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Featured researches published by Kaoru Sato.


Diabetes | 1987

Time Course of Islet Cell Antibodies and β-Cell Function in Non-Insulin-Dependent Stage of Type I Diabetes

Tetsuro Kobayashi; Tokuji Itoh; Kinori Kosaka; Kaoru Sato; Kimiyoshi Tsuji

The time course of islet cell antibodies (ICA) and serum C-peptides responses (CPRs) to oral glucose tolerance tests (OGTTs) were studied prospectively up to 60 (mean 35) mo in 32 ICA-positive subjects [28 with non-insulin-dependent diabetes (NIDDM) and 4 subjects with impaired glucose tolerance (IGT); mean age 45 yr], 96 matched subjects [56 with NIDDM, 8 with IGT, and 32 normal first-degree relatives of patients with insulin-dependent diabetes (IDDM); mean age 45 yr] who were negative for ICA at the beginning of the study. In addition, the effects of human leukocyte antigens(HLA) on the time course of ICA and (β-cell function were evaluated. In 10 subjects (8 with NIDDM and 2 with IGT) who were ICA positive, ICA became undetectable, even by sensitive ICA assay, 15 ± 2 mo (mean ± SE) after initiation of this study. In these subjects, integrated serum CPR values (σCPR) and 2-h blood glucose values in response to OGTTs improved significantly (P < .05-.01). In contrast, the remaining 22 subjects who were ICA positive were persistently positive for ICA. CPR and blood glucose responses deteriorated progressively in these 22 subjects, and 7 subjects in this group progressed to the insulin-dependent state. Serum CPR and blood glucose responses to OGTTs showed no remarkable changes in 64 patients (56 with NIDDM and 8 with IGT) and 32 normal first-degree relatives of patients with IDDM who remained negative for ICA throughout the study. The frequencies of HLABW54 and HLA-DR4 in 10 subjects who became ICA negative during the follow-up period were lower than those in 22 subjects with ICA throughout the study (uncorrected P < .02). The frequencies of these two antigens were higher in the 22 subjects with persistently positive ICA than in normal controls (uncorrected P < .02), whereas these differences were not observed in 10 subjects who became ICA negative during the study. The reversed β-cell function after negative conversion of ICA observed in our study yields a new insight into the natural history of type I diabetes, especially in late-onset cases. It suggests that HLA-related genetic predisposition is a prerequisite to the slowly progressive β-cell destruction through pancreatic autoimmunity.


Diabetes | 1986

The Prevalence of Islet Cell Antibodies in Japanese Insulin-dependent and Non-insulin-dependent Diabetic Patients Studied by Indirect Immunofluorescence and by a New Method

Tetsuro Kobayashi; Tadao Sugimoto; Tokuji Itoh; Kinori Kosaka; Toshiaki Tanaka; Seizo Suwa; Kaoru Sato; Kimiyoshi Tsuji

Islet cell antibodies (ICA) were measured in Japanese patients with insulin-dependent diabetes mellitus (IDDM) and non-insulin-dependent diabetes mellitus (NIDDM) by a standard, indirect immunofluorescence method (IF method) and by a newly established, threelayer immunofluorescence method applying a biotin-avidin system (BAS method). In addition, the relationship between ICA and HLA was studied in IDDM patients. ICA titers detected by the BAS method correlated well with those determined by the standard IF method (rs = 0.987, P < 0.01). The BAS method had about an eightfold higher sensitivity for ICA than the IF method. The overall prevalence of ICA detected by the BAS method (ICA-BAS) versus that by the IF method (ICAIF) was 41% (82/198) versus 28% (56/198) in IDDM patients and 3% (19/593) versus 2% (14/593) in patients with NIDDM. In IDDM patients, ICA-BAS was all positive <1 mo after the onset of diabetes, while the prevalence of ICA-IF was 83% (20/24) during the same period. The prevalence of ICA-IF decreased rapidly with the duration of disease, reaching a value of 6% (3/55) in the patients with a disease duration of 10 yr or more. The incidence of ICA-BAS also decreased with the duration of disease, although to a lesser degree than ICA-IF. No association was found between HLA types and persistence of ICA-BAS or -IF. These results suggest that pancreatic autoimmune processes occur in almost all Japanese IDDM patients. Although IDDM is less common in Japan than among Caucasians, the prevalence of ICA seems to be the same. The higher sensitivity of the BAS method may be of significant diagnostic value, especially in patients with a long duration of disease.


Journal of Reproductive Immunology | 1998

Presence of HSV-1 DNA in semen and menstrual blood.

Nadia El Borai; Christophe Lefèvre; Masato Inoue; Elena N. Naumova; Kaoru Sato; Shihoko Suzuki; Kimiyoshi Tsuji; Masaichi Yamamura

Using a specifically designed diagnostic PCR assay with nested primers the following could be achieved: (1) a group of 22 clinically indistinguishable women attending an infertility clinic, 18 with repeated embryo transfer failure, and asymptomatic for HSV-1 could be divided into two subgroups after testing their menstrual blood. An HSV-DNA positive (50%) and HSV-DNA negative group (50%) could be distinguished. None of the four controls were positive; (2) semen from 154 infertile and 24 fertile men was tested in relation to infertility. In the group of infertile men 37 (24%) were HSV-DNA positive but none of the fertile control (0%) was positive; (3) treatment of both partners with an antiviral drug resulted in two pregnancies; (4) HLA data on four of the couples in which the wifes menstrual blood was HSV positive was compared to seven HSV negative couples and 22 infertile, as well as 22 fertile couples. Clustering of class I HLA (B61 and Cw3) was found with a significant increase in Cw3 in both partners.


Human Immunology | 1982

HLA-D clusters associated with DR4 in the Japanese population.

Yoshisuke Nose; Kaoru Sato; Mariko Nakagawa; Keiko Kondoh; Hiroo Inouye; Kimiyoshi Tsuji

A study of HLA-D clusters associated with DR4 was performed in the Japanese population. These clusters consist of DYT, DKT2, DB3, and Dw4. Forty-two Japanese typed as DR4 were investigated, and it was found that 17 (40.5%) were DYT, 7 (16.7%) DKT2, 7 (16.7%) DB3, and 4 (9.5%) Dw4.


Transplantation | 1997

Association between HLA-DPB1 matching and 1-year rejection-free graft survival in high-risk corneal transplantation

Batmunkh Munkhbat; Masao Hagihara; Tadayuki Sato; Fumiko Tsuchida; Kaoru Sato; Jun Shimazaki; Kazuo Tsubota; Kimiyoshi Tsuji

We analyzed the effect of matching for HLA class II alleles on corneal graft outcome in a single-center, retrospective study from January 1991 through April 1996. The study involved 81 transplant recipients at high and low risk of corneal graft rejection, who were typed by the polymerase chain reaction-restriction fragment length polymorphism method and who completed at least 1-year of follow-up. The DRB1, DQB1, and DPB1 alleles were analyzed together and transplant recipients were subdivided into groups with matching (one to four alleles matched in the high risk or one to five alleles matched in the low risk) and without matching (no allele matched) for HLA class II. A significantly higher rate of 1-year rejection-free graft survival was revealed in high-risk transplant recipients with matching, compared with those without matching (P=0.0238). We have shown that matching for at least one HLA class II allele was actually beneficial in high-risk transplants. An analysis of matching for each allele separately, detected that only HLA-DPB1 matching was significantly associated with a higher rate of 1-year rejection-free graft survival in high-risk transplant recipients with matching (one or two alleles matched) compared with those without matching (no allele matched) (P=0.0139). In particular, matching for one DPB1 allele was significantly beneficial compared with no matching (P=0.0140). There was no significant effect of HLA-DRB1 and -DQB1 matching (P=0.3177 and P=0.2878, respectively). Furthermore, a strong association between DPB1 matching and 1-year rejection-free graft survival was observed in DRB1-incompatible high-risk transplant recipients (P=0.0308). Nevertheless, no significant effect of DPB1 matching was detected in DQB1-incompatible transplant recipients. Our findings indicate that HLA class II DNA typing is clinically relevant for corneal transplant recipients and that especially HLA-DPB1 matching has a beneficial effect in high-risk corneal transplantation.


Journal of Gastroenterology | 1997

Serum concentrations of soluble HLA-class I and CD8 forms in patients with viral hepatic disorders

Masao Hagihara; Tatsuo Shimura; Kentaro Takebe; Batmunkh Munkhbat; Katsumi Hosoi; Tatehiro Kagawa; Norihito Watanabe; Shohei Matsuzaki; Kozue Yamamoto; Kaoru Sato; Kimiyoshi Tsuji

Soluble HLA-class I and CD8 molecules were determined by sandwich ELISA in patients with viral-induced hepatic disorders. As a whole, the patients with hepatic disorders (acute hepatitis: AH; chronic hepatitis: CH; liver cirrhosis: LC; hepatocellular carcinoma: HCC) showed higher sHLA-class I and sCD8 levels than normal controls (P<0.001). AH patients had the highest sHLA-class I levels (mean, 3513±2112ng/ml), followed by CH (2896±1290ng/ml), LC (2293±1266ng/ml), and HCC (2221±1212ng/ml) sCD8 levels were highest in AH, followed by HCC, LC, and CH, in that order. Among histologically defined C virus-positive patients, sHLA-I levels were higher in those with chronic active hepatitis (CAH) 2A (3802±1124ng/ml) than in those with chronic persistent hepatitis (CPH; 2200±711ng/ml;P<0.01), the levels then decreased as the disease progressed (CAH2B, 3564±1783ng/ml, LC, 2376±1265ng/ml). In contrast, sCD8 values showed little difference among the disorders. sHLA-class I levels showed a positive correlation with sCD8 values both in whole patients and in patients with AH (P<0.01), but no correlation was shown, in any patients, with biochemical parameters such as GPT and GOT. These findings, taken together, suggest that hepatic destruction is not the only cause of sHLA-class I production, but that sHLA-class I levels, together with sCD8 levels, may reflect immunological activity in hepatic disorders.


Human Immunology | 1995

HLA and tumor necrosis factor β gene polymorphisms in Okinawa lung cancer patients: Comparative study with mainland Japan lung cancer patients

Masao Hagihara; Tatsuo Shimura; Kaoru Sato; Keiichiro Genga; Makoto Suzuki; Kimiyoshi Tsuji

The frequencies of HLA class I and II antigens and TNF-beta polymorphism in lung cancer patients were investigated in two areas with different immunogenetic backgrounds, in Okinawa and in mainland Japan (Honshu). In Okinawa frequencies of HLA-Cw3 in squamous cell lung carcinoma patients were higher and those of HLA-DR, both in all lung cancer and in adeno lung carcinoma patients, were lower compared to those of normal controls. Among serologic HLA-DR4-positive individuals, no difference of DRB1*04 gene allele frequency was shown between patients and controls. In Honshu no statistically significant difference of HLA-class I and II alleles frequencies was found; however, the frequency of TNF-beta 10.5-kb homozygote in lung cancer patients was lower than that of controls. For 2-year survival, there was no difference between DR4-positive and -negative individuals and also between each TNF-beta type in Okinawa. In contrast, Honshu patients with 10.5-kb homozygote showed an improved 5-year survival ratio compared to those with heterozygote. We postulate that different immunogenetic backgrounds or environments might have caused the varying HLA or TNF-beta association in the predisposition to or prognosis of lung cancer.


Tissue Antigens | 1997

Molecular analysis of HLA polymorphism in Khoton‐Mongolians

Batmunkh Munkhbat; Tadayuki Sato; Masao Hagihara; Kaoru Sato; Akinori Kimura; N. Munkhtuvshin; Kimiyoshi Tsuji


Clinical Endocrinology | 1992

Correlation of HLA types and clinical findings in Japanese patients with hyperthyroid Graves' disease: evidence indicating the existence of four subpopulations

Daisuke Inoue; Kaoru Sato; Tetsuya Enomolo; Hideo Sugawa; Masahiro Maeda; Hidetoshi Inoko; Kimiyoshi Tsuji; Toru Mori; Hlroo Imura


International Journal of Cancer | 1987

Altered HLA antigens expressed on T and B lymphocytes of adult T-cell leukemia/lymphoma patients and their relatives.

Shunro Sonoda; Shinji Yashiki; Kazuo Takahashi; Naomichi Arima; Yasuhisa Daitoku; Makoto Matsumoto; Tadashi Matsumoto; Mitsutoshi Tara; Koichi Shinmyozu; Kaoru Sato; Hidetoshi Inoko; Asako Ando; Kimiyoshi Tsiji

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