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小乳腺癌的病理学与行为学

Pathology and behavior of small breast carcinomas.

作者信息

Meyer J S, Fahrner M, Daniel F C

机构信息

Department of Pathology, St Luke's Hospital, Chesterfield, MO 63017, USA.

出版信息

Semin Diagn Pathol. 1999 Aug;16(3):257-68.

Abstract

Mammographic screening and increased public awareness have changed the clinical spectrum of breast carcinoma with important implications for therapy. Small invasive breast carcinomas T1a,b, defined as 1.0 cm or less in maximum diameter, now comprise 22% of invasive carcinomas in our institution, enabling comparison of 273 T1a,b with 563 T1c (1.1 to 2.0 cm), 447 T2 (2.1 to 5.0 cm), and 40 T3 (>5 cm) carcinomas. Nuclear measurements were made with calibrated ocular grids. Hormone receptors were measured in cytosol or immunohistochemically. S-phase fraction (SPF) was measured prospectively on all carcinomas by counting cells in histologic preparations after vitro labeling with tritiated thymidine or 5-bromo-2'deoxyuridine. T1a (0.2 to 0.5 cm) carcinomas were similar to T1b (0.6 to 1.0 cm) in histologic and biologic features, but T1b carcinomas had higher detection rates of axillary metastasis (0% v 10%). The latter may reflect longer duration of metastases, permitting growth to detectable size. Low-grade carcinoma types (mucinous, tubular, cribriform) became less frequent as T stage increased, with the major decrease occurring at T1b (0.6 to 1.0 cm)/T1c (1.1 to 2.0 cm) boundary. T1a,b carcinomas preponderantly had low-grade histologic and biochemical characteristics and low SPF. SPF increased significantly with increasing tumor size from T1b through T2 but not beyond T2. Increases in proportion of patients with axillary metastases occurred over each T transition. Estrogen and progesterone receptor (ER, PgR) positivity decreased with increasing stage. Larger tumors were significantly associated with younger patient age. While this may reflect ease of diagnosing small carcinomas after the menopause, young age was also associated with predictors of aggressive tumor behavior (high SPF, negative assays for ER, PgR). T1a,b patients with mid or high SPF or axillary metastases were more likely than others to have received cytotoxic adjuvant therapy. Conclusions are: (1) Development of cell lines that have metastatic capability appears to occur near the T1b/T1c interface, but they exist very early in some carcinomas. (2) T1a carcinomas may be managed without axillary dissection. When T1b patients are candidates for adjuvant therapy, we advocate sentinel node biopsy with intensive study for micrometastases. (3) Accurate determination of size is very important in prognosis of small breast carcinomas. (4) Prognostic efficacy of proliferation and other prognostic markers in retrospective studies, but not in our patients who often received adjuvant therapy, suggest that micrometastases from small breast carcinomas are highly responsive to adjuvant chemo/hormonal therapy.

摘要

乳腺钼靶筛查及公众意识的提高改变了乳腺癌的临床谱,对治疗具有重要意义。最大直径为1.0 cm或更小的小浸润性乳腺癌T1a、b,目前在我们机构的浸润性癌中占22%,使得能够将273例T1a、b癌与563例T1c(1.1至2.0 cm)、447例T2(2.1至5.0 cm)和40例T3(>5 cm)癌进行比较。使用校准的目镜网格进行核测量。通过在细胞溶质中测量或免疫组织化学方法检测激素受体。通过用氚标记的胸腺嘧啶核苷或5-溴-2'-脱氧尿苷进行体外标记后,在组织学切片中计数细胞,前瞻性地测量所有癌的S期分数(SPF)。T1a(0.2至0.5 cm)癌在组织学和生物学特征上与T1b(0.6至1.0 cm)相似,但T1b癌腋窝转移的检出率更高(0%对10%)。后者可能反映转移持续时间更长,使得生长至可检测大小。低级别癌类型(黏液性、管状、筛状)随着T分期增加而变得不那么常见,主要减少发生在T1b(0.6至1.0 cm)/T1c(1.1至2.0 cm)边界。T1a、b癌主要具有低级别组织学和生化特征以及低SPF。从T1b到T2,SPF随着肿瘤大小增加而显著增加,但超过T2后则不再增加。在每个T分期转变时,腋窝转移患者的比例都有所增加。雌激素和孕激素受体(ER、PgR)阳性率随着分期增加而降低。较大的肿瘤与患者年龄较轻显著相关。虽然这可能反映了绝经后小癌易于诊断,但年轻也与侵袭性肿瘤行为的预测指标(高SPF、ER和PgR检测阴性)相关。SPF为中等或高值或有腋窝转移的T1a、b患者比其他患者更有可能接受细胞毒性辅助治疗。结论为:(1)具有转移能力的细胞系的发展似乎发生在T1b/T1c界面附近,但在一些癌中很早就存在。(2)T1a癌可能无需腋窝清扫。当T1b患者是辅助治疗的候选者时,我们主张进行前哨淋巴结活检并对微转移进行深入研究。(3)准确确定大小在小乳腺癌的预后中非常重要。(4)增殖及其他预后标志物在回顾性研究中的预后效力,但在我们经常接受辅助治疗的患者中并非如此,这表明小乳腺癌的微转移对辅助化疗/激素治疗高度敏感。

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