and James A. Bibb

Subjects

cyclin-dependent kinase 5, pharmacokinetics, inhibitors, behavior, kinase inhibitors, Therapeutics. Pharmacology, RM1-950

Abstract

Cyclin-dependent kinase 5 (Cdk5) is a crucial regulator of neuronal signal transduction. Cdk5 activity is implicated in various neuropsychiatric and neurodegenerative conditions such as stress, anxiety, depression, addiction, Alzheimer’s disease, and Parkinson’s disease. While constitutive Cdk5 knockout is perinatally lethal, conditional knockout mice display resilience to stress-induction, enhanced cognition, neuroprotection from stroke and head trauma, and ameliorated neurodegeneration. Thus, Cdk5 represents a prime target for treatment in a spectrum of neurological and neuropsychiatric conditions. While intracranial infusions or treatment of acutely dissected brain tissue with compounds that inhibit Cdk5 have allowed the study of kinase function and corroborated conditional knockout findings, potent brain-penetrant systemically deliverable Cdk5 inhibitors are extremely limited, and no Cdk5 inhibitor has been approved to treat any neuropsychiatric or degenerative diseases to date. Here, we screened aminopyrazole-based analogs as potential Cdk5 inhibitors and identified a novel analog, 25–106, as a uniquely brain-penetrant anti-Cdk5 drug. We characterize the pharmacokinetic and dynamic responses of 25–106 in mice and functionally validate the effects of Cdk5 inhibition on open field and tail-suspension behaviors. Altogether, 25–106 represents a promising preclinical Cdk5 inhibitor that can be systemically administered with significant potential as a neurological/neuropsychiatric therapeutic.

Published

2022

5. Identification of potential binding pocket on viral oncoprotein HPV16 E6: a promising anti-cancer target for small molecule drug discovery

Author

Srikanth Kolluru, Rosemary Momoh, Lydia Lin, Jayapal Reddy Mallareddy, and John L. Krstenansky

Subjects

Human papilloma virus, HPV E6, Myricetin, Flavonol, Molecular modelling, Cytology, QH573-671

Abstract

Abstract Background Several human cancers, especially cervical cancer are caused by the infection of high risk strains of human papillomaviruses (HPV), notably HPV16. It is implicated that the oncoprotein E6 expressed from HPV, is inhibiting the apoptotic pathway by binding to adaptor molecule FADD (Fas-associated death domain). Inhibiting E6 interactions with FADD could provide a promising treatment for cervical cancer. There are few small molecules reported to inhibit such interactions. However, the FADD binding site information on the HPV E6 is not currently available. This binding site information may provide an opportunity to design new small molecule inhibitors to treat E6 mediated cancers. In this study we report the possible binding pocket on HPV16 E6 oncoprotein by using activity data of reported inhibitors through a stepwise molecular modeling approach. Results Blind docking and removing duplicates followed by visual inspection to determine ligand-receptor interactions provided 68 possible binding sites on the E6 protein. Individual docking of all known inhibitors lead to the identification of 28 pockets having some kind of correlation with their activity data. It was also observed that several of these pockets overlapped with each other, having some amino acids in common. Amino acids Leu50 and Cys51 were identified as key E6 residues for high affinity ligand binding which are seen in most of these pockets. In most cases, ligands demonstrated a hydrogen bond interaction with Cys51. Ala61, Arg131 and Gln107 were also frequently observed showing interactions among these pockets. A few amino acids unique to each ligand were also identified representing additional interactions at the receptor site. Conclusions After determining receptor-ligand interactions between E6 oncoprotein and the six known inhibitors, the amino acids Cys51, Leu50, Arg102, Arg131, Leu67, Val62, and Gln107 were identified to have importance in E6 inhibition. It was generally observed that Leu50 and Cys51 are necessary for high binding affinity with Cys51 being essential for hydrogen bonding. This study identified a potential binding pocket for the E6 inhibitors. Identification of the ligand binding pocket helps to design novel inhibitors of HPV16 E6 oncoprotein as a promising treatment for cervical cancer.

Published

2019

6. Radiotracers, tritium labelling of neuropeptides

Author

Géza Tóth, Jayapal Reddy Mallareddy, Fanni Tóth, Andrzej W. Lipkowski, and Dirk Tourwé

Subjects

Organic chemistry, QD241-441

Published

2012

7. Mycobacterium tuberculosis CitA activity is modulated by cysteine oxidation and pyruvate binding

Author

Rasangi Pathirage, Lorenza Favrot, Cecile Petit, Melvin Yamsek, Sarbjit Singh, Jayapal Reddy Mallareddy, Sandeep Rana, Amarnath Natarajan, and Donald R. Ronning

Subjects

Pharmacology, Organic Chemistry, Drug Discovery, Pharmaceutical Science, Molecular Medicine, Biochemistry

Abstract

The M. tuberculosis citrate synthase regulatory domain binds pyruvate to affect enzyme activity while cysteine oxidation in the same domain eliminates enzyme activity. This affords regulatory control at the protein level of entry to the TCA cycle.

Published

2023

8. DHODH inhibition enhances the efficacy of immune checkpoint blockade by increasing cancer cell antigen presentation

Author

Nicholas J. Mullen, Surendra K. Shukla, Ravi Thakur, Sai Sundeep Kollala, Dezhen Wang, Nina Chaika, Drew A. LaBreck, Jayapal Reddy Mallareddy, David H. Price, Amarnath Natarajan, Kamiya Mehla, David B. Sykes, Michael A. Hollingsworth, and Pankaj K. Singh

Abstract

Pyrimidine nucleotide biosynthesis is a druggable metabolic dependency of cancer cells, and chemotherapy agents targeting pyrimidine metabolism are the backbone of treatment for many cancers. Dihydroorotate dehydrogenase (DHODH) is an essential enzyme in the de novo pyrimidine biosynthesis pathway that can be targeted by clinically approved inhibitors. However, despite robust preclinical anticancer efficacy, DHODH inhibitors have shown limited single-agent efficacy in phase I clinical trials. Therefore, novel combination therapy strategies are necessary to realize the potential of these drugs. To search for therapeutic vulnerabilities induced by DHODH inhibition, we examined gene expression changes in cancer cells treated with the potent and selective DHODH inhibitor brequinar (BQ). This revealed that BQ treatment causes upregulation of antigen presentation pathway genes and cell surface MHC class I expression. Mechanistic studies showed that this effect is 1) strictly dependent on pyrimidine nucleotide depletion, 2) independent of canonical antigen presentation pathway transcriptional regulators, and 3) mediated by RNA polymerase II elongation control by positive transcription elongation factor B (P-TEFb). Furthermore, BQ showed impressive single-agent efficacy in the immunocompetent B16F10 melanoma model, and combination treatment with BQ and dual immune checkpoint blockade (anti-CTLA-4 plus anti-PD-1) significantly prolonged mouse survival compared to either therapy alone. Our results have important implications for the clinical development of DHODH inhibitors and provide a rationale for combination therapy with BQ and immune checkpoint blockade.

Published

2023

9. 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

10. 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

11. Selective CDK9 degradation using a proteolysis-targeting chimera (PROTAC) strategy

Author

Lidia Boghean, Amarnath Natarajan, Jayapal Reddy Mallareddy, and Sarbjit Singh

Subjects

Pharmacology, Flavonoids, Chemistry, Triazines, Proteolysis targeting chimera, Cancer, medicine.disease, Cyclin-Dependent Kinase 9, Cell biology, Thiazoles, Drug Discovery, Proteolysis, medicine, Molecular Medicine, Degradation (geology), Humans, Pyrazoles, Cyclin-dependent kinase 9, Protein Kinase Inhibitors

Published

2021

12. Inhibitors, PROTACs and Molecular Glues as Diverse Therapeutic Modalities to Target Cyclin-Dependent Kinase

Author

Amarnath Natarajan, Sandeep Rana, Jayapal Reddy Mallareddy, Lidia Boghean, and Sarbjit Singh

Subjects

Cancer Research, biology, Kinase, Chemistry, kinase, CDK, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Review, Cell cycle, Small molecule, Ubiquitin ligase, Cell biology, molecular glue, PROTAC, Oncology, Cyclin-dependent kinase, biology.protein, cancer, Cyclin-dependent kinase 6, Target protein, biological phenomena, cell phenomena, and immunity, RC254-282, CDK inhibitor

Abstract

Simple Summary Cyclin-dependent kinases (CDKs) are rich and viable therapeutic targets for various cancers. The emergence of event-driven pharmacology as an alternative to occupancy-driven pharmacology has begun to address the challenges associated with selectively targeting CDKs. In this review article, we summarize the CDK inhibitors that are currently in clinical trials. In addition, we provide an overview of PROTAC- and molecular glue-based strategies to modulate CDK function. Abstract The cyclin-dependent kinase (CDK) family of proteins play prominent roles in transcription, mRNA processing, and cell cycle regulation, making them attractive cancer targets. Palbociclib was the first FDA-approved CDK inhibitor that non-selectively targets the ATP binding sites of CDK4 and CDK6. In this review, we will briefly inventory CDK inhibitors that are either part of over 30 active clinical trials or recruiting patients. The lack of selectivity among CDKs and dose-limiting toxicities are major challenges associated with the development of CDK inhibitors. Proteolysis Targeting Chimeras (PROTACs) and Molecular Glues have emerged as alternative therapeutic modalities to target proteins. PROTACs and Molecular glues utilize the cellular protein degradation machinery to destroy the target protein. PROTACs are heterobifunctional molecules that form a ternary complex with the target protein and E3-ligase by making two distinct small molecule–protein interactions. On the other hand, Molecular glues function by converting the target protein into a “neo-substrate” for an E3 ligase. Unlike small molecule inhibitors, preclinical studies with CDK targeted PROTACs have exhibited improved CDK selectivity. Moreover, the efficacy of PROTACs and molecular glues are not tied to the dose of these molecular entities but to the formation of the ternary complex. Here, we provide an overview of PROTACs and molecular glues that modulate CDK function as emerging therapeutic modalities.

Published

2021

13. 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

14. 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

15. 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

16. Synthesis and pharmacological characterization of ethylenediamine synthetic opioids in human μ‐opiate receptor 1 (OPRM1) expressing cells

Author

Vincent Bustamante, Tim Lee, Kayla Yoshida, Tom Hsu, Alexander C. Zambon, Jayapal Reddy Mallareddy, and John L. Krstenansky

Subjects

media_common.quotation_subject, Analgesic, Gi alpha subunit, μ‐opioid receptor (OPRM1), Receptors, Opioid, mu, RM1-950, Pharmacology, 030226 pharmacology & pharmacy, Cell Line, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Cyclic AMP, medicine, Humans, General Pharmacology, Toxicology and Pharmaceutics, Internalization, Receptor, Gαi signaling, EC50, media_common, biased signaling, synthetic opioids, Molecular Structure, Original Articles, Ethylenediamines, Analgesics, Opioid, internalization, DAMGO, Neurology, chemistry, 030220 oncology & carcinogenesis, Morphine, Original Article, Therapeutics. Pharmacology, Enantiomer, medicine.drug

Abstract

Opioids are powerful analgesics acting via the human μ‐opiate receptor (hMOR). Opioid use is associated with adverse effects such as tolerance, addiction, respiratory depression, and constipation. Two synthetic opioids, AH‐7921 and U‐47700 that were developed in the 1970s but never marketed, have recently appeared on the illegal drug market and in forensic toxicology reports. These agents were initially characterized for their analgesic activity in rodents; however, their pharmacology at hMOR has not been delineated. Thus, we synthesized over 50 chemical analogs based on core AH‐7921 and U‐47700 structures to assess for their ability to couple to Gαi signaling and induce hMOR internalization. For both the AH‐7921 and U‐47700 analogs, the 3,4‐dichlorobenzoyl substituents were the most potent with comparable EC50 values for inhibition of cAMP accumulation; 26.49 ± 11.2 nmol L−1 and 8.8 ± 4.9 nmol L−1, respectively. Despite similar potencies for Gαi coupling, these two compounds had strikingly different hMOR internalization efficacies: U‐47700 (10 μmol L−1) induced ~25% hMOR internalization similar to DAMGO while AH‐7921 (10 μmol L−1) induced ~5% hMOR internalization similar to morphine. In addition, the R, R enantiomer of U‐47700 is significantly more potent than the S, S enantiomer at hMOR. In conclusion, these data suggest that U‐47700 and AH‐7921 analogs have high analgesic potential in humans, but with divergent receptor internalization profiles, suggesting that they may exhibit differences in clinical utility or abuse potential.

Published

2019

17. 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

18. Synthesis and binding characteristics of [3H]neuromedin N, a NTS2 receptor ligand

Author

Steven Ballet, Fanni Tóth, Sándor Benyhe, Magdalena Bujalska-Zadrożny, Patrycja Kleczkowska, Géza Tóth, Dirk Tourwé, Andrzej W. Lipkowski, and Jayapal Reddy Mallareddy

Subjects

Male, 0301 basic medicine, Agonist, Neurotensin receptor 2, medicine.drug_class, Stereochemistry, G protein, Ligands, Sulfur Radioisotopes, Tritium, Inhibitory Concentration 50, Radioligand Assay, 03 medical and health sciences, Cellular and Molecular Neuroscience, chemistry.chemical_compound, 0302 clinical medicine, Endocrinology, Opioid receptor, medicine, Animals, Receptors, Neurotensin, Rats, Wistar, Receptor, Neurotensin, Endocrine and Autonomic Systems, Chemistry, Brain, General Medicine, Receptor antagonist, Peptide Fragments, Rats, 030104 developmental biology, Spinal Cord, Neurology, Guanosine 5'-O-(3-Thiotriphosphate), Neuromedin N, 030217 neurology & neurosurgery, Protein Binding

Abstract

Neurotensin (NT) and its analog neuromedin N (NN) are formed by the processing of a common precursor in mammalian brain tissue and intestines. The biological effects mediated by NT and NN (e.g. analgesia, hypothermia) result from the interaction with G protein-coupled receptors. The goal of this study consisted of the synthesis and radiolabeling of NN, as well as the determination of the binding characteristics of [(3)H]NN and G protein activation by the cold ligand. In homologous displacement studies a weak affinity was determined for NN, with IC50 values of 454nM in rat brain and 425nM in rat spinal cord membranes. In saturation binding experiments the Kd value proved to be 264.8±30.18nM, while the Bmax value corresponded to 3.8±0.2pmol/mg protein in rat brain membranes. The specific binding of [(3)H]NN was saturable, interacting with a single set of homogenous binding sites. In sodium sensitivity experiments, a very weak inhibitory effect of Na(+) ions was observed on the binding of [(3)H]NN, resulting in an IC50 of 150.6mM. In [(35)S]GTPγS binding experiments the Emax value was 112.3±1.4% in rat brain and 112.9±2.4% in rat spinal cord membranes and EC50 values of 0.7nM and 0.79nM were determined, respectively. NN showed moderate agonist activities in stimulating G proteins. The stimulatory effect of NN could be maximally inhibited via use of the NTS2 receptor antagonist levocabastine, but not by the opioid receptor specific antagonist naloxone, nor by the NTS1 antagonist SR48692. These observations allow us to conclude that [(3)H]NN labels NTS2 receptors in rat brain membranes.

Published

2016

19. Recent advances in the discovery of small-molecule inhibitors of HIV-1 integrase

Author

Dai Lu, Eungi Choi, Jayapal Reddy Mallareddy, and Srikanth Kolluru

Subjects

0301 basic medicine, LEDGINs, medicine.medical_treatment, strand transfer inhibitors, Computational biology, Drug resistance, Review, 3′-processing, AIDS/HIV, 03 medical and health sciences, 0302 clinical medicine, Acquired immunodeficiency syndrome (AIDS), medicine, HIV integrase, chemistry.chemical_classification, Protease, biology, HIV integrase Inhibitors, virus diseases, medicine.disease, Small molecule, Reverse transcriptase, Integrase, 030104 developmental biology, Enzyme, chemistry, Viral replication, 030220 oncology & carcinogenesis, biology.protein, dual inhibitors, Biotechnology

Abstract

AIDS caused by the infection of HIV is a prevalent problem today. Rapid development of drug resistance to existing drug classes has called for the discovery of new targets. Within the three major enzymes (i.e., HIV-1 protease, HIV-1 reverse transcriptase and HIV-1 integrase [IN]) of the viral replication cycle, HIV-1 IN has been of particular interest due to the absence of human cellular homolog. HIV-1 IN catalyzes the integration of viral genetic material with the host genome, a key step in the viral replication process. Several novel classes of HIV IN inhibitors have been explored by targeting different sites on the enzyme. This review strives to provide readers with updates on the recent developments of HIV-1 IN inhibitors., Lay abstract AIDS is an epidemic disease that endangers the lives of millions of people across the world. The AIDS virus, also known as HIV, has developed resistance to the majority of available drugs on the market, thus requiring the need for new drugs. HIV integrase is one of the key viral enzymes required for viral cell proliferation. Since there is no similar enzyme in the human body, major emphasis is being made to develop therapeutics for this novel target. The drugs that are at various stages of development for this target are reviewed here.

Published

2018

20. Assessing the Activity of Synthetic Opioid AH‐7921 and U‐47700 Analogs in Cloned Human Mu‐Opioid Receptor Expressing Fibrosarcoma HT‐1080 Cells

Author

Emily Park, Edna Kemboi, Jayapal Reddy Mallareddy, Kayla Yoshida, Tim Lee, John L. Krstenansky, Tom Hsu, and Alexander C. Zambon

Subjects

Synthetic opioid, AH-7921, Chemistry, Pharmacology, medicine.disease, Biochemistry, U-47700, Genetics, medicine, μ-opioid receptor, Fibrosarcoma, Molecular Biology, Biotechnology, medicine.drug

Published

2018

21. Tritiated Opioid Receptor Ligands as Radiotracers

Author

Jayapal Reddy Mallareddy and Géza Tóth

Subjects

Pharmacology, Chemistry, medicine.drug_class, Central nervous system, Endogeny, Dynorphin, Ligands, Radioligand Assay, medicine.anatomical_structure, Opioid, Opioid receptor, Receptors, Opioid, Drug Discovery, medicine, Receptor, Opioid peptide, medicine.drug

Abstract

Tritiated opioid ligands are essential tools for the identification of opioid receptors. This review deals with the syntheses of tritiated opioid peptide derivatives, including enkephalins, dynorphins, dermorphins, deltorphins and endomorphins, and also discusses tritium-labeled nonpeptide opioids. It additionally focuses on the relevance of tritium-labeled opioid compounds as research tools for investigating opioid receptor pharmacology. Agonists and antagonists are used for the characterization of new opioid ligands by means of radioreceptor binding assays. Further topics covered in this review are the distribution of the endogenous peptides in the central nervous system and peripheral tissues, and degradation studies of opioids in brain membrane preparations and the blood.

Published

2014

22. Original article In vitro pharmacological evaluation of the radiolabeled C-terminal substance P analogue Lys-Phe-Phe-Gly-Leu-Met-NH2: Does a specific binding site exist?

Author

Jolanta Dyniewicz, Aleksandra Misicka, Aleksandra Tomczyszyn, Balazs Csibrany, Attila Keresztes, Géza Tóth, Andrzej W. Lipkowski, and Jayapal Reddy Mallareddy

Subjects

Chemistry, musculoskeletal, neural, and ocular physiology, Allosteric regulation, Substance P, digestive system, In vitro, Pathology and Forensic Medicine, chemistry.chemical_compound, Biochemistry, Radioligand, Neurology (clinical), Binding site, Pharmacophore, Receptor, Tachykinin receptor

Abstract

In the present paper, we report the synthesis, radiolabeling and comprehensive pharmacological evaluation of a C-terminally truncated tachykinin derivative, 3H-KFFGLM-NH2. The C-terminal fragments of endogenous tachykinins are pharmacophores responsible for interaction with the tachykinin receptors NK1, NK2 and NK3. The N-terminal fragments are responsible for modulation of receptor selectivity and interactions with other receptor systems. To evaluate and separate the function of an NK-pharmacophore from the activity of its parent neurokinin, KFFGLM-NH2 was synthesized in both tritiated and unlabeled forms. It has been proposed that the obtained NK-binding profiles of specific reference ligands and KFFGLM-NH2 differentiate monomeric and dimeric forms of NK receptors. We hypothesize that dimers of NK receptors could be specific receptor(s) for C-terminal fragments of all neurokinins as well as their C-terminal fragments, including H-KFFGLM-NH2. Dissociation of dimers into monomers opens access to additional allosteric binding sites. Fully elongated undecapeptide substance P interacts with both the "tachykinin pocket" and the "allosteric pocket" on the monomeric NK1 receptor, resulting in high and selective activation. However, C-terminal hexapeptide fragment analogues, recognizing only the "tachykinin pocket", may have less specific interactions with all tachykinin receptors in both monomeric and dimeric forms.

Published

2014

23. Radiotracers, tritium labelling of neuropeptides

Author

Dirk Tourwé, Andrzej W. Lipkowski, Jayapal Reddy Mallareddy, Fanni Tóth, and Géza Tóth

Subjects

Tritium illumination, Organic Chemistry, Radiochemistry, Neuropeptide, Substance P, lcsh:QD241-441, chemistry.chemical_compound, Nociceptin receptor, Metabolic pathway, lcsh:Organic chemistry, chemistry, Biochemistry, Labelling, Neuromedin N, Tritium

Abstract

Tritium labelled endomorphins (Tyr-Pro-Trp-Phe-NH 2, EM1, Tyr-Pro-Phe-Phe-NH 2, EM2) and their analogs, Angiotensin-IV (Val- Tyr-Ile-His-Pro -Phe) and its analogs, Neuromedin N (LysIle-Pro-Tyr-Ile-Leu) and a new nociceptin analog (P he-Phe-Gly-pFPhe-Thr-Gly-Aib-Arg-LysSer-Ala-Arg-Lys-Arg-Lys-Asn-Gln-NH 2) and Substance P analogs (Arg-Pro-Lys-Pro-Gln-GlnPhe-Phe-Gly-Leu-Nle-NH 2, Arg-Pro-Lys-Pro-Gln-Gln-Phe) were synthesized by catalytic dehalogenation or saturation of the precursor pepti des with tritium gas. The specific radioactivity of the neuropeptides is high, ranging from 0.6 TBq/ mmol to 2.8 TBq/mmol. The labelled peptides were characterized by radioreceptor bindin g assays and used in mapping their metabolic pathway using rat brain membrane preparation.

Published

2012

24. Transport Characteristics of Endomorphin-2 Analogues in Brain Capillary Endothelial Cells

Author

Judit Molnár, Csilla Fazakas, István A. Krizbai, Imola Wilhelm, Géza Tóth, Andrzej W. Lipkowski, Jayapal Reddy Mallareddy, and Péter Nagyőszi

Subjects

Pharmacology, Oligopeptide, Chemistry, Organic Chemistry, Blood–brain barrier, Biochemistry, In vitro, chemistry.chemical_compound, medicine.anatomical_structure, In vivo, Drug Discovery, Lipophilicity, medicine, Molecular Medicine, Opioid peptide, Receptor, Endomorphin

Abstract

Because of their poor metabolic stability and limited blood-brain barrier permeability, endomorphins have a low analgesic efficacy when administered systemically. Therefore, it is of great importance to design analogues with improved peptidase resistance and better delivery to the central nervous system. Recently, novel endomorphin-2 analogues have been synthesized, which proved to bind with high affinity and selectivity to the μ-opioid receptors and showed proteolytic resistance. In this study, we have analysed the transport characteristics of endomorphin-2 and three of its analogues [Dmt-Pro-Phe-Phe-NH(2) , Tyr-(1S,2R)Acpc-Phe-Phe-NH(2) and Tyr-(1S,2R)Achc-Phe-Phe-NH(2) ] using an in vitro blood-brain barrier model. The lipophilicity of the analogues, as assessed by their octanol/water partition coefficients, was higher than that of endomorphin-2. The flux of all four peptides from the apical (blood) side to the basolateral (brain) side was not saturable in the 10nm-1mm concentration range, suggesting that a passive mechanism plays a major role in their transport. The permeability coefficient of the analogues was significantly higher than that of endomorphin-2, suggesting increased blood-brain barrier penetration properties. We conclude that because of their good peptidase resistance and improved transport through brain endothelial cells, these endomorphin-2 analogues will have better analgesic properties in vivo.

Published

2012

25. In vitro pharmacological evaluation of the radiolabeled C-terminal substance P analogue Lys-Phe-Phe-Gly-Leu-Met-NH2: Does a specific binding site exist?

Author

Aleksandra, Tomczyszyn, Balazs, Csibrany, Attila, Keresztes, Jayapal Reddy, Mallareddy, Jolanta, Dyniewicz, Aleksandra, Misicka, Geza, Toth, and Andrzej W, Lipkowski

Subjects

Male, Binding Sites, Neurokinin A, Tachykinins, Animals, Female, Amino Acid Sequence, Rats, Wistar, Receptors, Neurokinin-1, Substance P, Peptides

Abstract

In the present paper, we report the synthesis, radiolabeling and comprehensive pharmacological evaluation of a C-terminally truncated tachykinin derivative, 3H-KFFGLM-NH2. The C-terminal fragments of endogenous tachykinins are pharmacophores responsible for interaction with the tachykinin receptors NK1, NK2 and NK3. The N-terminal fragments are responsible for modulation of receptor selectivity and interactions with other receptor systems. To evaluate and separate the function of an NK-pharmacophore from the activity of its parent neurokinin, KFFGLM-NH2 was synthesized in both tritiated and unlabeled forms. It has been proposed that the obtained NK-binding profiles of specific reference ligands and KFFGLM-NH2 differentiate monomeric and dimeric forms of NK receptors. We hypothesize that dimers of NK receptors could be specific receptor(s) for C-terminal fragments of all neurokinins as well as their C-terminal fragments, including H-KFFGLM-NH2. Dissociation of dimers into monomers opens access to additional allosteric binding sites. Fully elongated undecapeptide substance P interacts with both the "tachykinin pocket" and the "allosteric pocket" on the monomeric NK1 receptor, resulting in high and selective activation. However, C-terminal hexapeptide fragment analogues, recognizing only the "tachykinin pocket", may have less specific interactions with all tachykinin receptors in both monomeric and dimeric forms.

Published

2015

26. Synthesis and pharmacological evaluation of [(3)H]HS665, a novel, highly selective radioligand for the kappa opioid receptor

Author

Jayapal Reddy Mallareddy, Géza Tóth, Mariana Spetea, Elena Guerrieri, and Helmut Schmidhammer

Subjects

Pyrrolidines, Time Factors, Physiology, Cognitive Neuroscience, Population, Guinea Pigs, Benzeneacetamides, CHO Cells, Pharmacology, Transfection, Tritium, Biochemistry, κ-opioid receptor, law.invention, Guinea pig, Radioligand Assay, Cricetulus, law, Cricetinae, Phenethylamines, Radioligand, Animals, Humans, Receptor, Opioid peptide, education, education.field_of_study, Analgesics, Dose-Response Relationship, Drug, Chemistry, Naloxone, Chinese hamster ovary cell, Receptors, Opioid, kappa, Brain, Cell Biology, General Medicine, Analgesics, Opioid, Recombinant DNA, Protein Binding

Abstract

Herein we report the radiolabeling and pharmacological investigation of a novel radioligand, the N-cyclobutylmethyl substituted diphenethylamine [(3)H]HS665, designed to bind selectively to the kappa opioid peptide (KOP) receptor, a target of therapeutic interest for the treatment of a variety of human disorders (i.e., pain, affective disorders, drug addiction, and psychotic disorders). HS665 was prepared in tritium-labeled form by a dehalotritiated method resulting in a specific activity of 30.65 Ci/mmol. Radioligand binding studies were performed to establish binding properties of [(3)H]HS665 to the recombinant human KOP receptor in membranes from Chinese hamster ovary cells stably expressing human KOP receptors (CHOhKOP) and to the native neuronal KOP receptor in guinea pig brain membranes. Binding of [(3)H]HS665 was specific and saturable in both tissue preparations. A single population of high affinity binding sites was labeled by [(3)H]HS665 in membranes from CHOhKOP cells and guinea pig brain with similar equilibrium dissociation constants, Kd, 0.45 and 0.64 nM, respectively. Average receptor density of [(3)H]HS665 recognition sites were 5564 and 154 fmol/mg protein in CHOhKOP cells and guinea pig brain, respectively. This study shows that the new radioligand distinguishes and labels KOP receptors specifically in neuronal and cellular systems expressing KOP receptors, making this molecule a valuable tool in probing structural and functional mechanisms governing ligand-KOP receptor interactions in both a recombinant and native in vitro setting.

Published

2014

27. Design, Synthesis and Pharmacological Evaluation of Novel Endomorphin Analogues with Multiple Structural Modifications

Author

Jayapal Reddy Mallareddy

Published

2014

28. [3H]IVDE77, a novel radioligand with high affinity and selectivity for the insulin-regulated aminopeptidase

Author

Georges Vauquelin, Alexandros Nikolaou, Jayapal Reddy Mallareddy, Marko Poglitsch, Patrick Vanderheyden, Géza Tóth, Isabelle Van den Eynde, D. Tourwe, Jo A. Van Ginderachter, Department of Bio-engineering Sciences, Experimental Pharmacology, Molecular and Biochemical Pharmacology, Chemistry, Vriendenkring VUB, High Resolution NMR Centre, Organic Chemistry, and Cellular and Molecular Immunology

Subjects

Agonist, medicine.drug_class, Proteolysis, Biology, angiotensin II, Ligands, Aminopeptidase, Binding, Competitive, Cricetulus, Cricetinae, medicine, Radioligand, Animals, Humans, Cystinyl Aminopeptidase, Binding site, Pharmacology, Angiotensin II receptor type 1, medicine.diagnostic_test, Research Support, Non-U.S. Gov't, CHO cells, Azepines, In vitro, HEK293 Cells, Biochemistry, cardiovascular system, Oligopeptides, Intracellular, hormones, hormone substitutes, and hormone antagonists

Abstract

The hexapeptide angiotensin IV (Ang IV) induces diverse biological effects such as memory enhancement and protection against ischemic stroke. Studies on the mechanism of Ang IV however are hampered by its instability and its lack of selectivity. The high-affinity binding site for Ang IV is the insulin-regulated aminopeptidase (IRAP, EC 3.4.11.3), but Ang IV also acts as a weak agonist for the Ang II-receptor (AT1), implying the need for stable and highly selective Ang IV-analogues. Here we present the screening of novel Ang IV-analogues, selected on basis of high affinity for IRAP, high selectivity (compared to aminopeptidase N and the AT1 receptor) and resistance against proteases. The selected compound IVDE77 possesses a number of advantages compared to Ang IV: (i) it has a 40 times higher affinity for IRAP (Ki 1.71 nM), (ii) it does not activate the AT1 receptor, (iii) it is easily radiolabeled with tritium and (iv) it is resistant to proteolysis, even in human plasma. In addition, pre-treatment of intact CHO-K1 cells with IVDE77 led to a virtually complete inhibition of subsequent intracellular accumulation of [3H]IVDE77-IRAP complexes. IVDE77 thus represents the first Ang IV-analogue able to abolish IRAP-availability completely at the cell surface in vitro. In summary, IVDE77 is a useful tool for the detection of IRAP under physiological conditions, and may contribute to elucidating the mechanism of Ang IV to ascertain which functions are IRAP-dependent.

Published

2013

29. Stereoselective analysis of endomorphin diastereomers: resolution of biologically active analogues by capillary electrophoresis applying cyclodextrins as mobile phase additives

Author

Júlia Visy, Antal Péter, Krisztina Németh, Jayapal Reddy Mallareddy, Géza Tóth, and Celesztina Domonkos

Subjects

Analyte, Cyclodextrins, Chromatography, Resolution (mass spectrometry), Tetrapeptide, Chemistry, Clinical Biochemistry, Diastereomer, Pharmaceutical Science, Electrophoresis, Capillary, Stereoisomerism, Buffers, Hydrogen-Ion Concentration, Combinatorial chemistry, Analytical Chemistry, Electrophoresis, Isoelectric point, Capillary electrophoresis, Models, Chemical, Drug Discovery, Stereoselectivity, Isoelectric Point, Oligopeptides, Spectroscopy

Abstract

Seven diastereomer pairs of tetrapeptide analogues (TP) of endomorphin-1 and -2 were synthesized. A stereoselective capillary electrophoretic method was developed for controlling stereoisomeric ratio or purity. The isoelectric points of the tetrapeptides were between 8.3 and 8.9 as predicted and measured. A few of the analytes could be resolved without selectors due to the difference in their mobility. Neutral and anionic cyclodextrins (CDs) were applied in order to improve resolution. Stability constants as well as the mobilities of complexes were determined. Contributions of differences in the mobilities of free analytes and in the mobilities and stabilities of their complexes formed by CDs were equally important in the efficient resolution and migration order of diastereomers. As a result of the optimization of the pH of buffers and the concentration of the CD derivatives each diastereomer pair was resolved at baseline at least or better.

Published

2012

30. The Effect of Pro2 Modifications on the Structural and Pharmacological Properties of Endomorphin-2

Author

Katalin E. Kövér, Attila Keresztes, Jayapal Reddy Mallareddy, Géza Tóth, Attila Borics, and István Timári

Subjects

Male, Agonist, Magnetic Resonance Spectroscopy, Stereochemistry, medicine.drug_class, Proteolysis, Receptors, Opioid, mu, Substituent, Stereoisomerism, In Vitro Techniques, Molecular Dynamics Simulation, Mass Spectrometry, Protein Structure, Secondary, Radioligand Assay, Structure-Activity Relationship, chemistry.chemical_compound, Protein structure, Természettudományok, Drug Discovery, medicine, Animals, Structure–activity relationship, Rats, Wistar, Receptor, Kémiai tudományok, Solid-Phase Synthesis Techniques, medicine.diagnostic_test, Brain, Hydrogen Bonding, Nuclear magnetic resonance spectroscopy, Rats, Molecular Docking Simulation, chemistry, Molecular Medicine, Oligopeptides

Abstract

Endomorphins (EM-1 and EM-2) are selective, high affinity agonists of the μ-opioid (MOP) receptor, an important target in pain regulation. Their clinical use is impeded by their poor metabolic stability and limited entry to the central nervous system. In this study, the Pro(2) residue of EM-2 was modified systematically through substitution by hydroxyproline (Hyp), (S)-β-homoproline (βPro), 2-aminocyclopentene-1-carboxylic acid (ΔAcpc), or 2-aminocyclohexene-1-carboxylic acid (ΔAchc) to obtain stable MOP active compounds. Both Hyp(2) and βPro(2) substitution decreased receptor affinity. Analogues incorporating alicyclic β-amino acids exhibited diverse receptor binding properties, depending on the configuration of the substituent side-chain. (1S,2R)ΔAcpc(2)-EM-2 was shown to have MOP affinity and selectivity comparable to those of EM-2 and proved to act as agonist while being resistant to proteolysis. NMR and molecular dynamics (MD) studies revealed that bent backbone structures are predominant in the most potent analogues, while their presence is less pronounced in ligands of lower receptor affinity.

Published

2012

31. Transport characteristics of endomorphin-2 analogues in brain capillary endothelial cells

Author

Jayapal Reddy, Mallareddy, Géza, Tóth, Csilla, Fazakas, Judit, Molnár, Péter, Nagyőszi, Andrzej W, Lipkowski, István A, Krizbai, and Imola, Wilhelm

Subjects

Analgesics, Opioid, Blood-Brain Barrier, Animals, Brain, Endothelial Cells, Oligopeptides, Cells, Cultured, Permeability, Rats

Abstract

Because of their poor metabolic stability and limited blood-brain barrier permeability, endomorphins have a low analgesic efficacy when administered systemically. Therefore, it is of great importance to design analogues with improved peptidase resistance and better delivery to the central nervous system. Recently, novel endomorphin-2 analogues have been synthesized, which proved to bind with high affinity and selectivity to the μ-opioid receptors and showed proteolytic resistance. In this study, we have analysed the transport characteristics of endomorphin-2 and three of its analogues [Dmt-Pro-Phe-Phe-NH(2) , Tyr-(1S,2R)Acpc-Phe-Phe-NH(2) and Tyr-(1S,2R)Achc-Phe-Phe-NH(2) ] using an in vitro blood-brain barrier model. The lipophilicity of the analogues, as assessed by their octanol/water partition coefficients, was higher than that of endomorphin-2. The flux of all four peptides from the apical (blood) side to the basolateral (brain) side was not saturable in the 10nm-1mm concentration range, suggesting that a passive mechanism plays a major role in their transport. The permeability coefficient of the analogues was significantly higher than that of endomorphin-2, suggesting increased blood-brain barrier penetration properties. We conclude that because of their good peptidase resistance and improved transport through brain endothelial cells, these endomorphin-2 analogues will have better analgesic properties in vivo.

Published

2011

32. Asymmetric synthesis and conformational analysis by NMR spectroscopy and MD of Aba- and α-MeAba-containing dermorphin analogues

Author

Dirk Tourwé, Jayapal Reddy Mallareddy, Steven Ballet, José C. Martins, Rien De Wachter, Attila Keresztes, Fanni Tóth, Géza Tóth, Pieter M. S. Hendrickx, and Bart Vandormael

Subjects

Magnetic Resonance Spectroscopy, Stereochemistry, Protein Conformation, Deltorphin I, Phenylalanine, Receptors, Opioid, mu, Stereoisomerism, Molecular Dynamics Simulation, Ligands, Biochemistry, Methylation, chemistry.chemical_compound, Structure-Activity Relationship, Receptors, Opioid, delta, Drug Discovery, Animals, General Pharmacology, Toxicology and Pharmaceutics, Pharmacology, Chiral auxiliary, Organic Chemistry, Enantioselective synthesis, Hydrogen Bonding, Nuclear magnetic resonance spectroscopy, Dermorphin, Benzazepines, Rats, chemistry, Opioid Peptides, Molecular Medicine, Epimer, Enantiomer, Peptides

Abstract

Dermorphin analogues, containing a (S)- and (R)-4-amino1,2,4,5-tetrahydro-2-benzazepin-3-one scaffold (Aba) and the alpha-methylated analogues as conformationally constrained phenylalanines, were prepared. Asymmetric phase-transfer catalysis was unable to provide the (S)-alpha-Me-o-cyanophenylalanine precursor for (S)-alpha-MeAba in acceptable enantiomeric purity. However, by using a Schollkopf chiral auxiliary, this intermediate was obtained in 88% ee. [(S)-Aba 3-Gly 4] dermorphin retained mu-opioid affinity but displayed an increased delta-affinity. The corresponding R epimer was considerably less potent. In contrast, the [(R)-alpha-MeAba3-Gly4] dermorphin isomer was more potent than its S epimer. Tar-MD simulations of both non-methylated [Aba 3-Gly 4] dermorphin analogues showed a degree of folding at the C-terminal residues toward the N terminus of the peptide, without however, adopting a stabilized beta-turn conformation. The alpha-methylated analogues, on the other hand, exhibited a type I/I' beta-turn conformation over the alpha-MeAba3 and Gly4 residues, which was stabilized by a hydrogen bond involving Tyr5-H(N) and D-Ala 2-CO.

Published

2011

33. Design, synthesis, pharmacological evaluation, and structure-activity study of novel endomorphin analogues with multiple structural modifications

Author

Attila Keresztes, Dirk Tourwé, Jayapal Reddy Mallareddy, Katalin E. Kövér, Attila Borics, Géza Tóth, Chemistry, and Organic Chemistry

Subjects

Agonist, Male, Models, Molecular, Magnetic Resonance Spectroscopy, Molecular model, Stereochemistry, medicine.drug_class, COUPLING-CONSTANTS, ENZYMATIC DEGRADATION, Molecular Conformation, Receptors, Opioid, mu, Stereoisomerism, In Vitro Techniques, RAT-BRAIN, Ligands, ALPHA-AMINO ACIDS, chemistry.chemical_compound, Radioligand Assay, Structure-Activity Relationship, Természettudományok, Drug Stability, Drug Discovery, medicine, Structure–activity relationship, Animals, DIPEPTIDYL-PEPTIDASE IV, MU-OPIOID RECEPTORS, Amino Acids, Rats, Wistar, Kémiai tudományok, chemistry.chemical_classification, Chemistry, Ligand, Hydrolysis, Brain, Nuclear magnetic resonance spectroscopy, Combinatorial chemistry, BIOACTIVE CONFORMATION, Amino acid, Rats, nuclear magnetic resonance, Guanosine 5'-O-(3-Thiotriphosphate), ENDOGENOUS OPIATES, Molecular Medicine, Endomorphin, Oligopeptides, BIOLOGICAL-ACTIVITY

Abstract

This study reports on new proteolytically stable, pharmacologically active endomorphin analogues, incorporating Dmt(1), Achc(2), pFPhe(4), or beta MePhe(4) unnatural amino acids. Consistent with earlier results, it was found that the analogues carrying anti and Achc2 residues displayed the highest p-opioid receptor affinities, depending upon the configuration of the incorporated Achc(2). Combination of such derivatives with pFPhe(4) or beta MePhe(4) yielded further compounds with variable binding potencies. Combined application of Dmt(1), cis-(1S,2R)Achc(2), and pFPhe(4) (compound 16) resulted in the most potent analogue. Ligand stimulated [S-35]GTP gamma S binding assays indicated that the analogues retained their agonist activities and opioid receptor specificities. NMR and molecular modeling studies of the analogues containing beta MePhe(4) or pFPhe(4) confirmed the predominance of bent structures, however, it is apparent that bent structures are energetically more favored than random/extended structures for all studied compounds.

Published

2011

34. A putative pharmacophore model of μ-opioid receptor activity

Author

Katalin E. Kövér, Géza Tóth, Attila Borics, and Jayapal Reddy Mallareddy

Subjects

Pharmacology, Pharmacotherapy, Chemistry, Opioid receptor activity, General Medicine, Pharmacophore

Published

2011

35. Design, synthesis and pharmacological evaluation of novel endomorphin analogues with multiple structural modifications

Author

Attila Keresztes, Attila Borics, Géza Tóth, and Jayapal Reddy Mallareddy

Subjects

Pharmacology, chemistry.chemical_compound, Design synthesis, Chemistry, General Medicine, Endomorphin

Published

2011

36. Design, Synthesis, Pharmacological Evaluation, and Structure−Activity Study of Novel Endomorphin Analogues with Multiple Structural Modifications.

Author

Jayapal Reddy Mallareddy, Attila Borics, Attila Keresztes, Katalin E. Kövér, Dirk Tourwé, and Géza Tóth

Subjects

*DRUG design, *STRUCTURE-activity relationship in pharmacology, *OPIOID peptides, *PHARMACOLOGY, *LIGAND binding (Biochemistry), *OPIOID receptors, *NUCLEAR magnetic resonance, *MOLECULAR models

Abstract

This study reports on new proteolytically stable, pharmacologically active endomorphin analogues, incorporating Dmt1, Achc2, pFPhe4, or βMePhe4unnatural amino acids. Consistent with earlier results, it was found that the analogues carrying Dmt1and Achc2residues displayed the highest μ-opioid receptor affinities, depending upon the configuration of the incorporated Achc2. Combination of such derivatives with pFPhe4or βMePhe4yielded further compounds with variable binding potencies. Combined application of Dmt1, cis-(1S,2R)Achc2, and pFPhe4(compound 16) resulted in the most potent analogue. Ligand stimulated [35S]GTPγS binding assays indicated that the analogues retained their agonist activities and opioid receptor specificities. NMR and molecular modeling studies of the analogues containing βMePhe4or pFPhe4confirmed the predominance of bent structures, however, it is apparent that bent structures are energetically more favored than random/extended structures for all studied compounds. [ABSTRACT FROM AUTHOR]

Published

2011