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接触遗传毒性剂、宿主因素和生活方式会影响微核中着丝粒信号的数量:一项汇总重新分析。

Exposure to genotoxic agents, host factors, and lifestyle influence the number of centromeric signals in micronuclei: a pooled re-analysis.

作者信息

Iarmarcovai G, Bonassi S, Sari-Minodier I, Baciuchka-Palmaro M, Botta A, Orsière T

机构信息

Laboratory of Biogenotoxicology and Environmental Mutagenesis (EA 1784; IFR PMSE 112), Faculty of Medicine, Université de la Méditerranée, 27 Bd Jean Moulin, 13385 Marseille Cedex 5, France.

出版信息

Mutat Res. 2007 Feb 3;615(1-2):18-27. doi: 10.1016/j.mrfmmm.2006.09.005. Epub 2007 Jan 2.

Abstract

We pooled data from three biomonitoring studies using the cytokinesis-block micronucleus assay in peripheral blood lymphocytes in combination with fluorescence in situ hybridization. Centromere-positive micronuclei (C+MN) were classified in two groups: those containing one centromere (C1+MN) and those with two or more (Cx+MN). The three studies evaluated untreated cancer patients, welders, and pathologists/anatomists exposed to formaldehyde. The total number of subjects included in the pooled re-analysis was 113. A higher frequency of C+MN was observed in cancer patients and exposed workers, who showed significant differences from controls in all studies. C1+MN were particularly increased in the group of pathologists/anatomists, who showed a 3.29 times higher frequency than controls (95% CI: 2.04-5.30). A borderline increase in Cx+MN was observed in welders when compared to the corresponding control group (FR: 1.31; 95% CI: 0.99-1.74). An evident effect of gender was found, with significantly increased frequencies of all endpoints measuring aneuploidy in females (C+MN, C1+MN, and Cx+MN). Alcohol consumption had a significant effect on total MN frequency and particularly on C+MN and C1+MN. In conclusion, scoring the number of centromeric signals in the micronucleus assay provides additional information about the mechanism of action of various genotoxic agents, and the role of confounding factors may be more specifically accounted for. Indeed, C+MN could be efficiently used in biomonitoring studies as an independent biomarker of exposure and early biological effect. The use of centromeric signals allows the identification of two further endpoints, representing two alternative pathways of chromosome loss, i.e., impaired chromosome migration, leading to increased C1+MN frequency, and centrosome amplification, possibly leading to Cx+MN with two or more centromeric signals.

摘要

我们汇总了三项生物监测研究的数据,这些研究采用外周血淋巴细胞中的胞质分裂阻滞微核试验并结合荧光原位杂交技术。着丝粒阳性微核(C+MN)分为两组:含有一个着丝粒的微核(C1+MN)和含有两个或更多个着丝粒的微核(Cx+MN)。这三项研究评估了未接受治疗的癌症患者、焊工以及接触甲醛的病理学家/解剖学家。纳入汇总再分析的受试者总数为113人。在癌症患者和接触甲醛的工人中观察到较高频率的C+MN,在所有研究中,他们与对照组相比均存在显著差异。C1+MN在病理学家/解剖学家组中尤其增加,其频率比对照组高3.29倍(95%可信区间:2.04 - 5.30)。与相应对照组相比,焊工中Cx+MN出现临界性增加(频率比:1.31;95%可信区间:0.99 - 1.74)。发现性别有明显影响,女性中所有测量非整倍体的终点指标(C+MN、C1+MN和Cx+MN)频率均显著增加。饮酒对总微核频率有显著影响,尤其对C+MN和C1+MN有影响。总之,在微核试验中对着丝粒信号数量进行计分可提供有关各种遗传毒性剂作用机制的额外信息,并且可以更具体地考虑混杂因素的作用。实际上,C+MN可作为暴露和早期生物学效应的独立生物标志物有效地用于生物监测研究。使用着丝粒信号可识别另外两个终点指标,代表染色体丢失的两种替代途径,即染色体迁移受损导致C1+MN频率增加,以及中心体扩增,可能导致具有两个或更多个着丝粒信号的Cx+MN。

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