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Research Paper
Novel Splice Isoforms of STRADα Differentially Affect LKB1 Activity, Complex Assembly and Subcellular Localization.
Paola Marignani, Kristine Scott, Rosanna Bagnulo, Domenico Cannone, Eleonora Ferrari, Alessandro Stella, Ginevra Guanti, Cristiano Simone and Nicoletta Resta
volume 6 | issue 10
October 2007Pages: 1627 - 1631
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STRADα is a pseudokinase that forms a heterotrimeric complex with the scaffolding protein MO25 and the tumour suppressor serine threonine protein kinase LKB1. Mutations in the LKB1 gene are responsible for the Peutz-Jeghers Syndrome (PJS) characterized by a predisposition to hamartomatous polyps and hyperpigmentation of the buccal mucosa. Mutations in LKB1 have also been observed in some sporadic tumours unrelated to PJS. The LKB1/STRAD/MO25 complex is involved in the regulation of numerous signaling pathways including metabolism, proliferation, and cellular polarity of human intestinal epithelial cells.
Cell polarization, together with tissue-restricted transcription, represents the main feature of enterocyte differentiation. Since a full-length STRADα transcript has not been identified thus far in these cells, we evaluated the expression of endogenous STRADα in 5 colorectal cancer cell lines characterized by their diverse ability to differentiate in vitro. We report herein the discovery of several novel splice isoforms of STRADα that differentially affect the kinase activity, complex assembly, subcellular localization of LKB1 and the activation of the LKB1-dependent AMPK pathway.