研究者業績

渡辺 崇

ワタナベ タカシ  (Takashi Watanabe)

基本情報

所属
藤田医科大学 講師
学位
医学博士(名古屋大学)

J-GLOBAL ID
200901097880303580
researchmap会員ID
6000010170

外部リンク

学歴

 3

論文

 53
  • 渡辺 崇, 柳 久乃, 榎本 篤, サンペトラ・オルテア, 佐谷 秀行, 下野 洋平
    日本癌学会総会記事 80回 [P11-2] 2021年9月  
  • 下野 洋平, 西村 建徳, 河野 誠之, 渋谷 尚樹, 林 孝典, 柳 久乃, 渡辺 崇, 前田 真男, 掛地 吉弘, 河田 健司, 浅井 直也, 高尾 信太郎, 南 博信, 喜島 祐子, 鈴木 元, 後藤 典子
    日本癌学会総会記事 80回 [CS4-3] 2021年9月  
  • 渡辺 崇, 柳 久乃, 榎本 篤, サンペトラ・オルテア, 佐谷 秀行, 下野 洋平
    日本癌学会総会記事 80回 [P11-2] 2021年9月  
  • Mizuno M, Khaledian B, Maeda M, Hayashi T, Mizuno S, Munetsuna E, Watanabe T, Kono S, Okada S, Suzuki M, Takao S, Minami H, Asai N, Sugiyama F, Takahashi S, Shimono Y
    Cancers 13(16) 4238 2021年8月  査読有り招待有り
    Adipose tissue is a component of the tumor microenvironment and is involved in tumor progression. We have previously shown that adipokine adipsin (CFD) functions as an enhancer of tumor proliferation and cancer stem cell (CSC) properties in breast cancers. We established the Cfd-knockout (KO) mice and the mammary adipose tissue-derived stem cells (mADSCs) from them. Cfd-KO in mADSCs significantly reduced their ability to enhance tumorsphere formation of breast cancer patient-derived xenograft (PDX) cells, which was restored by the addition of Cfd in the culture medium. Hepatocyte growth factor (HGF) was expressed and secreted from mADSCs in a Cfd-dependent manner. HGF rescued the reduced ability of Cfd-KO mADSCs to promote tumorsphere formation in vitro and tumor formation in vivo by breast cancer PDX cells. These results suggest that HGF is a downstream effector of Cfd in mADSCs that enhances the CSC properties in breast cancers.
  • Hisano Yanagi, Takashi Watanabe, Tatsunori Nishimura, Takanori Hayashi, Seishi Kono, Hitomi Tsuchida, Munetsugu Hirata, Yuko Kijima, Shintaro Takao, Seiji Okada, Motoshi Suzuki, Kazuyoshi Imaizumi, Kenji Kawada, Hironobu Minami, Noriko Gotoh, Yohei Shimono
    Cancer science 111(12) 4359-4370 2020年12月  
    Metastatic progression remains the major cause of death in human breast cancer. Cancer cells with cancer stem cell (CSC) properties drive initiation and growth of metastases at distant sites. We have previously established the breast cancer patient-derived tumor xenograft (PDX) mouse model in which CSC marker CD44+ cancer cells formed spontaneous microscopic metastases in the liver. In this PDX mouse, the expression levels of S100A10 and its family proteins were much higher in the CD44+ cancer cells metastasized to the liver than those at the primary site. Knockdown of S100A10 in breast cancer cells suppressed and overexpression of S100A10 in breast cancer PDX cells enhanced their invasion abilities and 3D organoid formation capacities in vitro. Mechanistically, S100A10 regulated the matrix metalloproteinase activity and the expression levels of stem cell-related genes. Finally, constitutive knockdown of S100A10 significantly reduced their metastatic ability to the liver in vivo. These findings suggest that S100A10 functions as a metastasis promoter of breast CSCs by conferring both invasion ability and CSC properties in breast cancers.

MISC

 16

担当経験のある科目(授業)

 3

所属学協会

 1

共同研究・競争的資金等の研究課題

 9