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Identification of a Cancer Stem-like Population in the Lewis Lung Cancer Cell Line
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  • Identification of a Cancer Stem-like Population in the Lewis Lung Cancer Cell Line
  • Identification of a Cancer Stem-like Population in the Lewis Lung Cancer Cell Line
저자명
Zhang. An-Mei,Fan. Ye,Yao. Quan,Ma. Hu,Lin. Sheng,Zhu. Cong-Hui,Wang. Xin-Xin,Liu. Jia,Zhu. Bo,Sun. Jian-Guo,Chen. Zheng-Tang
간행물명
Asian Pacific journal of cancer prevention : APJCP
권/호정보
2012년|13권 3호|pp.761-766 (6 pages)
발행정보
아시아태평양암예방학회
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정기간행물|ENG|
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이 논문은 한국과학기술정보연구원과 논문 연계를 통해 무료로 제공되는 원문입니다.
서지반출

기타언어초록

Objective: Although various human cancer stem cells (CSCs) have been defined, their applications are restricted to immunocompromised models. Developing a novel CSC model which could be used in immunocompetent or transgenic mice is essential for further understanding of the biomolecular characteristics of tumor stem cells. Therefore, in this study, we analyzed murine lung cancer cells for the presence of CSCs. Methods: Side population (SP) cells were isolated by fluorescence activated cell sorting, followed by serum-free medium (SFM) culture, using Lewis lung carcinoma cell (LLC) line. The self-renewal, differentiated progeny, chemosensitivity, and tumorigenic properties in SP and non-SP cells were investigated through in vitro culture and in vivo serial transplantation. Differential expression profiles of stem cell markers were examined by RT-PCR. Results: The SP cell fraction comprised 1.1% of the total LLC population. SP cells were available to grow in SFM, and had significantly enhanced capacity for cell proliferation and colony formation. They were also more resistant to cisplatin in comparison to non-SP cells, and displayed increased tumorigenic ability. Moreover, SP cells showed higher mRNA expression of Oct-4, ABCG2, and CD44. Conclusion: We identified SP cells from a murine lung carcinoma, which possess well-known characteristics of CSCs. Our study established a useful model that should allow investigation of the biological features and pharmacosensitivity of lung CSCs, both in vitro and in syngeneic immunocompetent or transgenic/knockout mice.