Your search keyword '"Hosoe, Yuko"' showing total 12 results

1. A stearate-rich diet and oleate restriction directly inhibit tumor growth via the unfolded protein response.

Author

Ogura, Jumpei, Yamanoi, Koji, Ishida, Kentaro, Nakamura, Eijiro, Ito, Shinji, Aoyama, Naoki, Nakanishi, Yuki, Menju, Toshi, Kawaguchi, Kosuke, Hosoe, Yuko, Taki, Mana, Murakami, Ryusuke, Yamaguchi, Ken, Hamanishi, Junzo, and Mandai, Masaki

Published

2024

2. Development of healthy lifestyle consciousness index for gynecological cancer patients

Author

30583190, 50600061, 70868075, 20898077, 80378736, Higashiyama, Nozomi, Yamaguchi, Ken, Yamamoto, Yosuke, Ueda, Akihiko, Inayama, Yoshihide, Egawa, Miho, Yamanoi, Koji, Taki, Mana, Ukita, Masayo, Hosoe, Yuko, Horie, Akihito, Hamanishi, Junzo, Mandai, Masaki, 30583190, 50600061, 70868075, 20898077, 80378736, Higashiyama, Nozomi, Yamaguchi, Ken, Yamamoto, Yosuke, Ueda, Akihiko, Inayama, Yoshihide, Egawa, Miho, Yamanoi, Koji, Taki, Mana, Ukita, Masayo, Hosoe, Yuko, Horie, Akihito, Hamanishi, Junzo, and Mandai, Masaki

Abstract

PURPOSE: Healthy lifestyle is related to quality of life (QOL) after cancer diagnosis and prognosis. However, there are few reports on patients conscious of healthy lifestyle and patients requiring medical providers' attention regarding healthy lifestyle. We aimed to develop a healthy lifestyle consciousness index (HLCI) for cancer patients and evaluated its validity in gynecological cancer patients. METHODS: The HLCI was designed to assess degree of healthy lifestyle consciousness, including items regarding "diet, " "exercise, " "body weight, " and "sleep." Exploratory factor analysis was performed for dimensionality of the scale; Cronbach's alpha was calculated to assess internal-consistency reliability. For criterion-based validity, we calculated proportions of stage III/IV gynecological malignancies in those with categorized HLCI scores based on tertiles. Concurrent validity was evaluated between HLCI and other quality of life (QOL) scales including European Organization for Research and Treatment of Cancer QLQ-C30 in limited patients. RESULTS: HLCI comprised five 10-point items (0-45); higher values implied improved healthy lifestyle consciousness. Data from 108 gynecological malignancy patients at Kyoto University Hospital were analyzed. The mean age of subjects was 55.8 years; 36.1% of them had uterine corpus cancer; 34.3% were at stage III/IV of gynecological malignancy. The factor analysis revealed HLCI was unidimensional; the reliability based on Cronbach's alpha was satisfactory (0.88). The proportions of stage III/IV gynecological malignancies were 25.7%, 33.3%, and 44.4% in those with first (7-24 points), second (25-30 points), and third (31-46 points) tertiles of HLCI score, respectively. For patients with other QOL scales (n = 25), the mean scores of global health status of QLQ-C30 were 33.3, 50.0, and 83.3 for first, second, and third tertiles of HLCI score, respectively. CONCLUSION: HLCI was successfully validated; thus, patients with advanced stage

Published

2022

3. Tertiary lymphoid structures are associated with favorable survival outcomes in patients with endometrial cancer

Author

70868075, Qin, Meng, Hamanishi, Junzo, Ukita, Masayo, Yamanoi, Koji, Takamatsu, Shiro, Abiko, Kaoru, Murakami, Ryusuke, Miyamoto, Taito, Suzuki, Haruka, Ueda, Akihiko, Hosoe, Yuko, Horie, Akihito, Yamaguchi, Ken, Mandai, Masaki, 70868075, Qin, Meng, Hamanishi, Junzo, Ukita, Masayo, Yamanoi, Koji, Takamatsu, Shiro, Abiko, Kaoru, Murakami, Ryusuke, Miyamoto, Taito, Suzuki, Haruka, Ueda, Akihiko, Hosoe, Yuko, Horie, Akihito, Yamaguchi, Ken, and Mandai, Masaki

Abstract

Immunotherapy has experienced remarkable growth recently. Tertiary lymphoid structures (TLSs) and B cells may play a key role in the immune response and have a survival benefit in some solid tumors, but there have been no reports about their role in endometrial cancer (EC). We investigated the clinicopathological and pathobiological characteristics of the tumor microenvironment (TME) in EC. Patients with EC at Kyoto University Hospital during 2006–2011 were retrospectively included. In 104 patients with EC who met study inclusion criteria, 81 (77.9%) had TLSs, which consisted of areas rich in CD20⁺ B cells, CD8⁺ T cells, CD4⁺ T cells, and CD38⁺ plasma cells. The absence of TLS was independently associated with tumor progression (HR, 0.154; 95% CI, 0.044–0.536; P = 0.003). Patients with TLSs that included CD23⁺ germinal centers had better PFS. All tumor infiltrating lymphocytes were counted in the intratumor site. The number of CD20⁺ B cells was significantly larger in patients with TLSs than in those without TLS (P < 0.001). CD20⁺ B cells numbers were positively correlated with other TLSs. The larger number of CD20⁺ B cell was associated with better PFS (P = 0.015). TLSs and B cell infiltration into tumors are associated with favorable survival outcomes in patients with EC. They may represent an active immune reaction of the TME in endometrial cancer.

Published

2022

4. Development of healthy lifestyle consciousness index for gynecological cancer patients.

Author

Higashiyama, Nozomi, Yamaguchi, Ken, Yamamoto, Yosuke, Ueda, Akihiko, Inayama, Yoshihide, Egawa, Miho, Yamanoi, Koji, Taki, Mana, Ukita, Masayo, Hosoe, Yuko, Horie, Akihito, Hamanishi, Junzo, and Mandai, Masaki

Abstract

Purpose: Healthy lifestyle is related to quality of life (QOL) after cancer diagnosis and prognosis. However, there are few reports on patients conscious of healthy lifestyle and patients requiring medical providers' attention regarding healthy lifestyle. We aimed to develop a healthy lifestyle consciousness index (HLCI) for cancer patients and evaluated its validity in gynecological cancer patients. Methods: The HLCI was designed to assess degree of healthy lifestyle consciousness, including items regarding "diet," "exercise," "body weight," and "sleep." Exploratory factor analysis was performed for dimensionality of the scale; Cronbach's alpha was calculated to assess internal-consistency reliability. For criterion-based validity, we calculated proportions of stage III/IV gynecological malignancies in those with categorized HLCI scores based on tertiles. Concurrent validity was evaluated between HLCI and other quality of life (QOL) scales including European Organization for Research and Treatment of Cancer QLQ-C30 in limited patients. Results: HLCI comprised five 10-point items (0–45); higher values implied improved healthy lifestyle consciousness. Data from 108 gynecological malignancy patients at Kyoto University Hospital were analyzed. The mean age of subjects was 55.8 years; 36.1% of them had uterine corpus cancer; 34.3% were at stage III/IV of gynecological malignancy. The factor analysis revealed HLCI was unidimensional; the reliability based on Cronbach's alpha was satisfactory (0.88). The proportions of stage III/IV gynecological malignancies were 25.7%, 33.3%, and 44.4% in those with first (7–24 points), second (25–30 points), and third (31–46 points) tertiles of HLCI score, respectively. For patients with other QOL scales (n = 25), the mean scores of global health status of QLQ-C30 were 33.3, 50.0, and 83.3 for first, second, and third tertiles of HLCI score, respectively. Conclusion: HLCI was successfully validated; thus, patients with advanced stages or higher QOL might have strong consciousness regarding healthy lifestyle. HLCI may be useful in precision care for improved lifestyles and QOL. [ABSTRACT FROM AUTHOR]

Published

2022

5. Tertiary lymphoid structures are associated with favorable survival outcomes in patients with endometrial cancer.

Author

Qin, Meng, Hamanishi, Junzo, Ukita, Masayo, Yamanoi, Koji, Takamatsu, Shiro, Abiko, Kaoru, Murakami, Ryusuke, Miyamoto, Taito, Suzuki, Haruka, Ueda, Akihiko, Hosoe, Yuko, Horie, Akihito, Yamaguchi, Ken, and Mandai, Masaki

Subjects

TREATMENT effectiveness, TERTIARY structure, TUMOR-infiltrating immune cells, CANCER prognosis, B cells

Abstract

Immunotherapy has experienced remarkable growth recently. Tertiary lymphoid structures (TLSs) and B cells may play a key role in the immune response and have a survival benefit in some solid tumors, but there have been no reports about their role in endometrial cancer (EC). We investigated the clinicopathological and pathobiological characteristics of the tumor microenvironment (TME) in EC. Patients with EC at Kyoto University Hospital during 2006–2011 were retrospectively included. In 104 patients with EC who met study inclusion criteria, 81 (77.9%) had TLSs, which consisted of areas rich in CD20+ B cells, CD8+ T cells, CD4+ T cells, and CD38+ plasma cells. The absence of TLS was independently associated with tumor progression (HR, 0.154; 95% CI, 0.044–0.536; P = 0.003). Patients with TLSs that included CD23+ germinal centers had better PFS. All tumor infiltrating lymphocytes were counted in the intratumor site. The number of CD20+ B cells was significantly larger in patients with TLSs than in those without TLS (P < 0.001). CD20+ B cells numbers were positively correlated with other TLSs. The larger number of CD20+ B cell was associated with better PFS (P = 0.015). TLSs and B cell infiltration into tumors are associated with favorable survival outcomes in patients with EC. They may represent an active immune reaction of the TME in endometrial cancer. [ABSTRACT FROM AUTHOR]

Published

2022

6. Combination of gene set signatures correlates with response to nivolumab in platinum-resistant ovarian cancer.

Author

Murakami, Ryusuke, Hamanishi, Junzo, Brown, J. B., Abiko, Kaoru, Yamanoi, Koji, Taki, Mana, Hosoe, Yuko, Yamaguchi, Ken, Baba, Tsukasa, Matsumura, Noriomi, Konishi, Ikuo, and Mandai, Masaki

Subjects

NIVOLUMAB, OVARIAN cancer, DRUG resistance in cancer cells, BIOMARKERS, GENE expression

Abstract

Based on our previous phase II clinical trial of anti-programmed death-1 (PD-1) antibody nivolumab for platinum-resistant ovarian cancer (n = 19, UMIN000005714), we aimed to identify the biomarkers predictive of response. Tumor gene expression was evaluated by proliferative, mesenchymal, differentiated, and immunoreactive gene signatures derived from high-grade serous carcinomas and a signature established prior for ovarian clear cell carcinoma. Resulting signature scores were statistically assessed with both univariate and multivariate approaches for correlation to clinical response. Analyses were performed to identify pathways differentially expressed by either the complete response (CR) or progressive disease (PD) patient groups. The clear cell gene signature was scored significantly higher in the CR group, and the proliferative gene signature had significantly higher scores in the PD group where nivolumab was not effective (respective p values 0.005 and 0.026). Combinations of gene signatures improved correlation with response, where a visual projection of immunoreactive, proliferative, and clear cell signatures differentiated clinical response. An applicable clinical response prediction formula was derived. Ovarian cancer-specific gene signatures and related pathway scores provide a robust preliminary indicator for ovarian cancer patients prior to anti-PD-1 therapy decisions. [ABSTRACT FROM AUTHOR]

Published

2021

7. Acquisition of a side population fraction augments malignant phenotype in ovarian cancer

Author

70868075, 80378736, 20898077, Yamanoi, Koji, Baba, Tsukasa, Abiko, Kaoru, Hamanishi, Junzo, Yamaguchi, Ken, Murakami, Ryusuke, Taki, Mana, Hosoe, Yuko, Murphy, Susan K., Konishi, Ikuo, Mandai, Masaki, Matsumura, Noriomi, 70868075, 80378736, 20898077, Yamanoi, Koji, Baba, Tsukasa, Abiko, Kaoru, Hamanishi, Junzo, Yamaguchi, Ken, Murakami, Ryusuke, Taki, Mana, Hosoe, Yuko, Murphy, Susan K., Konishi, Ikuo, Mandai, Masaki, and Matsumura, Noriomi

Abstract

Side population (SP) cells harbor malignant phenotypes in cancer. The aim of this study was to identify genes that modulate the proportion of ovarian cancer SP cells. Using a shRNA library targeting 15, 000 genes, a functional genomics screen was performed to identify genes whose suppression increased the SP percentage. The biological effects caused by alteration of those identified genes were investigated in vitro and in vivo. We found that suppression of MSL3, ZNF691, VPS45, ITGB3BP, TLE2, and ZNF498 increased the proportion of SP cells. Newly generated SP cells exhibit greater capacity for sphere formation, single cell clonogenicity, and in vivo tumorigenicity. On the contrary, overexpression of MSL3, VPS45, ITGB3BP, TLE2, and ZNF498 decreased the proportion of SP cells, sphere formation capacity and single cell clonogenicity. In ovarian cancer cases, low expression of MSL3, ZNF691 and VPS45 was related to poor prognosis. Suppression of these six genes enhanced activity of the hedgehog pathway. Cyclopamine, a hedgehog pathway inhibitor, significantly decreased the number of SP cells and their sphere forming ability. Our results provide new information regarding molecular mechanisms favoring SP cells and suggest that Hedgehog signaling may provide a viable target for ovarian cancer.

Published

2019

8. Anti-VEGF therapy resistance in ovarian cancer is caused by GM-CSF-induced myeloid-derived suppressor cell recruitment.

Author

Horikawa, Naoki, Abiko, Kaoru, Matsumura, Noriomi, Baba, Tsukasa, Hamanishi, Junzo, Yamaguchi, Ken, Murakami, Ryusuke, Taki, Mana, Ukita, Masayo, Hosoe, Yuko, Koshiyama, Masafumi, Konishi, Ikuo, and Mandai, Masaki

Subjects

VASCULAR endothelial growth factor antagonists, GRANULOCYTE-macrophage colony-stimulating factor, BIOLOGICAL models, RESEARCH, OVARIAN tumors, ANIMAL experimentation, RESEARCH methodology, EVALUATION research, MEDICAL cooperation, COMPARATIVE studies, MICE

Abstract

Background: The mechanism of resistance development to anti-VEGF therapy in ovarian cancer is unclear. We focused on the changes in tumour immunity post anti-VEGF therapy.Methods: The frequencies of immune cell populations and hypoxic conditions in the resistant murine tumours and clinical samples were examined. The expression profiles of both the proteins and genes in the resistant tumours were analysed. The impact of granulocyte-monocyte colony-stimulating factor (GM-CSF) expression on myeloid-derived suppressor cell (MDSC) function in the resistant tumours was evaluated.Results: We found a marked increase and reduction in the number of Gr-1 + MDSCs and CD8 + lymphocytes in the resistant tumour, and the MDSCs preferentially infiltrated the hypoxic region. Protein array analysis showed upregulation of GM-CSF post anti-VEGF therapy. GM-CSF promoted migration and differentiation of MDSCs, which inhibited the CD8 + lymphocyte proliferation. Anti-GM-CSF therapy improved the anti-VEGF therapy efficacy, which reduced the infiltrating MDSCs and increased CD8 + lymphocytes. In immunohistochemical analysis of clinical samples, GM-CSF expression and MDSC infiltration was enhanced in the bevacizumab-resistant case.Conclusions: The anti-VEGF therapy induces tumour hypoxia and GM-CSF expression, which recruits MDSCs and inhibits tumour immunity. Targeting the GM-CSF could help overcome the anti-VEGF therapy resistance in ovarian cancers. [ABSTRACT FROM AUTHOR]

Published

2020

9. Snail promotes ovarian cancer progression by recruiting myeloid-derived suppressor cells via CXCR2 ligand upregulation

Author

20898077, 20508246, 80378736, 70868075, 60839140, Taki, Mana, Abiko, Kaoru, Baba, Tsukasa, Hamanishi, Junzo, Yamaguchi, Ken, Murakami, Ryusuke, Yamanoi, Koji, Horikawa, Naoki, Hosoe, Yuko, Nakamura, Eijiro, Sugiyama, Aiko, Mandai, Masaki, Konishi, Ikuo, Matsumura, Noriomi, 20898077, 20508246, 80378736, 70868075, 60839140, Taki, Mana, Abiko, Kaoru, Baba, Tsukasa, Hamanishi, Junzo, Yamaguchi, Ken, Murakami, Ryusuke, Yamanoi, Koji, Horikawa, Naoki, Hosoe, Yuko, Nakamura, Eijiro, Sugiyama, Aiko, Mandai, Masaki, Konishi, Ikuo, and Matsumura, Noriomi

Abstract

Snail is a major transcriptional factor that induces epithelial-mesenchymal transition (EMT). In this study, we explore the effect of Snail on tumor immunity. Snail knockdown in mouse ovarian cancer cells suppresses tumor growth in immunocompetent mice, associated with an increase of CD8+ tumor-infiltrating lymphocytes and a decrease of myeloid-derived suppressor cells (MDSCs). Snail knockdown reduces the expression of CXCR2 ligands (CXCL1 and CXCL2), chemokines that attract MDSCs to the tumor via CXCR2. Snail upregulates CXCR ligands through NF-kB pathway, and most likely, through direct binding to the promoters. A CXCR2 antagonist suppresses MDSC infiltration and delays tumor growth in Snail-expressing mouse tumors. Ovarian cancer patients show elevated serum CXCL1/2, which correlates with Snail expression, MDSC infiltration, and short overall survival. Thus, Snail induces cancer progression via upregulation of CXCR2 ligands and recruitment of MDSCs. Blocking CXCR2 represents an immunological therapeutic approach to inhibit progression of Snail-high tumors undergoing EMT.

Published

2018

10. VISTA expressed in tumour cells regulates T cell function.

Author

Mulati, Kumuluzi, Hamanishi, Junzo, Matsumura, Noriomi, Chamoto, Kenji, Mise, Nathan, Abiko, Kaoru, Baba, Tsukasa, Yamaguchi, Ken, Horikawa, Naoki, Murakami, Ryusuke, Taki, Mana, Budiman, Kharma, Zeng, Xiang, Hosoe, Yuko, Azuma, Miyuki, Konishi, Ikuo, and Mandai, Masaki

Abstract

Background: V-domain Ig suppressor of T cell activation (VISTA) is a novel inhibitory immune-checkpoint protein. VISTA expression on tumour cells and the associated regulatory mechanisms remain unclear. We investigated VISTA expression and function in tumour cells, and evaluated its mechanism and activity.Methods: VISTA in tumour cells was assessed by tissue microarray analysis, immunohistochemical staining and western blot. A series of in vitro assays were used to determine the function of tumour-expressed VISTA. In vivo efficacy was evaluated in syngeneic models.Results: VISTA was highly expressed in human ovarian and endometrial cancers. Upregulation of VISTA in endometrial cancer was related to the methylation status of the VISTA promoter. VISTA in tumour cells suppressed T cell proliferation and cytokine production in vitro, and decreased the tumour-infiltrating CD8+ T cells in vivo. Anti-VISTA antibody prolonged the survival of tumour-bearing mice.Conclusions: This is the first demonstration that VISTA is highly expressed in human ovarian and endometrial cancer cells, and that anti-VISTA antibody treatment significantly prolongs the survival of mice bearing tumours expressing high levels of VISTA. The data suggest that VISTA is a novel immunosuppressive factor within the tumour microenvironment, as well as a new target for cancer immunotherapy. [ABSTRACT FROM AUTHOR]

Published

2019

11. Menstrual cyclic change of metastin/GPR54 in endometrium.

Author

Baba, Tsukasa, Kang, Hyun, Hosoe, Yuko, Kharma, Budiman, Abiko, Kaoru, Matsumura, Noriomi, Hamanishi, Junzo, Yamaguchi, Ken, Yoshioka, Yumiko, Koshiyama, Masafumi, Mandai, Masaki, Murphy, Susan, and Konishi, Ikuo

Subjects

MENSTRUAL cycle, G protein coupled receptors, ENDOMETRIUM, LUTEINIZING hormone releasing hormone, KISSPEPTIN neurons, PROTEIN-protein interactions, CARCINOGENESIS, KISSPEPTINS

Abstract

Metastin/kisspeptin is encoded by KISS1 and functions as an endogenous ligand of GPR54. Interaction of metastin with GPR54 suppresses metastasis and also regulates release of gonadotropin-releasing hormone, which promotes secretion of estradiol (E2) and progesterone (P4). We have previously demonstrated epigenetic regulation of GPR54 in endometrial cancer and the potent role of metastin peptides in inhibiting metastasis in endometrial cancer. However, little is known about how the metastin-GPR54 axis is regulated in the endometrium, the precursor tissue of endometrial cancer. Endometrial stromal cells (ESCs) and endometrial glandular cells (EGCs) within the endometrium show morphological changes when exposed to E2 and P4. In this study, we show that metastin expression is induced in ESCs through decidualization, but is repressed in glandular components of atypical endometrial hyperplasia (AEH) and endometrial cancer relative to EGCs. The promoter of GPR54 is unmethylated in normal endometrium and in AEH. These results indicate metastin may function in decidualized endometrium to prepare for adequate placentation but this autocrine secretion of metastin is deregulated during oncogenesis to enable tumor cells to spread. [ABSTRACT FROM AUTHOR]

Published

2015

12. Acquisition of a side population fraction augments malignant phenotype in ovarian cancer.

Author

Yamanoi, Koji, Baba, Tsukasa, Abiko, Kaoru, Hamanishi, Junzo, Yamaguchi, Ken, Murakami, Ryusuke, Taki, Mana, Hosoe, Yuko, Murphy, Susan K., Konishi, Ikuo, Mandai, Masaki, and Matsumura, Noriomi

Subjects

OVARIAN cancer, CANCER cells, CANCER genes, GENE silencing, GENE expression

Abstract

Side population (SP) cells harbor malignant phenotypes in cancer. The aim of this study was to identify genes that modulate the proportion of ovarian cancer SP cells. Using a shRNA library targeting 15,000 genes, a functional genomics screen was performed to identify genes whose suppression increased the SP percentage. The biological effects caused by alteration of those identified genes were investigated in vitro and in vivo. We found that suppression of MSL3, ZNF691, VPS45, ITGB3BP, TLE2, and ZNF498 increased the proportion of SP cells. Newly generated SP cells exhibit greater capacity for sphere formation, single cell clonogenicity, and in vivo tumorigenicity. On the contrary, overexpression of MSL3, VPS45, ITGB3BP, TLE2, and ZNF498 decreased the proportion of SP cells, sphere formation capacity and single cell clonogenicity. In ovarian cancer cases, low expression of MSL3, ZNF691 and VPS45 was related to poor prognosis. Suppression of these six genes enhanced activity of the hedgehog pathway. Cyclopamine, a hedgehog pathway inhibitor, significantly decreased the number of SP cells and their sphere forming ability. Our results provide new information regarding molecular mechanisms favoring SP cells and suggest that Hedgehog signaling may provide a viable target for ovarian cancer. [ABSTRACT FROM AUTHOR]

Published

2019