Your search keyword '"Armando, Federico"' showing total 26 results

1. Filamentous fungus-produced human monoclonal antibody provides protection against SARS-CoV-2 in hamster and non-human primate models

Author

Kaiser, Franziska K, Hernandez, Mariana Gonzalez, Krüger, Nadine, Englund, Ellinor, Du, Wenjuan, Mykytyn, Anna Z, Raadsen, Mathijs P, Lamers, Mart M, Rodrigues Ianiski, Francine, Shamorkina, Tatiana M, Snijder, Joost, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Schreiner, Tom, Gruber-Dujardin, Eva, Bleyer, Martina, Batura, Olga, Erffmeier, Lena, Hinkel, Rabea, Rocha, Cheila, Mirolo, Monica, Drabek, Dubravka, Bosch, Berend-Jan, Emalfarb, Mark, Valbuena, Noelia, Tchelet, Ronen, Baumgärtner, Wolfgang, Saloheimo, Markku, Pöhlmann, Stefan, Grosveld, Frank, Haagmans, Bart L, Osterhaus, Albert D M E, Kaiser, Franziska K, Hernandez, Mariana Gonzalez, Krüger, Nadine, Englund, Ellinor, Du, Wenjuan, Mykytyn, Anna Z, Raadsen, Mathijs P, Lamers, Mart M, Rodrigues Ianiski, Francine, Shamorkina, Tatiana M, Snijder, Joost, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Schreiner, Tom, Gruber-Dujardin, Eva, Bleyer, Martina, Batura, Olga, Erffmeier, Lena, Hinkel, Rabea, Rocha, Cheila, Mirolo, Monica, Drabek, Dubravka, Bosch, Berend-Jan, Emalfarb, Mark, Valbuena, Noelia, Tchelet, Ronen, Baumgärtner, Wolfgang, Saloheimo, Markku, Pöhlmann, Stefan, Grosveld, Frank, Haagmans, Bart L, and Osterhaus, Albert D M E

Abstract

Monoclonal antibodies are an increasingly important tool for prophylaxis and treatment of acute virus infections like SARS-CoV-2 infection. However, their use is often restricted due to the time required for development, variable yields and high production costs, as well as the need for adaptation to newly emerging virus variants. Here we use the genetically modified filamentous fungus expression system Thermothelomyces heterothallica (C1), which has a naturally high biosynthesis capacity for secretory enzymes and other proteins, to produce a human monoclonal IgG1 antibody (HuMab 87G7) that neutralises the SARS-CoV-2 variants of concern (VOCs) Alpha, Beta, Gamma, Delta, and Omicron. Both the mammalian cell and C1 produced HuMab 87G7 broadly neutralise SARS-CoV-2 VOCs in vitro and also provide protection against VOC Omicron in hamsters. The C1 produced HuMab 87G7 is also able to protect against the Delta VOC in non-human primates. In summary, these findings show that the C1 expression system is a promising technology platform for the development of HuMabs in preventive and therapeutic medicine.

Published

2024

2. Filamentous fungus-produced human monoclonal antibody provides protection against SARS-CoV-2 in hamster and non-human primate models

Author

Virologie, Afd Biomol.Mass Spect. and Proteomics, Sub Biomol.Mass Spectrometry & Proteom., Infectious Diseases and Immunology - Virology, Kaiser, Franziska K, Hernandez, Mariana Gonzalez, Krüger, Nadine, Englund, Ellinor, Du, Wenjuan, Mykytyn, Anna Z, Raadsen, Mathijs P, Lamers, Mart M, Rodrigues Ianiski, Francine, Shamorkina, Tatiana M, Snijder, Joost, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Schreiner, Tom, Gruber-Dujardin, Eva, Bleyer, Martina, Batura, Olga, Erffmeier, Lena, Hinkel, Rabea, Rocha, Cheila, Mirolo, Monica, Drabek, Dubravka, Bosch, Berend-Jan, Emalfarb, Mark, Valbuena, Noelia, Tchelet, Ronen, Baumgärtner, Wolfgang, Saloheimo, Markku, Pöhlmann, Stefan, Grosveld, Frank, Haagmans, Bart L, Osterhaus, Albert D M E, Virologie, Afd Biomol.Mass Spect. and Proteomics, Sub Biomol.Mass Spectrometry & Proteom., Infectious Diseases and Immunology - Virology, Kaiser, Franziska K, Hernandez, Mariana Gonzalez, Krüger, Nadine, Englund, Ellinor, Du, Wenjuan, Mykytyn, Anna Z, Raadsen, Mathijs P, Lamers, Mart M, Rodrigues Ianiski, Francine, Shamorkina, Tatiana M, Snijder, Joost, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Schreiner, Tom, Gruber-Dujardin, Eva, Bleyer, Martina, Batura, Olga, Erffmeier, Lena, Hinkel, Rabea, Rocha, Cheila, Mirolo, Monica, Drabek, Dubravka, Bosch, Berend-Jan, Emalfarb, Mark, Valbuena, Noelia, Tchelet, Ronen, Baumgärtner, Wolfgang, Saloheimo, Markku, Pöhlmann, Stefan, Grosveld, Frank, Haagmans, Bart L, and Osterhaus, Albert D M E

Published

2024

3. Filamentous fungus-produced human monoclonal antibody provides protection against SARS-CoV-2 in hamster and non-human primate models

Author

Kaiser, Franziska K., Hernandez, Mariana Gonzalez, Krüger, Nadine, Englund, Ellinor, Du, Wenjuan, Mykytyn, Anna Z., Raadsen, Mathijs P., Lamers, Mart M., Rodrigues Ianiski, Francine, Shamorkina, Tatiana M., Snijder, Joost, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Schreiner, Tom, Gruber-Dujardin, Eva, Bleyer, Martina, Batura, Olga, Erffmeier, Lena, Hinkel, Rabea, Rocha, Cheila, Mirolo, Monica, Drabek, Dubravka, Bosch, Berend Jan, Emalfarb, Mark, Valbuena, Noelia, Tchelet, Ronen, Baumgärtner, Wolfgang, Saloheimo, Markku, Pöhlmann, Stefan, Grosveld, Frank, Haagmans, Bart L., Osterhaus, Albert D.M.E., Kaiser, Franziska K., Hernandez, Mariana Gonzalez, Krüger, Nadine, Englund, Ellinor, Du, Wenjuan, Mykytyn, Anna Z., Raadsen, Mathijs P., Lamers, Mart M., Rodrigues Ianiski, Francine, Shamorkina, Tatiana M., Snijder, Joost, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Schreiner, Tom, Gruber-Dujardin, Eva, Bleyer, Martina, Batura, Olga, Erffmeier, Lena, Hinkel, Rabea, Rocha, Cheila, Mirolo, Monica, Drabek, Dubravka, Bosch, Berend Jan, Emalfarb, Mark, Valbuena, Noelia, Tchelet, Ronen, Baumgärtner, Wolfgang, Saloheimo, Markku, Pöhlmann, Stefan, Grosveld, Frank, Haagmans, Bart L., and Osterhaus, Albert D.M.E.

Abstract

Monoclonal antibodies are an increasingly important tool for prophylaxis and treatment of acute virus infections like SARS-CoV-2 infection. However, their use is often restricted due to the time required for development, variable yields and high production costs, as well as the need for adaptation to newly emerging virus variants. Here we use the genetically modified filamentous fungus expression system Thermothelomyces heterothallica (C1), which has a naturally high biosynthesis capacity for secretory enzymes and other proteins, to produce a human monoclonal IgG1 antibody (HuMab 87G7) that neutralises the SARS-CoV-2 variants of concern (VOCs) Alpha, Beta, Gamma, Delta, and Omicron. Both the mammalian cell and C1 produced HuMab 87G7 broadly neutralise SARS-CoV-2 VOCs in vitro and also provide protection against VOC Omicron in hamsters. The C1 produced HuMab 87G7 is also able to protect against the Delta VOC in non-human primates. In summary, these findings show that the C1 expression system is a promising technology platform for the development of HuMabs in preventive and therapeutic medicine.

Published

2024

4. An ACE2-blocking antibody confers broad neutralization and protection against Omicron and other SARS-CoV-2 variants of concern

Author

European Commission, German Research Foundation, Federal Ministry of Education and Research (Germany), Ministry for Science and Culture of Lower Saxony, Du, Wenjuan [0000-0002-0790-9546], Hurdiss, Daniel L. [0000-0003-3834-5808], Drabek, Dubravka [0000-0002-9781-1701], Mykytyn, Anna Z. [0000-0001-7188-6871], González-Hernandez, Mariana [0000-0001-7019-2165], Muñoz-Santos, Diego [0000-0003-0591-0874], Lamers, Mart M. [0000-0002-1431-4022], Haperen, Rien van [0000-0001-9649-011X], Li, Wentao [0000-0002-7114-762X], Drulyte, Ieva [0000-0003-1117-7699], Wang, Chunyan [0000-0002-4584-259X], Solá Gurpegui, Isabel [0000-0002-5704-1917], Armando, Federico [0000-0002-2578-4409], Beythien, Georg [0000-0002-2192-2413], Ciurkiewicz, Malgorzata [0000-0001-6277-7366], Baumgärtner, Wolfgang [0000-0001-8151-5644], Guilfoyle, Kate [0000-0001-7292-3021], Kuppeveld, Frank J. M. van [0000-0001-5800-749X], Amerongen, Geert van [0000-0002-5469-6029], Haagmans, Bart L. [0000-0001-6221-2015], Enjuanes Sánchez, Luis [0000-0002-0854-0226], Osterhaus, Albert D. M. E. [0000-0001-6535-3497], Grosveld, Frank [0000-0002-7051-4715], Du, Wenjuan, Hurdiss, Daniel L., Drabek, Dubravka, Mykytyn, Anna Z., Kaiser, Franziska K., González-Hernandez, Mariana, Muñoz-Santos, Diego, Lamers, Mart M., Haperen, Rien van, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Solá Gurpegui, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, Lee, Joline van der, Kuppeveld, Frank J. M. van, Amerongen, Geert van, Haagmans, Bart L., Enjuanes Sánchez, Luis, Osterhaus, Albert D. M. E., Grosveld, Frank, Bosch, Berend Jan, European Commission, German Research Foundation, Federal Ministry of Education and Research (Germany), Ministry for Science and Culture of Lower Saxony, Du, Wenjuan [0000-0002-0790-9546], Hurdiss, Daniel L. [0000-0003-3834-5808], Drabek, Dubravka [0000-0002-9781-1701], Mykytyn, Anna Z. [0000-0001-7188-6871], González-Hernandez, Mariana [0000-0001-7019-2165], Muñoz-Santos, Diego [0000-0003-0591-0874], Lamers, Mart M. [0000-0002-1431-4022], Haperen, Rien van [0000-0001-9649-011X], Li, Wentao [0000-0002-7114-762X], Drulyte, Ieva [0000-0003-1117-7699], Wang, Chunyan [0000-0002-4584-259X], Solá Gurpegui, Isabel [0000-0002-5704-1917], Armando, Federico [0000-0002-2578-4409], Beythien, Georg [0000-0002-2192-2413], Ciurkiewicz, Malgorzata [0000-0001-6277-7366], Baumgärtner, Wolfgang [0000-0001-8151-5644], Guilfoyle, Kate [0000-0001-7292-3021], Kuppeveld, Frank J. M. van [0000-0001-5800-749X], Amerongen, Geert van [0000-0002-5469-6029], Haagmans, Bart L. [0000-0001-6221-2015], Enjuanes Sánchez, Luis [0000-0002-0854-0226], Osterhaus, Albert D. M. E. [0000-0001-6535-3497], Grosveld, Frank [0000-0002-7051-4715], Du, Wenjuan, Hurdiss, Daniel L., Drabek, Dubravka, Mykytyn, Anna Z., Kaiser, Franziska K., González-Hernandez, Mariana, Muñoz-Santos, Diego, Lamers, Mart M., Haperen, Rien van, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Solá Gurpegui, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, Lee, Joline van der, Kuppeveld, Frank J. M. van, Amerongen, Geert van, Haagmans, Bart L., Enjuanes Sánchez, Luis, Osterhaus, Albert D. M. E., Grosveld, Frank, and Bosch, Berend Jan

Abstract

The ongoing evolution of SARS-CoV-2 has resulted in the emergence of Omicron, which displays striking immune escape potential through mutations at key antigenic sites on the spike protein. Many of these mutations localize to the spike protein ACE2 receptor-binding domain, annulling the neutralizing activity of therapeutic antibodies that were effective against other Variants of Concern (VOCs) earlier in the pandemic. Here, we identified a receptor-blocking human monoclonal antibody, 87G7, that retained potent in vitro neutralizing activity against SARS-CoV-2 variants including the Alpha, Beta, Gamma, Delta and Omicron (BA.1/BA.2) VOCs. Using cryo-electron microscopy and site-directed mutagenesis experiments, we showed that 87G7 targets a patch of hydrophobic residues in the ACE2-binding site that are highly conserved in SARS-CoV-2 variants, explaining its broad neutralization capacity. 87G7 protected mice and/or hamsters prophylactically against challenge with all current SARS-CoV-2 VOCs, and showed therapeutic activity against SARS-CoV-2 challenge in both animal models. Our findings demonstrate that 87G7 holds promise as a prophylactic or therapeutic agent for COVID-19 that is more resilient to SARS-CoV-2 antigenic diversity.

Published

2022

5. Functional Granulocyte–Macrophage Colony-Stimulating Factor (GM-CSF) Delivered by Canine Histiocytic Sarcoma Cells Persistently Infected with Engineered Attenuated Canine Distemper Virus

Author

Marek, Katarzyna, Armando, Federico, Asawapattanakul, Thanaporn, Nippold, Vanessa Maria, Plattet, Philippe, Gerold, Gisa, Baumgärtner, Wolfgang, Puff, Christina, Marek, Katarzyna, Armando, Federico, Asawapattanakul, Thanaporn, Nippold, Vanessa Maria, Plattet, Philippe, Gerold, Gisa, Baumgärtner, Wolfgang, and Puff, Christina

Abstract

The immune response plays a key role in the treatment of malignant tumors. One important molecule promoting humoral and cellular immunity is granulocyte–macrophage colony-stimulating factor (GM-CSF). Numerous successful trials have led to the approval of this immune-stimulating molecule for cancer therapy. However, besides immune stimulation, GM-CSF may also accelerate tumor cell proliferation, rendering this molecule a double-edged sword in cancer treatment. Therefore, detailed knowledge about the in vitro function of GM-CSF produced by infected tumor cells is urgently needed prior to investigations in an in vivo model. The aim of the present study was to functionally characterize a persistent infection of canine histiocytic sarcoma cells (DH82 cells) with the canine distemper virus strain Onderstepoort genetically engineered to express canine GM-CSF (CDV-Ondneon-GM-CSF). The investigations aimed (1) to prove the overall functionality of the virally induced production of GM-CSF and (2) to determine the effect of GM-CSF on the proliferation and motility of canine HS cells. Infected cells consistently produced high amounts of active, pH-stable GM-CSF, as demonstrated by increased proliferation of HeLa cells. By contrast, DH82 cells lacked increased proliferation and motility. The significantly increased secretion of GM-CSF by persistently CDV-Ondneon-GM-CSF-infected DH82 cells, the pH stability of this protein, and the lack of detrimental effects on DH82 cells renders this virus strain an interesting candidate for future studies aiming to enhance the oncolytic properties of CDV for the treatment of canine histiocytic sarcomas.

Published

2023

6. Functional Granulocyte–Macrophage Colony-Stimulating Factor (GM-CSF) Delivered by Canine Histiocytic Sarcoma Cells Persistently Infected with Engineered Attenuated Canine Distemper Virus

Author

Marek, Katarzyna, Armando, Federico, Asawapattanakul, Thanaporn, Nippold, Vanessa Maria, Plattet, Philippe, Gerold, Gisa, Baumgärtner, Wolfgang, Puff, Christina, Marek, Katarzyna, Armando, Federico, Asawapattanakul, Thanaporn, Nippold, Vanessa Maria, Plattet, Philippe, Gerold, Gisa, Baumgärtner, Wolfgang, and Puff, Christina

Abstract

The immune response plays a key role in the treatment of malignant tumors. One important molecule promoting humoral and cellular immunity is granulocyte–macrophage colony-stimulating factor (GM-CSF). Numerous successful trials have led to the approval of this immune-stimulating molecule for cancer therapy. However, besides immune stimulation, GM-CSF may also accelerate tumor cell proliferation, rendering this molecule a double-edged sword in cancer treatment. Therefore, detailed knowledge about the in vitro function of GM-CSF produced by infected tumor cells is urgently needed prior to investigations in an in vivo model. The aim of the present study was to functionally characterize a persistent infection of canine histiocytic sarcoma cells (DH82 cells) with the canine distemper virus strain Onderstepoort genetically engineered to express canine GM-CSF (CDV-Ondneon-GM-CSF). The investigations aimed (1) to prove the overall functionality of the virally induced production of GM-CSF and (2) to determine the effect of GM-CSF on the proliferation and motility of canine HS cells. Infected cells consistently produced high amounts of active, pH-stable GM-CSF, as demonstrated by increased proliferation of HeLa cells. By contrast, DH82 cells lacked increased proliferation and motility. The significantly increased secretion of GM-CSF by persistently CDV-Ondneon-GM-CSF-infected DH82 cells, the pH stability of this protein, and the lack of detrimental effects on DH82 cells renders this virus strain an interesting candidate for future studies aiming to enhance the oncolytic properties of CDV for the treatment of canine histiocytic sarcomas.

Published

2023

7. Functional Granulocyte–Macrophage Colony-Stimulating Factor (GM-CSF) Delivered by Canine Histiocytic Sarcoma Cells Persistently Infected with Engineered Attenuated Canine Distemper Virus

Author

Marek, Katarzyna, Armando, Federico, Asawapattanakul, Thanaporn, Nippold, Vanessa Maria, Plattet, Philippe, Gerold, Gisa, Baumgärtner, Wolfgang, Puff, Christina, Marek, Katarzyna, Armando, Federico, Asawapattanakul, Thanaporn, Nippold, Vanessa Maria, Plattet, Philippe, Gerold, Gisa, Baumgärtner, Wolfgang, and Puff, Christina

Abstract

The immune response plays a key role in the treatment of malignant tumors. One important molecule promoting humoral and cellular immunity is granulocyte–macrophage colony-stimulating factor (GM-CSF). Numerous successful trials have led to the approval of this immune-stimulating molecule for cancer therapy. However, besides immune stimulation, GM-CSF may also accelerate tumor cell proliferation, rendering this molecule a double-edged sword in cancer treatment. Therefore, detailed knowledge about the in vitro function of GM-CSF produced by infected tumor cells is urgently needed prior to investigations in an in vivo model. The aim of the present study was to functionally characterize a persistent infection of canine histiocytic sarcoma cells (DH82 cells) with the canine distemper virus strain Onderstepoort genetically engineered to express canine GM-CSF (CDV-Ondneon-GM-CSF). The investigations aimed (1) to prove the overall functionality of the virally induced production of GM-CSF and (2) to determine the effect of GM-CSF on the proliferation and motility of canine HS cells. Infected cells consistently produced high amounts of active, pH-stable GM-CSF, as demonstrated by increased proliferation of HeLa cells. By contrast, DH82 cells lacked increased proliferation and motility. The significantly increased secretion of GM-CSF by persistently CDV-Ondneon-GM-CSF-infected DH82 cells, the pH stability of this protein, and the lack of detrimental effects on DH82 cells renders this virus strain an interesting candidate for future studies aiming to enhance the oncolytic properties of CDV for the treatment of canine histiocytic sarcomas.

Published

2023

8. Functional Granulocyte–Macrophage Colony-Stimulating Factor (GM-CSF) Delivered by Canine Histiocytic Sarcoma Cells Persistently Infected with Engineered Attenuated Canine Distemper Virus

Author

Marek, Katarzyna, Armando, Federico, Asawapattanakul, Thanaporn, Nippold, Vanessa Maria, Plattet, Philippe, Gerold, Gisa, Baumgärtner, Wolfgang, Puff, Christina, Marek, Katarzyna, Armando, Federico, Asawapattanakul, Thanaporn, Nippold, Vanessa Maria, Plattet, Philippe, Gerold, Gisa, Baumgärtner, Wolfgang, and Puff, Christina

Abstract

The immune response plays a key role in the treatment of malignant tumors. One important molecule promoting humoral and cellular immunity is granulocyte–macrophage colony-stimulating factor (GM-CSF). Numerous successful trials have led to the approval of this immune-stimulating molecule for cancer therapy. However, besides immune stimulation, GM-CSF may also accelerate tumor cell proliferation, rendering this molecule a double-edged sword in cancer treatment. Therefore, detailed knowledge about the in vitro function of GM-CSF produced by infected tumor cells is urgently needed prior to investigations in an in vivo model. The aim of the present study was to functionally characterize a persistent infection of canine histiocytic sarcoma cells (DH82 cells) with the canine distemper virus strain Onderstepoort genetically engineered to express canine GM-CSF (CDV-Ondneon-GM-CSF). The investigations aimed (1) to prove the overall functionality of the virally induced production of GM-CSF and (2) to determine the effect of GM-CSF on the proliferation and motility of canine HS cells. Infected cells consistently produced high amounts of active, pH-stable GM-CSF, as demonstrated by increased proliferation of HeLa cells. By contrast, DH82 cells lacked increased proliferation and motility. The significantly increased secretion of GM-CSF by persistently CDV-Ondneon-GM-CSF-infected DH82 cells, the pH stability of this protein, and the lack of detrimental effects on DH82 cells renders this virus strain an interesting candidate for future studies aiming to enhance the oncolytic properties of CDV for the treatment of canine histiocytic sarcomas.

Published

2023

9. Functional Granulocyte–Macrophage Colony-Stimulating Factor (GM-CSF) Delivered by Canine Histiocytic Sarcoma Cells Persistently Infected with Engineered Attenuated Canine Distemper Virus

Author

Marek, Katarzyna, Armando, Federico, Asawapattanakul, Thanaporn, Nippold, Vanessa Maria, Plattet, Philippe, Gerold, Gisa, Baumgärtner, Wolfgang, Puff, Christina, Marek, Katarzyna, Armando, Federico, Asawapattanakul, Thanaporn, Nippold, Vanessa Maria, Plattet, Philippe, Gerold, Gisa, Baumgärtner, Wolfgang, and Puff, Christina

Abstract

The immune response plays a key role in the treatment of malignant tumors. One important molecule promoting humoral and cellular immunity is granulocyte–macrophage colony-stimulating factor (GM-CSF). Numerous successful trials have led to the approval of this immune-stimulating molecule for cancer therapy. However, besides immune stimulation, GM-CSF may also accelerate tumor cell proliferation, rendering this molecule a double-edged sword in cancer treatment. Therefore, detailed knowledge about the in vitro function of GM-CSF produced by infected tumor cells is urgently needed prior to investigations in an in vivo model. The aim of the present study was to functionally characterize a persistent infection of canine histiocytic sarcoma cells (DH82 cells) with the canine distemper virus strain Onderstepoort genetically engineered to express canine GM-CSF (CDV-Ondneon-GM-CSF). The investigations aimed (1) to prove the overall functionality of the virally induced production of GM-CSF and (2) to determine the effect of GM-CSF on the proliferation and motility of canine HS cells. Infected cells consistently produced high amounts of active, pH-stable GM-CSF, as demonstrated by increased proliferation of HeLa cells. By contrast, DH82 cells lacked increased proliferation and motility. The significantly increased secretion of GM-CSF by persistently CDV-Ondneon-GM-CSF-infected DH82 cells, the pH stability of this protein, and the lack of detrimental effects on DH82 cells renders this virus strain an interesting candidate for future studies aiming to enhance the oncolytic properties of CDV for the treatment of canine histiocytic sarcomas.

Published

2023

10. An ACE2-blocking antibody confers broad neutralization and protection against Omicron and other SARS-CoV-2 variants of concern

Author

Du, Wenjuan, Hurdiss, Daniel L, Drabek, Dubravka, Mykytyn, Anna Z, Kaiser, Franziska K, González-Hernández, Mariana, Muñoz-Santos, Diego, Lamers, Mart M, van Haperen, Rien, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Sola, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, van der Lee, Joline, van Kuppeveld, Frank J M, van Amerongen, Geert, Haagmans, Bart L, Enjuanes, Luis, Osterhaus, Albert D M E, Grosveld, Frank, Bosch, Berend-Jan, Du, Wenjuan, Hurdiss, Daniel L, Drabek, Dubravka, Mykytyn, Anna Z, Kaiser, Franziska K, González-Hernández, Mariana, Muñoz-Santos, Diego, Lamers, Mart M, van Haperen, Rien, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Sola, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, van der Lee, Joline, van Kuppeveld, Frank J M, van Amerongen, Geert, Haagmans, Bart L, Enjuanes, Luis, Osterhaus, Albert D M E, Grosveld, Frank, and Bosch, Berend-Jan

Abstract

The ongoing evolution of SARS-CoV-2 has resulted in the emergence of Omicron, which displays notable immune escape potential through mutations at key antigenic sites on the spike protein. Many of these mutations localize to the spike protein ACE2 receptor binding domain, annulling the neutralizing activity of therapeutic antibodies that were effective against other variants of concern (VOCs) earlier in the pandemic. Here, we identified a receptor-blocking human monoclonal antibody, 87G7, that retained potent in vitro neutralizing activity against SARS-CoV-2 variants including the Alpha, Beta, Gamma, Delta, and Omicron (BA.1/BA.2) VOCs. Using cryo-electron microscopy and site-directed mutagenesis experiments, we showed that 87G7 targets a patch of hydrophobic residues in the ACE2-binding site that are highly conserved in SARS-CoV-2 variants, explaining its broad neutralization capacity. 87G7 protected mice and hamsters prophylactically against challenge with all current SARS-CoV-2 VOCs and showed therapeutic activity against SARS-CoV-2 challenge in both animal models. Our findings demonstrate that 87G7 holds promise as a prophylactic or therapeutic agent for COVID-19 that is more resilient to SARS-CoV-2 antigenic diversity.

Published

2022

11. An ACE2-blocking antibody confers broad neutralization and protection against Omicron and other SARS-CoV-2 variants of concern

Author

Virologie, dI&I I&I-1, Bedrijfsvoering, Du, Wenjuan, Hurdiss, Daniel L, Drabek, Dubravka, Mykytyn, Anna Z, Kaiser, Franziska K, González-Hernández, Mariana, Muñoz-Santos, Diego, Lamers, Mart M, van Haperen, Rien, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Sola, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, van der Lee, Joline, van Kuppeveld, Frank J M, van Amerongen, Geert, Haagmans, Bart L, Enjuanes, Luis, Osterhaus, Albert D M E, Grosveld, Frank, Bosch, Berend-Jan, Virologie, dI&I I&I-1, Bedrijfsvoering, Du, Wenjuan, Hurdiss, Daniel L, Drabek, Dubravka, Mykytyn, Anna Z, Kaiser, Franziska K, González-Hernández, Mariana, Muñoz-Santos, Diego, Lamers, Mart M, van Haperen, Rien, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Sola, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, van der Lee, Joline, van Kuppeveld, Frank J M, van Amerongen, Geert, Haagmans, Bart L, Enjuanes, Luis, Osterhaus, Albert D M E, Grosveld, Frank, and Bosch, Berend-Jan

Published

2022

12. An ACE2-blocking antibody confers broad neutralization and protection against Omicron and other SARS-CoV-2 variants of concern

Author

Virologie, dI&I I&I-1, Bedrijfsvoering, Du, Wenjuan, Hurdiss, Daniel L, Drabek, Dubravka, Mykytyn, Anna Z, Kaiser, Franziska K, González-Hernández, Mariana, Muñoz-Santos, Diego, Lamers, Mart M, van Haperen, Rien, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Sola, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, van der Lee, Joline, van Kuppeveld, Frank J M, van Amerongen, Geert, Haagmans, Bart L, Enjuanes, Luis, Osterhaus, Albert D M E, Grosveld, Frank, Bosch, Berend-Jan, Virologie, dI&I I&I-1, Bedrijfsvoering, Du, Wenjuan, Hurdiss, Daniel L, Drabek, Dubravka, Mykytyn, Anna Z, Kaiser, Franziska K, González-Hernández, Mariana, Muñoz-Santos, Diego, Lamers, Mart M, van Haperen, Rien, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Sola, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, van der Lee, Joline, van Kuppeveld, Frank J M, van Amerongen, Geert, Haagmans, Bart L, Enjuanes, Luis, Osterhaus, Albert D M E, Grosveld, Frank, and Bosch, Berend-Jan

Published

2022

13. Persistent Infection of a Canine Histiocytic Sarcoma Cell Line with Attenuated Canine Distemper Virus Expressing Vasostatin or Granulocyte-Macrophage Colony-Stimulating Factor

Author

Marek, Katarzyna, Armando, Federico, Nippold, Vanessa Maria, Rohn, Karl, Plattet, Philippe, Brogden, Graham, Gerold, Gisa, Baumgärtner, Wolfgang, Puff, Christina, Marek, Katarzyna, Armando, Federico, Nippold, Vanessa Maria, Rohn, Karl, Plattet, Philippe, Brogden, Graham, Gerold, Gisa, Baumgärtner, Wolfgang, and Puff, Christina

Abstract

Canine histiocytic sarcoma (HS) represents a neoplasia with poor prognosis. Due to the high metastatic rate of HS, there is urgency to improve treatment options and to prevent tumor metastases. Canine distemper virus (CDV) is a single-stranded negative-sense RNA (ssRNA (-)) virus with potentially oncolytic properties. Moreover, vasostatin and granulocyte-macrophage colony-stimulating factor (GM-CSF) are attractive molecules in cancer therapy research because of their anti-angiogenetic properties and potential modulation of the tumor microenvironment. In the present study, an in vitro characterization of two genetically engineered viruses based on the CDV strain Onderstepoort (CDV-Ond), CDV-Ondneon-vasostatin and CDV-Ondneon-GM-CSF was performed. Canine histiocytic sarcoma cells (DH82 cells) were persistently infected with CDV-Ond, CDV-Ondneon, CDV-Ondneon-vasostatin and CDV-Ondneon-GM-CSF and characterized on a molecular and protein level regarding their vasostatin and GM-CSF production. Interestingly, DH82 cells persistently infected with CDV-Ondneon-vasostatin showed a significantly increased number of vasostatin mRNA transcripts. Similarly, DH82 cells persistently infected with CDV-Ondneon-GM-CSF displayed an increased number of GM-CSF mRNA transcripts mirrored on the protein level as confirmed by immunofluorescence and Western blot. In summary, modified CDV-Ond strains expressed GM-CSF and vasostatin, rendering them promising candidates for the improvement of oncolytic virotherapies, which should be further detailed in future in vivo studies.

Published

2022

14. Persistent Infection of a Canine Histiocytic Sarcoma Cell Line with Attenuated Canine Distemper Virus Expressing Vasostatin or Granulocyte-Macrophage Colony-Stimulating Factor

Author

Marek, Katarzyna, Armando, Federico, Nippold, Vanessa Maria, Rohn, Karl, Plattet, Philippe, Brogden, Graham, Gerold, Gisa, Baumgärtner, Wolfgang, Puff, Christina, Marek, Katarzyna, Armando, Federico, Nippold, Vanessa Maria, Rohn, Karl, Plattet, Philippe, Brogden, Graham, Gerold, Gisa, Baumgärtner, Wolfgang, and Puff, Christina

Abstract

Canine histiocytic sarcoma (HS) represents a neoplasia with poor prognosis. Due to the high metastatic rate of HS, there is urgency to improve treatment options and to prevent tumor metastases. Canine distemper virus (CDV) is a single-stranded negative-sense RNA (ssRNA (-)) virus with potentially oncolytic properties. Moreover, vasostatin and granulocyte-macrophage colony-stimulating factor (GM-CSF) are attractive molecules in cancer therapy research because of their anti-angiogenetic properties and potential modulation of the tumor microenvironment. In the present study, an in vitro characterization of two genetically engineered viruses based on the CDV strain Onderstepoort (CDV-Ond), CDV-Ondneon-vasostatin and CDV-Ondneon-GM-CSF was performed. Canine histiocytic sarcoma cells (DH82 cells) were persistently infected with CDV-Ond, CDV-Ondneon, CDV-Ondneon-vasostatin and CDV-Ondneon-GM-CSF and characterized on a molecular and protein level regarding their vasostatin and GM-CSF production. Interestingly, DH82 cells persistently infected with CDV-Ondneon-vasostatin showed a significantly increased number of vasostatin mRNA transcripts. Similarly, DH82 cells persistently infected with CDV-Ondneon-GM-CSF displayed an increased number of GM-CSF mRNA transcripts mirrored on the protein level as confirmed by immunofluorescence and Western blot. In summary, modified CDV-Ond strains expressed GM-CSF and vasostatin, rendering them promising candidates for the improvement of oncolytic virotherapies, which should be further detailed in future in vivo studies.

Published

2022

15. Persistent Infection of a Canine Histiocytic Sarcoma Cell Line with Attenuated Canine Distemper Virus Expressing Vasostatin or Granulocyte-Macrophage Colony-Stimulating Factor

Author

Marek, Katarzyna, Armando, Federico, Nippold, Vanessa Maria, Rohn, Karl, Plattet, Philippe, Brogden, Graham, Gerold, Gisa, Baumgärtner, Wolfgang, Puff, Christina, Marek, Katarzyna, Armando, Federico, Nippold, Vanessa Maria, Rohn, Karl, Plattet, Philippe, Brogden, Graham, Gerold, Gisa, Baumgärtner, Wolfgang, and Puff, Christina

Abstract

Canine histiocytic sarcoma (HS) represents a neoplasia with poor prognosis. Due to the high metastatic rate of HS, there is urgency to improve treatment options and to prevent tumor metastases. Canine distemper virus (CDV) is a single-stranded negative-sense RNA (ssRNA (-)) virus with potentially oncolytic properties. Moreover, vasostatin and granulocyte-macrophage colony-stimulating factor (GM-CSF) are attractive molecules in cancer therapy research because of their anti-angiogenetic properties and potential modulation of the tumor microenvironment. In the present study, an in vitro characterization of two genetically engineered viruses based on the CDV strain Onderstepoort (CDV-Ond), CDV-Ondneon-vasostatin and CDV-Ondneon-GM-CSF was performed. Canine histiocytic sarcoma cells (DH82 cells) were persistently infected with CDV-Ond, CDV-Ondneon, CDV-Ondneon-vasostatin and CDV-Ondneon-GM-CSF and characterized on a molecular and protein level regarding their vasostatin and GM-CSF production. Interestingly, DH82 cells persistently infected with CDV-Ondneon-vasostatin showed a significantly increased number of vasostatin mRNA transcripts. Similarly, DH82 cells persistently infected with CDV-Ondneon-GM-CSF displayed an increased number of GM-CSF mRNA transcripts mirrored on the protein level as confirmed by immunofluorescence and Western blot. In summary, modified CDV-Ond strains expressed GM-CSF and vasostatin, rendering them promising candidates for the improvement of oncolytic virotherapies, which should be further detailed in future in vivo studies.

Published

2022

16. An ACE2-blocking antibody confers broad neutralization and protection against Omicron and other SARS-CoV-2 variants of concern

Author

Virologie, dI&I I&I-1, Bedrijfsvoering, Du, Wenjuan, Hurdiss, Daniel L, Drabek, Dubravka, Mykytyn, Anna Z, Kaiser, Franziska K, González-Hernández, Mariana, Muñoz-Santos, Diego, Lamers, Mart M, van Haperen, Rien, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Sola, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, van der Lee, Joline, van Kuppeveld, Frank J M, van Amerongen, Geert, Haagmans, Bart L, Enjuanes, Luis, Osterhaus, Albert D M E, Grosveld, Frank, Bosch, Berend-Jan, Virologie, dI&I I&I-1, Bedrijfsvoering, Du, Wenjuan, Hurdiss, Daniel L, Drabek, Dubravka, Mykytyn, Anna Z, Kaiser, Franziska K, González-Hernández, Mariana, Muñoz-Santos, Diego, Lamers, Mart M, van Haperen, Rien, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Sola, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, van der Lee, Joline, van Kuppeveld, Frank J M, van Amerongen, Geert, Haagmans, Bart L, Enjuanes, Luis, Osterhaus, Albert D M E, Grosveld, Frank, and Bosch, Berend-Jan

Published

2022

17. Persistent Infection of a Canine Histiocytic Sarcoma Cell Line with Attenuated Canine Distemper Virus Expressing Vasostatin or Granulocyte-Macrophage Colony-Stimulating Factor

Author

Marek, Katarzyna, Armando, Federico, Nippold, Vanessa Maria, Rohn, Karl, Plattet, Philippe, Brogden, Graham, Gerold, Gisa, Baumgärtner, Wolfgang, Puff, Christina, Marek, Katarzyna, Armando, Federico, Nippold, Vanessa Maria, Rohn, Karl, Plattet, Philippe, Brogden, Graham, Gerold, Gisa, Baumgärtner, Wolfgang, and Puff, Christina

Abstract

Canine histiocytic sarcoma (HS) represents a neoplasia with poor prognosis. Due to the high metastatic rate of HS, there is urgency to improve treatment options and to prevent tumor metastases. Canine distemper virus (CDV) is a single-stranded negative-sense RNA (ssRNA (-)) virus with potentially oncolytic properties. Moreover, vasostatin and granulocyte-macrophage colony-stimulating factor (GM-CSF) are attractive molecules in cancer therapy research because of their anti-angiogenetic properties and potential modulation of the tumor microenvironment. In the present study, an in vitro characterization of two genetically engineered viruses based on the CDV strain Onderstepoort (CDV-Ond), CDV-Ondneon-vasostatin and CDV-Ondneon-GM-CSF was performed. Canine histiocytic sarcoma cells (DH82 cells) were persistently infected with CDV-Ond, CDV-Ondneon, CDV-Ondneon-vasostatin and CDV-Ondneon-GM-CSF and characterized on a molecular and protein level regarding their vasostatin and GM-CSF production. Interestingly, DH82 cells persistently infected with CDV-Ondneon-vasostatin showed a significantly increased number of vasostatin mRNA transcripts. Similarly, DH82 cells persistently infected with CDV-Ondneon-GM-CSF displayed an increased number of GM-CSF mRNA transcripts mirrored on the protein level as confirmed by immunofluorescence and Western blot. In summary, modified CDV-Ond strains expressed GM-CSF and vasostatin, rendering them promising candidates for the improvement of oncolytic virotherapies, which should be further detailed in future in vivo studies.

Published

2022

18. Persistent Infection of a Canine Histiocytic Sarcoma Cell Line with Attenuated Canine Distemper Virus Expressing Vasostatin or Granulocyte-Macrophage Colony-Stimulating Factor

Author

Marek, Katarzyna, Armando, Federico, Nippold, Vanessa Maria, Rohn, Karl, Plattet, Philippe, Brogden, Graham, Gerold, Gisa, Baumgärtner, Wolfgang, Puff, Christina, Marek, Katarzyna, Armando, Federico, Nippold, Vanessa Maria, Rohn, Karl, Plattet, Philippe, Brogden, Graham, Gerold, Gisa, Baumgärtner, Wolfgang, and Puff, Christina

Abstract

Canine histiocytic sarcoma (HS) represents a neoplasia with poor prognosis. Due to the high metastatic rate of HS, there is urgency to improve treatment options and to prevent tumor metastases. Canine distemper virus (CDV) is a single-stranded negative-sense RNA (ssRNA (-)) virus with potentially oncolytic properties. Moreover, vasostatin and granulocyte-macrophage colony-stimulating factor (GM-CSF) are attractive molecules in cancer therapy research because of their anti-angiogenetic properties and potential modulation of the tumor microenvironment. In the present study, an in vitro characterization of two genetically engineered viruses based on the CDV strain Onderstepoort (CDV-Ond), CDV-Ondneon-vasostatin and CDV-Ondneon-GM-CSF was performed. Canine histiocytic sarcoma cells (DH82 cells) were persistently infected with CDV-Ond, CDV-Ondneon, CDV-Ondneon-vasostatin and CDV-Ondneon-GM-CSF and characterized on a molecular and protein level regarding their vasostatin and GM-CSF production. Interestingly, DH82 cells persistently infected with CDV-Ondneon-vasostatin showed a significantly increased number of vasostatin mRNA transcripts. Similarly, DH82 cells persistently infected with CDV-Ondneon-GM-CSF displayed an increased number of GM-CSF mRNA transcripts mirrored on the protein level as confirmed by immunofluorescence and Western blot. In summary, modified CDV-Ond strains expressed GM-CSF and vasostatin, rendering them promising candidates for the improvement of oncolytic virotherapies, which should be further detailed in future in vivo studies.

Published

2022

19. SARS-CoV-2 Omicron variant causes mild pathology in the upper and lower respiratory tract of hamsters

Author

Armando, Federico, Beythien, Georg, Kaiser, Franziska K., Allnoch, Lisa, Heydemann, Laura, Rosiak, Malgorzata, Becker, Svenja, Gonzalez-Hernandez, Mariana, Lamers, Mart M., Haagmans, Bart L., Guilfoyle, Kate, van Amerongen, Geert, Ciurkiewicz, Malgorzata, Osterhaus, Albert D.M.E., Baumgärtner, Wolfgang, Armando, Federico, Beythien, Georg, Kaiser, Franziska K., Allnoch, Lisa, Heydemann, Laura, Rosiak, Malgorzata, Becker, Svenja, Gonzalez-Hernandez, Mariana, Lamers, Mart M., Haagmans, Bart L., Guilfoyle, Kate, van Amerongen, Geert, Ciurkiewicz, Malgorzata, Osterhaus, Albert D.M.E., and Baumgärtner, Wolfgang

Abstract

Since its discovery in 2019, multiple variants of severe acute respiratory syndrome coronavirus-2 (SARS-CoV-2) have been identified. This study investigates virus spread and associated pathology in the upper and lower respiratory tracts of Syrian golden hamsters at 4 days post intranasal SARS-CoV-2 Omicron infection, in comparison to infection with variants of concern (VOCs) Gamma and Delta as well as ancestral strain 614 G. Pathological changes in the upper and lower respiratory tract of VOC Omicron infected hamsters are milder than those caused by other investigated strains. VOC Omicron infection causes a mild rhinitis with little involvement of the olfactory epithelium and minimal lesions in the lung, with frequent sparing of the alveolar compartment. Similarly, viral antigen, RNA and infectious virus titers are lower in respiratory tissues of VOC Omicron infected hamsters. These findings demonstrate that the variant has a decreased pathogenicity for the upper and lower respiratory tract of hamsters.

Published

2022

20. An ACE2-blocking antibody confers broad neutralization and protection against Omicron and other SARS-CoV-2 variants

Author

European Commission, German Research Foundation, Federal Ministry of Education and Research (Germany), Ministry for Science and Culture of Lower Saxony, Du, Wenjuan, Hurdiss, Daniel L., Drabek, Dubravka, Mykytyn, Anna Z., Kaiser, Franziska K., González-Hernandez, Mariana, Muñoz-Santos, Diego, Lamers, Mart M., Haperen, Rien van, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Solá Gurpegui, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, Lee, Joline van der, Kuppeveld, Frank J. M. van, Amerongen, Geert van, Haagmans, Bart L., Enjuanes Sánchez, Luis, Osterhaus, Albert D. M. E., Grosveld, Frank, Bosch, Berend Jan, European Commission, German Research Foundation, Federal Ministry of Education and Research (Germany), Ministry for Science and Culture of Lower Saxony, Du, Wenjuan, Hurdiss, Daniel L., Drabek, Dubravka, Mykytyn, Anna Z., Kaiser, Franziska K., González-Hernandez, Mariana, Muñoz-Santos, Diego, Lamers, Mart M., Haperen, Rien van, Li, Wentao, Drulyte, Ieva, Wang, Chunyan, Solá Gurpegui, Isabel, Armando, Federico, Beythien, Georg, Ciurkiewicz, Malgorzata, Baumgärtner, Wolfgang, Guilfoyle, Kate, Smits, Tony, Lee, Joline van der, Kuppeveld, Frank J. M. van, Amerongen, Geert van, Haagmans, Bart L., Enjuanes Sánchez, Luis, Osterhaus, Albert D. M. E., Grosveld, Frank, and Bosch, Berend Jan

Abstract

The ongoing evolution of SARS-CoV-2 has resulted in the emergence of Omicron, which displays striking immune escape potential. Many of its mutations localize to the spike protein ACE2 receptor-binding domain, annulling the neutralizing activity of most therapeutic monoclonal antibodies. Here we describe a receptor-blocking human monoclonal antibody, 87G7, that retains ultrapotent neutralization against SARS-CoV-2 variants including the Alpha, Beta, Gamma, Delta and Omicron (BA.1/BA.2) Variants-of-Concern (VOCs). Structural analysis reveals that 87G7 targets a patch of hydrophobic residues in the ACE2-binding site that are highly conserved in SARS-CoV-2 variants, explaining its broad neutralization capacity. 87G7 protects mice and/or hamsters against challenge with all current SARS-CoV-2 VOCs. Our findings may aid the development of sustainable antibody-based strategies against COVID-19 that are more resilient to SARS-CoV-2 antigenic diversity.

Published

2022

21. Rift Valley Fever Virus Non-Structural Protein S Is Associated with Nuclear Translocation of Active Caspase-3 and Inclusion Body Formation

Author

Michaely, Lukas Mathias, Rissmann, Melanie, Armando, Federico, von Arnim, Felicitas, Keller, Markus, Eiden, Martin, König, Rebecca, Gutjahr, Benjamin, Baumgärtner, Wolfgang, Groschup, Martin H., Ulrich, Reiner, Michaely, Lukas Mathias, Rissmann, Melanie, Armando, Federico, von Arnim, Felicitas, Keller, Markus, Eiden, Martin, König, Rebecca, Gutjahr, Benjamin, Baumgärtner, Wolfgang, Groschup, Martin H., and Ulrich, Reiner

Abstract

Rift Valley fever phlebovirus (RVFV) causes Rift Valley fever (RVF), an emerging zoonotic disease that causes abortion storms and high mortality rates in young ruminants as well as severe or even lethal complications in a subset of human patients. This study investigates the pathomechanism of intranuclear inclusion body formation in severe RVF in a mouse model. Liver samples from immunocompetent mice infected with virulent RVFV 35/74, and immunodeficient knockout mice that lack interferon type I receptor expression and were infected with attenuated RVFV MP12 were compared to livers from uninfected controls using histopathology and immunohistochemistry for RVFV nucleoprotein, non-structural protein S (NSs) and pro-apoptotic active caspase-3. Histopathology of the livers showed virus-induced, severe hepatic necrosis in both mouse strains. However, immunohistochemistry and immunofluorescence revealed eosinophilic, comma-shaped, intranuclear inclusions and an intranuclear (co-)localization of RVFV NSs and active caspase-3 only in 35/74-infected immunocompetent mice, but not in MP12-infected immunodeficient mice. These results suggest that intranuclear accumulation of RVFV 35/74 NSs is involved in nuclear translocation of active caspase-3, and that nuclear NSs and active caspase-3 are involved in the formation of the light microscopically visible inclusion bodies.

Published

2022

22. The upper respiratory tract of felids is highly susceptible to sars‐cov‐2 infection

Author

Krüger, Nadine, Rocha, Cheila, Runft, Sandra, Krüger, Johannes, Färber, Iris, Armando, Federico, Leitzen, Eva, Brogden, Graham, Gerold, Gisa, Pöhlmann, Stefan, Hoffmann, Markus, Baumgärtner, Wolfgang, Krüger, Nadine, Rocha, Cheila, Runft, Sandra, Krüger, Johannes, Färber, Iris, Armando, Federico, Leitzen, Eva, Brogden, Graham, Gerold, Gisa, Pöhlmann, Stefan, Hoffmann, Markus, and Baumgärtner, Wolfgang

Abstract

Natural or experimental infection of domestic cats and virus transmission from humans to captive predatory cats suggest that felids are highly susceptible to SARS‐CoV‐2 infection. However, it is unclear which cells and compartments of the respiratory tract are infected. To address this question, primary cell cultures derived from the nose, trachea, and lungs of cat and lion were inoculated with SARS‐CoV‐2. Strong viral replication was observed for nasal mucosa explants and tracheal air–liquid interface cultures, whereas replication in lung slices was less efficient. Infection was mainly restricted to epithelial cells and did not cause major pathological changes. Detection of high ACE2 levels in the nose and trachea but not lung further suggests that susceptibility of feline tissues to SARS‐CoV‐2 correlates with ACE2 expression. Collectively, this study demonstrates that SARS‐ CoV‐2 can efficiently replicate in the feline upper respiratory tract ex vivo and thus highlights the risk of SARS‐CoV‐2 spillover from humans to felids.

Published

2021

23. The upper respiratory tract of felids is highly susceptible to sars‐cov‐2 infection

Author

Krüger, Nadine, Rocha, Cheila, Runft, Sandra, Krüger, Johannes, Färber, Iris, Armando, Federico, Leitzen, Eva, Brogden, Graham, Gerold, Gisa, Pöhlmann, Stefan, Hoffmann, Markus, Baumgärtner, Wolfgang, Krüger, Nadine, Rocha, Cheila, Runft, Sandra, Krüger, Johannes, Färber, Iris, Armando, Federico, Leitzen, Eva, Brogden, Graham, Gerold, Gisa, Pöhlmann, Stefan, Hoffmann, Markus, and Baumgärtner, Wolfgang

Abstract

Natural or experimental infection of domestic cats and virus transmission from humans to captive predatory cats suggest that felids are highly susceptible to SARS‐CoV‐2 infection. However, it is unclear which cells and compartments of the respiratory tract are infected. To address this question, primary cell cultures derived from the nose, trachea, and lungs of cat and lion were inoculated with SARS‐CoV‐2. Strong viral replication was observed for nasal mucosa explants and tracheal air–liquid interface cultures, whereas replication in lung slices was less efficient. Infection was mainly restricted to epithelial cells and did not cause major pathological changes. Detection of high ACE2 levels in the nose and trachea but not lung further suggests that susceptibility of feline tissues to SARS‐CoV‐2 correlates with ACE2 expression. Collectively, this study demonstrates that SARS‐ CoV‐2 can efficiently replicate in the feline upper respiratory tract ex vivo and thus highlights the risk of SARS‐CoV‐2 spillover from humans to felids.

Published

2021

24. The upper respiratory tract of felids is highly susceptible to sars‐cov‐2 infection

Author

Krüger, Nadine, Rocha, Cheila, Runft, Sandra, Krüger, Johannes, Färber, Iris, Armando, Federico, Leitzen, Eva, Brogden, Graham, Gerold, Gisa, Pöhlmann, Stefan, Hoffmann, Markus, Baumgärtner, Wolfgang, Krüger, Nadine, Rocha, Cheila, Runft, Sandra, Krüger, Johannes, Färber, Iris, Armando, Federico, Leitzen, Eva, Brogden, Graham, Gerold, Gisa, Pöhlmann, Stefan, Hoffmann, Markus, and Baumgärtner, Wolfgang

Abstract

Natural or experimental infection of domestic cats and virus transmission from humans to captive predatory cats suggest that felids are highly susceptible to SARS‐CoV‐2 infection. However, it is unclear which cells and compartments of the respiratory tract are infected. To address this question, primary cell cultures derived from the nose, trachea, and lungs of cat and lion were inoculated with SARS‐CoV‐2. Strong viral replication was observed for nasal mucosa explants and tracheal air–liquid interface cultures, whereas replication in lung slices was less efficient. Infection was mainly restricted to epithelial cells and did not cause major pathological changes. Detection of high ACE2 levels in the nose and trachea but not lung further suggests that susceptibility of feline tissues to SARS‐CoV‐2 correlates with ACE2 expression. Collectively, this study demonstrates that SARS‐ CoV‐2 can efficiently replicate in the feline upper respiratory tract ex vivo and thus highlights the risk of SARS‐CoV‐2 spillover from humans to felids.

Published

2021

25. The upper respiratory tract of felids is highly susceptible to sars‐cov‐2 infection

Author

Krüger, Nadine, Rocha, Cheila, Runft, Sandra, Krüger, Johannes, Färber, Iris, Armando, Federico, Leitzen, Eva, Brogden, Graham, Gerold, Gisa, Pöhlmann, Stefan, Hoffmann, Markus, Baumgärtner, Wolfgang, Krüger, Nadine, Rocha, Cheila, Runft, Sandra, Krüger, Johannes, Färber, Iris, Armando, Federico, Leitzen, Eva, Brogden, Graham, Gerold, Gisa, Pöhlmann, Stefan, Hoffmann, Markus, and Baumgärtner, Wolfgang

Abstract

Natural or experimental infection of domestic cats and virus transmission from humans to captive predatory cats suggest that felids are highly susceptible to SARS‐CoV‐2 infection. However, it is unclear which cells and compartments of the respiratory tract are infected. To address this question, primary cell cultures derived from the nose, trachea, and lungs of cat and lion were inoculated with SARS‐CoV‐2. Strong viral replication was observed for nasal mucosa explants and tracheal air–liquid interface cultures, whereas replication in lung slices was less efficient. Infection was mainly restricted to epithelial cells and did not cause major pathological changes. Detection of high ACE2 levels in the nose and trachea but not lung further suggests that susceptibility of feline tissues to SARS‐CoV‐2 correlates with ACE2 expression. Collectively, this study demonstrates that SARS‐ CoV‐2 can efficiently replicate in the feline upper respiratory tract ex vivo and thus highlights the risk of SARS‐CoV‐2 spillover from humans to felids.

Published

2021

26. The upper respiratory tract of felids is highly susceptible to sars‐cov‐2 infection

Author

Krüger, Nadine, Rocha, Cheila, Runft, Sandra, Krüger, Johannes, Färber, Iris, Armando, Federico, Leitzen, Eva, Brogden, Graham, Gerold, Gisa, Pöhlmann, Stefan, Hoffmann, Markus, Baumgärtner, Wolfgang, Krüger, Nadine, Rocha, Cheila, Runft, Sandra, Krüger, Johannes, Färber, Iris, Armando, Federico, Leitzen, Eva, Brogden, Graham, Gerold, Gisa, Pöhlmann, Stefan, Hoffmann, Markus, and Baumgärtner, Wolfgang

Abstract

Natural or experimental infection of domestic cats and virus transmission from humans to captive predatory cats suggest that felids are highly susceptible to SARS‐CoV‐2 infection. However, it is unclear which cells and compartments of the respiratory tract are infected. To address this question, primary cell cultures derived from the nose, trachea, and lungs of cat and lion were inoculated with SARS‐CoV‐2. Strong viral replication was observed for nasal mucosa explants and tracheal air–liquid interface cultures, whereas replication in lung slices was less efficient. Infection was mainly restricted to epithelial cells and did not cause major pathological changes. Detection of high ACE2 levels in the nose and trachea but not lung further suggests that susceptibility of feline tissues to SARS‐CoV‐2 correlates with ACE2 expression. Collectively, this study demonstrates that SARS‐ CoV‐2 can efficiently replicate in the feline upper respiratory tract ex vivo and thus highlights the risk of SARS‐CoV‐2 spillover from humans to felids.

Published

2021