Your search keyword '"Kikuchi, Mihoko"' showing total 7 results

1. IL-17A, a possible biomarker for the evaluation of treatment response in Trypanosoma cruzi infected children: A 12-months follow-up study in Bolivia.

Author

Vásquez Velásquez, Clara, Russomando, Graciela, Espínola, Emilio E., Sanchez, Zunilda, Mochizuki, Kota, Roca, Yelin, Revollo, Jimmy, Guzman, Angelica, Quiroga, Benjamín, Rios Morgan, Susana, Vargas Ortiz, Roberto, Zambrana Ortega, Alberto, Espinoza, Eida, Nishizawa, Juan Eiki, Kamel, Mohamed Gomaa, Kikuchi, Mihoko, Mizukami, Shusaku, Na-Bangchang, Kesara, Tien Huy, Nguyen, and Hirayama, Kenji

Subjects

TRYPANOSOMA cruzi, CHAGAS' disease, DIAGNOSTIC use of polymerase chain reaction, DEVELOPMENTAL biology, CHILDREN

Abstract

Background: The National Program for Chagas disease was implemented in Bolivia in 2006, and it greatly decreased the number of infections through vector control. Subsequently, a treatment regimen of benznidazole (BNZ) was started in seropositive school-age children living in certified vector control areas. Methods and findings: We conducted a 12-month follow-up study and seven blood samples were taken during and after the treatment. Serology, conventional diagnostic PCR (cPCR) and quantitative Real-time PCR (qPCR) were performed. Plasma Th1/Th2/Th17 cytokines levels were also determined. Approximately 73 of 103 seropositive children complied with BNZ, with three interruptions due to side effects. To evaluate each individual’s treatment efficacy, the cPCR and qPCR values during the final 6 months of the follow-up period were observed. Among 57 children who completed follow-up, 6 individuals (11%) showed both cPCR(+) and qPCR(+) (non reactive), 24 (42%) cPCR(-) but qPCR(+) (ambiguous) and 27 (47%) cPCR(-) and qPCR(-) (reactive). Within 14 Th1/Th2/Th17 cytokines, IL-17A showed significantly higher levels in seropositive children before the treatment compared to age-matched seronegative children and significantly decreased to the normal level one-year after. Moreover, throughout the follow-up study, IL-17A levels were positively co-related to parasite counts detected by qPCR. At the 12 months’ time point, IL-17A levels of non-reactive subjects were significantly higher than either those of reactive or ambiguous subjects suggesting that IL-17A might be useful to determine the reactivity to BNZ treatment. Conclusions: Plasma levels of IL-17A might be a bio-marker for detecting persistent infection of T. cruzi and its chronic inflammation. [ABSTRACT FROM AUTHOR]

Published

2019

2. Spatial distribution and risk factors of Schistosoma haematobium and hookworm infections among schoolchildren in Kwale, Kenya.

Author

Chadeka, Evans Asena, Nagi, Sachiyo, Sunahara, Toshihiko, Cheruiyot, Ngetich Benard, Bahati, Felix, Ozeki, Yuriko, Inoue, Manabu, Osada-Oka, Mayuko, Okabe, Mayuko, Hirayama, Yukio, Changoma, Mwatasa, Adachi, Keishi, Mwende, Faith, Kikuchi, Mihoko, Nakamura, Risa, Kalenda, Yombo Dan Justin, Kaneko, Satoshi, Hirayama, Kenji, Shimada, Masaaki, and Ichinose, Yoshio

Subjects

SPATIAL distribution (Quantum optics), SCHISTOSOMIASIS, SCHISTOSOMIASIS treatment, HOOKWORM disease, SOCIAL status, GENETICS, PREVENTION

Abstract

Background: Large-scale schistosomiasis control programs are implemented in regions with diverse social and economic environments. A key epidemiological feature of schistosomiasis is its small-scale heterogeneity. Locally profiling disease dynamics including risk factors associated with its transmission is essential for designing appropriate control programs. To determine spatial distribution of schistosomiasis and its drivers, we examined schoolchildren in Kwale, Kenya. Methodology/Principal findings: We conducted a cross-sectional study of 368 schoolchildren from six primary schools. Soil-transmitted helminths and Schistosoma mansoni eggs in stool were evaluated by the Kato-Katz method. We measured the intensity of Schistosoma haematobium infection by urine filtration. The geometrical mean intensity of S. haematobium was 3.1 eggs/10 ml urine (school range, 1.4–9.2). The hookworm geometric mean intensity was 3.2 eggs/g feces (school range, 0–17.4). Heterogeneity in the intensity of S. haematobium and hookworm infections was evident in the study area. To identify factors associated with the intensity of helminth infections, we utilized negative binomial generalized linear mixed models. The intensity of S. haematobium infection was associated with religion and socioeconomic status (SES), while that of hookworm infection was related to SES, sex, distance to river and history of anthelmintic treatment. Conclusions/Significance: Both S. haematobium and hookworm infections showed micro-geographical heterogeneities in this Kwale community. To confirm and explain our observation of high S. haematobium risk among Muslims, further extensive investigations are necessary. The observed small scale clustering of the S. haematobium and hookworm infections might imply less uniform strategies even at finer scale for efficient utilization of limited resources. [ABSTRACT FROM AUTHOR]

Published

2017

3. HLA-A*33:01 as Protective Allele for Severe Dengue in a Population of Filipino Children.

Author

Mercado, Edelwisa Segubre, Espino, Fe Esperanza, Perez, Ma. Lucila M., Bilar, Josie M., Bajaro, Jemimah Dawn P., Huy, Nguyen Tien, Baello, Benilda Q, Kikuchi, Mihoko, and Hirayama, Kenji

Subjects

HLA histocompatibility antigens, ALLELES, JUVENILE diseases, DENGUE, COMPARATIVE studies, PATIENTS

Abstract

Dengue virus infection is a leading cause of morbidity among children in the Philippines in recent years. In order to investigate the association of HLA Class I and II alleles and dengue disease severity in a cohort of Filipino children, we performed a case control study in 2 hospitals in Metro Manila from June 2008 to December 2009. A total of 250 laboratory confirmed dengue patients and 300 healthy individuals aged 5 to 15 years old were typed for HLA-A, B and DRB1 alleles. The frequency of HLA-A*33:01 was significantly decreased in severe dengue (DHF/ DSS; Pc = 0.0016)) and DSS (Pc = 0.0032) compared to the background population. These findings support a previous study that this allele may confer protection against the severe form of dengue and provide the first evidence of HLA association with dengue in the Philippines. Future studies should be directed in investigating the possible mechanisms of protection. [ABSTRACT FROM AUTHOR]

Published

2015

4. Characterization of a Gene Family Encoding SEA (Sea-urchin Sperm Protein, Enterokinase and Agrin)-Domain Proteins with Lectin-Like and Heme-Binding Properties from Schistosoma japonicum.

Author

Mbanefo, Evaristus Chibunna, Kikuchi, Mihoko, Huy, Nguyen Tien, Shuaibu, Mohammed Nasir, Cherif, Mahamoud Sama, Yu, Chuanxin, Wakao, Masahiro, Suda, Yasuo, and Hirayama, Kenji

Subjects

*TETRAPYRROLES, *PORPHYRINS, *SCHISTOSOMA, *SCHISTOSOMATIDAE, *SCHISTOSOMA japonicum, *SERINE proteinases

Abstract

Background: We previously identified a novel gene family dispersed in the genome of Schistosoma japonicum by retrotransposon-mediated gene duplication mechanism. Although many transcripts were identified, no homolog was readily identifiable from sequence information. Methodology/Principal Findings: Here, we utilized structural homology modeling and biochemical methods to identify remote homologs, and characterized the gene products as SEA (sea-urchin sperm protein, enterokinase and agrin)-domain containing proteins. A common extracellular domain in this family was structurally similar to SEA-domain. SEA-domain is primarily a structural domain, known to assist or regulate binding to glycans. Recombinant proteins from three members of this gene family specifically interacted with glycosaminoglycans with high affinity, with potential implication in ligand acquisition and immune evasion. Similar approach was used to identify a heme-binding site on the SEA-domain. The heme-binding mode showed heme molecule inserted into a hydrophobic pocket, with heme iron putatively coordinated to two histidine axial ligands. Heme-binding properties were confirmed using biochemical assays and UV-visible absorption spectroscopy, which showed high affinity heme-binding (KD = 1.605×10−6 M) and cognate spectroscopic attributes of hexa-coordinated heme iron. The native proteins were oligomers, antigenic, and are localized on adult worm teguments and gastrodermis; major host-parasite interfaces and site for heme detoxification and acquisition. Conclusions: The results suggest potential role, at least in the nucleation step of heme crystallization (hemozoin formation), and as receptors for heme uptake. Survival strategies exploited by parasites, including heme homeostasis mechanism in hemoparasites, are paramount for successful parasitism. Thus, assessing prospects for application in disease intervention is warranted. [ABSTRACT FROM AUTHOR]

Published

2014

5. Characterization of a Gene Family Encoding SEA (Sea-urchin Sperm Protein, Enterokinase and Agrin)-Domain Proteins with Lectin-Like and Heme-Binding Properties from Schistosoma japonicum.

Author

Mbanefo, Evaristus Chibunna, Kikuchi, Mihoko, Huy, Nguyen Tien, Shuaibu, Mohammed Nasir, Cherif, Mahamoud Sama, Yu, Chuanxin, Wakao, Masahiro, Suda, Yasuo, and Hirayama, Kenji

Subjects

TETRAPYRROLES, PORPHYRINS, SCHISTOSOMA, SCHISTOSOMATIDAE, SCHISTOSOMA japonicum, SERINE proteinases

Abstract

Background: We previously identified a novel gene family dispersed in the genome of Schistosoma japonicum by retrotransposon-mediated gene duplication mechanism. Although many transcripts were identified, no homolog was readily identifiable from sequence information. Methodology/Principal Findings: Here, we utilized structural homology modeling and biochemical methods to identify remote homologs, and characterized the gene products as SEA (sea-urchin sperm protein, enterokinase and agrin)-domain containing proteins. A common extracellular domain in this family was structurally similar to SEA-domain. SEA-domain is primarily a structural domain, known to assist or regulate binding to glycans. Recombinant proteins from three members of this gene family specifically interacted with glycosaminoglycans with high affinity, with potential implication in ligand acquisition and immune evasion. Similar approach was used to identify a heme-binding site on the SEA-domain. The heme-binding mode showed heme molecule inserted into a hydrophobic pocket, with heme iron putatively coordinated to two histidine axial ligands. Heme-binding properties were confirmed using biochemical assays and UV-visible absorption spectroscopy, which showed high affinity heme-binding (KD = 1.605×10−6 M) and cognate spectroscopic attributes of hexa-coordinated heme iron. The native proteins were oligomers, antigenic, and are localized on adult worm teguments and gastrodermis; major host-parasite interfaces and site for heme detoxification and acquisition. Conclusions: The results suggest potential role, at least in the nucleation step of heme crystallization (hemozoin formation), and as receptors for heme uptake. Survival strategies exploited by parasites, including heme homeostasis mechanism in hemoparasites, are paramount for successful parasitism. Thus, assessing prospects for application in disease intervention is warranted. [ABSTRACT FROM AUTHOR]

Published

2014

6. Factors Associated with Dengue Shock Syndrome: A Systematic Review and Meta-Analysis.

Author

Huy, Nguyen Tien, Van Giang, Tran, Thuy, Dinh Ha Duy, Kikuchi, Mihoko, Hien, Tran Tinh, Zamora, Javier, and Hirayama, Kenji

Subjects

DENGUE hemorrhagic fever, META-analysis, EPIDEMIOLOGY, HETEROGENEITY, HEMATOCRIT, THROMBOCYTOPENIA, RANDOM effects model

Abstract

Background: The pathogenesis of dengue shock syndrome (DSS, grade 3 and 4) is not yet completely understood. Several factors are reportedly associated with DSS, a more severe form of dengue infection that reportedly causes 50 times higher mortality compared to that of dengue patients without DSS. However, the results from these reports remain inconclusive. To better understand the epidemiology, clinical manifestation, and pathogenesis of DSS for development of new therapy, we systematically reviewed and performed a meta-analysis of relevant studies that reported factors in both DSS and dengue hemorrhagic fever (DHF, grade 1 and 2) patients. Methods and Findings: PubMed, EMBASE, Scopus, Google Scholar, Dengue Bulletin, Cochrane Library, Virtual Health Library, and a manual search of reference lists of articles published before September 2010 were used to retrieve relevant studies. A meta-analysis using fixed- or random-effects models was used to calculate pooled odds ratios (OR) or event rate with corresponding 95% confidence intervals. Assessment of heterogeneity and publication bias, meta-regression analysis, subgroup analysis, sensitivity analysis, and analysis of factor-specific relationships were further performed. There were 198 studies constituting 203 data sets that met our eligibility criteria. Our meta-regression analysis showed a sustained reduction of DSS/dengue hemorrhagic fever (DHF) ratio over a period of 40 years in Southeast Asia, especially in Thailand. The meta-analysis revealed that age, female sex, neurological signs, nausea/vomiting, abdominal pain, gastrointestinal bleeding, hemoconcentration, ascites, pleural effusion, hypoalbuminemia, hypoproteinemia, hepatomegaly, levels of alanine transaminase and aspartate transaminase, thrombocytopenia, prothrombin time, activated partial thromboplastin time, fibrinogen level, primary/secondary infection, and dengue virus serotype-2 were significantly associated with DSS when pooling all original relevant studies. Conclusions: The results improve our knowledge of the pathogenesis of DSS by identifying the association between the epidemiology, clinical signs, and biomarkers involved in DSS. [ABSTRACT FROM AUTHOR]

Published

2013

7. CD19(+) B Cells Confer Protection against Experimental Cerebral Malaria in Semi-Immune Rodent Model

Author

Bao, Lam Quoc, Huy, Nguyen Tien, Kikuchi, Mihoko, Yanagi, Tetsuo, Senba, Masachika, Shuaibu, Mohammed Nasir, Honma, Kiri, Yui, Katsuyuki, and Hirayama, Kenji

Subjects

B cells, CEREBRAL malaria, JUVENILE diseases, INTERLEUKIN-10, PLASMODIUM berghei, LABORATORY mice, THERAPEUTICS

Abstract

In African endemic area, adults are less vulnerable to cerebral malaria than children probably because of acquired partial immunity or semi-immune status. Here, we developed an experimental cerebral malaria (ECM) model for semi-immune mice. C57BL/6 (B6) mice underwent one, two and three cycles of infection and radical treatment (1-cure, 2-cure and 3-cure, respectively) before being finally challenged with 104Plasmodium berghei ANKA without treatment. Our results showed that 100% of naïve (0-cure), 67% of 1-cure, 37% of 2-cure and none of 3-cure mice succumbed to ECM within 10 days post challenge infection. In the protected 3-cure mice, significantly higher levels of plasma IL-10 and lower levels of IFN-γ than the others on day 7 post challenge infection were observed. Major increased lymphocyte subset of IL-10 positive cells in 3-cure mice was CD5(−)CD19(+) B cells. Passive transfer of splenic CD19(+) cells from 3-cure mice protected naïve mice from ECM. Additionally, aged 3-cure mice were also protected from ECM 12 and 20 months after the last challenge infection. In conclusion, mice became completely resistant to ECM after three exposures to malaria. CD19(+) B cells are determinants in protective mechanism of semi-immune mice against ECM possibly via modulatory IL-10 for pathogenic IFN-γ production. [ABSTRACT FROM AUTHOR]

Published

2013