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Survival and clinicopathological characteristics of breast cancer patient according to different tumour subtypes as determined by hormone receptor and Her2 immunohistochemistry. A single institution survey spanning 1998 to 2010

机译:根据荷尔蒙受体和Her2免疫组织化学确定的不同肿瘤亚型,乳腺癌患者的生存和临床病理特征。 1998年至2010年的一次机构调查

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As far as recent breast cancer molecular subtype classification is concerned, much work has dealt with clinical outcomes for triple negative and Her2 patients. Less is known about the course of patients in the remaining subtypes. Molecular classification based on immunohistochemistry is widely available and correlates well with genetic microarray assessment, but at a lower cost. The aim of our investigation was to correlate immunohistochemical subtypes of breast cancer with clinical characteristics and patient outcomes. Since 1998, 1167 patients operated for 1191 invasive breast tumours were included in our database. Patients were regularly followed up until March 2010. Disease-free survival, overall mortality, and breast cancer-specific mortality at 5 years were calculated for the cohort.72% of tumours were ER+PR±HER2- group, 13% triple negative (ER-PR-HER2-), 10% ER+PR±HER2+ group, and 5% Her2 (ER-PR-HER2+). Cancer-specific survival was 94.2% for the ER+PR+HER2- subtype, 84.8% for the Her2 subtype, 83.3% for the ER+PR-HER2- subtype, and 78.6% for triple negatives. Distant metastases prevalence ranged from 7% to 22% across subtypes, increasing stepwise from ER+PR+HER2-, ER+PR+HER2+, ER+PR-HER2-, ER+PR-HER2+, ER-PR-HER2+ through triple negative. Small, low-grade tumours with low axillary burden were more likely to belong to the ER+PR±HER2- group. Conversely, larger high-grade tumours with significant axillary burden were more likely to belong to Her2 or triple negative groups. ER+PR±HER2- group patients with negative PR receptors performed more like Her2 or triple negative than like the rest of ER+PR±HER2± groups patients. Molecular classification of breast tumours based only on immunohistochemistry is quite useful on practical clinical grounds, as expected. ER+PR±HER2- group patients with negative PR receptors seem to be at high risk and deserve further consideration.
机译:就最近的乳腺癌分子亚型分类而言,三阴性和Her2患者的临床结局涉及很多工作。对于其余亚型的患者病程知之甚少。基于免疫组织化学的分子分类是广泛可用的,并且与遗传微阵列评估紧密相关,但是成本较低。我们研究的目的是将乳腺癌的免疫组织化学亚型与临床特征和患者预后相关联。自1998年以来,我们的数据库包括1167例1191例浸润性乳腺肿瘤手术患者。对患者进行定期随访,直到2010年3月。计算该队列的5年无病生存率,总体死亡率和乳腺癌特异性死亡率。72%的肿瘤为ER + PR±HER2-组,13%的三阴性( ER-PR-HER2-),10%ER + PR±HER2 +组和5%Her2(ER-PR-HER2 +)。 ER + PR + HER2-亚型的癌症特异性生存率为94.2%,Her2亚型为84.8%,ER + PR-HER2-亚型为83.3%,三阴性患者为78.6%。各亚型的远处转移发生率在7%至22%之间,从ER + PR + HER2-,ER + PR + HER2 +,ER + PR-HER2-,ER + PR-HER2 +,ER-PR-HER2 +逐步增加至三阴性。腋窝负担低的低级恶性肿瘤更可能属于ER + PR±HER2-组。相反,较大的,具有明显腋窝负担的高级肿瘤更可能属于Her2或三阴性组。带有PR受体阴性的ER + PR±HER2-组患者的表现比其他ER + PR±HER2±组患者更像Her2或三阴性。如所期望的,仅基于免疫组织化学的乳腺肿瘤的分子分类在实际临床上是非常有用的。 PR受体阴性的ER + PR±HER2-组患者似乎处于高风险中,值得进一步考虑。

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