Your search keyword '"Y. Sakoda"' showing total 357 results

1. Influence of horizontal loading height on subgrade reaction behavior acting on a pile

Author

S. Moriyasu, M. Okada, Y. Kikuchi, K. Sakimoto, Y. Sakoda, A. Mohri, S. Noda, and S. Oikawa

Subjects

Subgrade reaction, Geotechnical engineering, Pile, Geology

Published

2021

2. Oncogenic viruses: Oncorhynchus masou virus and Cyprinid herpesvirus

Author

M. Yoshimizu, H. Kasai, Y. Sakoda, N. Sano, and M. Sano

Subjects

viruses

Published

2017

3. Toll-like receptor 3 in nasal CD103

Author

H, Takaki, S, Kure, H, Oshiumi, Y, Sakoda, T, Suzuki, A, Ainai, H, Hasegawa, M, Matsumoto, and T, Seya

Subjects

Mice, Knockout, Lymphoid Tissue, Vaccination, Hemagglutinin Glycoproteins, Influenza Virus, Dendritic Cells, Nose, Immunity, Humoral, Immunoglobulin A, Toll-Like Receptor 3, Repressor Proteins, Mice, Basic-Leucine Zipper Transcription Factors, Influenza A Virus, H1N1 Subtype, Poly I-C, Orthomyxoviridae Infections, Antigens, CD, Influenza Vaccines, Transforming Growth Factor beta, Influenza, Human, Animals, Humans, Integrin alpha Chains, Cells, Cultured, Signal Transduction

Abstract

Intranasal inoculation with influenza hemagglutinin subunit with polyinosine-polycytidylic (polyI:C), a synthetic analog for double-stranded RNA, enhances production of vaccine-specific immunoglobulin (Ig) A, which is superior to IgG in prophylactic immunity. The mechanism whereby polyI:C skews to IgA production in the nasal-associated lymph tissue (NALT) was investigated in mouse models. Nasally instilled polyI:C was endocytosed into CD103

Published

2016

4. Immunity to virus infection (excluding retroviruses) (PP-025)

Author

R. M. Welsh, H. Momtaz, A. R. Thomsen, Y. Watanabe, V. Combes, X. Kong, W. T. Rothwell, M. Kanno, B. Kazemi, A. Shirani, D. Khachapuridze, M. Odenthal, R. Yanagisawa, Z. Ling, P. S. Ohashi, M. L. Freeman, Y. Lee, M Hernández, J. Miles, G. N. Milligan, Z. Liang, Paul G. Thomas, J. Tanaka, Ralph A. Tripp, E. Aguirre, S. Workman, A. Aguilar-Setien, T. Laurinolli, S. Lin, D. Kłosowska, S. Wang, O. Ikeda, K. Ostrow, K. Bogunia-Kubik, U. Kalinke, K. Lee, T. M. Ha, Katherine Kedzierska, G. K. Vikulov, M. Khodabandeh, R. J. Betts, Lisbeth Berrueta, M. Pasparakis, E. Kekäläinen, M. Hoshi, Z. Zeng, T. Toma, G. E. Kaiko, K. Huang, K. S. Lang, T. Ito, R. Hancock, L. Pham Van, U. B. Hellstrom, A. Lange, A. Meyers, R. Petraityte, E. Rizopulu, F. Xu, R. M. Zinkernagel, Y. Girerd-Chambaz, Katayoun Samimi-Rad, Seyed Moayed Alavian, T. Hsu, M. Schaller, D. S. Bowden, M. S. Rolph, H. Fujii, P. A. Lang, M. Akihiro, T. Furuta, S. P. Sylvan, Florian Kern, H. Shibata, Y. Ogawa, X. Zhang, F. Lai, H. Kida, U. Kumaraguru, J. Cardosa, Peter C. Doherty, Mark M. Davis, J. Pätzold, M. Matloubian, Y. Sakoda, P. Chaux, S. Lai, N. Nakajima, Y. Chen, K. Markiewicz, T. Tran, P. Chong, I. Lagereva, B. Sierra, E. Nazarov, M. Kikuchi, H. Ishida, C. Ferrari, David L. Woodland, A. G. Bean, M. H. Nelson, Z. J. Chen, D. M. Estes, M. R. Azar Pajoh, K. Vogt, M. A. Blackman, R. Todaka, S. Ma, W. Li, J. Sun, P. Lukianov, K. Gärtner, A. Vaheri, P. Wark, A. W. S. Yeung, A. Matsumura, L. Cao, I. Beĭkin, M. Recher, K. Eriksson, V. Wang, D. Webster, H. Yoshizawa, K. Hosiawa-Meagher, P. Sun, K. Katayama, H. Bisceglia, J. Du, M. Matsumoto, Z. Qu, P. J. Gaddi, M. R. Edwards, J. R. Carlyle, T. U. Aripova, A. G. Telcian, J. S. Yi, V. I. Afanasyeva, R. Kumar, B. Shaffaedin, S. Schoenberger, A. S. Khodjaeva, S. C. Weaver, D. Verthelyi, R. Sugamata, F. Ershov, R. Jafari Shakib, G. N. Feketea, A. Brook, H. Lei, Z. Qin, F. Vahedi, M. G. Guzmán, J. Huang, C. Ventura, A. Izquierdo, W. Siew Cheng, T. Kawamura, H. Keyvani, C. Ørskov, C. Tami, T. T. Tran, J. H. Fine, H. Kato, Z. J. Rakhmankulova, Y. A. Chen, J. C. Huang, K. Kobayashi, K. Kitamura, W. F. Carson, Azam Bolhassani, R. Rochford, J. Li, M. A. Bolkov, H. Liu, T. Ospelnikova, P. Storm, S. T. Smiley, L. A. Stanciu, F. Sánchez-García, M. Nakayama, M. B. Moreno-Altamrano, T. Wada, J. Deng, A. Perez, M. Puig, N. W. Lukacs, G. Liang, S. Jeon, L. C. Bonifaz-Alfonzo, S. Shimada, G. García, H. Marshall, A. Górski, S. Phipps, H. Tran, H. Kanegane, G. Korczak-Kowalska, C. Boni, J. Kyd, L. Rocha-Zavaleta, F. Garib, H. T. Q. Vu, M. Simadu, J. P. Twohig, B. G. Oliver, Shine Thomas, D. Chu, S. M. Cuff, Y. Lin, Z. Tian, S. Mäkelä, N. Mosaffa, M. Gołebiowska Wawrzyniak, R. Anderson, M. Brückel, T. P. Salazar-Mather, G. E. Grau, H. G. Durkin, I. R. Humphreys, W. Xi, H. Lin, Y. Sakakibara, A. Toga, P. Chen, K. Saito, Yasaman Taslimi, Leidith Berrueta-Carrillo, Y. Itoh, J. Sung, F. Liao, V. Emery, Y. Sato, S. Voigt, H. Horie, L. Simson, M. Larki, A. Hayashi, S. L. Rossi, R. Milne, R. Mirzaei, B. Evengård, Y. Liu, P. G. Mohr, B. Weiss-Steider, T. Nishimura, M. J. Crane, M. Høgh-Petersen, E. Sandalova, A. Dehghan, Z. Sharifnia, E. C. Y. Wang, H. Volk, M. L. Mora-García, C. M. Hogaboam, J. M. Clingan, A. T. Tan, N. Evstigneeva, P. Knolle, S. Hsieh, I. Kucinskaite-Kodze, M. Alvarez, Darrell L. Peterson, D. Tran, Sima Rafati, T. Seya, S. Marques, Tania Cukalac, F. Goshima, L. Perea-Martìnez, N. La Gruta, S. Kawachi, I. Hirono, M. Raeiszadeh, M. Koura, P. Holst, P. Kourilsky, R. Ganjali, J. P. Christensen, N. Hirankarn, L. Yao, A. Jakimiuk, J. Browne, I. V. Nesterova, M. Lu, M. Rezvani, C. Lin, B. A. Wu-Hsieh, G. P. Nolan, L. P. Bykova, B. Agrawal, K. Pérz-Saldaña, P. M. Niedzwiedzka-Rystwej, B. Pliego-Rivero, M. Farhadi, A. P. Godovalov, E. W. Newell, G. Hsu, L. T. P. Nguyen, Y. Chang, F. Rashidi, J. Tanguy, P. Kaiser, H. Lauterbach, F. Saito, R. Chua, P. W. Mason, I. A. Pashnina, H. Neekdan, Jamie Rossjohn, M. Toporkova, Luisa Barboza, H. Mitsui, M. C. Zaragoza-Ortega, E. L. Istomina, L. T. Dang, S. N. Boyarsky, A. Mesci, S. Vázquez, O. A. Aguilar, K. Shinoda, C. G. Silva, Stacie Woolard, M. Sadeghi, M. Jones, Farnaz Zahedifard, L. Wyatt, H. Dobashi, J. Simas, Henry Montes, N. Levchik, P. Kokhaei, C. Bartholdy, S. L. Kunkel, K. Suzuki, E. E. Ooi, Ashish Kumar, I. P. Balmasova, J. Ettinger, T. Nakayama, A. J. Zajac, R. Eftekhari, R. Lachmann, H. Inoue, D. Häussinger, D. Zhao, S. Koyasu, Chi Ma, Y. Keynan, M. V. Chikhladze, A. Hsu, F. Khodapanahandeh, W. Sun, K. Ogasawara, L. S. Tsai, M. Asano, A. Yachie, Stephanie Gras, J. Körner, N. Gaius, R. Gholamian-Dehkordi, Y. R. Sepiashvili, Y. Lu, Xinghao Ding, N. Vasilakis, D. Laccabue, H. Wu, J. Feng, S. Liu, X. Liang, M. Nowakowski, M. Krönke, K. I. Mattaei, D. V. Tran, K. L. O. Antonsdotter, K. Wong, B. Tzang, B. Dabirmanesh, H. Hochrein, Stephen J. Turner, A. Kulawik, D. Omagari, L. Skljar, O. Kovalenko, M. Seishima, H. Dienes, E. Rubinstein, L. Cervantes-Barragan, Y. Kim, I. Moro, U. Protzer, R. Sun, T. Mironova, D. M. Kemeny, J. Tavakkol Afshari, J. Mustonen, J. W. Lowenthal, T. P. Arstila, S. Kiabi, J. L. Munoz-Jordan, Z. S. Kamalov, Z. Wawrzyniak, C. Ahlm, K. Soda, Z. Mohtasham Amiri, Y. Aratani, T. Chumachenko, Y. Teruhito, Ali Eslamifar, J. Pedras-Vasconcelos, A. P. Durbin, N. J. C. King, H. Vu, M. Suter, T. Burgess, Z. Atai, T. Vo, E. R. Jellison, F. Li, M. C. Mohanty, E. V. Vlasova, T. Ball, H. Ishigaki, I. A. Tuzankina, C. R. Stewart, A. Flavigny, L. Nguyen, T. Sata, S. Akira, V. Kalihevich, E. Jaskula, O. Takeuchi, C. Aitken, K. Mohtashami, M. Bharadwaj, A. Bertoletti, Melisa Colmenares, H. Jenssen, S. Chen, J. Ramos-Castaneda, J. S. Ahn, D. Xilei, L. Hsu, A. Verschoor, M. Bandehpour, H. D. Volk, M. H. Bluth, M. Du, M. Tadashi, S. Mahalingam, C. Tsai, M. Arikata, Sophie A. Valkenburg, A. Monroy-García, M. Okamatsu, K. Rytwinski, K. Schmolke, D. B. Lewis, Siham Salmen, H. A. Mahgoub, C. Butts, A. Krishnamurthy, S. Moneer, H. Kondo, Ali Khamesipour, P. Ghyasemi-Dehkordi, L. Valdés, R. Aoki, L. A. Sandoval-Escobar, H. Ito, Natasha G. Swan, K. Dahlman-Wright, B. J. Hanson, P. M. Hansbro, P. Foster, M. Yasunami, Q. Ge, K. Tomizawa, U. Nivarthi, W. Wu, J. McCluskey, Y. Wang, J. Lee, J. McGrath, K. Yamamoto, J. Jan, L. Kjer-Nielsen, S. L. Johnston, H. Takaki, N. Prabhu, T. J. Standiford, B. Moss, L. Sanchez, P. Sodsai, M. Guzman, P. S. Foster, E. V. Shmeleva, A. Shestakov, T. Satoh, R. S. Kuzyaev, P. Wierzbicki, K. Fink, H. Rafat Panah, H. Ohtaki, J. Nakkuntod, E. S. Malova, K. Hirayama, H. Yagita, A. Zvirbliene, S. V. Mayer, B. Jin, L. Zuo, Z. Ardemasova, N. Harris, A. Kozar, S. Vostrukhin, J. Chang, C. Zhao, S. Kurata, S. Noorbakhsh, M. Muramatsu, E. Guillemard, O. Mikhailova, T. V. Vo, C. Fuentes-Miranda, P. Chaplin, D. Stabenow, N. Burdin, S. C. D. D. Abedelmalek, Y. Kuznetsova, Mohammad Taghikhani, D. K. Hong, A. B. Pérez, S. Yuichi, J. Hernández-Montes, O. Cruz y Cruz, T. Maciejewski, G. Siritsa, Elham Mohit, K. Morita, Y. Jiang, D. K. Krishnadas, K. Sasnauskas, W. M. Deptuła, H. Nguyen, J. Borysowski, K. Komiyama, C. Chuang, E. Markelova, N. Babel, K. R. Fowke, D. Thammanichanond, R. Kassub, C. Chirathaworn, A. Rizopulu, I. Gorelova, N. Van Rooijen, F. Pak, N. Bourne, D. Townsend, C. Krings, Y. Nishiyama, B. Ludewig, E. R. Winkelmann, J. M. Deshpande, S. Tsai, P. A. MacAry, Y. Mitsuya, S. Marashi, J. Niu, N. Watanabe, J. Schrezenmeir, R. M. Locksley, J. Jang, N. D. Yushchuk, Y. Su, S. Chowdhury, J. A. Juno, F. Ghazi, M. Hellard, H. Hengartner, Y. Ohmoto, W. Yang, R. B. Tesh, A. W. Ho, P. Kupatawintu, Z. Wang, P. Brundin, S. de la Motte, S. C. Bendall, M. Oshima, P. Tangkijvanich, T. Nagao, and B. M. M. Moreno-Altamirano

Subjects

Immunity, Immunology, Immunology and Allergy, General Medicine, Biology, Virology, Virus, Oncovirus

Published

2010

5. Drosophila MAGE controls neural precursor proliferation in postembryonic neurogenesis

Author

Kazuaki Yoshikawa, Isao Nishimura, and J.-Y. Sakoda

Subjects

endocrine system, Embryo, Nonmammalian, animal structures, Population, Apoptosis, Cell Count, Nerve Tissue Proteins, Biology, Nervous System, Animals, Genetically Modified, Neuroblast, RNA interference, In Situ Nick-End Labeling, Animals, Drosophila Proteins, Gene silencing, education, neoplasms, Mushroom Bodies, Cell Proliferation, Neurons, Genetics, education.field_of_study, Gene knockdown, Stem Cells, General Neuroscience, fungi, Neurogenesis, Pupa, Immunohistochemistry, Neural stem cell, Cell biology, Larva, Nerve Degeneration, Mushroom bodies, Drosophila, RNA Interference

Abstract

Necdin, a member of the MAGE family, is expressed abundantly in postmitotic neurons and is required for their differentiation and survival. In mammals, the MAGE family consists of more than 30 genes, whereas only one MAGE gene exists in the genome of nonmammalian vertebrates such as zebrafish and chicken. These nonmammalian MAGE genes are expressed in developing nervous system, and the primary structures of the encoded proteins resemble those of necdin-like MAGE proteins. Fruit fly Drosophila also carries a single necdin-like MAGE gene, which is highly expressed in neural stem cells (neuroblasts) during nervous system development. In the present study, we investigated the function of MAGE in Drosophila neurogenesis in vivo using an RNA interference (RNAi) -mediated gene knockdown system. Ubiquitous knockdown of Drosophila MAGE by double-stranded RNA injection into embryos was lethal at early stages of organogenesis. MAGE was then knocked down in developing mushroom bodies by RNAi-mediated gene silencing using the OK107-GAL4 driver. MAGE RNAi increased the population of proliferative neural precursors in larval mushroom bodies. At the pupal stage, RNAi-mediated MAGE knockdown led to a significant enlargement of the mushroom bodies as a result of increased neuronal population, presumably by accelerating the asymmetric division of neural stem cells. MAGE RNAi mushroom bodies of adult flies showed neurodegenerative changes such as vacuolation and nuclear DNA breaks, implying that supernumerary neurons undergo apoptosis during postpupal development. These results suggest that evolutionally conserved necdin-like MAGE is involved in both neural stem cell proliferation and neuronal survival during nervous system development.

Published

2008

6. Comparative Immunohistopathology in Pigs Infected with Highly Virulent or Less Virulent Strains of Hog Cholera Virus

Author

S. Yamada, M. Narita, K. Kimura, T. Shibahara, Y. Sakoda, K. Kawashima, and O. Mikami

Subjects

Male, 0301 basic medicine, Necrosis, Swine, 040301 veterinary sciences, T-Lymphocytes, Palatine Tonsil, Virulence, Spleen, Biology, Kidney, Classical Swine Fever, 0403 veterinary science, 03 medical and health sciences, Antigen, Ileum, medicine, Animals, Antigens, Viral, Pancreas, Histiocyte, B-Lymphocytes, General Veterinary, 04 agricultural and veterinary sciences, Hyperplasia, medicine.disease, Immunohistochemistry, Virology, Hematopoiesis, 030104 developmental biology, medicine.anatomical_structure, Classical Swine Fever Virus, Female, Lymph Nodes, medicine.symptom, CD8, Encephalitis

Abstract

Eight pigs were inoculated subcutaneously with a highly virulent hog cholera virus (HCV) strain ALD. The infected pigs developed severe illness and became moribund on postinoculation day (PID) 7 or PID 10. Histologic lesions were characterized by severe generalized vasculitis, necrosis of lymphocytes, and encephalitis. HCV antigen was detected in crypt tonsilar epithelial cells, macrophages, and reticular endothelial cells of lymphoid tissues. Antigen localization corresponded well with histologic lesions. Five pigs were inoculated with less virulent HCV Kanagawa/74 strain and were euthanatized on PID 30. All five infected pigs recovered from the illness but became stunted. They also had a slight follicular depletion of lymphocytes, histiocytic hyperplasia, and hematopoiesis in the spleen. Less virulent HCV antigen was observed in the tonsils, kidneys, pancreas, adrenal glands, and lungs. Although antigen localization was less associated with histologic lesions, immunoreactivity was stronger than that in the pigs infected with the ALD strain of HCV. An almost complete loss of B lymphocytes was recognized in pigs infected with the ALD strain and was correlated with follicular necrosis in lymphoid tissues. Loss of B lymphocytes was not prominent in the pigs infected with Kanagawa/74 strain. The number of CD4+ and CD8+ T lymphocytes was significantly higher than that in the noninfected control pigs.

Published

2000

7. Carboxyl terminus of the 34 kDa protein of Mycobacterium paratuberculosis shares homologous B-cell epitopes with Mycobacterium avium and Mycobacterium intracellulare

Author

M, Malamo, K, Okazaki, Y, Sakoda, and H, Kida

Subjects

Antigens, Bacterial, Mice, Inbred BALB C, Immunoblotting, Antibodies, Monoclonal, Cattle Diseases, Enzyme-Linked Immunosorbent Assay, Cross Reactions, Mycobacterium avium Complex, Antibodies, Bacterial, Recombinant Proteins, Cell Line, Mycobacterium, Mycobacterium avium subsp. paratuberculosis, Mice, Bacterial Proteins, Paratuberculosis, Animals, Epitopes, B-Lymphocyte, Cattle, Female, Rabbits, Mycobacterium avium

Abstract

Monoclonal antibodies (mAbs) against a recombinant carboxyl terminus of the 34 kDa protein of Mycobacterium paratuberculosis were produced in mice. Two of the mAbs cross-reacted with Mycobacterium avium and Mycobacterium intracellulare in both an elisa and immunoblot. The recombinant protein also reacted with polyclonal sera produced in rabbits against all three mycobacteria, indicating the presence of cross-reactive epitopes in the protein. To determine the reactivity of cattle sera against epitopes recognised by the mAbs, competition assays between bovine sera and the mAbs were carried out. Two mAbs were significantly inhibited by sera from cattle that were naturally infected with M paratuberculosis. The results indicate that epitopes on the carboxyl terminus of the 34 kDa protein common to M paratuberculosis, M avium and M intracellulare readily induce antibody production in naturally infected cattle. These epitopes reduce the diagnostic specificity of the carboxyl terminus of the 34 kDa protein, which was originally thought to contain only M paratuberculosis-specific epitopes.

Published

2007

8. Relationship of Odour and chemical structure in 1- and 2-alkyl alcohols and thiols

Author

A D Swift Karl, Y Sakoda, and S Hayashi

Subjects

chemistry.chemical_classification, Chemistry, Chemical structure, Organic chemistry, Alkyl

Published

2007

9. Library of influenza virus strains for vaccine and diagnostic use against highly pathogenic avian influenza and human pandemics

Author

H, Kida and Y, Sakoda

Subjects

Feces, Genomic Library, Asia, Ducks, Species Specificity, Influenza A virus, Influenza Vaccines, Influenza in Birds, Animals, Humans, Global Health, Alaska, Disease Outbreaks

Abstract

To prepare for the emergence of pandemic influenza in birds and mammals including humans, we have carried out global surveillance of avian influenza. Influenza A viruses of 48 combinations of 15 HA and 9 NA subtypes out of 135 theoretical combinations have been isolated from faecal samples of ducks in Alaska, Siberia, Mongolia, Taiwan, China and Japan. So far, viruses of 73 other combinations have been generated by genetic reassortment in chicken embryos. Thus, avian influenza viruses of 121 combinations of HA and NA subtypes have been stocked for use in vaccine and diagnosis. Their pathogenicity, antigenicity, genetic information, and yield in chicken embryo have been analysed and registered in the database.

Published

2006

10. [Visual field defect following macular hole surgery]

Author

S, Otsuka, A, Uemura, and Y, Sakoda

Subjects

Postoperative Complications, Vitrectomy, Vision Disorders, Humans, Female, Middle Aged, Visual Fields, Retinal Perforations

Abstract

We report three patients with inferotemporal visual field defect following pars plana vitrectomy for idiopathic macular hole. Two patients complained of the visual field defect early in the postoperative period, and one patient was asymptomatic but showed abnormalities in perimetry. The visual field defect remained unchanged during a follow-up study of 4 to 12 months. It is possible that inadvertent damage to the optic nerve associated with air/ fluid exchange or hyaloid membrane stripping caused the characteristic visual field defect.

Published

1996

11. [A case of ovarian mixed germ cell tumor consisting of four histological components]

Author

M, Nitta, Y, Sakoda, Y, Honda, H, Katabuchi, and H, Okamura

Subjects

Adult, Ovarian Neoplasms, Humans, Female, Neoplasms, Germ Cell and Embryonal

Published

1993

12. [The relationship between cervical maturity at cervical cerclage and its outcome]

Author

M, Ito, N, Kawasaki, T, Yoshimura, Y, Sakoda, and H, Okamura

Subjects

Adult, Fetal Membranes, Premature Rupture, Pregnancy, Apgar Score, Infant, Newborn, Pregnancy Outcome, Humans, Female, Uterine Cervical Incompetence, Cervix Uteri, Prognosis, Retrospective Studies

Published

1991

13. PP-4-31 The improvement of aspiration biopsy cytology by ultrasound guided high power aspiration

Author

T. Sashikata, Norio Kohno, K. Wakita, M. Takahashi, and Y. Sakoda

Subjects

Cancer Research, medicine.medical_specialty, Oncology, business.industry, Aspiration biopsy, Cytology, Medicine, Radiology, business, Ultrasound guided

Published

1996

14. Three Cases of Pseudarthrosis in the Scaphoid Bone

Author

T. Maehara, Y. Sakoda, and T. Sakou

Subjects

Pseudarthrosis, medicine.medical_specialty, Scaphoid bone, business.industry, medicine, medicine.disease, business, Surgery

Published

1974

15. Anterior decompression surgery on the cervical disorders due to the ossification of the posterior longitudinal ligament in the cervical spine

Author

T. Kozi, Y. Yano, T. Shimizu, S. Osako, T. Sakou, T. Maehara, Norio Morimoto, Yoshiyuki Morizono, K. Tomimura, Y. Sakoda, and H. Morinaga

Subjects

musculoskeletal diseases, medicine.medical_specialty, business.industry, Cervical Disorder, Decompression, Ossification, medicine.medical_treatment, Anterior decompression, Bone grafting, medicine.disease, Cervical spine, Surgery, Myelopathy, medicine, Vertebrectomy, medicine.symptom, business

Abstract

Since 1970 decompressive surgery has been performed upon 30 cases of cervical myelopathy due mainly to the ossification of the posterior longitudinal ligaments.Anterior decompression was carried out by way of subtotal vertebrectomy and the resection of the ossified posterior ligaments for 23 cases, followed by anterior interbody fusion with the strut bone grafting. For the remaining 7 cases, decompression laminectomy was operated on and for the last one both procedures. The anterior decompression results more effective improvement of ADL than decompression laminectomy.We thus far conclude that the anterior decompression is more advisable for those that ossifications were localized below the C3-4 level in the cervical spine.

Published

1976

16. Postoperative evaluation of the patients with lumbar spinal stenosis

Author

Norio Morimoto, T. Osako, S. Hatta, K. Tomimura, Y. Yano, Hideki Kawamura, M. Imabayashi, Y. Sakoda, T. Maehara, T. Sakou, M. Kizima, Yoshiyuki Morizono, T. Imakyure, and H. Morinaga

Subjects

medicine.medical_specialty, medicine.diagnostic_test, business.industry, medicine.medical_treatment, Lumbar spinal stenosis, Laminectomy, medicine.disease, Low back pain, Intermittent claudication, Surgery, Anesthesia, Facetectomy, Sensation, medicine, Postoperative results, medicine.symptom, business, Myelography

Abstract

Postoperative results were discussed in a series of 34 patients with lumbar spinal stenosis, treated by surgical procedure.Although most of them showed no evidence of remarkable neurological deficits, their chief complaints were low back pain, sensation of tingling on the legs, sciatics and intermittent claudication. Continuous priapismus and decbital sore in two cases were reported respectively.Decompressive laminectomy and facetectomy were effective for the relief of these symptoms.The diagnosis of lumbar spinal stenosis is usually suggested by the patient's symptoms but it can be determined by myelography.

Published

1975

17. A Case of Gargoylism

Author

H. Hirabe, Y. Sakoda, T. Hidaka, K. Yong, and Y. Kiyama

Subjects

Pathology, medicine.medical_specialty, Rib cage, business.industry, Coxa valga, Corneal opacity, Dwarfism, Anatomy, medicine.disease, Joints movement, Protuberant abdomen, Eleventh rib, Medicine, medicine.symptom, business, Congenital disorder

Abstract

Gagroylism, congenital disorder of mucopolysaccharide metabolism, was first described by Hunter in 1917. Its main clinical features are as follows; 1) mental retardation, 2) dwarfism, 3) Gargoyle appearance, 4) hepatomegaly and splenomegaly and 5) corneal opacity.Recently, we have observed a ten-years-old boy who suffered from protuberant abdomen and retardation of growth. Clinically, a limitation in joints movement and an umbilical herniation as well as the above mentioned features except corneal opacity, were existed. On X-ray examination, an enlarged Turkish saddle, oar-shaped ribs, cocave lenz-shaped vertebral bodies, coxa valga and hypoplastic carpalia were observed.We performed tetracycline bone labelling in this case. The number of tetracycline labelled osteons per mm2 of cortical cross section (symbol; Af) was 1.0 in the eleventh rib of this case. It was less than the Af in 10 age normal subjects.

Published

1975

18. Follow-up Study of Patients with the Ossification of the Posterior Longitudinal Ligaments in the Cervical Spine

Author

Yoshiyuki Morizono, Y. Yano, Y. Sakoda, Norio Morimoto, T. Sakou, T. Shimizu, T. Kooji, K. Tomimura, Hideki Kawamura, E. Shibuya, and T. Maehara

Subjects

medicine.medical_specialty, business.industry, Ossification, Incidence (epidemiology), Follow up studies, medicine.disease, Cervical spine, Surgery, Myelopathy, medicine.anatomical_structure, Medicine, Posterior longitudinal ligament, medicine.symptom, Severe disability, business, Cervical canal

Abstract

Since 1967, 120 patients with the ossification of the posterior longitudinal ligaments in the cervical spine have been treated in our clinic. 84 cases out of 120 had been followed up. Narrowing of the cervical canal in sagittal diameter due to the ossification, was 37 per cent in average in myelopathy and 24 per cent in non-myelopathy. The incidence of the level of the maximal ossificaticn were located in as the following order, C5, C6, C4, C3, C7 and C2.Conservative treatments were not so effective in most patients, but a few cases. Decompressive surgery should be taken into consideration before the patients with myelopathy had been fallen into severe disability.

Published

1976

19. A Case of Ewing's Sarcoma

Author

Y. Sakoda and N. Higashi

Subjects

Oncology, medicine.medical_specialty, business.industry, Internal medicine, medicine, Ewing's sarcoma, business, medicine.disease

Published

1972

20. [Clinical studies on 6 cases of embryonal carcinoma (author's transl)]

Author

C, Tayama, Y, Sakoda, K, Matsuura, A, Hashimoto, M, Nakayama, and M, Maeyama

Subjects

Adult, Ovarian Neoplasms, Adolescent, Mesonephroma, Teratoma, Humans, Female, alpha-Fetoproteins, Child

Published

1981

21. [A case of Fanconi's anemia in an adult (author's transl)]

Author

N, Nagatoshi, Y, Sakoda, N, Katayama, S, Kishimoto, and A, Yoshimura

Subjects

Adult, Chromosome Aberrations, Fanconi Anemia, Anemia, Aplastic, Humans, Female

Published

1975

22. Fetal blood velocity waveforms in uncomplicated pregnancy

Author

M, Ito, Y, Sakoda, T, Yunohara, M, Terao, K, Matsui, S, Fujisaki, and M, Maeyama

Subjects

Pregnancy, Humans, Female, Maternal-Fetal Exchange, Blood Flow Velocity, Umbilical Arteries, Ultrasonography

Abstract

Umbilical artery velocity waves were measured in fetuses from 94 normal pregnant women. In all, 183 determinations were carried out from the 14th to the 40th week of gestation. A combination of pulsed echo and real-time scanning was used to obtain blood waveforms from the umbilical arteries. The umbilical artery velocity wave can be readily differentiated from other fetal signals by its pattern. The systolic peak of the velocity wave was divided by the end diastolic value, thereby giving an S/D ratio. The S/D ratio in normal pregnancy declined from 7.6 to 2.0 from 14 to 40 weeks. Analysis of these waveforms indicated that the placenta is an organ of low vascular resistance and that placental resistance to blood flow declines with advancing gestational age in normal pregnancy. The umbilical artery S/D ratio provides a new and non-invasive marker of fetoplacental blood flow resistance.

Published

1986

23. [A case of abdominal desmoid during pregnancy]

Author

H, Katabuchi, K, Matsui, Y, Sakoda, S, Fujisaki, and H, Okamura

Subjects

Adult, Diagnosis, Differential, Leiomyoma, Pregnancy, Abdominal Neoplasms, Uterine Neoplasms, Humans, Female, Fibroma, Pregnancy Complications, Neoplastic, Abdominal Muscles

Published

1989

24. [The effects of cholera toxin in the release of beta-endorphin from the dispersed cells of the rat neurointermediate lobe]

Author

Y, Furuki, Y, Sakoda, Y, Hatada, M, Munemura, M, Maeyama, and M, Matsumura

Subjects

Male, Cholera Toxin, Pituitary Gland, beta-Endorphin, Cyclic AMP, Animals, Rats, Inbred Strains, Endorphins, In Vitro Techniques, Rats

Abstract

The intermediate lobe cells of pituitary gland synthesize and secrete bioactive peptides derived from proopiomelanocortin. In the present study, we investigated the effects of cholera toxin on the release of beta-endorphin (beta-Ep) from dispersed-intermediate lobe cells of rats. Cholera toxin added into culture medium, enhanced the intracellular accumulation of adenosine 3', 5'-monophosphate (cAMP) and the release of beta-endorphin like immunoreactive substance (beta-END-LIS). A positive dose-response relationship existed between the concentration of cholera toxin and the release of beta-END-LIS or the accumulation of cAMP. Maximal response was obtained with approximately 3 X 10(-10) M (in beta-END-LIS release) and 1 X 10(-9) M (in cAMP accumulation) concentration of cholera toxin. Incubation with cholera toxin (3 X 10(-8) M) resulted in a significant rise of cAMP accumulation after 20-30 min, and a 2-2.5 fold increase of beta-END-LIS release occurred after 60 min in comparison with nontreated cells. cAMP analog and phosphodiesterase inhibitor also increased the beta-END-LIS release). These results suggested the close relationship between cAMP accumulation and its biological effect (i.e. beta-END-LIS release).

Published

1984

25. [Stomach neoplasms associated with B-cell chronic lymphocytic leukemia]

Author

T, Saitoo, K, Kimura, M, Oda, T, Kawatsu, and Y, Sakoda

Subjects

Male, B-Lymphocytes, Stomach Neoplasms, Humans, Adenocarcinoma, Aged, Leukemia, Lymphoid

Published

1976

26. Edible bird's nest: N- and O-glycan analysis and synergistic anti-avian influenza virus activity with neuraminidase inhibitors.

Author

Sriwilaijaroen N, Hanamatsu H, Yokota I, Nishikaze T, Ijichi T, Takahashi T, Sakoda Y, Furukawa JI, and Suzuki Y

Subjects

Animals, Influenza in Birds virology, Influenza in Birds drug therapy, Enzyme Inhibitors pharmacology, Drug Synergism, Humans, Saliva virology, Hemagglutinin Glycoproteins, Influenza Virus metabolism, Polysaccharides pharmacology, Neuraminidase antagonists & inhibitors, Neuraminidase metabolism, Antiviral Agents pharmacology, Influenza A Virus, H5N1 Subtype drug effects, Birds, Oseltamivir pharmacology, Oseltamivir analogs & derivatives, Zanamivir pharmacology

Abstract

Zoonotic avian influenza viruses have continued to infect people on occasion. During treatment, antiviral resistant viruses have occasionally emerged, highlighting the need for a novel strategy for treating human illness. After pancreatin treatment, edible bird's nest (EBN), swiftlet saliva consumed for health purposes, possesses anti-avian viral activity by inhibiting receptor-binding hemagglutinin (HA) activity. Glycan analysis revealed an abundance of α2,3Neu5Ac decoy receptors in pancreatin-treated EBN. Fucosylated tri-α2,3Neu5Ac tri-antennary N-glycans (N-35) and di-α2,3Neu5Ac core 2 O-glycans (O-15) are predominant, accounting for 53.46% and 44.66% of total N- and O-glycan amounts, respectively. Isobologram analysis revealed that the treated EBN had a strong synergistic effect with either oseltamivir carboxylate or zanamivir, a competitive inhibitor of receptor-destroying neuraminidases (NAs), against the avian H5N1 virus. Taken together, EBN has the potential to be developed as a food-derived avian viral trap to prevent and decrease avian virus infection as well as in combination with a viral releasing-NA inhibitor to increase therapeutic potency, reduce toxicity, delay resistance development, and potentially prevent pandemic onset., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier B.V. All rights reserved.)

Published

2024

27. Genome sequencing of canine distemper virus isolates from unvaccinated dogs in Mongolia.

Author

Munkhtsetseg A, Batmagnai E, Odonchimeg M, Ganbat G, Enkhmandakh Y, Ariunbold G, Dolgorsuren T, Odbileg R, Dulam P, Tuvshintulga B, Sugimoto C, Sakoda Y, Yamagishi J, and Erdenechimeg D

Subjects

Animals, Dogs, Mongolia epidemiology, Phylogeny, Genetic Variation, Whole Genome Sequencing, Vero Cells, Male, Female, Chlorocebus aethiops, Distemper Virus, Canine genetics, Distemper Virus, Canine isolation & purification, Distemper Virus, Canine classification, Distemper virology, Distemper epidemiology, Genome, Viral

Abstract

Canine distemper virus (CDV) triggers a severe, often fatal disease in dogs and wildlife known as canine distemper (CD). Prior research has noted significant genetic diversity and recombination among CDV isolates from different geographical regions, potentially contributing to vaccine failures. Despite this, no genetic characterization of Mongolian CDVs has been conducted. This study, isolated CDVs from three unvaccinated dogs: two 10-month-old mixed-breeds and an 18-month-old Samoyed. All exhibited CD symptoms and subsequently died. Virus isolation was conducted using Vero/dog SLAM cells, with genome sequencing performed via nanopore technology. The mixed-breed dogs were infected with non-recombinant CDV isolates, forming a sister clade to the Asia-1 lineage prevalent in Asia. The Samoyed was infected with a non-recombinant CDV isolate, classifying as Asia-4 lineage sporadically reported in some Asian countries. This sequencing data offers foundational information on genetic diversity, aiding CD control measure development and benefiting future Eurasia and Asian studies., Competing Interests: Conflict of interest statement None of the authors of this paper have any financial or personal relationships with other individuals or organizations that could inappropriately influence or bias the content of the paper., (Copyright © 2024 Elsevier Ltd. All rights reserved.)

Published

2024

28. [A Case of Locally Advanced Breast Cancer with Ulceration, in Which the Combination of Mohs' Paste and Systemic Drug Therapy Resulted in Improvement of Quality of Life and Disease Control].

Author

Hashimoto T, Tsuchiya K, Sakoda Y, and Ogino M

Subjects

Humans, Female, Aged, Antineoplastic Combined Chemotherapy Protocols therapeutic use, Ulcer drug therapy, Carcinoma, Ductal, Breast drug therapy, Carcinoma, Ductal, Breast pathology, Combined Modality Therapy, Chlorides, Zinc Compounds, Breast Neoplasms drug therapy, Breast Neoplasms pathology, Quality of Life

Abstract

Locally advanced breast cancer can lead to self-destruction, necrosis, and malodor, which may reduce the patients' quality of life. We encountered a case where the combination of Mohs' paste and systemic drug therapy for locally advanced breast cancer improved quality of life and achieved marked disease control. The patient, a woman in her 70s, was referred to our department with suspected right breast cancer. After thorough examination, she was diagnosed with cT4bN3aM1(PUL), cStage Ⅳ, invasive ductal carcinoma, HER2 type. Mohs' paste treatment began on the 8th day, and systemic drug therapy was initiated on the 22nd day. Mohs' paste was applied once a week for a total of 4 times, resulting in significant tumor shrinkage. More than 6 months have passed since the start of treatment, and a complete response has been maintained, including pulmonary metastasis. Mohs' paste is a useful treatment for locally advanced breast cancer with self-destruction and necrosis.

Published

2024

29. Hemagglutinin and neuraminidase of a non-pathogenic H7N7 avian influenza virus coevolved during the acquisition of intranasal pathogenicity in chickens.

Author

Ichikawa T, Hiono T, Okamatsu M, Maruyama J, Kobayashi D, Matsuno K, Kida H, and Sakoda Y

Subjects

Animals, Virulence, Evolution, Molecular, Mutation, Poultry Diseases virology, Viral Proteins genetics, Viral Proteins metabolism, Chickens virology, Neuraminidase genetics, Neuraminidase metabolism, Influenza in Birds virology, Hemagglutinin Glycoproteins, Influenza Virus genetics, Hemagglutinin Glycoproteins, Influenza Virus metabolism, Influenza A Virus, H7N7 Subtype pathogenicity, Influenza A Virus, H7N7 Subtype genetics

Abstract

Polybasic amino acid residues at the hemagglutinin (HA) cleavage site are insufficient to induce the highly pathogenic phenotype of avian influenza viruses in chickens. In our previous study, an H7N7 avian influenza virus named "Vac2sub-P0", which is nonpathogenic despite carrying polybasic amino acids at the HA cleavage site, was passaged in chick air sacs, and a virus with high intravenous pathogenicity, Vac2sub-P3, was obtained. Intranasal infection with Vac2sub-P3 resulted in limited lethality in chickens; therefore, in this study, this virus was further passaged in chicken lungs, and the resultant virus, Vac2sub-P3L4, acquired high intranasal pathogenicity. Experimental infection of chickens with recombinant viruses demonstrated that mutations in HA and neuraminidase (NA) found in consecutive passages were responsible for the increased pathogenicity. The HA and NA functions of Vac2sub-P3L4 were compared with those of the parental virus in vitro; the virus growth at 40 °C was faster, the binding affinity to a sialic acid receptor was lower, and the rate of release by NA from the cell surface was lower, suggesting that these changes enabled the virus to replicate efficiently in chickens with high intranasal pathogenicity. This study demonstrates that viruses that are highly pathogenic when administered intranasally require additional adaptations for increased pathogenicity to be highly lethal to intranasally infected chickens., (© 2024. The Author(s), under exclusive licence to Springer-Verlag GmbH Austria, part of Springer Nature.)

Published

2024

30. Therapeutic Efficacy of IL7/CCL19-Expressing CAR-T Cells in Intractable Solid Tumor Models of Glioblastoma and Pancreatic Cancer.

Author

Ohta K, Sakoda Y, Adachi K, Shinozaki T, Nakajima M, Yasuda H, Nagano H, and Tamada K

Subjects

Humans, Animals, Mice, Cell Line, Tumor, ErbB Receptors metabolism, ErbB Receptors immunology, Brain Neoplasms immunology, Brain Neoplasms therapy, Brain Neoplasms pathology, T-Lymphocytes immunology, T-Lymphocytes metabolism, Female, Glioblastoma therapy, Glioblastoma immunology, Glioblastoma pathology, Pancreatic Neoplasms therapy, Pancreatic Neoplasms immunology, Pancreatic Neoplasms pathology, Immunotherapy, Adoptive methods, Receptors, Chimeric Antigen immunology, Receptors, Chimeric Antigen metabolism, Interleukin-7 metabolism, Xenograft Model Antitumor Assays

Abstract

Cancer immunotherapy using immune checkpoint inhibitors and its combination with other anticancer therapies has emerged as a new standard of care because of the encouraging therapeutic effects in various solid cancers. Nonetheless, glioblastoma and pancreatic cancer remain resistant to immunotherapy and represent intractable cancers with the poorest prognosis. We investigated the therapeutic effects of next-generation chimeric antigen receptor (CAR) T cells producing IL7 and chemokine (C-C motif) ligand 19 (CCL19; referred to as 7 × 19 CAR-T) in these intractable cancers. Cytotoxic activities and therapeutic effects of 7 × 19 CAR-T were evaluated in vitro and in vivo, in a model using EGFR variant III (EGFRvIII)-positive glioblastoma and anti-EGFRvIII CAR-T generated from healthy donor peripheral blood mononuclear cells (PBMC), or a model using HER2-positive pancreatic cancer organoids and anti-HER2 CAR-T generated from the same patient's PBMC. Anti-EGFRvIII 7 × 19 CAR-T exhibited cytotoxic activity specific to EGFRvIII-positive tumor, induced complete rejection of glioblastoma with massive T-cell infiltration and tumor cell death in the tumor tissues, and consequently prolonged mouse survival. Anti-HER2 7 × 19 CAR-T demonstrated a potent cytotoxic activity against autologous HER2-positive pancreatic cancer organoids and induced complete rejection of autologous tumor along with prolonged mouse survival. Our results suggest that 7 × 19 CAR-T could become a therapeutic option for glioblastoma and pancreatic cancer. To the best of our knowledge, this is the first study to demonstrate the therapeutic efficacy of next-generation CAR-T in an autologous model using patient-derived tumor organoids and CAR-T generated from the same patient's PBMC, in which unwanted allogeneic immune responses are fully excluded., Significance: Despite the clinical development of CAR T-cell therapy, its efficacy in solid cancers has yet to be established. This study explored the therapeutic potential and immunologic mechanisms of IL7/CCL19-producing CAR-T therapy in preclinical solid cancer models of glioblastoma and pancreatic cancer. We found that IL7/CCL19-producing CAR-T cells generated from the patient's PBMC showed potent therapeutic effects against the solid cancer model established by inoculating organoids from the autologous tumor tissue., (©2024 The Authors; Published by the American Association for Cancer Research.)

Published

2024

31. Cocirculation of Genetically Distinct Highly Pathogenic Avian Influenza H5N5 and H5N1 Viruses in Crows, Hokkaido, Japan.

Author

Hew YL, Hiono T, Monne I, Nabeshima K, Sakuma S, Kumagai A, Okamura S, Soda K, Ito H, Esaki M, Okuya K, Ozawa M, Yabuta T, Takakuwa H, Nguyen LB, Isoda N, Miyazawa K, Onuma M, and Sakoda Y

Subjects

Animals, Japan epidemiology, Influenza A virus genetics, Influenza A virus classification, Influenza in Birds virology, Influenza in Birds epidemiology, Influenza A Virus, H5N1 Subtype genetics, Influenza A Virus, H5N1 Subtype pathogenicity, Influenza A Virus, H5N1 Subtype classification, Influenza A Virus, H5N1 Subtype isolation & purification, Crows virology, Phylogeny

Abstract

We isolated highly pathogenic avian influenza (HPAI) H5N5 and H5N1 viruses from crows in Hokkaido, Japan, during winter 2023-24. They shared genetic similarity with HPAI H5N5 viruses from northern Europe but differed from those in Asia. Continuous monitoring and rapid information sharing between countries are needed to prevent HPAI virus transmission.

Published

2024

32. Molecular characterization of an avian rotavirus a strain detected from a large-billed crow (Corvus macrorhynchos) in Japan.

Author

Fujii Y, Masatani T, Nishiyama S, Takahashi T, Okajima M, Izumi F, Sakoda Y, Takada A, Ozawa M, Sugiyama M, and Ito N

Subjects

Animals, Japan, Crows virology, Rotavirus genetics, Rotavirus classification, Rotavirus isolation & purification, Rotavirus Infections virology, Rotavirus Infections veterinary, Rotavirus Infections transmission, Phylogeny, Bird Diseases virology, Bird Diseases transmission, Feces virology, Genotype

Abstract

Avian rotaviruses A (RVAs) are occasionally transmitted to animals other than the original hosts across species barriers. Information on RVAs carried by various bird species is important for identifying the origin of such interspecies transmission. In this study, to facilitate an understanding of the ecology of RVAs from wild birds, we characterized all of the genes of an RVA strain, JC-105, that was detected in a fecal sample of a large-billed crow (Corvus macrorhynchos) in Japan. All of the genes of this strain except for the VP4 and VP7 genes, which were classified as novel genotypes (P[56] and G40, respectively), were closely related to those of the avian-like RVA strain detected from a raccoon, indicating the possibility that crows had been involved in the transmission of avian RVAs to raccoons. Our findings highlight the need for further viral investigations in wild birds and mammals to understand the mechanisms of avian-to-mammal RVA transmission., Competing Interests: Declaration of competing interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2024 Elsevier Inc. All rights reserved.)

Published

2024

33. Evaluation of Immune Status of Pigs against Classical Swine Fever for Three Years after the Initiation of Vaccination in Gifu Prefecture, Japan.

Author

Kuwata K, Kuninaga N, Kimura Y, Makita K, Isoda N, Shimizu Y, and Sakoda Y

Abstract

In 2018, classical swine fever (CSF) reemerged in Gifu Prefecture, Japan, after 26 years of absence, and vaccination of domestic pigs using a live attenuated vaccine was initiated in 2019. Because the vaccine efficacy in piglets is influenced by the maternal antibody levels, vaccination should be administered at the optimal age by assuming the antibody level in sows. In this study, the shift in the antibody titer distribution in sows due to the initiation of vaccination to naïve herds and its influence on the vaccine-induced immunity rate in fattening pigs were investigated for 3 years. The results indicated that higher antibody titers were induced in first-generation sows after vaccine initiation because they were immunologically naïve, but the distribution of antibody titers shifted to lower levels along with their replacement with second-generation sows. The average vaccination age of fattening pigs became earlier year by year, and the vaccine-induced antibody rate was almost ≥80%. Based on the estimation of the optimal age for vaccination, it was found that vaccination at a younger age may reduce the risk of CSF infection. Taken together, the risk of CSF outbreaks can be reduced by administering vaccines at the optimal age based on the sequential monitoring of the sow's immune status.

Published

2024

34. Assessment of the Safety Profile of Chimeric Marker Vaccine against Classical Swine Fever: Reversion to Virulence Study.

Author

Huynh LT, Otsuka M, Kobayashi M, Ngo HD, Hew LY, Hiono T, Isoda N, and Sakoda Y

Subjects

Animals, Swine, Virulence, Vaccines, Marker immunology, Vaccines, Marker genetics, Vaccines, Marker administration & dosage, Vaccination, Classical Swine Fever prevention & control, Classical Swine Fever virology, Classical Swine Fever immunology, Viral Vaccines immunology, Viral Vaccines adverse effects, Viral Vaccines administration & dosage, Classical Swine Fever Virus immunology, Classical Swine Fever Virus genetics, Classical Swine Fever Virus pathogenicity, Vaccines, Attenuated immunology, Vaccines, Attenuated adverse effects, Vaccines, Attenuated administration & dosage

Abstract

Chimeric marker vaccine candidates, vGPE - /PAPeV E rns and vGPE - /PhoPeV E rns , have been generated and their efficacy and capability to differentiate infected from vaccinated animals were confirmed in previous studies. The safety profile of the two chimeric marker vaccine candidates, particularly in the potential reversion to virulence, was evaluated. Each virus was administered to pigs with a dose equivalent to the vaccination dose, and pooled tonsil homogenates were subsequently inoculated into further pigs. Chimeric virus vGPE - /PAPeV E rns displayed the most substantial attenuation, achieving this within only two passages, whereas vGPE - /PhoPeV E rns was detectable until the third passage and disappeared entirely by the fourth passage. The vGPE - strain, assessed alongside, consistently exhibited stable virus recovery across each passage without any signs of increased virulence in pigs. In vitro assays revealed that the type I interferon-inducing capacity of vGPE - /PAPeV E rns was significantly higher than that of vGPE - /PhoPeV E rns and vGPE - . In conclusion, the safety profile of the two chimeric marker vaccine candidates was affirmed. Further research is essential to ensure the stability of their attenuation and safety in diverse pig populations.

Published

2024

35. A pilot randomized controlled study to determine the effectiveness of video educational tool in BRCA1/2 pre-test counseling for Japanese breast cancer patients.

Author

Nakamura H, Morinaga S, Tsuchiya K, Sakoda Y, Ogino M, Ueno S, Tanino H, and Kunihisa T

Abstract

BRCA1/2 genetic testing has become clinically important in breast cancer care, but increasing demand may put a burden on the shortage of healthcare professionals. We performed a single-center, pilot randomized controlled study to assess the effectiveness of employing a video educational tool that included standard pre-test genetic counseling elements related to BRCA1/2. Patients with operable breast cancer who met the criteria for genetic testing based on age, sex, subtype, and family history were recruited. Sixty consenting participants were randomized 1:1 and placed in groups that received either traditional face-to-face pre-test counseling or video-viewing and face-to-face decisional support. To assess decisional conflict in the participants, surveys based on the Decisional Conflict Scale (DCS) were administered two times, once immediately after intervention and again 2-4 weeks later. The time taken for counseling and confirmation of whether the participants had undergone testing were also recorded. The difference in the total DCS scores between the two groups was not significantly different for either of the survey periods, and there was no significant difference in the number of participants who underwent testing (23/30 [76.7%] vs. 26/30 [86.7%]; p = 0.51). However, the "effective decision" subscale score was significantly higher in the video group 2-4 weeks after counseling (31.01 ± 16.82 vs. 21.43 ± 16.09; p = 0.04 [mean ± SD]). The time taken for counseling was significantly shorter in the video group (8.00 ± 4.5 vs. 27.00 ± 7.61 min; p < 0.001 [median ± SD]). Our findings indicate the potential benefit of the video educational tool for providing BRCA1/2-related information. These tools may also enable healthcare professionals to spend more time supporting psychological issues. Notably, after some time, patients may question whether their decision was appropriate. Therefore, it is necessary to identify those in conflict and provide them with proper support., (© 2024 National Society of Genetic Counselors.)

Published

2024

36. FOUR-WEEK ORAL ADMINISTRATION OF BALOXAVIR MARBOXIL AS AN ANTI-INFLUENZA VIRUS DRUG SHOWS NO TOXICITY IN CHICKENS.

Author

Miki M, Obara RD, Nishimura K, Shishido T, Ikenaka Y, Oka R, Sato K, Nakayama SMM, Kimura T, Kobayashi A, Aoshima K, Saito K, Hiono T, Isoda N, and Sakoda Y

Subjects

Animals, Administration, Oral, Pyridines administration & dosage, Thiepins administration & dosage, Thiepins pharmacology, Male, Influenza in Birds drug therapy, Female, Oxazines, Hydroxybutyrates administration & dosage, Triazines administration & dosage, Chickens, Dibenzothiepins administration & dosage, Antiviral Agents administration & dosage, Antiviral Agents pharmacology, Morpholines administration & dosage, Morpholines pharmacology, Pyridones administration & dosage, Pyridones pharmacology

Abstract

High pathogenicity avian influenza is an acute zoonotic disease with high mortality in birds caused by a high pathogenicity avian influenza virus (HPAIV). Recently, HPAIV has rapidly spread worldwide and has killed many wild birds, including endangered species. Baloxavir marboxil (BXM), an anti-influenza agent used for humans, was reported to reduce mortality and virus secretion from HPAIV-infected chickens ( Gallus domesticus , order Galliformes) at a dosage of ≥2.5 mg/kg when administered simultaneously with viral challenge. Application of this treatment to endangered birds requires further information on potential avian-specific toxicity caused by repeated exposure to BXM over the long term. To obtain information of potential avian-specific toxicity, a 4-wk oral repeated-dose study of BXM was conducted in chickens ( n = 6 or 7 per group), which are commonly used as laboratory avian species. The study was conducted in reference to the human pharmaceutical guidelines for nonclinical repeated-dose drug toxicity studies to evaluate systemic toxicity and exposure. No adverse changes were observed in any organs examined, and dose proportional increases in systemic exposure to active pharmaceutical ingredients were noted from 12.5 to 62.5 mg/kg per day. BXM showed no toxicity to chickens at doses of up to 62.5 mg/kg per day, at which systemic exposure was approximately 71 times higher than systemic exposure at 2.5 mg/kg, the reported efficacious dosage amount, in HPAIV-infected chickens. These results also suggest that BXM could be considered safe for treating HPAIV-infected endangered birds due to its high safety margin compared with the efficacy dose. The data in this study could contribute to the preservation of endangered birds by using BXM as a means of protecting biodiversity.

Published

2024

37. Phylogenetic analysis of small ruminant lentiviruses in Mongolian sheep supports an ancient east-west split for the genotype A.

Author

Davaasuren N, Molaee V, Erdene-Ochir TO, Nyamdavaa G, Ganzorig S, Mazzei M, Sakoda Y, Lühken G, and Tumenjargal S

Subjects

Animals, Sheep virology, Mongolia epidemiology, Visna-maedi virus genetics, Visna-maedi virus classification, Visna-maedi virus isolation & purification, Arthritis-Encephalitis Virus, Caprine genetics, Arthritis-Encephalitis Virus, Caprine classification, Arthritis-Encephalitis Virus, Caprine isolation & purification, Seroepidemiologic Studies, Phylogeny, Lentivirus Infections veterinary, Lentivirus Infections virology, Lentivirus Infections epidemiology, Sheep Diseases virology, Sheep Diseases epidemiology, Genotype

Abstract

The ovine maedi-visna virus (MVV) and caprine arthritis-encephalitis virus (CAEV) are small ruminant lentiviruses (SRLVs) with striking genetic and structural similarities. The presence of SRLV in Mongolian sheep and goats was serologically demonstrated more than a decade ago; however, the viral genotype remains unknown. In total, 329 blood samples were collected from two sheep breeds (i.e., Khalkha and Sumber) in Tov, Govisumber, Arkhangay, Dornogovi, Zavkhan, and Sukhbaatar provinces, Mongolia. Serological and phylogenetic analyses were performed regardless of any apparent clinical signs, although most of the animals appeared healthy. All sheep in three of the six provinces were seronegative, whereas the seroprevalence in the Tov, Govisumber, and Zavkhan provinces averaged 7.9%. Genomic DNA from seropositive animals was tested using hemi-nested polymerase chain reaction, and sub-genomic SRLV sequences were determined from nine samples. Mongolian SRLV sequences clustered within the divergent subtype A22, which was previously found only in Fertile Crescent regions, including Lebanon, Jordan, and Iran, where the first sheep-domestication (Ovis aries) occurred. According to the phylogenetic analysis, genotype A has two ancestors from the ancient Fertile Crescent: (1) Turkish strains and (2) Iranian, Jordanian, and Lebanese strains. The first ancestor spread westward, whereas the second spread eastward, ultimately reaching Mongolia., (© 2024. The Author(s), under exclusive licence to Springer Nature B.V.)

Published

2024

38. High Frequency of BRCA2 c.5576&#95;5579del Carriers in Kakogawa, Japan.

Author

Nakamura H, Mizumoto S, Tanino H, Niwa Y, Ogino M, Sakoda Y, Tsuchiya K, Kono S, Konishi M, Ueno S, and Kunihisa T

Abstract

Background/aim: Certain germline pathogenic variants (PVs), known as founder mutations, have been frequently observed in specific regions and ethnic groups. In Japan, several pathogenic variants of BRCA1/2 have been identified as founder mutations, with their distribution varying across different regions. This retrospective study aimed to further investigate the detailed distribution and correlation between genotype and clinical features among breast cancer patients., Patients and Methods: This study was conducted at Kobe University Hospital and three collaborating institutions. It included breast cancer patients who underwent BRCA1/2 genetic testing between July 1, 2018, and March 31, 2021, and were found to have germline PVs. Clinical characteristics and breast cancer subtypes were compared between carriers of BRCA2 c.5576&#95;5579del and those with other PVs. Additionally, the detection rate of BRCA2 c.5576&#95;5579del was compared with that observed in a previous report., Results: A total of 38 breast cancer patients were included; PVs in BRCA1 and BRCA2 were detected in 12 and 26 patients, respectively, 12 of whom were BRCA2 c.5576&#95;5579del carriers. BRCA2 c.5576&#95;5579del carriers were more likely to develop triple negative breast cancers among all BRCA2 PV carriers. BRCA2 c.5576&#95;5579del accounted for 30.8% of the PVs detected, with a particularly high frequency of 72.7% at Kakogawa Central City Hospital., Conclusion: BRCA2 c.5576&#95;5579del was detected with a particularly high frequency in Hyogo Prefecture, especially in Kakogawa city. In the future, a survey of the distribution of the BRCA2 c.5576&#95;5579del carriers may provide more clarity regarding their localization., Competing Interests: Sachiko Mizumoto, Hirokazu Tanino and Tomonari Kunihisa received a research grant from Ono Pharmaceutical Co. Ltd. Tomonari Kunihisa is a lecturer in an endowed chair founded by Hyogo Prefecture. The other Authors declare no conflicts of interest in relation to this study., (Copyright 2024, International Institute of Anticancer Research.)

Published

2024

39. Development of a dual immunochromatographic test strip to detect E2 and E rns antibodies against classical swine fever.

Author

Huynh LT, Sohn EJ, Park Y, Kim J, Shimoda T, Hiono T, Isoda N, Hong SH, Lee HN, and Sakoda Y

Abstract

Background: It is essential to consider a practical antibody test to successfully implement marker vaccines and validate vaccination efficacy against classical swine fever virus (CSFV). The test should include a serological antibody assay, combined with a tool for differentiating infected from vaccinated animals (DIVA). The immunochromatographic test strip (ICS) has been exclusively designed for detecting CSFV E2 antibodies while lacking in detecting E rns antibodies, which can be employed and satisfy DIVA strategy. This study developed a novel ICS for detecting CSFV E2/E rns dual-antibody. The effectiveness of ICS in evaluating the DIVA capability of two novel chimeric pestivirus vaccine candidates was assessed., Methods: Recombinant E2 or E rns protein was transiently expressed in the plant benthamiana using Agrobacterium tumefaciens . ICS was subsequently assembled, and goat anti-rabbit IgG and recombinant CSFV E2 or E rns protein were plated onto the nitrocellulose membrane as control and test lines, respectively. The sensitivity and specificity of ICS were evaluated using sera with different neutralizing antibody titers or positive for antibodies against CSFV and other pestiviruses. The coincidence rates for detecting E2 and E rns antibodies between ICS and commercial enzyme-linked immunosorbent assay (ELISA) kits were also computed. ICS performance for DIVA capability was evaluated using sera from pigs vaccinated with conventional vaccine or chimeric vaccine candidates., Results: E2 and E rns proteins were successfully expressed in N. benthamiana -produced recombinant proteins. ICS demonstrated high sensitivity in identifying CSFV E2 and E rns antibodies, even at the low neutralizing antibody titers. No cross-reactivity with antibodies from other pestiviruses was confirmed using ICS. There were high agreement rates of 93.0 and 96.5% between ICS and two commercial ELISA kits for E2 antibody testing. ICS also achieved strong coincidence rates of 92.9 and 89.3% with two ELISA kits for E rns antibody detection. ICS confirmed the absence of CSFV E rns -specific antibodies in sera from pigs vaccinated with chimeric vaccine candidates., Conclusion: E2 and E rns proteins derived from the plant showed great potential and can be used to engineer a CSFV E2/E rns dual-antibody ICS. The ICS was also highly sensitive and specific for detecting CSFV E2 and E rns antibodies. Significantly, ICS can fulfill the DIVA concept by incorporating chimeric vaccine candidates., Competing Interests: E-JS, YP, and JK were employed by BioApplications Inc. S-HH and H-NL were employed by Celltrix Co., Ltd. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2024 Huynh, Sohn, Park, Kim, Shimoda, Hiono, Isoda, Hong, Lee and Sakoda.)

Published

2024

40. Risk Factors for COVID-19 Cluster Infection in Hospitalized Patients.

Author

Sakoda Y, Matsumoto T, Yamaguchi M, Kudo A, Nakano K, and Maeno Y

Abstract

Introduction In Japan, in the seventh wave of coronavirus disease 2019 (COVID-19) from July 2022 to September 2022, followed by the eighth wave of COVID-19 from November 2022 to January 2023, nosocomial clusters became more frequent in many healthcare facilities. If a cluster occurs in a hospital, the restrictions on general healthcare and the impact on hospital management, as well as the impact on community healthcare, are enormous. We analyzed the risk factors for COVID-19 cluster infection in hospitalized patients. Methods We retrospectively collected cases of COVID-19 infection among hospitalized patients in the seventh and eighth waves. The occurrence of a COVID-19 patient in a hospitalized patient was defined as one event. Results A total of 40 events were observed in the seventh and eighth waves. There were 17 events that developed into clusters. The following factors showed a significant association with cluster infection in a univariate analysis: "seventh wave," "originated from healthcare worker," and "initial examination according to contact list." The multivariate analysis revealed that "originated from healthcare worker" was independently associated with cluster infection. Conclusion Preventing the development of COVID-19 clusters is very important for nosocomial infection control. Our study suggests that COVID-19 infection in a healthcare worker is a risk factor for the development of a cluster. When healthcare workers are infected with severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), it is often due to household transmission. Measures against household transmissions are important to prevent infection among healthcare workers., Competing Interests: The authors have declared that no competing interests exist., (Copyright © 2024, Sakoda et al.)

Published

2024

41. Establishment of a superinfection exclusion method for pestivirus titration using a recombinant reporter pestiviruses.

Author

Mimura Y, Hiono T, Huynh LT, Ogino S, Kobayashi M, Isoda N, and Sakoda Y

Subjects

Animals, Swine, Luciferases genetics, Pestivirus genetics, Superinfection veterinary, Classical Swine Fever Virus genetics, Swine Diseases

Abstract

Pestiviruses are classified into two biotypes based on their cytopathogenicity. As the majority of pestivirus field isolates are noncytopathogenic, their titration requires alternative methods rather than direct observation of cytopathogenic effects, such as immunostaining using specific antibodies or interference with cytopathogenic strains. However, these methods require microscopic observation to assess virus growth, which is time- and labor-intensive, especially when handling several samples. In this study, we developed a novel luciferase-based pestivirus titration method using the superinfection exclusion phenomenon with recombinant reporter pestiviruses that possessed an 11-amino-acid subunit derived from NanoLuc luciferase (HiBiT). In this method, swine kidney cells were inoculated with classical swine fever virus (CSFV) and superinfected with the reporter CSFV vGPE - /HiBiT 5 days postinoculation. Virus titer was determined based on virus growth measured in luminescence using the culture fluid 3 days after superinfection; the resultant virus titer was comparable to that obtained by immunoperoxidase staining. Furthermore, this method has proven to be applicable for the titration of border disease virus (BDV) by superinfection with both the homologous reporter BDV and heterologous reporter CSFV, suggesting that this novel virus titration method is a simple technique for automated virus detection based on the luciferase system.

Published

2024

42. A rapid and versatile reverse genetics approach for generating recombinant positive-strand RNA viruses that use IRES-mediated translation.

Author

Tamura T, Yamamoto H, Ogino S, Morioka Y, Tsujino S, Suzuki R, Hiono T, Suzuki S, Isoda N, Sakoda Y, and Fukuhara T

Subjects

Animals, Internal Ribosome Entry Sites genetics, Mammals genetics, Positive-Strand RNA Viruses genetics, Positive-Strand RNA Viruses metabolism, RNA, Viral genetics, Hepatitis C metabolism, Protein Biosynthesis, Reverse Genetics methods

Abstract

Reverse genetics systems have played a central role in developing recombinant viruses for a wide spectrum of virus research. The circular polymerase extension reaction (CPER) method has been applied to studying positive-strand RNA viruses, allowing researchers to bypass molecular cloning of viral cDNA clones and thus leading to the rapid generation of recombinant viruses. However, thus far, the CPER protocol has only been established using cap-dependent RNA viruses. Here, we demonstrate that a modified version of the CPER method can be successfully applied to positive-strand RNA viruses that use cap-independent, internal ribosomal entry site (IRES)-mediated translation. As a proof-of-concept, we employed mammalian viruses with different types (classes I, II, and III) of IRES to optimize the CPER method. Using the hepatitis C virus (HCV, class III), we found that inclusion in the CPER assembly of an RNA polymerase I promoter and terminator, instead of those from polymerase II, allowed greater viral production. This approach was also successful in generating recombinant bovine viral diarrhea virus (class III) following transfection of MDBK/293T co-cultures to overcome low transfection efficiency. In addition, we successfully generated the recombinant viruses from clinical specimens. Our modified CPER could be used for producing hepatitis A virus (HAV, type I) as well as de novo generation of encephalomyocarditis virus (type II). Finally, we generated recombinant HCV and HAV reporter viruses that exhibited replication comparable to that of the wild-type parental viruses. The recombinant HAV reporter virus helped evaluate antivirals. Taking the findings together, this study offers methodological advances in virology., Importance: The lack of versatility of reverse genetics systems remains a bottleneck in viral research. Especially when (re-)emerging viruses reach pandemic levels, rapid characterization and establishment of effective countermeasures using recombinant viruses are beneficial in disease control. Indeed, numerous studies have attempted to establish and improve the methods. The circular polymerase extension reaction (CPER) method has overcome major obstacles in generating recombinant viruses. However, this method has not yet been examined for positive-strand RNA viruses that use cap-independent, internal ribosome entry site-mediated translation. Here, we engineered a suitable gene cassette to expand the CPER method for all positive-strand RNA viruses. Furthermore, we overcame the difficulty of generating recombinant viruses because of low transfection efficiency. Using this modified method, we also successfully generated reporter viruses and recombinant viruses from a field sample without virus isolation. Taking these findings together, our adapted methodology is an innovative technology that could help advance virologic research., Competing Interests: The authors declare no conflict of interest.

Published

2024

43. Phylogenetic Analysis of Newcastle Disease Virus Isolated from Poultry in Live Bird Markets and Wild Waterfowl in Zambia.

Author

Kalonda A, Saasa N, Kajihara M, Nao N, Moonga L, Ndebe J, Mori-Kajihara A, Mukubesa AN, Sakoda Y, Sawa H, Takada A, and Simulundu E

Abstract

Poultry production is essential to the economy and livelihood of many rural Zambian households. However, the industry is threatened by infectious diseases, particularly Newcastle disease virus (NDV) infection. Therefore, this study employed next-generation sequencing to characterise six NDV isolates from poultry in Zambia's live bird markets (LBMs) and wild waterfowl. Four NDV isolates were detected from 410 faecal samples collected from chickens in LBMs in Lusaka and two from 2851 wild birds from Lochinvar National Park. Phylogenetic analysis revealed that the four NDVs from LBM clustered in genotype VII and sub-genotype VII.2 were closely related to viruses previously isolated in Zambia and other Southern African countries, suggesting possible local and regional transboundary circulation of the virus. In contrast, the two isolates from wild birds belonged to class I viruses, genotype 1, and were closely related to isolates from Europe and Asia, suggesting the possible introduction of these viruses from Eurasia, likely through wild bird migration. The fusion gene cleavage site motif for all LBM-associated isolates was 112 RRQKR|F 117 , indicating that the viruses are virulent, while the isolates from wild waterfowl had the typical 112 ERQER|L 117 avirulent motif. This study demonstrates the circulation of virulent NDV strains in LBMs and has, for the first time, characterised NDV from wild birds in Zambia. The study further provides the first whole genomes of NDV sub-genotype VII.2 and genotype 1 from Zambia and stresses the importance of surveillance and molecular analysis for monitoring the circulation of NDV genotypes and viral evolution.

Published

2024

44. The impact of PA/I38 substitutions and PA polymorphisms on the susceptibility of zoonotic influenza A viruses to baloxavir.

Author

Taniguchi K, Noshi T, Omoto S, Sato A, Shishido T, Matsuno K, Okamatsu M, Krauss S, Webby RJ, Sakoda Y, and Kida H

Subjects

Animals, Dogs, Humans, Swine, Oxazines pharmacology, Pyridines pharmacology, Pyridines therapeutic use, Antiviral Agents pharmacology, Antiviral Agents therapeutic use, Enzyme Inhibitors pharmacology, Enzyme Inhibitors therapeutic use, Amino Acid Substitution, Endonucleases genetics, Drug Resistance, Viral genetics, Influenza A virus genetics, Influenza A Virus, H5N1 Subtype genetics, Thiepins pharmacology, Thiepins therapeutic use, Influenza, Human, Orthomyxoviridae genetics, Dibenzothiepins, Morpholines, Pyridones, Triazines

Abstract

Genetic reassortment of avian, swine, and human influenza A viruses (IAVs) poses potential pandemic risks. Surveillance is important for influenza pandemic preparedness, but the susceptibility of zoonotic IAVs to the cap-dependent endonuclease inhibitor baloxavir acid (BXA) has not been thoroughly researched. Although an amino acid substitution at position 38 in the polymerase acidic protein (PA/I38) in seasonal IAVs reduces BXA susceptibility, PA polymorphisms at position 38 are rarely seen in zoonotic IAVs. Here, we examined the impact of PA/I38 substitutions on the BXA susceptibility of recombinant A(H5N1) viruses. PA mutants that harbored I38T, F, and M were 48.2-, 24.0-, and 15.5-fold less susceptible, respectively, to BXA than wild-type A(H5N1) but were susceptible to the neuraminidase inhibitor oseltamivir acid and the RNA polymerase inhibitor favipiravir. PA mutants exhibited significantly impaired replicative fitness in Madin-Darby canine kidney cells at 24 h postinfection. In addition, in order to investigate new genetic markers for BXA susceptibility, we screened geographically and temporally distinct IAVs isolated worldwide from birds and pigs. The results showed that BXA exhibited antiviral activity against avian and swine viruses with similar levels to seasonal isolates. All viruses tested in the study lacked the PA/I38 substitution and were susceptible to BXA. Isolates harboring amino acid polymorphisms at positions 20, 24, and 37, which have been implicated in the binding of BXA to the PA endonuclease domain, were also susceptible to BXA. These results suggest that monitoring of the PA/I38 substitution in animal-derived influenza viruses is important for preparedness against zoonotic influenza virus outbreaks., (© 2024. The Author(s).)

Published

2024

45. Development of short hairpin RNA expression vectors targeting the internal ribosomal entry site of the classical swine fever virus genomic RNA.

Author

Okamoto R, Ito N, Ide Y, Kitab B, Sakoda Y, and Tsukiyama-Kohara K

Subjects

Humans, Animals, Swine, RNA, Small Interfering genetics, HEK293 Cells, Genomics, Lentivirus genetics, Classical Swine Fever Virus genetics

Abstract

Background: Classical swine fever (CSF) is a fatal contagious disease affecting pigs caused by classical swine fever virus (CSFV). The disease can be transmitted by pigs and wild boars, and it is difficult to prevent and control. To obtain necessary information to establish the CSFV resistant animals in a future study, we designed lentiviral vector-delivered short hairpin RNAs (shRNAs) targeting the conserved domain III of the internal ribosomal entry site (IRES) of the CSFV genomic RNA., Results: First, we confirmed the effects of siRNAs on CSFV-IRES activity. We observed significant inhibition of CSFV-IRES activity by si42 (domain IIIa), si107 (domain IIIc), and si198 (domain IIIf) in SK-L cells and si56 (domain IIIb), si142 (domain IIId 1 ) and si198 in HEK293 cells without affecting the amount of luciferase RNA. Next, we constructed lentiviral vectors expressing shRNA based on siRNA sequences. Treatment with shRNA-expressing lentivirus was examined at 7 and 14 days post infection in SK-L cells and HEK293 cells, and CSFV-IRES was significantly suppressed at 14 days (sh42) post infection in HEK293 cells without significant cytotoxicity. Next, we examined the silencing effect of siRNA on CSFV replicon RNA and observed a significant effect by si198 after 2 days of treatment and by shRNA-expressing lentivirus (sh56, sh142, and sh198) infection after 14 days of treatment. Treatment of sh198-expressing lentivirus significantly suppressed CSFV infection at 3 days after infection., Conclusion: The IRES targeting sh198 expressing lentivirus vector can be a candidate tool for CSFV infection control., (© 2023. BioMed Central Ltd., part of Springer Nature.)

Published

2023

46. Susceptibility of common dabbling and diving duck species to clade 2.3.2.1 H5N1 high pathogenicity avian influenza virus: an experimental infection study.

Author

Soda K, Tomioka Y, Usui T, Ozaki H, Ito H, Nagai Y, Yamamoto N, Okamatsu M, Isoda N, Kajihara M, Sakoda Y, Takada A, and Ito T

Subjects

Animals, Ducks, Virulence, Influenza in Birds epidemiology, Influenza A Virus, H5N1 Subtype, Influenza A virus

Abstract

In the winter of 2010-2011, Japan experienced a large outbreak of infections caused by clade 2.3.2.1 H5N1 high pathogenicity avian influenza viruses (HPAIVs) in wild birds. Interestingly, many tufted ducks (Aythya fuligula), which are migratory diving ducks, succumbed to the infection, whereas only one infection case was reported in migratory dabbling duck species, the major natural hosts of the influenza A virus, during the outbreak. To assess whether the susceptibility of each duck species to HPAIVs was correlated with the number of cases, tufted duck and dabbling duck species (Eurasian wigeon, Mareca penelope; mallard, Anas platyrhynchos; Northern pintail, Anas acuta) were intranasally inoculated with A/Mandarin duck/Miyazaki/22M807-1/2011 (H5N1), an index clade 2.3.2.1 virus previously used for experimental infection studies in various bird species. All ducks observed for 10 days post-inoculation (dpi) mostly shed the virus via the oral route and survived. The tufted ducks shed a higher titer of the virus than the other dabbling duck species, and one of them showed apparent neurological symptoms after 7 dpi, which were accompanied by eye lesions. No clinical symptoms were observed in the dabbling ducks, although systemic infection and viremia were observed in some of them sacrificed at 3 dpi. These results suggest that the susceptibility of clade 2.3.2.1 HPAIVs might differ by duck species.

Published

2023

47. Detection of H5N1 High Pathogenicity Avian Influenza Viruses in Four Raptors and Two Geese in Japan in the Fall of 2022.

Author

Nabeshima K, Takadate Y, Soda K, Hiono T, Isoda N, Sakoda Y, Mine J, Miyazawa K, Onuma M, and Uchida Y

Subjects

Animals, Geese, Japan epidemiology, Virulence, Phylogeny, Seasons, Animals, Wild, Influenza A Virus, H5N1 Subtype, Influenza in Birds epidemiology, Raptors, Influenza A virus

Abstract

In the fall of 2022, high pathogenicity avian influenza viruses (HPAIVs) were detected from raptors and geese in Japan, a month earlier than in past years, indicating a shift in detection patterns. In this study, we conducted a phylogenetic analysis on H5N1 HPAIVs detected from six wild birds during the 2022/2023 season to determine their genetic origins. Our findings revealed that these HPAIVs belong to the G2 group within clade 2.3.4.4b, with all isolates classified into three subgroups: G2b, G2d, and G2c. The genetic background of the G2b virus (a peregrine falcon-derived strain) and G2d viruses (two raptors and two geese-derived strains) were the same as those detected in Japan in the 2021/2022 season. Since no HPAI cases were reported in Japan during the summer of 2022, it is probable that migratory birds reintroduced the G2b and G2d viruses. Conversely, the G2c virus (a raptor-derived strain) was first recognized in Japan in the fall of 2022. This strain might share a common ancestor with HPAIVs from Asia and West Siberia observed in the 2021/2022 season. The early migration of waterfowl to Japan in the fall of 2022 could have facilitated the early invasion of HPAIVs.

Published

2023

48. Generation and Efficacy of Two Chimeric Viruses Derived from GPE - Vaccine Strain as Classical Swine Fever Vaccine Candidates.

Author

Huynh LT, Isoda N, Hew LY, Ogino S, Mimura Y, Kobayashi M, Kim T, Nishi T, Fukai K, Hiono T, and Sakoda Y

Subjects

Swine, Animals, Vaccines, Marker, Antibodies, Viral, Vaccines, Attenuated, Classical Swine Fever, Viral Vaccines, Classical Swine Fever Virus genetics, Pestivirus genetics

Abstract

A previous study proved that vGPE - mainly maintains the properties of classical swine fever (CSF) virus, which is comparable to the GPE - vaccine seed and is a potentially valuable backbone for developing a CSF marker vaccine. Chimeric viruses were constructed based on an infectious cDNA clone derived from the live attenuated GPE - vaccine strain as novel CSF vaccine candidates that potentially meet the concept of differentiating infected from vaccinated animals (DIVA) by substituting the glycoprotein E rns of the GPE - vaccine strain with the corresponding region of non-CSF pestiviruses, either pronghorn antelope pestivirus (PAPeV) or Phocoena pestivirus (PhoPeV). High viral growth and genetic stability after serial passages of the chimeric viruses, namely vGPE - /PAPeV E rns and vGPE - /PhoPeV E rns , were confirmed in vitro. In vivo investigation revealed that two chimeric viruses had comparable immunogenicity and safety profiles to the vGPE - vaccine strain. Vaccination at a dose of 10 4.0 TCID 50 with either vGPE - /PAPeV E rns or vGPE - /PhoPeV E rns conferred complete protection for pigs against the CSF virus challenge in the early stage of immunization. In conclusion, the characteristics of vGPE - /PAPeV E rns and vGPE - /PhoPeV E rns affirmed their properties, as the vGPE - vaccine strain, positioning them as ideal candidates for future development of a CSF marker vaccine.

Published

2023

49. Therapeutic effects of anti-GM2 CAR-T cells expressing IL-7 and CCL19 for GM2-positive solid cancer in xenograft model.

Author

Sasaki T, Sakoda Y, Adachi K, Tokunaga Y, and Tamada K

Subjects

Mice, Animals, Humans, Interleukin-7 metabolism, Heterografts, T-Lymphocytes, Chemokine CCL19 metabolism, Receptors, Chimeric Antigen genetics, Receptors, Chimeric Antigen metabolism, Neoplasms metabolism

Abstract

Background: While chimeric antigen receptor (CAR)-T cell therapy has demonstrated excellent efficacy in hematopoietic malignancies, its clinical application in solid cancers has yet to be achieved. One of the reasons for such hurdle is a lack of suitable CAR targets in solid cancers., Methods: GM2 is one of the gangliosides, a group of glycosphingolipids with sialic acid in the glycan, and overexpressed in various types of solid cancers. In this study, by using interleukin (IL)-7 and chemokine (C-C motif) ligand 19 (CCL19)-producing human CAR-T system which we previously developed, a possibility of GM2 as a solid tumor target for CAR-T cell therapy was explored in a mouse model with human small-cell lung cancer., Results: Treatment with anti-GM2 IL-7/CCL19-producing CAR-T cells induced complete tumor regression along with an abundant T cell infiltration into the solid tumor tissue and long-term memory responses, without any detectable adverse events. In addition, as measures to control cytokine-release syndrome and neurotoxicity which could occur in association with clinical use of CAR-T cells, we incorporated Herpes simplex virus-thymidine kinase (HSV-TK), a suicide system to trigger apoptosis by administration of ganciclovir (GCV). HSV-TK-expressing anti-GM2 IL-7/CCL19-producing human CAR-T cells were efficiently eliminated by GCV administration in vivo., Conclusions: Our study revealed the promising therapeutic efficacy of anti-GM2 IL-7/CCL19-producing human CAR-T cells with an enhanced safety for clinical application in the treatment of patients with GM2-positive solid cancers., (© 2023 The Authors. Cancer Medicine published by John Wiley & Sons Ltd.)

Published

2023

50. Novel technologies for improving the safety and efficacy of CAR-T cell therapy.

Author

Ohta K, Sakoda Y, and Tamada K

Subjects

Humans, Receptors, Antigen, T-Cell, Immunotherapy, Adoptive adverse effects, Tumor Microenvironment, Cell- and Tissue-Based Therapy, Receptors, Chimeric Antigen, Neoplasms therapy, Hematologic Neoplasms drug therapy

Abstract

Chimeric antigen receptor-T (CAR-T) cell therapy has shown significant therapeutic efficacy in the treatment of hematological B-cell malignancies. However, the efficacy of CAR-T cell therapy against solid tumors is limited due to the heterogeneity of tumor antigens and the immunosuppressive tumor microenvironment. Therefore, there is strong demand for novel technologies to improve the efficacy of CAR-T cell therapy. In addition, as CAR-T cells often cause severe side effects, systems to control the activity of CAR-T cells so as to avoid or lessen the occurrence and intensity of these side effects are needed. Here, we describe recently emerging approaches to enhance and/or regulate CAR-T cell functions. These approaches have led to the development of CAR-T therapies with improved efficacy and safety, which are expected to be clinically applied to a variety of cancer types in combination with other therapies, such as immune checkpoint inhibitors, chemotherapy, molecular targeted drugs, and radiation therapy., (© 2022. Japanese Society of Hematology.)

Published

2023