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Bax-Interacting Factor-1 Expression in Prostate Cancer

机译:Bax交互因子1表达在前列腺癌中。

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Background: Bax-interacting factor (Bif)-1 protein is a member of the endophilin B family that binds to and activates the proapoptotic Bax protein in response to apoptotic signals. Loss of Bif-1 suppresses the intrinsic pathway of apoptosis and promotes tumorigenesis. We examined the expression levels of Bif-1 protein in human prostate cancer. Materials and Methods: Thirty-nine archival tissue specimens of human prostate cancer, and a human prostate cancer tissue microar-ray containing 19 samples of normal prostate, 26 samples of benign prostatic hyperplasias (BPHs), 30 samples of high-grade prostatic in-traepithelial neoplasia (PIN), and 153 samples of prostate cancer, were selected for immunohistochemical staining with Bif-1 antibody. The slides were scored by 2 independent observers. Results: Nontissue mi-croarray samples: moderate to strong Bif-1 staining was identified in 38 of 39 prostate cancer samples. In 32 cases, foci of PIN were identified adjacent to prostate cancer samples. Of these, 29 samples (90.6%) showed strong and diffuse Bif-1 staining. Benign prostatic hyperplasias, identified in 27 cases, was weakly Bif-1 positive in 88.9% of cases. Tissue microarray samples: 38.6% (59 of 153) of prostate cancer samples showed moderate to strong Bif-1 expression, and 21.6% (33 of 153) were Bif-1 negative. Bif-1 expression was moderate to strong in 76.7% (23 of 30) of PIN. Bif-1 was weak to moderate in 53.8% (14 of 26) of BPH and negative in 46.2% (12 of 26) of them. Low to moderate Bif-1 was seen in 89.5% of normal prostate samples. Conclusion: The loss of Bif-1 expression in a subset of prostate cancer samples is in agreement with the proapoptotic function of Bif-1. The significance of the increased Bif-1 in a subgroup of prostate cancer samples and in PIN remains to be determined. It seems that Bif-1 has a role in prostate cancer, providing the rationale for using Bif-1 as a target for prostate anticancer therapy.
机译:背景:Bax相互作用因子(Bif)-1蛋白是内啡肽B家族的成员,可响应凋亡信号而结合并激活促凋亡的Bax蛋白。 Bif-1的丢失抑制凋亡的内在途径并促进肿瘤发生。我们检查了人类前列腺癌中Bif-1蛋白的表达水平。材料和方法:39份人类前列腺癌的档案组织标本,以及一份人类前列腺癌组织微射线,其中包含19份正常前列腺样本,26份良性前列腺增生(BPH)样本,30份高级前列腺癌样本。选择上皮上皮瘤(PIN)和153例前列腺癌样本进行Bif-1抗体免疫组织化学染色。幻灯片由2位独立观察员进行了评分。结果:非组织微阵列样品:在39个前列腺癌样品中的38个中鉴定出中度至强Bif-1染色。在32例病例中,在前列腺癌样本附近发现了PIN病灶。在这些样本中,有29个样本(占90.6%)显示出强烈且弥漫的Bif-1染色。良性前列腺增生症(27例)在88.9%的病例中Bif-1阳性弱。组织微阵列样品:38.6%(153个中的59个)前列腺癌样品显示中度至强Bif-1表达,而21.6%(153个中的33个)Bif-1阴性。 Bif-1表达在PIN的76.7%(30个中的23个)中到中等。 Bif-1在BPH的53.8%(26个中的14)中处于弱到中度水平,在其中的46.2%(26中的12个)中为阴性。在89.5%的正常前列腺样本中观察到低至中度的Bif-1。结论:前列腺癌样本中Bif-1表达的丧失与Bif-1的凋亡功能相一致。 Bif-1在前列腺癌样品亚组和PIN中增加的意义尚待确定。似乎Bif-1在前列腺癌中起作用,为使用Bif-1作为前列腺抗癌治疗的靶标提供了理论依据。

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