家族性和散发性结直肠癌中累积的克隆性基因改变,伴有微卫星序列的广泛不稳定。
Accumulated clonal genetic alterations in familial and sporadic colorectal carcinomas with widespread instability in microsatellite sequences.
作者信息
Fujiwara T, Stolker J M, Watanabe T, Rashid A, Longo P, Eshleman J R, Booker S, Lynch H T, Jass J R, Green J S, Kim H, Jen J, Vogelstein B, Hamilton S R
机构信息
Department of Pathology, The Johns Hopkins University School of Medicine, Baltimore, Maryland, USA.
出版信息
Am J Pathol. 1998 Oct;153(4):1063-78. doi: 10.1016/S0002-9440(10)65651-9.
A subset of hereditary and sporadic colorectal carcinomas is defined by microsatellite instability (MSI), but the spectra of gene mutations have not been characterized extensively. Thirty-nine hereditary nonpolyposis colorectal cancer syndrome carcinomas (HNPCCa) and 57 sporadic right-sided colonic carcinomas (SRSCCa) were evaluated. Of HNPCCa, 95% (37/39) were MSI-positive as contrasted with 31% (18/57) of SRSCCa (P < 0.000001), but instability tended to be more widespread in SRSCCa (P = 0.08). Absence of nuclear hMSH2 mismatch repair gene product by immunohistochemistry was associated with germline hMSH2 mutation (P = 0.0007). The prevalence of K-ras proto-oncogene mutations was similar in HNPCCa and SRSCCa (30% (11/37) and 30% (16/54)), but no HNPCCa from patients with germline hMSH2 mutation had codon 13 mutation (P = 0.02), and two other HNPCCa had multiple K-ras mutations attributable to subclones. 18q allelic deletion and p53 gene product overexpression were inversely related to MSI (P = 0.0004 and P = 0.0001, respectively). Frameshift mutation of the transforming growth factor beta type II receptor gene was frequent in all MSI-positive cancers (85%, 46/54), but mutation of the E2F-4 transcription factor gene was more common in HNPCCa of patients with germline hMSH2 mutation than in those with germline bMLH1 mutation (100% (8/8) versus 40% (2/5), P = 0.04), and mutation of the Bax proapoptotic gene was more frequent in HNPCCa than in MSI-positive SRSCCa (55% (17/31) versus 13% (2/15), P = 0.01). The most common combination of mutations occurred in only 23% (8/35) of evaluable MSI-positive cancers. Our findings suggest that the accumulation of specific genetic alterations in MSI-positive colorectal cancers is markedly heterogeneous, because the occurrence of some mutations (eg, ras, E2F-4, and Bax genes), but not others (eg, transforming growth factor beta type II receptor gene), depends on the underlying basis of the mismatch repair deficiency. This genetic heterogeneity may contribute to the heterogeneous clinical and pathological features of MSI-positive cancers.
微卫星不稳定(MSI)可定义出一部分遗传性和散发性结直肠癌,但基因突变谱尚未得到广泛表征。对39例遗传性非息肉病性结直肠癌综合征癌(HNPCCa)和57例散发性右侧结肠癌(SRSCCa)进行了评估。HNPCCa中95%(37/39)为MSI阳性,而SRSCCa中这一比例为31%(18/57)(P<0.000001),但SRSCCa中的不稳定性往往更广泛(P = 0.08)。免疫组织化学检测显示无核hMSH2错配修复基因产物与种系hMSH2突变相关(P = 0.0007)。HNPCCa和SRSCCa中K-ras原癌基因突变的发生率相似(分别为30%(11/37)和30%(16/54)),但种系hMSH2突变患者的HNPCCa中无密码子13突变(P = 0.02),另外两例HNPCCa有多个归因于亚克隆的K-ras突变。18q等位基因缺失和p53基因产物过表达与MSI呈负相关(分别为P = 0.0004和P = 0.0001)。转化生长因子βⅡ型受体基因的移码突变在所有MSI阳性癌症中很常见(85%,46/54),但E2F-4转录因子基因突变在种系hMSH2突变患者的HNPCCa中比在种系bMLH1突变患者中更常见(100%(8/8)对40%(2/5),P = 0.04),Bax促凋亡基因突变在HNPCCa中比在MSI阳性的SRSCCa中更频繁(55%(17/31)对13%(2/15),P = 0.01)。最常见的突变组合仅出现在23%(8/35)可评估的MSI阳性癌症中。我们的研究结果表明,MSI阳性结直肠癌中特定基因改变的积累明显异质性,因为某些突变(如ras、E2F-4和Bax基因)的发生,但不是其他突变(如转化生长因子βⅡ型受体基因)取决于错配修复缺陷的潜在基础。这种基因异质性可能导致MSI阳性癌症临床和病理特征的异质性。
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