Khor Li Yan, Moughan Jennifer, Al-Saleem Tahseen, Hammond Elizabeth H, Venkatesan Varagur, Rosenthal Seth A, Ritter Mark A, Sandler Howard M, Hanks Gerald E, Shipley William U, Pollack Alan
Department of Radiation Oncology, Fox Chase Cancer Center, Philadelphia, Pennsylvania 19111, USA.
Clin Cancer Res. 2007 Jun 15;13(12):3585-90. doi: 10.1158/1078-0432.CCR-06-2972.
Bcl-2 is antiapoptotic, and its overexpression has been associated with resistance to androgen deprivation and poor outcome in some patients treated with radiotherapy. Bax is proapoptotic, regulating Bcl-2 through heterodimer formation. In a prior study, Bcl-2 and Bax were not related to outcome in locally advanced patients treated with radiotherapy or short-term androgen deprivation + radiotherapy (STAD+RT) on another Radiation Therapy Oncology Group trial (86-10). A follow-up investigation was carried out here in more contemporary high-risk men treated on Radiation Therapy Oncology Group 92-02 with STAD+RT or long-term AD+RT (LTAD+RT).
Adequate tissue was available to be analyzed immunohistochemically in 502 patients for Bcl-2 and 343 patients for Bax. Univariate and multivariate analyses by Cox proportional hazards models were applied to end points of failure.
Bcl-2 was positive in 45.6% cases, and Bax expression altered in 53.9% cases. Abnormal Bcl-2 was not related to any of the failure end points tested. Altered Bax expression was significantly associated with any failure (P = 0.023) and marginally with biochemical failure (P = 0.085). The combination of negative Bcl-2/normal Bax expression seemed more robust, being significantly related to reduced biochemical failure (P = 0.036) and any failure (P = 0.046). The predictive value of negative Bcl-2/normal Bax was most pronounced in those who received STAD+RT, as opposed to LTAD+RT.
Normal Bax expression was associated with significantly more favorable outcome. The combination of negative Bcl-2 and normal Bax was more consistently significant, particularly when STAD+RT was the treatment administered. These data suggest that LTAD+RT should be used when either Bcl-2 or Bax is abnormally expressed.
Bcl-2具有抗凋亡作用,其过表达与雄激素剥夺抵抗以及部分接受放疗的患者预后不良相关。Bax具有促凋亡作用,通过形成异二聚体调节Bcl-2。在先前一项研究中,在另一项放射治疗肿瘤学组试验(86-10)中,Bcl-2和Bax与接受放疗或短期雄激素剥夺+放疗(STAD+RT)的局部晚期患者的预后无关。在此对接受STAD+RT或长期雄激素剥夺+放疗(LTAD+RT)的更现代的高危男性进行了后续调查,这些患者参与了放射治疗肿瘤学组92-02试验。
有足够的组织可用于对502例患者进行Bcl-2免疫组化分析,对343例患者进行Bax免疫组化分析。通过Cox比例风险模型进行单因素和多因素分析以评估失败终点。
45.6%的病例Bcl-2呈阳性,53.9%的病例Bax表达改变。异常的Bcl-2与所检测的任何失败终点均无关。改变的Bax表达与任何失败显著相关(P = 0.023),与生化失败有边缘相关性(P = 0.085)。Bcl-2阴性/Bax正常表达的组合似乎更具优势,与生化失败减少(P = 0.036)和任何失败(P = 0.046)显著相关。Bcl-2阴性/Bax正常的预测价值在接受STAD+RT的患者中最为明显,与接受LTAD+RT的患者相反。
正常的Bax表达与明显更有利的预后相关。Bcl-2阴性和Bax正常的组合更一致地具有显著性,特别是当采用STAD+RT治疗时。这些数据表明,当Bcl-2或Bax异常表达时应使用LTAD+RT。
