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2. High pathogenic avian influenza A(H5) viruses of clade 2.3.4.4b in Europe - Why trends of virus evolution are more difficult to predict

Author

Fusaro, Alice, Zecchin, Bianca, Giussani, Edoardo, Palumbo, Elisa, Agüero-García, Montserrat, Bachofen, Claudia, Bálint, Ádám, Banihashem, Fereshteh, Banyard, Ashley C., Beerens, Nancy, Bourg, Manon, Briand, Francois Xavier, Bröjer, Caroline, Brown, Ian H., Brugger, Brigitte, Byrne, Alexander M.P., Cana, Armend, Christodoulou, Vasiliki, Dirbakova, Zuzana, Fagulha, Teresa, Fouchier, Ron A.M., Garza-Cuartero, Laura, Georgiades, George, Gjerset, Britt, Grasland, Beatrice, Groza, Oxana, Harder, Timm, Henriques, Ana Margarida, Hjulsager, Charlotte Kristiane, Ivanova, Emiliya, Janeliunas, Zygimantas, Krivko, Laura, Lemon, Ken, Liang, Yuan, Lika, Aldin, Malik, Peter, Mcmenamy, Michael J., Nagy, Alexander, Nurmoja, Imbi, Onita, Iuliana, Pohlmann, Anne, Revilla-Fernández, Sandra, Sánchez-Sánchez, Azucena, Savic, Vladimir, Slavec, Brigita, Smietanka, Krzysztof, Snoeck, Chantal J., Steensels, Mieke, Svansson, Vilhjálmur, Swieton, Edyta, Tammiranta, Niina, Tinak, Martin, Van Borm, Steven, Zohari, Siamak, Adlhoch, Cornelia, Baldinelli, Francesca, Terregino, Calogero, Monne, Isabella, Fusaro, Alice, Zecchin, Bianca, Giussani, Edoardo, Palumbo, Elisa, Agüero-García, Montserrat, Bachofen, Claudia, Bálint, Ádám, Banihashem, Fereshteh, Banyard, Ashley C., Beerens, Nancy, Bourg, Manon, Briand, Francois Xavier, Bröjer, Caroline, Brown, Ian H., Brugger, Brigitte, Byrne, Alexander M.P., Cana, Armend, Christodoulou, Vasiliki, Dirbakova, Zuzana, Fagulha, Teresa, Fouchier, Ron A.M., Garza-Cuartero, Laura, Georgiades, George, Gjerset, Britt, Grasland, Beatrice, Groza, Oxana, Harder, Timm, Henriques, Ana Margarida, Hjulsager, Charlotte Kristiane, Ivanova, Emiliya, Janeliunas, Zygimantas, Krivko, Laura, Lemon, Ken, Liang, Yuan, Lika, Aldin, Malik, Peter, Mcmenamy, Michael J., Nagy, Alexander, Nurmoja, Imbi, Onita, Iuliana, Pohlmann, Anne, Revilla-Fernández, Sandra, Sánchez-Sánchez, Azucena, Savic, Vladimir, Slavec, Brigita, Smietanka, Krzysztof, Snoeck, Chantal J., Steensels, Mieke, Svansson, Vilhjálmur, Swieton, Edyta, Tammiranta, Niina, Tinak, Martin, Van Borm, Steven, Zohari, Siamak, Adlhoch, Cornelia, Baldinelli, Francesca, Terregino, Calogero, and Monne, Isabella

Abstract

Since 2016, A(H5Nx) high pathogenic avian influenza (HPAI) virus of clade 2.3.4.4b has become one of the most serious global threats not only to wild and domestic birds, but also to public health. In recent years, important changes in the ecology, epidemiology, and evolution of this virus have been reported, with an unprecedented global diffusion and variety of affected birds and mammalian species. After the two consecutive and devastating epidemic waves in Europe in 2020–2021 and 2021–2022, with the second one recognized as one of the largest epidemics recorded so far, this clade has begun to circulate endemically in European wild bird populations. This study used the complete genomes of 1,956 European HPAI A(H5Nx) viruses to investigate the virus evolution during this varying epidemiological outline. We investigated the spatiotemporal patterns of A(H5Nx) virus diffusion to/from and within Europe during the 2020–2021 and 2021–2022 epidemic waves, providing evidence of ongoing changes in transmission dynamics and disease epidemiology. We demonstrated the high genetic diversity of the circulating viruses, which have undergone frequent reassortment events, providing for the first time a complete overview and a proposed nomenclature of the multiple genotypes circulating in Europe in 2020–2022. We described the emergence of a new genotype with gull adapted genes, which offered the virus the opportunity to occupy new ecological niches, driving the disease endemicity in the European wild bird population. The high propensity of the virus for reassortment, its jumps to a progressively wider number of host species, including mammals, and the rapid acquisition of adaptive mutations make the trend of virus evolution and spread difficult to predict in this unfailing evolving scenario., Since 2016, A(H5Nx) high pathogenic avian influenza (HPAI) virus of clade 2.3.4.4b has become one of the most serious global threats not only to wild and domestic birds, but also to public health. In recent years, important changes in the ecology, epidemiology, and evolution of this virus have been reported, with an unprecedented global diffusion and variety of affected birds and mammalian species. After the two consecutive and devastating epidemic waves in Europe in 2020-2021 and 2021-2022, with the second one recognized as one of the largest epidemics recorded so far, this clade has begun to circulate endemically in European wild bird populations. This study used the complete genomes of 1,956 European HPAI A(H5Nx) viruses to investigate the virus evolution during this varying epidemiological outline. We investigated the spatiotemporal patterns of A(H5Nx) virus diffusion to/from and within Europe during the 2020-2021 and 2021-2022 epidemic waves, providing evidence of ongoing changes in transmission dynamics and disease epidemiology. We demonstrated the high genetic diversity of the circulating viruses, which have undergone frequent reassortment events, providing for the first time a complete overview and a proposed nomenclature of the multiple genotypes circulating in Europe in 2020-2022. We described the emergence of a new genotype with gull adapted genes, which offered the virus the opportunity to occupy new ecological niches, driving the disease endemicity in the European wild bird population. The high propensity of the virus for reassortment, its jumps to a progressively wider number of host species, including mammals, and the rapid acquisition of adaptive mutations make the trend of virus evolution and spread difficult to predict in this unfailing evolving scenario.

Published
2024

3. A multi gene-approach genotyping method identifies 24 genetic clusters within the genotype II-European African swine fever viruses circulating from 2007 to 2022

Author

Gallardo, Carmina, Casado, Nadia, Soler, Alejandro, Djadjovski, Igor, Krivko, Laura, Madueno, Encarnacion, Nieto, Raquel, Perez, Covadonga, Simon, Alicia, Ivanova, Emiliya, Donescu, Daniel, Milićević, Vesna, Chondrokouki, Eleni, Nurmoja, Imbi, Frant, Maciej, Feliziani, Francesco, Vaclavek, Petr, Pileviciene, Simona, Marisa, Arias, Gallardo, Carmina, Casado, Nadia, Soler, Alejandro, Djadjovski, Igor, Krivko, Laura, Madueno, Encarnacion, Nieto, Raquel, Perez, Covadonga, Simon, Alicia, Ivanova, Emiliya, Donescu, Daniel, Milićević, Vesna, Chondrokouki, Eleni, Nurmoja, Imbi, Frant, Maciej, Feliziani, Francesco, Vaclavek, Petr, Pileviciene, Simona, and Marisa, Arias

Abstract

IntroductionAfrican swine fever (ASF) is a contagious viral disease of pigs and wild boar that poses a major threat to the global swine industry. The genotype II African swine fever virus (ASFV) entered the European Union (EU) in 2014 and since then fourteen countries have been affected, Italy and North Macedonia being the last in 2022. While whole genome sequencing remains the gold standard for the identification of new genetic markers, sequencing of multiple loci with significant variations could be used as a rapid and cost-effective alternative to track outbreaks and study disease evolution in endemic areas. Materials and methodsTo further our understanding of the epidemiology and spread of ASFV in Europe, 382 isolates collected during 2007 to 2022 were sequenced. The study was initially performed by sequencing the central variable region (CVR), the intergenic region (IGR) between the I73R and I329L genes and the O174L and K145R genes. For further discrimination, two new PCRs were designed to amplify the IGR between the 9R and 10R genes of the multigene family 505 (MGF505) and the IGR between the I329L and I215L genes. The sequences obtained were compared with genotype II isolates from Europe and Asia. ResultsThe combination of the results obtained by sequencing these variable regions allowed to differentiate the European II-ASFV genotypes into 24 different groups. In addition, the SNP identified in the IGR I329L-I215L region, not previously described, grouped the viruses from North Macedonia that caused the 2022 outbreaks with viruses from Romania, Bulgaria, Serbia and Greece, differentiating from other genotype II isolates present in Europe and Asia. Furthermore, tandem repeat sequence (TRS) within the 9R-10R genes of the multigene family 505 (MGF505) revealed eight different variants circulating. DiscussionThese findings describe a new multi-gene approach sequencing method that can be used in routine genotyping to determine the origin of new introductions in A

Published
2023

4. A multi gene-approach genotyping method identifies 24 genetic clusters within the genotype II-European African swine fever viruses circulating from 2007 to 2022

Author

European Commission, Gallardo, Carmina [0000-0003-3293-306X], Djadjovski, Igor [0000-0002-4820-3590], Krivko, Laura [0009-0000-3047-4061], Chondrokouki, Eleni [0000-0002-8476-1821], Frant, Maciej [0000-0002-7169-3735], Pileviciene, Simona [0000-0002-0262-3899], Gallardo, Carmina, Casado, Nadia, Soler, Alejandro, Djadjovski, Igor, Krivko, Laura, Madueño, Encarnación, Nieto, Raquel, Pérez, Covadonga, Simón, Alicia, Ivanova, Emiliya, Donescu, Daniel, Milicevik, Vesna, Chondrokouki, Eleni, Nurmoja, Imbi, Frant, Maciej, Feliziani, Francesco, Václavek, Petr, Pileviciene, Simona, Marisa, Arias, European Commission, Gallardo, Carmina [0000-0003-3293-306X], Djadjovski, Igor [0000-0002-4820-3590], Krivko, Laura [0009-0000-3047-4061], Chondrokouki, Eleni [0000-0002-8476-1821], Frant, Maciej [0000-0002-7169-3735], Pileviciene, Simona [0000-0002-0262-3899], Gallardo, Carmina, Casado, Nadia, Soler, Alejandro, Djadjovski, Igor, Krivko, Laura, Madueño, Encarnación, Nieto, Raquel, Pérez, Covadonga, Simón, Alicia, Ivanova, Emiliya, Donescu, Daniel, Milicevik, Vesna, Chondrokouki, Eleni, Nurmoja, Imbi, Frant, Maciej, Feliziani, Francesco, Václavek, Petr, Pileviciene, Simona, and Marisa, Arias

Abstract

African swine fever (ASF) is a contagious viral disease of pigs and wild boar that poses a major threat to the global swine industry. The genotype II African swine fever virus (ASFV) entered the European Union (EU) in 2014 and since then fourteen countries have been affected, Italy and North Macedonia being the last in 2022. While whole genome sequencing remains the gold standard for the identification of new genetic markers, sequencing of multiple loci with significant variations could be used as a rapid and cost-effective alternative to track outbreaks and study disease evolution in endemic areas.

Published
2023

5. A multi gene-approach genotyping method identifies 24 genetic clusters within the genotype II-European African swine fever viruses circulating from 2007 to 2022

Author

Gallardo, Carmina, primary, Casado, Nadia, additional, Soler, Alejandro, additional, Djadjovski, Igor, additional, Krivko, Laura, additional, Madueño, Encarnación, additional, Nieto, Raquel, additional, Perez, Covadonga, additional, Simon, Alicia, additional, Ivanova, Emiliya, additional, Donescu, Daniel, additional, Milicevik, Vesna, additional, Chondrokouki, Eleni, additional, Nurmoja, Imbi, additional, Frant, Maciej, additional, Feliziani, Francesco, additional, Václavek, Petr, additional, Pileviciene, Simona, additional, and Marisa, Arias, additional

Published
2023
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6. Development and Optimization of Indirect ELISAs for the Detection of Anti-Capripoxvirus Antibodies in Cattle, Sheep, and Goat Sera

Author

Berguido, Francisco J., primary, Gelaye, Esayas, additional, Liu, Yang, additional, Davaasuren, Batdorj, additional, Krstevski, Kiril, additional, Djadjovski, Igor, additional, Ivanova, Emiliya, additional, Goujgoulova, Gabriela, additional, Loitsch, Angelika, additional, Tuppurainen, Eeva, additional, Chibssa, Tesfaye Rufael, additional, Caufour, Philippe, additional, Samojlović, Milena, additional, Lazić, Sava, additional, Petrović, Tamaš, additional, Vidanović, Dejan, additional, Bertagnoli, Stéphane, additional, Grabherr, Reingard, additional, Diallo, Adama, additional, Cattoli, Giovanni, additional, and Lamien, Charles Euloge, additional

Published
2022
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7. Development and optimization of indirect ELISAs for the detection of anti-capripoxvirus antibodies in cattle, sheep, and goat sera

Author

Berguido, Francisco, Gelaye, Esayas, Liu, Yang, Davaasuren, Batdorj, Krstevski, Kiril, Djadjovski, Igor, Ivanova, Emiliya, Goujgoulova, Gabriela V., Loitsch, Angelika, Tuppurainen, Eeva, Chibssa, Tesfaye Rufael, Caufour, Philippe, Samojlović, Milena, Lazić, Sava, Petrović, Tamaš, Vidanović, Dejan, Bertagnoli, Stéphane, Grabherr, Reingard, Diallo, Adama, Cattoli, Giovanni, Lamien, Charles Euloge, Berguido, Francisco, Gelaye, Esayas, Liu, Yang, Davaasuren, Batdorj, Krstevski, Kiril, Djadjovski, Igor, Ivanova, Emiliya, Goujgoulova, Gabriela V., Loitsch, Angelika, Tuppurainen, Eeva, Chibssa, Tesfaye Rufael, Caufour, Philippe, Samojlović, Milena, Lazić, Sava, Petrović, Tamaš, Vidanović, Dejan, Bertagnoli, Stéphane, Grabherr, Reingard, Diallo, Adama, Cattoli, Giovanni, and Lamien, Charles Euloge

Abstract

Sheeppox (SPP), goatpox (GTP), and lumpy skin disease (LSD) are economically significant pox diseases of ruminants, caused by sheeppox virus (SPPV), goatpox virus (GTPV), and lumpy skin disease virus (LSDV), respectively. SPPV and GTPV can infect both sheep and goats, while LSDV mainly affects cattle. The recent emergence of LSD in Asia and Europe and the repeated incursions of SPP in Greece, Bulgaria, and Russia highlight how these diseases can spread outside their endemic regions, stressing the urgent need to develop high-throughput serological surveillance tools. We expressed and tested two recombinant truncated proteins, the capripoxvirus homologs of the vaccinia virus C-type lectin-like protein A34 and the EEV glycoprotein A36, as antigens for an indirect ELISA (iELISA) to detect anti-capripoxvirus antibodies. Since A34 outperformed A36 by showing no cross-reactivity to anti-parapoxvirus antibodies, we optimized an A34 iELISA using two different working conditions, one for LSD in cattle and one for SPP/GTP in sheep and goats. Both displayed sound sensitivities and specificities: 98.81% and 98.72%, respectively, for the LSD iELISA, and 97.68% and 95.35%, respectively, for the SPP/GTP iELISA, and did not cross-react with anti-parapoxvirus antibodies of cattle, sheep, and goats. These assays could facilitate the implementation of capripox control programs through serosurveillance and the screening of animals for trade.

Published
2022

9. DETERMINATION OF THE INTRA PARTICLE MASS TRANSFER RESISTANCE OF SO2 ADSORPTION ON NATURAL CLINOPTILOLITE.

Author

Kostova, Miryana A., Ivanova, Emiliya P., and Stefanov, Georgi C.

Subjects
*MASS transfer, *GAS absorption & adsorption, *CLINOPTILOLITE, *WASTE gases, *SULFUR dioxide mitigation, *INDUSTRIAL wastes
Abstract

Natural clinoptilolite is a suitable adsorbent for polar molecules such as water, alcohols and many other adsorptive components and it is also very selective in removing sulfur dioxide at low concentrations from gaseous mixtures such as the undesired industrial waste gases. This paper investigates the fixed bed adsorption of sulfur dioxide by natural clinoptilolite in labo ra tory scale in order to determine the Intra Particle Mass Transfer Resistance of the process. Several experimental adsorption runs at different fixed bed lengths and gas flow velo cities were made to achieve the Constant Pattern (CP) behavior and the CP--Break through Curves (BTC) were further examined though their Breakthrough Points and statistical characteristics (1st absolute and 2nd central statistical moments) by means of the Intra Particle Linear Driving Force Model (LDFQ) and the simple linear Shilov's relation in order to estimate the Intra Par ticle Mass Transfer Resistance. The results were quantitatively discussed in comparison to the Macro Pore Mass Transfer Resistance, using the binary molecular and Knudsen diffu si vi ties and in accordance with the bi-porous structure of the zeolite as well. A comparison was also made to the Intra Particle Mass Transfer Resistance from the Intra Particle Diffusion Model (DMQ) at Langmuir and at linear equilibrium. [ABSTRACT FROM AUTHOR]

Published
2015

10. High pathogenic avian influenza A(H5) viruses of clade 2.3.4.4b in Europe-Why trends of virus evolution are more difficult to predict.

Author

Fusaro A, Zecchin B, Giussani E, Palumbo E, Agüero-García M, Bachofen C, Bálint Á, Banihashem F, Banyard AC, Beerens N, Bourg M, Briand FX, Bröjer C, Brown IH, Brugger B, Byrne AMP, Cana A, Christodoulou V, Dirbakova Z, Fagulha T, Fouchier RAM, Garza-Cuartero L, Georgiades G, Gjerset B, Grasland B, Groza O, Harder T, Henriques AM, Hjulsager CK, Ivanova E, Janeliunas Z, Krivko L, Lemon K, Liang Y, Lika A, Malik P, McMenamy MJ, Nagy A, Nurmoja I, Onita I, Pohlmann A, Revilla-Fernández S, Sánchez-Sánchez A, Savic V, Slavec B, Smietanka K, Snoeck CJ, Steensels M, Svansson V, Swieton E, Tammiranta N, Tinak M, Van Borm S, Zohari S, Adlhoch C, Baldinelli F, Terregino C, and Monne I

Abstract

Since 2016, A(H5Nx) high pathogenic avian influenza (HPAI) virus of clade 2.3.4.4b has become one of the most serious global threats not only to wild and domestic birds, but also to public health. In recent years, important changes in the ecology, epidemiology, and evolution of this virus have been reported, with an unprecedented global diffusion and variety of affected birds and mammalian species. After the two consecutive and devastating epidemic waves in Europe in 2020-2021 and 2021-2022, with the second one recognized as one of the largest epidemics recorded so far, this clade has begun to circulate endemically in European wild bird populations. This study used the complete genomes of 1,956 European HPAI A(H5Nx) viruses to investigate the virus evolution during this varying epidemiological outline. We investigated the spatiotemporal patterns of A(H5Nx) virus diffusion to/from and within Europe during the 2020-2021 and 2021-2022 epidemic waves, providing evidence of ongoing changes in transmission dynamics and disease epidemiology. We demonstrated the high genetic diversity of the circulating viruses, which have undergone frequent reassortment events, providing for the first time a complete overview and a proposed nomenclature of the multiple genotypes circulating in Europe in 2020-2022. We described the emergence of a new genotype with gull adapted genes, which offered the virus the opportunity to occupy new ecological niches, driving the disease endemicity in the European wild bird population. The high propensity of the virus for reassortment, its jumps to a progressively wider number of host species, including mammals, and the rapid acquisition of adaptive mutations make the trend of virus evolution and spread difficult to predict in this unfailing evolving scenario., Competing Interests: None declared., (© The Author(s) 2024. Published by Oxford University Press.)

Published
2024
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