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NF2/Merlin Inactivation and Potential Therapeutic Targets in Mesothelioma
NF2/Merlin Inactivation and Potential Therapeutic Targets in Mesothelioma
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NF2/Merlin Inactivation and Potential Therapeutic Targets in Mesothelioma
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NF2/Merlin Inactivation and Potential Therapeutic Targets in Mesothelioma
NF2/Merlin Inactivation and Potential Therapeutic Targets in Mesothelioma
Journal Article

NF2/Merlin Inactivation and Potential Therapeutic Targets in Mesothelioma

2018
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Overview
The neurofibromatosis type 2 (NF2) gene encodes merlin, a tumor suppressor protein frequently inactivated in schwannoma, meningioma, and malignant mesothelioma (MM). The sequence of merlin is similar to that of ezrin/radixin/moesin (ERM) proteins which crosslink actin with the plasma membrane, suggesting that merlin plays a role in transducing extracellular signals to the actin cytoskeleton. Merlin adopts a distinct closed conformation defined by specific intramolecular interactions and regulates diverse cellular events such as transcription, translation, ubiquitination, and miRNA biosynthesis, many of which are mediated through Hippo and mTOR signaling, which are known to be closely involved in cancer development. MM is a very aggressive tumor associated with asbestos exposure, and genetic alterations in NF2 that abrogate merlin’s functional activity are found in about 40% of MMs, indicating the importance of NF2 inactivation in MM development and progression. In this review, we summarize the current knowledge of molecular events triggered by NF2/merlin inactivation, which lead to the development of mesothelioma and other cancers, and discuss potential therapeutic targets in merlin-deficient mesotheliomas.