Hiroko Awa scite author profile

Hiroko Awa

2Publications

9Citation Statements Received

57Citation Statements Given

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Fujita Health University

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Effects of Combined Treatment with Branched-Chain Amino Acids, Citric Acid, L-Carnitine, Coenzyme Q10, Zinc, and Various Vitamins in Tumor-Bearing Mice

Awa

Futamura

Higashiguchi

et al. 2017

Biological & Pharmaceutical Bulletin

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A functional dietary supplement (FDS) containing Coenzyme Q10, branched-chain amino acids and L-carnitine was administered to tumor-bearing mice, investigating its effects on tumor and muscle tissues. Experiment (A): B16 melanoma cells were implanted subcutaneously into the right side of the abdomen of 8-to 9-week-old C57BL/6J mice. The mice were divided into two groups: a FDS group that received oral administration of FDS (n=10), and a control group that received oral administration of glucose (n=10). The moribund condition was used as the endpoint, and median survival time was determined. Experiment (B): On day 21 after tumor implantation, tumors, soleus muscle, gastrocnemius muscle, and suprahyoid muscles were collected. Tumor and muscle weight and other aspects were evaluated in each group: FDS group (n=15) and control group (n=15). The median survival time was comparable (21 d in the FDS group vs. 18 d in the control group, p=0.30). However, cumulative food intake was significantly higher in the FDS group than the control group (p=0.011). Metastasis of melanoma to the lung was observed in the control group but not in the FDS group (p=0.043). The weight of the suprahyoid muscles was significantly higher in the FDS group than in the control group (p=0.0045). The weight of the tumor was significantly lower in the FDS group than in the control group (p=0.013). The results possibly suggest oral administration of FDS in tumor-bearing mice enhances the maintenance of suprahyoid muscles, resulting in an extended feeding period and suppression of tumor growth and metastasis.Key words cancer therapy; cachexia; metabolism; branched-chain amino acid; functional maintenance Cancer cachexia is a syndrome that affects many patients with advanced cancer. It is characterized by refractory malnutrition and has significant impact on prognosis and QOL. Managing cachexia is therefore a high priority when providing palliative care. Cachexia is a complex metabolic syndrome, with loss of muscle mass being a primary symptom. Development of cachexia involves many factors and accompanies progressive functional impairment, but the pathogenesis remains unknown. 1,2) Recent studies suggest that metabolic and neuroendocrinological abnormalities in cancer cachexia are caused by inflammatory cytokines secreted by the tumor and host cells and other tumor-derived substances. It is essential for cancer patients to maintain good nutritional status for better prognosis and QOL. As such, managing cancer cachexia is a major goal for the future of cancer therapy and palliative care. Since its foundation in 2003, our laboratory has implemented a unique nutritional support system to manage cancer cachexia.3-5) With the nutritional support, patients with cachexia have shown reduced symptoms and improved bodily function through control of metabolic dynamics. We have developed a functional dietary supplement (FDS) for improving symptoms and function, containing Coenzyme Q10 (CoQ10), branchedchain amino acids (BCAA), L-carnitine and citric acid and repo...

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A Clinical Study on Administration of Opioid Antagonists in Terminal Cancer Patients: 7 Patients Receiving Opioid Antagonists Following Opioids among 2443 Terminal Cancer Patients Receiving Opioids

Uekuzu

Higashiguchi

Futamura

et al. 2017

Biological & Pharmaceutical Bulletin

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There have been few detailed reports on respiratory depression due to overdoses of opioids in terminal cancer patients. We investigated the situation of treatment with opioid antagonists for respiratory depression that occurred after administration of opioid at optimal doses in terminal cancer patients, to clarify pathological changes as well as causative factors. In 2443 terminal cancer patients receiving opioids, 7 patients (0.3%) received opioid antagonists: 6, morphine (hydrochloride, 5; sulfate, 1); 1, oxycodone. The median dosage of opioids was 13.3 mg/d, as converted to morphine injection. Respiratory depression occurred on this daily dose in 4 patients and after changed dose and route in 3 patients. Opioids were given through the vein in 6 patients and by the enteral route in 1 patient. Concomitant drugs included nonsteroidal anti-inflammatory drugs in 3 patients and zoledronic acid in 2 patients. In morphine-receiving patients, renal functions were significantly worsened at the time of administration of an opioid antagonist than the day before the start of opioid administration. These findings indicate that the proper use of opioids was safe and acceptable in almost all terminal cancer patients. In rare cases, however, a risk toward respiratory depression onset is indicated because morphine and morphine-6-glucuronide become relatively excessive owing to systemic debility due to disease progression, especially respiratory and renal dysfunctions. At the onset of respiratory depression, appropriate administration of an opioid antagonist mitigated the symptoms. Thereafter, opioid switching or continuous administration at reduced dosages of the same opioids prevented the occurrence of serious adverse events.

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Hiroko Awa

Effects of Combined Treatment with Branched-Chain Amino Acids, Citric Acid, L-Carnitine, Coenzyme Q10, Zinc, and Various Vitamins in Tumor-Bearing Mice

A Clinical Study on Administration of Opioid Antagonists in Terminal Cancer Patients: 7 Patients Receiving Opioid Antagonists Following Opioids among 2443 Terminal Cancer Patients Receiving Opioids

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