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本文引用的文献

1
Characterization of sperm chromatin quality in testicular cancer and Hodgkin's lymphoma patients prior to chemotherapy.化疗前睾丸癌和霍奇金淋巴瘤患者精子染色质质量的特征分析
Hum Reprod. 2008 May;23(5):1044-52. doi: 10.1093/humrep/den081. Epub 2008 Mar 17.
2
Reversibility of the effects of subchronic exposure to the cancer chemotherapeutics bleomycin, etoposide, and cisplatin on spermatogenesis, fertility, and progeny outcome in the male rat.亚慢性暴露于癌症化疗药物博来霉素、依托泊苷和顺铂对雄性大鼠精子发生、生育能力及子代结局影响的可逆性
J Androl. 2008 Jul-Aug;29(4):408-17. doi: 10.2164/jandrol.107.004218. Epub 2008 Feb 22.
3
Infertility and testis cancer.不孕症与睾丸癌。
Urol Clin North Am. 2007 May;34(2):269-77; abstract xi. doi: 10.1016/j.ucl.2007.02.002.
4
Effects of the chemotherapy cocktail used to treat testicular cancer on sperm chromatin integrity.用于治疗睾丸癌的化疗合剂对精子染色质完整性的影响。
J Androl. 2007 Mar-Apr;28(2):241-9; discussion 250-1. doi: 10.2164/jandrol.106.001487. Epub 2006 Oct 4.
5
Calcium activation of the LMO4 transcription complex and its role in the patterning of thalamocortical connections.LMO4转录复合体的钙激活及其在丘脑皮质连接模式形成中的作用。
J Neurosci. 2006 Aug 9;26(32):8398-408. doi: 10.1523/JNEUROSCI.0618-06.2006.
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Advances in the treatment of testicular cancer.睾丸癌治疗的进展
Drugs. 2006;66(5):641-59. doi: 10.2165/00003495-200666050-00005.
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Epigenetic regulation of testis-specific gene expression.睾丸特异性基因表达的表观遗传调控。
Ann N Y Acad Sci. 2005 Dec;1061:226-42. doi: 10.1196/annals.1336.025.
8
Surveillance programs for stage I nonseminomatous germ cell tumors of the testis.睾丸I期非精原细胞性生殖细胞肿瘤的监测方案。
Urol Oncol. 2006 Jan-Feb;24(1):68-74. doi: 10.1016/j.urolonc.2005.07.006.
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Trends in testicular cancer incidence and mortality in 22 European countries: continuing increases in incidence and declines in mortality.22个欧洲国家睾丸癌发病率和死亡率的趋势:发病率持续上升,死亡率持续下降。
Int J Cancer. 2006 Jun 15;118(12):3099-111. doi: 10.1002/ijc.21747.
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Gene regulation in spermatogenesis.精子发生中的基因调控。
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用于治疗睾丸癌的化疗鸡尾酒对雄性棕色挪威大鼠生殖细胞基因表达谱的影响。

Impact of the chemotherapy cocktail used to treat testicular cancer on the gene expression profile of germ cells from male Brown-Norway rats.

作者信息

Delbès Geraldine, Chan Donovan, Pakarinen Pirjo, Trasler Jacquetta M, Hales Barbara F, Robaire Bernard

机构信息

Department of Pharmacology and Therapeutics, McGill University, Montreal Children's Hospital Research Institute, Montréal, Québec, Canada H3G 1Y6.

出版信息

Biol Reprod. 2009 Feb;80(2):320-7. doi: 10.1095/biolreprod.108.072108. Epub 2008 Nov 5.

DOI:10.1095/biolreprod.108.072108
PMID:18987330
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC2848733/
Abstract

Advances in treatment for testicular cancer that include the coadministration of bleomycin, etoposide, and cisplatin (BEP) have brought the cure rate to higher than 90%%. The goal of this study was to elucidate the impact of BEP treatment on gene expression in male germ cells. Brown-Norway rats were treated for 9 wk with vehicle (0x) or BEP at doses equivalent to 0.3x and 0.6x the human dose. At the end of treatment, spermatogenesis was affected, showing altered histology and a decreased sperm count; spermatozoa had a higher number of DNA breaks. After 9 wk of treatment, round spermatids were isolated, and RNA was extracted and probed on Rat230-2.0 Affymetrix arrays. Of the 31 099 probe sets present on the array, 59%% were expressed in control round spermatids. BEP treatment significantly altered the expression of 221 probe sets, with at least a 1.5-fold change compared with controls; 80% were upregulated. We observed a dose-dependent increase in the expression of oxidative stress response genes and no change in the expression of genes involved in DNA repair. BEP upregulated genes were implicated in pathways related to Jun and Junb protooncogenes. Increased mRNA levels of Jun and Junb were confirmed by quantitative RT-PCR; furthermore, JUN protein was increased in elongating spermatids. Thus, BEP exposure triggers an oxidative stress response in round spermatids and induces many pathways that may lead to the survival of damaged cells and production of abnormal sperm.

摘要

睾丸癌治疗方法的进展,包括联合使用博来霉素、依托泊苷和顺铂(BEP),已使治愈率超过90%。本研究的目的是阐明BEP治疗对雄性生殖细胞基因表达的影响。用载体(0x)或相当于人类剂量0.3倍和0.6倍的BEP对棕色挪威大鼠进行9周治疗。治疗结束时,精子发生受到影响,组织学改变,精子数量减少;精子的DNA断裂数量增加。治疗9周后,分离出圆形精子细胞,提取RNA并在Rat230-2.0 Affymetrix芯片上进行检测。芯片上存在的31099个探针组中,59%在对照圆形精子细胞中表达。BEP治疗显著改变了221个探针组的表达,与对照组相比至少有1.5倍的变化;80%上调。我们观察到氧化应激反应基因的表达呈剂量依赖性增加,而参与DNA修复的基因表达没有变化。BEP上调的基因与Jun和Junb原癌基因相关的信号通路有关。通过定量RT-PCR证实Jun和Junb的mRNA水平增加;此外,在伸长的精子细胞中JUN蛋白增加。因此,暴露于BEP会在圆形精子细胞中引发氧化应激反应,并诱导许多可能导致受损细胞存活和异常精子产生的信号通路。