人平衡核苷转运蛋白-1 在鼠(10D7G2)和兔(SP120)抗体之间表达的一致性及其与胰腺癌辅助化疗临床结局的关系:来自 JASPAC 01 试验的协作研究。
Concordance of human equilibrative nucleoside transporter-1 expressions between murine (10D7G2) and rabbit (SP120) antibodies and association with clinical outcomes of adjuvant chemotherapy for pancreatic cancer: A collaborative study from the JASPAC 01 trial.
机构信息
Division of Hepato-Biliary-Pancreatic Surgery, Shizuoka Cancer Center Hospital, Nagaizumi, Japan.
Division of Gastrointestinal Medical Oncology, National Cancer Center Hospital, Tokyo, Japan.
出版信息
Cancer Rep (Hoboken). 2022 May;5(5):e1507. doi: 10.1002/cnr2.1507. Epub 2021 Jul 29.
BACKGROUND
Expression of human equilibrative nucleoside transporter-1 (hENT1) is reported to predict survival of gemcitabine (GEM)-treated patients. However, predictive values of immunohistochemical hENT1 expression may differ according to the antibodies, 10D7G2 and SP120.
AIM
We aimed to investigate the concordance of immunohistochemical hENT1 expression between the two antibodies and prognosis.
METHODS
The subjects of this study were totally 332 whose formalin-fixed paraffin-embedded specimens and/or unstained sections were obtained. The individual H-scores and four classifications according to the staining intensity were applied for the evaluation of hENT1 expression by 10D7G2 and SP120, respectively.
RESULTS
The highest concordance rate (79.8%) was obtained when the cut-off between high and low hENT1 expression using SP120 was set between moderate and strong. There were no correlations of hENT1 mRNA level with H-score (p = .258). Although the hENT1 mRNA level was significantly different among four classifications using SP120 (p = .011), there was no linear relationship among them. Multivariate analyses showed that adjuvant GEM was a significant predictor of the patients with low hENT1 expression using either 10D7G2 (Hazard ratio [HR] 2.39, p = .001) or SP120 (HR 1.84, p < .001). In contrast, agent for adjuvant chemotherapy was not significant predictor for the patients with high hENT1 expression regardless of the kind of antibody.
CONCLUSION
The present study suggests that the two antibodies for evaluating hENT1 expression are equivalent depending on the cut-off point and suggests that S-1 is the first choice of adjuvant chemotherapy for pancreatic cancer with low hENT1 expression, whereas either S-1 or GEM can be introduced for the pancreatic cancer with high hENT1 expression, no matter which antibody is used.
背景
已报道人嘧啶核苷转运蛋白-1(hENT1)的表达可预测吉西他滨(GEM)治疗患者的生存情况。然而,免疫组织化学 hENT1 表达的预测价值可能因抗体 10D7G2 和 SP120 而异。
目的
我们旨在研究两种抗体的免疫组织化学 hENT1 表达的一致性及其与预后的关系。
方法
本研究共纳入 332 例福尔马林固定石蜡包埋标本和/或未经染色的切片的患者。采用 10D7G2 和 SP120 分别对 hENT1 表达进行评估,应用 H 评分和染色强度的四个分类。
结果
当使用 SP120 确定高和低 hENT1 表达的截止值介于中度和强之间时,获得了最高的一致性率(79.8%)。hENT1 mRNA 水平与 H 评分之间无相关性(p =.258)。尽管使用 SP120 进行的四个分类中 hENT1 mRNA 水平存在显著差异(p =.011),但它们之间没有线性关系。多变量分析显示,辅助 GEM 是低 hENT1 表达患者的显著预测因素,无论使用 10D7G2(危险比 [HR] 2.39,p =.001)还是 SP120(HR 1.84,p <.001)。相比之下,辅助化疗药物不是高 hENT1 表达患者的显著预测因素,而与使用的抗体无关。
结论
本研究表明,两种评估 hENT1 表达的抗体取决于截止点,当 hENT1 表达低时,S-1 是胰腺癌辅助化疗的首选药物,而当 hENT1 表达高时,无论使用哪种抗体,S-1 或 GEM 均可用于胰腺癌。
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