Jin Guanghua, Mao Xiaoyun, Qiao Zhen, Chen Bo, Jin Feng
Department of Breast Surgery, The First Affiliated Hospital of China Medical University, Shenyang, Liaoning 110001, People's Republic of China,
Onco Targets Ther. 2019 Jan 18;12:625-634. doi: 10.2147/OTT.S186981. eCollection 2019.
RAP80 is a member of BRCA1-A complex, which plays an important role in regulating the cell cycle checkpoint and DNA damage repair in the nucleus.
We investigated RAP80 expression in breast cancer and its paired normal breast tissues to further analyze its role in the biological behavior of breast cancer cells.
RAP80 expression in breast cancer (62.3%, 101/162) was significantly lower than that in adjacent normal breast tissues (<0.05). RAP80 expression was related to tumor size, lymph node metastasis, TNM stage, and molecular subtype (<0.05). RAP80 mRNA expression was significantly lower in triple-negative breast cancer than other types. The mRNA and protein of RAP80 were obvious in MCF-7 and very weak in ZR-75 or MDA-MB-231, so we picked MCF-7 to be transfected with RAP80 siRNA. The survival rate of both cells decreased in a dose-dependent manner and the IC50 value for cisplatin in MCF-7 RAP80 siRNA cells was 0.83 µg/mL, and 1.69 µg/mL in wild-type MCF-7 according to MTT. RAP80 siRNA transfection upregulated the apoptosis and downregulated invasive or migrating ability of MCF-7. RAP80 siRNA also upregulated the protein expression of Caspase-3, cleaved Caspase-3, Apaf-1, Cytochrome C, Bax, and Fas, and downregulated the protein expression of Bcl-2.
RAP80 expression was related to ER or PR activity. Inhibition of RAP80 expression can induce apoptosis in breast cancer cells and improve chemosensitivity to cisplatin. Tumor cells can activate protective responses to inhibit cell cycle progression, which may be related to RAP80, and repair cisplatin-induced DNA damage. RAP80 is related to BRCA1's effect, which can be used as an interesting target for pharmacological modulation that can increase the efficiency of cisplatin chemotherapy.
RAP80是BRCA1-A复合物的成员,在调节细胞核中的细胞周期检查点和DNA损伤修复中起重要作用。
我们研究了RAP80在乳腺癌及其配对的正常乳腺组织中的表达,以进一步分析其在乳腺癌细胞生物学行为中的作用。
乳腺癌中RAP80的表达(62.3%,101/162)明显低于相邻正常乳腺组织(<0.05)。RAP80表达与肿瘤大小、淋巴结转移、TNM分期和分子亚型相关(<0.05)。三阴性乳腺癌中RAP80 mRNA表达明显低于其他类型。RAP80的mRNA和蛋白在MCF-7中明显,在ZR-75或MDA-MB-231中非常弱,因此我们选择MCF-7用RAP80 siRNA进行转染。根据MTT法,两种细胞的存活率均呈剂量依赖性下降,MCF-7 RAP80 siRNA细胞中顺铂的IC50值为0.83μg/mL,野生型MCF-7中为1.69μg/mL。RAP80 siRNA转染上调了MCF-7的凋亡率,下调了其侵袭或迁移能力。RAP80 siRNA还上调了Caspase-3、裂解的Caspase-3、Apaf-1、细胞色素C、Bax和Fas的蛋白表达,下调了Bcl-2的蛋白表达。
RAP80表达与雌激素受体或孕激素受体活性相关。抑制RAP80表达可诱导乳腺癌细胞凋亡并提高对顺铂的化疗敏感性。肿瘤细胞可激活保护性反应以抑制细胞周期进程,这可能与RAP80有关,并修复顺铂诱导的DNA损伤。RAP80与BRCA1的作用相关,可作为一种有趣的药理学调节靶点,以提高顺铂化疗的效率。
