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三阴性乳腺癌肿瘤的基因表达分子亚型:免疫反应的重要性

Gene-expression molecular subtyping of triple-negative breast cancer tumours: importance of immune response.

作者信息

Jézéquel Pascal, Loussouarn Delphine, Guérin-Charbonnel Catherine, Campion Loïc, Vanier Antoine, Gouraud Wilfried, Lasla Hamza, Guette Catherine, Valo Isabelle, Verrièle Véronique, Campone Mario

机构信息

Unité Mixte de Génomique du Cancer, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France.

Unité de Bioinfomique, Institut de Cancérologie de l'Ouest - site René Gauducheau, Bd J. Monod, 44805, Saint Herblain Cedex, France.

出版信息

Breast Cancer Res. 2015 Mar 20;17:43. doi: 10.1186/s13058-015-0550-y.

Abstract

INTRODUCTION

Triple-negative breast cancers need to be refined in order to identify therapeutic subgroups of patients.

METHODS

We conducted an unsupervised analysis of microarray gene-expression profiles of 107 triple-negative breast cancer patients and undertook robust functional annotation of the molecular entities found by means of numerous approaches including immunohistochemistry and gene-expression signatures. A triple-negative external cohort (n=87) was used for validation.

RESULTS

Fuzzy clustering separated triple-negative tumours into three clusters: C1 (22.4%), C2 (44.9%) and C3 (32.7%). C1 patients were older (mean=64.6 years) than C2 (mean=56.8 years; P=0.03) and C3 patients (mean=51.9 years; P=0.0004). Histological grade and Nottingham prognostic index were higher in C2 and C3 than in C1 (P<0.0001 for both comparisons). Significant event-free survival (P=0.03) was found according to cluster membership: patients belonging to C3 had a better outcome than patients in C1 (P=0.01) and C2 (P=0.02). Event-free survival analysis results were confirmed when our cohort was pooled with the external cohort (n=194; P=0.01). Functional annotation showed that 22% of triple-negative patients were not basal-like (C1). C1 was enriched in luminal subtypes and positive androgen receptor (luminal androgen receptor). C2 could be considered as an almost pure basal-like cluster. C3, enriched in basal-like subtypes but to a lesser extent, included 26% of claudin-low subtypes. Dissection of immune response showed that high immune response and low M2-like macrophages were a hallmark of C3, and that these patients had a better event-free survival than C2 patients, characterized by low immune response and high M2-like macrophages: P=0.02 for our cohort, and P=0.03 for pooled cohorts.

CONCLUSIONS

We identified three subtypes of triple-negative patients: luminal androgen receptor (22%), basal-like with low immune response and high M2-like macrophages (45%), and basal-enriched with high immune response and low M2-like macrophages (33%). We noted out that macrophages and other immune effectors offer a variety of therapeutic targets in breast cancer, and particularly in triple-negative basal-like tumours. Furthermore, we showed that CK5 antibody was better suited than CK5/6 antibody to subtype triple-negative patients.

摘要

引言

三阴性乳腺癌需要进一步细化,以确定患者的治疗亚组。

方法

我们对107例三阴性乳腺癌患者的基因芯片基因表达谱进行了无监督分析,并通过包括免疫组织化学和基因表达特征在内的多种方法对所发现的分子实体进行了可靠的功能注释。使用一个三阴性外部队列(n = 87)进行验证。

结果

模糊聚类将三阴性肿瘤分为三个簇:C1(22.4%)、C2(44.9%)和C3(32.7%)。C1组患者的年龄(平均64.6岁)大于C2组(平均56.8岁;P = 0.03)和C3组患者(平均51.9岁;P = 0.0004)。C2和C3组的组织学分级和诺丁汉预后指数高于C1组(两组比较P均<0.0001)。根据聚类成员情况发现了显著的无事件生存期差异(P = 0.03):C3组患者的预后优于C1组(P = 0.01)和C2组(P = 0.02)。当我们的队列与外部队列合并(n = 194;P = 0.01)时,无事件生存期分析结果得到证实。功能注释显示,22%的三阴性患者不是基底样型(C1)。C1组富含腔面亚型和雄激素受体阳性(腔面雄激素受体)。C2组可被视为几乎纯粹的基底样簇。C3组富含基底样亚型,但程度较轻,包括26%的claudin低表达亚型。对免疫反应的剖析表明,高免疫反应和低M2样巨噬细胞是C3组的特征,并且这些患者的无事件生存期优于C2组患者,C2组的特征是低免疫反应和高M2样巨噬细胞:我们的队列中P = 0.02,合并队列中P = 0.03。

结论

我们确定了三阴性患者的三种亚型:腔面雄激素受体型(22%)、免疫反应低和M2样巨噬细胞高的基底样型(45%)以及免疫反应高和M2样巨噬细胞低的富含基底样型(33%)。我们指出,巨噬细胞和其他免疫效应器在乳腺癌,尤其是三阴性基底样肿瘤中提供了多种治疗靶点。此外,我们表明CK5抗体比分型三阴性患者时CK5/6抗体更合适。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/51e9/4389408/27cef804c175/13058_2015_550_Fig1_HTML.jpg

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