Your search keyword '"Eleni Kourkouta"' showing total 9 results

1. Booster vaccination with Ad26.COV2.S or an Omicron-adapted vaccine in pre-immune hamsters protects against Omicron BA.2

Author

Maarten Swart, Joan van der Lubbe, Sonja Schmit-Tillemans, Ella van Huizen, Johan Verspuij, Ana Izquierdo Gil, Ying Choi, Chenandly Daal, Aditya Perkasa, Adriaan de Wilde, Erwin Claassen, Rineke de Jong, Katrin E. Wiese, Lisette Cornelissen, Marieke van Es, Marjolein van Heerden, Eleni Kourkouta, Issam Tahiri, Michel Mulders, Jessica Vreugdenhil, Karin Feddes - de Boer, Leacky Muchene, Jeroen Tolboom, Liesbeth Dekking, Jarek Juraszek, Jort Vellinga, Jerome Custers, Rinke Bos, Hanneke Schuitemaker, Frank Wegmann, Ramon Roozendaal, Harmjan Kuipers, and Roland Zahn

Subjects

Immunologic diseases. Allergy, RC581-607, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Abstract Since the original outbreak of the SARS-CoV-2 virus, several rapidly spreading SARS-CoV-2 variants of concern (VOC) have emerged. Here, we show that a single dose of Ad26.COV2.S (based on the Wuhan-Hu-1 spike variant) protects against the Gamma and Delta variants in naive hamsters, supporting the observed maintained vaccine efficacy in humans against these VOC. Adapted spike-based booster vaccines targeting Omicron variants have now been authorized in the absence of human efficacy data. We evaluated the immunogenicity and efficacy of Ad26.COV2.S.529 (encoding a stabilized Omicron BA.1 spike) in naive mice and in hamsters with pre-existing immunity to the Wuhan-Hu-1 spike. In naive mice, Ad26.COV2.S.529 elicited higher neutralizing antibody titers against SARS-CoV-2 Omicron BA.1 and BA.2, compared with Ad26.COV2.S. However, neutralizing titers against the SARS-CoV-2 B.1 (D614G) and Delta variants were lower after primary vaccination with Ad26.COV2.S.529 compared with Ad26.COV2.S. In contrast, we found comparable Omicron BA.1 and BA.2 neutralizing titers in hamsters with pre-existing Wuhan-Hu-1 spike immunity after vaccination with Ad26.COV2.S, Ad26.COV2.S.529 or a combination of the two vaccines. Moreover, all three vaccine modalities induced equivalent protection against Omicron BA.2 challenge in these animals. Overall, our data suggest that an Omicron BA.1-based booster in rodents does not improve immunogenicity and efficacy against Omicron BA.2 over an Ad26.COV2.S booster in a setting of pre-existing immunity to SARS-CoV-2.

Published

2023

2. Suppression of Mutant Protein Expression in SCA3 and SCA1 Mice Using a CAG Repeat-Targeting Antisense Oligonucleotide

Author

Eleni Kourkouta, Rudie Weij, Anchel González-Barriga, Melissa Mulder, Ruurd Verheul, Sieto Bosgra, Bas Groenendaal, Jukka Puoliväli, Jussi Toivanen, Judith C.T. van Deutekom, and Nicole A. Datson

Subjects

Therapeutics. Pharmacology, RM1-950

Abstract

Spinocerebellar ataxia type 3 (SCA3) and type 1 (SCA1) are dominantly inherited neurodegenerative disorders that are currently incurable. Both diseases are caused by a CAG-repeat expansion in exon 10 of the Ataxin-3 and exon 8 of the Ataxin-1 gene, respectively, encoding an elongated polyglutamine tract that confers toxic properties to the resulting proteins. We have previously shown lowering of the pathogenic polyglutamine protein in Huntington’s disease mouse models using (CUG)7, a CAG repeat-targeting antisense oligonucleotide. Here we evaluated the therapeutic capacity of (CUG)7 for SCA3 and SCA1, in vitro in patient-derived cell lines and in vivo in representative mouse models. Repeated intracerebroventricular (CUG)7 administration resulted in a significant reduction of mutant Ataxin-3 and Ataxin-1 proteins throughout the brain of SCA3 and SCA1 mouse models, respectively. Furthermore, in both a SCA3 patient cell line and the MJD84.2 mouse model, (CUG)7 induced formation of a truncated Ataxin-3 protein species lacking the polyglutamine stretch, likely arising from (CUG)7-mediated exon 10 skipping. In contrast, skipping of exon 8 of Ataxin-1 did not significantly contribute to the Ataxin-1 protein reduction observed in (CUG)7-treated SCA1154Q/2Q mice. These findings support the therapeutic potential of a single CAG repeat-targeting AON for the treatment of multiple polyglutamine disorders. Keywords: antisense oligonucleotide, SCA1, SCA3, polyglutamine disorders, exon skip, CAG repeat

Published

2019

3. Detailed genetic and functional analysis of the hDMDdel52/mdx mouse model.

Author

Alper Yavas, Rudie Weij, Maaike van Putten, Eleni Kourkouta, Chantal Beekman, Jukka Puoliväli, Timo Bragge, Toni Ahtoniemi, Jeroen Knijnenburg, Marlies Elisabeth Hoogenboom, Yavuz Ariyurek, Annemieke Aartsma-Rus, Judith van Deutekom, and Nicole Datson

Subjects

Medicine, Science

Abstract

Duchenne muscular dystrophy (DMD) is a severe, progressive neuromuscular disorder caused by reading frame disrupting mutations in the DMD gene leading to absence of functional dystrophin. Antisense oligonucleotide (AON)-mediated exon skipping is a therapeutic approach aimed at restoring the reading frame at the pre-mRNA level, allowing the production of internally truncated partly functional dystrophin proteins. AONs work in a sequence specific manner, which warrants generating humanized mouse models for preclinical tests. To address this, we previously generated the hDMDdel52/mdx mouse model using transcription activator like effector nuclease (TALEN) technology. This model contains mutated murine and human DMD genes, and therefore lacks mouse and human dystrophin resulting in a dystrophic phenotype. It allows preclinical evaluation of AONs inducing the skipping of human DMD exons 51 and 53 and resulting in restoration of dystrophin synthesis. Here, we have further characterized this model genetically and functionally. We discovered that the hDMD and hDMDdel52 transgene is present twice per locus, in a tail-to-tail-orientation. Long-read sequencing revealed a partial deletion of exon 52 (first 25 bp), and a 2.3 kb inversion in intron 51 in both copies. These new findings on the genomic make-up of the hDMD and hDMDdel52 transgene do not affect exon 51 and/or 53 skipping, but do underline the need for extensive genetic analysis of mice generated with genome editing techniques to elucidate additional genetic changes that might have occurred. The hDMDdel52/mdx mice were also evaluated functionally using kinematic gait analysis. This revealed a clear and highly significant difference in overall gait between hDMDdel52/mdx mice and C57BL6/J controls. The motor deficit detected in the model confirms its suitability for preclinical testing of exon skipping AONs for human DMD at both the functional and molecular level.

Published

2020

4. The expanded CAG repeat in the huntingtin gene as target for therapeutic RNA modulation throughout the HD mouse brain.

Author

Nicole A Datson, Anchel González-Barriga, Eleni Kourkouta, Rudie Weij, Jeroen van de Giessen, Susan Mulders, Outi Kontkanen, Taneli Heikkinen, Kimmo Lehtimäki, and Judith C T van Deutekom

Subjects

Medicine, Science

Abstract

The aim of these studies was to demonstrate the therapeutic capacity of an antisense oligonucleotide with the sequence (CUG)7 targeting the expanded CAG repeat in huntingtin (HTT) mRNA in vivo in the R6/2 N-terminal fragment and Q175 knock-in Huntington's disease (HD) mouse models. In a first study, R6/2 mice received six weekly intracerebroventricular infusions with a low and high dose of (CUG)7 and were sacrificed 2 weeks later. A 15-60% reduction of both soluble and aggregated mutant HTT protein was observed in striatum, hippocampus and cortex of (CUG)7-treated mice. This correction at the molecular level resulted in an improvement of performance in multiple motor tasks, increased whole brain and cortical volume, reduced levels of the gliosis marker myo-inositol, increased levels of the neuronal integrity marker N-aceyl aspartate and increased mRNA levels of the striatal marker Darpp-32. These neuroanatomical and neurochemical changes, together with the improved motor performance, suggest that treatment with (CUG)7 ameliorates basal ganglia dysfunction. The HTT-lowering was confirmed by an independent study in Q175 mice using a similar (CUG)7 AON dosing regimen, further demonstrating a lasting reduction of mutant HTT protein in striatum, hippocampus and cortex for up to 18 weeks post last infusion along with an increase in motor activity. Based on these encouraging results, (CUG)7 may thus offer an interesting alternative HTT-lowering strategy for HD.

Published

2017

5. Immunogenicity of an Ad26-based SARS-CoV-2 Omicron Vaccine in Naïve Mice and SARS-CoV-2 Spike Pre-immune Hamsters

Author

Maarten Swart, Adriaan de Wilde, Sonja Schmit-Tillemans, Johan Verspuij, Chenandly Daal, Ying Choi, Aditya Perkasa, Eleni Kourkouta, Issam Tahiri, Michel Mulders, Ana Izquierdo Gil, Leacky Muchene, Jarek Juraszek, Jort Vellinga, Jerome Custers, Rinke Bos, Hanneke Schuitemaker, Frank Wegmann, Ramon Roozendaal, Harmjan Kuipers, and Roland Zahn

Abstract

The severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) Omicron variant sparked concern due to its fast spread and the unprecedented number of mutations in the spike protein that enables it to partially evade spike-based COVID-19 vaccine-induced humoral immunity. In anticipation of a potential need for an Omicron spike-based vaccine, we generated an Ad26 vector encoding an Omicron (BA.1) spike protein (Ad26.COV2.S.529). Ad26.COV2.S.529 encodes for a prefusion stabilized spike protein, similar to the current COVID-19 vaccine Ad26.COV2.S encoding the Wuhan-Hu-1 spike protein. We verified that spike expression by Ad26.COV2.S.529 was comparable to Ad26.COV2.S. Immunogenicity of Ad26.COV2.S.529 was then evaluated in naïve mice and SARS-CoV-2 Wuhan-Hu-1 spike pre-immunized hamsters. In naïve mice, Ad26.COV2.S.529 elicited robust neutralizing antibodies against SARS-CoV-2 Omicron (BA.1) but not to SARS-CoV-2 Delta (B.1.617.2), while the opposite was observed for Ad26.COV2.S. In pre-immune hamsters, Ad26.COV2.S.529 vaccination resulted in robust increases in neutralizing antibody titers against both SARS-CoV-2 Omicron (BA.1) and Delta (B.1.617.2), while Ad26.COV2.S vaccination only increased neutralizing antibody titers against the Delta variant. Our data imply that Ad26.COV2.S.529 can both expand and boost a Wuhan-Hu-1 spike-primed humoral immune response to protect against distant SARS-CoV-2 variants.

Published

2022

6. Suppression of Mutant Protein Expression in SCA3 and SCA1 Mice Using a CAG Repeat-Targeting Antisense Oligonucleotide

Author

Melissa Mulder, Ruurd C. Verheul, Judith C.T. van Deutekom, Bas Groenendaal, Nicole A. Datson, Eleni Kourkouta, Anchel González-Barriga, Sieto Bosgra, Jukka Puoliväli, Jussi Toivanen, and Rudie Weij

Subjects

antisense oligonucleotide, 0301 basic medicine, congenital, hereditary, and neonatal diseases and abnormalities, Mutant, Biology, Article, polyglutamine disorders, SCA1, 03 medical and health sciences, Exon, 0302 clinical medicine, SCA3, Mutant protein, Drug Discovery, medicine, Gene, CAG repeat, exon skip, lcsh:RM1-950, Polyglutamine tract, medicine.disease, Molecular biology, lcsh:Therapeutics. Pharmacology, 030104 developmental biology, Cell culture, 030220 oncology & carcinogenesis, Toxicity, Spinocerebellar ataxia, Molecular Medicine

Abstract

Spinocerebellar ataxia type 3 (SCA3) and type 1 (SCA1) are dominantly inherited neurodegenerative disorders that are currently incurable. Both diseases are caused by a CAG-repeat expansion in exon 10 of the Ataxin-3 and exon 8 of the Ataxin-1 gene, respectively, encoding an elongated polyglutamine tract that confers toxic properties to the resulting proteins. We have previously shown lowering of the pathogenic polyglutamine protein in Huntington’s disease mouse models using (CUG)7, a CAG repeat-targeting antisense oligonucleotide. Here we evaluated the therapeutic capacity of (CUG)7 for SCA3 and SCA1, in vitro in patient-derived cell lines and in vivo in representative mouse models. Repeated intracerebroventricular (CUG)7 administration resulted in a significant reduction of mutant Ataxin-3 and Ataxin-1 proteins throughout the brain of SCA3 and SCA1 mouse models, respectively. Furthermore, in both a SCA3 patient cell line and the MJD84.2 mouse model, (CUG)7 induced formation of a truncated Ataxin-3 protein species lacking the polyglutamine stretch, likely arising from (CUG)7-mediated exon 10 skipping. In contrast, skipping of exon 8 of Ataxin-1 did not significantly contribute to the Ataxin-1 protein reduction observed in (CUG)7-treated SCA1154Q/2Q mice. These findings support the therapeutic potential of a single CAG repeat-targeting AON for the treatment of multiple polyglutamine disorders. Keywords: antisense oligonucleotide, SCA1, SCA3, polyglutamine disorders, exon skip, CAG repeat

Published

2019

7. Immunogenicity and efficacy of one and two doses of Ad26.COV2.S COVID vaccine in adult and aged NHP

Author

Jerome Custers, Jessica Vreugdenhil, Roland Zahn, Adriaan H. de Wilde, Frank Wegmann, Babs E. Verstrepen, Ella van Huizen, Ivanela Kondova, Joan E.M. van der Lubbe, Jeroen Tolboom, Joke Drijver, Mandy Jongeneelen, Joost Vaneman, Dominika N. Czapska-Casey, Laura Solforosi, Eric J. Snijder, Willy M. J. M. Bogers, Miranda R.M. Baert, Daniel Veldman, Kinga P. Böszörményi, Hanneke Schuitemaker, Leacky Muchene, Eleni Kourkouta, Harmjan Kuipers, Ying Choi, Ernst J. Verschoor, Ana Izquierdo Gil, Marjolein van Heerden, Marieke A. Stammes, Tim J. Dalebout, Liesbeth Dekking, Petra Mooij, Krisztian Kaszas, Ramon Roozendaal, Sanne Kroos, Sebenzile K. Myeni, Jeroen Huizingh, Remko Van Der Vlugt, Boerries Brandenburg, Marjolein Kikkert, Sietske K. Rosendahl Huber, Gerrit Koopman, and Dan H. Barouch

Subjects

CD4-Positive T-Lymphocytes, Male, 0301 basic medicine, Aging, COVID-19 Vaccines, Immunology, Dose-Response Relationship, Immunologic, CD8-Positive T-Lymphocytes, medicine.disease_cause, Bronchoalveolar Lavage, Article, Adenoviridae, Body Temperature, Infectious Disease and Host Defense, 03 medical and health sciences, 0302 clinical medicine, Immunity, medicine, Animals, Immunology and Allergy, 030212 general & internal medicine, Neutralizing antibody, Lung, Coronavirus, biology, SARS-CoV-2, business.industry, Immunogenicity, Vaccination, COVID-19, Viral Load, Antibodies, Neutralizing, Macaca mulatta, Immunity, Humoral, Kinetics, Regimen, Treatment Outcome, 030104 developmental biology, Spike Glycoprotein, Coronavirus, Humoral immunity, biology.protein, Female, Antibody, business

Abstract

While single-dose COVID-19 vaccines are preferred, two-dose regimens may improve efficacy. Immunogenicity of Ad26.COV2.S is improved in NHPs after a second dose, whereas both regimens protect animals against SARS-CoV-2 disease and elicit neutralizing antibodies against SARS-CoV-2 variants of concern to varying degrees independent of regimen., Safe and effective coronavirus disease–19 (COVID-19) vaccines are urgently needed to control the ongoing pandemic. While single-dose vaccine regimens would provide multiple advantages, two doses may improve the magnitude and durability of immunity and protective efficacy. We assessed one- and two-dose regimens of the Ad26.COV2.S vaccine candidate in adult and aged nonhuman primates (NHPs). A two-dose Ad26.COV2.S regimen induced higher peak binding and neutralizing antibody responses compared with a single dose. In one-dose regimens, neutralizing antibody responses were stable for at least 14 wk, providing an early indication of durability. Ad26.COV2.S induced humoral immunity and T helper cell (Th cell) 1–skewed cellular responses in aged NHPs that were comparable to those in adult animals. Aged Ad26.COV2.S-vaccinated animals challenged 3 mo after dose 1 with a SARS-CoV-2 spike G614 variant showed near complete lower and substantial upper respiratory tract protection for both regimens. Neutralization of variants of concern by NHP sera was reduced for B.1.351 lineages while maintained for the B.1.1.7 lineage independent of Ad26.COV2.S vaccine regimen.

Published

2021

8. Detailed genetic and functional analysis of the hDMDdel52/mdx mouse model

Author

Eleni Kourkouta, Maaike van Putten, Annemieke Aartsma-Rus, Toni Ahtoniemi, Yavuz Ariyurek, Chantal Beekman, Timo Bragge, Alper Yavas, Marlies Elisabeth Hoogenboom, Rudie Weij, Nicole A. Datson, Jeroen Knijnenburg, Jukka Puoliväli, and Judith C.T. van Deutekom

Subjects

Male, 0301 basic medicine, mdx mouse, Heredity, Physiology, Genetic Linkage, Duchenne muscular dystrophy, Artificial Gene Amplification and Extension, Duchenne Muscular Dystrophy, Biochemistry, Polymerase Chain Reaction, Muscular Dystrophies, Dystrophin, Mice, Exon, Medical Conditions, 0302 clinical medicine, Medicine and Health Sciences, Transgenes, Gait, Transcription activator-like effector nuclease, Mammalian Genomics, Multidisciplinary, Animal Models, Genomics, Exons, Biomechanical Phenomena, Phenotype, Experimental Organism Systems, Neurology, X-Linked Traits, Sex Linkage, Medicine, Gait Analysis, Research Article, musculoskeletal diseases, congenital, hereditary, and neonatal diseases and abnormalities, Science, Transgene, Mouse Models, Computational biology, Biology, Research and Analysis Methods, Genome Complexity, 03 medical and health sciences, Model Organisms, Genetics, medicine, Animals, Humans, Molecular Biology Techniques, Molecular Biology, Clinical Genetics, Biological Locomotion, Biology and Life Sciences, Proteins, Computational Biology, medicine.disease, Introns, Exon skipping, Muscular Dystrophy, Duchenne, Cytoskeletal Proteins, Disease Models, Animal, 030104 developmental biology, Animal Genomics, Humanized mouse, Animal Studies, Mice, Inbred mdx, biology.protein, Gene Deletion, 030217 neurology & neurosurgery

Abstract

Duchenne muscular dystrophy (DMD) is a severe, progressive neuromuscular disorder caused by reading frame disrupting mutations in the DMD gene leading to absence of functional dystrophin. Antisense oligonucleotide (AON)-mediated exon skipping is a therapeutic approach aimed at restoring the reading frame at the pre-mRNA level, allowing the production of internally truncated partly functional dystrophin proteins. AONs work in a sequence specific manner, which warrants generating humanized mouse models for preclinical tests. To address this, we previously generated the hDMDdel52/mdx mouse model using transcription activator like effector nuclease (TALEN) technology. This model contains mutated murine and human DMD genes, and therefore lacks mouse and human dystrophin resulting in a dystrophic phenotype. It allows preclinical evaluation of AONs inducing the skipping of human DMD exons 51 and 53 and resulting in restoration of dystrophin synthesis. Here, we have further characterized this model genetically and functionally. We discovered that the hDMD and hDMDdel52 transgene is present twice per locus, in a tail-to-tail-orientation. Long-read sequencing revealed a partial deletion of exon 52 (first 25 bp), and a 2.3 kb inversion in intron 51 in both copies. These new findings on the genomic make-up of the hDMD and hDMDdel52 transgene do not affect exon 51 and/or 53 skipping, but do underline the need for extensive genetic analysis of mice generated with genome editing techniques to elucidate additional genetic changes that might have occurred. The hDMDdel52/mdx mice were also evaluated functionally using kinematic gait analysis. This revealed a clear and highly significant difference in overall gait between hDMDdel52/mdx mice and C57BL6/J controls. The motor deficit detected in the model confirms its suitability for preclinical testing of exon skipping AONs for human DMD at both the functional and molecular level.

Published

2020

9. L2 The expanded cag repeat in the huntingtin gene as target for therapeutic RNA modulation throughout the R6/2 and Q175 HD mouse brain

Author

Nicole A. Datson, Outi Kontkanen, Judith C.T. van Deutekom, Taneli Heikkinen, Anchel González-Barriga, Kimmo Lehtimäki, and Eleni Kourkouta

Subjects

congenital, hereditary, and neonatal diseases and abnormalities, medicine.medical_specialty, Messenger RNA, Huntingtin, Hippocampus, Striatum, Biology, Molecular biology, Psychiatry and Mental health, Endocrinology, Neurochemical, nervous system, Gliosis, Dopamine, Internal medicine, medicine, Gene silencing, Surgery, Neurology (clinical), medicine.symptom, medicine.drug

Abstract

Background Different “huntingtin-lowering” therapeutic strategies based on RNA modulation are in early development for Huntington’s disease (HD). Aims The aim of this study was to demonstrate the therapeutic potential of an antisense oligonucleotide (AON), with a (CUG)7 sequence targeting the CAG repeat in huntingtin (HTT) mRNA, in two different HD mouse models. Methods/techniques The R6/2 HD N-terminal fragment mouse model was used to assess the extent of phenotypic reversal, while silencing duration of huntingtin mRNA and protein was investigated in the Q175 HD mouse knock-in model. Both R6/2 and Q175 mice received six weekly intracerebroventricular infusions with (CUG)7 or vehicle and were sacrificed between 2 weeks (R6/2) up to 18 weeks (Q175) post last infusion. Levels of mutant HTT mRNA and protein were quantified by RT-qPCR and TR-FRET respectively. Results/outcome A highly significant and strong (~90%) reduction of mutant HTT mRNA levels was observed throughout the brain of (CUG)7-treated R6/2 mice, with a significant reduction of both soluble and aggregated mutant HTT protein in striatum, hippocampus and cortex. Furthermore, HTT-lowering increased whole brain and cortical volume and improved the performance of multiple motor tasks. In addition, reduced striatal levels of the gliosis marker myo-inositol were observed in (CUG)7-treated mice, along with increased mRNA levels of the striatal marker Darpp-32, a well-known integrator of dopamine signalling. These neuroanatomical and neurochemical changes, together with the improved motor performance, suggest that treatment with (CUG)7 ameliorates basal ganglia dysfunction. In Q175 mice a long lasting effect of treatment with (CUG)7 was observed on soluble mutant HTT protein levels, with a reduction of at least 30% persisting up to 18 weeks post-treatment in cortex, striatum and hippocampus. Conclusions These encouraging results support further preclinical development of the AON (CUG)7 as a therapeutic strategy for HD.

Published

2016