Npgrj_NM_1547 348..353
نویسندگان
چکیده
Motor neuron degeneration resulting from the aggregation of the androgen receptor with an expanded polyglutamine tract (AR-polyQ) has been linked to the development of spinal and bulbar muscular atrophy (SBMA or Kennedy disease). Here we report that adding 5-hydroxy-1,7-bis(3,4-dimethoxyphenyl)-1,4,6-heptatrien-3-one (ASC-J9) disrupts the interaction between AR and its coregulators, and also increases cell survival by decreasing AR-polyQ nuclear aggregation and increasing AR-polyQ degradation in cultured cells. Intraperitoneal injection of ASC-J9 into AR-polyQ transgenic SBMA mice markedly improved disease symptoms, as seen by a reduction in muscular atrophy. Notably, unlike previous approaches in which surgical or chemical castration was used to reduce SBMA symptoms, ASC-J9 treatment ameliorated SBMA symptoms by decreasing AR-97Q aggregation and increasing VEGF164 expression with little change of serum testosterone. Moreover, mice treated with ASC-J9 retained normal sexual function and fertility. Collectively, our results point to a better therapeutic and preventative approach to treating SBMA, by disrupting the interaction between AR and AR coregulators.
منابع مشابه
A Complete Bibliography of Publications in the Journal of Cryptology
abelian [326, 408, 91, 337]. Abstract [117]. Accelerated [512]. Accelerating [398]. Achieve [477]. Acoustic [525]. Adaptive [241, 390, 471]. Adaptively [523, 390]. Adic [130]. Advance [279]. Adversarial [458]. Adversaries [353, 345, 357, 403, 450, 472, 501, 236]. Adversary [173]. AES [373, 474, 346, 459]. AES-192 [474]. AES-256 [474]. AES-like [459]. after [76]. Against [353, 480, 520, 348, 500...
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