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Oncology Reports
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Print ISSN: 1021-335X Online ISSN: 1791-2431
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March 2005 Volume 13 Issue 3

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International Journal of Molecular Medicine

International Journal of Molecular Medicine

International Journal of Molecular Medicine is an international journal devoted to molecular mechanisms of human disease.

International Journal of Oncology

International Journal of Oncology

International Journal of Oncology is an international journal devoted to oncology research and cancer treatment.

Molecular Medicine Reports

Molecular Medicine Reports

Covers molecular medicine topics such as pharmacology, pathology, genetics, neuroscience, infectious diseases, molecular cardiology, and molecular surgery.

Oncology Reports

Oncology Reports

Oncology Reports is an international journal devoted to fundamental and applied research in Oncology.

Experimental and Therapeutic Medicine

Experimental and Therapeutic Medicine

Experimental and Therapeutic Medicine is an international journal devoted to laboratory and clinical medicine.

Oncology Letters

Oncology Letters

Oncology Letters is an international journal devoted to Experimental and Clinical Oncology.

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Explores a wide range of biological and medical fields, including pharmacology, genetics, microbiology, neuroscience, and molecular cardiology.

Molecular and Clinical Oncology

Molecular and Clinical Oncology

International journal addressing all aspects of oncology research, from tumorigenesis and oncogenes to chemotherapy and metastasis.

World Academy of Sciences Journal

World Academy of Sciences Journal

Multidisciplinary open-access journal spanning biochemistry, genetics, neuroscience, environmental health, and synthetic biology.

International Journal of Functional Nutrition

International Journal of Functional Nutrition

Open-access journal combining biochemistry, pharmacology, immunology, and genetics to advance health through functional nutrition.

International Journal of Epigenetics

International Journal of Epigenetics

Publishes open-access research on using epigenetics to advance understanding and treatment of human disease.

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Article

CYP17 polymorphism as a risk factor of tamoxifen-induced hepatic steatosis in breast cancer patients

  • Authors:
    • Takenao Ohnishi
    • Yasuhiro Ogawa
    • Toshiji Saibara
    • Akihito Nishioka
    • Shinji Kariya
    • Mitsutaka Fukumoto
    • Saburo Onishi
    • Shoji Yoshida
  • View Affiliations / Copyright

    Affiliations: Department of Tumor Radiology, Kochi Medical School, Oko-cho, Nankoku, Kochi 783-8505, Japan. tohnishi@med.kochi-u.ac.jp
  • Pages: 485-489
    |
    Published online on: March 1, 2005
       https://doi.org/10.3892/or.13.3.485
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Abstract

Oral administration of tamoxifen, an endocrine therapy for breast cancer, often induces hepatic steatosis (THS, tamoxifen-induced hepatic steatosis) as a complication, which can progress to non-alcoholic steatohepatitis (NASH). The development of this complication is strongly associated with three clinical risk factors; specifically, insulin resistance, central obesity, and hypertriglyceridemia, however a genetic predisposition to THS has yet to be investigated. The aim of this study is to determine whether genetic polymorphism of the P450c17α enzyme coded for by the CYP17 gene, responsible for regulating serum estrogen, has an association with THS. After obtaining informed consent from 180 eligible breast cancer patients treated with tamoxifen, DNA was collected and analyzed by restriction fragment length polymorphism assay and classified into alleles defined as A1 and A2. The absence or presence and extent of THS was evaluated by calculating the liver/spleen (L/S) ratio based on Hounsfield units with a CT scanner. Administration of tamoxifen led to THS (L/S ratio <0.9) in 57 (31.7%) of 180 patients while the remaining 123 (68.3%) patients did not develop THS. A significant difference in the distribution of CYP17 genotypes was observed between patients who developed THS and those who did not (P=0.021). A significantly higher frequency of the A2 allele was seen in the THS group (odds ratio, 1.90; 95% confidence interval, 1.21-2.99). Our study provides the first evidence that CYP17 polymorphism participates in the development of THS, and sheds light on the genetic causes of this side effect and genetic differences between tamoxifen-treated individuals.

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Copy and paste a formatted citation
Spandidos Publications style
Ohnishi T, Ogawa Y, Saibara T, Nishioka A, Kariya S, Fukumoto M, Onishi S and Yoshida S: CYP17 polymorphism as a risk factor of tamoxifen-induced hepatic steatosis in breast cancer patients. Oncol Rep 13: 485-489, 2005.
APA
Ohnishi, T., Ogawa, Y., Saibara, T., Nishioka, A., Kariya, S., Fukumoto, M. ... Yoshida, S. (2005). CYP17 polymorphism as a risk factor of tamoxifen-induced hepatic steatosis in breast cancer patients. Oncology Reports, 13, 485-489. https://doi.org/10.3892/or.13.3.485
MLA
Ohnishi, T., Ogawa, Y., Saibara, T., Nishioka, A., Kariya, S., Fukumoto, M., Onishi, S., Yoshida, S."CYP17 polymorphism as a risk factor of tamoxifen-induced hepatic steatosis in breast cancer patients". Oncology Reports 13.3 (2005): 485-489.
Chicago
Ohnishi, T., Ogawa, Y., Saibara, T., Nishioka, A., Kariya, S., Fukumoto, M., Onishi, S., Yoshida, S."CYP17 polymorphism as a risk factor of tamoxifen-induced hepatic steatosis in breast cancer patients". Oncology Reports 13, no. 3 (2005): 485-489. https://doi.org/10.3892/or.13.3.485
Copy and paste a formatted citation
x
Spandidos Publications style
Ohnishi T, Ogawa Y, Saibara T, Nishioka A, Kariya S, Fukumoto M, Onishi S and Yoshida S: CYP17 polymorphism as a risk factor of tamoxifen-induced hepatic steatosis in breast cancer patients. Oncol Rep 13: 485-489, 2005.
APA
Ohnishi, T., Ogawa, Y., Saibara, T., Nishioka, A., Kariya, S., Fukumoto, M. ... Yoshida, S. (2005). CYP17 polymorphism as a risk factor of tamoxifen-induced hepatic steatosis in breast cancer patients. Oncology Reports, 13, 485-489. https://doi.org/10.3892/or.13.3.485
MLA
Ohnishi, T., Ogawa, Y., Saibara, T., Nishioka, A., Kariya, S., Fukumoto, M., Onishi, S., Yoshida, S."CYP17 polymorphism as a risk factor of tamoxifen-induced hepatic steatosis in breast cancer patients". Oncology Reports 13.3 (2005): 485-489.
Chicago
Ohnishi, T., Ogawa, Y., Saibara, T., Nishioka, A., Kariya, S., Fukumoto, M., Onishi, S., Yoshida, S."CYP17 polymorphism as a risk factor of tamoxifen-induced hepatic steatosis in breast cancer patients". Oncology Reports 13, no. 3 (2005): 485-489. https://doi.org/10.3892/or.13.3.485
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