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本文引用的文献

1
Src family kinase oncogenic potential and pathways in prostate cancer as revealed by AZD0530.AZD0530揭示的Src家族激酶在前列腺癌中的致癌潜力及通路
Oncogene. 2008 Oct 23;27(49):6365-75. doi: 10.1038/onc.2008.250. Epub 2008 Aug 4.
2
Inhibition of protein kinase c-Src as a therapeutic approach for cancer and bone metastases.抑制蛋白激酶c-Src作为癌症和骨转移的一种治疗方法。
Anticancer Agents Med Chem. 2008 Apr;8(3):342-9. doi: 10.2174/187152008783961905.
3
Regulation of Id1 expression by SRC: implications for targeting of the bone morphogenetic protein pathway in cancer.SRC对Id1表达的调控:对癌症中骨形态发生蛋白通路靶向治疗的意义。
Cancer Res. 2008 Apr 1;68(7):2250-8. doi: 10.1158/0008-5472.CAN-07-6403.
4
Cancer statistics, 2008.2008年癌症统计数据。
CA Cancer J Clin. 2008 Mar-Apr;58(2):71-96. doi: 10.3322/CA.2007.0010. Epub 2008 Feb 20.
5
Nonreceptor tyrosine kinases in prostate cancer.前列腺癌中的非受体酪氨酸激酶
Neoplasia. 2007 Feb;9(2):90-100. doi: 10.1593/neo.06694.
6
Inappropriate activation of the androgen receptor by nonsteroids: involvement of the Src kinase pathway and its therapeutic implications.非甾体类物质对雄激素受体的不适当激活:Src激酶途径的参与及其治疗意义。
Cancer Res. 2006 Nov 1;66(21):10449-59. doi: 10.1158/0008-5472.CAN-06-2582.
7
Evaluation of prostate-specific antigen declines for surrogacy in patients treated on SWOG 99-16.SWOG 99-16研究中接受治疗患者的前列腺特异性抗原下降情况用于代孕评估。
J Natl Cancer Inst. 2006 Apr 19;98(8):516-21. doi: 10.1093/jnci/djj129.
8
Resveratrol inhibits Src and Stat3 signaling and induces the apoptosis of malignant cells containing activated Stat3 protein.白藜芦醇抑制Src和Stat3信号传导,并诱导含有活化Stat3蛋白的恶性细胞凋亡。
Mol Cancer Ther. 2006 Mar;5(3):621-9. doi: 10.1158/1535-7163.MCT-05-0268.
9
Action of the Src family kinase inhibitor, dasatinib (BMS-354825), on human prostate cancer cells.Src家族激酶抑制剂达沙替尼(BMS-354825)对人前列腺癌细胞的作用。
Cancer Res. 2005 Oct 15;65(20):9185-9. doi: 10.1158/0008-5472.CAN-05-1731.
10
HIF-1alpha, STAT3, CBP/p300 and Ref-1/APE are components of a transcriptional complex that regulates Src-dependent hypoxia-induced expression of VEGF in pancreatic and prostate carcinomas.缺氧诱导因子-1α(HIF-1α)、信号转导和转录激活因子3(STAT3)、CREB结合蛋白/ p300(CBP/p300)以及氧化还原因子-1/脱嘌呤嘧啶核酸内切酶(Ref-1/APE)是一种转录复合物的组成成分,该复合物可调节Src依赖的缺氧诱导的胰腺癌和前列腺癌中血管内皮生长因子(VEGF)的表达。
Oncogene. 2005 Apr 28;24(19):3110-20. doi: 10.1038/sj.onc.1208513.

Src激酶抑制剂AZD0530用于晚期去势抵抗性前列腺癌患者的II期试验:一项加利福尼亚癌症联盟研究。

A phase II trial of the Src-kinase inhibitor AZD0530 in patients with advanced castration-resistant prostate cancer: a California Cancer Consortium study.

作者信息

Lara Primo N, Longmate Jeff, Evans Christopher P, Quinn David I, Twardowski Przemyslaw, Chatta Gurkamal, Posadas Edwin, Stadler Walter, Gandara David R

机构信息

University of California Davis Cancer Center, Sacramento, California 95817, USA.

出版信息

Anticancer Drugs. 2009 Mar;20(3):179-84. doi: 10.1097/CAD.0b013e328325a867.

DOI:10.1097/CAD.0b013e328325a867
PMID:19396016
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC3225398/
Abstract

Prostate cancer cells undergo neuroendocrine differentiation during androgen deprivation and secrete neuropeptides, hence activating androgen receptor-regulated genes. Src-family protein kinases are involved in neuropeptide-induced prostate cancer growth and migration. A phase II trial of AZD0530, an oral Src-family kinase inhibitor, in patients with advanced castration resistant prostate cancer was conducted. The primary endpoint was prostate cancer-specific antigen (PSA) response rate, defined as a 30% or greater decrease. A two-stage Simon design was used. Eligibility criteria included documentation of castration resistance (including antiandrogen withdrawal), adequate end-organ function, and performance status, and not more than one prior taxane-based chemotherapy regimen. AZD0530 was given at 175 mg orally once daily continuously. Rapid accrual led to 28 patients registering in the first stage. Median age was 67 years. Sixteen patients had performance status (PS) 0, eight patients had PS 1, and four patients had PS 2. Nine patients (32%) had prior docetaxel-based chemotherapy. Five patients had transient PSA reductions not meeting PSA response criteria. Median progression-free survival time was 8 weeks. Treatment was generally well tolerated. AZD0530, a potent oral Src kinase inhibitor, is feasible and tolerable in this pretreated patient population but possessed little clinical efficacy as monotherapy. Strong preclinical evidence warrants further investigation of AZD0530 in earlier-stage prostate cancer or as combination therapy.

摘要

前列腺癌细胞在雄激素剥夺期间会经历神经内分泌分化并分泌神经肽,从而激活雄激素受体调控的基因。Src家族蛋白激酶参与神经肽诱导的前列腺癌生长和迁移。对口服Src家族激酶抑制剂AZD0530开展了一项针对晚期去势抵抗性前列腺癌患者的II期试验。主要终点是前列腺癌特异性抗原(PSA)反应率,定义为降低30%或更多。采用了两阶段西蒙设计。入选标准包括去势抵抗的记录(包括抗雄激素撤药)、足够的终末器官功能和体能状态,且既往接受不超过一种基于紫杉烷的化疗方案。AZD0530以175mg口服,每日一次,持续给药。快速入组导致28例患者在第一阶段登记。中位年龄为67岁。16例患者体能状态(PS)为0,8例患者PS为1,4例患者PS为2。9例患者(32%)既往接受过基于多西他赛的化疗。5例患者PSA出现短暂降低,但未达到PSA反应标准。中位无进展生存时间为8周。治疗总体耐受性良好。AZD0530是一种有效的口服Src激酶抑制剂,在这群经过预处理的患者中可行且耐受性良好,但作为单一疗法临床疗效甚微。强有力的临床前证据支持在早期前列腺癌中或作为联合疗法对AZD0530进行进一步研究。