Search

Your search keyword '"Hiroshi Miyamoto"' showing total 961 results
Start Over Author "Hiroshi Miyamoto" Database OpenAIRE
961 results on '"Hiroshi Miyamoto"'

4. Clinical Outcomes of Comprehensive Genomic Profiling Tests for Gastrointestinal Cancers : Experience from Tokushima University Hospital

Author

Yasushi Sato, Yasuyuki Okada, Yasuteru Fujino, Tomoyuki Kawaguchi, Yoshifumi Kida, Yasuhiro Mitsui, Hironori Tanaka, Tetsu Tomonari, Shinji Kitamura, Koichi Okamoto, Yutaka Kawano, Hiroshi Miyamoto, Masahiro Sogabe, and Tetsuji Takayama

Subjects
genotype-matched therapy, General Medicine, Comprehensive genomic profiling, gastrointestinal cancers, General Biochemistry, Genetics and Molecular Biology
Abstract

In Japan, cancer genome profiling (CGP) for cancer patients without standard treatment has been covered by public insurance since June 2019. This study analyzed data of 122 patients with gastrointestinal tumors who underwent CGP to clarify cancer genome medicine’s current status and possible problems at the Tokushima University Hospital. The major types of cancer included pancreatic (n = 30), colorectal (n = 25), biliary tract (n = 15), gastric (n = 11), and hepatocellular carcinoma (n = 8). CGP tests included F1CDx in 70 patients (57%), F1LCDx in 36 (30%), TSO500 in 14 (11%), and NCC Oncopanel in 2 (2%). Actionable gene alterations were identified in 72 patients (59%), but only 5 patients (4%) were treated for pancreatic (n = 1), colorectal (n = 3), and small bowel cancers (n = 1). The main reasons for not receiving genotype-matched therapy included the lack of appropriate drugs or clinical trials that matched the actionable gene alterations (n = 40) and the inability to participate in clinical trials (n = 10). There is still not a sufficient number of patients receiving genotype-matched treatment for gastrointestinal cancers. To promote cancer genome medicine in regional areas, attempts to improve access to genotype-matched therapies are required, as well as to promote the development of new molecular-targeted drugs and clinical trials for these drugs.

Published
2023

5. Two cases of anal squamous cell carcinoma achieving complete response after docetaxel + cisplatin + S-1 (DCS) induction chemotherapy followed by chemoradiation

Author

Megumi Yamasaki, Yasushi Sato, Koichi Okamoto, Akira Fukuya, Tomoyuki Kawaguchi, Kazuyoshi Noda, Kaizo Kagemoto, Yasuhiro Mitsui, Hiroshi Miyamoto, and Tetsuji Takayama

Subjects
Gastroenterology, General Medicine
Abstract

Anal squamous cell carcinoma (ASCC) is an uncommon tumor. However, its incidence is increasing worldwide. Surgical resection of locally advanced cases requires permanent anal prosthesis. Thus, chemoradiotherapy (CRT) is preferred as the first-line treatment; however, high local recurrence rate remains an issue. Here, we describe two cases of locally advanced ASCC treated with docetaxel + cisplatin + S-1 (DCS) followed by CRT with S-1 that showed complete response. The two patients, aged 69 and 65 years, were diagnosed with ASCC (cStage IIIB) at our hospital. Due to extensive lymph node metastases, the patients were treated with triple induction chemotherapy (DCS) followed by CRT with S-1. Positron emission tomography/computed tomography performed six months after starting the treatment showed disappearance of tumors, indicating a complete response. The patients continued to receive S-1 for one year and achieved relapse-free long-term survival since the completion of treatment. Therefore, induction chemotherapy with DCS, prior to CRT with S-1 may benefit patients with locally advanced ASCC.

Published
2022
Full Text
View/download PDF

6. <scp>TIMP1</scp>promotes cell proliferation and invasion capability of right‐sided colon cancers via the<scp>FAK</scp>/Akt signaling pathway

Author

Beibei Ma, Hiroyuki Ueda, Koichi Okamoto, Masahiro Bando, Shota Fujimoto, Yasuyuki Okada, Tomoyuki Kawaguchi, Hironori Wada, Hiroshi Miyamoto, Mitsuo Shimada, Yasushi Sato, and Tetsuji Takayama

Subjects
Cancer Research, Tissue Inhibitor of Metalloproteinase-1, Oncology, Colonic Neoplasms, Humans, General Medicine, Prognosis, Colorectal Neoplasms, Signal Transduction, Cell Proliferation
Abstract

Although right-sided colorectal cancer (CRC) shows a worse prognosis than left-sided CRC, the underlying mechanism remains unclear. We established patient-derived organoids (PDOs) from left- and right-sided CRCs and directly compared cell proliferation and invasion capability between them. We then analyzed the expression of numerous genes in signal transduction pathways to clarify the mechanism of the differential prognosis. Cell proliferation activity and invasion capability in right-sided cancer PDOs were significantly higher than in left-sided cancer PDOs and normal PDOs, as revealed by Cell Titer Glo and transwell assays, respectively. We then used quantitative RT-PCR to compare 184 genes in 30 pathways among right-sided and left-sided cancer and normal PDOs and found that the TIMP1 mRNA level was highest in right-sided PDOs. TIMP1 protein levels were upregulated in right-sided PDOs compared with normal PDOs but was downregulated in left-sided PDOs. TIMP1 knockdown with shRNA significantly decreased cell proliferation activity and invasion capability in right-sided PDOs but not in left-sided PDOs. Moreover, TIMP1 knockdown significantly decreased pFAK and pAkt expression levels in right-sided PDOs but not in left-sided PDOs. A database analysis of The Cancer Genome Atlas revealed that TIMP1 expression in right-sided CRCs was significantly higher than in left-sided CRCs. Kaplan-Meier survival analysis showed significantly shorter overall survival in high-TIMP1 patients versus low-TIMP1 patients with right-sided CRCs but not left-sided CRCs. Our data suggest that TIMP1 is overexpressed in right-sided CRCs and promotes cell proliferation and invasion capability through the TIMP1/FAK/Akt pathway, leading to a poor prognosis. The TIMP1/FAK/Akt pathway can be a target for therapeutic agents in right-sided CRCs.

Published
2022
Full Text
View/download PDF

7. Resveratrol inhibits development of colorectal adenoma via suppression of <scp>LEF1</scp> ; comprehensive analysis with connectivity map

Author

Hironori Wada, Yasushi Sato, Shota Fujimoto, Koichi Okamoto, Masahiro Bando, Tomoyuki Kawaguchi, Hiroshi Miyamoto, Naoki Muguruma, Katsuhisa Horimoto, Yui Matsuzawa, Michihiro Mutoh, and Tetsuji Takayama

Subjects
Adenoma, Mice, Cancer Research, Oncology, Resveratrol, Lymphoid Enhancer-Binding Factor 1, Animals, General Medicine, Colorectal Neoplasms, Wnt Signaling Pathway, Chemoprevention, Rats
Abstract

Although many chemopreventive studies on colorectal tumors have been reported, no effective and safe preventive agent is currently available. We searched for candidate preventive compounds against colorectal tumor comprehensively from United States Food and Drug Administration (FDA)-approved compounds by using connectivity map (CMAP) analysis coupled with in vitro screening with colorectal adenoma (CRA) patient-derived organoids (PDOs). We generated CRA-specific gene signatures based on the DNA microarray analysis of CRA and normal epithelial specimens, applied them to CMAP analysis with 1309 FDA-approved compounds, and identified 121 candidate compounds that should cancel the gene signatures. We narrowed them down to 15 compounds, and evaluated their inhibitory effects on the growth of CRA-PDOs in vitro. We finally identified resveratrol, one of the polyphenolic phytochemicals, as a compound showing the strongest inhibitory effect on the growth of CRA-PDOs compared with normal epithelial PDOs. When resveratrol was administered to Apc

Published
2022
Full Text
View/download PDF

8. Vitamin D Receptor Antagonist MeTC7 Inhibits PD-L1

Author

Moore, Negar Khazan, Emily R. Quarato, Niloy A. Singh, Cameron W. A. Snyder, Taylor Moore, John P. Miller, Masato Yasui, Yuki Teramoto, Takuro Goto, Sabeeha Reshi, Jennifer Hong, Naixin Zhang, Diya Pandey, Priyanka Srivastava, Alexandra Morell, Hiroki Kawano, Yuko Kawano, Thomas Conley, Deepak M. Sahasrabudhe, Naohiro Yano, Hiroshi Miyamoto, Omar Aljitawi, Jane Liesveld, Michael W. Becker, Laura M. Calvi, Alexander S. Zhovmer, Erdem D. Tabdanov, Nikolay V. Dokholyan, David C. Linehan, Jeanne N. Hansen, Scott A. Gerber, Ashoke Sharon, Manoj K. Khera, Peter W. Jurutka, Natacha Rochel, Kyu Kwang Kim, Rachael B. Rowswell-Turner, Rakesh K. Singh, and Richard G.

Subjects
PD-L1, AML, MDS, vitamin D, VDR, small molecule, M2H assay, efferocytosis
Abstract

Small-molecule inhibitors of PD-L1 are postulated to control immune evasion in tumors similar to antibodies that target the PD-L1/PD-1 immune checkpoint axis. However, the identity of targetable PD-L1 inducers is required to develop small-molecule PD-L1 inhibitors. In this study, using chromatin immunoprecipitation (ChIP) assay and siRNA, we demonstrate that vitamin D/VDR regulates PD-L1 expression in acute myeloid leukemia (AML) and myelodysplastic syndrome (MDS) cells. We have examined whether a VDR antagonist, MeTC7, can inhibit PD-L1. To ensure that MeTC7 inhibits VDR/PD-L1 without off-target effects, we examined competitive inhibition of VDR by MeTC7, utilizing ligand-dependent dimerization of VDR-RXR, RXR-RXR, and VDR-coactivators in a mammalian 2-hybrid (M2H) assay. MeTC7 inhibits VDR selectively, suppresses PD-L1 expression sparing PD-L2, and inhibits the cell viability, clonogenicity, and xenograft growth of AML cells. MeTC7 blocks AML/mesenchymal stem cells (MSCs) adhesion and increases the efferocytotic efficiency of THP-1 AML cells. Additionally, utilizing a syngeneic colorectal cancer model in which VDR/PD-L1 co-upregulation occurs in vivo under radiation therapy (RT), MeTC7 inhibits PD-L1 and enhances intra-tumoral CD8+T cells expressing lymphoid activation antigen-CD69. Taken together, MeTC7 is a promising small-molecule inhibitor of PD-L1 with clinical potential.

Published
2023
Full Text
View/download PDF

9. Initial therapeutic results of atezolizumab plus bevacizumab for unresectable advanced hepatocellular carcinoma and the importance of hepatic functional reserve

Author

Tetsu Tomonari, Joji Tani, Yasushi Sato, Hironori Tanaka, Takahiro Tanaka, Tatsuya Taniguchi, Morishita Asahiro, Koichi Okamoto, Masahiro Sogabe, Hiroshi Miyamoto, Naoki Muguruma, Tsutomu Masaki, and Tetsuji Takayama

Subjects
atezolizumab, Cancer Research, Oncology, Radiology, Nuclear Medicine and imaging, hepatocellular carcinoma, bevacizumab
Abstract

Aim: We analyzed the association between the modified albumin–bilirubin (mALBI) grade and therapeutic efficacy of atezolizumab plus bevacizumab (Atezo+Bev) for the treatment of unresectable hepatocellular carcinoma (u-HCC). Methods: In this retrospective observational study, we included 71 u-HCC patients treated with Atezo+Bev between September 2020 and September 2021. Patients were grouped corresponding to the mALBI grade at the start of treatment (mALBI 1+2a or mALBI 2b+3) and analyzed for therapeutic effect and the transition rate to secondary treatment. Results: According to the Response Evaluation Criteria in Solid Tumors, the overall response rate was significantly higher for the mALBI 1+2a group, than for the mALBI 2b+3 group, with 26.2% and 3.4%, respectively. The progression-free survival (PFS) was significantly longer in the mALBI 1+2a group (10.5 months) than in the mALBI 2b+3 group (3.0 months). In the multivariate analysis, an mALBI of 1+2a was found to be an independent factor of PFS. The rate of second-line treatment with multi-targeted agents was also significantly higher in the mALBI 1+2a group. Conclusions: In real-world practice, Atezo+Bev treatment might have higher therapeutic efficacy in u-HCC patients with mALBI 1+2a.

Published
2022

10. Prostatic malakoplakia: clinicopathological assessment of a multi‐institutional series of 49 patients

Author

Andres M Acosta, Ankur R Sangoi, Fiona Maclean, Kiril Trpkov, Adeboye O Osunkoya, Katrina Collins, Hiroshi Miyamoto, Michelle S Hirsch, Emily Chan, Maria Tretiakova, Sambit K Mohanty, Seema Kaushal, Kristine M Cornejo, Manju Aron, Gabriela Quiroga‐Garza, Kanika Arora, Jane K Nguyen, Sean R Williamson, Jonathan I Epstein, and Andres Matoso

Subjects
Male, Prostatectomy, Histology, Malacoplakia, Prostate, Humans, Prostatic Neoplasms, General Medicine, Prostate-Specific Antigen, Magnetic Resonance Imaging, Aged, Pathology and Forensic Medicine
Abstract

Prostatic malakoplakia (MP) is rare, with only case reports and small series ( five patients) available in the literature. In this study we analysed an international multi-institutional series of 49 patients with prostatic MP to more clearly define its clinicopathological features. The median age was 67 years and the median serum prostate-specific antigen (PSA) was 7.5 ng/ml. MP was clinically manifest in most cases (28 of 45 patients with data available, 62%). Of 43 patients with detailed clinical history available, 21 (49%) had concurrent or metachronous malignancies (including prostate cancer). Diabetes or insulin resistance was present in 11 patients (26%). Additionally, three patients had a history of solid organ transplantation and one had HIV. Of note, six of 34 patients (18%) without concurrent prostate cancer had an abnormal digital rectal examination and/or lesions on magnetic resonance imaging (MRI) with prostate imaging reporting and data system (PIRADS) scores 4-5. The initial diagnosis was made on core biopsies (25 of 49, 51%), transurethal resection specimens (12 of 49, 24%), radical prostatectomies (10 of 49, 20%), Holmium-laser enucleation (one of 49, 2%) and cystoprostatectomy (one of 49, 2%). Tissue involvement was more commonly diffuse or multifocal (40 of 49, 82%). Von Kossa and periodic acid-Schiff stains were positive in 35 of 38 (92%) and 26 of 27 lesions (96%), respectively. Of note, two cases were received in consultation by the authors with a preliminary diagnosis of mesenchymal tumour/tumour of the specialised prostatic stroma. The present study suggests that prostatic MP is often associated with clinical findings that may mimic those of prostate cancer in a subset of patients. Moreover, MP may be found incidentally in patients with concurrent prostate cancer.

Published
2022
Full Text
View/download PDF

12. A Novel CT-Based Radiomics Model for Predicting Response and Prognosis of Chemoradiotherapy in Esophageal Squamous Cell Carcinoma

Author

Akinari Kasai, Jinsei Miyoshi, Yasushi Sato, Koichi Okamoto, Hiroshi Miyamoto, Takashi Kawanaka, Masafumi Harada, Masakazu Goto, Takahiro Yoshida, Akihiro Haga, and Tetsuji Takayama

Abstract

No clinically relevant biomarker has been identified for predicting the response of esophageal squamous cell carcinoma (ESCC) to chemoradiotherapy (CRT). Herein, we established a CT-based radiomics model with artificial intelligence (AI) to predict the response and prognosis of CRT in ESCC. A total of 44 ESCC patients (stage I-IV) were enrolled in this study; training (n = 27) and validation (n = 17) cohorts. First, we extracted a total of 476 radiomics features from three-dimensional CT images of cancer lesions in training cohort, selected 110 features associated with the CRT response by ROC analysis (AUC ≥ 0.7) and identified 12 independent features, excluding correlated features by Pearson’s correlation analysis (r ≥ 0.7). Based on the 12 features, we constructed 5 prediction models of different machine learning algorithms (Random Forest (RF), Ridge Regression, Naive Bayes, Support Vector Machine, and Artificial Neural Network models). Among those, the RF model showed the highest AUC in the training cohort (0.99, p

Published
2023
Full Text
View/download PDF

13. Supplementary Figure S1 from Nuclear Factor-κB Promotes Urothelial Tumorigenesis and Cancer Progression via Cooperation with Androgen Receptor Signaling

Author

Hiroshi Miyamoto, Momokazu Gotoh, George J. Netto, Guiyang Jiang, Taichi Mizushima, Hiroki Ide, and Satoshi Inoue

Abstract

Relationship between the expression levels of NF-κB/p65 versus p-NF-κB/p65 (A), AR versus NF-κB/p65 (B), and AR versus p-NF-κB/p65 (C) in bladder tumor specimens. Scatter plots show the distribution of IHC scores (0/1+/2+/3+) of two proteins. The Spearman's correlation coefficient (CC) and P value are indicated in each dot plot.

Published
2023
Full Text
View/download PDF

18. Figure S7 from Androgen Receptor Signaling Reduces the Efficacy of Bacillus Calmette-Guérin Therapy for Bladder Cancer via Modulating Rab27b-Induced Exocytosis

Author

Hiroshi Miyamoto, Leonardo O. Reis, Mitsunori Fukuda, Etsuko Miyagi, Mehrsa Jalalizadeh, Ikuma Kato, Hiroki Ide, Satoshi Inoue, Bin Han, Peng Li, Takashi Kawahara, Guiyang Jiang, and Taichi Mizushima

Abstract

Representative histological images of mouse xenografts of MB49-derived sublines.

Published
2023
Full Text
View/download PDF

20. Data from Androgen Receptor Signaling Reduces the Efficacy of Bacillus Calmette-Guérin Therapy for Bladder Cancer via Modulating Rab27b-Induced Exocytosis

Author

Hiroshi Miyamoto, Leonardo O. Reis, Mitsunori Fukuda, Etsuko Miyagi, Mehrsa Jalalizadeh, Ikuma Kato, Hiroki Ide, Satoshi Inoue, Bin Han, Peng Li, Takashi Kawahara, Guiyang Jiang, and Taichi Mizushima

Abstract

Although intravesical bacillus Calmette-Guérin (BCG) immunotherapy has been the gold standard for nonsurgical management of non–muscle-invasive bladder cancer, a considerable number of patients exhibit resistance to the adjuvant treatment with unexplained mechanisms. This study aimed to investigate whether and how androgen receptor (AR) signals modulate BCG cytotoxicity in bladder cancer. AR knockdown or overexpression in bladder cancer lines resulted in induction or reduction, respectively, in intracellular BCG quantity and its cytotoxic activity. Microarray screening identified Rab27b, a small GTPase known to mediate bacterial exocytosis, which was upregulated in BCG-resistant cells and downregulated in AR-shRNA cells. Knockdown of Rab27b, or its effector SYTL3, or overexpression of Rab27b also induced or reduced, respectively, BCG quantity and cytotoxicity. In addition, treatment with GW4869, which was previously shown to inhibit Rab27b-dependent secretion, induced them and reduced Rab27b expression in bladder cancer cells. Meanwhile, AR expression was upregulated in BCG-resistant lines, compared with respective controls. In a mouse orthotopic xenograft model, Rab27b/SYTL3 knockdown or GW4869 treatment enhanced the amount of BCG within tumors and its suppressive effect on tumor growth. Moreover, in non–muscle-invasive bladder cancer specimens from patients subsequently undergoing BCG therapy, positivity of AR/Rab27b expression was associated with significantly higher risks of tumor recurrence. AR activation thus correlates with resistance to BCG treatment, presumably via upregulating Rab27b expression. Mechanistically, it is suggested that BCG elimination from urothelial cells is induced by Rab27b/SYTL3-mediated exocytosis. Accordingly, Rab27b inactivation, potentially via antiandrogenic drugs and/or exocytosis inhibition are anticipated to sensitize the efficacy of BCG therapy, especially in patients with BCG-refractory AR/Rab27b-positive bladder cancer.

Published
2023
Full Text
View/download PDF

22. Data from Nuclear Factor-κB Promotes Urothelial Tumorigenesis and Cancer Progression via Cooperation with Androgen Receptor Signaling

Author

Hiroshi Miyamoto, Momokazu Gotoh, George J. Netto, Guiyang Jiang, Taichi Mizushima, Hiroki Ide, and Satoshi Inoue

Abstract

We investigated the role of NF-κB in the development and progression of urothelial cancer as well as cross-talk between NF-κB and androgen receptor (AR) signals in urothelial cells. Immunohistochemistry in surgical specimens showed that the expression levels of NF-κB/p65 (P = 0.015)/phospho-NF-κB/p65 (P < 0.001) were significantly elevated in bladder tumors, compared with those in nonneoplastic urothelial tissues. The rates of phospho-NF-κB/p65 positivity were also significantly higher in high-grade (P = 0.015)/muscle-invasive (P = 0.033) tumors than in lower grade/non–muscle-invasive tumors. Additionally, patients with phospho-NF-κB/p65-positive muscle-invasive bladder cancer had significantly higher risks of disease progression (P < 0.001) and cancer-specific mortality (P = 0.002). In immortalized human normal urothelial SVHUC cells stably expressing AR, NF-κB activators and inhibitors accelerated and prevented, respectively, their neoplastic transformation induced by a chemical carcinogen 3-methylcholanthrene. Bladder tumors were identified in 56% (mock), 89% (betulinic acid), and 22% (parthenolide) of N-butyl-N-(4-hydroxybutyl)nitrosamine-treated male C57BL/6 mice at 22 weeks of age. NF-κB activators and inhibitors also significantly induced and reduced, respectively, cell proliferation/migration/invasion of AR-positive bladder cancer lines, but not AR-knockdown or AR-negative lines, and their growth in xenograft-bearing mice. In both nonneoplastic and neoplastic urothelial cells, NF-κB activators/inhibitors upregulated/downregulated, respectively, AR expression, whereas AR overexpression was associated with increases in the expression levels of NF-κB/p65 and phospho-NF-κB/p65. Thus, NF-κB appeared to be activated in bladder cancer, which was associated with tumor progression. NF-κB activators/inhibitors were also found to modulate tumorigenesis and tumor outgrowth in AR-activated urothelial cells. Accordingly, NF-κB inhibition, together with AR inactivation, has the potential of being an effective chemopreventive and/or therapeutic approach for urothelial carcinoma. Mol Cancer Ther; 17(6); 1303–14. ©2018 AACR.

Published
2023
Full Text
View/download PDF

26. Data from Androgen Receptor Signaling Reduces Radiosensitivity in Bladder Cancer

Author

Hiroshi Miyamoto, Mototsugu Oya, Kuang-Hsiang Chuang, Guiyang Jiang, Taichi Mizushima, Satoshi Inoue, and Hiroki Ide

Abstract

Although radiotherapy often with chemotherapy has been shown to offer a survival benefit comparable with that of radical cystectomy in select patients with bladder cancer, the development of radiosensitization strategies may significantly enhance its application. Notably, emerging preclinical evidence has indicated the involvement of androgen receptor (AR) signaling in urothelial cancer progression. We here assessed whether AR signals could contribute to modulating radiosensitivity in bladder cancer cells. Ionizing radiation reduced the numbers of viable cells or colonies of AR-negative lines more significantly than those of AR-positive lines. Similarly, in AR-positive cells cultured in androgen-depleted conditions, dihydrotestosterone treatment lowered the effects of irradiation. Meanwhile, an antiandrogen hydroxyflutamide enhanced them in AR-positive cells cultured in the presence of androgens. AR knockdown or hydroxyflutamide treatment also resulted in a delay in DNA double-strand break repair 4–24 hours after irradiation. We then established “radiation-resistant” sublines and found considerable elevation of the expression of AR as well as DNA repair genes, such as ATR, CHEK1, and PARP-1, in these sublines, compared with respective controls. Furthermore, dihydrotestosterone induced the expression of these DNA repair genes in irradiated AR-positive cells, and hydroxyflutamide antagonized the androgen effects. Finally, in a mouse xenograft model, low-dose flutamide was found to enhance the inhibitory effects of irradiation, and its tumor size was similar to that of AR knockdown line with radiation alone. These findings suggest that AR activity inversely correlates with radiosensitivity in bladder cancer. Accordingly, antiandrogenic drugs may function as sensitizers of irradiation, especially in patients with AR-positive urothelial cancer. Mol Cancer Ther; 17(7); 1566–74. ©2018 AACR.

Published
2023
Full Text
View/download PDF

27. Figure S3 from Androgen Receptor Signaling Reduces the Efficacy of Bacillus Calmette-Guérin Therapy for Bladder Cancer via Modulating Rab27b-Induced Exocytosis

Author

Hiroshi Miyamoto, Leonardo O. Reis, Mitsunori Fukuda, Etsuko Miyagi, Mehrsa Jalalizadeh, Ikuma Kato, Hiroki Ide, Satoshi Inoue, Bin Han, Peng Li, Takashi Kawahara, Guiyang Jiang, and Taichi Mizushima

Abstract

Effects of Rab27b knockdown or overexpression on BCG cytotoxicity in bladder cancer cells.

Published
2023
Full Text
View/download PDF

29. Supplementary Figure S4 from Nuclear Factor-κB Promotes Urothelial Tumorigenesis and Cancer Progression via Cooperation with Androgen Receptor Signaling

Author

Hiroshi Miyamoto, Momokazu Gotoh, George J. Netto, Guiyang Jiang, Taichi Mizushima, Hiroki Ide, and Satoshi Inoue

Abstract

Effects of NF-κB activation/inhibition on bladder cancer cell growth. MTT assay was performed in: UMUC3 cells cultured in media containing charcoal-stripped FBS (CS-FBS) with ethanol (mock), BA (10 μM), or PAR (10 μM) (A); UMUC3 cells cultured in media containing CS-FBS with DHT (10 nM) and ethanol (mock), BA (10 μM), or PAR (10 μM) (C); UMUC3 cells cultured in media containing normal FBS with ethanol (mock), TNF-α (20 ng/mL), or DHMEQ (10 µg/mL) (E); or UMUC3-control-shRNA or UMUC3-NF-κB-shRNA cells cultured in media containing normal FBS (G) for 72 hours. Cell viability is presented relative to that of mock treatment or control-shRNA. Wound-healing assay was performed in: UMUC3 cells cultured in media containing charcoal-stripped FBS (CS-FBS) with ethanol (mock), BA (10 μM), or PAR (10 μM) (B); UMUC3 cells cultured in media containing CS-FBS with DHT (10 nM) and ethanol (mock), BA (10 μM), or PAR (10 μM) (D); UMUC3 cells cultured in media containing normal FBS with ethanol (mock), TNF-α (20 ng/mL), or DHMEQ (10 µg/mL) (F); or UMUC3-control-shRNA or UMUC3-NF-κB-shRNA cells cultured in media containing normal FBS (H). The cells grown to confluence were gently scratched and the wound area was measured after 18-hour culture. The migration determined by the rate of cells filling the wound area is presented relative to that of each line with mock treatment or control-shRNA. Each value represents the mean (+SD) from three independent experiments. *P

Published
2023
Full Text
View/download PDF

30. Figure S6 from Androgen Receptor Signaling Reduces the Efficacy of Bacillus Calmette-Guérin Therapy for Bladder Cancer via Modulating Rab27b-Induced Exocytosis

Author

Hiroshi Miyamoto, Leonardo O. Reis, Mitsunori Fukuda, Etsuko Miyagi, Mehrsa Jalalizadeh, Ikuma Kato, Hiroki Ide, Satoshi Inoue, Bin Han, Peng Li, Takashi Kawahara, Guiyang Jiang, and Taichi Mizushima

Abstract

Effects of Rab27b overexpression or knockdown on the expression of AR, Rab27a, and SYTL3, as well as fibronectin/integrin and macropinocytosis-related molecules, in bladder cancer cells.

Published
2023
Full Text
View/download PDF

32. Figure S4 from Androgen Receptor Signaling Reduces the Efficacy of Bacillus Calmette-Guérin Therapy for Bladder Cancer via Modulating Rab27b-Induced Exocytosis

Author

Hiroshi Miyamoto, Leonardo O. Reis, Mitsunori Fukuda, Etsuko Miyagi, Mehrsa Jalalizadeh, Ikuma Kato, Hiroki Ide, Satoshi Inoue, Bin Han, Peng Li, Takashi Kawahara, Guiyang Jiang, and Taichi Mizushima

Abstract

Effects of Rab27b/SYTL3 knockdown or GW4869 treatment on the proliferation of bladder cancer cells.

Published
2023
Full Text
View/download PDF

34. Supplementary Figure 1 from Contrary Regulation of Bladder Cancer Cell Proliferation and Invasion by Dexamethasone-Mediated Glucocorticoid Receptor Signals

Author

Hiroshi Miyamoto, Hitoshi Ishiguro, Yi Li, Koji Izumi, and Yichun Zheng

Abstract

PDF file - 5939K, The expression of GR in human BC. A, GR mRNA expression was analyzed in UMUC3, TCC-SUP, J82, and 5637 cells by RT-PCR, and transcripts (163 bp) were separated on an agarose gel. PCR products derived from GAPDH mRNA (71 bp) served as an internal control. B, Cell extracts from UMUC3, TCC-SUP, J82, and 5637 were analyzed on western blotting, using an antibody to GR (95 kDa, with a second band at 90 kDa). β-Actin protein (43 kDa) served as an internal control. C, Immunohistochemistry (IHC) of GR in bladder TMA, including benign urothelium, primary urothelial carcinoma, and lymph node (LN) metastasis. The Kaplan-Meier analysis was performed to assess progression-free survival in patients with BC, according to the levels of GR expression. Comparison was made by log-rank test. Tumor progression was defined as development of local recurrence or metastatic tumor.

Published
2023
Full Text
View/download PDF

39. Data from Contrary Regulation of Bladder Cancer Cell Proliferation and Invasion by Dexamethasone-Mediated Glucocorticoid Receptor Signals

Author

Hiroshi Miyamoto, Hitoshi Ishiguro, Yi Li, Koji Izumi, and Yichun Zheng

Abstract

In patients with advanced bladder cancer, glucocorticoids are frequently given to reduce acute toxicity, particularly hyperemesis, during chemotherapy, as well as to improve cachectic conditions. However, it remains unclear whether glucocorticoids directly affect the development and progression of bladder cancer through the glucocorticoid receptor pathway. Glucocorticoid receptor expression was first investigated in human bladder cancer lines and tissue microarrays. Then, the effects of dexamethasone on glucocorticoid receptor transcription, cell proliferation, apoptosis/cell cycle, and invasion were examined in bladder cancer lines. Finally, mouse xenograft models for bladder cancer were used to assess the efficacy of dexamethasone on tumor progression. All the cell lines and tissues examined were found to express glucocorticoid receptor. Dexamethasone increased glucocorticoid receptor–mediated reporter activity and cell proliferation, and inhibited apoptosis in the presence or absence of cisplatin. In contrast, dexamethasone suppressed cell invasion, the expression of its related genes [MMP-2/MMP-9, interleukin (IL)-6, VEGF], and the activity of MMP-2/MMP-9, and also induced mesenchymal-to-epithelial transition. In addition, dexamethasone increased IκBα protein levels and cytosolic accumulation of NF-κB. In xenograft-bearing mice, dexamethasone slightly augmented the growth of the inoculated tumors but completely prevented the development of bloody ascites, suggestive of peritoneal dissemination of tumor cells, and actual metastasis. In all these assays, dexamethasone effects were abolished by a glucocorticoid receptor antagonist or glucocorticoid receptor knockdown via RNA interference. Thus, glucocorticoid receptor activation resulted in promotion of cell proliferation via inhibiting apoptosis yet repression of cell invasion and metastasis. These results may provide a basis of developing improved chemotherapy regimens, including or excluding glucocorticoid receptor agonists/antagonists, for urothelial carcinoma. Mol Cancer Ther; 11(12); 2621–32. ©2012 AACR.

Published
2023
Full Text
View/download PDF

40. Figure S5 from Androgen Receptor Signaling Reduces the Efficacy of Bacillus Calmette-Guérin Therapy for Bladder Cancer via Modulating Rab27b-Induced Exocytosis

Author

Hiroshi Miyamoto, Leonardo O. Reis, Mitsunori Fukuda, Etsuko Miyagi, Mehrsa Jalalizadeh, Ikuma Kato, Hiroki Ide, Satoshi Inoue, Bin Han, Peng Li, Takashi Kawahara, Guiyang Jiang, and Taichi Mizushima

Abstract

Effects of Rab27b overexpression on BCG cytotoxicity in bladder cancer cells.

Published
2023
Full Text
View/download PDF

45. Supplementary Figures from Infiltrating Macrophages Promote Prostate Tumorigenesis via Modulating Androgen Receptor-Mediated CCL4–STAT3 Signaling

Author

Chawnshang Chang, Wen-Jye Lin, Hiroshi Miyamoto, Lei Li, Liang Liang, Kuo-Pao Lai, Kouji Izumi, and Lei-Ya Fang

Abstract

PDF file, 1659K, S1. Effects of THP-1 on cell migration, acinar morphogenesis, and downstream signaling in BPH-1 cells. S2. H&E staining of the anterior prostate from athymic nude mice 60 days after orthoptoic injection of either THP-1 or RWPE-1 cells. S3. Elevated pSTAT3 in mouse prostate epithelial cells (mPrE) after co-culture with mouse macrophages. S4. THP-1 cells were cultured alone for 48 hrs, and the expressions of cytokines were determined by a human cytokine array (R&D Systems). S5. qPCR (A) and Western blot analysis (B) of p53 and PTEN expression levels in RWPE-1 cells and RWPE-1/THP-1 cells after long term co-culture for 5 days. S6. The role of CCL4 and macrophage AR in the modulation of EMT markers and CCR1 expression in RWPE-1 cells. S7. Effects of macrophages AR silencing on BPH-1 cells during co-culture. S8. Generation and confirmation of MARKO/PTEN+/- mice. S9. CCL4 expression in prostate cancer does not associate with pathologic stage, lymph node metastasis, and recurrent-free survival. S10. IHC Staining of Mouse PTEN knockout prostate using an anti-Snail antibody.

Published
2023
Full Text
View/download PDF

48. The Clinical Impact of Comedonecrosis Within Intraductal Carcinoma of the Prostate

Author

Ying, Wang, Yuki, Teramoto, Samuel J, Weisenthal, Takuro, Goto, and Hiroshi, Miyamoto

Subjects
body regions, Medical Laboratory Technology, General Medicine, skin and connective tissue diseases, neoplasms, Pathology and Forensic Medicine
Abstract

Context.— Intraductal carcinoma of the prostate (IDC-P) is considered a distinct form of aggressive prostate cancer where comedonecrosis, a grade 5 pattern, is occasionally present. Meanwhile, assigning a Gleason grade to IDC-P remains controversial. Objective.— To assess the clinical significance of necrosis associated with IDC-P. Design.— We compared radical prostatectomy (RP) findings and oncologic outcomes in men with prostate cancer exhibiting IDC-P with (IDC-P+/N+) versus without (IDC-P+/N−) comedonecrosis. Results.— Of the 558 RPs examined, IDC-P was present in 213 cases (38.2%), including 167 (78.4%) with IDC-P+/N− and 46 (21.6%) with IDC-P+/N+. When comparing IDC-P+/N− versus IDC-P+/N+ cases, the presence of necrosis was significantly associated with higher tumor grade, higher incidence of pT3/pT3b or pN1 disease, and larger estimated tumor volume. Outcome analysis revealed a significantly higher risk of disease progression in IDC-P+/N+ patients than in IDC-P+/N− patients (P < .001). Significant differences in progression-free survival between IDC-P+/N− and IDC-P+/N+ patients were also seen in subgroups, such as those without (P = .01) or with (P = .03) adjuvant therapy immediately after RP, those with pN0 disease (P < .001), and, more interestingly, those exhibiting conventional Gleason pattern 5 component (P = .02). Multivariate analysis showed significance for IDC-P+/N+ when IDC-P (grade 4) and IDC-P+/N+ (grade 5) were (hazard ratio, 1.768; P = .049) or were not (hazard ratio, 2.000; P = .008) incorporated into the Gleason score. Conclusions.— IDC-P+/N+ was found to be associated with worse histopathologic features on RP and poorer prognosis as an independent predictor. Pathologists may thus need to report the presence or absence of not only IDC-P but also comedonecrosis within IDC-P.

Published
2022
Full Text
View/download PDF

49. Prognostic significance of NY-ESO-1 antigen and PIGR expression in esophageal tumors of CHP-NY-ESO-1-vaccinated patients as adjuvant therapy

Author

Yasuhiro Nagata, Shinichi Kageyama, Takeshi Ishikawa, Satoshi Kokura, Tetsuya Okayama, Tetsuya Abe, Masahiko Murakami, Koji Otsuka, Tomotake Ariyoshi, Takashi Kojima, Ken Taniguchi, Shinichiro Kobayashi, Hideaki Shimada, Satoshi Yajima, Takashi Suzuki, Satoshi Hirano, Takahiro Tsuchikawa, Toshiaki Shichinohe, Shugo Ueda, Kengo Kanetaka, Akira Yoneda, Hisashi Wada, Yuichiro Doki, Hiroki Yamaue, Masahiro Katsuda, Masaki Ohi, Hiromi Yasuda, Ken Kondo, Masato Kataoka, Yasuhiro Kodera, Masahiko Koike, Taizo Shiraishi, Yoshihiro Miyahara, Naoki Goshima, Eriko Fukuda, Kei Yamaguchi, Eiichi Sato, Hiroaki Ikeda, Tomomi Yamada, Masaharu Osako, Kaoru Hirai, Hiroshi Miyamoto, Takashi Watanabe, and Hiroshi Shiku

Subjects
Cancer Research, Esophageal Neoplasms, Antibodies, Neoplasm, Immunology, Receptors, Polymeric Immunoglobulin, Membrane Proteins, Prognosis, Cancer Vaccines, Immunoglobulin A, Oncology, Antigens, Neoplasm, Immunoglobulin G, Humans, Immunology and Allergy, Esophageal Squamous Cell Carcinoma, Fluorouracil, Cisplatin, Glucans
Abstract

The aim of this study was to determine the efficacy and the biomarkers of the CHP-NY-ESO-1 vaccine complexed with full-length NY-ESO-1 protein and a cholesteryl pullulan (CHP) in patients with esophageal squamous cell carcinoma (ESCC) after surgery. We conducted a randomized phase II trial. Fifty-four patients with NY-ESO-1-expressing ESCC who underwent radical surgery following cisplatin/5-fluorouracil-based neoadjuvant chemotherapy were assigned to receive either CHP-NY-ESO-1 vaccination or observation as control. Six doses of CHP-NY-ESO-1 were administered subcutaneously once every two weeks, followed by nine more doses once every four weeks. The endpoints were disease-free survival (DFS) and safety. Exploratory analysis of tumor tissues using gene-expression profiles was also performed to seek the biomarker. As there were no serious adverse events in 27 vaccinated patients, we verified the safety of the vaccine. DFS in 2 years were 56.0% and 58.3% in the vaccine arm and in the control, respectively. Twenty-four of 25 patients showed NY-ESO-1-specific IgG responses after vaccination. Analysis of intra-cohort correlations among vaccinated patients revealed that 5% or greater expression of NY-ESO-1 was a favorable factor. Comprehensive analysis of gene expression profiles revealed that the expression of the gene encoding polymeric immunoglobulin receptor (PIGR) in tumors had a significantly favorable impact on outcomes in the vaccinated cohort. The high PIGR-expressing tumors that had higher NY-ESO-1-specific IgA response tended to have favorable prognosis. These results suggest that PIGR would play a major role in tumor immunity in an antigen-specific manner during NY-ESO-1 vaccinations. The IgA response may be relevant.

Published
2022
Full Text
View/download PDF

50. Clinicopathologic Spectrum of Secondary Solid Tumors of the Prostate of Nonurothelial Origin

Author

Andres M. Acosta, Jennifer B. Gordetsky, Katrina Collins, Adeboye O. Osunkoya, Ankur R. Sangoi, Hiroshi Miyamoto, Chia-Sui Kao, Kiril Trpkov, Geert J.L.H. Van Leenders, Sara E. Wobker, Fiona Maclean, Priti Lal, Reba E. Daniel, Fadi Brimo, Matthew Wasco, Michelle S. Hirsch, Nicholas Baniak, Julio A. Diaz-Perez, Kristine M. Cornejo, Bonnie Choy, Rohit Mehra, Sean R. Williamson, Jonathan I. Epstein, Andres Matoso, and Pathology

Subjects
Male, Prostate, Humans, Prostatic Neoplasms, Surgery, Adenocarcinoma, Neoplasms, Germ Cell and Embryonal, Anatomy, Colorectal Neoplasms, Pathology and Forensic Medicine
Abstract

Secondary involvement of the prostate by urothelial or hematolymphoid neoplasms is relatively common and well-described. In contrast, less is known about the clinicopathologic spectrum of secondary solid tumors of the prostate of nonurothelial origin. This study evaluated a series of secondary nonurothelial solid tumors of the prostate diagnosed at 21 institutions. Eighty-five patients with a median age at diagnosis of 64 years were included. Sixty-two patients had clinically manifest disease (62/85, 73%), 10 were diagnosed incidentally (10/85, 12%), and 13 (13/85, 15%) had no detailed clinical data available about symptomatology at presentation. Among patients with clinically manifest disease, the most common symptoms and signs were lower urinary tract symptoms (either obstructive of irritative; 36/62, 58%), abdominal or pelvic pain or discomfort (16/62, 26%), and hematuria (12/62, 19%). Metastasis and direct invasion occurred at roughly similar frequencies (47% vs. 42%) in this series, and in 11% of the cases, the mechanism of spread to the prostate was unclear/uncertain. Overall, among tumors with confirmed sites of origin, the most common primary sites were gastrointestinal tract (53/85, 62%), lung (9/85, 11%), skin (6/85, 7%), and testis (4/85, 5%). Among metastases, the most common tumor types were lung carcinomas (9/40, 23%), colorectal adenocarcinomas (7/40, 18%), melanoma (6/40, 15%), and germ cell tumors (6/40, 15%). This study demonstrated that secondary involvement of the prostate by solid tumors of nonurothelial origin is commonly symptomatic and that the most frequent sites of origin are the gastrointestinal tract, lung, skin, and testis. These findings are worth considering when lesions with unusual cytomorphology and/or architecture are encountered in prostate specimens.

Published
2022
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results