Mansour E G, Ravdin P M, Dressler L
Cancer Care Center, Case Western Reserve University, Cleveland, Ohio.
Cancer. 1994 Jul 1;74(1 Suppl):381-400. doi: 10.1002/cncr.2820741326.
Several investigators, the SEER data, and the ECOG/Intergroup study have shown that patients with small tumors (< 0.5 cm) have a recurrence rate of less than 2%, compared to 20-25% for large tumors (> or = 5 cm). Nuclear grade and tumor differentiation are established indicators; however, the interobserver lack of concordance has thwarted their use in clinical trials. The presence of peritumoral lymphatic and blood vessel invasion (PLBI) is associated with a relative risk of recurrence of 4.7. The predictive value of the presence of hormone receptors in tumors is associated with a favorable disease free and overall survival difference of 8-10%; however, this advantage is being eroded by the early appearance of other factors, such as the epidermal growth factor receptor (EGFR), proliferative capacity (S-phase), nuclear grade, and HER-2/neu oncogene. Concordance among the different methods of hormone-receptor assay (immunocytochemical, sucrose gradient, and dextran-coated charcoal) is essential to refine the true value of these factors. DNA flow cytometry measurements of ploidy (DNA content) and S-phase fraction are the most characterized of the prognostic factors. There are conflicting reports regarding the clinical significance of ploidy status, while measurements of S-phase fraction clearly indicate a robust association with disease free and overall survival. Our data continue to show that S-phase, but not ploidy, can predict time to recurrence significantly in untreated patients, even when data are stratified for tumor size. HER-2/neu oncogene is expressed in about 50% of ductal carcinoma in situ and 14% of invasive ductal carcinoma. The presence of this oncogene at high copy number may be a useful independent marker of poor prognosis and may be associated with drug resistance and correlated with tumor recurrence and shorter survival. EGFR could be measured in most breast tumors, and the level of its expression has inversely correlated with estrogen receptor protein expression. The value of EGFR as a predictor of prognosis remains controversial and is still being investigated. Cathepsin-D provides a provocative biologic rationale but is hindered by different and incongruent methods of analysis. The majority of large studies with more than 3-years' follow-up suggests that high cathepsin-D levels may be predictive of greater recurrence and lower survival. Angiogenesis has been implicated as a critical component of the metastatic process. Early studies show that tumor angiogenesis is an independent and highly significant prognostic indicator, and its presence may suggest the selection of "anti-angiogenic therapy."(ABSTRACT TRUNCATED AT 400 WORDS)
几位研究者、监测、流行病学与最终结果(SEER)数据以及东部肿瘤协作组(ECOG)/国际协作组研究均表明,肿瘤较小(<0.5厘米)的患者复发率低于2%,而大肿瘤(≥5厘米)患者的复发率为20%-25%。核分级和肿瘤分化是既定指标;然而,观察者间缺乏一致性阻碍了它们在临床试验中的应用。肿瘤周围淋巴管和血管侵犯(PLBI)的存在与复发相对风险4.7相关。肿瘤中激素受体的存在对无病生存期和总生存期有有利影响,差异为8%-10%;然而,其他因素如表皮生长因子受体(EGFR)、增殖能力(S期)、核分级和HER-2/neu癌基因的早期出现正在削弱这一优势。不同激素受体检测方法(免疫细胞化学、蔗糖梯度法和葡聚糖包被活性炭法)之间的一致性对于明确这些因素的真实价值至关重要。DNA倍体(DNA含量)和S期分数的流式细胞术测量是最具特征的预后因素。关于倍体状态的临床意义存在相互矛盾的报道,而S期分数测量清楚地表明与无病生存期和总生存期有密切关联。我们的数据继续表明,即使对肿瘤大小进行分层,S期而非倍体能够显著预测未治疗患者的复发时间。HER-2/neu癌基因在约50%的原位导管癌和14%的浸润性导管癌中表达。该癌基因高拷贝数的存在可能是预后不良的一个有用的独立标志物,可能与耐药性相关,并与肿瘤复发和较短生存期相关。大多数乳腺肿瘤都可检测到EGFR,其表达水平与雌激素受体蛋白表达呈负相关。EGFR作为预后预测指标的价值仍存在争议,仍在研究中。组织蛋白酶-D提供了一个引人关注的生物学原理,但受到不同且不一致的分析方法的阻碍。大多数随访超过3年的大型研究表明,高组织蛋白酶-D水平可能预示更高的复发率和更低的生存率。血管生成被认为是转移过程的一个关键组成部分。早期研究表明,肿瘤血管生成是一个独立且高度显著的预后指标,其存在可能提示选择“抗血管生成治疗”。(摘要截选至400字)
