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BikDD eliminates breast cancer initiating cells and synergizes with lapatinib for breast cancer treatment.


ABSTRACT: Breast cancer initiating cells (BCICs), which can fully recapitulate the tumor origin and are often resistant to chemo- and radiotherapy, are currently considered as a major obstacle for breast cancer treatment. Here, we show that BIKDD, a constitutively active mutant form of proapoptotic gene, BIK, effectively induces apoptosis of breast cancer cells and synergizes with lapatinib. Most importantly, BikDD significantly reduces BCICs through co-antagonism of its binding partners Bcl-2, Bcl-xL, and Mcl-1, suggesting a potential therapeutic strategy targeting BCICs. Furthermore, we developed a cancer-specific targeting approach for breast cancer that selectively expresses BikDD in breast cancer cells including BCICs, and demonstrated its potent antitumor activity and synergism with lapatinib in vitro and in vivo.

SUBMITTER: Lang JY 

PROVIDER: S-EPMC3172580 | biostudies-literature | 2011 Sep

REPOSITORIES: biostudies-literature

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BikDD eliminates breast cancer initiating cells and synergizes with lapatinib for breast cancer treatment.

Lang Jing-Yu JY   Hsu Jennifer L JL   Meric-Bernstam Funda F   Chang Chun-Ju CJ   Wang Qingfei Q   Bao Yi Y   Yamaguchi Hirohito H   Xie Xiaoming X   Woodward Wendy A WA   Yu Dihua D   Hortobagyi Gabriel N GN   Hung Mien-Chie MC  

Cancer cell 20110901 3


Breast cancer initiating cells (BCICs), which can fully recapitulate the tumor origin and are often resistant to chemo- and radiotherapy, are currently considered as a major obstacle for breast cancer treatment. Here, we show that BIKDD, a constitutively active mutant form of proapoptotic gene, BIK, effectively induces apoptosis of breast cancer cells and synergizes with lapatinib. Most importantly, BikDD significantly reduces BCICs through co-antagonism of its binding partners Bcl-2, Bcl-xL, an  ...[more]

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