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18 results on '"Sako, Yukiya"'

1. A Dual Adjuvant System for Intranasal Boosting of Local and Systemic Immunity for Influenza Vaccination

Author

Sato-Kaneko, Fumi, Yao, Shiyin, Lao, Fitzgerald S, Sako, Yukiya, Jin, Jasmine, Shukla, Nikunj M, Cottam, Howard B, Chan, Michael, Belsuzarri, Masiel M, Carson, Dennis A, and Hayashi, Tomoko

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Clinical Sciences, Immunology, Influenza, Infectious Diseases, Lung, Biotechnology, Immunization, Pneumonia & Influenza, Prevention, Emerging Infectious Diseases, Biodefense, Vaccine Related, 3.4 Vaccines, Prevention of disease and conditions, and promotion of well-being, Infection, intranasal pulmonary boosting regimen, influenza virus infection, TLR4 agonist, TLR7 agonist, combination adjuvant, liposomal formulation, Clinical sciences, Medical microbiology
Abstract

Systemically vaccinated individuals against COVID-19 and influenza may continue to support viral replication and shedding in the upper airways, contributing to the spread of infections. Thus, a vaccine regimen that enhances mucosal immunity in the respiratory mucosa is needed to prevent a pandemic. Intranasal/pulmonary (IN) vaccines can promote mucosal immunity by promoting IgA secretion at the infection site. Here, we demonstrate that an intramuscular (IM) priming-IN boosting regimen with an inactivated influenza A virus adjuvanted with the liposomal dual TLR4/7 adjuvant (Fos47) enhances systemic and local/mucosal immunity. The IN boosting with Fos47 (IN-Fos47) enhanced antigen-specific IgA secretion in the upper and lower respiratory tracts compared to the IM boosting with Fos47 (IM-Fos47). The secreted IgA induced by IN-Fos47 was also cross-reactive to multiple influenza virus strains. Antigen-specific tissue-resident memory T cells in the lung were increased after IN boosting with Fos47, indicating that IN-Fos47 established tissue-resident T cells. Furthermore, IN-Fos47 induced systemic cross-reactive IgG antibody titers comparable to those of IM-Fos47. Neither local nor systemic reactogenicity or adverse effects were observed after IN delivery of Fos47. Collectively, these results indicate that the IM/IN regimen with Fos47 is safe and provides both local and systemic anti-influenza immune responses.

Published
2022

2. A Triple High Throughput Screening for Extracellular Vesicle Inducing Agents With Immunostimulatory Activity

Author

Shukla, Nikunj M, Sato-Kaneko, Fumi, Yao, Shiyin, Pu, Minya, Chan, Michael, Lao, Fitzgerald S, Sako, Yukiya, Saito, Tetsuya, Messer, Karen, Hayashi, Tomoko, Cottam, Howard B, Corr, Maripat, and Carson, Dennis A

Subjects
Pharmacology and Pharmaceutical Sciences, Biomedical and Clinical Sciences, Prevention, Biotechnology, Biodefense, Vaccine Related, 5.1 Pharmaceuticals, Development of treatments and therapeutic interventions, exosome, NFkB, HTS, compounds, immune, extracellular, adjuvant, reporter cells, Pharmacology and pharmaceutical sciences
Abstract

Extracellular vesicles (EVs) play an important role in intercellular communication and regulation of cells, especially in the immune system where EVs can participate in antigen presentation and may have adjuvant effects. We aimed to identify small molecule compounds that can increase EV release and thereby enhance the immunogenicity of vaccines. We utilized a THP-1 reporter cell line engineered to release EV-associated tetraspanin (CD63)-Turbo-luciferase to quantitatively measure EVs released in culture supernatants as a readout of a high throughput screen (HTS) of 27,895 compounds. In parallel, the cytotoxicity of the compounds was evaluated by PrestoBlue dye assay. For screening immunostimulatory potency, we performed two additional independent HTS on the same compound library using NF-κB and interferon-stimulated response element THP-1 reporter cell lines. Hit compounds were then identified in each of the 3 HTS's, using a "Top X″ and a Gaussian Mixture Model approach to rule out false positive compounds and to increase the sensitivity of the hit selection. Thus, 644 compounds were selected as hits which were further evaluated for induction of IL-12 in murine bone-marrow derived dendritic cells (mBMDCs) and for effects of cell viability. The resulting 130 hits were then assessed from a medicinal chemistry perspective to remove compounds with functional group liabilities. Finally, 80 compounds were evaluated as vaccine adjuvants in vivo using ovalbumin as a model antigen. We analyzed 18 compounds with adjuvant activity for their ability to induce the expression of co-stimulatory molecules on mBMDCs. The full complement of data was then used to cluster the compounds into 4 distinct biological activity profiles. These compounds were also evaluated for quantitation of EV release and spider plot overlays were generated to compare the activity profiles of compounds within each cluster. This tiered screening process identified two compounds that belong to the 4-thieno-2-thiopyrimidine scaffold with identical screening profiles supporting data reproducibility and validating the overall screening process. Correlation patterns in the adjuvanticity data suggested a role for CD63 and NF-κB pathways in potentiating antigen-specific antibody production. Thus, our three independent cell-based HTS campaigns led to identification of immunostimulatory compounds that release EVs and have adjuvant activity.

Published
2022

5. Branchpoints as potential targets of exon-skipping therapies for genetic disorders

Author

20964018, 20589593, 10208423, Ohara, Hiroaki, Hosokawa, Motoyasu, Awaya, Tomonari, Hagiwara, Atsuko, Kurosawa, Ryo, Sako, Yukiya, Ogawa, Megumu, Ogasawara, Masashi, Noguchi, Satoru, Goto, Yuichi, Takahashi, Ryosuke, Nishino, Ichizo, Hagiwara, Masatoshi, 20964018, 20589593, 10208423, Ohara, Hiroaki, Hosokawa, Motoyasu, Awaya, Tomonari, Hagiwara, Atsuko, Kurosawa, Ryo, Sako, Yukiya, Ogawa, Megumu, Ogasawara, Masashi, Noguchi, Satoru, Goto, Yuichi, Takahashi, Ryosuke, Nishino, Ichizo, and Hagiwara, Masatoshi

Abstract

Fukutin (FKTN) c.647+2084G>T creates a pseudo-exon with a premature stop codon, which causes Fukuyama congenital muscular dystrophy (FCMD). We aimed to ameliorate aberrant splicing of FKTN caused by this variant. We screened compounds focusing on splicing regulation using the c.647+2084G>T splicing reporter and discovered that the branchpoint, which is essential for splicing reactions, could be a potential therapeutic target. To confirm the effectiveness of branchpoints as targets for exon skipping, we designed branchpoint-targeted antisense oligonucleotides (BP-AONs). This restored normal FKTN mRNA and protein production in FCMD patient myotubes. We identified a functional BP by detecting splicing intermediates and creating BP mutations in the FKTN reporter gene; this BP was non-redundant and sufficiently blocked by BP-AONs. Next, a BP-AON was designed for a different FCMD-causing variant, which induces pathogenic exon trapping by a common SINE-VNTR-Alu-type retrotransposon. Notably, this BP-AON also restored normal FKTN mRNA and protein production in FCMD patient myotubes. Our findings suggest that BPs could be potential targets in exon-skipping therapeutic strategies for genetic disorders.

Published
2023

6. Identification of a Novel Small Molecule That Enhances the Release of Extracellular Vesicles with Immunostimulatory Potency via Induction of Calcium Influx

Author

Sako, Yukiya, primary, Sato-Kaneko, Fumi, additional, Shukla, Nikunj M., additional, Yao, Shiyin, additional, Belsuzarri, Masiel M., additional, Chan, Michael, additional, Saito, Tetsuya, additional, Lao, Fitzgerald S., additional, Kong, Helen, additional, Puffer, Marina, additional, Messer, Karen, additional, Pu, Minya, additional, Cottam, Howard B., additional, Carson, Dennis A., additional, and Hayashi, Tomoko, additional

Published
2023
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8. A Triple High Throughput Screening for Extracellular Vesicle Inducing Agents With Immunostimulatory Activity

Author

Shukla, Nikunj M., primary, Sato-Kaneko, Fumi, additional, Yao, Shiyin, additional, Pu, Minya, additional, Chan, Michael, additional, Lao, Fitzgerald S., additional, Sako, Yukiya, additional, Saito, Tetsuya, additional, Messer, Karen, additional, Hayashi, Tomoko, additional, Cottam, Howard B., additional, Corr, Maripat, additional, and Carson, Dennis A., additional

Published
2022
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9. A Triple High Throughput Screening for Extracellular Vesicle Inducing Agents With Immunostimulatory Activity

Author

Shukla, Nikunj M., Sato-Kaneko, Fumi, Yao, Shiyin, Pu, Minya, Chan, Michael, Lao, Fitzgerald S., Sako, Yukiya, Saito, Tetsuya, Messer, Karen, Hayashi, Tomoko, Cottam, Howard B., Corr, Maripat, and Carson, Dennis A.

Subjects
Pharmacology, reporter cells, Prevention, extracellular, Pharmacology and Pharmaceutical Sciences, NFkB, Vaccine Related, adjuvant, 5.1 Pharmaceuticals, Biodefense, exosome, Pharmacology (medical), HTS, compounds, immune, Development of treatments and therapeutic interventions, Biotechnology
Abstract

Extracellular vesicles (EVs) play an important role in intercellular communication and regulation of cells, especially in the immune system where EVs can participate in antigen presentation and may have adjuvant effects. We aimed to identify small molecule compounds that can increase EV release and thereby enhance the immunogenicity of vaccines. We utilized a THP-1 reporter cell line engineered to release EV-associated tetraspanin (CD63)-Turbo-luciferase to quantitatively measure EVs released in culture supernatants as a readout of a high throughput screen (HTS) of 27,895 compounds. In parallel, the cytotoxicity of the compounds was evaluated by PrestoBlue dye assay. For screening immunostimulatory potency, we performed two additional independent HTS on the same compound library using NF-κB and interferon-stimulated response element THP-1 reporter cell lines. Hit compounds were then identified in each of the 3 HTS’s, using a “Top X″ and a Gaussian Mixture Model approach to rule out false positive compounds and to increase the sensitivity of the hit selection. Thus, 644 compounds were selected as hits which were further evaluated for induction of IL-12 in murine bone-marrow derived dendritic cells (mBMDCs) and for effects of cell viability. The resulting 130 hits were then assessed from a medicinal chemistry perspective to remove compounds with functional group liabilities. Finally, 80 compounds were evaluated as vaccine adjuvants in vivo using ovalbumin as a model antigen. We analyzed 18 compounds with adjuvant activity for their ability to induce the expression of co-stimulatory molecules on mBMDCs. The full complement of data was then used to cluster the compounds into 4 distinct biological activity profiles. These compounds were also evaluated for quantitation of EV release and spider plot overlays were generated to compare the activity profiles of compounds within each cluster. This tiered screening process identified two compounds that belong to the 4-thieno-2-thiopyrimidine scaffold with identical screening profiles supporting data reproducibility and validating the overall screening process. Correlation patterns in the adjuvanticity data suggested a role for CD63 and NF-κB pathways in potentiating antigen-specific antibody production. Thus, our three independent cell-based HTS campaigns led to identification of immunostimulatory compounds that release EVs and have adjuvant activity.

Published
2022

10. Small Molecule Calcium Channel Activator Potentiates Adjuvant Activity

Author

Saito, Tetsuya, primary, Shukla, Nikunj M., additional, Sato-Kaneko, Fumi, additional, Sako, Yukiya, additional, Hosoya, Tadashi, additional, Yao, Shiyin, additional, Lao, Fitzgerald S., additional, Messer, Karen, additional, Pu, Minya, additional, Chan, Michael, additional, Chu, Paul J., additional, Cottam, Howard B., additional, Hayashi, Tomoko, additional, Carson, Dennis A., additional, and Corr, Maripat, additional

Published
2022
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11. Small Molecule Potentiator of Adjuvant Activity Enhancing Survival to Influenza Viral Challenge

Author

Saito, Tetsuya, primary, Sako, Yukiya, additional, Sato-Kaneko, Fumi, additional, Hosoya, Tadashi, additional, Yao, Shiyin, additional, Lao, Fitzgerald S., additional, Shpigelman, Jonathan, additional, Messer, Karen, additional, Pu, Minya, additional, Shukla, Nikunj M., additional, Chan, Michael, additional, Chu, Paul J., additional, Cottam, Howard B., additional, Hayashi, Tomoko, additional, Carson, Dennis A., additional, and Corr, Maripat, additional

Published
2021
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15. RBM24 promotes U1 snRNP recognition of the mutated 5′ splice site in theIKBKAPgene of familial dysautonomia

Author

Ohe, Kenji, primary, Yoshida, Mayumi, additional, Nakano-Kobayashi, Akiko, additional, Hosokawa, Motoyasu, additional, Sako, Yukiya, additional, Sakuma, Maki, additional, Okuno, Yukiko, additional, Usui, Tomomi, additional, Ninomiya, Kensuke, additional, Nojima, Takayuki, additional, Kataoka, Naoyuki, additional, and Hagiwara, Masatoshi, additional

Published
2017
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16. Development of an orally available inhibitor of CLK1 for skipping a mutated dystrophin exon in Duchenne muscular dystrophy

Author

00372524, 20600505, 10208423, Sako, Yukiya, Ninomiya, Kensuke, Okuno, Yukiko, Toyomoto, Masayasu, Nishida, Atsushi, Koike, Yuka, Ohe, Kenji, Kii, Isao, Yoshida, Suguru, Hashimoto, Naohiro, Hosoya, Takamitsu, Matsuo, Masafumi, Hagiwara, Masatoshi, 00372524, 20600505, 10208423, Sako, Yukiya, Ninomiya, Kensuke, Okuno, Yukiko, Toyomoto, Masayasu, Nishida, Atsushi, Koike, Yuka, Ohe, Kenji, Kii, Isao, Yoshida, Suguru, Hashimoto, Naohiro, Hosoya, Takamitsu, Matsuo, Masafumi, and Hagiwara, Masatoshi

Abstract

Duchenne muscular dystrophy (DMD) is a fatal progressive muscle-wasting disease. Various attempts are underway to convert severe DMD to a milder phenotype by modulating the splicing of the dystrophin gene and restoring its expression. In our previous study, we reported TG003, an inhibitor of CDC2-like kinase 1 (CLK1), as a splice-modifying compound for exon-skipping therapy; however, its metabolically unstable feature hinders clinical application. Here, we show an orally available inhibitor of CLK1, named TG693, which promoted the skipping of the endogenous mutated exon 31 in DMD patient-derived cells and increased the production of the functional exon 31-skipped dystrophin protein. Oral administration of TG693 to mice inhibited the phosphorylation of serine/arginine-rich proteins, which are the substrates of CLK1, and modulated pre-mRNA splicing in the skeletal muscle. Thus, TG693 is a splicing modulator for the mutated exon 31 of the dystrophin gene in vivo, possibly possessing therapeutic potential for DMD patients.

Published
2017

17. RBM24 promotes U1 snRNP recognition of the mutated 5′ splice site in the IKBKAPgene of familial dysautonomia

Author

Ohe, Kenji, Yoshida, Mayumi, Nakano-Kobayashi, Akiko, Hosokawa, Motoyasu, Sako, Yukiya, Sakuma, Maki, Okuno, Yukiko, Usui, Tomomi, Ninomiya, Kensuke, Nojima, Takayuki, Kataoka, Naoyuki, and Hagiwara, Masatoshi

Abstract

The 5′ splice site mutation (IVS20+6T>C) of the inhibitor of κ light polypeptide gene enhancer in B cells, kinase complex-associated protein(IKBKAP) gene in familial dysautonomia (FD) is at the sixth intronic nucleotide of the 5′ splice site. It is known to weaken U1 snRNP recognition and result in an aberrantly spliced mRNA product in neuronal tissue, but normally spliced mRNA in other tissues. Aberrantly spliced IKBKAPmRNA abrogates IKK complex-associated protein (IKAP)/elongator protein 1 (ELP1) expression and results in a defect of neuronal cell development in FD. To elucidate the tissue-dependent regulatory mechanism, we screened an expression library of major RNA-binding proteins (RBPs) with our mammalian dual-color splicing reporter system and identified RBM24 as a regulator. RBM24 functioned as a cryptic intronic splicing enhancer binding to an element (IVS20+13–29) downstream from the intronic 5′ splice site mutation in the IKBKAPgene and promoted U1 snRNP recognition only to the mutated 5′ splice site (and not the wild-type 5′ splice site). Our results show that tissue-specific expression of RBM24 can explain the neuron-specific aberrant splicing of IKBKAPexon 20 in familial dysautonomia, and that ectopic expression of RBM24 in neuronal tissue could be a novel therapeutic target of the disease.

Published
2017
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18. RBM24 promotes U1 snRNP recognition of the mutated 5' splice site in the IKBKAP gene of familial dysautonomia.

Author

Ohe K, Yoshida M, Nakano-Kobayashi A, Hosokawa M, Sako Y, Sakuma M, Okuno Y, Usui T, Ninomiya K, Nojima T, Kataoka N, and Hagiwara M

Subjects
Alternative Splicing, Animals, Cell Line, Exons, Gene Expression, Gene Knockdown Techniques, Genes, Reporter, High-Throughput Screening Assays, Humans, Introns, Mice, Models, Biological, Organ Specificity genetics, Protein Binding, RNA Precursors chemistry, RNA Precursors genetics, Regulatory Sequences, Nucleic Acid, Transcriptional Elongation Factors, Carrier Proteins genetics, Dysautonomia, Familial genetics, Dysautonomia, Familial metabolism, Mutation, RNA Splice Sites, RNA-Binding Proteins metabolism, Ribonucleoprotein, U1 Small Nuclear metabolism
Abstract

The 5' splice site mutation (IVS20+6T>C) of the inhibitor of κ light polypeptide gene enhancer in B cells, kinase complex-associated protein ( IKBKAP ) gene in familial dysautonomia (FD) is at the sixth intronic nucleotide of the 5' splice site. It is known to weaken U1 snRNP recognition and result in an aberrantly spliced mRNA product in neuronal tissue, but normally spliced mRNA in other tissues. Aberrantly spliced IKBKAP mRNA abrogates IKK complex-associated protein (IKAP)/elongator protein 1 (ELP1) expression and results in a defect of neuronal cell development in FD. To elucidate the tissue-dependent regulatory mechanism, we screened an expression library of major RNA-binding proteins (RBPs) with our mammalian dual-color splicing reporter system and identified RBM24 as a regulator. RBM24 functioned as a cryptic intronic splicing enhancer binding to an element (IVS20+13-29) downstream from the intronic 5' splice site mutation in the IKBKAP gene and promoted U1 snRNP recognition only to the mutated 5' splice site (and not the wild-type 5' splice site). Our results show that tissue-specific expression of RBM24 can explain the neuron-specific aberrant splicing of IKBKAP exon 20 in familial dysautonomia, and that ectopic expression of RBM24 in neuronal tissue could be a novel therapeutic target of the disease., (© 2017 Ohe et al.; Published by Cold Spring Harbor Laboratory Press for the RNA Society.)

Published
2017
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