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首页> 外文期刊>Carcinogenesis >The presence of the intron 3 16 bp duplication polymorphism of p53 (rs17878362) in breast cancer is associated with a low Delta 40p53:p53 ratio and better outcome
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The presence of the intron 3 16 bp duplication polymorphism of p53 (rs17878362) in breast cancer is associated with a low Delta 40p53:p53 ratio and better outcome

机译:p53(rs17878362)的内含子3 16 bp复制多态性的存在与低Delta 40p53:p53比率和更好的预后相关

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摘要

Breast cancer is the most common female cancer, but it has relatively low rates of p53 mutations, suggesting other mechanisms are responsible for p53 inactivation. We have shown that the p53 isoform, Delta 40p53, is highly expressed in breast cancer, where it may contribute to p53 inactivation. Delta 40p53 can be produced by alternative splicing of p53 in intron 2 and this is regulated by the formation of G-quadruplex structures in p53 intron 3, from which the nucleotides forming these structures overlap with a common polymorphism, rs17878362. rs17878362 alters p53 splicing to decrease fully spliced p53 messenger RNA (mRNA) in vitro following ionizing radiation and this in turn alters Delta 40p53:p53. Hence, the presence of rs17878362 may be important in regulating Delta 40p53:p53 in breast cancer. This study aimed to determine if rs17878362 was associated with altered Delta 40p53 and p53 expression and outcome in breast cancer. We sequenced p53 in breast tumours from 139 patients and compared this with Delta 40p53 and p53 mRNA expression. We found that the ratio of Delta 40p53:p53 was significantly lower in tumours homozygous for the polymorphic A2 allele compared with those who were wild-type (A1/A1). Furthermore, there was a lower proportion of breast cancers carrying the A2 allele from patients who subsequently developed metastasis compared with those that did not. Finally, we show that patients whose tumours carried the polymorphic A2 allele had significantly better disease-free survival. These results show that rs17878362 is associated with a low Delta 40p53:p53 ratio in breast cancer and that this is associated with better outcome.
机译:乳腺癌是最常见的女性癌症,但它的p53突变发生率相对较低,表明其他机制可导致p53失活。我们已经显示p53异构体Delta 40p53在乳腺癌中高度表达,在乳腺癌中它可能导致p53失活。 δ40p53可以通过内含子2中p53的可变剪接产生,这受p53内含子3中G-四链体结构的形成所调节,从中形成这些结构的核苷酸与一个常见的多态性rs17878362重叠。 rs17878362在电离辐射后体外改变p53剪接,以减少完全剪接的p53信使RNA(mRNA),进而改变Delta 40p53:p53。因此,rs17878362的存在可能对调节乳腺癌中的Delta 40p53:p53很重要。这项研究旨在确定rs17878362是否与乳腺癌中Delta 40p53和p53表达及结果的改变有关。我们对139位患者的乳腺肿瘤中的p53进行了测序,并将其与Delta 40p53和p53 mRNA表达进行了比较。我们发现,与野生型(A1 / A1)相比,多态性A2等位基因纯合子的肿瘤中Delta 40p53:p53的比率明显更低。此外,与那些没有转移的患者相比,携带A2等位基因的乳腺癌患者随后发生转移的比例更低。最后,我们表明,肿瘤携带多态性A2等位基因的患者的无病生存期明显更好。这些结果表明,rs17878362与乳腺癌中Delta 40p53:p53比率低有关,并且这与更好的结局有关。

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