Young Christian D, Nolte Erica C, Lewis Andrew, Serkova Natalie J, Anderson Steven M
Department of Pathology, University of Colorado Denver, Research Complex I, South Tower, Mail Stop 8104, 12801 East 17thAvenue, Aurora, CO 80045, USA.
Breast Cancer Res. 2008;10(4):R70. doi: 10.1186/bcr2132. Epub 2008 Aug 13.
ErbB2, a member of the epidermal growth factor receptor (EGFR) family, is overexpressed in 20% to 30% of human breast cancer cases and forms oncogenic signalling complexes when dimerised to ErbB3 or other EGFR family members.
We crossed mouse mammary tumour virus (MMTV)-myr-Akt1 transgenic mice (which express constitutively active Akt1 in the mammary gland) with MMTV-c-ErbB2 transgenic mice to evaluate the role of Akt1 activation in ErbB2-induced mammary carcinoma using immunoblot analysis, magnetic resonance spectroscopy and histological analyses.
Bitransgenic MMTV-c-ErbB2, MMTV-myr-Akt1 mice develop mammary tumours twice as fast as MMTV-c-ErbB2 mice. The bitransgenic tumours were less organised, had more mitotic figures and fewer apoptotic cells. However, many bitransgenic tumours displayed areas of extensive necrosis compared with tumours from MMTV-c-ErbB2 mice. The two tumour types demonstrate dramatically different expression and activation of EGFR family members, as well as different metabolic profiles. c-ErbB2 tumours demonstrate overexpression of EGFR, ErbB2, ErbB3 and ErbB4, and activation/phosphorylation of both ErbB2 and ErbB3, underscoring the importance of the entire EGFR family in ErbB2-induced tumourigenesis. Tumours from bitransgenic mice overexpress the myr-Akt1 and ErbB2 transgenes, but there was dramatically less overexpression and phosphorylation of ErbB3, diminished phosphorylation of ErbB2, decreased level of EGFR protein and undetectable ErbB4 protein. There was also an observable attenuation in a subset of tyrosine-phosphorylated secondary signalling molecules in the bitransgenic tumours compared with c-ErbB2 tumours, but Erk was activated/phosphorylated in both tumour types. Finally, the bitransgenic tumours were metabolically more active as indicated by increased glucose transporter 1 (GLUT1) expression, elevated lactate production and decreased intracellular glucose (suggesting increased glycolysis).
Expression of activated Akt1 in MMTV-c-ErbB2 mice accelerates tumourigenesis with a reduced requirement for signalling through the EGFR family, as well as a reduced requirement for a subset of downstream signaling molecules with a metabolic shift in the tumours from bitransgenic mice. The reduction in signalling downstream of ErbB2 when Akt is activated suggest a possible mechanism by which tumour cells can become resistant to ErbB2-targeted therapies, necessitating therapies that target oncogenic signalling events downstream of ErbB2.
ErbB2是表皮生长因子受体(EGFR)家族的成员之一,在20%至30%的人类乳腺癌病例中过表达,当与ErbB3或其他EGFR家族成员二聚化时会形成致癌信号复合物。
我们将小鼠乳腺肿瘤病毒(MMTV)-myr-Akt1转基因小鼠(在乳腺中组成性表达活性Akt1)与MMTV-c-ErbB2转基因小鼠杂交,通过免疫印迹分析、磁共振波谱分析和组织学分析来评估Akt1激活在ErbB2诱导的乳腺癌中的作用。
双转基因MMTV-c-ErbB2、MMTV-myr-Akt1小鼠发生乳腺肿瘤的速度是MMTV-c-ErbB2小鼠的两倍。双转基因肿瘤的组织结构较差,有更多的有丝分裂象和更少的凋亡细胞。然而,与MMTV-c-ErbB2小鼠的肿瘤相比,许多双转基因肿瘤显示出广泛的坏死区域。这两种肿瘤类型在EGFR家族成员的表达和激活以及代谢谱方面表现出显著差异。c-ErbB2肿瘤显示EGFR、ErbB2、ErbB3和ErbB4过表达,以及ErbB2和ErbB3的激活/磷酸化,强调了整个EGFR家族在ErbB2诱导的肿瘤发生中的重要性。双转基因小鼠的肿瘤过表达myr-Akt1和ErbB2转基因,但ErbB3的过表达和磷酸化明显减少,ErbB2的磷酸化减少,EGFR蛋白水平降低且未检测到ErbB4蛋白。与c-ErbB2肿瘤相比,双转基因肿瘤中一部分酪氨酸磷酸化的二级信号分子也有明显减弱,但两种肿瘤类型中的Erk均被激活/磷酸化。最后,双转基因肿瘤的代谢活性更高,表现为葡萄糖转运蛋白1(GLUT1)表达增加、乳酸产生增加和细胞内葡萄糖减少(提示糖酵解增加)。
在MMTV-c-ErbB2小鼠中激活的Akt1的表达加速了肿瘤发生,对通过EGFR家族的信号传导需求减少,对一部分下游信号分子的需求也减少,双转基因小鼠肿瘤出现代谢转变。当Akt被激活时ErbB2下游信号传导的减少提示了肿瘤细胞可能对ErbB2靶向治疗产生耐药性的一种可能机制,因此需要针对ErbB2下游致癌信号事件的治疗方法。
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