研究者業績

安藤 洋介

アンドウ ヨウスケ  (Yosuke Ando)

基本情報

所属
藤田医科大学 薬物治療情報学 講師

研究者番号
00812215
ORCID ID
 https://orcid.org/0000-0001-8166-8165
J-GLOBAL ID
202301008464538088
researchmap会員ID
R000059639

論文

 20
  • Seira Nishibe-Toyosato, Yosuke Ando, Yutaka Torii, Ryoko Ichikawa, Akiko Owaki, Hironori Miyamura, Eiji Nishio, Hidezo Matsuda, Naho Tsujii-Fujii, Akane Shimato-Isobe, Kotone Mukaiji, Kaori Ito, Takahiro Hayashi, Takuma Fujii, Shigeki Yamada
    In vivo (Athens, Greece) 38(5) 2374-2382 2024年9月  査読有り責任著者
    BACKGROUND/AIM: The frequency rate of injection site reactions (ISR) due to fosaprepitant meglumine (Fos APR) has been shown to vary depending on the types of combined anticancer drug. This study aimed to elucidate the impact of Fos APR on ISR in patients receiving paclitaxel and carboplatin, with and without bevacizumab therapy (TC±Bev). PATIENTS AND METHODS: This study focused on patients with gynecologic cancer (n=93) who received TC±Bev administration at Fujita Health University Hospital from March 2016 to February 2020, and monitored up to six cycles. The patients were randomly assigned to the Fos APR group (n=47) and the Aprepitant (APR) group (n=46). Using Visual Infusion Phlebitis (VIP) scores, ISR was evaluated by comparing the VIP scores of all cycles using a linear mixed model. The risk factors that contribute to the occurrence of vascular pain throughout all cycles were also examined. RESULTS: The VIP scores of all cycles showed a near significant intergroup difference (p=0.071). Factors that affected the development of vascular pain included Fos APR and age (p=0.027 and 0.049, respectively). Regarding age, patients aged <65 years had a higher risk. Four patients underwent a switch from the originally assigned neurokinin-1 receptor antagonist; in all of these cases, Fos APR was changed to APR for vascular pain. CONCLUSION: Fos APR may increase the risk for ISR associated with TC±Bev therapy for gynecological cancer.
  • Hironori Fujii, Masami Tsuchiya, Daichi Watanabe, Ryo Otsuka, Daisuke Hirate, Katsuyuki Takahashi, Makiko Go, Toshihiro Kudo, Kazuhiro Shimomura, Yosuke Ando, Shinya Tani, Takao Takahashi, Katsuhisa Hayashi, Miki Chin, Naomi Matsunami, Masaya Takahashi, Akiko Hasegawa, Takashi Uchida, Hironobu Hashimoto, Akiko Kubo, Nobuhisa Matsuhashi, Akio Suzuki, Junichi Nishimura, Naoki Inui, Hirotoshi Iihara
    Supportive Care in Cancer 32(5) 2024年5月  査読有り
    Background: Trifluridine/tipiracil (TAS-102) is an oral anticancer drug with adequate efficacy in unresectable colorectal cancer, but frequently also induces chemotherapy-induced nausea and vomiting (CINV). To investigate the occurrence of CINV and antiemetic therapy in patients with colorectal cancer treated with TAS-102 (JASCC-CINV 2001). Methods: We conducted a multicenter, prospective, observational study in patients with colorectal cancer who received TAS-102 without dose reduction for the first time. Primary endpoint was the incidence of vomiting during the overall period. Secondary endpoints were the incidence of nausea, significant nausea, anorexia, other adverse events (constipation, diarrhea, insomnia, fatigue, dysgeusia) and patient satisfaction. Patient diaries were used for primary and secondary endpoints. All adverse events were subjectively assessed using PRO-CTCAE ver 1.0. and CTCAE ver 5.0. Results: Data from 100 of the 119 enrolled patients were analyzed. The incidence of vomiting, nausea, and significant nausea was 13%, 67%, and 36%, respectively. The incidence of vomiting in patients with and without prophylactic antiemetic therapy were 20.8% and 10.5%, respectively. Prophylactic antiemetics were given to 24% of patients, of whom 70% received D2 antagonists. Multivariate Cox proportional hazards analysis showed that experience of CINV in previous treatment tended to be associated with vomiting (hazard ratio [HR]: 7.13, 95% confidence interval [CI]: 0.87–58.5, P = 0.07), whereas prophylactic antiemetic administration was not (HR: 1.61, 95 CI: 0.50–5.21, P = 0.43). With regard to patient satisfaction, the proportion of patients who were "very satisfied," "satisfied," "slightly satisfied" or "somewhat satisfied" was 81.8%. Conclusions: The low incidence of vomiting and high patient satisfaction suggest that TAS-102 does not require the use of uniform prophylactic antiemetic treatments. However, patients with the experience of CINV in previous treatment might require prophylactic antiemetic treatment.
  • Noriaki Matsumoto, Tomohiro Mizuno, Yosuke Ando, Koki Kato, Masanori Nakanishi, Tsuyoshi Nakai, Jeannie K Lee, Yoshitaka Kameya, Wataru Nakamura, Kiyoshi Takahara, Ryoichi Shiroki, Shigeki Yamada
    Clinical drug investigation 2024年4月29日  査読有り
    BACKGROUND: Chemotherapy-induced thrombocytopenia is often a use-limiting adverse reaction to gemcitabine and cisplatin (GC) combination chemotherapy, reducing therapeutic intensity, and, in some cases, requiring platelet transfusion. OBJECTIVE: A retrospective cohort study was conducted on patients with urothelial cancer at the initiation of GC combination therapy and the objective was to develop a prediction model for the incidence of severe thrombocytopenia using machine learning. METHODS: We performed receiver operating characteristic analysis to determine the cut-off values of the associated factors. Multivariate analyses were conducted to identify risk factors associated with the occurrence of severe thrombocytopenia. The prediction model was constructed from an ensemble model and gradient-boosted decision trees to estimate the risk of an outcome using the risk factors associated with the occurrence of severe thrombocytopenia. RESULTS: Of 186 patients included in this study, 46 (25%) experienced severe thrombocytopenia induced by GC therapy. Multivariate analyses revealed that platelet count ≤ 21.4 (×104/µL) [odds ratio 7.19, p < 0.01], hemoglobin ≤ 12.1 (g/dL) [odds ratio 2.41, p = 0.03], lymphocyte count ≤ 1.458 (×103/µL) [odds ratio 2.47, p = 0.02], and dose of gemcitabine ≥ 775.245 (mg/m2) [odds ratio 4.00, p < 0.01] were risk factors of severe thrombocytopenia. The performance of the prediction model using these associated factors was high (area under the curve 0.76, accuracy 0.82, precision 0.68, recall 0.50, and F-measure 0.58). CONCLUSIONS: Platelet count, hemoglobin level, lymphocyte count, and gemcitabine dose contributed to the development of a novel prediction model to identify the incidence of GC-induced severe thrombocytopenia.
  • Yosuke Ando, Yuki Shibata, Takuma Ishihara, Seira Nishibe-Toyosato, Kaori Ito, Nanaho Miyata-Hiraga, Kenji Kawada, Yoshiaki Ikeda, Takahiro Hayashi, Kazuyoshi Imaizumi, Shigeki Yamada
    In vivo (Athens, Greece) 38(2) 767-773 2024年  査読有り筆頭著者責任著者
    BACKGROUND/AIM: Renal dysfunction necessitates S-1 dose reduction. However, decreased dihydropyrimidine dehydrogenase (DPD) activity may lead to adverse events due to 5-FU. The guidelines provided by pharmaceutical companies state that total bilirubin (T-Bil) should be ≤upper limit of normal (ULN)×1.5 as a reference value for safely taking S-1. Nevertheless, the relationship between the degree of liver dysfunction and S-1 dose reduction has not been clearly established. PATIENTS AND METHODS: This study focused on patients who received S-1 monotherapy for various types of cancer. The primary outcome was defined as the variation between blood sampling results on the test day and the subsequent test. The variation data were categorized based on the difference in T-Bil: Low T-Bil group (≤2.25) and High T-Bil group (>2.25). RESULTS: The number of patients that underwent S-1 monotherapy was 883 and the running number was 7,511; Low T-Bil group included 7,245 and High T-Bil group included 266. Examination of the effect of the T-Bil Group on clinical outcomes revealed a correlation with red blood cell (RBC) count, platelet (PLT) count, and T-Bil level. When the impact of the interaction between the T-Bil Group and any of the clinical outcomes, such as the RBC count, PLT count, and T-Bil level, was determined, each outcome showed a significant decrease in the High T-Bil group compared with the Low T-Bil group. CONCLUSION: S-1 administration in patients with liver dysfunction accompanied by elevated T-Bil levels may cause thrombocytopenia.
  • Seira Nishibe-Toyosato, Yosuke Ando, Nayu Nakasuji, Takahiro Hayashi, Kaori Ito, Hidezo Matsuda, Naho Tsujii, Masahiro Tsuge, Kazuyoshi Imaizumi, Kenji Kawada, Shigeki Yamada
    Biological & pharmaceutical bulletin 46(3) 505-510 2023年  査読有り責任著者
    Pharmaceutical consultation targeting outpatients at the Fujita Health University Hospital (Japan) provides support to patients undergoing anticancer drug treatment. This study aimed to explore factors that affect the comprehension of cancer chemotherapy among outpatients who received cancer treatment at our hospital. A questionnaire survey was conducted, and comprehension was scored on a scale of 1-5 (1, no comprehension; 5, full comprehension). When factors other than age and sex [the influence of which on comprehension has been reported in previous reports] were noted, differences in comprehension between the questionnaire items were comparatively analyzed according to the presence/absence of the relevant factors. Overall, 536 patients were included. Age (<70 years) and pharmacist interventions were identified as factors contributing to a comprehension score. The levels of comprehension regarding the name of the cancer chemotherapy, content/schedule of the treatment, purposes of the prescribed drugs, and objectives of blood tests were significantly higher in the group that received the pharmaceutical interventions; conversely, the level of comprehension for the self-management of adverse events was significantly lower in this group than in the group that did not receive any pharmaceutical interventions. Age and interventions by the pharmacist affected the comprehension of cancer chemotherapy by patients.
  • Misaki Morisaku, Kaori Ito, Anna Ogiso, Misa Imai, Yoshiko Hiraoka, Miho Zennami, Masahiro Tsuge, Maiko Mori, Seira Toyosato, Hidezo Matsuda, Yosuke Ando, Masutaka Tokuda, Akihiro Tomita, Shigeki Yamada
    Fujita medical journal 8(2) 59-64 2022年5月  査読有り
    OBJECTIVES: Zinc (Zn) is a cofactor for more than 200 enzymes within the human body. Zn deficiency can result in cell-mediated immune dysfunction. Furthermore, serum Zn levels have been reported to be associated with nutritional status, but this association has not been clarified in malignant lymphoma. This study aimed to examine the deficiency of serum Zn levels and clarify the factors that are correlated with serum Zn in malignant lymphoma. METHODS: Initial malignant lymphoma was diagnosed in patients at Fujita Health University Hospital between April 2011 and March 2019. Based on the serum Zn levels, the study population was divided into "deficient" and "low or normal". For the serum Zn levels of patients undergoing pre-chemotherapy, laboratory parameters and nutritional factors were included. We compared these factors between the abovementioned two groups, and the serum Zn levels with its correlation factors were investigated. RESULTS: A total of 77 patients (Deficient group, n=20 and Low or Normal group, n=57) were enrolled. Histology, hemoglobin, serum albumin levels, Glasgow Prognostic Score (GPS), neutrophile-lymphocyte ratio (NLR), prognostic nutrition index (PNI) and Controlling Nutritional Status (CONUT) were significantly different between the two groups. Of these parameters, only serum albumin level was significantly associated with serum Zn level (p=0.0024; estimated regression coefficient, 9.51; adjusted coefficient of determination, 0.28). CONCLUSIONS: Poor nutritional status at the initial diagnosis may have affected Zn deficiency in initial malignant lymphoma.
  • Misaki Morisaku, Kaori Ito, Tatsuki Shimomura, Shoko Maeda, Maiko Mori, Seira Toyosato, Yosuke Ando, Takenao Koseki, Masami Kawahara, Akihiro Tomita, Shigeki Yamada
    In vivo (Athens, Greece) 36(6) 2910-2917 2022年  査読有り
    BACKGROUND/AIM: Early palliative care (EPC) intervention in patients with solid tumors can provide many benefits. However, studies on patients with hematological malignancies are limited, and there is no data on patients with lymphoma. We conducted a preliminary retrospective survey of palliative care (PC) intervention in patients with lymphoma to clarify the effect of EPC on overall survival (OS). PATIENTS AND METHODS: The first palliative care consultation (PC1) was retrospectively reviewed from medical records in Japan. Patients with lymphoma requiring inpatient PC at our institution from January 2012 to December 2018 were recruited. We conducted receiver operating characteristic (ROC) analysis; patients were divided into two groups (early and delayed), and the survival periods and palliative care team (PCT) referral details were compared. RESULTS: The analysis included 77 patients with lymphoma [median age, 71 (64-79)] years. The median period to PC1 from the initial diagnosis was 395 (180-1,086) days. ROC analysis revealed an optimal PC intervention timing of 140 days. OS was significantly longer in the early group than that in the delayed group. The most common counseling details for the PCT were symptom relief and palliative care transfer (36.8% and 35.2%, respectively). CONCLUSION: This real-world evaluation of PC intervention for inpatients with lymphoma revealed that PC intervention was provided at approximately 13 months following initial diagnosis. EPC intervention from diagnosis to 140 days may improve OS in patients with lymphoma; however further large-scale studies are required to verify this finding.
  • Maeda, A., Yoshida, H., Inoue, H., Ejiri, M., Yamaguchi, S., Kushihara, H., Yamamoto, Y., Ando, Y., Sato, Y., Tashiro, Y., Hasegawa, A., Takahara, Y., Mizutani, M., Oze, I., Shimizu, J.
    Annals of Palliative Medicine 10(3) 2021年  査読有り
  • Nishibe-Toyosato, S., Ando, Y., Goto, Y., Hayashi, T., Ito, K., Matsuda, H., Tsujii, N., Tsuge, M., Kawada, K., Imaizumi, K., Yamada, S.
    Biological and Pharmaceutical Bulletin 44(9) 2021年  査読有り責任著者
  • Matsuoka, H., Hayashi, T., Takigami, K., Imaizumi, K., Shiroki, R., Ohmiya, N., Sugiura, K., Kawada, K., Sawaki, A., Maeda, K., Ando, Y., Uyama, I.
    BMC Cancer 20(1) 2020年  査読有り
  • Ando, Y., Hayashi, T., Shiouchi, H., Tanaka, C., Ito, K., Nishibe, S., Miyata, N., Horiba, R., Yanagi, H., Fujii, T., Kawada, K., Ikeda, Y., Yamada, S.
    Biological and Pharmaceutical Bulletin 43(4) 2020年  査読有り筆頭著者
  • Ando, Y., Hayashi, T., Sugimoto, R., Nishibe, S., Ito, K., Kawada, K., Ikeda, Y., Yamada, S., Imaizumi, K.
    Investigational New Drugs 38(4) 2020年  査読有り筆頭著者
  • Ito, K., Hayashi, T., Inaguma, Y., Terazawa, T., Ando, M., Ando, Y., Tsuge, M., Kato, A., Shimato, A., Suzuki, S., Kato, S., Tomita, A., Yamada, S., Emi, N.
    Biological and Pharmaceutical Bulletin 42(10) 2019年  査読有り
  • Ohta, H., Hayashi, T., Murai, S., Shiouchi, H., Ando, Y., Kumazawa, S., Ito, K., Ikeda, Y., Matsuoka, H., Maeda, K., Kawada, K., Yasuda, K., Yamada, S.
    Cancer Chemotherapy and Pharmacology 79(5) 2017年  査読有り
  • Ando, Y., Hayashi, T., Ujita, M., Murai, S., Ohta, H., Ito, K., Yamaguchi, T., Funatsu, M., Ikeda, Y., Imaizumi, K., Kawada, K., Yasuda, K., Yamada, S.
    Cancer Chemotherapy and Pharmacology 78(1) 2016年  査読有り筆頭著者
  • Tomono, A., Ito, K., Hayashi, T., Ando, M., Ando, Y., Tsuge, M., Okamoto, A., Inaguma, Y., Okamoto, M., Emi, N., Yamada, S.
    Cancer Chemotherapy and Pharmacology 78(2) 2016年  査読有り
  • Ito, K., Okamoto, M., Inaguma, Y., Okamoto, A., Ando, M., Ando, Y., Tsuge, M., Tomono, A., Kakumae, Y., Hayashi, T., Yamada, S., Emi, N.
    Oncology (Switzerland) 91(6) 2016年  査読有り
  • Ando, Y., Hayashi, T., Ito, K., Suzuki, E., Mine, N., Miyamoto, A., Oya, M., Matsuda, H., Isaji, A., Nakanishi, T., Imaizumi, K., Shibata, T., Okada, T., Sakurai, K., Naito, K., Uyama, I., Kawada, K., Takahashi, H., Yamada, S.
    Supportive Care in Cancer 24(2) 2016年  査読有り筆頭著者
  • Kaori Ito, Masataka Okamoto, Maiko Ando, Yosuke Ando, Eri Suzuki, Akinao Okamoto, Yoko Inaguma, Takahiro Hayashi, Shigeki Yamada, Nobuhiko Emi
    ANNALS OF ONCOLOGY 26 96-97 2015年11月  査読有り
  • Satomi Kumazawa, Hiroshi Matsuoka, Yosuke Ando, Maiko Ando, Yukiko Kakumae, Kaori Ito, Hideki Ohta, Shigeki Yamada, Kotaro Maeda
    ANNALS OF ONCOLOGY 25 2014年10月  査読有り

MISC

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書籍等出版物

 4

講演・口頭発表等

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