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Dive into the research topics where Yukie Y. Kikuti is active.

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Featured researches published by Yukie Y. Kikuti.


Environmental Health and Preventive Medicine | 2012

Lack of an association human dioxin detoxification gene polymorphisms with endometriosis in Japanese women: results of a pilot study

Yasunari Matsuzaka; Yukie Y. Kikuti; Ken-ichi Goya; Takahiro Suzuki; Li-yi Cai; Akira Oka; Hidetoshi Inoko; Jerzy K. Kulski; Shun-ichiro Izumi; Minoru Kimura

ObjectivesEndometriosis is a chronic disease caused by the presence of endometrial tissue in ectopic locations outside the uterus. Chronic exposure to the environmental pollutant dioxin has been correlated with an increased incidence in the development of endometriosis in non-human primates. We have therefore examined whether there is an association between the polymorphisms of ten dioxin detoxification genes and endometriosis in Japanese women.MethodsThis was a pilot study in which 100 patients with endometriosis and 143 controls were enrolled. The prevalence of five microsatellite and 28 single nucleotide polymorphism markers within ten dioxin detoxification genes (AhR, AHRR, ARNT, CYP1A1, CYP2E1, EPHX1, GSTM1, GSTP1, GSTT1, NAT2) was examined.ResultsTaking into account that this analysis was a preliminary study due to its small sample size and genetic power, the results did not show any statistically significant difference between the cases and controls for any of the allele and genotype frequency distributions examined. In addition, no significant associations between the allele/genotype of all polymorphisms and the stage (I–II or III–IV) of endometriosis were observed.ConclusionBased on the findings of this pilot study, we conclude the polymorphisms of the ten dioxin detoxification genes analyzed did not contribute to the etiology of endometriosis among our patients.


Environmental Health and Preventive Medicine | 2012

Failure to detect significant association between estrogen receptor-alpha gene polymorphisms and endometriosis in Japanese women

Yasunari Matsuzaka; Yukie Y. Kikuti; Shun-ichiro Izumi; Ken-ichi Goya; Takahiro Suzuki; Li-yi Cai; Akira Oka; Hidetoshi Inoko; Jerzy K. Kulski; Minoru Kimura

ObjectivesThe aim of the study was to test whether estrogen receptor 1 (ESR1) gene polymorphisms are correlated with the risk of the development of endometriosis in Japanese women, as a preliminary study.MethodsTo compare allelic frequencies and genotype distributions, a case-control study of 100 affected women and 143 women with no evidence of disease was performed using 10 microsatellite repeat markers and 66 single-nucleotide polymorphisms (SNPs) in the ESR1 gene region.ResultsAlthough our results might be insufficient to detect genetic susceptibility, owing to the small sample size and low genetic power, statistical analysis of the differences in allelic frequency between the cases and controls at each microsatellite locus demonstrated that no microsatellite locus in the ESR1 gene displayed a significant association with the disease when multiple testing was taken into account. Also, there were no statistically significant differences in the SNP allele frequencies and genotypes between the cases and controls when multiple testing was taken into account.ConclusionThe findings in our pilot study suggest that ESR1 polymorphisms do not contribute to endometriosis susceptibility.


Tissue Antigens | 2010

Mapping of susceptibility locus for endometriosis within the HLA region using microsatellite markers in Japanese women

Yasunari Matsuzaka; Yukie Y. Kikuti; Shun-ichiro Izumi; Takahiro Suzuki; Li-yi Cai; Ken-ichi Goya; Hidetoshi Inoko; T. Makino; Jerzy K. Kulski; Minoru Kimura

Endometriosis is a female disorder characterized by the presence of uterine endometrial tissue in ectopic loci. Previous studies reported a higher prevalence of particular human leukocyte antigen (HLA) in endometriosis. In order to confirm the association between endometriosis and the HLA region, 15 polymorphic microsatellite markers distributed in the HLA class II to class III region were subjected to association analysis by polymerase chain reaction (PCR)-based DNA typing of 89 patients and 136 healthy controls. Statistical analysis of the allelic frequency at each microsatellite locus showed that there were no statistically significant differences in the allele frequency distributions between the cases and controls. This finding suggests that the etiology of endometriosis does not involve the HLA class II genomic region and a portion of class III genomic region in the Japanese population.


Journal of Clinical and Experimental Hematopathology | 2016

Composite Follicular Lymphoma and CD5-Positive Nodal Marginal Zone Lymphoma.

Masashi Miyaoka; Tomoki Kikuchi; Joaquim Carreras; Yukie Y. Kikuti; Ken Omachi; Minoru Kojima; Kiyoshi Ando; Naoya Nakamura

Composite CD10-positive low-grade B-cell and CD5-positive low-grade B-cell lymphoma is extremely rare. We report a case of a composite follicular lymphoma (FL) and CD5-positive nodal marginal zone lymphoma (NMZL) in a resected inguinal lymph node of a 72-year-old Japanese male. Histologically, multiple follicles had reactive-germinal centers with tingible body macrophages, a thin mantle zone and a wide marginal zone. The wide marginal zone consisted of medium-sized cells having slightly indented nuclei and clear cytoplasm, indicating monocytoid cells with CD5-positive B-cells. Several follicles had germinal centers filled with many centrocytes, with CD10-positive B-cells. Polymerase chain reaction/sequence analysis of the immunoglobulin heavy chain gene obtained from microdissected regions of CD5-positive NMZL and FL showed different sequences within the CDR3 region. To our knowledge, this is the first report of FL and CD5-positive NMZL.


Environmental Toxicology | 2014

Association of sick building syndrome with neuropathy target esterase (NTE) activity in Japanese

Yasunari Matsuzaka; Tomoichi Ohkubo; Yukie Y. Kikuti; Akiko Mizutani; Michio Tsuda; Yoshiko Aoyama; Kazuhiko Kakuta; Akira Oka; Hidetoshi Inoko; Kou Sakabe; Satoshi Ishikawa; Jerzy K. Kulski; Minoru Kimura

Sick building syndrome (SBS) is a set of several clinically recognizable symptoms reported by occupants of a building without a clear cause. Neuropathy target esterase (NTE) is a membrane bound serine esterase and its reaction with organophosphates (OPs) can lead to OP‐induced delayed neuropathy (OPIDN) and nerve axon degeneration. The aim of our study was to determine whether there was a difference in NTE activity in the peripheral blood mononuclear cells (PBMCs) of Japanese patients with SBS and healthy controls and whether PNPLA6 (alias NTE) gene polymorphisms were associated with SBS. We found that the enzymatic activity of NTE was significantly higher (P < 0.0005) in SBS patients compared with controls. Moreover, population with an AA genotype of a single nucleotide polymorphism (SNP), rs480208, in intron 21 of the PNPLA6 gene strongly reduced the activity of NTE. Fifty‐eight SNP markers within the PNPLA6 gene were tested for association in a case–control study of 188 affected individuals and 401 age‐matched controls. Only one SNP, rs480208, was statistically different in genotype distribution (P = 0.005) and allele frequency (P = 0.006) between the cases and controls (uncorrected for testing multiple SNP sites), but these were not significant by multiple corrections. The findings of the association between the enzymatic activity of NTE and SBS in Japanese show for the first time that NTE activity might be involved with SBS.


Environmental Toxicology and Pharmacology | 2010

Association study between sick building syndrome and polymorphisms of seven human detoxification genes in the Japanese

Yasunari Matsuzaka; Yukie Y. Kikuti; Akiko Mizutani; Yoshiko Aoyama; Kazuhiko Kakuta; Akira Oka; Hidetoshi Inoko; Kou Sakabe; Satoshi Ishikawa; Jerzy K. Kulski; Minoru Kimura

Sick building syndrome (SBS) is a chronic disorder caused by exposure to diverse indoor environmental or chemical pollutants. This study examined the association between seven detoxification genes (CYP1A1, CYP2E1, EPHX1, GSTM1, GSTT1, GSTP1, and NAT2) and SBS in the Japanese population. One hundred eighty patients with SBS and 401 healthy controls were enrolled in this study. We examined the prevalence for total of eleven genetic polymorphisms of detoxification genes. However, no statistically significant differences in allele and genotype frequency distributions of eleven genetic polymorphisms of these detoxification genes were found between patients and controls. On this basis, we conclude that the polymorphisms that we assessed for the detoxification genes do not contribute to the etiology of SBS.


Tissue Antigens | 1992

PCR‐RFLP is as sensitive and reliable as PCR‐SSO in HLA class II genotyping

Nobuhisa Mizuki; Shigeaki Ohno; Kazuhito Sugimura; Takeshi Seki; Yukie Y. Kikuti; Asako Ando; Masao Ota; Kimiyoshi Tsuji; Hidetoshi Inoko


Genes & Genetic Systems | 2006

Construction of mouse 129/Ola BAC library for targeting experiments using E14 embryonic stem cells.

Masato Ohtsuka; Kenta Ishii; Yukie Y. Kikuti; Takayuki Warita; Daisuke Suzuki; Masahiro Sato; Minoru Kimura; Hidetoshi Inoko


Journal of Clinical and Experimental Hematopathology | 2010

Characteristics of CD5-Positive Splenic Marginal Zone Lymphoma with Leukemic Manifestation ; Clinical, Flow Cytometry, and Histopathological Findings of 11 Cases

Minoru Kojima; Eriko Sato; Kazuo Oshimi; Takuhei Murase; Tadashi Koike; Sinichirou Tsunoda; Toshiharu Matsumoto; Kousuke Marutsuka; Daisuke Ogiya; Makiko Moriuchi; Mami Tokunaka; Yukie Y. Kikuti; Tomoki Kikuchi; Naoya Nakamura; Kiyoshi Ando


Analytical Biochemistry | 2007

One-step generation of recombineering constructs by asymmetric-end ligation and negative selection

Masato Ohtsuka; Akiko Mizutani; Yukie Y. Kikuti; Jerzy K. Kulski; Masahiro Sato; Minoru Kimura; Masafumi Tanaka; Hidetoshi Inoko

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Akiko Mizutani

Teikyo Heisei University

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