The antitumor effect of LJ-529, a novel agonist to A3 adenosine receptor, in both estrogen receptor-positive and estrogen receptor-negative human breast cancers
- Authors
- Chung, Heekyoung; Jung, Ji-Youn; Cho, Sung-Dae; Hong, Kyung-A; Kim, Hyun-Jun; Shin, Dong-Hui; Kim, HKim, Hwan; Kim, Hea Ok; Shin, Dae Hong; Lee, Hyuk Woo; Jeong, Lak Shin; Kong, Gu
- Issue Date
- Mar-2006
- Publisher
- American Association for Cancer Research
- Citation
- Molecular Cancer Therapeutics, v.5, no.3, pp 685 - 692
- Pages
- 8
- Indexed
- SCIE
SCOPUS
- Journal Title
- Molecular Cancer Therapeutics
- Volume
- 5
- Number
- 3
- Start Page
- 685
- End Page
- 692
- URI
- https://scholarworks.bwise.kr/hanyang/handle/2021.sw.hanyang/181700
- DOI
- 10.1158/1535-7163.MCT-05-0245
- ISSN
- 1535-7163
1538-8514
- Abstract
- Agonists to A3 adenosine receptor (A3AR) have been reported to inhibit cell growth and/or induce apoptosis in various tumors. We tested the effect of a novel A3AR agonist generically known as LJ-529 in breast cancer cells. Anchorage-dependent cell growth and in vivo tumor growth were attenuated by LJ-529, independently of its estrogen receptor (ER) alpha status. In addition, apoptosis was induced as evidenced by the activation of caspase-3 and c-poly (ADP)ribose polymerase. Furthermore, the Wnt signaling pathway was down-regulated and P27(kip) was induced by LJ-529. In ER-positive cells, the expression of ER was down-regulated by LJ-529, which might have additionally contributed to attenuated cell proliferation. In ER-negative, c-ErbB2-overexpressing SK-BR-3 cells, the expression of c-ErbB2 and its downstream extracellular signal-regulated kinase pathway were down-regulated by LJ-529. However, such effect of LJ-529 acted independently of its receptor because no A3AR was detected by reverse transcription-PCR in all four cell lines tested. In conclusion, our novel findings open the possibility of LJ-529 as an effective therapeutic agent against both ER-positive and ER-negative breast cancers, particularly against the more aggressive ER-negative, c-ErbB2-overexpressing types.
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