Grosset Andrée-Anne, Labrie Marilyne, Gagné Donald, Vladoiu Maria-Claudia, Gaboury Louis, Doucet Nicolas, St-Pierre Yves
INRS-Institut Armand-Frappier, 531 Blv, des Prairies, Laval, Quebec H7V 1B7, Canada.
BMC Cancer. 2014 Nov 3;14:801. doi: 10.1186/1471-2407-14-801.
Resistance to apoptosis induced by anti-cancer drugs is a major obstacle for the treatment of aggressive forms of breast cancer. Galectin-7 (gal-7) was recently shown to be specifically expressed in basal-like but not in luminal subtypes of human breast cancer.
We generated a mutant form of gal-7 (R74S). Arginine 74 is the structural equivalent of arginine 186 found in human galectin-3. Mutation R186S was previously shown to abolish the biological function of galectin-3.
Mutation of arginine 74 induced only limited and local changes to the gal-7 fold. Recombinant forms of R74S and wtgal-7 were also equally effective at forming dimers in solution. Analysis of the thermodynamic parameters by isothermal titration calorimetry (ITC) indicated, however, that binding of lactose to gal-7 was inhibited by the R74S mutation. Using confocal microscopy and electron microscopy, we confirmed the expression of gal-7 in the cytosolic and nuclear compartments of breast cancer cells and the ability of gal-7 to translocate to mitochondria. The mutation at position 74, however, greatly reduced the expression of gal-7 in the nuclear and mitochondrial compartments. Interestingly, cells expressing mutated gal-7 were equally if not even more resistant to drug-induced apoptosis when compared to cells expressing wtgal-7. We also found that both wtgal-7 and R74S inhibited dox-induced PARP-1 cleavage and p53 protein expression. The inhibition of p53 correlated with a decrease in p21 protein expression and CDKN1A mRNA. Furthermore, analysis of nuclear and cytoplasmic fractions showed that both wild type and R74S mutant gal-7 inhibited p53 nuclear translocation, possibly by increasing degradation of cytosolic p53.
These findings pose a challenge to the paradigm that has guided the design of galectin-specific inhibitors for the treatment of cancer. This study suggests that targeting CRD-independent cytosolic gal-7 in breast cancer cells may be a valuable strategy for the treatment of this disease. Our study will thus complement efforts towards improving selectivity of targeted anticancer agents.
抗癌药物诱导的细胞凋亡抗性是侵袭性乳腺癌治疗的主要障碍。最近研究表明,半乳糖凝集素-7(gal-7)在人乳腺癌的基底样亚型中特异性表达,而在管腔亚型中不表达。
我们构建了一种gal-7突变体形式(R74S)。精氨酸74在结构上等同于人类半乳糖凝集素-3中的精氨酸186。先前研究表明,R186S突变会消除半乳糖凝集素-3的生物学功能。
精氨酸74的突变仅对半乳糖凝集素-7的折叠结构产生有限的局部变化。R74S和野生型gal-7的重组形式在溶液中形成二聚体的效果同样有效。然而,通过等温滴定量热法(ITC)分析热力学参数表明,R74S突变抑制了乳糖与gal-7的结合。利用共聚焦显微镜和电子显微镜,我们证实了gal-7在乳腺癌细胞的胞质和核区室中的表达以及gal-7转运至线粒体的能力。然而,74位的突变极大地降低了gal-7在核区室和线粒体区室中的表达。有趣的是,与表达野生型gal-7的细胞相比,表达突变型gal-7的细胞对药物诱导的细胞凋亡具有同等甚至更强的抗性。我们还发现,野生型gal-7和R74S均抑制阿霉素诱导的PARP-1裂解和p53蛋白表达。p53的抑制与p21蛋白表达和CDKN1A mRNA的减少相关。此外,对核和细胞质组分的分析表明,野生型和R74S突变型gal-7均抑制p53核转位,可能是通过增加胞质p53的降解来实现。
这些发现对指导设计用于癌症治疗的半乳糖凝集素特异性抑制剂的范例提出了挑战。本研究表明,靶向乳腺癌细胞中不依赖CRD的胞质gal-7可能是治疗该疾病的一种有价值的策略。因此,我们的研究将补充提高靶向抗癌药物选择性的努力。
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