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Lowe syndrome patient cells display mTOR-and RhoGTPase-dependent phenotypes alleviated by rapamycin and statins

Oxford. 2020-05; 
Kayalvizhi Madhivanan, Swetha Ramadesikan, Wen-Chieh Hsieh, Mariana C Aguilar, Claudia B Hanna, Robert L Bacallao, R Claudio Aguilar
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Proteins, Expression, Isolation and Analysis … Glutamine and 10% fetal bovine serum (FBS) at 37 oC in a 5% CO2 incubator. OCRL1-/- (OCRL KO) HK2 and HEK293T cells were prepared by GenScript Inc. Piscataway, NJ, USA and maintained under same conditions than their normal counterparts … Get A Quote

摘要

Lowe syndrome (LS) is an X-linked developmental disease characterized by cognitive deficiencies, bilateral congenital cataracts and renal dysfunction. Unfortunately, this disease leads to the early death of affected children often due to kidney failure. Although this condition was first described in the early 1950s and the affected gene (OCRL1) was identified in the early 1990s, its pathophysiological mechanism is not fully understood and there is no LS-specific cure available to patients. Here we report two important signaling pathways affected in LS patient cells. While RhoGTPase signaling abnormalities led to adhesion and spreading defects as compared to normal controls, PI3K/mTOR hyperactivation interfered ... More

關鍵詞

phenotypestatinssignal transductionrapamycinadhesionstissue membraneoculocerebrorenal syndromemtor serine-threonine kinases
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