Department of Biochemistry and Molecular Medicine, University of California at Davis Comprehensive Cancer Center, Sacramento, California 95817, USA.
J Biol Chem. 2013 Jul 26;288(30):21593-605. doi: 10.1074/jbc.M113.486050. Epub 2013 May 30.
Lrig1 is the founding member of the Lrig family of transmembrane leucine-rich repeat proteins, which also includes Lrig2 and Lrig3. Lrig1 is a negative regulator of oncogenic receptor tyrosine kinases, including ErbB and Met receptors, and promotes receptor degradation. Lrig1 has recently emerged as both a tumor suppressor and a key regulator of epidermal and epithelial stem cell quiescence. Despite this, little is known of the mechanisms by which Lrig1 is regulated. Lrig3 was recently reported to increase ErbB receptor expression suggesting that it may function in a manner opposite to Lrig1. In this study, we explore the interaction between Lrig1 and Lrig3 and demonstrate that Lrig1 and Lrig3 functionally oppose one another. Lrig3 opposes Lrig1 negative regulatory activity and stabilizes ErbB receptors. Conversely, Lrig1 destabilizes Lrig3, limiting Lrig3's positive effects on receptors and identifying Lrig3 as a new target of Lrig1. These studies provide new insight into the regulation of Lrig1 and uncover a complex cross-talk between Lrig1 and Lrig3.
Lrig1 是跨膜亮氨酸丰富重复蛋白 Lrig 家族的创始成员,该家族还包括 Lrig2 和 Lrig3。Lrig1 是致癌受体酪氨酸激酶(包括 ErbB 和 Met 受体)的负调节剂,可促进受体降解。Lrig1 最近不仅被认为是肿瘤抑制因子,还是表皮和上皮干细胞静止的关键调节因子。尽管如此,Lrig1 的调控机制仍知之甚少。最近有报道称 Lrig3 可增加 ErbB 受体的表达,表明其可能以与 Lrig1 相反的方式发挥作用。在这项研究中,我们探讨了 Lrig1 和 Lrig3 之间的相互作用,并证明 Lrig1 和 Lrig3 在功能上相互拮抗。Lrig3 拮抗 Lrig1 的负调控活性并稳定 ErbB 受体。相反,Lrig1 使 Lrig3 不稳定,限制了 Lrig3 对受体的正向作用,并将 Lrig3 确定为 Lrig1 的新靶标。这些研究为 Lrig1 的调控提供了新的见解,并揭示了 Lrig1 和 Lrig3 之间复杂的交叉对话。
