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Featured researches published by Nobuko Serizawa.


International Journal of Oncology | 2014

Phase I clinical trial of peptide vaccination with URLC10 and VEGFR1 epitope peptides in patients with advanced gastric cancer

Yoshie Higashihara; Junko Kato; Akihito Nagahara; Kentaro Izumi; Masae Konishi; Tomohiro Kodani; Nobuko Serizawa; Taro Osada; Sumio Watanabe

Peptide vaccine treatment has attracted attention in recent years as a new therapy option for chemotherapy-resistant, advanced, unresectable cancer. The safety of peptide vaccination with HLA-A*2402-restricted URLC10-A24-177 and VEGFR1-A12-9 1084 epitope peptides (fixed 2-mg dose) was investigated in a phase I clinical trial of patients with advanced gastric cancer who were refractory to chemotherapy. We determined the HLA genotype of the subjects after enrollment, results of which were held by the evaluation committee and kept from both patients and investigators until completion of the study. The primary end-point was safety of the peptide vaccination. The secondary end-points were immunological responses and clinical outcome, which were compared between the HLA-A*2402-positive and HLA-A*2402-negative groups. The peptides were subcutaneously administered on day 1, 8, 15 and 22 within a 28-day treatment cycle. A total of 14 patients was enrolled in this study; 12 of the 14 patients received 4 or more vaccinations (at least 1 course). No patient had a severe treatment-related adverse event. Findings from evaluation of clinical responses after a single course showed that 4 cases had stable disease and 8 cases had progressive disease. The median overall survival time (MST) for the 12 patients was 3.9 months. The MSTs in the HLA-A*2402-positive and HLA-A*2402-negative groups were, 4.2 and 3.6 months (p= 0.9164), respectively. The results of this study showed that vaccination with URLC10 and VEGFR1 peptides was a safe treatment for advanced gastric cancer. This trial was registered with University Hospital Medical Information Network (UMIN, no. 000002409).


Journal of Gastroenterology and Hepatology | 2007

Orthotopic hepatocellular carcinoma model with a controlled and reproducible tumorigenicity

Hironao Okubo; Yoshiyuki Takei; Nobuko Serizawa; Nobuyuki Enomoto; Kenichi Ikejima; Nobuhiro Sato

Background:  To explore therapeutic strategies for hepatocellular carcinoma (HCC) there is a need for a suitable and reproducible animal model. However, most models produced thus far have drawbacks such as high rates of artificial tumor dissemination and complexity of the implantation technique. To circumvent these issues, we selected an appropriate HCC cell line coupled with a simple modality to prevent unintended tumor cell dissemination.


Advances in Medical Sciences | 2010

Phase I study of Paclitaxel, Cisplatin and 5-fluorouracil combination chemotherapy for unresectable / recurrent gastric cancer

Junko Kato; Akihito Nagahara; Katsuyori Iijima; Tomohiro Kodani; Yoshie Higashihara; Miho Yoshimura; Nobuko Serizawa; Taro Osada; Takashi Yoshizawa; Michiro Otaka; Sumio Watanabe

PURPOSE We investigated the safety of triple combination therapy by addition of Paclitaxel (PTX) to Cisplatin (CDDP) and 5-fluorouracil (5-FU) combination therapy, which was considered the conventional standard therapy for patients with unresectable / recurrent gastric cancer. MATERIAL AND METHODS The doses of PTX and CDDP were fixed at 80 and 50 mg/m2. They were administered on days 1 and 8, followed by a resting period of 20 days. 5-FU 300 mg/m2 at a maximum dose of 500 mg/m2 was administered at levels 0 and 2, respectively, and the dose was increased by 100 mg/m2 until the maximum tolerated dose (MTD). It was administered on days 1 - 5 and 8 - 12, followed by a resting period of 16 days. RESULTS Twelve patients enrolled in this study. Of them, three patients were excluded from evaluation because treatment continuation was not feasible. There were 4 leukopenia and 7 neutropenia cases with hematological toxicity at grade 3 or higher. They were observed at all dose levels, but no case showed infection. In terms of non-hematological toxicity at grade 3 or higher, there were two patients with nausea and vomiting and two patients with diarrhea, one patient with mucositis, one patient with anorexia. All patients with non-hematological toxicity at grade 3 or higher were at level 2. The dose-limiting toxicity (DLT) was observed at level 2, and 5-FU at 400 mg (level 1) was adopted. CONCLUSIONS We proved in this study that PTX, CDDP, and 5-FU combination chemotherapy was a safe treatment.


Medical Science Monitor | 2010

Response to chemotherapy in a case of gastric adenocarcinoma producing granulocyte colony-stimulating factor

Hiroki Mori; Tomoyoshi Shibuya; Taro Osada; Tomohiro Kodani; Yoshie Higashihara; Nobuko Serizawa; Junko Kato; Akihito Nagahara; Tatsuo Ogihara; Sumio Watanabe


Hepatology Research | 2006

Effect of low-molecular-weight heparin on the commitment of bone marrow cells to liver sinusoidal endothelial cells in CCl4-induced liver injury

Nobuko Serizawa; Yoshiyuki Takei; Hironao Okubo; Shunhei Yamasina; Nobuyuki Enomoto; Nobuhiro Sato


Journal of Clinical Oncology | 2015

Management tips for the low incidence, of adverse events and well efficacy of regorafenib for metastatic colorectal cancer in Juntendo University Medical Hospital.

Yoshie Higashihara; Nobuko Serizawa; Junko Kato; Tomohiro Kodani; Taro Osada; Akihito Nagahara; Sumio Watanabe


Gastroenterology | 2015

Tu1951 Pancreatoblastoma in an Adult: Case Report

Kentaro Izumi; Akihito Nagahara; Hirofumi Fukushima; Yuji Shimada; Yoshie Higashihara; Nobuko Serizawa; Junko Kato; Taro Osada; Takashi Yao; Sumio Watanabe


Juntendo Medical Journal | 2014

Summary of Gastrointestinal Cancer Chemotherapy Symposium on August 5, 2014. "Fudan University - Juntendo University"

Sumio Watanabe; Nobuko Serizawa; Jin Kan Sai; Yang Jianwei; Shunsuke Kato


Gastroenterology | 2013

Tu1606 Galectin-3 Regulates Gastric Cancer Cell Proliferation Through EGFR Signaling Pathway.

Nobuko Serizawa; Akihito Nagahara; Shunhei Yamashina; Gentaro Taniguchi; Sumio Watanabe


Gastroenterology | 2012

Mo1559 Phase I Clinical Trial of Peptide Vaccination With Urlc10 and VEGFR1 Epitope Peptides in Patients With Advanced Gastric Cancer

Yoshie Higashihara; Junko Kato; Nobuko Serizawa; Tomohiro Kodani; Masae Konishi; Taro Osada; Takashi Yoshizawa; Akihito Nagahara; Sumio Watanabe

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