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Effect of anti-DR5 and chemotherapy on basal-like breast cancer

机译:抗DR5和化学疗法对基底样乳腺癌的作用

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The purpose is to evaluate sensitivity of basal-like breast cancer to treatment with anti-DR5 alone and in combination with chemotherapy. Cytotoxicity of TRA-8 anti-DR5 alone and in combination with doxorubicin or paclitaxel was examined. The role of a DR5-associated molecule (DDX3) in the regulation of apoptosis by recruitment of cIAP1 to the DR5/DDX3 complex was studied. SUM159 and 2LMP orthotopic xenografts were treated with TRA-8 alone and in combination with Abraxane or doxorubicin, and tumor growth inhibition determined. Diffusion-weighted magnetic resonance imaging was used to monitor early tumor response. The majority (12/15) of basal-like cell lines were very sensitive to TRA-8-induced cytotoxicity (IC50 values of 1.0–49 ng/ml). In contrast, 8/11 luminal or HER2-positive cell lines were resistant (IC50 > 1,000 ng/ml). Enhanced killing of basal-like cell lines was produced by combination treatment with TRA-8 and doxorubicin. Majority of basal cell lines expressed lower levels of DR5-associated DDX3 and cIAP1 than luminal and HER2-positive cell lines. TRA-8 inhibited growth of basal xenografts and produced 20% complete 2LMP tumor regressions. TRA-8 and chemotherapy produced greater 2LMP growth inhibition than either alone. An increase in apparent diffusion coefficient in 2LMP tumors was measured in a week of therapy with TRA-8 and Abraxane. Basal-like cell lines were more sensitive to TRA-8-mediated cytotoxicity than HER2-over-expressing and luminal cell lines, and chemotherapy enhanced cytotoxicity. High sensitivity of basal cells to TRA-8 correlated with low expression of DR5/DDX3/cIAP1 complex. Treatment with TRA-8 and chemotherapy may be an effective therapy for basal-like breast cancer.
机译:目的是评估基底样乳腺癌对单独使用抗DR5和联合化疗治疗的敏感性。检查了TRA-8抗DR5单独和与阿霉素或紫杉醇联用的细胞毒性。研究了DR5相关分子(DDX3)在通过将cIAP1募集到DR5 / DDX3复合物中来调控细胞凋亡的作用。将SUM159和2LMP原位异种移植物单独用TRA-8并与阿布罗生或阿霉素组合治疗,并确定肿瘤生长抑制作用。扩散加权磁共振成像用于监测早期肿瘤反应。大部分(12/15)基底样细胞系对TRA-8诱导的细胞毒性非常敏感(IC 50 值为1.0–49 ng / ml)。相反,8/11腔或HER2阳性细胞系具有耐药性(IC 50

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