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3. Molecular Cloning and Characterization of Taurocyamine Kinase from Clonorchis sinensis: A Candidate Chemotherapeutic Target.

Author

Xiao, Jing-ying, Lee, Ji-Yun, Tokuhiro, Shinji, Nagataki, Mitsuru, Jarilla, Blanca R., Nomura, Haruka, Kim, Tae Im, Hong, Sung-Jong, and Agatsuma, Takeshi

Subjects
CLONORCHIS sinensis, MOLECULAR cloning, DRUG development, CANCER chemotherapy, GENITALIA
Abstract

Background: Adult Clonorchis sinensis lives in the bile duct and causes endemic clonorchiasis in East Asian countries. Phosphagen kinases (PK) constitute a highly conserved family of enzymes, which play a role in ATP buffering in cells, and are potential targets for chemotherapeutic agents, since variants of PK are found only in invertebrate animals, including helminthic parasites. This work is conducted to characterize a PK from C. sinensis and to address further investigation for future drug development. Methology/Principal findings: A cDNA clone encoding a putative polypeptide of 717 amino acids was retrieved from a C. sinensis transcriptome. This polypeptide was homologous to taurocyamine kinase (TK) of the invertebrate animals and consisted of two contiguous domains. C. sinensis TK (CsTK) gene was reported and found consist of 13 exons intercalated with 12 introns. This suggested an evolutionary pathway originating from an arginine kinase gene group, and distinguished annelid TK from the general CK phylogenetic group. CsTK was found not to have a homologous counterpart in sequences analysis of its mammalian hosts from public databases. Individual domains of CsTK, as well as the whole two-domain enzyme, showed enzymatic activity and specificity toward taurocyamine substrate. Of the CsTK residues, R58, I60 and Y84 of domain 1, and H60, I63 and Y87 of domain 2 were found to participate in binding taurocyamine. CsTK expression was distributed in locomotive and reproductive organs of adult C. sinensis. Developmentally, CsTK was stably expressed in both the adult and metacercariae stages. Recombinant CsTK protein was found to have low sensitivity and specificity toward C. sinensis and platyhelminth-infected human sera on ELISA. Conclusion: CsTK is a promising anti-C. sinensis drug target since the enzyme is found only in the C. sinensis and has a substrate specificity for taurocyamine, which is different from its mammalian counterpart, creatine. Author Summary: The food-borne clonorchiasis imposes public health problems on inhabitants in endemic areas. Praziquantel has been employed as an efficacious anthelminthic in large-scale campaigns as well as for individual treatment of Clonorchis sinensis human infections. Although praziquantel continues to have good efficacy, new drug development for this parasite has been recognized as a crucial issue to be investigated intensively. Clonorchis sinensis adults generate energy through glycolysis, actively utilizing exogenous glucose, and produce a large amount of eggs each day. Taurocyamine kinase (CsTK) is distributed abundantly in the locomotive and reproductive organs, and is an important enzyme in energy generation and homeostasis in adult C. sinensis. Enzymes of the glycolytic pathway are also expressed abundantly in these organs and in tegument, implying these organs play central roles which are essential for survival and reproduction of C. sinensis. The TK enzymes, including CsTK, are found only among invertebrate organisms and have substrate specificity for taurocyamine, which are significantly different from phosphagen kinases of vertebrate animals. With these molecular biological, enzymatic, and evolutionary characteristics, we propose here that CsTK could be a target for development of chemotherapeutic agents against C. sinensis and be a biomolecular model for other human-infecting trematodes. [ABSTRACT FROM AUTHOR]

Published
2013
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4. Molecular Cloning and Characterization of Taurocyamine Kinase from Clonorchis sinensis: A Candidate Chemotherapeutic Target.

Author

Xiao, Jing-ying, Lee, Ji-Yun, Tokuhiro, Shinji, Nagataki, Mitsuru, Jarilla, Blanca R., Nomura, Haruka, Kim, Tae Im, Hong, Sung-Jong, and Agatsuma, Takeshi

Subjects
MOLECULAR cloning, CLONORCHIS sinensis, CLONORCHIASIS, BILE duct diseases, PHYSIOLOGICAL effects of enzymes, ANTISENSE DNA
Abstract

Background: Adult Clonorchis sinensis lives in the bile duct and causes endemic clonorchiasis in East Asian countries. Phosphagen kinases (PK) constitute a highly conserved family of enzymes, which play a role in ATP buffering in cells, and are potential targets for chemotherapeutic agents, since variants of PK are found only in invertebrate animals, including helminthic parasites. This work is conducted to characterize a PK from C. sinensis and to address further investigation for future drug development. Methology/Principal findings: A cDNA clone encoding a putative polypeptide of 717 amino acids was retrieved from a C. sinensis transcriptome. This polypeptide was homologous to taurocyamine kinase (TK) of the invertebrate animals and consisted of two contiguous domains. C. sinensis TK (CsTK) gene was reported and found consist of 13 exons intercalated with 12 introns. This suggested an evolutionary pathway originating from an arginine kinase gene group, and distinguished annelid TK from the general CK phylogenetic group. CsTK was found not to have a homologous counterpart in sequences analysis of its mammalian hosts from public databases. Individual domains of CsTK, as well as the whole two-domain enzyme, showed enzymatic activity and specificity toward taurocyamine substrate. Of the CsTK residues, R58, I60 and Y84 of domain 1, and H60, I63 and Y87 of domain 2 were found to participate in binding taurocyamine. CsTK expression was distributed in locomotive and reproductive organs of adult C. sinensis. Developmentally, CsTK was stably expressed in both the adult and metacercariae stages. Recombinant CsTK protein was found to have low sensitivity and specificity toward C. sinensis and platyhelminth-infected human sera on ELISA. Conclusion: CsTK is a promising anti-C. sinensis drug target since the enzyme is found only in the C. sinensis and has a substrate specificity for taurocyamine, which is different from its mammalian counterpart, creatine. [ABSTRACT FROM AUTHOR]

Published
2013
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5. Effect of Sophy β-Glucan on Immunity and Growth Performance in Broiler Chicken.

Author

RAJAPAKSE, Jayanthe R. P. V., BUDDHIKA, M. D. P., NAGATAKI, Mitsuru, NOMURA, Haruka, WATANABE, Yoshiya, IKEUE, Yasunori, and AGATSUMA, Takeshi

Subjects
BROILER chickens, IMMUNITY, POULTRY growth, IMMUNOGLOBULINS, GLUCANS, WATER, BODY weight
Abstract

The article presents the results of a study on the influence of Sophy ß-glucan on the growth and immunity development in broiler chicken. According to the authors, broiler chickens treated with one percent of ß-glucan and ad libitum with water resulted an increase in the mean body weight and the mean antibody titres, illustrating the presence of immue stimulating effect of ß-glucan. They add that the immuno-modularity role of ß-glucan in partitioning nutrients towards growth could be the reason for the improved growth of broiler chicken.

Published
2010
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6. Making the Japanese Empire: Nationality and Family Register in Taiwan, 1871-1899.

Author

Nomura, Haruka

Subjects
*CITIZENSHIP, *VITAL records (Births, deaths, etc.), *IMPERIALISM, *SOVEREIGNTY, HISTORY of Taiwan -- To 1895
Abstract

This paper aims to reconnect the history of modern Japan with that of Japan's colonies by examining debates over the legal inclusion and exclusion of colonial Taiwan in 1899. It examines why and how an inconsistent legal structure evolved within the Japanese Empire. I argue that the creation of the Japanese nation was intertwined with the empire, and that this can be seen in the discriminatory deployment of the Family Register and Nationality Laws. Japan included Taiwan within the scope of the Nationality Law to achieve full sovereignty over its territory but also excluded the colonised people of Taiwan from the family register system to deny them citizenship. The rapid reconfiguration of the idea of 'Japan' under the strong influence of the West added significant ambivalence to this process, and thus to the making of the nation-empire. [ABSTRACT FROM AUTHOR]

Published
2010
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7. Aureobasidium-Derived Soluble Branched (1,3-1,6) α-Glucan (Sophy α-glucan) Enhances Natural Killer Activity in Leishmania amazonensis-Infected Mice.

Author

Yatawara, Lalani, Wickramasinghe, Susiji, Nagataki, Mitsuru, Takamoto, Misa, Nomura, Haruka, Ikeue, Yasunori, Watanabe, Yoshiya, and Agatsum, Takeshi

Subjects
GLUCANS, KILLER cells, INTERFERONS, INTERLEUKIN-4, CELLULAR immunity, LEISHMANIA, LABORATORY mice
Abstract

The β-glucans derived from yeast cell walls have been reported for having many immunomodulatory activities in vivo and in vitro. In this study, Aureobasidium-derived soluble branched (1,3-1,6) β-glucan (Sophy β-glucan) was checked for natural killer (NK) activity and for the production of IFN-γ and IL-4 in Leishmania amazonensis infection. The main experiment was performed with a group of female C57BL/6 and BALB/c mice, orally supplemented with 5% of Sophy β-glucan and infected with promastogotes of L. amazonensis (1 x 107) into the footpad. Increase in the footpad thickness with time was observed in BALB/c mice in spite of the oral Sophy b-glucan supplement, but it was less in C57BL/6 mice. The difference in overall mean footpad thickness between 'infection only' versus 'infection + glucan' groups was statistically significant (P < 0.001). High NK activity in C57BL/6 than BALB/c mice was observed in 'glucan only' group compared to the control group and also in 'infection + glucan' group compared to 'infection only' group. The difference in the NK activity among these groups was significant (P < 0.05). The IFN-γ level increased at weeks 7 and 8 post-infection in C57BL/6 mice and was significantly high in 'infection + glucan' group compared to the 'infection only' group (P < 0.05). IL-4 levels did not increase up to detectable levels throughout the study. The results led a conclusion that Sophy β-glucan enhances NK activity and cellular immunity in L. amazonensis-infected mice. [ABSTRACT FROM AUTHOR]

Published
2009
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8. CDK5/p35-Dependent Microtubule Reorganization Contributes to Homeostatic Shortening of the Axon Initial Segment.

Author

Jahan I, Adachi R, Egawa R, Nomura H, and Kuba H

Subjects
Animals, Female, Male, Chickens, Microtubules metabolism, Neurons metabolism, Phosphorylation, Axon Initial Segment metabolism, Cyclin-Dependent Kinase 5 metabolism
Abstract

The structural plasticity of the axon initial segment (AIS) contributes to the homeostatic control of activity and optimizes the function of neural circuits; however, the underlying mechanisms are not fully understood. In this study, we prepared a slice culture containing nucleus magnocellularis from chickens of both sexes that reproduces most features of AIS plasticity in vivo , regarding its effects on characteristics of AIS and cell-type specificity, and revealed that microtubule reorganization via activation of CDK5 underlies plasticity. Treating the culture with a high-K + medium shortened the AIS and reduced sodium current and membrane excitability, specifically in neurons tuned to high-frequency sound, creating a tonotopic difference in AIS length in the nucleus. Pharmacological analyses revealed that this AIS shortening was driven by multiple Ca 2+ pathways and subsequent signaling molecules that converge on CDK5 via the activation of ERK1/2. AIS shortening was suppressed by overexpression of dominant-negative CDK5, whereas it was facilitated by the overexpression of p35, an activator of CDK5. Notably, p35(T138A), a phosphorylation-inactive mutant of p35, did not shorten the AIS. Moreover, microtubule stabilizers occluded AIS shortening during the p35 overexpression, indicating that CDK5/p35 mediated AIS shortening by promoting disassembly of microtubules at distal AIS. This study highlights the importance of microtubule reorganization and regulation of CDK5 activity in structural AIS plasticity and the tuning of AIS characteristics in neurons. SIGNIFICANCE STATEMENT The structural plasticity of AIS has a strong impact on the output of neurons and plays a fundamental role in the physiology and pathology of the brain. However, the mechanisms linking neuronal activity to structural changes in AIS are not well understood. In this study, we prepared an organotypic culture of avian auditory brainstem, reproducing most AIS plasticity features in vivo , and we revealed that activity-dependent AIS shortening occurs through the disassembly of microtubules at distal AIS via activation of CDK5/p35 signals. This study emphasizes the importance of microtubule reorganization and regulation of CDK5 activity in structural AIS plasticity and tonotopic differentiation of AIS structures in the brainstem auditory circuit., (Copyright © 2023 the authors.)

Published
2023
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9. The adjuvant effect of Sophy β-glucan to the antibody response in poultry immunized by the avian influenza A H5N1 and H5N2 vaccines.

Author

Le T, Le T, Doan TH, Quyen D, Le KX, Pham V, Nagataki M, Nomura H, Ikeue Y, Watanabe Y, and Agatsuma T

Subjects
Animals, Ascomycota chemistry, Ascomycota metabolism, Chickens, Ducks, Hemagglutination Inhibition Tests, Immunization, Influenza A Virus, H5N1 Subtype physiology, Influenza A Virus, H5N2 Subtype physiology, Influenza Vaccines administration & dosage, Influenza in Birds prevention & control, Influenza in Birds virology, Poultry Diseases prevention & control, Poultry Diseases virology, Vaccines, Inactivated administration & dosage, Vaccines, Inactivated immunology, beta-Glucans administration & dosage, Adjuvants, Immunologic administration & dosage, Antibody Formation, Influenza A Virus, H5N1 Subtype immunology, Influenza A Virus, H5N2 Subtype immunology, Influenza Vaccines immunology, Influenza in Birds immunology, Poultry Diseases immunology, beta-Glucans immunology
Abstract

Avian influenza virus vaccines produced in oil-emulsified inactivated form with antigen content of at least 160 hemagglutinin units (HAU) induced immunity in birds. However, in addition to enhancing the effect of the adjuvant(s), other additional supplemented biological compounds included in inactivated vaccines could produce higher levels of antibody. We examined in chickens, Vietnamese ducks, and muscovy ducks the adjuvant effect of Sophy β-glucan (SBG), a β-1,3-1,6 glucan produced by the black yeast Aureobasidium pollulans strain AF0-202, when administered with an avian influenza H5 subtype vaccine. In Experiment 1, 40 chickens (ISA Brown hybrid), allocated to four groups of ten each, were immunized with Oil-H5N1(VN), Oil-H5N1(CN), Oil-H5N2(CN), and saline (control group), respectively. In Experiment 2, chickens (ISA Brown hybrid), muscovy ducks (French hybrid), and Vietnamese ducks (indigenous Vietnamese) were used to further assess the effect of SBG on immunogenicity of the Oil-H5N1(VN) Vietnamese vaccine. ELISA and hemagglutination inhibition (HI) assays were used to assess the antibody response. The H5 subtype vaccines initiated significantly higher immune responses in the animals dosed with SBG, with 1.0-1.5 log2 higher HI titers and 10-20% ELISA seroconversion, compared with those not dosed with β-glucan. Notably, some of the animals dosed with SBG induced HI titers higher than 9.0 log2 following boosting immunization. Taken together, our serial studies indicated that SBG is a potential effector, such as enhancing the immune response to the H5 vaccines tested.

Published
2011

10. Aureobasidium-derived soluble branched (1,3-1,6) beta-glucan (Sophy beta-glucan) enhances natural killer activity in Leishmania amazonensis-infected mice.

Author

Yatawara L, Wickramasinghe S, Nagataki M, Takamoto M, Nomura H, Ikeue Y, Watanabe Y, and Agatsuma T

Subjects
Administration, Oral, Animals, Cytotoxicity Tests, Immunologic, Female, Foot pathology, Glucans administration & dosage, Glucans pharmacology, Immunologic Factors administration & dosage, Immunologic Factors pharmacology, Interferon-gamma biosynthesis, Interleukin-4 biosynthesis, Killer Cells, Natural drug effects, Leishmaniasis, Cutaneous immunology, Leishmaniasis, Cutaneous pathology, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Severity of Illness Index, Time Factors, Ascomycota chemistry, Glucans isolation & purification, Glucans therapeutic use, Immunologic Factors isolation & purification, Immunologic Factors therapeutic use, Killer Cells, Natural immunology, Leishmania mexicana immunology, Leishmaniasis, Cutaneous drug therapy
Abstract

The beta-glucans derived from yeast cell walls have been reported for having many immunomodulatory activities in vivo and in vitro. In this study, Aureobasidium-derived soluble branched (1,3-1,6) beta-glucan (Sophy beta-glucan) was checked for natural killer (NK) activity and for the production of IFN-gamma and IL-4 in Leishmania amazonensis infection. The main experiment was performed with a group of female C57BL/6 and BALB/c mice, orally supplemented with 5% of Sophy beta-glucan and infected with promastogotes of L. amazonensis (1 x 10(7)) into the footpad. Increase in the footpad thickness with time was observed in BALB/c mice in spite of the oral Sophy beta-glucan supplement, but it was less in C57BL/6 mice. The difference in overall mean footpad thickness between 'infection only' versus 'infection + glucan' groups was statistically significant (P < 0.001). High NK activity in C57BL/6 than BALB/c mice was observed in 'glucan only' group compared to the control group and also in 'infection + glucan' group compared to 'infection only' group. The difference in the NK activity among these groups was significant (P < 0.05). The IFN-gamma level increased at weeks 7 and 8 post-infection in C57BL/6 mice and was significantly high in 'infection + glucan' group compared to the 'infection only' group (P < 0.05). IL-4 levels did not increase up to detectable levels throughout the study. The results led a conclusion that Sophy beta-glucan enhances NK activity and cellular immunity in L. amazonensis-infected mice.

Published
2009
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