通过BRAF V600E突变分层的微卫星稳定型结直肠癌表现出不同的染色体不稳定模式。
Microsatellite stable colorectal cancers stratified by the BRAF V600E mutation show distinct patterns of chromosomal instability.
作者信息
Bond Catherine E, Nancarrow Derek J, Wockner Leesa F, Wallace Leanne, Montgomery Grant W, Leggett Barbara A, Whitehall Vicki L J
机构信息
Conjoint Gastroenterology Laboratory, QIMR Berghofer Medical Research Institute, Brisbane, Queensland, Australia; School of Medicine, University of Queensland, Brisbane, Queensland, Australia.
Cancer Control Group, QIMR Berghofer Medical Research Institute, Brisbane, Queensland, Australia; Oncogenomics Group, QIMR Berghofer Medical Research Institute, Brisbane, Queensland, Australia.
出版信息
PLoS One. 2014 Mar 20;9(3):e91739. doi: 10.1371/journal.pone.0091739. eCollection 2014.
The BRAF (V600E) mutation in colorectal cancers that are microsatellite stable (MSS) confers a poor patient prognosis, whereas BRAF mutant microsatellite-unstable (MSI) colorectal cancers have an excellent prognosis. BRAF wild type cancers are typically MSS and display chromosomal instability (CIN). CIN has not been extensively studied on a genome-wide basis in relation to BRAF mutational status in colorectal cancer. BRAF mutant/MSS (BRAFmut/MSS) cancers (n = 33) and BRAF mutant/MSI (BRAFmut/MSI) cancers (n = 30) were compared for presence of copy number aberrations (CNAs) indicative of CIN, with BRAF wild type/MSS (BRAFwt/MSS) cancers (n = 18) using Illumina CytoSNP-12 arrays. BRAFmut/MSS and BRAFwt/MSS cancers showed comparable numbers of CNAs/cancer at 32.8 and 29.8 respectively. However, there were differences in patterns of CNA length between MSS cohorts, with BRAFmut/MSS cancers having significantly greater proportions of focal CNAs compared to BRAFwt/MSS cancers (p<0.0001); whereas whole chromosomal arm CNAs were more common in BRAFwt/MSS cancers (p<0.0001). This related to a reduced average CNA length in BRAFmut/MSS compared to BRAFwt/MSS cancers (20.7 Mb vs 33.4 Mb;p<0.0001); and a smaller average percent of CIN affected genomes in BRAFmut/MSS compared to BRAFwt/MSS cancers (23.9% vs 34.9% respectively). BRAFmut/MSI cancers were confirmed to have low CNA rates (5.4/cancer) and minimal CIN-affected genomes (average of 4.5%) compared to MSS cohorts (p<0.0001). BRAFmut/MSS cancers had more frequent deletion CNAs compared to BRAFwt/MSS cancers on 6p and 17q at loci not typically correlated with colorectal cancer, and greater amplification CNAs on 8q and 18q compared to BRAFwt/MSS cancers. These results indicate that comparable rates of CIN occur between MSS subgroups, however significant differences in their patterns of instability exist, with BRAFmut/MSS cancers showing a 'focal pattern' and BRAFwt/MSS cancers having a 'whole arm pattern' of CIN. This and the genomic loci more frequently affected in BRAFmut/MSS cancers provides further evidence of the biological distinctions of this important cancer subgroup.
在微卫星稳定(MSS)的结直肠癌中,BRAF(V600E)突变预示患者预后不良,而BRAF突变的微卫星不稳定(MSI)结直肠癌预后良好。BRAF野生型癌症通常为MSS且表现出染色体不稳定(CIN)。关于结直肠癌中BRAF突变状态与CIN的关系,尚未在全基因组范围内进行广泛研究。使用Illumina CytoSNP - 12芯片,比较了BRAF突变/MSS(BRAFmut/MSS)癌症(n = 33)和BRAF突变/MSI(BRAFmut/MSI)癌症(n = 30)中指示CIN的拷贝数变异(CNA)的存在情况,并与BRAF野生型/MSS(BRAFwt/MSS)癌症(n = 18)进行比较。BRAFmut/MSS和BRAFwt/MSS癌症的每个癌症CNA数量分别为32.8和29.8,二者相当。然而,MSS队列之间CNA长度模式存在差异,与BRAFwt/MSS癌症相比,BRAFmut/MSS癌症的局灶性CNA比例显著更高(p<0.0001);而全染色体臂CNA在BRAFwt/MSS癌症中更常见(p<0.0001)。这与BRAFmut/MSS癌症相比BRAFwt/MSS癌症的平均CNA长度缩短有关(20.7 Mb对33.4 Mb;p<0.0001);并且与BRAFwt/MSS癌症相比,BRAFmut/MSS癌症中受CIN影响的基因组平均百分比更小(分别为23.9%对34.9%)。与MSS队列相比,BRAFmut/MSI癌症被证实具有低CNA率(每个癌症5.4个)和最小的受CIN影响的基因组(平均4.5%)(p<0.0001)。与BRAFwt/MSS癌症相比,BRAFmut/MSS癌症在6p和17q上与结直肠癌通常不相关的位点有更频繁的缺失CNA,在8q和18q上有比BRAFwt/MSS癌症更大的扩增CNA。这些结果表明,MSS亚组之间CIN发生率相当,但它们的不稳定模式存在显著差异,BRAFmut/MSS癌症表现出“局灶模式”,BRAFwt/MSS癌症具有CIN的“全臂模式”。这以及BRAFmut/MSS癌症中更频繁受影响的基因组位点为这个重要癌症亚组的生物学差异提供了进一步证据。
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