Chang Joan, Nicolau Monica M, Cox Thomas R, Wetterskog Daniel, Martens John W M, Barker Holly E, Erler Janine T
Breast Cancer Res. 2013;15(4):R67. doi: 10.1186/bcr3461.
Lysyl oxidase-like 2 (LOXL2) is a matrix-remodeling enzyme that has been shown to play a key role in invasion and metastasis of breast carcinoma cells. However, very little is known about its role in normal tissue homeostasis. Here, we investigated the effects of LOXL2 expression in normal mammary epithelial cells to gain insight into how LOXL2 mediates cancer progression.
LOXL2 was expressed in MCF10A normal human mammary epithelial cells. The 3D acinar morphogenesis of these cells was assessed, as well as the ability of the cells to form branching structures on extracellular matrix (ECM)-coated surfaces. Transwell-invasion assays were used to assess the invasive properties of the cells. Clinically relevant inhibitors of ErbB2, lapatinib and Herceptin (traztuzumab), were used to investigate the role of ErbB2 signaling in this model. A retrospective study on a previously published breast cancer patient dataset was carried out by using Disease Specific Genomic Analysis (DSGA) to investigate the correlation of LOXL2 mRNA expression level with metastasis and survival of ErbB2-positive breast cancer patients.
Fluorescence staining of the acini revealed increased proliferation, decreased apoptosis, and disrupted polarity, leading to abnormal lumen formation in response to LOXL2 expression in MCF10A cells. When plated onto ECM, the LOXL2-expressing cells formed branching structures and displayed increased invasion. We noted that LOXL2 induced ErbB2 activation through reactive oxygen species (ROS) production, and ErbB2 inhibition by using Herceptin or lapatinib abrogated the effects of LOXL2 on MCF10A cells. Finally, we found LOXL2 expression to be correlated with decreased overall survival and metastasis-free survival in breast cancer patients with ErbB2-positive tumors.
These findings suggest that LOXL2 expression in normal epithelial cells can induce abnormal changes that resemble oncogenic transformation and cancer progression, and that these effects are driven by LOXL2-mediated activation of ErbB2. LOXL2 may also be a beneficial marker for breast cancer patients that could benefit most from anti-ErbB2 therapy.
赖氨酰氧化酶样2(LOXL2)是一种基质重塑酶,已被证明在乳腺癌细胞的侵袭和转移中起关键作用。然而,关于其在正常组织稳态中的作用却知之甚少。在此,我们研究了LOXL2在正常乳腺上皮细胞中的表达影响,以深入了解LOXL2如何介导癌症进展。
在MCF10A正常人乳腺上皮细胞中表达LOXL2。评估这些细胞的三维腺泡形态发生以及细胞在细胞外基质(ECM)包被表面形成分支结构的能力。使用Transwell侵袭实验评估细胞的侵袭特性。使用临床上相关的ErbB2抑制剂拉帕替尼和赫赛汀(曲妥珠单抗)来研究ErbB2信号通路在该模型中的作用。通过疾病特异性基因组分析(DSGA)对先前发表的乳腺癌患者数据集进行回顾性研究,以调查LOXL2 mRNA表达水平与ErbB2阳性乳腺癌患者转移和生存的相关性。
腺泡的荧光染色显示,MCF10A细胞中因LOXL2表达而导致增殖增加、凋亡减少和极性破坏,进而导致管腔形成异常。当接种到ECM上时,表达LOXL2的细胞形成分支结构并显示出侵袭增加。我们注意到LOXL2通过产生活性氧(ROS)诱导ErbB2激活,使用赫赛汀或拉帕替尼抑制ErbB2可消除LOXL2对MCF10A细胞的影响。最后,我们发现LOXL2表达与ErbB2阳性肿瘤的乳腺癌患者总生存期和无转移生存期降低相关。
这些发现表明,正常上皮细胞中LOXL2的表达可诱导类似于致癌转化和癌症进展的异常变化,并且这些效应由LOXL2介导的ErbB2激活驱动。LOXL2也可能是最能从抗ErbB2治疗中获益的乳腺癌患者的有益标志物。
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