4-硝基喹啉1-氧化物诱导大鼠舌癌的多遗传易感性和抗性

Jun-ichi Tanuma , Motoo Kitano , Hayase Shisa , Hiroshi Hiai
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引用次数: 9

摘要

大鼠口服4-硝基喹啉1-氧化物(4NQO)可引起高发病率的舌癌(TCs)。大鼠近交系Dark-Agouti (DA)菌株对4nqo诱导的TCs的敏感性明显高于Wistar-Furth (WF)菌株。我们之前对两种菌株杂交的研究假设DA大鼠具有半显性易感基因,WF大鼠具有半显性抗性基因。这一假设得到了pcr微卫星遗传分析的证实。以直径为5 mm的TCS的数量为定量参数,我们在Chr 19的D19Mit9位点附近定位了一个有利于TC发育的数量性状位点Stc1(对TC的敏感性),LOD评分峰值为6.08。Chr 3和Chr 14的2个区域的易感性呈弱连锁,但无统计学意义。另一方面,在D1Mit1和D1Mit3位点之间的Chr. 1上定位了另一个提供抗TC的数量性状位点Rtc1,其LOD值峰值为3.30。舌部或上消化道肿瘤数量、较大肿瘤发生频率及最大肿瘤大小等定量参数密切相关,主要由Stc1和Rtc1决定。因此,DA和WF杂交对4nqo诱导的TCs的易感性可以用这两个位点的基因型组合来解释。讨论了Stc1和Rtc1可能的候选基因。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Polygenetic susceptibility and resistance to 4-nitroquinoline 1-oxide-induced tongue carcinomas in the rat

Oral administration of 4-nitroquinoline 1-oxide (4NQO) to rats induced a high incidence of tongue carcinomas (TCs). The inbred Dark-Agouti (DA) strain of rats showed much higher susceptibility to 4NQO-induced TCs than the Wistar-Furth (WF) strain. Our previous study on crosses between the two strains postulated a semidominant susceptibility gene in DA and a semidominant resistance gene in WF rats. This hypothesis was confirmed by the genetic analysis of the back-crosses to either parent with PCR-based microsatellite assay. Using the number of TCS with >5 mm diameter as a quantitative parameter, we mapped a quantitative trait locus Stc1 (Susceptibility to TC) favouring TC development near the locus D19Mit9 on Chr. 19 with a peak LOD score of 6.08. Two other regions in Chr. 3 and Chr. 14 showed weak linkage for susceptibility, but were not statistically significant. On the other hand, another quantitative trait locus Rtc1 (Resistance to TC) providing resistance to TCs was mapped on Chr. 1 between the loci of D1Mit1 and D1Mit3 with a peak LOD score of 3.30. Quantitative parameters such as the number of tumours in the tongue or upper alimentary tract, the frequency of larger tumours and their maximum size were closely correlated and principally determined by Stc1 and Rtc1. Therefore the susceptibility to 4NQO-induced TCs in crosses between DA and WF is explained by the combinations of genotypes at these two loci. Possible candidate genes for Stc1 and Rtc1 are discussed.

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