Your search keyword '"2A"' showing total 149 results

1. Adoption of the 2A Ribosomal Skip Principle to Track Assembled Virions of Pepper Mild Mottle Virus in Nicotiana benthamiana.

Author

Jiao, Mengting, Yin, Yueyan, Tian, Yanzhen, Lei, Jianing, Lin, Lin, Wu, Jian, Lu, Yuwen, Zheng, Hongying, Yan, Fei, Wang, Jianguang, and Peng, Jiejun

Subjects

VIRION, NICOTIANA benthamiana, PEPPERS, CYTOSKELETAL proteins, FOOT & mouth disease, PEPTIDES, CUCUMBER mosaic virus, MOSAIC viruses

Abstract

The coat protein (CP) is an important structural protein that plays many functional roles during the viral cycle. In this study, the CP of pepper mild mottle virus (PMMoV) was genetically fused to GFP using the foot-and-mouth disease virus peptide 2A linker peptide and the construct (PMMoV-GFP2A) was shown to be infectious. The systemic spread of the virus was monitored by its fluorescence in infected plants. Electron microscopy and immunocolloidal gold labelling confirmed that PMMoV-GFP2A forms rod-shaped particles on which GFP is displayed. Studies of tissue ultrastructure and virion self-assembly confirmed that PMMoV-GFP2A could be used to monitor the real-time dynamic changes of CP location during virus infection. Aggregations of GFP-tagged virions appeared as fluorescent plaques in confocal laser microscopy. Altogether, PMMoV-GFP2A is a useful tool for studying the spatial and temporal changes of PMMoV CP during viral infection. [ABSTRACT FROM AUTHOR]

Published

2024

2. The role of the encephalomyocarditis virus type 1 proteins L and 2A in the inhibition of the synthesis of cellular proteins and the accumulation of viral proteins during infection

Author

Yury Yu. Ivin, Anna A. Butusova, Ekaterina E. Gladneva, Galina Ya. Kolomijtseva, Yusuf K. Khapchaev, and Aydar A. Ishmukhametov

Subjects

emcv-1, cardioviruses, picornaviruses, «security» proteins, leader protein, 2a, translation inhibition, processing, Microbiology, QR1-502

Abstract

Introduction. Infection of cells with encephalomyocarditis virus type 1 (EMCV-1, Cardiovirus A: Picornaviridae) is accompanied by suppression of cellular protein synthesis. The main role in the inhibition of cellular translation is assigned to the L and 2A «security» proteins. The mechanism of the possible influence of the L protein on cellular translation is unknown. There are hypotheses about the mechanism of influence of 2A protein on the efficiency of cap-dependent translation, which are based on interaction with translation factors and ribosome subunits. However, the available experimental data are contradictory, obtained using different approaches, and do not form a unified model of the interaction between the L and 2A proteins and the cellular translation machinery. Aim. To study the role of L and 2A «security» proteins in the suppression of translation of cellular proteins and the efficiency of translation and processing of viral proteins in infected cells. Materials and methods. Mutant variants of EMCV-1 were obtained to study the properties of L and 2A viral proteins: Zfmut, which has a defective L; Δ2A encoding a partially deleted 2A; ZfmutΔ2A containing mutations in both proteins. Translational processes in infected cells were studied by Western-blot and the pulse method of incorporating radioactively labeled amino acids (14C) into newly synthesized proteins, followed by radioautography. Results. The functional inactivation of the 2A protein does not affect the inhibition of cellular protein synthesis. A direct correlation was found between the presence of active L protein and specific inactivation of cellular protein synthesis at an early stage of viral infection. Nonspecific suppression of the translational processes of the infected cell, accompanied by phosphorylation of eIF2α, occurs at the late stage of infection. Partial removal of the 2A protein from the EMCV-1 genome does not affect the development of this process, while inactivation of the L protein accelerates the onset of complete inhibition of protein synthesis. Partial deletion of the 2A disrupts the processing of viral capsid proteins. Suppression of L protein functions leads to a decrease in the efficiency of viral translation. Conclusion. A study of the role of EMCV-1 L and 2A proteins during the translational processes of an infected cell, first performed using infectious viral pathogens lacking active L and 2A proteins in one experiment, showed that 2A protein is not implicated in the inhibition of cellular translation in HeLa cells; L protein seems to play an important role not only in the specific inhibition of cellular translation but also in maintaining the efficient synthesis of viral proteins; 2A protein is involved not only in primary but also in secondary processing of EMCV-1 capsid proteins.

Published

2023

3. Adoption of the 2A Ribosomal Skip Principle to Track Assembled Virions of Pepper Mild Mottle Virus in Nicotiana benthamiana

Author

Mengting Jiao, Yueyan Yin, Yanzhen Tian, Jianing Lei, Lin Lin, Jian Wu, Yuwen Lu, Hongying Zheng, Fei Yan, Jianguang Wang, and Jiejun Peng

Subjects

2A, pepper mild mottle virus, coat protein, self-assembly, Botany, QK1-989

Abstract

The coat protein (CP) is an important structural protein that plays many functional roles during the viral cycle. In this study, the CP of pepper mild mottle virus (PMMoV) was genetically fused to GFP using the foot-and-mouth disease virus peptide 2A linker peptide and the construct (PMMoV-GFP2A) was shown to be infectious. The systemic spread of the virus was monitored by its fluorescence in infected plants. Electron microscopy and immunocolloidal gold labelling confirmed that PMMoV-GFP2A forms rod-shaped particles on which GFP is displayed. Studies of tissue ultrastructure and virion self-assembly confirmed that PMMoV-GFP2A could be used to monitor the real-time dynamic changes of CP location during virus infection. Aggregations of GFP-tagged virions appeared as fluorescent plaques in confocal laser microscopy. Altogether, PMMoV-GFP2A is a useful tool for studying the spatial and temporal changes of PMMoV CP during viral infection.

Published

2024

4. Generation of bicistronic Dmp1-Cre knock-in mice using a self-cleaving 2A peptide.

Author

Nakamura, Takashi, Honda, Sayako, Ito, Shinichirou, Mizoguchi, Toshihide, Yamamoto, Takehiro, Kasahara, Masataka, Kabe, Yasuaki, Matsuo, Koichi, and Suematsu, Makoto

Subjects

*PEPTIDES, *TRANSGENIC mice, *EXTRACELLULAR matrix proteins, *GENE expression, *MICE

Abstract

Introduction: The conditional manipulation of genes using the Cre recombinase-locus of crossover in P1 (Cre/loxP) system is an important tool for revealing gene functions and cell lineages in vivo. The outcome of this method is dependent on the performance of Cre-driver mouse strains. In most cases, Cre knock-in mice show better specificity than randomly inserted Cre transgenic mice. However, following knock-in, the expression of the original gene replaced by Cre is lost. Materials and methods: We generated a new differentiated osteoblast- and osteocyte-specific Cre knock-in mouse line that carries the viral T2A sequence encoding a 2A self-cleaving peptide at the end of the coding region of the dentin matrix protein 1 (Dmp1) gene accompanied by the Cre gene. Results: We confirmed that Dmp1-T2A-Cre mice showed high Cre expression in osteoblasts, osteocytes, odontoblasts, and periodontal ligament cells and that the 2A self-cleaving peptide efficiently produced both Dmp1 and Cre proteins. Furthermore, unlike the Dmp1 knockout mice, homozygous Dmp1-T2A-Cre mice showed no skeletal abnormalities. Analysis using the Cre reporter strain confirmed differentiated osteoblast- and osteocyte-specific Cre-mediated recombination in the skeleton. Furthermore, recombination was also detected in some nuclei of skeletal muscle cells, spermatocytes, and intestinal cells. Conclusion: 2A-Cre functions effectively in vivo, and Dmp1-T2A-Cre knock-in mice are a useful tool for studying the functioning of various genes in hard tissues. [ABSTRACT FROM AUTHOR]

Published

2023

5. Stimulation of homologous recombination in plants expressing heterologous recombinases

Author

Abdellah Barakate, Ewan Keir, Helena Oakey, and Claire Halpin

Subjects

Intrachromosomal homologous recombination, Gene targeting, Gene editing, 2A, Translational-recoding, Pollen, Botany, QK1-989

Abstract

Abstract Background Current excitement about the opportunities for gene editing in plants have been prompted by advances in CRISPR/Cas and TALEN technologies. CRISPR/Cas is widely used to knock-out or modify genes by inducing targeted double-strand breaks (DSBs) which are repaired predominantly by error-prone non-homologous end-joining or microhomology-mediated end joining resulting in mutations that may alter or abolish gene function. Although such mutations are random, they occur at sufficient frequency to allow useful mutations to be routinely identified by screening. By contrast, gene knock-ins to replace entire genes with alternative alleles or copies with specific characterised modifications, is not yet routinely possible. Gene replacement (or gene targeting) by homology directed repair occurs at extremely low frequency in higher plants making screening for useful events unfeasible. Homology directed repair might be increased by inhibiting non-homologous end-joining and/or stimulating homologous recombination (HR). Here we pave the way to increasing gene replacement efficiency by evaluating the effect of expression of multiple heterologous recombinases on intrachromosomal homologous recombination (ICR) in Nicotiana tabacum plants. Results We expressed several bacterial and human recombinases in different combinations in a tobacco transgenic line containing a highly sensitive β-glucuronidase (GUS)-based ICR substrate. Coordinated simultaneous expression of multiple recombinases was achieved using the viral 2A translational recoding system. We found that most recombinases increased ICR dramatically in pollen, where HR will be facilitated by the programmed DSBs that occur during meiosis. DMC1 expression produced the greatest stimulation of ICR in primary transformants, with one plant showing a 1000-fold increase in ICR frequency. Evaluation of ICR in homozygous T2 plant lines revealed increases in ICR of between 2-fold and 380-fold depending on recombinase(s) expressed. By comparison, ICR was only moderately increased in vegetative tissues and constitutive expression of heterologous recombinases also reduced plant fertility. Conclusion Expression of heterologous recombinases can greatly increase the frequency of HR in plant reproductive tissues. Combining such recombinase expression with the use of CRISPR/Cas9 to induce DSBs could be a route to radically improving gene replacement efficiency in plants.

Published

2020

6. Synthesis and anti-tumor properties of derivatives [4- (41-chlorophenyl)-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[c,d]azulen-1-yl-metil]-para-tolylamine

Author

S. A. Demchenko, V. V. Sukhoveev, О. V. Моsкаlеnко, Yu. A. Fedchenkova, G. P. Potebnia, and A. M. Demchenko

Subjects

derivatives of [4-(41-chlorophenyl)-5, 8-tetrahydro-2, 2a, 8a-triaza¬cyclopenta[c, d]azulen-1-yl-metil]-para-tolylamine, antitumor properties, leukemia, 5-fluorouracil, Therapeutics. Pharmacology, RM1-950, Pharmacy and materia medica, RS1-441

Abstract

Leukemia, as a part of hemoblastosises, is a malignant blood system disease, which is characterized by bone marrow damage, caused by leukemic stem cells, which appear due to disruption of self-renewal and differentiation of hempoetic stem cells and predecessor cells. In their turn, hemoblastoses are divided into two groups: bone marrow (acute leukemia, chronical leukemia, paraproteinemic hemoblastoses) and outside bone marrow (lymphogranulomatosis, or Hodgkin lymphoma, and non-Hodgkin malignant mymphomas). Nowadays in Ukraine, different kinds of leukemia are cured by various drugs, which have many side effects. Increase in effectivity of chemotherapy of tumor disease is primarily related to creation of new antitumor drugs of selective action. Which is why search for biologically active compounds with antitumor activity is a perspective direction in creation of new drugs. Aim of this work was synthesis of compounds with potential antitumor properties in a variety of [4-(41-chlorophenyl)-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[c,d]-azulen-1-yl-methyl]-para-tolylamin derivatives. As the objects of our studies, we have picked the derivatives of [4-(41-chlorophenyl)-5,6,7,8-tetrahydro-2,2а,8а-triazacyclopenta[c,d]-azulen-1-yl-methyl]-para-tolilamin (8 and 10 a, b). [4-(41-Chlorphenyl)-5,6,7,8-tetrahydro-2,2а,8а-triazacyclopenta[c,d]azulen-1-yl-methyl]-para-tolylamin (8) was obtained by boiling of equimolar quantities of 3-(41-methylphenyl)aminomethyl-6,7,8,9-tetrahydro-5Н-[1,2,4]triazolo[4,3-a]azepin (5) and α-brom-4-chloracetophenon in ethylacetate. Thioamides (10 a, b) were obtained by interaction of amin (8) with corresponding arylisothiocyanates (9 а, b) in dry benzene. Antitumor activity of [4-(41-chlorphenyl)-5,6,7,8-tetrahydro-2,2а,8а-triazacyclopenta[c,d]azulen-1-yl-methyl]-para-tolylamin (8) was studied in National Cancer Institute of Health, USA within Development Therapeutic Program. In experimental conditions [4-(41-chlorphenyl)-5,6,7,8-tetrahydro-2,2а,8а-triazacyclopenta[c,d]azulen-1-yl-methyl]-para-tolylamin (8) showed ability to inhibit growth of cancerous leukemia cells of CCRF-CEM, HL-60(TB), K-562, MOLT-4, RPMI-8226 and SR lines, higher than standard – 5-fluorouracil. Towards HL-60(TB) cells [4-(41-chlorphenyl)-5,6,7,8-tetrahydro-2,2а,8а- triazacyclopenta[c,d]azulen-1-yl-methyl]-para-tolylamin exceeds standard in effectivity by 64.68%. For K-562, MOLT-4, RPMI-8226 and SR cells, those numbers are equal to: 85.88%, 84.95%, 42.10% and 36.82% correspondingly. Towards CCRF-CEM cells, this compound not only inhibits cell growth and division, but also destroys them by 20.34%. Thus conducted studies confirm perceptivity of search for compounds with antitumor action on the basis of [4-(41-chlorophenyl)-5,6,7,8-tetrahydro-2,2а,8а-triazacyclopenta[c,d]azulen-1-yl­methyl]-para-tolylamin.

Published

2020

7. Synthesis and antiviral properties derivatives of 1-(para-tolyl)-4-aryl-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulene-3-carbothioic acid arylamides

Author

S. A. Demchenko, Yu. A. Fedchenkova, А. М. Іvаsеnко, V.V. Sukhoveev, and A. M. Demchenko

Subjects

derivatives of 5, 8-tetrahydro-2, 2a, 8a-triazacyclopenta[cd]azulene-3-carbothioic acid, ribavirin, amizone, antiviral activity, Therapeutics. Pharmacology, RM1-950, Pharmacy and materia medica, RS1-441

Abstract

Nowadays, H1N1 – strain of so called «swine» or «mexican» subspecie A virus, which is still not studied, and which spreads through aerosol and contact is known to many world countries. Significant number of lethal cases during influenza pandemic season in Ukraine was observed. It should be noted, that patients went to the hospitals in very severe cases, which is why registered daily lethality is in 31,6% of cases. Everything listed above had made it necessary to conduct preventive measures on global and national levels. One of such measures is creation of new direct action medicinal agents. The goal of this work was the synthesis of compounds with potential antiviral properties in variety of 5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid derivatives. We have chosen derivatives of 5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid (6 a–e and 7 a–h), which were synthesized by boiling of 1-(para-tolyl)-4-aryl-5,6,7,8-tetrahydro-2,2a,4a-triazacyclopenta[cd]azulenes (5a or 5b) with corresponding arylisothiocyanates in dry benzene. Antiviral activity of phenylamid 1-(para-tolyl)-4-phenyl-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid against Flu A H1N1 California/07/2009 was researched in Southern Research Institute – SRI, Birmingham, Alabama). Variety of new derivatives of 5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid. Composition and structure of all synthesized compounds are proven by data of element analysis and 1Н NMR spectroscopy. In conducted researches of antiviral activity of phenylamide 1-(para-tolyl)-4-phenyl-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid against Flu A H1N1 California/07/2009, it was found out, that synthesized compound shows pronounced antiviral activity, compared to reference medicinal agents Ribavirin and Amizon. Therefore, conducted researches confirm perspective of development of a new domestic medicinal agent with antiviral activity, based on derivatives of 5,6,7,8,-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid.

Published

2019

8. Legitimacy and Significance of Art. 2A in the Constitution of Islamic Republic of Pakistan, 1973.

Author

Ahmed, Naveed, Khan, Ali Nawaz, and Munir, Bakht

Subjects

*CONSTITUTIONS, *LEGAL sanctions, *DELEGATION of authority, *HUMAN beings, *ISLAM, *HUMANITARIAN assistance

Abstract

Religion is a nearly common institution in humanity. It is found in all societies past and present. All the prehistoric societies have the influence of religions in their societies. Religion goes back to commencement of the culture itself. There is no primeval society without religion. It is social treatise that deals with familiarity and restraint. Religion is concerned with the shared beliefs and practices of human being. Allah being creator of this universe delegates his authority to those who owes it as a sacred trust in order to maintain peace and justice on this earth as per his commandments. Islam is an ideology sanctioned by revealed law. It is a way of life universal, humanitarian, eternal and egalitarian based on equality, fraternity, justice and liberty. Now, it is the duty of the state as well as the people of Pakistan to resort to the golden rules of Islam as enunciated by the Holy Quran and Muhammad (PBUH), in all fields of life. The key concern of this research is to evaluate the legitimacy of Art. 2A in the constitution of Pakistan and how is it practiced in Pakistan? [ABSTRACT FROM AUTHOR]

Published

2021

9. Encephalomyocarditis Virus 2A Protein Inhibited Apoptosis by Interaction with Annexin A2 through JNK/c-Jun Pathway

Author

Ruochan Han, Lin Liang, Tong Qin, Sa Xiao, and Ruiying Liang

Subjects

encephalomyocarditis virus, 2A, apoptosis, annexin A2, JNK/c-Jun pathway, Microbiology, QR1-502

Abstract

Encephalomyocarditis virus can cause myocarditis and encephalitis in pigs and other mammals, thus posing a potential threat to public health safety. The 2A protein is an important virulence factor of EMCV. Previous studies have shown that the 2A protein may be related to the inhibition of apoptosis by virus, but its specific molecular mechanism is not clear. In this study, the 2A protein was expressed in Escherichia coli in order to find interacting cell proteins. A pull down assay, coupled with mass spectrometry, revealed that the 2A protein possibly interacted with annexin A2. Co-immunoprecipitation assays and confocal imaging analysis further demonstrated that the 2A protein interacted with annexin A2 in cells. In reducing the expression of annexin A2 by siRNA, the ability of the 2A protein to inhibit apoptosis was weakened and the proliferation of EMCV was slowed down. These results suggest that annexin A2 is closely related to the inhibition of apoptosis by 2A. Furthermore, both RT-PCR and western blot results showed that the 2A protein requires annexin A2 interaction to inhibit apoptosis via JNK/c-Jun pathway. Taken together, our data indicate that the 2A protein inhibits apoptosis by interacting with annexin A2 via the JNK/c-Jun pathway. These findings provide insight into the molecular pathogenesis underlying EMCV infection.

Published

2022

10. Az endoszkópos és a mikroszkópos stapedotomia eredményeinek összehasonlítása -- Irodalmi áttekintés és metaanalízis.

Author

István, Tóth, Alexandros, Koukkoullis, Noémi, Gede, Zsolt, Szakács, Péter, Hegyi, Gábor, Varga, István, Pap, Kinga, Harmat, Adrienne, Németh, István, Szanyi, László, Lujber, Péter, Révész, and Imre, Gerlinger

Abstract

Copyright of Otorhinolaryngologia Hungarica / Fül-Orr-Gégegyógyászat is the property of Hungarian Society of Oto-Rhino-Laryngology, Head & Neck Surgery and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2020

11. Expression of a Malassezia Codon Optimized mCherry Fluorescent Protein in a Bicistronic Vector.

Author

Goh, Joleen P. Z., Ianiri, Giuseppe, Heitman, Joseph, and Dawson, Thomas L.

Subjects

MALASSEZIA, CHIMERIC proteins, AMINO acid sequence, CELL imaging, MUTAGENESIS, FLUORESCENT proteins, PEPTIDE antibiotics

Abstract

The use of fluorescent proteins allows a multitude of approaches from live imaging and fixed cells to labeling of whole organisms, making it a foundation of diverse experiments. Tagging a protein of interest or specific cell type allows visualization and studies of cell localization, cellular dynamics, physiology, and structural characteristics. In specific instances fluorescent fusion proteins may not be properly functional as a result of structural changes that hinder protein function, or when overexpressed may be cytotoxic and disrupt normal biological processes. In our study, we describe application of a bicistronic vector incorporating a Picornavirus 2A peptide sequence between a NAT antibiotic selection marker and mCherry. This allows expression of multiple genes from a single open reading frame and production of discrete protein products through a cleavage event within the 2A peptide. We demonstrate integration of this bicistronic vector into a model Malassezia species, the haploid strain M. furfur CBS 14141, with both active selection, high fluorescence, and proven proteolytic cleavage. Potential applications of this technology can include protein functional studies, Malassezia cellular localization, and co-expression of genes required for targeted mutagenesis. [ABSTRACT FROM AUTHOR]

Published

2020

12. Stimulation of homologous recombination in plants expressing heterologous recombinases.

Author

Barakate, Abdellah, Keir, Ewan, Oakey, Helena, and Halpin, Claire

Subjects

*PLANT fertility, *RECOMBINASES, *PLANT genes, *GENE targeting, *GENOME editing, *SILICON solar cells, *HOMOLOGOUS recombination

Abstract

Background: Current excitement about the opportunities for gene editing in plants have been prompted by advances in CRISPR/Cas and TALEN technologies. CRISPR/Cas is widely used to knock-out or modify genes by inducing targeted double-strand breaks (DSBs) which are repaired predominantly by error-prone non-homologous end-joining or microhomology-mediated end joining resulting in mutations that may alter or abolish gene function. Although such mutations are random, they occur at sufficient frequency to allow useful mutations to be routinely identified by screening. By contrast, gene knock-ins to replace entire genes with alternative alleles or copies with specific characterised modifications, is not yet routinely possible. Gene replacement (or gene targeting) by homology directed repair occurs at extremely low frequency in higher plants making screening for useful events unfeasible. Homology directed repair might be increased by inhibiting non-homologous end-joining and/or stimulating homologous recombination (HR). Here we pave the way to increasing gene replacement efficiency by evaluating the effect of expression of multiple heterologous recombinases on intrachromosomal homologous recombination (ICR) in Nicotiana tabacum plants. Results: We expressed several bacterial and human recombinases in different combinations in a tobacco transgenic line containing a highly sensitive β-glucuronidase (GUS)-based ICR substrate. Coordinated simultaneous expression of multiple recombinases was achieved using the viral 2A translational recoding system. We found that most recombinases increased ICR dramatically in pollen, where HR will be facilitated by the programmed DSBs that occur during meiosis. DMC1 expression produced the greatest stimulation of ICR in primary transformants, with one plant showing a 1000-fold increase in ICR frequency. Evaluation of ICR in homozygous T2 plant lines revealed increases in ICR of between 2-fold and 380-fold depending on recombinase(s) expressed. By comparison, ICR was only moderately increased in vegetative tissues and constitutive expression of heterologous recombinases also reduced plant fertility. Conclusion: Expression of heterologous recombinases can greatly increase the frequency of HR in plant reproductive tissues. Combining such recombinase expression with the use of CRISPR/Cas9 to induce DSBs could be a route to radically improving gene replacement efficiency in plants. [ABSTRACT FROM AUTHOR]

Published

2020

13. N6-methyladenosine modifications enhance enterovirus 71 ORF translation through METTL3 cytoplasmic distribution.

Author

Yao, Min, Dong, Yangchao, Wang, Yuan, Liu, He, Ma, Hongwei, Zhang, Hui, Zhang, Liang, Cheng, Linfeng, Lv, Xin, Xu, Zhikai, Zhang, Fanglin, Lei, Yingfeng, and Ye, Wei

Subjects

*FOOT & mouth disease, *RNA metabolism, *NUCLEAR proteins, *RNA modification & restriction, *VIRAL proteins, *POST-translational modification

Abstract

During replication, numerous viral RNAs are modified by N6-methyladenosine (m6A), the most abundant internal RNA modification. m6A is believed to regulate elements of RNA metabolism, such as splicing, stability, translation, secondary structure formation, and viral replication. In this study, we assessed the occurrence of m6A modification of the EV71 genome in human cells and revealed a preferred, conserved modification site across diverse viral strains. A single m6A modification at the 5' UTR-VP4 junction was shown to perform a protranslational function. Depletion of the METTL3 methyltransferase or treatment with 3-deazaadenosine significantly reduced EV71 replication. Specifically, METTL3 colocalized with the viral dsRNA replication intermediate in the cytoplasm during EV71 infection. As a nuclear resident protein, METTL3 relies on the binding of the nuclear import protein karyopherin to its nuclear localization signal (NLS) for nuclear translocation. We observed that EV71 2A and METTL3 share nuclear import proteins. The results of this study revealed an inner mechanism by which EV71 2A regulates the subcellular location of METTL3 to amplify its own gene expression, providing an increased understanding of RNA epitranscriptomics during the EV71 replication cycle. Proposed role of EV71 2A in regulating the nucleocytoplasmic localization of METTL3 and the dynamics of EV71 RNA m6A modification in regulating viral protein translation in cells. Upon entering the cell, the genomic ORF of EV71 is translated, and cleaved 2A can interact with the nuclear import chaperone karyopherin alpha to retain METTL3 in the cytosol and modify EV71 RNA, leading to subsequent enhancement of translation. Image 1 • The most prevalent causative enterovirus of hand, foot and mouth disease, EV71 RNA genome is m6A modified in human cells. • Enriched EV71 m6A modification peaks in human cells similar to those found in a monkey-derived cell cultured virus. • METTL3 methyltransferase binds and modify EV71 RNA, and enhanced EV71 replication. • 2A share the same karyopherin alpha subunits interaction with METTL3. [ABSTRACT FROM AUTHOR]

Published

2020

14. Evaluation of Gaussia luciferase and foot-and-mouth disease virus 2A translational interrupter chimeras as polycistronic reporters for transgene expression

Author

Michael Puckette, Thomas Burrage, John G. Neilan, and Max Rasmussen

Subjects

Gaussia luciferase, Foot-and-mouth disease virus, 2A, Bicistronic, Polycistronic, Biomarker, Biotechnology, TP248.13-248.65

Abstract

Abstract Background The Gaussia princeps luciferase is used as a stand-alone reporter of transgene expression for in vitro and in vivo expression systems due to the rapid and easy monitoring of luciferase activity. We sought to simultaneously quantitate production of other recombinant proteins by transcriptionally linking the Gaussia princeps luciferase gene to other genes of interest through the foot-and-mouth disease virus 2A translational interrupter sequence. Results We produced six plasmids, each encoding a single open reading frame, with the foot-and-mouth disease virus 2A sequence placed either N-terminal or C-terminal to the Gaussia princeps luciferase gene. Two plasmids included novel Gaussia princeps luciferase variants with the position 1 methionine deleted. Placing a foot-and-mouth disease virus 2A translational interrupter sequence on either the N- or C-terminus of the Gaussia princeps luciferase gene did not prevent the secretion or luminescence of resulting chimeric luciferase proteins. We also measured the ability of another polycistronic plasmid vector with a 2A-luciferase sequence placed downstream of the foot-and-mouth disease virus P1 and 3C protease genes to produce of foot-and-mouth disease virus-like particles and luciferase activity from transfected cells. Incorporation of the 2A-luciferase sequence into a transgene encoding foot-and-mouth disease virus structural proteins retained luciferase activity and the ability to form virus-like particles. Conclusions We demonstrated a mechanism for the near real-time, sequential, non-destructive quantitative monitoring of transcriptionally-linked recombinant proteins and a valuable method for monitoring transgene expression in recombinant vaccine constructs.

Published

2017

15. CVB3 Nonstructural 2A Protein Modulates SREBP1a Signaling via the MEK/ERK Pathway.

Author

Lei Wang, Wei Xie, Le Zhang, Defeng Li, Hua Yu, Junzhi Xiong, Jin Peng, Jing Qiu, Halei Sheng, Xiaomei He, and Kebin Zhang

Subjects

*COXSACKIEVIRUS diseases, *MYOCARDITIS, *EXTRACELLULAR signal-regulated kinases, *LIPID metabolism, *CARRIER proteins, *VIRAL replication

Abstract

Coxsackievirus B3 (CVB3) is the predominant pathogen of viral myocarditis. In our previous study, we found that CVB3 caused abnormal lipid accumulation in host cells. However, the underlying mechanisms by which CVB3 disrupts and exploits the host lipid metabolism are not well understood. Sterol regulatory element binding protein 1 (SREBP1) is the major transcriptional factor in lipogenic genes expression. In this study, we demonstrated that CVB3 infection and nonstructural 2A protein upregulated and activated SREBP1a at the transcriptional level. Deletion analysis of SREBP1a promoter revealed that two regions, -1821/-1490 and -312/+217, in this promoter were both required for its activation by 2A. These promoter regions possessed several binding motifs for transcription factor SP1. Next, we used SP1-specific small interfering RNAs (siRNAs) to confirm that SP1 might be the essential factor in SREBP1a upregulation by 2A. Furthermore, we showed that MEK/ERK pathway was involved in the activation of SREBP1a by 2A and that blocking this signaling pathway with the specific inhibitor U0126 attenuated SREBP1a activation and lipid accumulation by 2A. Finally, we showed that inhibition of SREBP1 with siRNAs attenuated lipid accumulation induced by CVB3 infection and reduced virus replication. Moreover, inhibition of the MEK/ERK pathway also led to reduction of SREBP1a activation, lipid accumulation, and virus replication during CVB3 infection. Taken together, these data demonstrate that CVB3 nonstructural 2A protein activates SREBP1a at the transcription level through a mechanism involving MEK/ERK signaling pathway and SP1 transcription factor, which promotes cellular lipid accumulation and benefits virus replication. [ABSTRACT FROM AUTHOR]

Published

2018

16. HBcrAg Levels Are Associated With Virological Response to Treatment With Interferon in Patients With Hepatitis Delta

Author

P. Lehmann, Svenja Hardtke, Benjamin Maasoumy, Michael P. Manns, Markus Cornberg, Cihan Yurdaydin, Heiner Wedemeyer, Benjamin Heidrich, Birgit Bremer, Katja Deterding, Lisa Sandmann, Yurdaydın, Cihan (ORCID 0000-0002-5419-7158 & YÖK ID 189330), Sandmann, L., Deterding, K., Heidrich, B., Hardtke, S., Lehmann, P., Bremer, B., Manns, M. P., Cornberg, M., Wedemeyer, H., Maasoumy, B., HIDIT-II Study Group, and School of Medicine

Subjects

HBsAg, medicine.medical_specialty, viruses, Placebo, medicine.disease_cause, Antiviral Agents, Gastroenterology, Virus, Viral Relapse, Hepatitis B, Chronic, Internal medicine, medicine, Humans, Adverse effect, Hepatitis B virus, Core-related antigen, B-virus, Pegylated interferon, Surface-antigen, Myrcludex B, RNA, Alpha-2A, DNA, 2A, Hepatology, Coinfection, business.industry, Standard treatment, Interferon-alpha, virus diseases, Hepatitis B, medicine.disease, Hepatitis B Core Antigens, DNA, Viral, Hepatitis Delta Virus, business

Abstract

Standard treatment of hepatitis delta virus (HDV) infection remains pegylated-interferon alfa (peg-IFN?) in most centers, which is not only associated with rather low efficacy but several adverse events. Hepatitis B core-related antigen (HBcrAg) is linked to intrahepatic covalently closed circular DNA levels and has previously been suggested as response predictor in IFN-based treatment of hepatitis B virus (HBV) mono-infection. This study aimed to investigate the value of HBcrAg in the management of patients with HBV/HDV co-infection undergoing peg-IFN? treatment. The Hep-Net-International-Delta-Hepatitis-Intervention Trial-2 study included 120 patients co-infected with HBV/HDV. Patients were treated for 96 weeks with peg-IFN? and either tenofovir or placebo. Ninety-nine patients with HDV-RNA results 24 weeks after end of treatment (FU24) were included in this analysis, of whom 32 patients (32.3%) had undetectable HDV RNA at FU24. HBcrAg was measured at baseline, week 12, 24, 48, 96, and FU24. HBcrAg levels showed no significant correlation with HDV RNA but were significantly linked to treatment outcome. HBcrAg levels < 4.5 log IU/mL at baseline, week 24, and week 48 had high negative predictive value (NPV) for achieving undetectable HDV RNA at FU24 (81.8%, 87.1% and 95.0%, respectively). Similarly, HBcrAg levels at week 96 were significantly higher in patients with viral relapse until FU24 (3.0 vs. 3.63 log IU/mL; P = 0.0089). Baseline, week 24, and week 48 HBcrAg levels were also associated with the likelihood of achieving HBsAg level < 100 IU/mL at FU24 (HBcrAg < 3.0 log IU/mL: NPV 91.7%, 90.4% and 92.3%, respectively). Test statistics improved when combining HBcrAg with additional viral and clinical parameters. Conclusion: HBcrAg is linked to treatment response to peg-IFN? in patients with HBV/HDV co-infection and could be a promising marker to determine treatment futility., Fujirebio Europe; Gilead Sciences; F. Hoffmann?La Roche; HepNet Study House

Published

2021

17. [The role of the encephalomyocarditis virus type 1 proteins L and 2A in the inhibition of the synthesis of cellular proteins and the accumulation of viral proteins during infection].

Author

Ivin YY, Butusova AA, Gladneva EE, Kolomijtseva GY, Khapchaev YK, and Ishmukhametov AA

Subjects

Humans, HeLa Cells, Capsid Proteins genetics, Mutation, Viral Proteins genetics, Viral Proteins metabolism, Encephalomyocarditis virus genetics, Encephalomyocarditis virus metabolism

Abstract

Introduction: Infection of cells with encephalomyocarditis virus type 1 (EMCV-1, Cardiovirus ) is accompanied by suppression of cellular protein synthesis. The main role in the inhibition of cellular translation is assigned to the L and 2A «security» proteins. The mechanism of the possible influence of the L protein on cellular translation is unknown. There are hypotheses about the mechanism of influence of 2A protein on the efficiency of cap-dependent translation, which are based on interaction with translation factors and ribosome subunits. However, the available experimental data are contradictory, obtained using different approaches, and do not form a unified model of the interaction between the L and 2A proteins and the cellular translation machinery.A : Picornaviridae ) is accompanied by suppression of cellular protein synthesis. The main role in the inhibition of cellular translation is assigned to the L and 2A «security» proteins. The mechanism of the possible influence of the L protein on cellular translation is unknown. There are hypotheses about the mechanism of influence of 2A protein on the efficiency of cap-dependent translation, which are based on interaction with translation factors and ribosome subunits. However, the available experimental data are contradictory, obtained using different approaches, and do not form a unified model of the interaction between the L and 2A proteins and the cellular translation machinery., Aim: To study the role of L and 2A «security» proteins in the suppression of translation of cellular proteins and the efficiency of translation and processing of viral proteins in infected cells., Materials and Methods: Mutant variants of EMCV-1 were obtained to study the properties of L and 2A viral proteins: Zfmut , which has a defective L; Δ encoding a partially deleted 2A; 2 A encoding a partially deleted 2A; Zfmut& Δ 2 A containing mutations in both proteins. Translational processes in infected cells were studied by Western-blot and the pulse method of incorporating radioactively labeled amino acids ( 14 C) into newly synthesized proteins, followed by radioautography., Results: The functional inactivation of the 2A protein does not affect the inhibition of cellular protein synthesis. A direct correlation was found between the presence of active L protein and specific inactivation of cellular protein synthesis at an early stage of viral infection. Nonspecific suppression of the translational processes of the infected cell, accompanied by phosphorylation of eIF2α, occurs at the late stage of infection. Partial removal of the 2A protein from the EMCV-1 genome does not affect the development of this process, while inactivation of the L protein accelerates the onset of complete inhibition of protein synthesis. Partial deletion of the 2A disrupts the processing of viral capsid proteins. Suppression of L protein functions leads to a decrease in the efficiency of viral translation., Conclusion: A study of the role of EMCV-1 L and 2A proteins during the translational processes of an infected cell, first performed using infectious viral pathogens lacking active L and 2A proteins in one experiment, showed that 2A protein is not implicated in the inhibition of cellular translation in HeLa cells; L protein seems to play an important role not only in the specific inhibition of cellular translation but also in maintaining the efficient synthesis of viral proteins; 2A protein is involved not only in primary but also in secondary processing of EMCV-1 capsid proteins.

Published

2023

18. Synthesis, Docking Studies and Pharmacological Evaluation of Serotoninergic Ligands Containing a 5-Norbornene-2-Carboxamide Nucleus

Author

Rosa Sparaco, Ewa Kędzierska, Agnieszka A. Kaczor, Anna Bielenica, Elisa Magli, Beatrice Severino, Angela Corvino, Ewa Gibuła-Tarłowska, Jolanta H. Kotlińska, Giorgia Andreozzi, Paolo Luciano, Elisa Perissutti, Francesco Frecentese, Marcello Casertano, Anna Leśniak, Magdalena Bujalska-Zadrożny, Małgorzata Oziębło, Raffaele Capasso, Vincenzo Santagada, Giuseppe Caliendo, Ferdinando Fiorino, Sparaco, R., Kedzierska, E., Kaczor, A. A., Bielenica, A., Magli, E., Severino, B., Corvino, A., Gibula-Tarlowska, E., Kotlinska, J. H., Andreozzi, G., Luciano, P., Perissutti, E., Frecentese, F., Casertano, M., Lesniak, A., Bujalska-Zadrozny, M., Ozieblo, M., Capasso, R., Santagada, V., Caliendo, G., and Fiorino, F.

Subjects

5-norbornene-2-carboxilic acid, Organic Chemistry, and 5-HT, 5-HT, Pharmaceutical Science, Ligands, arylpiperazine derivative, Norbornanes, Analytical Chemistry, serotonin, Molecular Docking Simulation, Structure-Activity Relationship, receptor ligand, Chemistry (miscellaneous), Receptors, Serotonin, Drug Discovery, Receptor, Serotonin, 5-HT1A, Molecular Medicine, arylpiperazine derivatives, 5-HT1A, 5-HT2A and 5-HT2C receptor ligands, Physical and Theoretical Chemistry, 1A, Piperazine, 2A, 2C

Abstract

A new series of 5-norbornene-2-carboxamide derivatives was prepared and their affinities to the 5-HT1A, 5-HT2A, and 5-HT2C receptors were evaluated and compared to a previously synthesized series of derivatives characterized by exo-N-hydroxy-5-norbornene-2,3-dicarboximidenucleus, in order to identify selective ligands for the above-mentioned subtype receptors. Arylpiperazines represents one of the most important classes of 5-HT1AR ligands, and recent research concerning new derivatives has been focused on the modification of one or more portions of such pharmacophore. The combination of structural elements (heterocyclic nucleus, propyl chain and 4-substituted piperazine), known to be critical to the affinity to 5-HT1A receptors, and the proper selection of substituents led to compounds with high specificity and affinity towards serotoninergic receptors. The most active compounds were selected for further in vivo assays to determine their functional activity. Finally, to rationalize the obtained results, molecular docking studies were performed. The results of the pharmacological studies showed that Norbo-4 and Norbo-18 were the most active and promising derivatives for the serotonin receptor considered in this study.

Published

2022

19. Advanced multigene expression system for Nannochloropsis salina using 2A self-cleaving peptides.

Author

Koh, Hyun Gi, Kang, Nam Kyu, Kim, Eun Kyung, Jeon, Seungjib, Shin, Sung-Eun, Lee, Bongsoo, and Chang, Yong Keun

Subjects

*PEPTIDES, *MICROALGAE, *GENE expression, *PROMOTERS (Genetics), *GENETIC engineering, *ALGAE

Abstract

Even though there has been much interest in genetic engineering of microalgae, its progress has been slow due to the difficulty and limitation of available techniques. Currently, genetic modification in most microalgal strains is confined to single gene transformation. Here, a multigene expression system for the oleaginous model strain Nannochloropsis salina was developed with glycine-serine-glycine spacer linked 2A self-cleaving peptides (2A) for the first time. An efficiency test of the four most widely used 2As revealed that two different types of 2As T2A and E2A have the best performance in N. salina with a maximum cleavage rate of nearly 45%. The system was able to express the linked sequence of the selection marker sh ble and the fluorescence protein sfCherry with intact functions. Because 2A enabled multigene expression in the single cassette form, the use of 2A also reduced the vector size, which along with the stronger promoter resulted in a 9-fold increase in the transformation efficiency. Furthermore, confirmative screening accuracy of more than 90% was observed. Hence, the 2A applied vector system is expected to be beneficial in microalgal research field because it enables multigene expression as well as offering improved transformation and screening efficiency. [ABSTRACT FROM AUTHOR]

Published

2018

20. Production of foot-and-mouth disease virus capsid proteins by the TEV protease.

Author

Puckette, Michael, Smith, Justin D., Gabbert, Lindsay, Schutta, Christopher, Barrera, José, Clark, Benjamin A., Neilan, John G., and Rasmussen, Max

Subjects

*FOOT & mouth disease virus, *VIRAL proteins, *PROTEOLYTIC enzymes, *PROTEIN precursors, *PROTEIN expression

Abstract

Protective immunity to viral pathogens often includes production of neutralizing antibodies to virus capsid proteins. Many viruses produce capsid proteins by expressing a precursor polyprotein and related protease from a single open reading frame. The foot-and-mouth disease virus (FMDV) expresses a 3C protease (3Cpro) that cleaves a P1 polyprotein intermediate into individual capsid proteins, but the FMDV 3Cpro also degrades many host cell proteins and reduces the viability of host cells, including subunit vaccine production cells. To overcome the limitations of using the a wild-type 3Cpro in FMDV subunit vaccine expression systems, we altered the protease restriction sequences within a FMDV P1 polyprotein to enable production of FMDV capsid proteins by the Tobacco Etch Virus NIa protease (TEVpro). Separate TEVpro and modified FMDV P1 proteins were produced from a single open reading frame by an intervening FMDV 2A sequence. The modified FMDV P1 polyprotein was successfully processed by the TEVpro in both mammalian and bacterial cells. More broadly, this method of polyprotein production and processing may be adapted to other recombinant expression systems, especially plant-based expression. [ABSTRACT FROM AUTHOR]

Published

2018

21. Immunogenicity of a secreted, C-terminally truncated, form of bovine viral diarrhea virus E2 glycoprotein as a potential candidate in subunit vaccine development

Author

Lo, Yi Ting, Ryan, Martin Denis, Luke, Garry Alec, Chang, Wan Chen, Wu, Hsing Chieh, BBSRC, and University of St Andrews. School of Biology

Subjects

MCC, QR355, RM, Multidisciplinary, QH301 Biology, Subunit vaccines, DAS, RM Therapeutics. Pharmacology, QH301, E2, SDG 3 - Good Health and Well-being, Glycoprotein, 2A, QR355 Virology, BVDV

Abstract

Funding: This work was supported by the Taiwan Ministry of Science and Technology [MOST-106-2911-I-020-501; MOST-107-2313-B-020-011-MY3] and the UK Biotechnology and Biological Sciences Research Council [BB/P025080/1]. Both current live, attenuated, and killed virus vaccines for bovine viral diarrhea virus (BVDV) have their limitations. Here, we report the development of a BVDV subunit vaccine by (i) the expression of a secreted form of a recombinant E2 glycoprotein using BHK21 cells and (ii) determination of the immune responses in mice. The E2 glycoprotein was modified by deletion of the C-terminal transmembrane anchor domain and fusion to a V5 epitope tag. This allowed detection using anti-V5 monoclonal antibodies together with simple purification of the expressed, secreted, form of E2 from the cell media. Furthermore, we genetically fused green fluorescent protein (GFP) linked to E2 via a Thosea asigna virus 2A (T2A) ribosome skipping sequence thereby creating a self-processing polyprotein [GFP-T2A-BVDV-E2trunk-V5], producing discrete [GFP-T2A] and [E2trunk-V5] translation products: GFP fluorescence acts, therefore, as a surrogate marker of E2 expression, BALB/c mice were inoculated with [E2trunk-V5] purified from cell media and both humoral and cellular immune responses were observed. Our antigen expression system provides, therefore, both (i) a simple antigen purification protocol together with (ii) a feasible strategy for further, large-scale, production of vaccines. Publisher PDF

Published

2022

22. Connectivity Mapping Using a Novel sv2a Loss-of-Function Zebrafish Epilepsy Model as a Powerful Strategy for Anti-epileptic Drug Discovery

Author

Yifan Zhang, Lise Heylen, Michèle Partoens, James D. Mills, Rafal M. Kaminski, Patrice Godard, Michel Gillard, Peter A. M. de Witte, and Aleksandra Siekierska

Subjects

Science & Technology, SV2A, GENE-EXPRESSION SIGNATURES, LEVETIRACETAM, SYNAPTIC VESICLE PROTEIN, Neurosciences, INHIBITION, BINDING CHARACTERISTICS, zebrafish, HUMAN BRAIN, Cellular and Molecular Neuroscience, connectivity mapping (CMap), epilepsy, RAT, SEIZURES, Neurosciences & Neurology, LIGAND, Molecular Biology, Life Sciences & Biomedicine, 2A

Abstract

Synaptic vesicle glycoprotein 2A (SV2A) regulates action potential-dependent neurotransmitter release and is commonly known as the primary binding site of an approved anti-epileptic drug, levetiracetam. Although several rodent knockout models have demonstrated the importance of SV2A for functional neurotransmission, its precise physiological function and role in epilepsy pathophysiology remains to be elucidated. Here, we present a novel sv2a knockout model in zebrafish, a vertebrate with complementary advantages to rodents. We demonstrated that 6 days post fertilization homozygous sv2a–/– mutant zebrafish larvae, but not sv2a+/– and sv2a+/+ larvae, displayed locomotor hyperactivity and spontaneous epileptiform discharges, however, no major brain malformations could be observed. A partial rescue of this epileptiform brain activity could be observed after treatment with two commonly used anti-epileptic drugs, valproic acid and, surprisingly, levetiracetam. This observation indicated that additional targets, besides Sv2a, maybe are involved in the protective effects of levetiracetam against epileptic seizures. Furthermore, a transcriptome analysis provided insights into the neuropathological processes underlying the observed epileptic phenotype. While gene expression profiling revealed only one differentially expressed gene (DEG) between wildtype and sv2a+/– larvae, there were 4386 and 3535 DEGs between wildtype and sv2a–/–, and sv2a+/– and sv2a–/– larvae, respectively. Pathway and gene ontology (GO) enrichment analysis between wildtype and sv2a–/– larvae revealed several pathways and GO terms enriched amongst up- and down-regulated genes, including MAPK signaling, synaptic vesicle cycle, and extracellular matrix organization, all known to be involved in epileptogenesis and epilepsy. Importantly, we used the Connectivity map database to identify compounds with opposing gene signatures compared to the one observed in sv2a–/– larvae, to finally rescue the epileptic phenotype. Two out of three selected compounds rescued electrographic discharges in sv2a–/– larvae, while negative controls did not. Taken together, our results demonstrate that sv2a deficiency leads to increased seizure vulnerability and provide valuable insight into the functional importance of sv2a in the brain in general. Furthermore, we provided evidence that the concept of connectivity mapping represents an attractive and powerful approach in the discovery of novel compounds against epilepsy.

Published

2022

23. Evaluation of Gaussia luciferase and foot-and- mouth disease virus 2A translational interrupter chimeras as polycistronic reporters for transgene expression.

Author

Puckette, Michael, Burrage, Thomas, Neilan, John G., and Rasmussen, Max

Subjects

*FOOT & mouth disease, *LUCIFERASES, *CHIMERISM, *TRANSGENE expression, *RECOMBINANT proteins

Abstract

Background: The Gaussia princeps luciferase is used as a stand-alone reporter of transgene expression for in vitro and in vivo expression systems due to the rapid and easy monitoring of luciferase activity. We sought to simultaneously quantitate production of other recombinant proteins by transcriptionally linking the Gaussia princeps luciferase gene to other genes of interest through the foot-and-mouth disease virus 2A translational interrupter sequence. Results: We produced six plasmids, each encoding a single open reading frame, with the foot-and-mouth disease virus 2A sequence placed either N-terminal or C-terminal to the Gaussia princeps luciferase gene. Two plasmids included novel Gaussia princeps luciferase variants with the position 1 methionine deleted. Placing a foot-and-mouth disease virus 2A translational interrupter sequence on either the N- or C-terminus of the Gaussia princeps luciferase gene did not prevent the secretion or luminescence of resulting chimeric luciferase proteins. We also measured the ability of another polycistronic plasmid vector with a 2A-luciferase sequence placed downstream of the foot-and-mouth disease virus P1 and 3C protease genes to produce of foot-and-mouth disease virus-like particles and luciferase activity from transfected cells. Incorporation of the 2A-luciferase sequence into a transgene encoding foot-and-mouth disease virus structural proteins retained luciferase activity and the ability to form virus-like particles. Conclusions: We demonstrated a mechanism for the near real-time, sequential, non-destructive quantitative monitoring of transcriptionally-linked recombinant proteins and a valuable method for monitoring transgene expression in recombinant vaccine constructs. [ABSTRACT FROM AUTHOR]

Published

2017

24. Differential Disruption of Nucleocytoplasmic Trafficking Pathways by Rhinovirus 2A Proteases.

Author

Watters, Kelly, Inankur, Bahar, Gardiner, Jaye C., Warrick, Jay, Sherer, Nathan M., Yin, John, and Palmenberg, Ann C.

Subjects

*COMMON cold treatments, *NUCLEOCYTOPLASMIC interactions, *PROTEOLYTIC enzymes, *RNA viruses, *VIRAL proteins

Abstract

The RNA rhinoviruses (RV) encode 2A proteases (2Apro) that contribute essential polyprotein processing and host cell shutoff functions during infection, including the cleavage of Phe/Gly-containing nucleoporin proteins (Nups) within nuclear pore complexes (NPC). Within the 3 RV species, multiple divergent genotypes encode diverse 2Apro sequences that act differentially on specific Nups. Since only subsets of Phe/Gly motifs, particularly those within Nup62, Nup98, and Nup153, are recognized by transport receptors (karyopherins) when trafficking large molecular cargos through the NPC, the processing preferences of individual 2Apro predict RV genotype-specific targeting of NPC pathways and cargos. To test this idea, transformed HeLa cell lines were created with fluorescent cargos (mCherry) for the importin α/β, transportin 1, and transportin 3 import pathways and the Crm1-mediated export pathway. Live-cell imaging of single cells expressing recombinant RV 2Apro (A16, A45, B04, B14, B52, C02, and C15) showed disruption of each pathway with measurably different efficiencies and reaction rates. The B04 and B52 proteases preferentially targeted Nups in the import pathways, while B04 and C15 proteases were more effective against the export pathway. Virus-type-specific trends were also observed during infection of cells with A16, B04, B14, and B52 viruses or their chimeras, as measured by NF-B (p65/Rel) translocation into the nucleus and the rates of virus-associated cytopathic effects. This study provides new tools for evaluating the host cell response to RV infections in real time and suggests that differential 2Apro activities explain, in part, strain-dependent host responses and diverse RV disease phenotypes. [ABSTRACT FROM AUTHOR]

Published

2017

25. Synthesis and anti-tumor properties of derivatives [4- (41-chlorophenyl)-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[c,d]azulen-1-yl-metil]-para-tolylamine

Author

Yu. A. Fedchenkova, G. P. Potebnia, О. V. Моsкаlеnко, S. A. Demchenko, V. V. Sukhoveev, and A. M. Demchenko

Subjects

Antitumor activity, 8-tetrahydro-2, antitumor properties, lcsh:RM1-950, leukemia, lcsh:RS1-441, d]azulen-1-yl-metil]-para-tolylamine, Medicinal chemistry, derivatives of [4-(41-chlorophenyl)-5, lcsh:Pharmacy and materia medica, lcsh:Therapeutics. Pharmacology, 5-fluorouracil, 8a-triaza¬cyclopenta[c, 2a

Abstract

Leukemia, as a part of hemoblastosises, is a malignant blood system disease, which is characterized by bone marrow damage, caused by leukemic stem cells, which appear due to disruption of self-renewal and differentiation of hempoetic stem cells and predecessor cells. In their turn, hemoblastoses are divided into two groups: bone marrow (acute leukemia, chronical leukemia, paraproteinemic hemoblastoses) and outside bone marrow (lymphogranulomatosis, or Hodgkin lymphoma, and non-Hodgkin malignant mymphomas). Nowadays in Ukraine, different kinds of leukemia are cured by various drugs, which have many side effects. Increase in effectivity of chemotherapy of tumor disease is primarily related to creation of new antitumor drugs of selective action. Which is why search for biologically active compounds with antitumor activity is a perspective direction in creation of new drugs. Aim of this work was synthesis of compounds with potential antitumor properties in a variety of [4-(41-chlorophenyl)-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[c,d]-azulen-1-yl-methyl]-para-tolylamin derivatives. As the objects of our studies, we have picked the derivatives of [4-(41-chlorophenyl)-5,6,7,8-tetrahydro-2,2а,8а-triazacyclopenta[c,d]-azulen-1-yl-methyl]-para-tolilamin (8 and 10 a, b). [4-(41-Chlorphenyl)-5,6,7,8-tetrahydro-2,2а,8а-triazacyclopenta[c,d]azulen-1-yl-methyl]-para-tolylamin (8) was obtained by boiling of equimolar quantities of 3-(41-methylphenyl)aminomethyl-6,7,8,9-tetrahydro-5Н-[1,2,4]triazolo[4,3-a]azepin (5) and α-brom-4-chloracetophenon in ethylacetate. Thioamides (10 a, b) were obtained by interaction of amin (8) with corresponding arylisothiocyanates (9 а, b) in dry benzene. Antitumor activity of [4-(41-chlorphenyl)-5,6,7,8-tetrahydro-2,2а,8а-triazacyclopenta[c,d]azulen-1-yl-methyl]-para-tolylamin (8) was studied in National Cancer Institute of Health, USA within Development Therapeutic Program. In experimental conditions [4-(41-chlorphenyl)-5,6,7,8-tetrahydro-2,2а,8а-triazacyclopenta[c,d]azulen-1-yl-methyl]-para-tolylamin (8) showed ability to inhibit growth of cancerous leukemia cells of CCRF-CEM, HL-60(TB), K-562, MOLT-4, RPMI-8226 and SR lines, higher than standard – 5-fluorouracil. Towards HL-60(TB) cells [4-(41-chlorphenyl)-5,6,7,8-tetrahydro-2,2а,8а- triazacyclopenta[c,d]azulen-1-yl-methyl]-para-tolylamin exceeds standard in effectivity by 64.68%. For K-562, MOLT-4, RPMI-8226 and SR cells, those numbers are equal to: 85.88%, 84.95%, 42.10% and 36.82% correspondingly. Towards CCRF-CEM cells, this compound not only inhibits cell growth and division, but also destroys them by 20.34%. Thus conducted studies confirm perceptivity of search for compounds with antitumor action on the basis of [4-(41-chlorophenyl)-5,6,7,8-tetrahydro-2,2а,8а-triazacyclopenta[c,d]azulen-1-yl­methyl]-para-tolylamin.

Published

2020

26. Pulsed Electromagnetic Fields: A Novel Attractive Therapeutic Opportunity for Neuroprotection After Acute Cerebral Ischemia

Author

Fioravante Capone, Micaela Liberti, Fabrizio Vincenzi, Giorgio Aicardi, Simona Salati, Francesca Apollonio, Vincenzo Di Lazzaro, Katia Varani, Ruggero Cadossi, Capone F., Salati S., Vincenzi F., Liberti M., Aicardi G., Apollonio F., Varani K., Cadossi R., and Di Lazzaro V.

Subjects

acute ischemic stroke, Adenosine, Ischemia, Socio-culturale, Neuroprotection, Brain Ischemia, Brain ischemia, Electromagnetic Fields, medicine, Animals, adenosine receptor, 2A, Stroke, Ischemic Stroke, biophysical stimulation, business.industry, Penumbra, Receptors, Purinergic P1, General Medicine, medicine.disease, Adenosine receptor, adenosine receptors, Anesthesiology and Pain Medicine, Neurology, A2A adenosine receptors, Infarction, Adjunctive treatment, neuroprotection, Neurology (clinical), pulsed electromagnetic fields, business, Neuroscience, medicine.drug

Abstract

Objectives Acute cerebral ischemia is characterized by several pathological processes evolving during time, which contribute to the final tissue damage. Secondary processes, such as prolonged inflammatory response, impaired mitochondrial function and oxidative stress, are responsible for the progression of brain injury to the peri-infarct area, called "penumbra." Adenosine has been shown to play a crucial role in regulating the inflammatory cascade following brain ischemia. Pulsed electromagnetic fields (PEMFs) act as modulators of adenosine receptors, increasing the functionality of the endogenous adenosine. In particular, PEMF exposure induces a significant upregulation of A2A and A3 adenosine receptors in different neuronal cell types. Several lines of evidence suggest that PEMF exposure might play a neuroprotective role after ischemic damage. Materials and methods This review summarizes the current knowledge on the mechanism of action of PEMFs and their biological effects on neuronal damage both in preclinical and clinical studies. Results PEMFs counteract hypoxia-induced apoptosis and ROS production in neuronal-like cells and exert a strong anti-inflammatory effect on microglial cells. Data from stroke animal models showed that PEMFs exposure is able to reduce the size of the infarct area and decrease the levels of pro-inflammatory mediators. In clinical studies, PEMFs stimulation proved to be safe and well tolerated. Preliminary results on acute ischemic stroke patients showed a dose-dependent reduction in the lesion size. Conclusions Altogether, these data demonstrate the efficacy of PEMFs against several mechanisms underlying ischemic damage and suggest that PEMFs might represent a novel noninvasive adjunctive treatment for acute ischemic stroke, providing neuroprotection and reducing functional deficits following ischemia.

Published

2022

27. Synthesis and antiviral properties derivatives of 1-(para-tolyl)-4-aryl-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulene-3-carbothioic acid arylamides

Author

A. M. Demchenko, Yu. A. Fedchenkova, V. V. Sukhoveev, А. М. Іvаsеnко, and S. A. Demchenko

Subjects

Element analysis, 8-tetrahydro-2, ribavirin, Aryl, lcsh:RM1-950, lcsh:RS1-441, Nuclear magnetic resonance spectroscopy, Influenza pandemic, Azulene, Medicinal chemistry, Virus, amizone, lcsh:Pharmacy and materia medica, chemistry.chemical_compound, lcsh:Therapeutics. Pharmacology, chemistry, derivatives of 5, antiviral activity, 2a, 8a-triazacyclopenta[cd]azulene-3-carbothioic acid

Abstract

Nowadays, H1N1 – strain of so called «swine» or «mexican» subspecie A virus, which is still not studied, and which spreads through aerosol and contact is known to many world countries. Significant number of lethal cases during influenza pandemic season in Ukraine was observed. It should be noted, that patients went to the hospitals in very severe cases, which is why registered daily lethality is in 31,6% of cases. Everything listed above had made it necessary to conduct preventive measures on global and national levels. One of such measures is creation of new direct action medicinal agents. The goal of this work was the synthesis of compounds with potential antiviral properties in variety of 5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid derivatives. We have chosen derivatives of 5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid (6 a–e and 7 a–h), which were synthesized by boiling of 1-(para-tolyl)-4-aryl-5,6,7,8-tetrahydro-2,2a,4a-triazacyclopenta[cd]azulenes (5a or 5b) with corresponding arylisothiocyanates in dry benzene. Antiviral activity of phenylamid 1-(para-tolyl)-4-phenyl-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid against Flu A H1N1 California/07/2009 was researched in Southern Research Institute – SRI, Birmingham, Alabama). Variety of new derivatives of 5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid. Composition and structure of all synthesized compounds are proven by data of element analysis and 1Н NMR spectroscopy. In conducted researches of antiviral activity of phenylamide 1-(para-tolyl)-4-phenyl-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid against Flu A H1N1 California/07/2009, it was found out, that synthesized compound shows pronounced antiviral activity, compared to reference medicinal agents Ribavirin and Amizon. Therefore, conducted researches confirm perspective of development of a new domestic medicinal agent with antiviral activity, based on derivatives of 5,6,7,8,-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulen-3-carbotionic acid.

Published

2019

28. Abusos y condiciones de servidumbre relacionados con la implementación de los programas de trabajadores huéspedes (el caso tamaulipeco)

Author

Simón Pedro Izcara Palacios

Subjects

visas h, 2a, migración, jornaleros, contratos laborales, tamaulipas, Urban groups. The city. Urban sociology, HT101-395, Social sciences (General), H1-99

Abstract

Las visas H-2A para trabajadores agrarios temporales son muy controvertidas. Así, los grupos defensores de los jornaleros han argumentado que éstas no protegen a la mano de obra estadounidense y propician el abuso y la explotación de los trabajadores foráneos. Tamaulipas presenta una larga tradición de emigración de su población rural a Estados Unidos en busca de empleos agrarios. La preferencia de los empleadores estadounidenses por los jornaleros tamaulipecos se debe a la cercanía de Tamaulipas con la frontera estadounidense, que abarata los costos de transporte, y a la experiencia de los jornaleros tamaulipecos en la realización de actividades muy demandantes físicamente, como la pizca de la naranja. Este artículo analiza el nivel de cumplimiento de los contratos laborales de los trabajadores tamaulipecos que emigran a Estados Unidos con visas temporales H-2A para trabajar en la agricultura.

Published

2010

29. '2A-Like' Signal Sequences Mediating Translational Recoding: A Novel Form of Dual Protein Targeting.

Author

Roulston, Claire, Luke, Garry A., Felipe, Pablo, Ruan, Lin, Cope, Jonathan, Nicholson, John, Sukhodub, Andriy, Tilsner, Jens, and Ryan, Martin D.

Subjects

*SIGNAL peptides, *AMINO acid sequence, *OLIGOPEPTIDES, *POLYPEPTIDES, *CHEMICAL synthesis, *EXOCYTOSIS, *CYTOPLASM

Abstract

We report the initial characterization of an N-terminal oligopeptide '2A-like' sequence that is able to function both as a signal sequence and as a translational recoding element. Owing to this translational recoding activity, two forms of nascent polypeptide are synthesized: (i) when 2A-mediated translational recoding has not occurred: the nascent polypeptide is fused to the 2A-like N-terminal signal sequence and the fusion translation product is targeted to the exocytic pathway, and, (ii) a translation product where 2A-mediated translational recoding has occurred: the 2A-like signal sequence is synthesized as a separate translation product and, therefore, the nascent (downstream) polypeptide lacks the 2A-like signal sequence and is localized to the cytoplasm. This type of dual-functional signal sequence results, therefore, in the partitioning of the translation products between the two sub-cellular sites and represents a newly described form of dual protein targeting. [ABSTRACT FROM AUTHOR]

Published

2016

30. Real-Time Temporal Dynamics of Bicistronic Expression Mediated by Internal Ribosome Entry Site and 2A Cleaving Sequence

Author

Lee, Soomin, Kim, Jeong-Ah, Kim, Hee-Dae, Chung, Sooyoung, Kim, Kyungjin, and Choe, Han Kyoung

Subjects

Gene Expression Regulation, Viral, Models, Molecular, Teschovirus, internal ribosome entry site, Genetic Vectors, Green Fluorescent Proteins, Articles, expression dynamics, Internal Ribosome Entry Sites, Luminescent Proteins, Mice, HEK293 Cells, real-time fluorescent imaging, multicistronic elements, Animals, Humans, Encephalomyocarditis virus, 2A

Abstract

Multicistronic elements, such as the internal ribosome entry site (IRES) and 2A-like cleavage sequence, serve crucial roles in the eukaryotic ectopic expression of exogenous genes. For utilization of multicistronic elements, the cleavage efficiency and order of elements in multicistronic vectors have been investigated; however, the dynamics of multicistronic element-mediated expression remains unclear. Here, we investigated the dynamics of encephalomyocarditis virus (EMCV) IRES- and porcine teschovirus-1 2A (p2A)-mediated expression. By utilizing real-time fluorescent imaging at a minute-level resolution, we monitored the expression of fluorescent reporters bridged by either EMCV IRES or p2A in two independent cultured cell lines, HEK293 and Neuro2a. We observed significant correlations for the two fluorescent reporters in both multicistronic elements, with a higher correlation coefficient for p2A in HEK293 but similar coefficients for IRES-mediated expression and p2A-mediated expression in Neuro2a. We further analyzed the causal relationship of multicistronic elements by convergent cross mapping (CCM). CCM revealed that in all four conditions examined, the expression of the preceding gene causally affected the dynamics of the subsequent gene. As with the cross correlation, the predictive skill of p2A was higher than that of IRES in HEK293, while the predictive skills of the two multicistronic elements were indistinguishable in Neuro2a. To summarize, we report a significant temporal correlation in both EMCV IRES- and p2A-mediated expression based on the simple bicistronic vector and real-time fluorescent monitoring. The current system also provides a valuable platform to examine the dynamic aspects of expression mediated by diverse multicistronic elements under various physiological conditions.

Published

2019

31. Experimental Evidence of A2A–D2 Receptor–Receptor Interactions in the Rat and Human Carotid Body

Author

Elena Stocco, Maria Martina Sfriso, Giulia Borile, Martina Contran, Silvia Barbon, Filippo Romanato, Veronica Macchi, Diego Guidolin, Raffaele De Caro, and Andrea Porzionato

Subjects

dopamine D2 receptors, Physiology, in situ PLA, receptors, type I cells, Adenosine A2A receptor, Proximity ligation assay, lcsh:Physiology, Physiology (medical), Dopamine receptor D2, heterodimes, medicine, adenosine A, 2A, carotid body, dopamine D, 2, Receptor, lcsh:QP1-981, Tyrosine hydroxylase, Chemistry, adenosine A2A receptors, Colocalization, Intermittent hypoxia, Cell biology, medicine.anatomical_structure, Carotid body

Abstract

Adenosine A2A receptors (A2AR) and dopamine D2 receptors (D2R) are known to be involved in the physiological response to hypoxia, and their expression/activity may be modulated by chronic sustained or intermittent hypoxia. To date, A2AR and D2R can form transient physical receptor–receptor interactions (RRIs) giving rise to a dynamic equilibrium able to influence ligand binding and signaling, as demonstrated in different native tissues and transfected mammalian cell systems. Given the presence of A2AR and D2R in type I cells, type II cells, and afferent nerve terminals of the carotid body (CB), the aim of this work was to demonstrate here, for the first time, the existence of A2AR–D2R heterodimers by in situ proximity ligation assay (PLA). Our data by PLA analysis and tyrosine hydroxylase/S100 colocalization indicated the formation of A2AR–D2R heterodimers in type I and II cells of the CB; the presence of A2AR–D2R heterodimers also in afferent terminals is also suggested by PLA signal distribution. RRIs could play a role in CB dynamic modifications and plasticity in response to development/aging and environmental stimuli, including chronic intermittent/sustained hypoxia. Exploring other RRIs will allow for a broad comprehension of the regulative mechanisms these interactions preside over, with also possible clinical implications.

Published

2021

32. Improved and versatile viral 2 A platforms for dependable and inducible high-level expression of dicistronic nuclear genes in Chlamydomonas reinhardtii.

Author

Plucinak, Thomas M., Horken, Kempton M., Jiang, Wenzhi, Fostvedt, Jessica, Nguyen, Sanh Tan, and Weeks, Donald P.

Subjects

*GENE expression in plants, *CHLAMYDOMONAS reinhardtii, *BIOMARKERS, *PLANTS, *PLANT genes, *PEPTIDES, *CONFOCAL fluorescence microscopy

Abstract

A significantly improved viral 2A peptide system for dependable high-level expression of dicistronic genes in Chlamydomonas reinhardtii has been developed. Data are presented demonstrating that use of an especially proficient 'extended FMDV 2A' coding region allows production of two independent protein products from a dicistronic gene with almost complete efficiency. Importantly, results are also presented that demonstrate the utility of this 2A system for efficient high-level expression of foreign genes in C. reinhardtii, which has not previously been reliably achievable in this algal model system. To expand the versatility of the 2A expression system, a number of commonly used selectable marker proteins were assessed for their compatibility with the extended FMDV 2A peptide. Additional experiments demonstrate the feasibility and utility of 2A-containing dicistronic systems that rely on a strong conditional promoter for transcriptional control and a low-expression marker gene for selection. This strategy allows easy and efficient delivery of genes of interest whose expression levels require regulation either to mitigate potential toxicity or allow differential expression under controlled experimental conditions. Finally, as an additional practical demonstration of the utility of the extended FMDV 2A system, confocal fluorescence microscopy is used to demonstrate that native and foreign proteins of interest bearing post-translational remnants of the extended FMDV 2A peptide localize correctly to various cellular compartments, including a striking demonstration of the almost exclusive localization of the Rubisco small subunit protein to the pyrenoid of the C. reinhardtii chloroplast in cells maintained under ambient CO2 concentrations. [ABSTRACT FROM AUTHOR]

Published

2015

33. Replication-competent influenza A viruses expressing a red fluorescent protein.

Author

Nogales, Aitor, Baker, Steven F., and Martínez-Sobrido, Luis

Subjects

*VIRAL disease treatment, *VIRAL replication, *INFLUENZA A virus, *FLUORESCENT proteins, *IN vitro studies, *LABORATORY mice

Abstract

Like most animal viruses, studying influenza A in model systems requires secondary methodologies to identify infected cells. To circumvent this requirement, we describe the generation of replication-competent influenza A red fluorescent viruses. These influenza A viruses encode mCherry fused to the viral non-structural 1 (NS1) protein and display comparable growth kinetics to wild-type viruses in vitro . Infection of cells with influenza A mCherry viruses was neutralized with monoclonal antibodies and inhibited with antivirals to levels similar to wild-type virus. Influenza A mCherry viruses were also able to lethally infect mice, and strikingly, dose- and time-dependent kinetics of viral replication were monitored in whole excised mouse lungs using an in vivo imaging system (IVIS). By eliminating the need for secondary labeling of infected cells, influenza A mCherry viruses provide an ideal tool in the ongoing struggle to better characterize the virus and identify new therapeutics against influenza A viral infections. [ABSTRACT FROM AUTHOR]

Published

2015

34. The silent point mutations at the cleavage site of 2A/2B have no effect on the self-cleavage activity of 2A of foot-and-mouth disease virus.

Author

Gao, Zong-liang, Zhou, Jian-hua, Zhang, Jie, Ding, Yao-zhong, and Liu, Yong-sheng

Subjects

*FOOT & mouth disease, *VIRUS diseases, *POINT mutation (Biology), *AMINO acids, *NUCLEOTIDE sequence

Abstract

The 2A region of the foot-and-mouth disease virus (FMDV) polyprotein is 18 amino acids in length, and 2A self-cleavage site (2A/2B) contains a conserved amino acid motif G 2A /P 2B . To investigate the synonymous codon usage for Glycine at the 2A/2B cleavage site of FMDV, 66 2A/2B 1 nucleotide sequences were aligned and found that the synonymous codon usage of G 2A is conserved and GGG was the most frequently used. To examine the role of synonymous codons for G 2A in self-cleavage efficiency of 2A/2B, recombinant constructs which contains the chloramphenicol acetyltransferase protein (CAT) and enhanced green fluorescent protein (EGFP) linked by the FMDV 2A sequence with four synonymous codons for G 2A were produced. The activities of all the F2As based plasmids were determined in CHO cells. The results showed that the synonymous codon usage patterns for G 2A at the cleavage site (2A/2B) have no effect on the cleavage efficiency. This suggests that the synonymous codon usage of 2A peptide has no effect on the cleavage efficiency of FMDV 2A element. [ABSTRACT FROM AUTHOR]

Published

2014

35. Targeting adenosine receptor by polydeoxyribonucleotide: An effective therapeutic strategy to induce white-to-brown adipose differentiation and to curb obesity

Author

Violetta Squadrito, Domenica Altavilla, Giovanni Pallio, Federica Mannino, Francesco Squadrito, Domenico Antonio Giorgi, Natasha Irrera, Alessandra Bitto, Letteria Minutoli, Vincenzo Arcoraci, and Igor Pirrotta

Subjects

0301 basic medicine, medicine.medical_specialty, Ucp1, adipocytes, Pharmaceutical Science, Adipose tissue, White adipose tissue, Article, A2A receptor, 2A, receptor, Adipocytes, Browning process, Polydeoxyribonucleotide, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Pharmacy and materia medica, Adipocyte, Internal medicine, Lipid droplet, Drug Discovery, Brown adipose tissue, medicine, Oil Red O, PRDM16, Adiponectin, browning process, RS1-441, 030104 developmental biology, Endocrinology, medicine.anatomical_structure, chemistry, Molecular Medicine, Medicine, polydeoxyribonucleotide, 030217 neurology & neurosurgery

Abstract

Obesity is a worldwide chronic metabolic disease characterized by an abnormal fat accumulation and represents one of the main risk factors for several diseases. White adipose tissue is the primary site for energy storage in the form of triglycerides, whereas brown adipose tissue does not store energy-providing lipids but rather dissipates it by producing heat. White-to-brown adipocyte trans-differentiation could represent a new target of anti-obesity strategies and result in fat reduction. Previous studies indicated that adenosine receptor activation induces trans-differentiation of white adipocytes to brown adipocytes. The aim of this study was to evaluate the effects of polydeoxyribonucleotide (PDRN), an A2Ar receptor agonist, in an in vitro model of browning. Mouse 3T3-L1 pre-adipocytes were differentiated in mature adipocytes with specific culture media and then treated with PDRN (10 µg/mL), PDRN + ZM241385 (1 µM), CGS21680 (1 µM) and CGS + ZM241385 for 24 h. Cell viability was studied by MTT assay, and browning induction was evaluated by Oil Red O staining and by RT-qPCR to study gene expression of browning markers. PDRN, as well as CGS21680, reduced the accumulation of lipids, cell volume and lipid droplet size, increased the expression of UCP1, PRDM16 and DIO2, considered as browning markers, and reduced the expression of FASn and FABP4, considered as whitening markers. In addition, PDRN decreased leptin expression and enhanced adiponectin mRNA levels. All these effects were abrogated when PDRN was co-incubated with the A2Ar antagonist ZM241385. In conclusion, these results suggest that PDRN is able to induce the white-to-brown adipose differentiation through A2Ar stimulation. Since PDRN is a safe drug already available in the market for other therapeutic indications, its “anti-obesity” potential warrants investigation in a clinical scenario.

Published

2021

36. Lysergic acid diethylamide (LSD) promotes social behavior through mTORC1 in the excitatory neurotransmission

Author

Antonio Inserra, Justine P Enns, Luca Posa, Jelena Popic, He Qianzi, Agnieszka Skalecka, Danilo De Gregorio, Argel Aguilar-Valles, Christopher K. Lafferty, Athanasios Markopoulos, Martha Lopez-Canul, Jonathan P. Britt, Nahum Sonenberg, Stefano Comai, Gabriella Gobbi, de Gregorio, D., Popic, J., Enns, J. P., Inserra, A., Skalecka, A., Markopoulos, A., Posa, L., Lopez-Canul, M., Qianzi, H., Lafferty, C. K., Britt, J. P., Comai, S., Aguilar-Valles, A., Sonenberg, N., and Gobbi, G.

Subjects

Male, 5-HT, Prefrontal Cortex, AMPA receptor, Mechanistic Target of Rapamycin Complex 1, Neurotransmission, Receptors, N-Methyl-D-Aspartate, Synaptic Transmission, 2A, LSD, Glutamatergic, AMPA, Avoidance Learning, medicine, 5-HT2A, Animals, Receptors, AMPA, Social behavior, Phosphorylation, 5-HT receptor, Lysergic acid diethylamide, Neurons, Multidisciplinary, Behavior, Animal, Chemistry, Pyramidal Cells, TOR Serine-Threonine Kinases, MTOR, Long-term potentiation, Biological Sciences, Mice, Inbred C57BL, Optogenetics, Lysergic Acid Diethylamide, nervous system, Receptors, Serotonin, Synapses, Excitatory postsynaptic potential, NMDA receptor, Proto-Oncogene Proteins c-akt, Neuroscience, medicine.drug

Abstract

Significance Social behavior (SB) is a fundamental hallmark of human interaction. Repeated administration of low doses of the 5-HT2A agonist lysergic acid diethylamide (LSD) in mice enhances SB by potentiating 5-HT2A and AMPA receptor neurotransmission in the mPFC via an increasing phosphorylation of the mTORC1, a protein involved in the modulation of SB. Moreover, the inactivation of mPFC glutamate neurotransmission impairs SB and nullifies the prosocial effects of LSD. Finally, LSD requires the integrity of mTORC1 in excitatory glutamatergic, but not in inhibitory neurons, to produce prosocial effects. This study unveils a mechanism contributing to the role of 5-HT2A agonism in the modulation of SB., Clinical studies have reported that the psychedelic lysergic acid diethylamide (LSD) enhances empathy and social behavior (SB) in humans, but its mechanism of action remains elusive. Using a multidisciplinary approach including in vivo electrophysiology, optogenetics, behavioral paradigms, and molecular biology, the effects of LSD on SB and glutamatergic neurotransmission in the medial prefrontal cortex (mPFC) were studied in male mice. Acute LSD (30 μg/kg) injection failed to increase SB. However, repeated LSD (30 μg/kg, once a day, for 7 days) administration promotes SB, without eliciting antidepressant/anxiolytic-like effects. Optogenetic inhibition of mPFC excitatory neurons dramatically inhibits social interaction and nullifies the prosocial effect of LSD. LSD potentiates the α-amino-3-hydroxy-5-methyl-4-isoxazole propionate (AMPA) and 5-HT2A, but not N-methyl-D-aspartate (NMDA) and 5-HT1A, synaptic responses in the mPFC and increases the phosphorylation of the serine-threonine protein kinases Akt and mTOR. In conditional knockout mice lacking Raptor (one of the structural components of the mTORC1 complex) in excitatory glutamatergic neurons (Raptorf/f:Camk2alpha-Cre), the prosocial effects of LSD and the potentiation of 5-HT2A/AMPA synaptic responses were nullified, demonstrating that LSD requires the integrity of mTORC1 in excitatory neurons to promote SB. Conversely, in knockout mice lacking Raptor in GABAergic neurons of the mPFC (Raptorf/f:Gad2-Cre), LSD promotes SB. These results indicate that LSD selectively enhances SB by potentiating mPFC excitatory transmission through 5-HT2A/AMPA receptors and mTOR signaling. The activation of 5-HT2A/AMPA/mTORC1 in the mPFC by psychedelic drugs should be explored for the treatment of mental diseases with SB impairments such as autism spectrum disorder and social anxiety disorder.

Published

2021

37. Guanosine-Mediated Anxiolytic-Like Effect: Interplay with Adenosine A1 and A2A Receptors

Author

Renata Ciccarelli, Giuseppa Mudò, Patrizia Di Iorio, Roberta Garozzo, Fulvio Plescia, Daniele F. Condorelli, Monica Frinchi, Francisco Ciruela, Natale Belluardo, Valentina Di Liberto, Francesco Caciagli, Vincenzo Verdi, Maria Grillo, Università degli studi di Palermo - University of Palermo, Institut de psychiatrie et neurosciences de Paris (IPNP - U1266 Inserm), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Paris (UP), Universitat de Barcelona (UB), University of Catania [Italy], University 'G. d'Annunzio' of Chieti-Pescara [Chieti and Pescara, Italy], Frinchi M., Verdi V., Plescia F., Ciruela F., Grillo M., Garozzo R., Condorelli D.F., Di Iorio P., Caciagli F., Ciccarelli R., Belluardo N., Di Liberto V., Mudo' G., Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Paris Cité (UPCité), and Martinez Rico, Clara

Subjects

Light, Pharmacology, Anxiety, Settore BIO/09 - Fisiologia, Hippocampus, lcsh:Chemistry, chemistry.chemical_compound, 0302 clinical medicine, Receptor, lcsh:QH301-705.5, Spectroscopy, caffeine, 0303 health sciences, Behavior, Animal, General Medicine, Darkness, 3. Good health, Computer Science Applications, adenosine, CCPA, [SDV.NEU]Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], A1R, Caffeine, medicine.drug, Receptor, Adenosine A2A, Guanosine, Catalysis, Article, Inorganic Chemistry, 03 medical and health sciences, medicine, Animals, [SDV.NEU] Life Sciences [q-bio]/Neurons and Cognition [q-bio.NC], Physical and Theoretical Chemistry, Binding site, 2A, Molecular Biology, 030304 developmental biology, Dose-Response Relationship, Drug, Receptor, Adenosine A1, behavior, Organic Chemistry, Cell Membrane, Antagonist, Adenosine, Adenosine receptor, Rats, guanosine, A2AR, lcsh:Biology (General), lcsh:QD1-999, chemistry, 030217 neurology & neurosurgery

Abstract

Acute or chronic administration of guanosine (GUO) induces anxiolytic-like effects, for which the adenosine (ADO) system involvement has been postulated yet without a direct experimental evidence. Thus, we aimed to investigate whether adenosine receptors (ARs) are involved in the GUO-mediated anxiolytic-like effect, evaluated by three anxiety-related paradigms in rats. First, we confirmed that acute treatment with GUO exerts an anxiolytic-like effect. Subsequently, we investigated the effects of pretreatment with ADO or A1R (CPA, CCPA) or A2AR (CGS21680) agonists 10 min prior to GUO on a GUO-induced anxiolytic-like effect. All the combined treatments blocked the GUO anxiolytic-like effect, whereas when administered alone, each compound was ineffective as compared to the control group. Interestingly, the pretreatment with nonselective antagonist caffeine or selective A1R (DPCPX) or A2AR (ZM241385) antagonists did not modify the GUO-induced anxiolytic-like effect. Finally, binding assay performed in hippocampal membranes showed that [3H]GUO binding became saturable at 100&ndash, 300 nM, suggesting the existence of a putative GUO binding site. In competition experiments, ADO showed a potency order similar to GUO in displacing [3H]GUO binding, whereas AR selective agonists, CPA and CGS21680, partially displaced [3H]GUO binding, but the sum of the two effects was able to displace [3H]GUO binding to the same extent of ADO alone. Overall, our results strengthen previous data supporting GUO-mediated anxiolytic-like effects, add new evidence that these effects are blocked by A1R and A2AR agonists and pave, although they do not elucidate the mechanism of GUO and ADO receptor interaction, for a better characterization of GUO binding sites in ARs.

Published

2020

38. Functional Analysis of Expression of Human Ecto-Nucleoside Triphosphate Diphosphohydrolase-1 and/or Ecto-5′-Nucleotidase in Pig Endothelial Cells.

Author

De Giorgi, M., Pelikant-Malecka, I., Sielicka, A., Slominska, E. M., Giovannoni, R., Cinti, A., Cerrito, M. G., Lavitrano, M., and Smolenski, R. T.

Subjects

*NUCLEOSIDE triphosphatase, *ENDOTHELIAL cells, *GENE expression, *XENOGRAFTS, *ADENOSINE monophosphate, *CELL lines, *GENE transfection

Abstract

Adenine nucleosides and nucleotides are important signaling molecules involved in control of key mechanisms of xenotransplant rejection. Extracellular pathway that converts ATP and ADP to AMP, and AMP to adenosine mainly mediated by ecto-nucleoside triphosphate diphosphohydrolase 1, (ENTPD1 or CD39) and ecto-5′-nucleotidase (E5NT or CD73) respectively, is considered as important target for xenograft protection. To clarify feasibility of combined expression of human ENTPD1 and E5NT and to study its functional effect we transfected pig endothelial cell line (PIEC) with both genes together. To do this we have produced a dicistronic construct bearing F2A sequence in frame between human E5NT and human ENTPD1 coding sequences. PIEC cells were mock-transfected as transfection control or transfected with plasmids encoding human ENTPD1 or human E5NT. PIEC cells were exposed to 50 μM ATP or 50 μM ADP or 50 μM AMP. Conversion of extracellular substrates into products (ATP/ADP/AMP/adenosine) was measured by HPLC in the media collected at specific time intervals. Following addition of AMP, production of adenosine in the medium of E5NT/ENTPD1- and E5NT- transfected cells increased to 14.2 ± 1.1 and 24.5 ± 3.4 μM respectively while it remained below 1 μM in controls and in ENTPD1-transfected cells. A marked increase of adenosine formation from ADP or ATP was observed only in E5NT/ENTPD1-transfected cells (11.7 ± 0.1 and 5.7 ± 2.2 μM respectively) but not in any other condition studied. This study indicates feasibility and functionality of combined expression of human E5NT and ENTPD1 in pig endothelial cells using F2A sequence bearing construct. [ABSTRACT FROM AUTHOR]

Published

2014

39. Expression of a Malassezia Codon Optimized mCherry Fluorescent Protein in a Bicistronic Vector

Author

Joleen P. Z. Goh, Giuseppe Ianiri, Joseph Heitman, and Thomas L. Dawson

Subjects

0301 basic medicine, Microbiology (medical), 030106 microbiology, Immunology, lcsh:QR1-502, Mutagenesis (molecular biology technique), tagging, Computational biology, Biology, Microbiology, lcsh:Microbiology, 03 medical and health sciences, Live cell imaging, 2A, Gene, Cellular localization, Malassezia, fluorescent, transformation, bicistronic, multicistronic, Fusion protein, Open reading frame, Transformation (genetics), 030104 developmental biology, Infectious Diseases, mCherry

Abstract

The use of fluorescent proteins allows a multitude of approaches from live imaging and fixed cells to labeling of whole organisms, making it a foundation of diverse experiments. Tagging a protein of interest or specific cell type allows visualization and studies of cell localization, cellular dynamics, physiology, and structural characteristics. In specific instances fluorescent fusion proteins may not be properly functional as a result of structural changes that hinder protein function, or when overexpressed may be cytotoxic and disrupt normal biological processes. In our study, we describe application of a bicistronic vector incorporating a Picornavirus 2A peptide sequence between a NAT antibiotic selection marker and mCherry. This allows expression of multiple genes from a single open reading frame and production of discrete protein products through a cleavage event within the 2A peptide. We demonstrate integration of this bicistronic vector into a model Malassezia species, the haploid strain M. furfur CBS 14141, with both active selection, high fluorescence, and proven proteolytic cleavage. Potential applications of this technology can include protein functional studies, Malassezia cellular localization, and co-expression of genes required for targeted mutagenesis.

Published

2020

40. Stimulation of homologous recombination in plants expressing heterologous recombinases

Author

Ewan Keir, Helena Oakey, Claire Halpin, and Abdellah Barakate

Subjects

0106 biological sciences, 0301 basic medicine, Gene Expression, Translational-recoding, Plant Science, Biology, 01 natural sciences, Homology directed repair, Recombinases, 03 medical and health sciences, Genome editing, lcsh:Botany, Tobacco, Recombinase, CRISPR, Transgenes, Homologous Recombination, Gene, 2A, Gene Editing, Transcription activator-like effector nuclease, fungi, Homozygote, Gene targeting, food and beverages, Cell biology, lcsh:QK1-989, Meiosis, 030104 developmental biology, Mutation, Pollen, Intrachromosomal homologous recombination, CRISPR-Cas Systems, Homologous recombination, 010606 plant biology & botany, Research Article

Abstract

Background Current excitement about the opportunities for gene editing in plants have been prompted by advances in CRISPR/Cas and TALEN technologies. CRISPR/Cas is widely used to knock-out or modify genes by inducing targeted double-strand breaks (DSBs) which are repaired predominantly by error-prone non-homologous end-joining or microhomology-mediated end joining resulting in mutations that may alter or abolish gene function. Although such mutations are random, they occur at sufficient frequency to allow useful mutations to be routinely identified by screening. By contrast, gene knock-ins to replace entire genes with alternative alleles or copies with specific characterised modifications, is not yet routinely possible. Gene replacement (or gene targeting) by homology directed repair occurs at extremely low frequency in higher plants making screening for useful events unfeasible. Homology directed repair might be increased by inhibiting non-homologous end-joining and/or stimulating homologous recombination (HR). Here we pave the way to increasing gene replacement efficiency by evaluating the effect of expression of multiple heterologous recombinases on intrachromosomal homologous recombination (ICR) in Nicotiana tabacum plants. Results We expressed several bacterial and human recombinases in different combinations in a tobacco transgenic line containing a highly sensitive β-glucuronidase (GUS)-based ICR substrate. Coordinated simultaneous expression of multiple recombinases was achieved using the viral 2A translational recoding system. We found that most recombinases increased ICR dramatically in pollen, where HR will be facilitated by the programmed DSBs that occur during meiosis. DMC1 expression produced the greatest stimulation of ICR in primary transformants, with one plant showing a 1000-fold increase in ICR frequency. Evaluation of ICR in homozygous T2 plant lines revealed increases in ICR of between 2-fold and 380-fold depending on recombinase(s) expressed. By comparison, ICR was only moderately increased in vegetative tissues and constitutive expression of heterologous recombinases also reduced plant fertility. Conclusion Expression of heterologous recombinases can greatly increase the frequency of HR in plant reproductive tissues. Combining such recombinase expression with the use of CRISPR/Cas9 to induce DSBs could be a route to radically improving gene replacement efficiency in plants.

Published

2020

41. Receptor-independent modulation of cAMP-dependent protein kinase and protein phosphatase signaling in cardiac myocytes by oxidizing agents

Author

Ulrike Fuchs, Sonia Donzelli, Julia Pflaumenbaum, Mona Brandt, Steven Schulz, Mara Goetz, Frederik Flenner, Janice Raabe, Konstantina Stathopoulou, Friederike Cuello, Sakthivel Sadayappan, Sönke Harder, Angelika Piasecki, Simon Diering, Viacheslav O. Nikolaev, Laura Rathjens, and Elisabeth Ehler

Subjects

0301 basic medicine, Male, cardiomyocyte, troponin-i, Acetates, Biochemistry, Mice, cardiovascular disease, catalytic subunit, c phosphorylation, Phosphoprotein Phosphatases, Myocyte, Protein phosphorylation, Myocytes, Cardiac, Phosphorylation, phospholamban, Diamide, Chemistry, Kinase, Cardiac myocyte, Oxidants, Cell biology, Rabbits, 2a, Oxidation-Reduction, Nitroso Compounds, Signal Transduction, oxidation, kinase, Phosphatase, cardiac myocyte, phosphatase, redox regulation, 03 medical and health sciences, Animals, Humans, Rats, Wistar, Protein kinase A, Molecular Biology, 1-nitrosocyclohexyl acetate, 030102 biochemistry & molecular biology, hydrogen-peroxide, heart-failure, Protein phosphatase 2, Cell Biology, dephosphorylation, Cyclic AMP-Dependent Protein Kinases, protein kinase a (pka), Rats, 030104 developmental biology, nitroxyl, Cattle, Receptors, Adrenergic, beta-1

Abstract

The contraction and relaxation of the heart is controlled by stimulation of the beta 1-adrenoreceptor (AR) signaling cascade, which leads to activation of cAMP-dependent protein kinase (PKA) and subsequent cardiac protein phosphorylation. Phosphorylation is counteracted by the main cardiac protein phosphatases, PP2A and PP1. Both kinase and phosphatases are sensitive to intramolecular disulfide formation in their catalytic subunits that inhibits their activity. Additionally, intermolecular disulfide formation between PKA type I regulatory subunits (PKA-RI) has been described to enhance PKA's affinity for protein kinase A anchoring proteins, which alters its subcellular distribution. Nitroxyl donors have been shown to affect contractility and relaxation, but the mechanistic basis for this effect is unclear. The present study investigates the impact of several nitroxyl donors and the thiol-oxidizing agent diamide on cardiac myocyte protein phosphorylation and oxidation. Although all tested compounds equally induced intermolecular disulfide formation in PKA-RI, only 1-nitrosocyclohexalycetate (NCA) and diamide induced reproducible protein phosphorylation. Phosphorylation occurred independently of beta(1)-AR activation, but was abolished after pharmacological PKA inhibition and thus potentially attributable to increased PKA activity. NCA treatment of cardiac myocytes induced translocation of PKA and phosphatases to the myofilament compartment as shown by fractionation, immunofluorescence, and proximity ligation assays. Assessment of kinase and phosphatase activity within the myofilament fraction of cardiac myocytes after exposure to NCA revealed activation of PKA and inhibition of phosphatase activity thus explaining the increase in phosphorylation. The data suggest that the NCA-mediated effect on cardiac myocyte protein phosphorylation orchestrates alterations in the kinase/phosphatase balance.

Published

2020

42. Expression of a

Author

Joleen P Z, Goh, Giuseppe, Ianiri, Joseph, Heitman, and Thomas L, Dawson

Subjects

Luminescent Proteins, Open Reading Frames, Malassezia, Cellular and Infection Microbiology, fluorescent, multicistronic, transformation, Genetic Vectors, bicistronic, tagging, Brief Research Report, Codon, 2A

Abstract

The use of fluorescent proteins allows a multitude of approaches from live imaging and fixed cells to labeling of whole organisms, making it a foundation of diverse experiments. Tagging a protein of interest or specific cell type allows visualization and studies of cell localization, cellular dynamics, physiology, and structural characteristics. In specific instances fluorescent fusion proteins may not be properly functional as a result of structural changes that hinder protein function, or when overexpressed may be cytotoxic and disrupt normal biological processes. In our study, we describe application of a bicistronic vector incorporating a Picornavirus 2A peptide sequence between a NAT antibiotic selection marker and mCherry. This allows expression of multiple genes from a single open reading frame and production of discrete protein products through a cleavage event within the 2A peptide. We demonstrate integration of this bicistronic vector into a model Malassezia species, the haploid strain M. furfur CBS 14141, with both active selection, high fluorescence, and proven proteolytic cleavage. Potential applications of this technology can include protein functional studies, Malassezia cellular localization, and co-expression of genes required for targeted mutagenesis.

Published

2020

43. PROTEIN PHOSPHATASE 2A-B′ γ Controls Botrytis cinerea Resistance and Developmental Leaf Senescence

Author

Zsófia Winter, Shengchun Li, Graham Noctor, Mikael Brosché, Saijaliisa Kangasjärvi, Katariina Vuorinen, Verena Jeschke, Meike Burow, Eva-Mari Aro, Peter J. Gollan, Jarkko Salojärvi, Moona Rahikainen, Guido Durian, Kirk Overmyer, Erich Glawischnig, Jaakko Kangasjärvi, Molecular Plant Biology, University of Turku, DynaMo Center of Excellence for Dynamic Molecular Interactions (DynaMo), Department of Plant and Environmental Sciences [Copenhagen], Faculty of Science [Copenhagen], University of Copenhagen = Københavns Universitet (KU)-University of Copenhagen = Københavns Universitet (KU)-Faculty of Science [Copenhagen], University of Copenhagen = Københavns Universitet (KU)-University of Copenhagen = Københavns Universitet (KU), Organismal and Evolutionary Biology Research Program, Faculty of Biological and Environmental Sciences, Viikki Plant Science Centre, University of Helsinki-University of Helsinki-Viikki Plant Science Centre, University of Helsinki-University of Helsinki, Chair of Genetics, Department of Plant Sciences, Technical University of Munich (TUM)-Technical University of Munich (TUM), Institut des Sciences des Plantes de Paris-Saclay (IPS2 (UMR_9213 / UMR_1403)), Université d'Évry-Val-d'Essonne (UEVE)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Université de Paris (UP)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), Academy of FinlandEuropean Commission289687307719303757317218Academy of Finland307335University of Turku Doctoral Programme in Molecular Life Sciences Turku University Foundation Finnish Cultural Foundation Danmarks Grundforskningsfond99Villumfonden 13169Scandinavian Society for Plant Physiology German Research Foundation (DFG)GL346/5University of Helsinki Doctoral Program in Plant Science Ella and Georg Ehrnrooth Foundation Finnish Functional Genomics Centre, University of Turku Abo Akademi Biocenter Finland, Organismal and Evolutionary Biology Research Programme, Viikki Plant Science Centre (ViPS), Plant stress and natural variation, Bioinformatics for Molecular Biology and Genomics (BMBG), Plant ROS-Signalling, Doctoral Programme in Plant Sciences, Plant-Fungal Interactions Group, University of Copenhagen = Københavns Universitet (UCPH)-University of Copenhagen = Københavns Universitet (UCPH)-Faculty of Science [Copenhagen], University of Copenhagen = Københavns Universitet (UCPH)-University of Copenhagen = Københavns Universitet (UCPH), Helsingin yliopisto = Helsingfors universitet = University of Helsinki-Helsingin yliopisto = Helsingfors universitet = University of Helsinki-Viikki Plant Science Centre, Helsingin yliopisto = Helsingfors universitet = University of Helsinki-Helsingin yliopisto = Helsingfors universitet = University of Helsinki, Technische Universität Munchen - Université Technique de Munich [Munich, Allemagne] (TUM)-Technische Universität Munchen - Université Technique de Munich [Munich, Allemagne] (TUM), and Université d'Évry-Val-d'Essonne (UEVE)-Université Paris-Saclay-Centre National de la Recherche Scientifique (CNRS)-Université Paris Cité (UPCité)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE)

Subjects

0106 biological sciences, Senescence, Physiology, Transcription Factor, Arabidopsis, Expression, Plant Science, Biology, Plant disease resistance, 01 natural sciences, Gene, chemistry.chemical_compound, Genetics, Defense, Arabidopsis thaliana, Responses, [SDV.BV]Life Sciences [q-bio]/Vegetal Biology, Receptor-like Kinase, Protein kinase A, Botrytis cinerea, Disease Resistance, 2. Zero hunger, fungi, food and beverages, Protein phosphatase 2, biology.organism_classification, 11831 Plant biology, Salicylic-acid, Cell biology, chemistry, 2a, Salicylic acid, 010606 plant biology & botany

Abstract

International audience; Plants optimize their growth and survival through highly integrated regulatory networks that coordinate defensive measures and developmental transitions in response to environmental cues. Protein phosphatase 2A (PP2A) is a key signaling component that controls stress reactions and growth at different stages of plant development, and the PP2A regulatory subunit PP2A-B'gamma is required for negative regulation of pathogenesis responses and for maintenance of cell homeostasis in short-day conditions. Here, we report molecular mechanisms by which PP2A-B'gamma regulates Botrytis cinerea resistance and leaf senescence in Arabidopsis (Arabidopsis thaliana). We extend the molecular functionality of PP2A-B'gamma to a protein kinase-phosphatase interaction with the defense-associated calcium-dependent protein kinase CPK1 and present indications this interaction may function to control CPK1 activity. In presenescent leaf tissues, PP2A-B'gamma is also required to negatively control the expression of salicylic acid-related defense genes, which have recently proven vital in plant resistance to necrotrophic fungal pathogens. In addition, we find the premature leaf yellowing of pp2a-b'gamma depends on salicylic acid biosynthesis via SALICYLIC ACID INDUCTION DEFICIENT2 and bears the hallmarks of developmental leaf senescence. We propose PP2A-B'gamma age-dependently controls salicylic acid-related signaling in plant immunity and developmental leaf senescence.

Published

2020

44. Swedish review strengthens grounds for concluding that radiation from cellular and cordless phones is a probable human carcinogen.

Author

Davis, Devra Lee, Kesari, Santosh, Soskolne, Colin L., Miller, Anthony B., and Stein, Yael

Subjects

*ELECTROMAGNETIC radiation, *CELL phones, *CORDLESS telephones, *HUMAN carcinogenesis, *TUMOR risk factors, *MICROWAVES

Abstract

Abstract: With 5.9 billion reported users, mobile phones constitute a new, ubiquitous and rapidly growing exposure worldwide. Mobile phones are two-way microwave radios that also emit low levels of electromagnetic radiation. Inconsistent results have been published on potential risks of brain tumors tied with mobile phone use as a result of important methodological differences in study design and statistical power. Some studies have examined mobile phone users for periods of time that are too short to detect an increased risk of brain cancer, while others have misclassified exposures by placing those with exposures to microwave radiation from cordless phones in the control group, or failing to attribute such exposures in the cases. In 2011, the World Health Organization, International Agency for Research on Cancer (IARC) advised that electromagnetic radiation from mobile phone and other wireless devices constitutes a “possible human carcinogen,” 2B. Recent analyses not considered in the IARC review that take into account these methodological shortcomings from a number of authors find that brain tumor risk is significantly elevated for those who have used mobile phones for at least a decade. Studies carried out in Sweden indicate that those who begin using either cordless or mobile phones regularly before age 20 have greater than a fourfold increased risk of ipsilateral glioma. Given that treatment for a single case of brain cancer can cost between $100,000 for radiation therapy alone and up to $1 million depending on drug costs, resources to address this illness are already in short supply and not universally available in either developing or developed countries. Significant additional shortages in oncology services are expected at the current growth of cancer. No other environmental carcinogen has produced evidence of an increased risk in just one decade. Empirical data have shown a difference in the dielectric properties of tissues as a function of age, mostly due to the higher water content in children's tissues. High resolution computerized models based on human imaging data suggest that children are indeed more susceptible to the effects of EMF exposure at microwave frequencies. If the increased brain cancer risk found in young users in these recent studies does apply at the global level, the gap between supply and demand for oncology services will continue to widen. Many nations, phone manufacturers, and expert groups, advise prevention in light of these concerns by taking the simple precaution of “distance” to minimize exposures to the brain and body. We note than brain cancer is the proverbial “tip of the iceberg”; the rest of the body is also showing effects other than cancers. [Copyright &y& Elsevier]

Published

2013

45. The synthesis and the study of the antitumor activity of 1,4-diaryl-5,6,7,8-tetrahydro-2,2a,8a triazacyclopenta[cd]azulene derivatives

Author

Demchenko, S. A., Fedchenkova, Yu. A., Bobkova, L. S., Artemchuk, L. P., Demchenko, A. M., Demchenko, S. A., Fedchenkova, Yu. A., Bobkova, L. S., Artemchuk, L. P., and Demchenko, A. M.

Abstract

Aim. To synthesize, prove the structural framework and study the antitumor activity of 1,4-diaryl-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta [cd]azulene derivatives.Results and discussion. To determine the antineoplastic activity of 1-phenyl-4-aryl-5,6,7,8-tetrahydro-2,2a,8a-triazacyclopenta[cd]azulenes 7a-g and 1-(41-bromophenyl)-4-aryl-5,6,7,8-tetra-hydro-2,2a,8a-triazacyclopenta [cd]azulenes 7h-k the study in vitro was carried out on 60 lines of cancer cells (leukemia, non-small cell lung cancer, colon cancer, CNS cancer, melanoma, ovarian cancer, renal cancer, prostate cancer and breast cancer) under the effect of the substance in the concentration of 10-5 mol/l according to the standard procedure of the mitotic activity assessment of the new potential bioactive compounds by the fluorescent coloring method (sulphorhodamine B as a dye) performed in the US National Institute of cancer within the Development Therapeutic Program.Experimental part. 2-Methoxy-3,4,5,6-tetrahydro-7H-azepine was obtained by alkylation of caprolactam with dimethyl sulfate. 3-Phenyl or (41-bromophenyl)-(6,7,8,9-tetrahydro-5H-[1,2,4]triazolo[4,3-a]azepine 4 a,b was obtained by condensation of 2-methoxy-3,4,5,6-tetrahydro-7H-azepine 1 with 4-bromobenzoic acid hydrazide and subsequent cyclization of the intermediate product. The 1Н-NMR spectra were recorded on a Bruker VXR-300 spectrometer (Germany) with the working frequency of 299.945 MHz, in DMSO-d6 using tetramethylsilane (TMS) as an internal standard. The purity of the compounds synthesized was controlled by TLC on the Silufol UV-254 plates in the system of chloroform – methanol (9 : 1). Conclusions. New chemical compounds – derivatives of 1-phenyl(41-bromphenyl)-4-aryl-5,6,7,8-tetrahydro-2,2a,8a-triaza-cyclopenta[cd]azulene have been synthesized. The anticancer activity of the compounds obtained on 60 lines of tumor cells in the US National Cancer Institute has been studied. The high-active compounds that exhibit high levels of the ant, Цель работы –синтезировать, доказать структурное строение и провести изучение противоопухолевой активности производных 1,4-диарил-5,6,7,8-тетрагидро-2,2А, 8а-триазациклопента[cd]азулена.Результаты и их обсуждение. Для определения противоопухолевой активности 1-фенил-4-арил-5,6,7,8-тетрагидро-2,2а, 8а-триазациклопента [cd] азулена 7a-g и 1-(41-бромфенил)-4-арил-5,6,7,8-тетрагидро-2,2а,8а-триазациклопента[cd]азулена 7h-k было проведено исследование in vitro на 60 линиях раковых клеток (лейкемии, легких, толстого кишечника, ЦНС, меланомы, яичников, почек, простаты, молочной железы) при воздействии вещества в концентрации 10-5 моль/л по стандартной процедуре оценки митотической активности новых потенциальных биологически активных соединений методом флуоресцентной окраски (краситель – сульфородамин Б), выполненных в Национальном институте рака США (National Cancer Institute of Health, USA) в рамках Development Therapeutic Program.Экспериментальная часть. 2-метокси-3,4,5,6-тетрагидро-7H-азепин получено алкилированием капролактама диметилсульфатом. 3-(41-бромфенил)-6,7,8,9-тетрагидро-5H-[1,2,4]триазоло[4,3-a]азепин получено конденсацией 2-метокси-3,4,5,6-тетрагидро-7H-азепин с гидразидом парабромбензойной кислоты и последующей циклизацией промежуточного продукта. Спектры ПМР были зарегистрированы на спектрометре Bruker VXR-300, рабочая частота – 299,945 МГц, внутренний стандарт ТМС. Контроль за чистотой синтезированных соединений осуществлялся с помощью ТСХ на пластинках Silufol UV-254 в системе хлороформ – метанол 9 : 1.Выводы. Синтезированы новые химические соединения – производные 1,4-диарил-5,6,7,8-тетрагидро-2,2а,8а-триазациклопента[cd]азулена. Изучена противораковая активность полученных соединений на 60 линиях опухолевых клеток в Национальном институте рака США. Идентифицированы высокоактивные соединения, которые проявили высокий уровень противоопухолевой активности., Мета роботи – синтезувати, довести структурну будову та провести вивчення протипухлинної активності похідних 1,4-діарил-5,6,7,8-тетрагідро-2,2а,8а-триазациклопента[cd]азуленів.Результати та їх обговорення. Для визначення протипухлинної активності 1-феніл-4-арил-5,6,7,8- тетрагідро-2,2а,8а-триазациклопента[cd]азулену 7a-g та 1-(41-бромфеніл)-4-арил-5,6,7,8-тетрагідро-2,2а,8а-триазациклопента[cd]азулену 7h-k дослідження проведено in vitro на 60 лініях ракових клітин (лейкемії, легень, товстого кишківника, ЦНС, меланоми, яєчників, нирок, простати, молочної залози) при дії речовини в концентрації 10-5 моль/л за стандартною процедурою оцінки мітотичної активності нових потенційних біологічно активних сполук методом флуоресцентного зафарбування (барвник – сульфородамін Б), виконаних у Національному інституті раку США (National Cancer Institute of Health, USA) в рамках Development Therapeutic Program.Експериментальна частина. 2-Метокси-3,4,5,6-тетрагідро-7H-азепін одержано алкілуванням капролактаму диметилсульфатом. 3-(41-Бромфеніл)-6,7,8,9-тетрагідро-5H-[1,2,4]триазоло[4,3-a]азепін одержано конденсацією 2-метокси-3,4,5,6-тетрагідро-7H-азепіну з гідразидом пара-бромбензойної кислоти та подальшою циклізацією проміжного продукту. Спектри ПМР були зареєстровані на спектрометрі Bruker VXR-300, робоча частота – 299,945 МГц, внутрішній стандарт ТМС. Контроль за чистотою синтезованих сполук здійснювався за допомогою ТШХ на пластинках Silufol UV-254 в системі хлороформ – метанол 9 : 1.Висновки. Синтезовані нові хімічні речовини – похідні 1,4-діарил-5,6,7,8-тетрагідро-2,2а,8а-триазациклопента [cd]азулену. Вивчена протиракова активність одержаних сполук на 60 лініях пухлинних клітин в Національному інституті раку США. Ідентифіковані високоактивні сполуки, які проявили високий рівень протипухлинної активності.

Published

2019

46. Versatile co-expression of graft-protective proteins using 2A-linked cassettes.

Author

Fisicaro, Nella, Londrigan, Sarah L., Brady, Jamie L., Salvaris, Evelyn, Nottle, Mark B., O'Connell, Philip J., Robson, Simon C., d'Apice, Anthony J. F., Lew, Andrew M., and Cowan, Peter J.

Subjects

*XENOTRANSPLANTATION, *THROMBOMODULIN, *GENE transfection, *CYTOLOGICAL research, *WESTERN immunoblotting, *LABORATORY mice

Abstract

Fisicaro N, Londrigan SL, Brady JL, Salvaris E, Nottle MB, O'Connell PJ, Robson SC, d'Apice AJF, Lew AM, Cowan PJ. Versatile co-expression of graft-protective proteins using 2A-linked cassettes. Xenotransplantation 2011; 18: 121-130. © 2011 John Wiley & Sons A/S. Expression of multiple graft-protective proteins targeted to different locations (i.e., intracellular, cell surface, and secreted) has become an increasingly important goal in xenotransplantation. The 2A 'ribosome skip' signal is used as a linker to enable transgene co-expression, but some studies have shown that post-translational modification and trafficking of 2A-linked proteins may be adversely affected depending on their position relative to 2A. We tested whether several relevant proteins, subject to a range of processing and localization mechanisms, could be efficiently co-expressed using the 2A system. Six expression cassettes were constructed, each containing up to four 2A-linked open reading frames, encoding combinations of human CD55, thrombomodulin (TBM), CD39, CTLA4-Ig and hygromycin resistance. Each linker incorporated a furin cleavage site to remove the carboxy-terminal extension that remains on upstream proteins after 2A processing. The cassettes were used to produce vectors for transfection, adenoviral transduction and transgenesis. Expression was detected by flow cytometry and/or Western blotting. All proteins were expressed in the appropriate location following transient transfection of COS-7 cells, irrespective of the number of linked genes. The percentage of stable transfectants expressing a linked gene was increased 10-fold (from 4-5% to 58-67%) by incorporating the hygromycin resistance gene into the cassette. Stable transfection of transgenic GalT KO pig fibroblasts with a hygromycin- TBM-CD39 construct resulted in surface expression of both TBM and CD39 by the majority of hygromycin-resistant cells. Expression was maintained after flow cytometric sorting and expansion. Adenoviral transduction of NIT-1 mouse insulinoma cells with a TBM-CD39 construct resulted in strong expression of both genes on the cell surface. Mice transgenic for 3-gene (CD55- TBM-CD39) or 4-gene (CD55- TBM-CTLA4Ig-CD39) constructs expressed all genes except CD55. These results confirm the versatility of the 2A system, and demonstrate that careful construct design can minimize potential problems with post-translational modification and trafficking. In addition, incorporation of a selection marker into the 2A-linked chain can dramatically increase the proportion of stable transfectants expressing proteins of interest. This provides a powerful method for the rapid modification of existing genetically modified pigs. [ABSTRACT FROM AUTHOR]

Published

2011

47. Application of two bicistronic systems involving 2A and IRES sequences to the biosynthesis of carotenoids in rice endosperm.

Author

Ha, Sun‐Hwa, Liang, Ying Shi, Jung, Harin, Ahn, Mi‐Jeong, Suh, Seok‐Cheol, Kweon, Soon‐Jong, Kim, Dong‐Hern, Kim, Young‐Mi, and Kim, Ju‐Kon

Subjects

*TRANSGENIC rice, *PLANT biotechnology, *BIOCHEMISTRY, *ENDOSPERM, *CAROTENOIDS

Abstract

Coordination of multiple transgenes is essential for metabolic engineering of biosynthetic pathways. Here, we report the utilization of two bicistronic systems involving the 2A sequence from the foot-and-mouth disease virus and the internal ribosome entry site (IRES) sequence from the crucifer-infecting tobamovirus to the biosynthesis of carotenoids in rice endosperm. Two carotenoid biosynthetic genes, phytoene synthase ( Psy) from Capsicum and carotene desaturase ( CrtI) from Pantoea, were linked via either the synthetic 2A sequence that was optimized for rice codons or the IRES sequence under control of the rice globulin promoter, generating PAC ( sy-2 - rtI) and PIC ( sy- RES- rtI) constructs, respectively. The transgenic endosperm of PAC rice had a more intense golden color than did PIC rice, demonstrating that 2A was more efficient than IRES in coordinating gene expression. The 2A and IRES constructs were equally effective in driving transgene transcription. However, immunoblot analysis of CRTI, a protein encoded by the downstream open reading frame of the bicistronic constructs, revealed that 2A was ninefold more effective than IRES in driving translation. The PAC endosperms accumulated an average of 1.3 μg/g of total carotenoids, which was ninefold higher than was observed for PIC endosperms. In particular, accumulation of β-carotene was much higher in PAC endosperms than in PIC endosperms. Collectively, these results demonstrate that both 2A and IRES systems can coordinate the expression of two biosynthetic genes, with the 2A system exhibiting greater efficiency. Thus, the 2A expression system described herein is an effective new tool for multigene stacking in crop biotechnology. [ABSTRACT FROM AUTHOR]

Published

2010

48. Coexpression of double or triple copies of the rabies virus glycoprotein gene using a ‘self-cleaving’ 2A peptide-based replication-defective human adenovirus serotype 5 vector

Author

Tan, Yeping, Liang, Hongru, Chen, Aie, and Guo, Xiaofeng

Subjects

*RABIES virus, *FOOT & mouth disease, *RECOMBINANT viruses, *ADENOVIRUSES, *VIRAL proteins, *GENE expression, *NUCLEOTIDE sequence, *BIOLOGICAL assay

Abstract

Abstract: Rabies virus glycoprotein (RVG) is a major structural protein and antigen of rabies virus that induces a highly immunogenic response. In the present study, we have used 2A self-cleaving sequence of the foot-and-mouth disease virus (FMDV) to express double or triple copies of the RVG from a single open reading frame derived from human adenovirus 5 (AdHu5). The recombinant adenoviruses produce similar virus titers, indicating that the insertion of double or triple copies of the RVG gene linked with the FMDV 2A sequence does not affect virus replication. The RVG was efficiently expressed by constructs containing the 2A sequence and retained its antigenic property. The 2A self-cleaving peptide mediated efficient generation of individual glycoprotein in transient expression assay and did not lead to an altered surface distribution of RVG. Flow cytometry demonstrated that the expression levels of RVG were improved in recombinant Ads carrying multiple RVG gene copies. We conclude that ribosome skipping induced by the FMDV 2A sequence is an effective strategy to express multiple glycoprotein genes of rabies virus in adenoviruses and 2A-containing recombinant Ads may represent an attractive alternative to other coexpression strategies for multiple gene expression. [Copyright &y& Elsevier]

Published

2010

49. PDRN, a natural bioactive compound, blunts inflammation and positively reprograms healing genes in an 'in vitro' model of oral mucositis

Author

Natasha Irrera, Domenica Altavilla, Mario Vaccaro, Federica Mannino, Vincenzo Arcoraci, Giovanni Pallio, Francesco Squadrito, Violetta Squadrito, Giuseppe Picciolo, Letteria Minutoli, and Giacomo Picciolo

Subjects

Vascular Endothelial Growth Factor A, 0301 basic medicine, Agonist, medicine.drug_class, medicine.medical_treatment, Anti-Inflammatory Agents, Gingiva, Adenosine A2A receptor, Inflammation, RM1-950, Pharmacology, A2A receptor, Oral mucositis, 03 medical and health sciences, Polydeoxyribonucleotides, 0302 clinical medicine, Mucositis, Humans, Medicine, Receptor, Wnt Signaling Pathway, Cells, Cultured, Stomatitis, Wound Healing, Epidermal Growth Factor, 2A, receptor, Polydeoxyribonucleotide, Cytokines, Epithelial Cells, Fibroblasts, Inflammation Mediators, Mouth Mucosa, business.industry, Growth factor, Wnt signaling pathway, General Medicine, medicine.disease, 030104 developmental biology, Mechanism of action, 030220 oncology & carcinogenesis, Therapeutics. Pharmacology, medicine.symptom, business

Abstract

Oral mucositis is a side effect hard to treat following high dose chemotherapy or radiotherapy. Adenosine A2A receptor stimulation blocks NF-κB and boosts the Wnt/β-catenin signaling, thus blunting inflammation and triggering growth factor codifying genes. Polydeoxyribonucleotide (PDRN) is a registered drug that activates the A2A receptor. Therefore, the aim of this study was to evaluate PDRN effects in an “in vitro” model of oral mucositis induced by prompting an inflammatory phenotype in human gingival fibroblasts (GF) and human oral mucosal epithelial cells (EC). GF and EC were stimulated with LPS (2 μg/ml) alone or in combination with i) PDRN (100 μg/ml); ii) PDRN plus ZM241385 (1 μM) as an A2AR antagonist; iii) CGS21680 (1 μM) as an A2AR agonist. LPS boosted NF-κB, TNF-α and IL-6 expression, decreased IL-10 levels and downregulated both Wnt/β-catenin, VEGF and EGF expression. PDRN reverted the LPS-induced phenotype as well as CGS21680. Co-incubation with ZM241385 abolished PDRN effects, thus confirming A2A receptor involvement in PDRN mechanism of action. These results suggest that PDRN efficacy may be due to a “dual mode” of action: NF-κB inhibition and Wnt/β-catenin signaling activation. However, these interesting findings need to be confirmed by animal and clinical studies.

Published

2021

50. Encephalomyocarditis Virus 2A Protein Inhibited Apoptosis by Interaction with Annexin A2 through JNK/c-Jun Pathway.

Author

Han, Ruochan, Liang, Lin, Qin, Tong, Xiao, Sa, and Liang, Ruiying

Subjects

*VIRAL proteins, *APOPTOSIS inhibition, *APOPTOSIS, *ANNEXINS, *MASS spectrometry, *IMAGE analysis

Abstract

Encephalomyocarditis virus can cause myocarditis and encephalitis in pigs and other mammals, thus posing a potential threat to public health safety. The 2A protein is an important virulence factor of EMCV. Previous studies have shown that the 2A protein may be related to the inhibition of apoptosis by virus, but its specific molecular mechanism is not clear. In this study, the 2A protein was expressed in Escherichia coli in order to find interacting cell proteins. A pull down assay, coupled with mass spectrometry, revealed that the 2A protein possibly interacted with annexin A2. Co-immunoprecipitation assays and confocal imaging analysis further demonstrated that the 2A protein interacted with annexin A2 in cells. In reducing the expression of annexin A2 by siRNA, the ability of the 2A protein to inhibit apoptosis was weakened and the proliferation of EMCV was slowed down. These results suggest that annexin A2 is closely related to the inhibition of apoptosis by 2A. Furthermore, both RT-PCR and western blot results showed that the 2A protein requires annexin A2 interaction to inhibit apoptosis via JNK/c-Jun pathway. Taken together, our data indicate that the 2A protein inhibits apoptosis by interacting with annexin A2 via the JNK/c-Jun pathway. These findings provide insight into the molecular pathogenesis underlying EMCV infection. [ABSTRACT FROM AUTHOR]

Published

2022