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识别p53反式激活域I特定抑制剂缓解前列腺癌治疗的副作用

Identifying p53 Transactivation Domain 1-Specific Inhibitors to Alleviate the Side Effects of Prostate Cancer Therapy
作者:Attardi, L. D.Raj, N. 作者单位:Stanford Univ., CA. 加工时间:2014-10-24 信息来源:科技报告(AD) 索取原文[14 页]
关键词:前列腺癌;逮捕(过程);化疗;脱氧核糖核的酸;放射疗法;治疗;组织(生物学)
摘 要:The p53 transactivation domain 1 (TAD1) plays a critical role in inducing p53 mediated cell-cycle arrest and apoptosis in response to acute DNA damage caused by irradiation. During radiation therapy of cancers, this p53- induced apoptosis triggers various deleterious pathological side effects in normal tissues. Interestingly, recent studies from our laboratory have demonstrated that p53 TAD1 is completely dispensable for tumor suppression in diverse mouse cancer models. We hypothesize that specific inhibition of p53 TAD1 should ameliorate the p53-associated pathologies occurring in response to acute DNA damage, while keeping p53-mediated tumor suppression intact, thus allowing improvement in the therapeutic index of radiation therapy in cancer. Importantly, because the majority of cancers, such as advanced prostate cancers, have inactivated the p53 pathway, such inhibitors should not compromise the efficacy of treating tumors. We propose to perform high-throughput chemical library screens to identify specific inhibitor of p53 TAD1 that may be administered as adjuvants of chemotherapy and radiotherapy in the context of prostate cancer.
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