Chatterjee Arpita, Kosmacek Elizabeth A, Oberley-Deegan Rebecca E
Department of Biochemistry and Molecular Biology, University of Nebraska Medical Center, Omaha, Nebraska 68198.
Radiat Res. 2017 Mar;187(3):367-381. doi: 10.1667/RR14623.1. Epub 2017 Feb 22.
Prostate cancer patients who undergo radiotherapy frequently suffer from side effects caused by radiation-induced damage to normal tissues adjacent to the tumor. Exposure of these normal cells during radiation treatment can result in tissue fibrosis and cellular senescence, which ultimately leads to postirradiation-related chronic complications including urinary urgency and frequency, erectile dysfunction, urethral stricture and incontinence. Radiation-induced reactive oxygen species (ROS) have been reported as the most potent causative factor for radiation damage to normal tissue. While MnTE-2-PyP, a ROS scavenger, protects normal cells from radiation-induced damage, it does not protect cancer cells during radiation treatment. However, the mechanism by which MnTE-2-PyP provides protection from radiation-induced fibrosis has been unclear. Our current study reveals the underlying molecular mechanism of radiation protection by MnTE-2-PyP in normal mouse prostate fibroblast cells. To investigate the role of MnTE-2-PyP in normal tissue protection after irradiation, primary prostate fibroblasts from C57BL/6 mice were cultured in the presence or absence of MnTE-2-PyP and exposed to 2 Gy of X rays. We found that MnTE-2-PyP could protect primary prostate fibroblasts from radiation-induced activation, as measured by the contraction of collagen discs, and senescence, detected by beta-galactosidase staining. We observed that MnTE-2-PyP inhibited the TGF-β-mediated fibroblast activation pathway by downregulating the expression of TGF-β receptor 2, which in turn reduced the activation and/or expression of SMAD2, SMAD3 and SMAD4. As a result, SMAD2/3-mediated transcription of profibrotic markers was reduced by MnTE-2-PyP. Due to the inhibition of the TGF-β pathway, fibroblasts treated with MnTE-2-PyP could resist radiation-induced activation and senescence. NADPH oxidase 4 (NOX4) expression is upregulated after irradiation and produces ROS. As was observed with MnTE-2-PyP treatment, NOX4 fibroblasts were protected from radiation-induced fibroblast activation and senescence. However, NOX4 fibroblasts had reduced levels of active TGF-β1, which resulted in decreased TGF-β signaling. Therefore, our data suggest that reduction of ROS levels, either by MnTE-2-PyP treatment or by eliminating NOX4 activity, significantly protects normal prostate tissues from radiation-induced tissue damage, but that these approaches work on different components of the TGF-β signaling pathway. This study proposes a crucial insight into the molecular mechanism executed by MnTE-2-PyP when utilized as a radioprotector. An understanding of how this molecule works as a radioprotector will lead to a better controlled mode of treatment for post therapy complications in prostate cancer patients.
接受放射治疗的前列腺癌患者经常遭受因辐射对肿瘤附近正常组织造成损伤而引起的副作用。在放射治疗期间,这些正常细胞受到照射会导致组织纤维化和细胞衰老,最终引发与放疗相关的慢性并发症,包括尿急、尿频、勃起功能障碍、尿道狭窄和尿失禁。辐射诱导产生的活性氧(ROS)据报道是导致正常组织辐射损伤的最主要因素。虽然ROS清除剂MnTE-2-PyP可保护正常细胞免受辐射诱导的损伤,但在放射治疗期间它并不能保护癌细胞。然而,MnTE-2-PyP提供辐射诱导纤维化防护的机制尚不清楚。我们目前的研究揭示了MnTE-2-PyP在正常小鼠前列腺成纤维细胞中提供辐射防护的潜在分子机制。为了研究MnTE-2-PyP在照射后对正常组织的保护作用,将来自C57BL/6小鼠的原代前列腺成纤维细胞在有或无MnTE-2-PyP的情况下进行培养,并暴露于2 Gy的X射线下。我们发现,通过胶原蛋白圆盘收缩来衡量,MnTE-2-PyP可以保护原代前列腺成纤维细胞免受辐射诱导的激活,通过β-半乳糖苷酶染色检测发现其可防止细胞衰老。我们观察到,MnTE-2-PyP通过下调TGF-β受体2的表达来抑制TGF-β介导的成纤维细胞激活途径,这反过来又降低了SMAD2、SMAD3和SMAD4的激活和/或表达。结果,MnTE-2-PyP减少了SMAD2/3介导的促纤维化标志物的转录。由于TGF-β途径受到抑制,用MnTE-2-PyP处理的成纤维细胞可以抵抗辐射诱导的激活和衰老。照射后NADPH氧化酶4(NOX4)的表达上调并产生活性氧。正如用MnTE-2-PyP处理所观察到的那样,NOX4成纤维细胞免受辐射诱导的成纤维细胞激活和衰老。然而,NOX4成纤维细胞中活性TGF-β1水平降低,导致TGF-β信号传导减少。因此,我们的数据表明,通过MnTE-2-PyP处理或消除NOX4活性来降低活性氧水平,可显著保护正常前列腺组织免受辐射诱导的组织损伤,但这些方法作用于TGF-β信号通路的不同组分。这项研究为MnTE-2-PyP用作辐射防护剂时所执行的分子机制提供了关键见解。了解该分子如何作为辐射防护剂发挥作用,将有助于更好地控制前列腺癌患者治疗后并发症的治疗模式。
