Basal-like型乳腺癌临床特征与生存分析

目的分析Basal-like型乳腺癌所占比例、临床特征以及生存情况,为Basal-like型乳腺癌临床诊治提供参考依据。方法回顾性分析我院经手术治疗、资料完整、经病理确诊的女性乳腺癌患者171例。Basal-like型乳腺癌的判定采用Nielsen标准。比较Basal-like型乳腺癌与非Basal-like型乳腺癌的临床病理特征、复发转移及生存情况。结果 Basal-like型乳腺癌26例,占15.3%。Basal-like型乳腺癌具有组织学分级高(Basal-like型与非Basal-like型乳腺癌组织学分级Ⅲ级的比例分别为:69.23%和30.34%,P<0.001),淋巴结转移阳性率低(34.62%和58.62%,P=0.023),淋巴结转移率低(41.38%和65.38%,P=0.038)的特点。与非Basal-like型乳腺癌相比,Basal-like型乳腺癌肺转移发生率较高(15.38%和3.45%,P=0.012)。Basal-like型乳腺癌和非Basal-like型乳腺癌的5年生存率分别为70.3%和87.9%(P=0.042),5年无病生存率分别为59.5%和80.3%(P=0.013)。结论本组患者并没有发现回、汉族患者Basal-like型乳腺癌的发病率差别。本组Basal-like型乳腺癌患者具有组织学分级高、淋巴结转移阳性率低、淋巴结转移率低、易于发生肺转移和预后较差的特点。

Cancer stem cells and early stage basal-like breast cancer

Ductal carcinoma in situ （DCIS） is a category of early stage, non-invasive breast tumor defined by the intraductal proliferation of malignant breast epithelial cells. DCIS is a heterogeneous disease composed of multiple molecular subtypes including luminal, HER2 and basal-like types, which are characterized by immuno-histochemical analyses and gene expression profiling. Following surgical and radiation therapies, patients with luminal-type, estrogen receptor-positive DCIS breast tumors can benefit from adjuvant endocrine-based treatment. However, there are no available targeted therapies for patients with basal-like DCIS （BL-DCIS） tumors due to their frequent lack of endocrine receptors and HER2 amplification, rendering them potentially susceptible to recurrence. Moreover, multiple lines of evidence suggest that DCIS is a non-obligate precursor of invasive breast carcinoma. This raises the possibility that targeting precursor BL-DCIS is a promising strategy to prevent BL-DCIS patients from the development of invasive basal-like breast cancer. An accumulating body of evidence demonstrates the existence of cancer stem-like cells （CSCs） in BL-DCIS, which potentially determine the features of BL-DCIS and their ability to progress into invasive cancer. This review encompasses the current knowledge in regard to the characteristics of BL-DCIS, identifcation of CSCs, and their biological properties in BL-DCIS. We summarize recently discovered relevant molecular signaling alterations that promote the generation of CSCs in BL-DCIS and the progression of BL-DCIS to invasive breast cancer, as well as the infuence of the tissue microenvironment on CSCs and the invasive transition. Finally, we discuss the translational implic-ations of these fndings for the prognosis and prevention of BL-DCIS relapse and progression.

CD44^+/CD24^-表型与BRCA1及basal-like乳腺癌的相关性

目的探讨CD44+/CD24-表型与BRCA1及basal-like乳腺癌的相关性。方法收集经病理诊断为乳腺癌患者的手术切除石蜡标本共217例,根据免疫学标志物把217例乳腺癌划分为5类分子亚型:basal-like型、luminalA型、luminal B型、Her2过表达型和normalbreast-like型。应用免疫组织化学检测CK5/6、BRCA1和CD44/CD24双染的情况,分析CD44+/CD24-表型与basal-like乳腺癌及BRCA1相关性乳腺癌的关系。结果 217例乳腺癌标本例中,luminalA型130例、luminal B型15例、HER2过表达型21例、basal-like型29例、Normalbreast-like型22例。BRCA1相关性乳腺癌57例。basal-like乳腺癌组织中BRCA1缺失率86%(25/29),明显高于乳腺癌其他分子亚型(P<0.001)。basal-like乳腺癌组织中含CD44+/CD24-肿瘤细胞者20例(20/29,69%),明显高于乳腺癌其他分子亚型(P=0.003);BRCA1相关性乳腺癌中含CD44+/CD24-肿瘤细胞者53例(53/57,93%)。结论 BRCA1基因突变与basal-like乳腺癌有关;CD44+/CD24-干细胞表型主要存在于basal-like乳腺癌及BRCA1相关性乳腺癌中。

Basal-like乳腺癌与干细胞的研究进展

0引言 目前基于基因谱将乳腺癌划分为5个分子亚型[1-2],其中Basa1-1ike乳腺癌具有独特的基因表型和形态特点,其恶性程度高,侵袭性强,临床预后差,引起了国内外肿瘤学家的高度关注。肿瘤干细胞是最近几年来肿瘤发生机制研究领域的热点,笔者就Basal-1ike乳腺癌及其与乳腺癌干细胞相关性作一综述。

探讨可手术的Luminal B型和Basal-like型乳腺癌亚型临床特征及预后

目的 探讨分析可手术的Luminal B型和Basal-like型乳腺癌患者临床病理特征与预后情况。方法 选取2018年02月-2019年02月收治可手术的Luminal B型和Basal-like型乳腺癌亚型患者各30名,依次分为Luminal B型组与Basal-like型组。分析患者临床病理特征与手术后1年预后情况。结果 Luminal B型组与Basal-like型组患者病理分型、淋巴结转移数、肿块直径以及侵犯皮肤与胸壁情况对比无明显差异(P>0.05);Luminal B型组组织学分级相比Basal-like型明显更低(P<0.05);两组患者的放射治疗率、内分泌治疗和全身化疗率均基本一致(P>0.05);Luminal B型组患者术后1年生存率相比Basal-like型组患者明显更高(P<0.05)。结论 Luminal B型乳腺癌患者组织学分级相比Basal-like型更低,且Luminal B型患者预后相比Basal-like型患者更好。

Luminal型与Basal-like型乳腺癌差异miRNAs的表达与预后分析

目的分析Luminal型和Basal-like型乳腺癌之间差异表达的microRNAs(miRNAs),探讨其表达水平与Luminal型和Basal-like型乳腺癌预后的关系。方法从基因表达综合数据库(GEO)中下载包含Luminal和Basal-like乳腺癌患者相关的miRNAs微阵列数据集GSE81000与GSE40267,利用GEO2R在线分析工具筛选Luminal和Basal-like乳腺癌之间差异表达的miRNAs。通过mirDIP数据库预测其靶基因,并采用实时荧光定量PCR(quantitative real-time PCR,qRT-PCR)在人乳腺癌细胞MCF-7和MDA-MB-468中验证miRNAs的差异表达。利用METABRIC数据库,采用KaplanMeier Plotter在线工具分析miR-199a-5p和miR-199b-5p表达水平与Luminal型和Basal-like型乳腺癌预后的关系。结果筛选出了35种在Luminal型和Basal-like型乳腺癌中差异表达的miRNAs。相较于Luminal型,18种miRNAs在Basal-like型中表达下调,17种表达上调。靶基因预测结果显示,35种差异表达miRNAs的潜在靶基因共4180个,其中最相关的靶基因有19个,对应的差异miRNAs为miR-199a-5p、miR-199b-5p。相较于Luminal型乳腺癌,miR-199a-5p和miR-199b-5p在Basal-like型乳腺癌中表达下调。qRT-PCR检测结果表明,miR-199a-5p和miR-199b-5p在MCF-7(Luminal型)和MDA-MB-468(Basal-like型)细胞中的表达水平与GEO2R分析结果趋势一致。生存分析结果表明,miR-199a-5p与miR-199b-5p低表达与Luminal A型乳腺癌患者的总生存率降低显著相关。结论共筛选出35个在Luminal型和Basal-like型乳腺癌中差异表达的miRNAs。其中,miR-199a-5p、miR-199b-5p与乳腺癌的预后相关,有望成为治疗的新靶点。

Basal-like型乳腺癌的研究进展

乳腺癌是女性最常见的恶性肿瘤。目前人们往往根据肿瘤病理组织学情况判断乳腺癌的预后。近年来,人们发现生物学指标不仅有助于判断肿瘤的预后,还能预测肿瘤对治疗的反应。根据浸润性乳腺癌基因表达情况,可以将乳腺癌分为4个亚型,即luminalA,luminalB,HER2过表达和basal-like型。各型有不同的临床预后,Basal-like型的临床预后较差。本文将简单介绍乳腺癌分子亚型的分布情况,概述basal-like型乳腺癌的特性以及其预后情况的近期研究进展。

Methyltransferase 3A-mediated promoter methylation represses retinoic acid receptor responder 3 expression in basal-like breast cancer

Retinoic acid receptor responder 3(RARRES3)has been characterized as a tumor suppressor in multiple types of cancer.This study aimed to examine the expression profile of RARRES3 across the PAM50 subtypes of breast cancer.The DNA methylation status of RARRES3 was checked in the basal-like subtype,and the underlying mechanisms of its dysregulation were explored.RNA-sequencing(seq)and methylation data from The Cancer Genome Atlas were used for in-silico analysis.Basal-like representative SUM149 and MDA-MB-468 cell lines were used for in vitro and in vivo studies.Compared to tumor-adjacent normal tissues,only the basal-like tumor tissues had significantly downregulated RARRES3 expression.The methylation level of four CpG sites in the promoter region showed a strong negative correlation with RARRES3 expression.The gene coding for DNA methyltransferase 3A(DNMT3A)had consistent positive correlations with the methylation of the CpG sites.Chromatin Immunoprecipitation-quantitative polymerase chain-reaction and bisulfite sequencing PCR showed that DNMT3A could bind to the promoter region of RARRES3 and promote methylation of the CpG sites within the region.DNMT3A knockdown significantly restored RARRES3 expression at the mRNA and protein level in the two cell lines.CCK-8,colony formation,and flow cytometric analysis showed that RARRES3 overexpression attenuated the growth-promoting effects of DNMT3A overexpression and also weakened the DNMT3A overexpression-induced activation of ERK1/2 and PI3K/AKT signaling.In summary,this study revealed that DNMT3A enhances promoter methylation of the RARRES3 gene and suppresses its transcription in basal-like breast cancer.The DNMT3A-RARRES3 signaling pathway might be a potential target for the treatment of this tumor subtype.

Cytotoxicity Study of Gold Nanoparticles on the Basal-Like Triple-Negative HCC-1937 Breast Cancer Cell Line

The Triple Negative “Basal-like” breast cancer (TNBL) tumours have a high proliferative capacity and develop a resistance phenotype associated with metastases. However, the management of TNBL carcinomas is still not standardized. Among the promising trails, gold nanoparticles could be a relevant tool for the development of a targeted treatment for this breast cancer subtype in monotherapy, associated and/or conjugated with other drugs. In this work, we report the cytotoxicity impact of gold nanoparticles wrapped in Poly-Ethylene Glycol (PEG) on the TNBL HCC-1937 breast cancer cell line. PEG-coated gold nanoparticles (PEG-Au NPs) were synthesized by a two-step method using a reduction process followed by a post-functionalization called PEGylation. PEG-Au NPs were characterized using transmission electron microscopy and X-ray diffraction. The gold content of the samples was determined using atomic absorption spectrometer. The cytotoxicity tests were performed using Sulforhodamine B survival test and resazurin viability test. PEG-Au NPs impact analysis on HCC1937 TNBL cell line showed a clear toxic action of type dose dependent and at long term. These PEGylated gold nanoparticles present a promising tool for the development of tumor-specific radiosensitizing vectors, with or without the association of other treatment strategies.

Differential Expression of Glu-Tubulin in Basal-Like Phenotype Carcinoma of the Mammary Gland

High levels of tubulin expression have been described in a variety of human malignant tumors, and glu-tubulin, in which the C-terminal tyrosine of α-tubulin is removed by tubulin carboxypeptidase. Over-expression has been reported in the malignant tumors of the mammary gland and correlated with poor prognosis immunohistochemically. Furthermore, Nielsen et al. proposed that the use of a panel of four markers (ER, HER 2, CK 5/6, and EGFR) could accurately identify basal-like phenotype carcinoma (BPC) with widely available standard pathologic tools. In our study, major prognostic factors such as patient age, tumor size, histological grade, axillary lymph node metastasis, vessel invasion, and local recurrence in BPC were not significantly different from non BP carcinoma (NBPC). However, the BPC group showed a higher ratio of distant metastasis than that of the NBPC group. In triple-negative carcinoma (TNC) cases, staining for glu-tubulin was observed in 46 cases (63.8%), which consisted of 42 of the 58 BPC patients (72.4%) and 4 of the 14 NBPC patients (28.6%). A significant association was found between the expression of glu-tubulin and BPC, but not NBPC. It seems that our findings also agree with the observation that BPC exhibits aggressive biological behavior and increases the content of glu-tubulin, which plays a greater role in migration and invasion.

C1orf106, an innate immunity activator, is amplified in breast cancer and is required for basal-like/luminal progenitor fate decision

Basal-like breast cancer with a luminal progenitor gene expression profile is an aggressive subtype of breast cancer with a poorer prognosis compared with other subtypes.However,genes that specifically promote basal-like breast cancer development remain largely unknown.Here,we report that a novel gene C1orf106 plays an important role in maintaining the feature of basal-like/luminal progenitors.C1orf106 is frequently amplified and overexpressed in basal-like breast cancer and is associated with a poor outcome in patients.In human TCGA database,C1orf106 expression was correlated with upregulation of ELF5 and downregulation of GATA3,two transcription factors that regulate mammary gland stem cell fate.Enhanced expression of C1orf106 promotes tumor progression and expression of basal-like/luminal progenitor marker ELF5;depletion of C1orf106 suppresses tumorigenesis and expression of basal-like/luminal progenitor marker GATA3.These findings suggest that C1orf106 maintains the basal-like/luminal progenitor character through balancing the expression of ELF5 and GATA3.Taken together,we demonstrated that C1orf106 is an important regulator for basal-like/luminal progenitors and targeting C1orf106 is of therapeutic value for breast cancer.

重构长非编码RNA介导的乳腺癌basal-like亚型相关药物互作网络

目的基于长非编码RNA(lncRNA)及mRNA双重表达谱,构建乳腺癌basal-like亚型相关的lncRNA-mRNA-drug互作网络。方法以乳腺癌basal-like亚型为疾病模型,基于新一代测序技术构建乳腺癌长非编码RNA与编码RNA转录组分子图谱,采用关联有罪的原理识别了basal-like亚型中显著差异改变的lncRNA-mRNA共表达对,进而结合药物及其靶关系构建lncRNA-mRNA-drug互作网络。结果基于RNA-seq数据获得的双重表达谱共识别了1 122个差异表达的lncRNA和6 370个差异表达的mRNA,利用DAVID识别了显著富集的29个生物学功能及8条KEGG通路,最终结合药物及其靶关系构建了非编码RNA介导的乳腺癌亚型相关的药物互作网络。结论基于TCGA的lncRNA及mRNA双重表达谱,从计算系统生物学角度提出了识别乳腺癌basal-like亚型相关风险lncRNA新策略,构建了非编码RNA介导的乳腺癌basal-like亚型相关药物互作网络,为解析乳腺癌basal-like亚型分子机制及药物重定位提供了重要的科学依据。

AKR1B1 promotes basal-like breast cancer progression by activating the EMT program

Subject Code:H16With the support by the National Natural Science Foundation of China,a study by the research groups led by Prof.Dong Chenfang(董辰方)from Zhejiang University School of Medicine demonstrates that AKR1B1promotes basal-like breast cancer progression by apositive feedback loop that activates the

整合生物信息学分析基底型乳腺癌的核心基因

目的整合生物信息学挖掘并分析与基底型乳腺癌(basal-like breast cancer,BLBC)的预后相关的核心基因。方法首先,从GEO数据库中遴选与乳腺癌分子分型相关的数据集,数据处理后利用WGCNA筛选与BLBC相关的模块。然后,借助蛋白-蛋白互作(protein-protein interaction,PPI)网络和cytohubba筛选出模块中差异最大的前10%基因作为候选基因,对候选基因进行生存分析和表达分析得到核心基因。最后,利用TIMER、TISIDB等生信工具探索核心基因表达和肿瘤免疫浸润、趋化因子及免疫调节剂的相关性并构建核心基因转录调控网络。结果利用WGCNA筛选出与BLBC相关的黑色模块中共891个基因,从差异性最大的80个候选基因中分析获得ESPL1和CCNB2两个核心基因。结果显示,两个核心基因与BLBC免疫细胞浸润有关,主要包括Th2细胞、CD8+T细胞、内皮细胞和肿瘤相关成纤维细胞。而且,核心基因表达水平与趋化因子、免疫刺激因子、免疫抑制因子及MHC分子相关。核心基因上游转录调控网络表明22种转录因子同时调控两个核心基因。结论ESPL1和CCNB2是BLBC的预后标志物且与肿瘤免疫相关。

CD44^+/CD24^-表型在乳腺癌分子亚型中的表达和分布

目的:研究CD44+/CD24-表型在乳腺癌中的表达并探讨其与乳腺癌各分子亚型的相关性.方法:根据免疫学标志物(ER,PR,HER2,CK5/6,P53)把217例乳腺癌划分为5类分子亚型:basal-like型、LuminalA型、LuminalB型、Her2过表达型和Normalbreast-like型.应用双重免疫组织化学检测CD44/CD24双染的情况,分析CD44+/CD24-表型与乳腺癌5个分子亚型的相关性.结果:217例乳腺癌病例中,luminalA型130例、luminalB型15例、HER2过表达型21例、basal-like型29例、Normalbreast-like型22例.38%的乳腺癌组织表达CD44+/CD24-表型,CD44+/CD24-表型在basal-like型、Lu-minalA型、LuminalB型、Her2过表达型、Normalbreast-like型乳腺癌中表达率分别为69.0%,36.2%,26.7%,19.0%,31.8%.CD44+/CD24-表型在乳腺癌各分子亚型中的表达具有显著差异性(P=0.003),高表达在basal-like乳腺癌中(69%).结论:CD44+/CD24-乳腺癌干细胞与basal-like乳腺癌有相关性;其他乳腺癌干细胞标志物仍需得到进一步鉴定.

基底细胞样乳腺癌中CIP2A及c-myc蛋白表达及意义

目的探讨CIP2A、c-myc在基底细胞样乳腺癌(basal-like breast carcinoma,BLBC)、非基底细胞样乳腺癌(non-basal-likebreast cancer,NON-BLBC)及正常乳腺组织中的表达及其之间的相互关系。方法采用免疫组化MaxVision两步法对43例BLBC、53例NON-BLBC及20例正常乳腺组织中CIP2A、c-myc的表达进行检测。结果 CIP2A、c-myc蛋白在BLBC中的表达明显高于正常乳腺组织,且与BLBC淋巴结转移及临床分期有关,差异均有统计学意义(P<0.05)。CIP2A与c-myc蛋白的表达呈正相关(r=0.446,P<0.01)。结论 CIP2A可能与BLBC的发生、发展相关,且进一步支持CIP2A与c-myc之间的正反馈调节作用。

Caspase-9、Bcl-2和Bax在基底细胞样乳腺癌组织中的表达及意义

目的探讨半胱天冬氨酸蛋白酶-9(Caspase-9)、B淋巴细胞瘤/白血病-2(Bcl-2)基因、Bcl-2同源拮抗蛋白/致死蛋白(Bax)基因在基底细胞样乳腺癌(BLBC)发生、发展中的作用。方法采用免疫组化法检测43例BLBC标本(BLBC组)、57例非BLBC乳腺癌标本(非BLBC组)及60例正常乳腺组织标本(正常组)Caspase-9、Bcl-2及Bax蛋白的表达水平,分析三者表达的相关性及其与BLBC临床病理特征的关系。结果 BLBC组、非BLBC组Bcl-2表达率均明显高于正常组,Caspase-9和Bax表达率均低于正常组,P均<0.05;Caspase-9、Bcl-2及Bax表达与BLBC淋巴结转移及临床分期相关,与年龄、肿瘤大小无关,Caspase-9与Bax表达呈正相关(r=0.572,P<0.05),Caspase-9与Bcl-2、Bax与Bcl-2表达均呈负相关(r=-0.381,r=-0.408,P<0.05)。结论 Caspase-9与Bax在BLBC组织中均呈低表达,Bcl-2呈高表达;三者在BLBC的发生、发展中共同发挥作用。

基底细胞样乳腺癌的形态学和免疫组织化学研究

目的观察基底细胞样乳腺癌(basal-like breast carcinoma,BLBCs)的形态学和免疫组织化学特征,并探讨其诊断标准。方法对45例BLBCs与15例腔A型乳腺癌进行形态学观察及免疫组化检测,使用一抗包括CK5/6、CK14、SMA、CD10、p63、CD117、EGFR、Vim、cyclin E、SKP2、Ki-67等指标。结果BLBCs形态学特征主要有:推进性生长方式(P=0.000);肿瘤间质有不同程度的淋巴细胞浸润(P=0.000);地图样坏死(P=0.000);非典型髓样癌特征(P=0.015);泡状核样(P=0.017);核分裂象多见(P=0.000);BLBCs高度表达以下免疫指标:CK5/6(P=0.000)、Vim(P=0.000)、CD117(P=0.018)、cyclin E(P=0.000)、SKP2(P=0.007)。结论BLBCs是经基因表型证实的一种特殊亚型的乳腺浸润性癌,形态学特征结合免疫组化特点可替代性诊断BLBCs。

黄芪多糖对基底细胞样乳腺癌细胞增殖和Akt磷酸化的影响

目的:观察黄芪多糖对基底细胞样乳腺癌细胞株MDA-MB-468细胞增殖和Akt蛋白磷酸化的影响。方法:用不同浓度的黄芪多糖(Astragalus polysaccharide,APS)干预MDA-MB-468细胞,用甲基噻唑基四唑法检测不同浓度APS干预对MDA-MB-468细胞增殖的量效和时效关系。用细胞内蛋白质印迹法检测APS干预MDA-MB-468细胞株1、2、4和7d后对磷酸化Akt(phospho-Akt,p-Akt)(Thr308)和p-Akt(Ser473)蛋白表达水平的影响,以及p53/鼠双微体2(murine double minute 2,MDM2)信号转导通路中的关键靶点p53、MDM2和人第10号染色体上磷酸酶和张力蛋白同源缺失的基因(phosphatase and tensin homolog deleted on chromosome ten,PTEN)蛋白表达水平的影响。用小干扰RNA(small interfering RNA,siRNA)技术沉默PTEN的表达,用细胞内蛋白质印迹法检测APS干预MDA-MB-468细胞2d对p-Akt(Thr308)和p-Akt(Ser473)蛋白表达水平的影响。结果:1和0.5mg/mL的APS对MDA-MB-468细胞的增殖有明显的抑制作用。1和0.5mg/mL的APS干预1、2、4和7d后能下调p-Akt(Thr308)的表达;干预1和2d后下调p-Akt(Ser473)的表达,上调MDM2蛋白的表达;干预7d后上调p53和PTEN蛋白的表达。PTEN沉默后,APS在干预2d后对p-Akt(Thr308)和p-Akt(Ser473)的表达没有影响,细胞增殖的抑制率低于PTEN未沉默时。结论:APS能抑制MDA-MB-468细胞的增殖,下调MDA-MB-468细胞Akt磷酸化的水平,其抑制MDA-MB-468细胞增殖的机制可能与通过对p53/MDM2正负反馈环的调节从而上调p53和PTEN蛋白的表达有关。

受体三阴性乳腺癌的研究进展

根据免疫组化染色的特征,将ER、PR和HER2受体均阴性的乳腺癌称之为受体三阴性乳腺癌,三阴性乳腺癌是具有独特生物学及临床特征的乳腺癌亚型,与基底细胞样乳腺癌有较高的一致性,复发早、进展快、生存短。对于三阴性乳腺癌的治疗,目前并没有推荐的化疗方案,而针对三阴性乳腺癌的靶向治疗正在进行临床研究。