Identification of circulating endorepellin LG3 fragment: Potential use as a serological biomarker for breast cancer

Authors
Chang, Jong WookKang, Un-BeomKim, Dong HyunYi, Jae KyoLee, Jong WonNoh, Dong-YoungLee, CheoljuYu, Myeong-Hee
Issue Date
2008-01
Publisher
WILEY-V C H VERLAG GMBH
Citation
PROTEOMICS CLINICAL APPLICATIONS, v.2, no.1, pp.23 - 32
Abstract
Comparative proteome analysis was performed on the cultured media of human nontumor and malignant breast cell lines, Hs578Bst and Hs578T, respectively, in search of a serological biomarker(s) for breast cancer. Proteins in the conditioned media were separated by 2-D PAGE and then visualized by silver-staining. Eight proteins changed differentially by more than twofold were identified by MALDI-TOF/TOF MS. Among the proteins identified, the terminal laminin-like globular (LG3) domain of endorepellin, which was recently reported as an antiangiogenesis factor, was decreased in the cancer cell line. We confirmed the bone morphogenic protein-1 (BMP-1) mediated cleavage site on the N-terminus of endorepellin LG3 fragment. This finding suggests that the LG3 fragment is specifically released by a BMP-1 driven limited proteolytic process. The protein was also detected in plasma by Western blot analysis and selected reaction monitoring (SRM). The plasma level of the endorepellin LG3 fragment was significantly lower in breast cancer patients compared to healthy donors (p = 0.017; n = 12). The LG3 protein concentration in the control plasma was measured at approximately 3.7 pmol/mL compared to 1.8 pmol/mL in plasma from the cancer patients. We suggest that these results support the potential use of the endorepellin LG3 fragment as a new serological biomarker for breast cancer.
Keywords
TISSUE GROWTH-FACTOR; PROTEOMIC ANALYSIS; IN-VIVO; DISCOVERY; PROTEINS; PERLECAN; MICROENVIRONMENT; METASTASIS; REVEALS; MARKERS; TISSUE GROWTH-FACTOR; PROTEOMIC ANALYSIS; IN-VIVO; DISCOVERY; PROTEINS; PERLECAN; MICROENVIRONMENT; METASTASIS; REVEALS; MARKERS; biomarker; breast cancer; endorepellin LG3 fragment; selected reaction monitoring
ISSN
1862-8346
URI
https://pubs.kist.re.kr/handle/201004/133866
DOI
10.1002/prca.200780049
Appears in Collections:
KIST Article > 2008
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