Your search keyword '"James R. Fuchs"' showing total 142 results

1. Anti-tumor effects of the eIF4A inhibitor didesmethylrocaglamide and its derivatives in human and canine osteosarcomas

Author

Janet L. Oblinger, Jack Wang, Georgia D. Wetherell, Garima Agarwal, Tyler A. Wilson, Nicole R. Benson, Joelle M. Fenger, James R. Fuchs, A. Douglas Kinghorn, and Long-Sheng Chang

Subjects

Osteosarcoma, Didesmethylrocaglamide (DDR), Rocaglamide (Roc), eIF4A inhibitor, p38 stress-activated protein kinase, RhoB, Medicine, Science

Abstract

Abstract Inhibition of translation initiation using eIF4A inhibitors like (−)-didesmethylrocaglamide [(−)-DDR] and (−)-rocaglamide [(−)-Roc] is a potential cancer treatment strategy as they simultaneously diminish multiple oncogenic drivers. We showed that human and dog osteosarcoma cells expressed higher levels of eIF4A1/2 compared with mesenchymal stem cells. Genetic depletion of eIF4A1 and/or 2 slowed osteosarcoma cell growth. To advance preclinical development of eIF4A inhibitors, we demonstrated the importance of (−)-chirality in DDR for growth-inhibitory activity. Bromination of DDR at carbon-5 abolished growth-inhibitory activity, while acetylating DDR at carbon-1 was tolerated. Like (−)-DDR, (±)-DDR, and (−)-Roc, (±)-DDR-acetate increased γH2A.X levels and induced G2/M arrest and apoptosis. Consistent with translation inhibition, these rocaglates decreased the levels of several mitogenic kinases, the STAT3 transcription factor, and the stress-activated protein kinase p38. However, phosphorylated p38 was greatly enhanced in treated cells, suggesting activation of stress response pathways. RNA sequencing identified RHOB as a top upregulated gene in both (−)-DDR- and (−)-Roc-treated osteosarcoma cells, but the Rho inhibitor Rhosin did not enhance the growth-inhibitory activity of (−)-DDR or (−)-Roc. Nonetheless, these rocaglates potently suppressed tumor growth in a canine osteosarcoma patient-derived xenograft model. These results suggest that these eIF4A inhibitors can be leveraged to treat both human and dog osteosarcomas.

Published

2024

2. The structural and mechanistic bases for the viral resistance to allosteric HIV-1 integrase inhibitor pirmitegravir

Author

Tung Dinh, Zahira Tber, Juan S. Rey, Seema Mengshetti, Arun S. Annamalai, Reed Haney, Lorenzo Briganti, Franck Amblard, James R. Fuchs, Peter Cherepanov, Kyungjin Kim, Raymond F. Schinazi, Juan R. Perilla, Baek Kim, and Mamuka Kvaratskhelia

Subjects

HIV-1 integrase, antiretroviral drug, ALLINI, pirmitegravir, Microbiology, QR1-502

Abstract

ABSTRACT Allosteric HIV-1 integrase (IN) inhibitors (ALLINIs) are investigational antiretroviral agents that potently impair virion maturation by inducing hyper-multimerization of IN and inhibiting its interaction with viral genomic RNA. The pyrrolopyridine-based ALLINI pirmitegravir (PIR) has recently advanced into phase 2a clinical trials. Previous cell culture-based viral breakthrough assays identified the HIV-1(Y99H/A128T IN) variant that confers substantial resistance to this inhibitor. Here, we have elucidated the unexpected mechanism of viral resistance to PIR. Although both Tyr99 and Ala128 are positioned within the inhibitor binding V-shaped cavity at the IN catalytic core domain (CCD) dimer interface, the Y99H/A128T IN mutations did not substantially affect the direct binding of PIR to the CCD dimer or functional oligomerization of full-length IN. Instead, the drug-resistant mutations introduced a steric hindrance at the inhibitor-mediated interface between CCD and C-terminal domain (CTD) and compromised CTD binding to the CCDY99H/A128T + PIR complex. Consequently, full-length INY99H/A128T was substantially less susceptible to the PIR-induced hyper-multimerization than the WT protein, and HIV-1(Y99H/A128T IN) conferred >150-fold resistance to the inhibitor compared with the WT virus. By rationally modifying PIR, we have developed its analog EKC110, which readily induced hyper-multimerization of INY99H/A128T in vitro and was ~14-fold more potent against HIV-1(Y99H/A128T IN) than the parent inhibitor. These findings suggest a path for developing improved PIR chemotypes with a higher barrier to resistance for their potential clinical use.IMPORTANCEAntiretroviral therapies save the lives of millions of people living with HIV (PLWH). However, the evolution of multi-drug-resistant viral phenotypes is a major clinical problem, and there are limited or no treatment options for heavily treatment-experienced PLWH. Allosteric HIV-1 integrase inhibitors (ALLINIs) are a novel class of antiretroviral compounds that work by a unique mechanism of binding to the non-catalytic site on the viral protein and inducing aberrant integrase multimerization. Accordingly, ALLINIs potently inhibit both wild-type HIV-1 and all drug-resistant viral phenotypes that have so far emerged against currently used therapies. Pirmitegravir, a highly potent and safe investigational ALLINI, is currently advancing through clinical trials. Here, we have elucidated the structural and mechanistic bases behind the emergence of HIV-1 integrase mutations in infected cells that confer resistance to pirmitegravir. In turn, our findings allowed us to rationally develop an improved ALLINI with substantially enhanced potency against the pirmitegravir-resistant virus.

Published

2024

3. G 2 Retro as a two-step graph generative models for retrosynthesis prediction

Author

Ziqi Chen, Oluwatosin R. Ayinde, James R. Fuchs, Huan Sun, and Xia Ning

Subjects

Chemistry, QD1-999

Abstract

Abstract Retrosynthesis is a procedure where a target molecule is transformed into potential reactants and thus the synthesis routes can be identified. Recently, computational approaches have been developed to accelerate the design of synthesis routes. In this paper,we develop a generative framework G 2 Retro for one-step retrosynthesis prediction. G 2 Retro imitates the reversed logic of synthetic reactions. It first predicts the reaction centers in the target molecules (products), identifies the synthons needed to assemble the products, and transforms these synthons into reactants. G 2 Retro defines a comprehensive set of reaction center types, and learns from the molecular graphs of the products to predict potential reaction centers. To complete synthons into reactants, G 2 Retro considers all the involved synthon structures and the product structures to identify the optimal completion paths, and accordingly attaches small substructures sequentially to the synthons. Here we show that G 2 Retro is able to better predict the reactants for given products in the benchmark dataset than the state-of-the-art methods.

Published

2023

4. Tomatidine targets ATF4-dependent signaling and induces ferroptosis to limit pancreatic cancer progression

Author

Debasmita Mukherjee, Srija Chakraborty, Lena Bercz, Liliana D’Alesio, Jessica Wedig, Molly A. Torok, Timothy Pfau, Hannah Lathrop, Shrina Jasani, Abigail Guenther, Jake McGue, Daniel Adu-Ampratwum, James R. Fuchs, Timothy L. Frankel, Maciej Pietrzak, Stacey Culp, Anne M. Strohecker, Aleksander Skardal, and Thomas A. Mace

Subjects

Therapeutics, Microenvironment, Cancer, Science

Abstract

Summary: Pancreatic ductal adenocarcinoma (PDAC) is an aggressive cancer with high metastasis and therapeutic resistance. Activating transcription factor 4 (ATF4), a master regulator of cellular stress, is exploited by cancer cells to survive. Prior research and data reported provide evidence that high ATF4 expression correlates with worse overall survival in PDAC. Tomatidine, a natural steroidal alkaloid, is associated with inhibition of ATF4 signaling in multiple diseases. Here, we discovered that in vitro and in vivo tomatidine treatment of PDAC cells inhibits tumor growth. Tomatidine inhibited nuclear translocation of ATF4 and reduced the transcriptional binding of ATF4 with downstream promoters. Tomatidine enhanced gemcitabine chemosensitivity in 3D ECM-hydrogels and in vivo. Tomatidine treatment was associated with induction of ferroptosis signaling validated by increased lipid peroxidation, mitochondrial biogenesis, and decreased GPX4 expression in PDAC cells. This study highlights a possible therapeutic approach utilizing a plant-derived metabolite, tomatidine, to target ATF4 activity in PDAC.

Published

2023

5. Efficacy of quorum sensing and growth inhibitors alone and in combination against avian pathogenic Escherichia coli infection in chickens

Author

Yosra A. Helmy, Dipak Kathayat, Gary Closs, Jr, Katie Galgozy, James R. Fuchs, and Gireesh Rajashekara

Subjects

APEC, growth inhibitor, quorum sensing inhibitor, oral challenge, field simulated conditions, Animal culture, SF1-1100

Abstract

ABSTRACT: Avian pathogenic E. coli (APEC), a causative agent of colibacillosis, is associated with high mortality and morbidity which results in severe economic losses to the poultry industry worldwide. APEC can be transmitted to humans through the consumption of contaminated poultry products. The limited effect of the current vaccines and the advent of drug-resistant strains have necessitated the development of alternative therapies. Previously, we identified 2 small molecules (SMs; [quorum sensing inhibitor; QSI-5] and [growth inhibitor; GI-7]) with high efficacy in vitro and in chickens subcutaneously challenged with APEC O78. Here, we optimized the oral challenge dose of APEC O78 in chickens to mimic the infection in the natural settings, evaluated the efficacy of the GI-7, QSI-5, and combination of GI-7 and QSI-5 (GI7+ QSI-5) in chickens orally infected with APEC, and compared their efficacy to sulfadimethoxine (SDM), an antibiotic currently used to treat APEC. Using the optimized dose of each SM in drinking water, GI-7, QSI-5, GI7+ QSI-5, and SDM were evaluated in chickens challenged with the optimized dose of APEC O78 (1 × 109 CFU/chicken; orally; d 2 of age) and grown on built-up floor litter. Reduction in mortality was 90, 80, 80, and 70% in QSI-5, GI-7+QSI-5, GI-7, and SDM treated groups compared to the positive control (PC), respectively. GI-7, QSI-5, GI-7+QSI-5, and SDM reduced the APEC load in the cecum by 2.2, 2.3, 1.6, and 0.6 logs and in the internal organs by 1.3, 1.2, 1.4, and 0.4 logs compared to PC (P < 0.05), respectively. The cumulative pathological lesions scores were 0.51, 0.24, 0.0, 0.53, and 1.53 in GI-7, QSI-5, GI-7+QSI-5, SDM, and PC groups, respectively. Overall, GI-7 and QSI-5 individually have promising effects as a potential antibiotic-independent approach to control APEC infections in chickens.

Published

2023

6. PHY34 inhibits autophagy through V-ATPase V0A2 subunit inhibition and CAS/CSE1L nuclear cargo trafficking in high grade serous ovarian cancer

Author

Amrita Salvi, Alexandria N. Young, Andrew C. Huntsman, Melissa R. Pergande, Melissa A. Korkmaz, Rathnayake A. Rathnayake, Brittney K. Mize, A. Douglas Kinghorn, Xiaoli Zhang, Kiira Ratia, Markus Schirle, Jason R. Thomas, Scott M. Brittain, Claude Shelton, Leslie N. Aldrich, Stephanie M. Cologna, James R. Fuchs, and Joanna E. Burdette

Subjects

Cytology, QH573-671

Abstract

Abstract PHY34 is a synthetic small molecule, inspired by a compound naturally occurring in tropical plants of the Phyllanthus genus. PHY34 was developed to have potent in vitro and in vivo anticancer activity against high grade serous ovarian cancer (HGSOC) cells. Mechanistically, PHY34 induced apoptosis in ovarian cancer cells by late-stage autophagy inhibition. Furthermore, PHY34 significantly reduced tumor burden in a xenograft model of ovarian cancer. In order to identify its molecular target/s, we undertook an unbiased approach utilizing mass spectrometry-based chemoproteomics. Protein targets from the nucleocytoplasmic transport pathway were identified from the pulldown assay with the cellular apoptosis susceptibility (CAS) protein, also known as CSE1L, representing a likely candidate protein. A tumor microarray confirmed data from mRNA expression data in public databases that CAS expression was elevated in HGSOC and correlated with worse clinical outcomes. Overexpression of CAS reduced PHY34 induced apoptosis in ovarian cancer cells based on PARP cleavage and Annexin V staining. Compounds with a diphyllin structure similar to PHY34 have been shown to inhibit the ATP6V0A2 subunit of V(vacuolar)-ATPase. Therefore, ATP6V0A2 wild-type and ATP6V0A2 V823 mutant cell lines were tested with PHY34, and it was able to induce cell death in the wild-type at 246 pM while the mutant cells were resistant up to 55.46 nM. Overall, our data demonstrate that PHY34 is a promising small molecule for cancer therapy that targets the ATP6V0A2 subunit to induce autophagy inhibition while interacting with CAS and altering nuclear localization of proteins.

Published

2022

7. Identification and Optimization of a Novel HIV‑1 Integrase Inhibitor

Author

Daniel Adu-Ampratwum, Yuhan Pan, Pratibha C. Koneru, Janet Antwi, Ashley C. Hoyte, Jacques Kessl, Patrick R. Griffin, Mamuka Kvaratskhelia, James R. Fuchs, and Ross C. Larue

Subjects

Chemistry, QD1-999

Published

2022

8. Structural and Mechanistic Bases of Viral Resistance to HIV-1 Capsid Inhibitor Lenacapavir

Author

Stephanie M. Bester, Daniel Adu-Ampratwum, Arun S. Annamalai, Guochao Wei, Lorenzo Briganti, Bridget C. Murphy, Reed Haney, James R. Fuchs, and Mamuka Kvaratskhelia

Subjects

HIV-1, capsid, antiretroviral agents, drug resistance mechanisms, structure, Microbiology, QR1-502

Abstract

ABSTRACT Lenacapavir (LEN) is a long-acting, highly potent HIV-1 capsid (CA) inhibitor. The evolution of viral variants under the genetic pressure of LEN identified Q67H, N74D, and Q67H/N74D CA substitutions as the main resistance associated mutations (RAMs). Here, we determined high-resolution structures of CA hexamers containing these RAMs in the absence and presence of LEN. Our findings reveal that the Q67H change induces a conformational switch, which adversely affects the inhibitor binding. In the unliganded protein, the His67 side chain adopts the closed conformation by projecting into the inhibitor binding pocket and thereby creating steric hindrance with respect to LEN. Upon the inhibitor binding, the His67 side chain repositions to the open conformation that closely resembles the Gln67 side chain in the WT protein. We propose that the switch from the closed conformation to the open conformation, which is needed to accommodate LEN, accounts for the reduced inhibitor potency with respect to the Q67H CA variant. The N74D CA change results in the loss of a direct hydrogen bond and in induced electrostatic repulsions between CA and LEN. The double Q67H/N74D substitutions exhibited cumulative effects of respective single amino acid changes. An examination of LEN binding kinetics to CA hexamers revealed that Q67H and N74D CA changes adversely influenced the inhibitor binding affinity (KD) by primarily affecting the dissociation rate constant (koff). We used these structural and mechanistic findings to rationally modify LEN. The resulting analog exhibited increased potency against the Q67H/N74D viral variant. Thus, our studies provide a means for the development of second-generation inhibitors with enhanced barriers to resistance. IMPORTANCE LEN is an investigational long-acting agent for future HIV-1 treatment regimens. While ongoing clinical trials have highlighted a largely beneficial profile of LEN for the treatment of HIV-1 infected people with limited therapy options, one notable shortcoming is a relatively low barrier of viral resistance to the inhibitor. Cell culture-based viral breakthrough assays identified N74D, Q67H, and N74D/Q67H capsid changes as the main resistance associated mutations (RAMs). N74D and Q67H capsid substitutions have also emerged in clinical trials in some patients who received subcutaneous LEN. Understanding the structural basis behind viral resistance to LEN is expected to aid in the rational development of improved inhibitors with enhanced barriers to resistance. Here, we report high resolution structures of the main drug resistant capsid variants, which provide mechanistic insight into the viral resistance to LEN. We used these findings to develop an improved inhibitor, which exhibited enhanced activity against the viral Q67H/N74D capsid phenotype compared with that of parental LEN.

Published

2022

9. Evaluation of Novel Quorum Sensing Inhibitors Targeting Auto-Inducer 2 (AI-2) for the Control of Avian Pathogenic Escherichia coli Infections in Chickens

Author

Yosra A. Helmy, Dipak Kathayat, Loic Deblais, Vishal Srivastava, Gary Closs, Robert J. Tokarski, Oluwatosin Ayinde, James R. Fuchs, and Gireesh Rajashekara

Subjects

APEC, quorum sensing, inhibitors, anti-virulence, auto-inducer 2, QSI-5, Microbiology, QR1-502

Abstract

ABSTRACT Avian pathogenic Escherichia coli (APEC) associated with colibacillosis results in high morbidity and mortality, and severe economic losses to the poultry industry. APEC is a zoonotic pathogen and can infect humans through contaminated poultry products. Vaccination and antibiotic treatment are currently used to control APEC infections; however, the limited effect of vaccines and the emergence of antibiotic-resistant strains have necessitated the development of novel therapeutics. Here, we evaluated seven quorum sensing inhibitors (QSI) identified in our previous study, in APEC-infected chickens. QSIs were administered orally (~92 to 120 μg/bird) and chickens were challenged subcutaneously with APEC. Among them, QSI-5 conferred the best protection (100% reduction in mortality, 82% to 93% reduction in lesions [airsacculitis, perihepatitis, lung congestion, pericarditis] severity, and 5.2 to 6.1 logs reduction in APEC load). QSI-5 was further tested in chickens raised on built-up floor litter using an optimized dose (1 mg/L) in drinking water. QSI-5 reduced the mortality (88.4%), lesion severity (72.2%), and APEC load (2.8 logs) in chickens, which was better than the reduction observed with currently used antibiotic sulfadimethoxine (SDM; mortality 35.9%; lesion severity up to 36.9%; and APEC load up to 2.4 logs). QSI-5 was detected in chicken's blood after 0.5 h with no residues in muscle, liver, and kidney. QSI-5 increased the body weight gain with no effect on the feed conversion ratio and cecal microbiota of the chickens. Metabolomic studies revealed reduced levels of 5′-methylthioadenosine in QSI-5-treated chicken serum. In conclusion, QSI-5 displayed promising effects in chickens and thus, represents a novel anti-APEC therapeutic. IMPORTANCE Avian pathogenic Escherichia coli (APEC), a subgroup of ExPEC, is a zoonotic pathogen with public health importance. Quorum sensing is a mechanism that regulates virulence, biofilm formation, and pathogenesis in bacteria. Here, we identified a novel quorum sensing autoinducer-2 inhibitor, QSI-5, which showed higher anti-APEC efficacy in chickens compared to the currently used antibiotic, sulfadimethoxine at a much lower dose (up to 4,500 times). QSI-5 is readily absorbed with no residues in the tissues. QSI-5 also increased the chicken’s body weight gain and did not impact the cecal microbiota composition. Overall, QSI-5 represents a promising lead compound for developing novel anti-virulence therapies with significant implications for treating APEC infections in chickens as well as other ExPEC associated infections in humans. Further identification of its target(s) and understanding the mechanism of action of QSI-5 in APEC will add to the future novel drug development efforts that can overcome the antimicrobial resistance problem.

Published

2022

10. Evaluation of synergy between host and pathogen-directed therapies against intracellular Leishmania donovani

Author

M. Shamim Hasan Zahid, Monica M. Johnson, Robert J. Tokarski, II, Abhay R. Satoskar, James R. Fuchs, Eric M. Bachelder, and Kristy M. Ainslie

Subjects

Infectious and parasitic diseases, RC109-216

Abstract

Visceral leishmaniasis (VL) is associated with treatment complications due to the continued growth of resistant parasites toward currently available pathogen-directed therapeutics. To limit the emergence and combat resistant parasites there is a need to develop new anti-leishmanial drugs and alternative treatment approaches, such as host-directed therapeutics (HDTs). Discovery of new anti-leishmanial drugs including HDTs requires suitable in vitro assay systems. Herein, we modified and evaluated a series of resazurin assays against different life-stages of the VL causing parasite, Leishmania donovani to identify novel HDTs. We further analyzed the synergy of combinatorial interactions between traditionally used pathogen-directed drugs and HDTs for clearance of intracellular L. donovani. The inhibitory concentration at 50% (IC50) of the five evaluated therapies [amphotericin B (AMB), miltefosine, paromomycin, DNER-4, and AR-12 (OSU-03012)] was determined against promastigotes, extracellular amastigotes, and intracellular amastigotes of L. donovani via a resazurin-based assay and compared to image-based microscopy. Using the resazurin-based assay, all evaluated therapies showed reproducible anti-leishmanial activity against the parasite's different life-stages. These results were consistent to the traditional image-based technique. The gold standard of therapy, AMB, showed the highest potency against intracellular L. donovani, and was further evaluated for combinatorial effects with the HDTs. Among the combinations analyzed, pathogen-directed AMB and host-directed AR-12 showed a synergistic reduction of intracellular L. donovani compared to individual treatments. The modified resazurin assay used in this study demonstrated a useful technique to measure new anti-leishmanial drugs against both intracellular and extracellular parasites. The synergistic interactions between pathogen-directed AMB and host-directed AR-12 showed a great promise to combat VL, with the potential to reduce the emergence of drug-resistant strains. Keywords: Visceral leishmaniasis, Resazurin assay, Host-directed therapy, Combinatorial therapy, AR-12, DNER-4

Published

2019

11. Insertional Mutagenesis Identifies a STAT3/Arid1b/β-catenin Pathway Driving Neurofibroma Initiation

Author

Jianqiang Wu, Vincent W. Keng, Deanna M. Patmore, Jed J. Kendall, Ami V. Patel, Edwin Jousma, Walter J. Jessen, Kwangmin Choi, Barbara R. Tschida, Kevin A.T. Silverstein, Danhua Fan, Eric B. Schwartz, James R. Fuchs, Yuanshu Zou, Mi-Ok Kim, Eva Dombi, David E. Levy, Gang Huang, Jose A. Cancelas, Anat O. Stemmer-Rachamimov, Robert J. Spinner, David A. Largaespada, and Nancy Ratner

Subjects

Biology (General), QH301-705.5

Abstract

To identify genes and signaling pathways that initiate Neurofibromatosis type 1 (NF1) neurofibromas, we used unbiased insertional mutagenesis screening, mouse models, and molecular analyses. We mapped an Nf1-Stat3-Arid1b/β-catenin pathway that becomes active in the context of Nf1 loss. Genetic deletion of Stat3 in Schwann cell progenitors (SCPs) and Schwann cells (SCs) prevents neurofibroma formation, decreasing SCP self-renewal and β-catenin activity. β-catenin expression rescues effects of Stat3 loss in SCPs. Importantly, P-STAT3 and β-catenin expression correlate in human neurofibromas. Mechanistically, P-Stat3 represses Gsk3β and the SWI/SNF gene Arid1b to increase β-catenin. Knockdown of Arid1b or Gsk3β in Stat3fl/fl;Nf1fl/fl;DhhCre SCPs rescues neurofibroma formation after in vivo transplantation. Stat3 represses Arid1b through histone modification in a Brg1-dependent manner, indicating that epigenetic modification plays a role in early tumorigenesis. Our data map a neural tumorigenesis pathway and support testing JAK/STAT and Wnt/β-catenin pathway inhibitors in neurofibroma therapeutic trials.

Published

2016

12. Identification of a Small Molecule Anti-biofilm Agent Against Salmonella enterica

Author

Jasmine Moshiri, Darpan Kaur, Chido M. Hambira, Jenna L. Sandala, Jacob A. Koopman, James R. Fuchs, and John S. Gunn

Subjects

biofilm, chronic infection, Salmonella, Typhoid, anti-biofilm, Microbiology, QR1-502

Abstract

Biofilm formation is a common strategy utilized by bacterial pathogens to establish persistence in a host niche. Salmonella enterica serovar Typhi, the etiological agent of Typhoid fever, relies on biofilm formation in the gallbladder to chronically colonize asymptomatic carriers, allowing for transmission to uninfected individuals. S. enterica serovar Typhimurium utilizes biofilms to achieve persistence in human and animal hosts, an issue of both clinical and agricultural importance. Here, we identify a compound that selectively inhibits biofilm formation in both S. Typhi and S. Typhimurium serovars at early stages of biofilm development with an EC50 of 21.0 and 7.4 μM, respectively. We find that this compound, T315, also reduces biofilm formation in Acinetobacter baumannii, a nosocomial and opportunistic pathogen with rising antibiotic resistance. T315 treatment in conjunction with sub-MIC dosing of ciprofloxacin further reduces S. enterica biofilm formation, demonstrating the potential of such combination therapies for therapeutic development. Through synthesis of two biotin-labeled T315 probes and subsequent pull-down and proteomics analysis, we identified a T315 binding target: WrbA, a flavin mononucleotide-dependent NADH:quinone oxidoreductase. Using a S. Typhimurium strain lacking WrbA we demonstrate that this factor contributes to endogenous S. enterica biofilm formation processes and is required for full T315 anti-biofilm activity. We suggest WrbA as a promising target for further development of anti-biofilm agents in Salmonella, with potential for use against additional bacterial pathogens. The development of anti-biofilm therapeutics will be essential to combat chronic carriage of Typhoid fever and thus accomplish a meaningful reduction of global disease burden.

Published

2018

13. Supplemental Figures w/ Legends from Phyllanthusmin Derivatives Induce Apoptosis and Reduce Tumor Burden in High-Grade Serous Ovarian Cancer by Late-Stage Autophagy Inhibition

Author

Joanna E. Burdette, James R. Fuchs, Leslie N. Aldrich, Mitch A. Phelps, Xiaoli Zhang, A. Douglas Kinghorn, Steven M. Swanson, Hongyan Wang, Salane King, Christopher C. Coss, Shamalatha Kolli, Sarmistha Mazumder, Daniel D. Lantvit, Melissa A. Korkmaz, Andrew C. Huntsman, Denisse Herrera, and Alexandria N. Young

Abstract

SF1: Synthesis & characterization of PHYs, SF2: Purity of PHYs, SF3: PHY34 cytotoxicity in various cancer types, SF4: Additional in vivo data, SF5: PHY25 & 30 cytotoxicity time course.

Published

2023

14. Data from Phyllanthusmin Derivatives Induce Apoptosis and Reduce Tumor Burden in High-Grade Serous Ovarian Cancer by Late-Stage Autophagy Inhibition

Author

Joanna E. Burdette, James R. Fuchs, Leslie N. Aldrich, Mitch A. Phelps, Xiaoli Zhang, A. Douglas Kinghorn, Steven M. Swanson, Hongyan Wang, Salane King, Christopher C. Coss, Shamalatha Kolli, Sarmistha Mazumder, Daniel D. Lantvit, Melissa A. Korkmaz, Andrew C. Huntsman, Denisse Herrera, and Alexandria N. Young

Abstract

High-grade serous ovarian cancer (HGSOC) is a lethal gynecological malignancy with a need for new therapeutics. Many of the most widely used chemotherapeutic drugs are derived from natural products or their semi-synthetic derivatives. We have developed potent synthetic analogues of a class of compounds known as phyllanthusmins, inspired by natural products isolated from Phyllanthus poilanei Beille. The most potent analogue, PHY34, had the highest potency in HGSOC cell lines in vitro and displayed cytotoxic activity through activation of apoptosis. PHY34 exerts its cytotoxic effects by inhibiting autophagy at a late stage in the pathway, involving the disruption of lysosomal function. The autophagy activator, rapamycin, combined with PHY34 eliminated apoptosis, suggesting that autophagy inhibition may be required for apoptosis. PHY34 was readily bioavailable through intraperitoneal administration in vivo where it significantly inhibited the growth of cancer cell lines in hollow fibers, as well as reduced tumor burden in a xenograft model. We demonstrate that PHY34 acts as a late-stage autophagy inhibitor with nanomolar potency and significant antitumor efficacy as a single agent against HGSOC in vivo. This class of compounds holds promise as a potential, novel chemotherapeutic and demonstrates the effectiveness of targeting the autophagic pathway as a viable strategy for combating ovarian cancer. Mol Cancer Ther; 17(10); 2123–35. ©2018 AACR.

Published

2023

15. Supplementary Figure 2 from Pancreatic Cancer-Associated Stellate Cells Promote Differentiation of Myeloid-Derived Suppressor Cells in a STAT3-Dependent Manner

Author

Gregory B. Lesinski, Mark Bloomston, Tanios Bekaii-Saab, Wendy L. Frankel, Tim D. Eubank, James R. Fuchs, Gregory S. Young, Markus Mair, Sylwia Wojcik, Amy Collins, Zeenath Ameen, and Thomas A. Mace

Abstract

PDF file - 1835K, Supplementary Figure S2. PSC supernatants do not signal through STAT1 and STAT5.

Published

2023

16. Supplementary Figure 1 from Pancreatic Cancer-Associated Stellate Cells Promote Differentiation of Myeloid-Derived Suppressor Cells in a STAT3-Dependent Manner

Author

Gregory B. Lesinski, Mark Bloomston, Tanios Bekaii-Saab, Wendy L. Frankel, Tim D. Eubank, James R. Fuchs, Gregory S. Young, Markus Mair, Sylwia Wojcik, Amy Collins, Zeenath Ameen, and Thomas A. Mace

Abstract

PDF file - 793K, Supplementary Figure S1. PSC secrete variable or undetectable levels of PGE2.

Published

2023

17. Supplementary Figure Legend from Pancreatic Cancer-Associated Stellate Cells Promote Differentiation of Myeloid-Derived Suppressor Cells in a STAT3-Dependent Manner

Author

Gregory B. Lesinski, Mark Bloomston, Tanios Bekaii-Saab, Wendy L. Frankel, Tim D. Eubank, James R. Fuchs, Gregory S. Young, Markus Mair, Sylwia Wojcik, Amy Collins, Zeenath Ameen, and Thomas A. Mace

Abstract

PDF file - 55K

Published

2023

18. Discovery of Anticancer Agents of Diverse Natural Origin

Author

Leslie N. Aldrich, Joanna E. Burdette, Esperanza Carcache de Blanco, Christopher C. Coss, Alessandra S. Eustaquio, James R. Fuchs, A. Douglas Kinghorn, Amanda MacFarlane, Brittney K. Mize, Nicholas H. Oberlies, Jimmy Orjala, Cedric J. Pearce, Mitch A. Phelps, Liva Harinantenaina Rakotondraibe, Yulin Ren, Djaja Doel Soejarto, Brent R. Stockwell, Jack C. Yalowich, and Xiaoli Zhang

Subjects

Pharmacology, Biological Products, Organic Chemistry, Pharmaceutical Science, Antineoplastic Agents, Plants, Article, Analytical Chemistry, Structure-Activity Relationship, Complementary and alternative medicine, Neoplasms, Drug Discovery, Molecular Medicine, Humans

Abstract

Research progress from mainly over the last five years is described for a multidisciplinary collaborative program project directed toward the discovery of potential anticancer agents from a broad range of taxonomically defined organisms. Selected lead compounds with potential as new antitumor agents that are representative of considerable structural diversity have continued to be obtained from each of tropical plants, terrestrial and aquatic cyanobacteria, and filamentous fungi. Recently, a new focus has been on the investigation of the constituents of U.S. lichens and their fungal mycobionts. A medicinal chemistry and pharmacokinetics component of the project has optimized structurally selected lead natural products, leading to enhanced cytotoxic potencies against selected cancer cell lines. Biological testing has shown several compounds to have in vivo activity, and relevant preliminary structure-activity relationship and mechanism of action studies have been performed. Several promising lead compounds worthy of further investigation have been identified from the most recent collaborative work performed.

Published

2023

19. Bifunctional degraders of cyclin dependent kinase 9 (CDK9): Probing the relationship between linker length, properties, and selective protein degradation

Author

Robert J. Tokarski, Chia M. Sharpe, Andrew C. Huntsman, Brittney K. Mize, Oluwatosin R. Ayinde, Emily H. Stahl, James R. Lerma, Andrew Reed, Bridget Carmichael, Natarajan Muthusamy, John C. Byrd, and James R. Fuchs

Subjects

Pharmacology, Organic Chemistry, Drug Discovery, General Medicine

Published

2023

20. Pentalinonsterol, a Phytosterol from Pentalinon andrieuxii, is Immunomodulatory through Phospholipase A2 in Macrophages toward its Antileishmanial Action

Author

Gaurav Gupta, Sanjay Varikuti, Thomas J. Hund, Abhay R. Satoskar, Sainath R. Kotha, Andrew B. Shelton, Travis O. Gurney, Narasimham L. Parinandi, Nidhi Srivastava, A. Douglas Kinghorn, and James R. Fuchs

Subjects

biology, Chemistry, medicine.medical_treatment, Biophysics, Cell Biology, General Medicine, Pharmacology, Leishmania, biology.organism_classification, Biochemistry, In vitro, Proinflammatory cytokine, chemistry.chemical_compound, Cytokine, Phospholipase A2, In vivo, medicine, biology.protein, Macrophage, Arachidonic acid

Abstract

Our earlier in vitro and in vivo studies have revealed that the phytosterol, pentalinonsterol (cholest-4,20,24-trien-3-one) (PEN), isolated from the roots of Pentalinon andrieuxii, possesss immunomodulatory properties in macrophages and dendritic cells. Leishmaniasis, caused by the infection of Leishmania spp. (a protozoan parasite), is emerging as the second-leading cause of mortality among the tropical diseases and there is an unmet need for a pharmacological intervention of leishmaniasis. Given the beneficial immunomodulatory actions and lipophilic properties of PEN, the objective of this study was to elucidate the mechanism(s) of action of the immunomodulatory action(s) of PEN in macrophages through the modulation of phospholipase A2 (PLA2) activity that might be crucial in the antileishmanial action of PEN. Therefore, in this study, we investigated whether PEN would modulate the activity of PLA2 in RAW 264.7 macrophages and mouse bone marrow-derived primary macrophages (BMDMs) in vitro and further determined how the upstream PLA2 activation would regulate the downstream cytokine release in the macrophages. Our current results demonstrated that (i) PEN induced PLA2 activation (arachidonic acid release) in a dose- and time-dependent manner that was regulated upstream by the mitogen-activated protein kinases (MAPKs); (ii) the PEN-induced activation of PLA2 was attenuated by the cPLA2-specific pharmacological inhibitors; and (iii) the cPLA2-specific pharmacological inhibitors attenuated the release of inflammatory cytokines from the macrophages. For the first time, our current study demonstrated that PEN exhibited its immunomodulatory actions through the activation of cPLA2 in the macrophages, which potentially could be used in the development of a pharmacological intervention against leishmaniasis.

Published

2021

21. Semisynthetic Derivatives of the Verticillin Class of Natural Products through Acylation of the C11 Hydroxy Group

Author

Cedric J. Pearce, Nicholas H. Oberlies, Joanna E. Burdette, Michael G Doyle, James R. Fuchs, Andrew C. Huntsman, and Chiraz Soumia M. Amrine

Subjects

Carbamate, 010405 organic chemistry, Stereochemistry, Chemistry, medicine.medical_treatment, Organic Chemistry, Prodrug, 01 natural sciences, Biochemistry, In vitro, 0104 chemical sciences, Acylation, 010404 medicinal & biomolecular chemistry, chemistry.chemical_compound, Sulfonate, In vivo, Drug Discovery, medicine, Reactivity (chemistry), Fermentation

Abstract

[Image: see text] The verticillins, a class of epipolythiodioxopiperazine alkaloids (ETPs) first described 50 years ago with the discovery of verticillin A (1), have gained attention due to their potent activity against cancer cells, noted both in vitro and in vivo. In this study, the complex scaffold afforded through optimized fermentation was used as a feedstock for semisynthetic efforts designed to explore the reactivity of the C11 and C11′ hydroxy substituents. Functionality introduced at these positions would be expected to impact not only the potency but also the pharmacokinetic properties of the resulting compound. With this in mind, verticillin H (2) was used as a starting material to generate nine semisynthetic analogues (4–12) containing a variety of ester, carbonate, carbamate, and sulfonate moieties. Likewise, verticillin A succinate (13) was synthesized from 1 to demonstrate the successful application of this strategy to other ETPs. The synthesized compounds and their corresponding starting materials (i.e., 1 and 2) were screened for activity against a panel of melanoma, breast, and ovarian cancer cell lines: MDA-MB-435, MDA-MB-231, and OVCAR3. All analogues retained IC(50) values in the nanomolar range, comparable to, and in some cases more potent than, the parent compounds.

Published

2021

22. Structural and mechanistic bases for a potent HIV-1 capsid inhibitor

Author

Patrick R. Griffin, Nikoloz Shkriabai, Valentine V. Courouble, Arun S. Annamalai, Daniel Adu-Ampratwum, Parmit K. Singh, Ashwanth C. Francis, Naseer Iqbal, Guochao Wei, Peter Van Blerkom, James H. Morrison, Mamuka Kvaratskhelia, Eric M. Poeschla, Francisco J. Asturias, Gregory B. Melikyan, Alan Engelman, Haiyan Zhao, James R. Fuchs, and S.M. Bester

Subjects

Anti-HIV Agents, viruses, Protein domain, Human immunodeficiency virus (HIV), Crystallography, X-Ray, medicine.disease_cause, Article, Cofactor, 03 medical and health sciences, Capsid, Protein Domains, medicine, Humans, 030304 developmental biology, mRNA Cleavage and Polyadenylation Factors, 0303 health sciences, Multidisciplinary, biology, 030306 microbiology, Chemistry, Cryoelectron Microscopy, HEK 293 cells, Deuterium Exchange Measurement, Antiretroviral therapy, Cell biology, Chromatin, Nuclear Pore Complex Proteins, HEK293 Cells, HIV-1, biology.protein, Nuclear transport, HeLa Cells

Abstract

The potent HIV-1 capsid inhibitor GS-6207 is an investigational principal component of long-acting antiretroviral therapy. We found that GS-6207 inhibits HIV-1 by stabilizing and thereby preventing functional disassembly of the capsid shell in infected cells. X-ray crystallography, cryo–electron microscopy, and hydrogen-deuterium exchange experiments revealed that GS-6207 tightly binds two adjoining capsid subunits and promotes distal intra- and inter-hexamer interactions that stabilize the curved capsid lattice. In addition, GS-6207 interferes with capsid binding to the cellular HIV-1 cofactors Nup153 and CPSF6 that mediate viral nuclear import and direct integration into gene-rich regions of chromatin. These findings elucidate structural insights into the multimodal, potent antiviral activity of GS-6207 and provide a means for rationally developing second-generation therapies.

Published

2020

23. 15N Stable Isotope Labeling and Comparative Metabolomics Facilitates Genome Mining in Cultured Cyanobacteria

Author

James R. Fuchs, Daniel S. May, Aleksej Krunic, Tyler A. Wilson, Camila M. Crnkovic, and Jimmy Orjala

Subjects

0301 basic medicine, Cyanobacteria, Nostoc, biology, 010405 organic chemistry, Chemistry, BACTÉRIAS, General Medicine, Secondary metabolite, biology.organism_classification, ENCODE, Mass spectrometry, 01 natural sciences, Biochemistry, Genome, Article, 0104 chemical sciences, 03 medical and health sciences, 030104 developmental biology, Metabolomics, medicine, Molecular Medicine, Gene, medicine.drug

Abstract

As genome mining becomes a more widely used approach to identify bacterial natural products, the challenge of matching biosynthetic gene clusters to their cognate secondary metabolites has become more apparent. Bioinformatic platforms such as AntiSMASH have made great progress in predicting chemical structures from genetic information, however the predicted structures are often incomplete. This complicates identifying the predicted compounds by mass spectrometry. Secondary metabolites produced by cyanobacteria represent a unique opportunity for bridging this gap. Cultured cyanobacteria incorporate inorganic nitrogen provided in chemically defined media into all nitrogen-containing secondary metabolites. Thus, stable isotope labeling with (15)N labeled nitrate and subsequent comparative metabolomics can be used to match biosynthetic gene clusters to their cognate compounds in cell extracts. Analysis of the sequenced genome of Nostoc sp. UIC 10630 identified six biosynthetic gene clusters predicted to encode the production of a secondary metabolite with at least one nitrogen atom. Comparative metabolomic analysis of the (15)N labeled and unlabeled cell extracts revealed four nitrogen containing compounds that contained the same number of nitrogen atoms as were predicted in the biosynthetic gene clusters. Two of the four compounds were new secondary metabolites, and their structures were elucidated by NMR, HRESIMS, and MS/MS.

Published

2020

24. Evaluation of synergy between host and pathogen-directed therapies against intracellular Leishmania donovani

Author

Eric M. Bachelder, Abhay R. Satoskar, Robert J. Tokarski, Kristy M. Ainslie, James R. Fuchs, M. Shamim Hasan Zahid, and Monica M. Johnson

Subjects

0301 basic medicine, Paromomycin, Pharmacology, Mice, chemistry.chemical_compound, 0302 clinical medicine, Pharmacology (medical), Visceral leishmaniasis, Mice, Inbred BALB C, Sulfonamides, Drug Synergism, DNER-4, 3. Good health, Infectious Diseases, Synergy, Leishmaniasis, Visceral, Drug Therapy, Combination, Intracellular, medicine.drug, Combinatorial therapy, Phosphorylcholine, 030231 tropical medicine, Antiprotozoal Agents, Leishmania donovani, Biology, Article, Host-directed therapy, Host-Parasite Interactions, lcsh:Infectious and parasitic diseases, 03 medical and health sciences, Amphotericin B, parasitic diseases, medicine, Animals, Humans, lcsh:RC109-216, Amastigote, Life Cycle Stages, Miltefosine, Resazurin, medicine.disease, biology.organism_classification, 030104 developmental biology, chemistry, Resazurin assay, Pyrazoles, Parasitology, AR-12

Abstract

Visceral leishmaniasis (VL) is associated with treatment complications due to the continued growth of resistant parasites toward currently available pathogen-directed therapeutics. To limit the emergence and combat resistant parasites there is a need to develop new anti-leishmanial drugs and alternative treatment approaches, such as host-directed therapeutics (HDTs). Discovery of new anti-leishmanial drugs including HDTs requires suitable in vitro assay systems. Herein, we modified and evaluated a series of resazurin assays against different life-stages of the VL causing parasite, Leishmania donovani to identify novel HDTs. We further analyzed the synergy of combinatorial interactions between traditionally used pathogen-directed drugs and HDTs for clearance of intracellular L. donovani. The inhibitory concentration at 50% (IC50) of the five evaluated therapies [amphotericin B (AMB), miltefosine, paromomycin, DNER-4, and AR-12 (OSU-03012)] was determined against promastigotes, extracellular amastigotes, and intracellular amastigotes of L. donovani via a resazurin-based assay and compared to image-based microscopy. Using the resazurin-based assay, all evaluated therapies showed reproducible anti-leishmanial activity against the parasite's different life-stages. These results were consistent to the traditional image-based technique. The gold standard of therapy, AMB, showed the highest potency against intracellular L. donovani, and was further evaluated for combinatorial effects with the HDTs. Among the combinations analyzed, pathogen-directed AMB and host-directed AR-12 showed a synergistic reduction of intracellular L. donovani compared to individual treatments. The modified resazurin assay used in this study demonstrated a useful technique to measure new anti-leishmanial drugs against both intracellular and extracellular parasites. The synergistic interactions between pathogen-directed AMB and host-directed AR-12 showed a great promise to combat VL, with the potential to reduce the emergence of drug-resistant strains., Graphical abstract Image 1, Highlights • An inexpensive and simple modified resazurin drug screening assay for Leishmania donovani. • Anti-leishmanial therapies are evaluated in axenic amastigotes, promastigotes, and intracellular Leishmania donovani. • Identification of synergistic, additive, and antagonistic activity between therapies. • Amphotericin B and host-directed AR-12 had significant synergistic anti-leishmanial activity.

Published

2019

25. Novel narrow spectrum benzyl thiophene sulfonamide derivatives to control Campylobacter

Author

Loic Deblais, Dipak Kathayat, James R. Fuchs, Ulyana Muñoz Acuña, Janet Antwi, Yosra A. Helmy, Huang-Chi Huang, Esperanza J. Carcache de Blanco, Anand Kumar, and Gireesh Rajashekara

Subjects

0301 basic medicine, Colon, 030106 microbiology, Campylobacteriosis, Campylobacter coli, Microbial Sensitivity Tests, Thiophenes, Drug resistance, medicine.disease_cause, 01 natural sciences, Campylobacter jejuni, Cell Line, Microbiology, Foodborne Diseases, 03 medical and health sciences, Minimum inhibitory concentration, Campylobacter Infections, Drug Resistance, Bacterial, Drug Discovery, medicine, Animals, Humans, Cecum, Pharmacology, Sulfonamides, Bacteria, biology, 010405 organic chemistry, Chemistry, Campylobacter, Sulfonamide (medicine), Antimicrobial, biology.organism_classification, medicine.disease, Anti-Bacterial Agents, 0104 chemical sciences, Chickens, medicine.drug

Abstract

Campylobacter is a leading cause of bacterial foodborne gastroenteritis worldwide, and poultry are a major source of human campylobacteriosis. The control of Campylobacter from farm to fork is challenging due to emergence of microbial resistance and lack of effective control methods. We identified a benzyl thiophene sulfonamide based small molecule (compound 1) with a minimal inhibitory concentration (MIC) of 100 μM against Campylobacter jejuni 81–176 and Campylobacter coli ATCC33559, good drug-like properties, and low toxicity on eukaryotic cells. Compound 1 was used as a lead for the preparation of 13 analogues. Two analogues, compounds 4 and 8 (TH-4 and TH-8), were identified with better antimicrobial properties than compound 1. TH-4 and TH-8 had a MIC of 12.5 μM and 25 μM for C. coli and 50 μM and 100 μM for C. jejuni, respectively. Cytological studies revealed that both compounds affected C. jejuni envelope integrity. Further, both compounds had no effect on other foodborne pathogens. TH-4 and TH-8 had a minimal impact on the chicken cecal microbiota and were not toxic to colon epithelial cells and chicken macrophages, and red blood cells at 200 µM. Further, TH-4 and TH-8 reduced the Campylobacter load in chicken ceca (up to 2-log reduction) when infected chickens were orally treated for 5 days with 0.254 mg kg−1; as well as against internalized Campylobacter in Caco-2 cells at 12.5 µM and higher. Our study identified two novel specific and safe benzyl thiophene sulfonamide derivatives having potential for control of Campylobacter in chickens and humans.

Published

2019

26. Potential Anticancer Agents Characterized from Selected Tropical Plants

Author

Steven M. Swanson, Yulin Ren, Joanna E. Burdette, Djaja D. Soejarto, Esperanza J. Carcache de Blanco, James R. Fuchs, and A. Douglas Kinghorn

Subjects

Pharmaceutical Science, Computational biology, Biology, 01 natural sciences, Article, Analytical Chemistry, Structure-Activity Relationship, chemistry.chemical_compound, Drug Discovery, Xanthone, Tropical plants, Pharmacology, Lignan, chemistry.chemical_classification, Tropical Climate, Molecular Structure, 010405 organic chemistry, Extramural, Organic Chemistry, Biflavonoid, Plants, Antineoplastic Agents, Phytogenic, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Complementary and alternative medicine, chemistry, Cancer cell, Molecular Medicine

Abstract

Higher plants are well known for their value in affording clinically useful anticancer agents, with such compounds acting against cancer cells by a range of mechanisms of action. There remains a strong interest in the discovery and development of plant secondary metabolites as additional cancer chemotherapeutic lead compounds. In the present review, progress on the discovery of plant-derived compounds of the biflavonoid, lignan, sesquiterpene, steroid, and xanthone structural types is presented. Several potential anticancer leads of these types have been characterized from tropical plants collected in three countries as part of our ongoing collaborative multi-institutional project. Preliminary structure-activity relationships and work on in vivo testing and cellular mechanisms of action are also discussed. In addition, the relevant work reported by other groups on the same compound classes is included herein.

Published

2019

27. Novel small molecule IL-6 inhibitor suppresses autoreactive Th17 development and promotes Treg development

Author

Emma E. Kraus, Nivedita Jena, Chenglong Li, Marissa C. Granitto, Marissa F. Farinas, Amy E. Lovett-Racke, E Y Zhao, Wei Pei, G Perottino, James R. Fuchs, Michael K. Racke, S I Aqel, V Kumari, Yuhong Yang, and L Mao

Subjects

0301 basic medicine, Adoptive cell transfer, biology, Chemistry, Effector, Immunology, Experimental autoimmune encephalomyelitis, Interleukin, medicine.disease, In vitro, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, STAT protein, biology.protein, Cancer research, medicine, Immunology and Allergy, Signal transduction, Interleukin 6, 030215 immunology

Abstract

Summary Multiple sclerosis (MS) is the leading cause of non-traumatic neurological disability in the United States in young adults, but current treatments are only partially effective, making it necessary to develop new, innovative therapeutic strategies. Myelin-specific interleukin (IL)-17-producing T helper type 17 (Th17) cells are a major subset of CD4 T effector cells (Teff) that play a critical role in mediating the development and progression of MS and its mouse model, experimental autoimmune encephalomyelitis (EAE), while regulatory T cells (Treg) CD4 T cells are beneficial for suppressing disease. The IL-6/signal transducer and activator of transcription 3 (STAT-3) signaling pathway is a key regulator of Th17 and Treg cells by promoting Th17 development and suppressing Treg development. Here we show that three novel small molecule IL-6 inhibitors, madindoline-5 (MDL-5), MDL-16 and MDL-101, significantly suppress IL-17 production in myelin-specific CD4 T cells in a dose-dependent manner in vitro. MDL-101 showed superior potency in suppressing IL-17 production compared to MDL-5 and MDL-16. Treatment of myelin-specific CD4 T cells with MDL-101 in vitro reduced their encephalitogenic potential following their subsequent adoptive transfer. Furthermore, MDL-101 significantly suppressed proliferation and IL-17 production of anti-CD3-activated effector/memory CD45RO+CD4+ human CD4 T cells and promoted human Treg development. Together, these data demonstrate that these novel small molecule IL-6 inhibitors have the potential to shift the Teff : Treg balance, which may provide a novel therapeutic strategy for ameliorating disease progression in MS.

Published

2019

28. Pentalinonsterol, a Phytosterol from Pentalinon andrieuxii, is Immunomodulatory through Phospholipase A

Author

Sanjay, Varikuti, Andrew B, Shelton, Sainath R, Kotha, Travis, Gurney, Gaurav, Gupta, Thomas J, Hund, James R, Fuchs, A Douglas, Kinghorn, Nidhi, Srivastava, Abhay R, Satoskar, and Narasimham L, Parinandi

Subjects

Mice, Phospholipases A2, Sterols, Macrophages, Animals, Phytosterols

Abstract

Our earlier in vitro and in vivo studies have revealed that the phytosterol, pentalinonsterol (cholest-4,20,24-trien-3-one) (PEN), isolated from the roots of Pentalinon andrieuxii, possesss immunomodulatory properties in macrophages and dendritic cells. Leishmaniasis, caused by the infection of Leishmania spp. (a protozoan parasite), is emerging as the second-leading cause of mortality among the tropical diseases and there is an unmet need for a pharmacological intervention of leishmaniasis. Given the beneficial immunomodulatory actions and lipophilic properties of PEN, the objective of this study was to elucidate the mechanism(s) of action of the immunomodulatory action(s) of PEN in macrophages through the modulation of phospholipase A

Published

2021

29. Phyllanthusmin Derivatives Induce Apoptosis and Reduce Tumor Burden in High-Grade Serous Ovarian Cancer by Late-Stage Autophagy Inhibition

Author

Shamalatha Kolli, Denisse Herrera, Salane King, James R. Fuchs, Leslie N. Aldrich, A. Douglas Kinghorn, Daniel D. Lantvit, Christopher C. Coss, Xiaoli Zhang, Joanna E. Burdette, Mitch A. Phelps, Melissa A. Korkmaz, Alexandria N. Young, Sarmistha Mazumder, Steven M. Swanson, Hongyan Wang, and Andrew C. Huntsman

Subjects

0301 basic medicine, Cancer Research, Cell Survival, Apoptosis, Article, 03 medical and health sciences, Ovarian tumor, 0302 clinical medicine, In vivo, Cell Line, Tumor, Autophagy, medicine, Animals, Humans, Cytotoxic T cell, Neoplasm Staging, Ovarian Neoplasms, Dose-Response Relationship, Drug, Chemistry, medicine.disease, Antineoplastic Agents, Phytogenic, Xenograft Model Antitumor Assays, In vitro, Cystadenocarcinoma, Serous, Tumor Burden, Disease Models, Animal, 030104 developmental biology, Oncology, Cell culture, 030220 oncology & carcinogenesis, Cancer research, Female, Neoplasm Grading, Lysosomes, Ovarian cancer

Abstract

High-grade serous ovarian cancer (HGSOC) is a lethal gynecological malignancy with a need for new therapeutics. Many of the most widely used chemotherapeutic drugs are derived from natural products or their semi-synthetic derivatives. We have developed potent synthetic analogues of a class of compounds known as phyllanthusmins, inspired by natural products isolated from Phyllanthus poilanei Beille. The most potent analogue, PHY34, had the highest potency in HGSOC cell lines in vitro and displayed cytotoxic activity through activation of apoptosis. PHY34 exerts its cytotoxic effects by inhibiting autophagy at a late stage in the pathway, involving the disruption of lysosomal function. The autophagy activator, rapamycin, combined with PHY34 eliminated apoptosis, suggesting that autophagy inhibition may be required for apoptosis. PHY34 was readily bioavailable through intraperitoneal administration in vivo where it significantly inhibited the growth of cancer cell lines in hollow fibers, as well as reduced tumor burden in a xenograft model. We demonstrate that PHY34 acts as a late-stage autophagy inhibitor with nanomolar potency and significant antitumor efficacy as a single agent against HGSOC in vivo. This class of compounds holds promise as a potential, novel chemotherapeutic and demonstrates the effectiveness of targeting the autophagic pathway as a viable strategy for combating ovarian cancer. Mol Cancer Ther; 17(10); 2123–35. ©2018 AACR.

Published

2018

30. Calothrixamides A and B from the Cultured Cyanobacterium Calothrix sp. UIC 10520

Author

Diana Kao, Nicholas H. Oberlies, James R. Fuchs, Joanna E. Burdette, Daniel S. May, Tyler A. Wilson, Aleksej Krunic, Jimmy Orjala, and Camila M. Crnkovic

Subjects

Cyanobacteria, Magnetic Resonance Spectroscopy, Pharmaceutical Science, Mass spectrometry, 01 natural sciences, Article, Analytical Chemistry, chemistry.chemical_compound, Cell Line, Tumor, Drug Discovery, Humans, Derivatization, Chemical decomposition, Pharmacology, chemistry.chemical_classification, Chromatography, Natural product, biology, 010405 organic chemistry, Chemistry, Fatty Acids, Organic Chemistry, Fatty acid, Nuclear magnetic resonance spectroscopy, biology.organism_classification, Amides, 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, Complementary and alternative medicine, Molecular Medicine, Water Microbiology, Two-dimensional nuclear magnetic resonance spectroscopy

Abstract

Cyanobacteria are a source of chemically diverse metabolites with potential medicinal and biotechnological applications. Rapid identification of compounds is central to expedite the natural product discovery process. Mass spectrometry has been shown to be an important tool for dereplication of complex natural product samples. In addition, chromatographic separation and complementary spectroscopic analysis (e.g., UV) can enhance the confidence of the dereplication process. Here, we applied a droplet-liquid microjunction-surface sampling probe (droplet probe) coupled with UPLC-PDA-HRMS-MS/ MS to identify two new natural products in situ from the freshwater strain Calothrix sp. UIC 10520. This allowed us to prioritize this strain for chemical investigation based on the presence of new metabolites very early in our discovery process, saving both time and resources. Subsequently, calothrixamides A (1) and B (2) were isolated from large-scale cultures, and the structures were elucidated by 1D and 2D NMR spectroscopy and mass spectrometry. The absolute configurations were determined by a combination of chemical degradation reactions, derivatization methods (Mosher’s, Marfey’s, and phenylglycine methyl ester), and J-based configurational analysis. Calothrixamides showed no cytotoxic activity against the MDA-MB-435, MDA-MB-231, and OVCAR3 cancer cell lines. They represent the first functionalized long-chain fatty acid amides reported from the Calothrix genus and from a freshwater cyanobacterium.

Published

2018

31. Resistance to pyridine-based inhibitor KF116 reveals an unexpected role of integrase in HIV-1 Gag-Pol polyprotein proteolytic processing

Author

Alan Engelman, James R. Fuchs, Pratibha C. Koneru, Ross C. Larue, Matthew J. Kobe, Augusta Jamin, Mamuka Kvaratskhelia, and Ashley C. Hoyte

Subjects

0301 basic medicine, Polyproteins, Pyridines, viruses, Dimer, Allosteric regulation, Morphogenesis, Gene Products, gag, Gene Products, pol, HIV Integrase, Protein aggregation, Crystallography, X-Ray, Microbiology, Biochemistry, Subclass, 03 medical and health sciences, chemistry.chemical_compound, Drug Resistance, Viral, Humans, HIV Integrase Inhibitors, Molecular Biology, biology, Chemistry, Cell Biology, Surface Plasmon Resonance, Integrase, HEK293 Cells, 030104 developmental biology, Viral replication, Proteolysis, HIV-1, biology.protein

Abstract

The pyridine-based multimerization selective HIV-1 integrase (IN) inhibitors (MINIs) are a distinct subclass of allosteric IN inhibitors. MINIs potently inhibit HIV-1 replication during virion maturation by inducing hyper- or aberrant IN multimerization but are largely ineffective during the early steps of viral replication. Here, we investigated the mechanism for the evolution of a triple IN substitution (T124N/V165I/T174I) that emerges in cell culture with a representative MINI, KF116. We show that HIV-1 NL4-3(IN T124N/V165I/T174I) confers marked (>2000-fold) resistance to KF116. Two IN substitutions (T124N/T174I) directly weaken inhibitor binding at the dimer interface of the catalytic core domain but at the same time markedly impair HIV-1 replication capacity. Unexpectedly, T124N/T174I IN substitutions inhibited proteolytic processing of HIV-1 polyproteins Gag and Gag-Pol, resulting in immature virions. Strikingly, the addition of the third IN substitution (V165I) restored polyprotein processing, virus particle maturation, and significant levels of replication capacity. These results reveal an unanticipated role of IN for polyprotein proteolytic processing during virion morphogenesis. The complex evolutionary pathway for the emergence of resistant viruses, which includes the need for the compensatory V165I IN substitution, highlights a relatively high genetic barrier exerted by MINI KF116. Additionally, we have solved the X-ray structure of the drug-resistant catalytic core domain protein, which provides means for rational development of second-generation MINIs.

Published

2017

32. Corrigendum to 'FLLL12 induces apoptosis in lung cancer cells through a p53/p73-independent but death receptor 5-dependent pathway' [Canc. Lett. 363 (2015) 166–175]

Author

A.R.M. Ruhul Amin, Dong M. Shin, Zhuo (Georgia) Chen, Abedul Haque, James R. Fuchs, Mohammad Aminur Rahman, and Fadlo R. Khuri

Subjects

Cancer Research, Text mining, Oncology, Apoptosis, business.industry, TNFRSF10B, Cancer research, medicine, business, Lung cancer, medicine.disease

Published

2021

33. STarFish: A Stacked Ensemble Target Fishing Approach and its Application to Natural Products

Author

Nicholas T. Cockroft, James R. Fuchs, and Xiaolin Cheng

Subjects

Databases, Factual, Computer science, General Chemical Engineering, Library and Information Sciences, computer.software_genre, 01 natural sciences, Synthetic data, Article, Set (abstract data type), Machine Learning, 0103 physical sciences, Drug Discovery, Humans, Biological Products, 010304 chemical physics, Artificial neural network, Proteins, General Chemistry, chEMBL, 0104 chemical sciences, Computer Science Applications, Random forest, Data set, 010404 medicinal & biomolecular chemistry, Identification (information), Logistic Models, ROC Curve, Multilayer perceptron, Data mining, Neural Networks, Computer, computer

Abstract

Target fishing is the process of identifying the protein target of a bioactive small molecule. To do so experimentally requires a significant investment of time and resources, which can be expedited with a reliable computational target fishing model. The development of computational target fishing models using machine learning has become very popular over the last several years because of the increased availability of large amounts of public bioactivity data. Unfortunately, the applicability and performance of such models for natural products has not yet been comprehensively assessed. This is, in part, due to the relative lack of bioactivity data available for natural products compared to synthetic compounds. Moreover, the databases commonly used to train such models do not annotate which compounds are natural products, which makes the collection of a benchmarking set difficult. To address this knowledge gap, a data set composed of natural product structures and their associated protein targets was generated by cross-referencing 20 publicly available natural product databases with the bioactivity database ChEMBL. This data set contains 5589 compound-target pairs for 1943 unique compounds and 1023 unique targets. A synthetic data set comprising 107 190 compound-target pairs for 88 728 unique compounds and 1907 unique targets was used to train k-nearest neighbors, random forest, and multilayer perceptron models. The predictive performance of each model was assessed by stratified 10-fold cross-validation and benchmarking on the newly collected natural product data set. Strong performance was observed for each model during cross-validation with area under the receiver operating characteristic (AUROC) scores ranging from 0.94 to 0.99 and Boltzmann-enhanced discrimination of receiver operating characteristic (BEDROC) scores from 0.89 to 0.94. When tested on the natural product data set, performance dramatically decreased with AUROC scores ranging from 0.70 to 0.85 and BEDROC scores from 0.43 to 0.59. However, the implementation of a model stacking approach, which uses logistic regression as a meta-classifier to combine model predictions, dramatically improved the ability to correctly predict the protein targets of natural products and increased the AUROC score to 0.94 and BEDROC score to 0.73. This stacked model was deployed as a web application, called STarFish, and has been made available for use to aid in target identification for natural products.

Published

2019

34. Author response: HIV-1 integrase tetramers are the antiviral target of pyridine-based allosteric integrase inhibitors

Author

Stephanie V Rebensburg, Ronald M. Levy, Gregory B. Melikyan, Daniel Adu-Ampratwum, Ashley C. Hoyte, Alan Engelman, Mamuka Kvaratskhelia, Ross C. Larue, Michael F. Wempe, Dmitry Lyumkis, Nanjie Deng, Ashwanth C. Francis, Jared J. Lindenberger, Pratibha C. Koneru, and James R. Fuchs

Subjects

chemistry.chemical_compound, chemistry, Pyridine, Allosteric regulation, Hiv 1 integrase, Integrase inhibitor, Virology

Published

2019

35. HIV-1 integrase tetramers are the antiviral target of pyridine-based allosteric integrase inhibitors

Author

Nanjie Deng, Daniel Adu-Ampratwum, Mamuka Kvaratskhelia, Jared J. Lindenberger, Pratibha C. Koneru, Ross C. Larue, Gregory B. Melikyan, Alan Engelman, James R. Fuchs, Dmitry Lyumkis, Ashley C. Hoyte, Ashwanth C. Francis, Ronald M. Levy, Stephanie V Rebensburg, and Michael F. Wempe

Subjects

0301 basic medicine, Models, Molecular, QH301-705.5, Pyridines, Science, viruses, 030106 microbiology, Allosteric regulation, Integrase inhibitor, HIV Integrase, Antiviral Agents, General Biochemistry, Genetics and Molecular Biology, Virus, 03 medical and health sciences, chemistry.chemical_compound, Allosteric Regulation, Protein Domains, Humans, HIV Integrase Inhibitors, Biology (General), Microbiology and Infectious Disease, General Immunology and Microbiology, biology, Chemistry, General Neuroscience, allosteric inhibitors, HEK 293 cells, Wild type, Stereoisomerism, General Medicine, Virology, 3. Good health, Integrase, 030104 developmental biology, HEK293 Cells, Capsid, Dolutegravir, biology.protein, HIV-1, Medicine, integrase, Protein Multimerization, Research Article, HeLa Cells

Abstract

Allosteric HIV-1 integrase (IN) inhibitors (ALLINIs) are a promising new class of antiretroviral agents that disrupt proper viral maturation by inducing hyper-multimerization of IN. Here we show that lead pyridine-based ALLINI KF116 exhibits striking selectivity for IN tetramers versus lower order protein oligomers. IN structural features that are essential for its functional tetramerization and HIV-1 replication are also critically important for KF116 mediated higher-order IN multimerization. Live cell imaging of single viral particles revealed that KF116 treatment during virion production compromises the tight association of IN with capsid cores during subsequent infection of target cells. We have synthesized the highly active (-)-KF116 enantiomer, which displayed EC50 of ~7 nM against wild type HIV-1 and ~10 fold higher, sub-nM activity against a clinically relevant dolutegravir resistant mutant virus suggesting potential clinical benefits for complementing dolutegravir therapy with pyridine-based ALLINIs., eLife digest HIV-1 inserts its genetic code into human genomes, turning healthy cells into virus factories. To do this, the virus uses an enzyme called integrase. Front-line treatments against HIV-1 called “integrase strand-transfer inhibitors” stop this enzyme from working. These inhibitors have helped to revolutionize the treatment of HIV/AIDS by protecting the cells from new infections. But, the emergence of drug resistance remains a serious problem. As the virus evolves, it changes the shape of its integrase protein, substantially reducing the effectiveness of the current therapies. One way to overcome this problem is to develop other therapies that can kill the drug resistant viruses by targeting different parts of the integrase protein. It should be much harder for the virus to evolve the right combination of changes to escape two or more treatments at once. A promising class of new compounds are “allosteric integrase inhibitors”. These chemical compounds target a part of the integrase enzyme that the other treatments do not yet reach. Rather than stopping the integrase enzyme from inserting the viral code into the human genome, the new inhibitors make integrase proteins clump together and prevent the formation of infectious viruses. At the moment, these compounds are still experimental. Before they are ready for use in people, researchers need to better understand how they work, and there are several open questions to answer. Integrase proteins work in groups of four and it is not clear how the new compounds make the integrases form large clumps, or what this does to the virus. Understanding this should allow scientists to develop improved versions of the drugs. To answer these questions, Koneru et al. first examined two of the new compounds. A combination of molecular analysis and computer modelling revealed how they work. The compounds link many separate groups of four integrases with each other to form larger and larger clumps, essentially a snowball effect. Live images of infected cells showed that the clumps of integrase get stuck outside of the virus’s protective casing. This leaves them exposed, allowing the cell to destroy the integrase enzymes. Koneru et al. also made a new compound, called (-)-KF116. Not only was this compound able to tackle normal HIV-1, it could block viruses resistant to the other type of integrase treatment. In fact, in laboratory tests, it was 10 times more powerful against these resistant viruses. Together, these findings help to explain how allosteric integrase inhibitors work, taking scientists a step closer to bringing them into the clinic. In the future, new versions of the compounds, like (-)-KF116, could help to tackle drug resistance in HIV-1.

Published

2019

36. An Isoquinoline Scaffold as a Novel Class of Allosteric HIV-1 Integrase Inhibitors

Author

Tyler A. Wilson, Pratibha C. Koneru, Stephanie V. Rebensburg, Jared J. Lindenberger, Matthew J. Kobe, Nicholas T. Cockroft, Daniel Adu-Ampratwum, Ross C. Larue, Mamuka Kvaratskhelia, and James R. Fuchs

Subjects

Organic Chemistry, Drug Discovery, Biochemistry

Abstract

[Image: see text] Allosteric HIV-1 integrase inhibitors (ALLINIs) are a new class of potential antiretroviral therapies with a unique mechanism of action and drug resistance profile. To further extend this class of inhibitors via a scaffold hopping approach, we have synthesized a series of analogues possessing an isoquinoline ring system. Lead compound 6l binds in the v-shaped pocket at the IN dimer interface and is highly selective for promoting higher-order multimerization of inactive IN over inhibiting IN-LEDGF/p75 binding. Importantly, 6l potently inhibited HIV-1(NL4–3) (A128T IN), which confers marked resistance to archetypal quinoline-based ALLINIs. Thermal degradation studies indicated that at elevated temperatures the acetic acid side chain of specific isoquinoline derivatives undergo decarboxylation reactions. This reactivity has implications for the synthesis of various ALLINI analogues.

Published

2018

37. Site-Selective C–H Functionalization of (Hetero)Arenes via Transient, Non-Symmetric Iodanes

Author

David A. Nagib, Andrew D. Chen, Chido M. Hambira, James R. Fuchs, and Stacy C. Fosu

Subjects

Chemistry, General Chemical Engineering, Biochemistry (medical), Non symmetric, 02 engineering and technology, General Chemistry, 010402 general chemistry, 021001 nanoscience & nanotechnology, 01 natural sciences, Biochemistry, Combinatorial chemistry, Article, 0104 chemical sciences, Materials Chemistry, Site selective, Environmental Chemistry, Surface modification, Reactivity (chemistry), 0210 nano-technology, Selectivity

Abstract

A strategy for C–H functionalization of arenes and heteroarenes has been developed to allow site-selective incorporation of various anions, including Cl, Br, OMs, OTs, and OTf. This approach is enabled by in situ generation of reactive, non-symmetric iodanes by combining anions and bench-stable PhI(OAc)(2). The utility of this mechanism is demonstrated via para-selective chlorination of medicinally relevant arenes, as well as site-selective C–H chlorination of heteroarenes. Spectroscopic, computational, and competition experiments describe the unique nature, reactivity, and selectivity of these transient, unsymmetrical iodanes.

Published

2018

38. Specialized metabolites of the United States lichen Niebla homalea and their antiproliferative activities

Author

Yan Zhang, Choon Yong Tan, Liva Harinantenaina Rakotondraibe, A. Douglas Kinghorn, James R. Fuchs, and Richard W. Spjut

Subjects

0106 biological sciences, Circular dichroism, Magnetic Resonance Spectroscopy, Lichens, Stereochemistry, Ethyl acetate, Plant Science, Horticulture, 01 natural sciences, Biochemistry, Niebla, Article, chemistry.chemical_compound, Ascomycota, Niebla homalea, Cell Line, Tumor, Humans, Lichen, Molecular Biology, Ovarian Neoplasms, biology, 010405 organic chemistry, Usnic acid, General Medicine, Nuclear magnetic resonance spectroscopy, biology.organism_classification, United States, 0104 chemical sciences, chemistry, Chemotaxonomy, Female, 010606 plant biology & botany

Abstract

Three undescribed stictanes, nieblastictanes A−C, two flavicanes, nieblaflavicanes A and B, together with three already reported stictanes, along with the known compounds (+)-usnic acid, sekikaic acid, divaricatic acid, and divaricatinic acid methyl ester were isolated from an ethyl acetate extract of the western North American lichen Niebla homalea. The structures of the new and known compounds were established by spectroscopic methods including nuclear magnetic resonance spectroscopy, mass spectrometry and electronic circular dichroism. Among the compounds isolated, usnic acid exhibited moderately potent antiproliferative activities against the A2780 ovarian (IC50 3.8 μM) and MCF-7 breast cancer (IC50 6.8 μM) cell lines. A plausible mode of formation of the chlorine-containing compound nieblastictane C is provided and the contribution of the isolated compounds to the chemotaxonomy of United States lichen species of the genus Niebla is also discussed.

Published

2020

39. Computational and synthetic approaches for developing Lavendustin B derivatives as allosteric inhibitors of HIV-1 integrase

Author

Stefania Ferro, Mamuka Kvaratskhelia, James R. Fuchs, Rosaria Gitto, Laura De Luca, Ashley C. Hoyte, Fatima E. Agharbaoui, and Maria Rosa Buemi

Subjects

0301 basic medicine, Anti-HIV Agents, Protein Conformation, Stereochemistry, In silico, Allosteric regulation, Integrase inhibitor, Lavendustin B, Chemistry Techniques, Synthetic, HIV Integrase, Molecular Dynamics Simulation, Molecular mechanics, Article, ALLINI, Computational studies, HIV-1, IN-LEDGF/p75 binding, Integrase, LEDGF/p75, Pharmacology, Drug Discovery3003 Pharmaceutical Science, Organic Chemistry, 03 medical and health sciences, 0302 clinical medicine, Allosteric Regulation, Drug Discovery, medicine, Humans, Pharmacology, Virtual screening, biology, Chemistry, Organic Chemistry, General Medicine, Combinatorial chemistry, Salicylates, meta-Aminobenzoates, Integrase, Molecular Docking Simulation, 030104 developmental biology, Mechanism of action, Drug Design, 030220 oncology & carcinogenesis, HIV-1, biology.protein, medicine.symptom, HeLa Cells

Abstract

Through structure-based virtual screening and subsequent activity assays of selected natural products, Lavendustin B was previously identified as an inhibitor of HIV-1 integrase (IN) interaction with its cognate cellular cofactor, lens epithelium-derived growth factor (LEDGF/p75). In order to improve the inhibitory potency we have employed in silico-based approaches. Particularly, a series of new analogues was designed and docked into the LEDGF/p75 binding pocket of HIV-1 IN. To identify promising leads we used the Molecular Mechanics energies combined with the Generalized Born and Surface Area continuum solvation (MM-GBSA) method, molecular dynamics simulations and analysis of hydrogen bond occupancies. On the basis of these studies, six analogues of Lavendustine B, containing the benzylamino-hydroxybenzoic scaffold, were selected for synthesis and structure activity-relationship (SAR) studies. Our results demonstrated a good correlation between computational and experimental data, and all six analogues displayed an improved potency for inhibiting IN binding to LEDGF/p75 in vitro to respect to the parent compound Lavendustin B. Additionally, these analogs show to inhibit weakly LEDGF/p75-independent IN catalytic activity suggesting a multimodal allosteric mechanism of action. Nevertheless, for the synthesized compounds similar profiles for HIV-1 inhibition and cytoxicity were highlighted. Taken together, our studies elucidated the mode of action of Lavendustin B analogs and provided a path for their further development as a new promising class of HIV-1 integrase inhibitors.

Published

2016

40. A New Class of Allosteric HIV-1 Integrase Inhibitors Identified by Crystallographic Fragment Screening of the Catalytic Core Domain

Author

James R. Fuchs, Arthur J. Olson, Mamuka Kvaratskhelia, Stefano Forli, Lei Feng, Janet Antwi, D. Patel, Ronald M. Levy, Pratibha C. Koneru, Joseph D. Bauman, Erik Serrao, Nanjie Deng, Alan Engelman, Jacques J. Kessl, and Eddy Arnold

Subjects

Models, Molecular, 0301 basic medicine, Stereochemistry, Mutant, Allosteric regulation, Carboxylic Acids, HIV Infections, HIV Integrase, Thiophenes, Biology, Crystallography, X-Ray, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, Allosteric Regulation, Catalytic Domain, Drug Discovery, Humans, HIV Integrase Inhibitors, Molecular Biology, 030102 biochemistry & molecular biology, Drug discovery, Quinoline, HEK 293 cells, Cell Biology, Integrase, Molecular Docking Simulation, Crystallography, HEK293 Cells, 030104 developmental biology, chemistry, Viral replication, Protein Structure and Folding, HIV-1, biology.protein, Lead compound

Abstract

HIV-1 integrase (IN) is essential for virus replication and represents an important multifunctional therapeutic target. Recently discovered quinoline-based allosteric IN inhibitors (ALLINIs) potently impair HIV-1 replication and are currently in clinical trials. ALLINIs exhibit a multimodal mechanism of action by inducing aberrant IN multimerization during virion morphogenesis and by competing with IN for binding to its cognate cellular cofactor LEDGF/p75 during early steps of HIV-1 infection. However, quinoline-based ALLINIs impose a low genetic barrier for the evolution of resistant phenotypes, which highlights a need for discovery of second-generation inhibitors. Using crystallographic screening of a library of 971 fragments against the HIV-1 IN catalytic core domain (CCD) followed by a fragment expansion approach, we have identified thiophenecarboxylic acid derivatives that bind at the CCD-CCD dimer interface at the principal lens epithelium-derived growth factor (LEDGF)/p75 binding pocket. The most active derivative (5) inhibited LEDGF/p75-dependent HIV-1 IN activity in vitro with an IC50 of 72 μm and impaired HIV-1 infection of T cells at an EC50 of 36 μm. The identified lead compound, with a relatively small molecular weight (221 Da), provides an optimal building block for developing a new class of inhibitors. Furthermore, although structurally distinct thiophenecarboxylic acid derivatives target a similar pocket at the IN dimer interface as the quinoline-based ALLINIs, the lead compound, 5, inhibited IN mutants that confer resistance to quinoline-based compounds. Collectively, our findings provide a plausible path for structure-based development of second-generation ALLINIs.

Published

2016

41. STAT3 as a potential therapeutic target in ALDH+ and CD44+/CD24+ stem cell-like pancreatic cancer cells

Author

Li Lin, Jiayuh Lin, Pui-Kai Li, Tianshu Liu, Chenglong Li, Jiagao Lü, Haiyan Ma, David Jou, Yina Wang, and James R. Fuchs

Subjects

cancer stem cells, STAT3 Transcription Factor, 0301 basic medicine, Cancer Research, Curcumin, Cell Survival, pancreatic cancer, Cell, Aldehyde dehydrogenase, Anthraquinones, STAT3, 03 medical and health sciences, 0302 clinical medicine, Cancer stem cell, Spheroids, Cellular, Pancreatic cancer, Tumor Cells, Cultured, medicine, Humans, CD44, skin and connective tissue diseases, CD24, Sulfonamides, biology, Oncogene, CD24 Antigen, Articles, Aldehyde Dehydrogenase, Cell cycle, medicine.disease, Molecular biology, Enzyme Activation, Pancreatic Neoplasms, Hyaluronan Receptors, 030104 developmental biology, medicine.anatomical_structure, Oncology, 030220 oncology & carcinogenesis, Neoplastic Stem Cells, biology.protein, Cancer research, Stem cell

Abstract

Persistent activation of signal transducers and activators of transcription 3 (STAT3) is commonly detected in many types of cancer including pancreatic cancer. Whether STAT3 is activated in stem cell-like pancreatic cancer cells and the effect of STAT3 inhibition, is still unknown. Flow cytometry was used to isolate pancreatic cancer stem-like cells which are identified by both aldehyde dehydrogenase (ALDH)-positive (ALDH+) as well as cluster of differentiation (CD) 44-positive/CD24-positive subpopulations (CD44+/CD24+). STAT3 activation and the effects of STAT3 inhibition by STAT3 inhibitors, LLL12, FLLL32, and Stattic in ALDH+ and CD44+/CD24+ cells were examined. Our results showed that ALDH+ and CD44+/CD24+ pancreatic cancer stem-like cells expressed higher levels of phosphorylated STAT3, an active form of STAT3, compared to ALDH-negative (ALDH-) and CD44-negative/CD24-negative (CD44-/CD24-) pancreatic cancer cells, suggesting that STAT3 is activated in pancreatic cancer stem-like cells. Small molecular STAT3 inhibitors inhibited STAT3 phosphorylation, STAT3 downstream target gene expression, cell viability, and tumorsphere formation in ALDH+ and CD44+/CD24+ cells. Our results indicate that STAT3 is a novel therapeutic target in pancreatic cancer stem-like cells and inhibition of activated STAT3 in these cells by STAT3 inhibitors may offer an effective treatment for pancreatic cancer.

Published

2016

42. Allosteric HIV-1 integrase inhibitors promote aberrant protein multimerization by directly mediating inter-subunit interactions: Structural and thermodynamic modeling studies

Author

Nanjie Deng, Ashley C. Hoyte, Alan Engelman, Mamuka Kvaratskhelia, Mosaad S. Mohamed, Ronald M. Levy, James R. Fuchs, and Yara E. Mansour

Subjects

0301 basic medicine, 030102 biochemistry & molecular biology, biology, Chemistry, Dimer, Protein subunit, Allosteric regulation, Biochemistry, Aberrant protein, Integrase, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Docking (molecular), Hiv 1 integrase, Biophysics, biology.protein, CTD, Molecular Biology

Abstract

Allosteric HIV-1 integrase (IN) inhibitors (ALLINIs) bind at the dimer interface of the IN catalytic core domain (CCD), and potently inhibit HIV-1 by promoting aberrant, higher-order IN multimerization. Little is known about the structural organization of the inhibitor-induced IN multimers and important questions regarding how ALLINIs promote aberrant IN multimerization remain to be answered. On the basis of physical chemistry principles and from our analysis of experimental information, we propose that inhibitor-induced multimerization is mediated by ALLINIs directly promoting inter-subunit interactions between the CCD dimer and a C-terminal domain (CTD) of another IN dimer. Guided by this hypothesis, we have built atomic models of inter-subunit interfaces in IN multimers by incorporating information from hydrogen-deuterium exchange (HDX) measurements to drive protein-protein docking. We have also developed a novel free energy simulation method to estimate the effects of ALLINI binding on the association of the CCD and CTD. Using this structural and thermodynamic modeling approach, we show that multimer inter-subunit interface models can account for several experimental observations about ALLINI-induced multimerization, including large differences in the potencies of various ALLINIs, the mechanisms of resistance mutations, and the crucial role of solvent exposed R-groups in the high potency of certain ALLINIs. Our study predicts that CTD residues Tyr226, Trp235 and Lys266 are involved in the aberrant multimer interfaces. The key finding of the study is that it suggests the possibility of ALLINIs facilitating inter-subunit interactions between an external CTD and the CCD-CCD dimer interface.

Published

2016

43. The Competitive Interplay between Allosteric HIV-1 Integrase Inhibitor BI/D and LEDGF/p75 during the Early Stage of HIV-1 Replication Adversely Affects Inhibitor Potency

Author

Erik Serrao, Frederic D. Bushman, Alan Engelman, Venkatasubramanian Dharmarajan, Ashley C. Hoyte, Alison Slaughter, Jacques J. Kessl, Patrick R. Griffin, James R. Fuchs, Matthew R. Plumb, Ross C. Larue, Mamuka Kvaratskhelia, Amit Sharma, and Lei Feng

Subjects

0301 basic medicine, Allosteric regulation, Integrase inhibitor, HIV Infections, HIV Integrase, Virus Replication, Biochemistry, Article, 03 medical and health sciences, Allosteric Regulation, Tetramer, Humans, HIV Integrase Inhibitors, Binding site, 030102 biochemistry & molecular biology, biology, HEK 293 cells, General Medicine, Molecular biology, In vitro, Integrase, HEK293 Cells, 030104 developmental biology, Viral replication, HIV-1, biology.protein, Intercellular Signaling Peptides and Proteins, Molecular Medicine

Abstract

Allosteric HIV-1 integrase inhibitors (ALLINIs) have recently emerged as a promising class of antiretroviral agents and are currently in clinical trials. In infected cells, ALLINIs potently inhibit viral replication by impairing virus particle maturation but surprisingly exhibit a reduced EC50 for inhibiting HIV-1 integration in target cells. To better understand the reduced antiviral activity of ALLINIs during the early stage of HIV-1 replication, we investigated the competitive interplay between a potent representative ALLINI, BI/D, and LEDGF/p75 with HIV-1 integrase. While the principal binding sites of BI/D and LEDGF/p75 overlap at the integrase catalytic core domain dimer interface, we show that the inhibitor and the cellular cofactor induce markedly different multimerization patterns of full-length integrase. LEDGF/p75 stabilizes an integrase tetramer through the additional interactions with the integrase N-terminal domain, whereas BI/D induces protein–protein interactions in C-terminal segments that lead to aberrant, higher-order integrase multimerization. We demonstrate that LEDGF/p75 binds HIV-1 integrase with significantly higher affinity than BI/D and that the cellular protein is able to reverse the inhibitor induced aberrant, higher-order integrase multimerization in a dose-dependent manner in vitro. Consistent with these observations, alterations of the cellular levels of LEDGF/p75 markedly affected BI/D EC50 values during the early steps of HIV-1 replication. Furthermore, genome-wide sequencing of HIV-1 integration sites in infected cells demonstrate that LEDGF/p75-dependent integration site selection is adversely affected by BI/D treatment. Taken together, our studies elucidate structural and mechanistic details of the interplay between LEDGF/p75 and BI/D during the early stage of HIV-1 replication.

Published

2016

44. Overcoming chemo/radio-resistance of pancreatic cancer by inhibiting STAT3 signaling

Author

Fengtian He, Chad Allen Highfill, Ling Li, Liang Xu, Jiqin Lian, Xiaoqing Wu, Jiayuh Lin, Min Ji, Rebecca T. Marquez, Wenhua Tang, Ke Li, and James R. Fuchs

Subjects

0301 basic medicine, Gerontology, medicine.medical_treatment, pancreatic cancer, Stem cell marker, Deoxycytidine, Radiation Tolerance, chemo/radio-resistance, Mice, Random Allocation, 0302 clinical medicine, Pancreatic tumor, Antineoplastic Combined Chemotherapy Protocols, Medicine, education.field_of_study, lip-FLLL32, Drug Synergism, Chemoradiotherapy, 3. Good health, Oncology, 030220 oncology & carcinogenesis, Female, Stem cell, medicine.drug, Research Paper, Signal Transduction, STAT3 Transcription Factor, Curcumin, Population, Mice, Nude, 03 medical and health sciences, Radioresistance, Pancreatic cancer, Cell Line, Tumor, pSTAT3, Animals, Humans, education, business.industry, medicine.disease, Survival Analysis, Gemcitabine, Radiation therapy, Pancreatic Neoplasms, 030104 developmental biology, Drug Resistance, Neoplasm, Cancer research, CSCs, business

Abstract

// Xiaoqing Wu 1, 2, 3 , Wenhua Tang 1, 2 , Rebecca T. Marquez 1 , Ke Li 1 , Chad A. Highfill 1 , Fengtian He 1, 2, 4 , Jiqin Lian 2, 4 , Jiayuh Lin 5 , James R. Fuchs 6 , Min Ji 3 , Ling Li 2, 7 , Liang Xu 1, 2 1 Departments of Molecular Biosciences and Radiation Oncology, University of Kansas, Lawrence, KS, USA 2 Department of Radiation Oncology, University of Michigan Medical School, Ann Arbor, MI, USA 3 School of Chemistry and Chemical Engineering, Southeast University, Nanjing, Jiangsu, China 4 Department of Biochemistry and Molecular Biology, Third Military Medical University, Chongqing, China 5 Department of Pediatrics, College of Medicine, Ohio State University, Columbus, OH, USA 6 Division of Medicinal Chemistry and Pharmacognosy, College of Pharmacy, Ohio State University, Columbus, OH, USA 7 Department of Cell Biology and Cell Engineering Research Centre, State Key Laboratory of Cancer Biology, Fourth Military Medical University, Xi’an, Shanxi, China Correspondence to: Liang Xu, e-mail: xul@ku.edu Ling Li, e-mail: liling25@fmmu.edu.cn Keywords: chemo/radio-resistance, pSTAT3, pancreatic cancer, lip-FLLL32, CSCs Received: September 22, 2015 Accepted: January 23, 2016 Published: February 12, 2016 ABSTRACT Chemo/radio-therapy resistance to the deadly pancreatic cancer is mainly due to the failure to kill pancreatic cancer stem cells (CSCs). Signal transducer and activator of transcription 3 (STAT3) is activated in pancreatic CSCs and, therefore, may be a valid target for overcoming therapeutic resistance. Here we investigated the potential of STAT3 inhibition in sensitizing pancreatic cancer to chemo/radio-therapy. We found that the levels of nuclear pSTAT3 in pancreatic cancer correlated with advanced tumor grade and poor patient outcome. Liposomal delivery of a STAT3 inhibitor FLLL32 (Lip-FLLL32) inhibited STAT3 phosphorylation and STAT3 target genes in pancreatic cancer cells and tumors. Consequently, Lip-FLLL32 suppressed pancreatic cancer cell growth, and exhibited synergetic effects with gemcitabine and radiation treatment in vitro and in vivo . Furthermore, Lip-FLLL32 reduced ALDH1-positive CSC population and modulated several potential stem cell markers. These results demonstrate that Lip-FLLL32 suppresses pancreatic tumor growth and sensitizes pancreatic cancer cells to radiotherapy through inhibition of CSCs in a STAT3-dependent manner. By targeting pancreatic CSCs, Lip-FLLL32 provides a novel strategy for pancreatic cancer therapy via overcoming radioresistance.

Published

2016

45. Abstract 1950: The eIF4A inhibitors didesmethylrocaglamide and rocaglamide as effective treatments for pediatric bone and soft-tissue sarcomas

Author

Ryan Roberts, A. Douglas Kinghorn, Barry R. O'Keefe, James R. Fuchs, Janet L. Oblinger, Garima Agarwal, Tyler A. Wilson, Chang Long-Sheng, and Jerry M. Collins

Subjects

Cancer Research, Cell growth, business.industry, Mesenchymal stem cell, Cell, Cancer, medicine.disease, Metastasis, chemistry.chemical_compound, medicine.anatomical_structure, Oncology, Rocaglamide, chemistry, medicine, Cancer research, Osteosarcoma, Sarcoma, business

Abstract

Background: Development of an effective medical therapy for osteosarcoma and Ewing sarcoma, the two most common aggressive forms of pediatric bone and soft-tissue sarcomas, is urgently needed as current treatments are inadequate particularly for those with recurrent or metastatic diseases. To achieve this goal, we have identified two natural eIF4A inhibitors, rocaglamide (Roc) and didesmethylrocaglamide (DDR), which potently inhibit proliferation of a series of commonly-used osteosarcoma and Ewing sarcoma cell lines. We also demonstrated that Roc effectively suppresses tumor growth in patient-derived xenograft (PDX) models of osteosarcoma and Ewing sarcoma. Both Roc- and DDR-treated sarcoma cells show decreased levels of multiple oncogenic kinases, including insulin-like growth factor-1 receptor (IGF-1R). Importantly, these rocaglamides are not sensitive to multidrug resistance 1 (MDR1) efflux. In addition, Roc exhibits 50% oral bioavailability, is well-tolerated in mice, and does not induce pulmonary toxicity in dogs as found with another eIF4A inhibitor silvestrol (Chang et al. Mol Cancer Ther. 2019; In Revision). Methods: Various osteosarcoma and Ewing sarcoma cell lines were treated with DDR and Roc, followed by cell proliferation assay, flow cytometry, and immunoblotting. Mesenchymal stem cells (MSCs) were used as a control for comparing the expression levels of the eIF4F components important for translation initiation. RNA interference (RNAi) and CRISPR/Cas9 techniques were used to verify eIF4A dependency. An orthotopic cell line-derived xenograft (CDX), a metastatic xenograft, and a PDX models for osteosarcoma and immunohistochemistry were used to assess antitumor efficacy. Results: We hypothesize that osteosarcoma and Ewing sarcoma cells are highly addicted to active protein synthesis and that Roc and DDR, by acting as potent eIF4A inhibitors with an ability to induce apoptosis and the DNA damage response, effectively eliminate these malignant sarcomas. We found that various osteosarcoma and Ewing sarcoma cell lines expressed higher levels of eIF4A2, but not eIF4A1, eIF4E, and eIF4G, than MSCs, suggesting a role of eIF4A2 in enhancing protein translation in these sarcoma cells. RNAi knockdown and CRISPR/Cas9 knockout experiments are being evaluated to verify this finding. Both DDR and Roc effectively blocked tumor growth in an orthotopic CDX model. As found with Roc previously, DDR also potently inhibited the growth of an osteosarcoma PDX model. Both rocaglamides were well tolerated at 3 mg/kg by IP every other day and did not cause any significant changes in body weight, compared with vehicle-treated controls. We are presently determining the effects of Roc and DDR on osteosarcoma metastasis. Conclusions: The potent anti-tumor activity and favorable toxicity profile of Roc and DDR suggest that these rocaglamides should be further evaluated as potential treatments for osteosarcomas and Ewing sarcomas. Citation Format: Long-Sheng Chang, Janet L. Oblinger, Garima Agarwal, Tyler A. Wilson, Ryan Roberts, James Fuchs, Barry R. O'Keefe, A. Douglas Kinghorn, Jerry M. Collins. The eIF4A inhibitors didesmethylrocaglamide and rocaglamide as effective treatments for pediatric bone and soft-tissue sarcomas [abstract]. In: Proceedings of the Annual Meeting of the American Association for Cancer Research 2020; 2020 Apr 27-28 and Jun 22-24. Philadelphia (PA): AACR; Cancer Res 2020;80(16 Suppl):Abstract nr 1950.

Published

2020

46. Pentalinonsterol exhibits the immunomodulatory action in macrophages through activation of Phospholipase A 2

Author

Nidhi Srivastava, Abhay R. Satoskar, Narasimham L. Parinandi, Travis O. Gurney, James R. Fuchs, Sanjay Varikuti, Blake Shelton, Guarav Gupta, Dougles Kinghorn, and Sainath R. Kotha

Subjects

Phospholipase A, Action (philosophy), Chemistry, Genetics, Molecular Biology, Biochemistry, Biotechnology, Cell biology

Published

2020

47. Identification of a Small Molecule Anti-biofilm Agent Against Salmonella enterica

Author

John S. Gunn, Jasmine Moshiri, Chido M. Hambira, James R. Fuchs, Darpan Kaur, Jenna L. Sandala, and Jacob A. Koopman

Subjects

0301 basic medicine, Microbiology (medical), Serotype, Salmonella, 030106 microbiology, lcsh:QR1-502, medicine.disease_cause, Microbiology, biofilm, lcsh:Microbiology, Typhoid fever, 03 medical and health sciences, Antibiotic resistance, Typhoid, medicine, anti-biofilm, Original Research, biology, Biofilm, biochemical phenomena, metabolism, and nutrition, chronic infection, biology.organism_classification, medicine.disease, 3. Good health, Acinetobacter baumannii, Ciprofloxacin, 030104 developmental biology, Salmonella enterica, medicine.drug

Abstract

Biofilm formation is a common strategy utilized by bacterial pathogens to establish persistence in a host niche. Salmonella enterica serovar Typhi, the etiological agent of Typhoid fever, relies on biofilm formation in the gallbladder to chronically colonize asymptomatic carriers, allowing for transmission to uninfected individuals. S. enterica serovar Typhimurium utilizes biofilms to achieve persistence in human and animal hosts, an issue of both clinical and agricultural importance. Here, we identify a compound that selectively inhibits biofilm formation in both S. Typhi and S. Typhimurium serovars at early stages of biofilm development with an EC50 of 21.0 and 7.4 μM, respectively. We find that this compound, T315, also reduces biofilm formation in Acinetobacter baumannii, a nosocomial and opportunistic pathogen with rising antibiotic resistance. T315 treatment in conjunction with sub-MIC dosing of ciprofloxacin further reduces S. enterica biofilm formation, demonstrating the potential of such combination therapies for therapeutic development. Through synthesis of two biotin-labeled T315 probes and subsequent pull-down and proteomics analysis, we identified a T315 binding target: WrbA, a flavin mononucleotide-dependent NADH:quinone oxidoreductase. Using a S. Typhimurium strain lacking WrbA we demonstrate that this factor contributes to endogenous S. enterica biofilm formation processes and is required for full T315 anti-biofilm activity. We suggest WrbA as a promising target for further development of anti-biofilm agents in Salmonella, with potential for use against additional bacterial pathogens. The development of anti-biofilm therapeutics will be essential to combat chronic carriage of Typhoid fever and thus accomplish a meaningful reduction of global disease burden.

Published

2018

48. Synthesis and antiproliferative activity of derivatives of the phyllanthusmin class of arylnaphthalene lignan lactones

Author

Andrew C. Huntsman, Soumendrakrishna Karmahapatra, Alexandria N. Young, Joanna E. Burdette, Malcolm S. Cole, Hee Byung Chai, Denisse Herrera, Jack C. Yalowich, Yulin Ren, John L. Woodard, A. Douglas Kinghorn, James R. Fuchs, Ragu Kanagasabai, and Pratiq A. Patel

Subjects

Stereochemistry, Clinical Biochemistry, Pharmaceutical Science, Antineoplastic Agents, Naphthalenes, 010402 general chemistry, 01 natural sciences, Biochemistry, Lignans, Article, chemistry.chemical_compound, Lactones, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, Humans, Topoisomerase II Inhibitors, Benzodioxoles, Glycosides, Molecular Biology, IC50, Etoposide, Lignan, chemistry.chemical_classification, biology, Molecular Structure, 010405 organic chemistry, Topoisomerase, Organic Chemistry, Stereoisomerism, Carbohydrate, 0104 chemical sciences, Aglycone, chemistry, Cell culture, Acetylation, biology.protein, Molecular Medicine, Drug Screening Assays, Antitumor, Lactone

Abstract

A series of arylnaphthalene lignan lactones based on the structure of the phyllanthusmins, a class of potent natural products possessing diphyllin as the aglycone, has been synthesized and screened for activity against multiple cancer cell lines. SAR exploration was performed on both the carbohydrate and lactone moieties of this structural class. These studies have revealed the importance of functionalization of the carbohydrate hydroxy groups with both acetylated and methylated analogues showing increased potency relative to those with unsubstituted sugar moieties. In addition, the requirement for the presence and position of the C-ring lactone has been demonstrated through reduction and selective re-oxidation of the lactone ring. The most potent compound in this study displayed an IC50 value of 18 nM in an HT-29 assay with several others ranging from 50 to 200 nM. In an effort to elucidate their potential mechanism(s) of action, the DNA topoisomerase IIa inhibitory activity of the most potent compounds was examined based on previous reports of structurally similar compounds, but does not appear to contribute significantly to their antiproliferative effects.

Published

2017

49. A Novel Sterol Isolated from a Plant Used by Mayan Traditional Healers Is Effective in Treatment of Visceral Leishmaniasis Caused by Leishmania donovani

Author

C. Benjamin Naman, Sanjay Varikuti, Kristy M. Ainslie, Steve Oghumu, Heidi M. Snider, Andrew C. Huntsman, Abhay R. Satoskar, Dalia Abdelhamid, Narasimham L. Parinandi, Kevin J. Peine, Andrew B. Shelton, Sainath R. Kotha, James R. Fuchs, A. Douglas Kinghorn, Li Pan, Gaurav Gupta, Eric M. Bachelder, Tracey L. Papenfuss, and Latha Rao

Subjects

Drug, media_common.quotation_subject, Leishmania donovani, Spleen, Drug resistance, Biology, medicine.disease, biology.organism_classification, Article, Sterol, Microbiology, Infectious Diseases, medicine.anatomical_structure, Visceral leishmaniasis, Amphotericin B, Toxicity, Immunology, medicine, media_common, medicine.drug

Abstract

Visceral leishmaniasis (VL), caused by the protozoan parasite Leishmania donovani, is a global health problem affecting millions of people worldwide. Treatment of VL largely depends on therapeutic drugs such as pentavalent antimonials, amphotericin B, and others, which have major drawbacks due to drug resistance, toxicity, and high cost. In this study, for the first time, we have successfully demonstrated the synthesis and antileishmanial activity of the novel sterol pentalinonsterol (PEN), which occurs naturally in the root of a Mexican medicinal plant, Pentalinon andrieuxii. In the experimental BALB/c mouse model of VL induced by infection with L. donovani, intravenous treatment with liposome-encapsulated PEN (2.5 mg/kg) led to a significant reduction in parasite burden in the liver and spleen. Furthermore, infected mice treated with liposomal PEN showed a strong host-protective TH1 immune response characterized by IFN-γ production and formation of matured hepatic granulomas. These results indicate that PEN could be developed as a novel drug against VL.

Published

2015

50. FLLL12 induces apoptosis in lung cancer cells through a p53/p73-independent but death receptor 5-dependent pathway

Author

Mohammad Aminur Rahman, Dong M. Shin, Fadlo R. Khuri, Abedul Haque, Zhuo Georgia Chen, James R. Fuchs, and A.R.M. Ruhul Amin

Subjects

Cancer Research, Curcumin, Lung Neoplasms, Poly ADP ribose polymerase, Sulforhodamine B, Apoptosis, Biology, Article, chemistry.chemical_compound, Annexin, In vivo, Cell Line, Tumor, medicine, Humans, Lung cancer, Tumor Suppressor Proteins, Nuclear Proteins, Tumor Protein p73, medicine.disease, Molecular biology, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Receptors, TNF-Related Apoptosis-Inducing Ligand, Oncology, chemistry, Cell culture, Cancer research, Tumor Suppressor Protein p53, Signal Transduction

Abstract

Unlike chemotherapy drugs, the safety of natural compounds such as curcumin has been well established. However, the potential use of curcumin in cancer has been compromised by its low bioavailability, limited tissue distribution and rapid biotransformation leading to low in vivo efficacy. To circumvent these problems, more potent and bioavailable analogs have been synthesized. In the current study, we investigated the mechanism of anti-tumor effect of one such analog, FLLL12, in lung cancers. IC50 values measured by sulforhodamine B (SRB) assay at 72 h and apoptosis assays (annexin V staining, cleavage of PARP and caspase-3) suggest that FLLL12 is 5–10-fold more potent than curcumin against a panel of premalignant and malignant lung cancer cell lines, depending on the cell line. Moreover, FLLL12 induced the expression of death receptor-5 (DR5). Ablation of the expression of the components of the extrinsic apoptotic pathway (DR5, caspase-8 and Bid) by siRNA significantly protected cells from FLLL12-induced apoptosis (p < 0.05). Analysis of mRNA expression revealed that FLLL-12 had no significant effect on the expression of DR5 mRNA expression. Interestingly, inhibition of global phosphatase activity as well as protein tyrosine phosphatases (PTPs), but not of alkaline phosphatases, strongly inhibited DR5 expression and significantly inhibited apoptosis (p < 0.05), suggesting the involvement of PTPs in the regulation of DR5 expression and apoptosis. We further showed that the apoptosis is independent of p53 and p73. Taken together, our results strongly suggest that FLLL12 induces apoptosis of lung cancer cell lines by post-transcriptional regulation of DR5 through activation of protein tyrosine phosphatase(s).

Published

2015