TSC2
TSC1
结节性硬化
PI3K/AKT/mTOR通路
癌症研究
激酶
医学
西罗莫司
RPTOR公司
生物
信号转导
内科学
病理
细胞生物学
作者
Laifong Lee,Paul Sudentas,Brian Donohue,Kirsten Asrican,Aelaf Worku,Victoria Walker,Yanping Sun,Karl Schmidt,Mitchell S. Albert,Nisreen El‐Hashemite,Alan S. Lader,Hiroaki Onda,Hongbing Zhang,David J. Kwiatkowski,Sandra L. Dabora
摘要
Tuberous sclerosis complex (TSC) is a familial tumor disorder for which there is no effective medical therapy. Disease-causing mutations in the TSC1 or TSC2 gene lead to increased mammalian target of rapamycin (mTOR) kinase activity in the conserved mTOR signaling pathway, which regulates nutrient uptake, cell growth, and protein translation. The normal function of TSC1 and TSC2 gene products is to form a complex that reduces mTOR kinase activity. Thus, mTOR kinase inhibition may be a useful targeted therapeutic approach. Elevated interferon-gamma (IFN-gamma) expression is associated with decreased severity of kidney tumors in TSC patients and mouse models; therefore, IFN-gamma also has therapeutic potential. We studied cohorts of Tsc2+/- mice and a novel mouse model of Tsc2-null tumors in order to evaluate the efficacy of targeted therapy for TSC. We found that treatment with either an mTOR kinase inhibitor (CCI-779, a rapamycin analog) or with IFN-gamma reduced the severity of TSC-related disease without significant toxicity. These results constitute definitive preclinical data that justify proceeding with clinical trials using these agents in selected patients with TSC and related disorders.
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