Ekholm Maria, Grabau Dorthe, Bendahl Pär-Ola, Bergh Jonas, Elmberger Göran, Olsson Hans, Russo Leila, Viale Giuseppe, Fernö Mårten
Department of Clinical Sciences Lund, Division of Oncology and Pathology, Lund University , Lund , Sweden.
Acta Oncol. 2015 Jul;54(7):1040-8. doi: 10.3109/0284186X.2015.1037012. Epub 2015 May 11.
Biomarkers are crucial for decisions regarding adjuvant therapy in primary breast cancer, and their correct assessment is therefore of the utmost importance.
To investigate the concordance between Swedish pathology departments and a reference laboratory, for routine analysis of oestrogen receptor (ER), progesterone receptor (PR), Ki67, and human epidermal growth factor receptor 2 (HER2), alone, and in combination (St Gallen subtypes).
This survey included 27 of the 28 pathology laboratories in Sweden, covering 98% of cases of primary breast cancer surgery in Sweden. Paraffin-embedded tumour blocks (n = 270) were collected and sent to the central reference laboratory, together with the originally stained slides, for re-analysis. The primary evaluations were previously performed according to national Swedish guidelines, without any knowledge of the subsequent central assessment.
The agreement for ER, PR, and Ki67 was 99% [kappa value (κ) = 0.95], 95% (κ = 0.85), and 85% (κ = 0.70), respectively. The agreement for HER2 (0/1 + vs. 2+/3+) was 85% (κ = 0.64), but when equivocal tumours were further analysed with in situ hybridisation, only one discrepancy was observed. Discrepancies between results for ER and PR seem to be explained by analytical differences, whereas the interpretation of staining seems to be more critical for Ki67 and HER2 immunohistochemistry. The agreement between the results from the Swedish laboratories and the reference laboratory, based on the St Gallen subtypes, was 88% (κ = 0.81).
When applying national guidelines, highly reproducible results were obtained in routine assessment of breast cancer biomarkers, and the results of this study confirm the clinical utility of these markers for decisions regarding the treatment of primary breast cancer.
生物标志物对于原发性乳腺癌辅助治疗的决策至关重要,因此其正确评估极为重要。
调查瑞典各病理科与一家参考实验室之间,在单独及联合(圣加仑亚型)对雌激素受体(ER)、孕激素受体(PR)、Ki67和人表皮生长因子受体2(HER2)进行常规分析时的一致性。
本调查涵盖了瑞典28家病理实验室中的27家,覆盖瑞典98%的原发性乳腺癌手术病例。收集石蜡包埋的肿瘤组织块(n = 270)并连同原始染色玻片一起送至中央参考实验室进行重新分析。最初的评估是根据瑞典国家指南进行的,且对后续的中央评估一无所知。
ER、PR和Ki67的一致性分别为99%[kappa值(κ)= 0.95]、95%(κ = 0.85)和85%(κ = 0.70)。HER2(0/1 + 与2 + /3 +)的一致性为85%(κ = 0.64),但当对可疑肿瘤进一步进行原位杂交分析时,仅观察到一处差异。ER和PR结果之间的差异似乎可以用分析差异来解释,而对于Ki67和HER2免疫组化,染色的解读似乎更为关键。基于圣加仑亚型,瑞典各实验室与参考实验室结果之间的一致性为88%(κ = 0.81)。
在应用国家指南时,乳腺癌生物标志物的常规评估获得了高度可重复的结果,本研究结果证实了这些标志物在原发性乳腺癌治疗决策中的临床实用性。
