Additional file 1: of Targeting the SPOCK1-snail/slug axis-mediated epithelial-to-mesenchymal transition by apigenin contributes to repression of prostate cancer metastasis

Chien, Ming-Hsien; Lin, Yung-Wei; Wen, Yu-Ching; Yang, Yi-Chieh; Hsiao, Michael; Chang, Junn-Liang; Huang, Hsiang-Ching; Lee, Wei-Jiunn

doi:10.6084/m9.figshare.8252111.v1

13046_2019_1247_MOESM1_ESM.docx (1.02 MB)

Additional file 1: of Targeting the SPOCK1-snail/slug axis-mediated epithelial-to-mesenchymal transition by apigenin contributes to repression of prostate cancer metastasis

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posted on 2019-06-10, 05:00 authored by Ming-Hsien Chien, Yung-Wei Lin, Yu-Ching Wen, Yi-Chieh Yang, Michael Hsiao, Junn-Liang Chang, Hsiang-Ching Huang, Wei-Jiunn Lee

Figure S1. Wound-healing assay of apigenin (API)-treated DU145 prostate cancer cells. Figure S2. Migration and Matrigel invasion assay of DU145 cells using a Transwell system. Figure S3. SPOCK1 is critical for apigenin (API)-modulated invasiveness of prostate cancer cells. Figure S4. Akt is a downstream regulator of SPOCK1 to regulate Snail family expression in apigenin (API)-treated prostate cancer cells. Table S1. Normalization of wound healing, cell invasion and migration to cell viability under API treatment. (DOCX 1043 kb)

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Prostate cancer SPOCK1 Metastasis Snail Slug Epithelial-to-mesenchymal transition Apigenin

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Additional file 1: of Targeting the SPOCK1-snail/slug axis-mediated epithelial-to-mesenchymal transition by apigenin contributes to repression of prostate cancer metastasis

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