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癌症幸存者后代中的哨兵突变及其他突变效应。

Sentinel and other mutational effects in offspring of cancer survivors.

作者信息

Mulvihill J J

机构信息

National Cancer Institute, Clinical Epidemiology Branch, Bethesda, Maryland 20892.

出版信息

Prog Clin Biol Res. 1990;340C:179-86.

PMID:2381923
Abstract

To date, no agent has been documented to cause germ cell mutation in human beings, with the possible exception of radiation causing abnormal meiotic chromosomes in testes. For studies in humans, mutation epidemiologists prefer the cohort approach, starting with an exposed population and looking for mutations that may be expressed in offspring as variants in health, chromosomes, proteins, or nucleic acids. Currently patients with cancer are the cohort exposed to the largest doses of potential mutagens, i.e., radiotherapy and drugs. In 12 large studies with over 825 patients and 1573 pregnancies, 46 (4%) of 1240 liveborns had a major birth defect, a rate comparable to that in the general population. One of these was a classic sentinel phenotype, i.e., a new sporadic case of a dominant mendelian syndrome. In collaboration with 5 U.S. cancer registries, we interviewed a retrospective cohort of 2383 patients diagnosed with cancer under age 20 years, from 1945 through 1975. Records were sought to verify major genetic disease, defined as a cytogenetic or single gene disorder or 1 of 15 isolated birth defects. In 2308 offspring of survivors, 5 had a chromosomal syndrome, 11 had a single gene disorder, and 62 had at least one major malformation. Among 4722 offspring of sibling controls, the respective numbers were 7, 12, and 127, nonsignificant differences. 7% of the parents of the offspring with possibly new mutations received potentially mutagenic therapy, compared with 12% of parents of normal children. Since pregnancy in or by cancer survivors is still a rare event, future efforts to document germ cell mutation may be best studied through international cooperation coupled with diverse laboratory measures of mutation.

摘要

迄今为止,尚无任何因素被证实可导致人类生殖细胞发生突变,睾丸中减数分裂染色体异常的辐射可能是唯一的例外。对于人类研究,突变流行病学家更倾向于队列研究方法,即从暴露人群入手,寻找可能在后代中表现为健康、染色体、蛋白质或核酸变异的突变。目前,癌症患者是暴露于最大剂量潜在诱变剂(即放疗和药物)的队列。在12项涉及825名以上患者和1573次妊娠的大型研究中,1240名活产儿中有46名(4%)患有严重出生缺陷,这一比例与普通人群相当。其中一例是典型的哨兵表型,即一种新的散发型显性孟德尔综合征病例。我们与美国5个癌症登记处合作,对1945年至1975年间诊断为20岁以下癌症的2383名患者进行了回顾性队列访谈。查找记录以核实主要遗传疾病,主要遗传疾病定义为细胞遗传学或单基因疾病或15种孤立出生缺陷之一。在幸存者的2308名后代中,5名患有染色体综合征,11名患有单基因疾病,62名至少有一处严重畸形。在4722名同胞对照的后代中,相应数字分别为7名、12名和127名,差异无统计学意义。后代可能有新突变的父母中,7%接受了潜在诱变治疗,而正常儿童的父母中这一比例为12%。由于癌症幸存者怀孕或生育仍然是罕见事件,未来记录生殖细胞突变的工作可能最好通过国际合作以及多种突变实验室检测方法来进行研究。

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引用本文的文献

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Congenital anomalies in the children of cancer survivors: a report from the childhood cancer survivor study.癌症幸存者儿童的先天畸形:来自儿童癌症幸存者研究的报告。
J Clin Oncol. 2012 Jan 20;30(3):239-45. doi: 10.1200/JCO.2011.37.2938. Epub 2011 Dec 12.
2
Chronic graft-versus-host disease and late effects after hematopoietic stem cell transplantation.造血干细胞移植后的慢性移植物抗宿主病及晚期效应
Int J Hematol. 2002 Aug;76 Suppl 2:15-28. doi: 10.1007/BF03165081.
3
Case-control study of congenital anomalies in children of cancer patients.
癌症患者子女先天性异常的病例对照研究。
BMJ. 1993 Jul 17;307(6897):164-8. doi: 10.1136/bmj.307.6897.164.