Abou El Hassan M A I, Heijn M, Rabelink M J W E, van der Vijgh W J F, Bast A, Hoeben R C
Department of Medical Oncology, Free University Medical Center, PO Box 7057, 1007 MB Amsterdam, The Netherlands.
Cancer Gene Ther. 2003 Apr;10(4):270-7. doi: 10.1038/sj.cgt.7700564.
Doxorubicin-induced cardiotoxicity is related to its production of free radicals that specifically affect heart tissue because of its low antioxidant status. Monohydroxyethylrutoside (monoHER), a potent antioxidant flavonoid, is under development as a protector against doxorubicin-induced cardiotoxicity. The overexpression of high levels of superoxide dismutase (sod) protects against free radical damage in transgenic mice. Seeking alternatives besides the few cardioprotectors that are presently under investigation, the aim of the present study was to investigate the protective effect of cardiac gene transfer of CuZn-sod compared with that of the presently most promising cardioprotector monoHER against doxorubicin-induced cardiotoxic effects on neonatal rat cardiac myocytes (NeRCaMs) in vitro. NeRCaMs were infected with different multiplicity of infections (MOIs) of adenovirus encoding CuZn-sod (AdCuZn-sod). A control infection with an adenovirus vector encoding a nonrelated protein was included. The overexpression of CuZn-sod was characterized within 3 days postinfection. For doxorubicin treatment, NeRCaMs were divided into three groups. The first group was infected with AdCuZn-sod before treatment with doxorubicin (0-50 microM). The second and third groups were treated with doxorubicin (0-50 microM) alone and with 1 mM monoHER, respectively. The LDH release and survival of treated cells were measured 24 and 48 hours after doxorubicin treatment. The beating rate was followed during the 3 days after doxorubicin (0-100 microM) treatment. At the third day after infection with an MOI of 25 plaque-forming unit (PFU) of AdCuZn-sod/cell, the activity of CuZn-sod significantly increased (five-fold, P=.029). Higher MOI produced cytopathic effects (CPEs). Doxorubicin alone produced significant concentration- and time-dependent reduction in NeRCaMs beating rate and survival (P < .0005). Doxorubicin (> or =50 microM)-treated cells ceased to beat after 24 hours. This cytotoxicity was associated with an increase in the LDH release from the treated cells (P <.0005). The five-fold increase in the activity of CuZn-sod did not protect against any of the cytotoxic effects of doxorubicin on NeRCaMs. In contrast, monoHER (1 mM) protected against the lethal effects of doxorubicin on the survival, LDH release and the beating rate of NeRCaMs (P <.004) during 48 hours after doxorubicin treatment. Doxorubicin-treated (< or =100 microM) cells continued beating for >72 hours in the presence of monoHER. The present study showed the lack of adenoviral CuZn-sod gene-transfer to protect myocardiocytes against doxorubicin-induced toxicity and confirms the efficacy of monoHER cardioprotection. Thus, a gene-therapy strategy involving overexpression of CuZn-sod to protect against doxorubicin-induced cardiotoxicity is not feasible with the currently available adenovirus vectors.
阿霉素诱导的心脏毒性与其产生自由基有关,由于心脏组织抗氧化状态低,这些自由基会特异性地影响心脏组织。单羟基乙基芦丁(monoHER)是一种有效的抗氧化类黄酮,正在开发用作预防阿霉素诱导的心脏毒性的保护剂。在转基因小鼠中,高水平超氧化物歧化酶(sod)的过表达可防止自由基损伤。除了目前正在研究的少数心脏保护剂外,本研究的目的是研究与目前最有前景的心脏保护剂monoHER相比,铜锌超氧化物歧化酶(CuZn-sod)心脏基因转移对体外培养的新生大鼠心肌细胞(NeRCaMs)阿霉素诱导的心脏毒性作用的保护效果。NeRCaMs用编码CuZn-sod的腺病毒的不同感染复数(MOI)进行感染。包括用编码无关蛋白的腺病毒载体进行对照感染。在感染后3天内对CuZn-sod的过表达进行表征。对于阿霉素处理,NeRCaMs分为三组。第一组在用阿霉素(0 - 50 microM)处理前用AdCuZn-sod感染。第二组和第三组分别单独用阿霉素(0 - 50 microM)和1 mM monoHER处理。在阿霉素处理后24小时和48小时测量处理后细胞的乳酸脱氢酶(LDH)释放和存活率。在阿霉素(0 - 100 microM)处理后的3天内监测搏动率。在用AdCuZn-sod/细胞的25个噬斑形成单位(PFU)的MOI感染后第三天,CuZn-sod的活性显著增加(五倍,P = 0.029)。更高的MOI产生细胞病变效应(CPEs)。单独使用阿霉素使NeRCaMs的搏动率和存活率显著降低,且呈浓度和时间依赖性(P < 0.0005)。用阿霉素(≥50 microM)处理的细胞在24小时后停止搏动。这种细胞毒性与处理后细胞中LDH释放增加有关(P < 0.0005)。CuZn-sod活性增加五倍并不能预防阿霉素对NeRCaMs的任何细胞毒性作用。相比之下,在阿霉素处理后的48小时内,monoHER(1 mM)可预防阿霉素对NeRCaMs的存活、LDH释放和搏动率产生的致死作用(P < 0.004)。在存在monoHER的情况下,用阿霉素(≤100 microM)处理的细胞持续搏动超过72小时。本研究表明腺病毒介导的CuZn-sod基因转移不能保护心肌细胞免受阿霉素诱导的毒性,并证实了monoHER心脏保护作用的有效性。因此,目前可用的腺病毒载体采用涉及CuZn-sod过表达以预防阿霉素诱导的心脏毒性的基因治疗策略是不可行的。
