Pasca Fenesan Mihaela-Maria, Cosma Andrei Alexandru, Melnic Eugen, Cimpean Anca Maria, Cozma Gabriel Veniamin, Negru Alina Gabriela
Department of Microscopic Morphology/Histology, Doctoral School in Medicine, Department of Clinical Oncology, Victor Babeș University of Medicine and Pharmacy, Timisoara, ROU.
Department of Pathology, Nicolae Testemitanu State University of Medicine and Pharmacy, Chișinău, MDA.
Cureus. 2024 Dec 17;16(12):e75908. doi: 10.7759/cureus.75908. eCollection 2024 Dec.
Alpha-smooth muscle actin (αSMA) has been widely investigated in malignancies, primarily concerning its expression in cancer-associated fibroblasts (CAFs) inside the tumor stroma. Microscopic examination indicates that αSMA expression is not confined to the tumor stromal compartment but is also present in a subset of tumor cells, and this expression correlates with an enhanced invasive phenotype of malignant cells from lung, liver, or ovarian malignancies. Information on actin expression in breast cancer (BC) cells is scarce, and its influence on clinicopathological characteristics remains ambiguous due to conflicting findings in the literature.
To examine the αSMA tumor score in breast cancer cells utilizing digital image analysis (DIA) methodologies and to critically analyze the varying effects of αSMA tumor score values on clinicopathologic parameters, particularly focusing on tumor cell invasiveness, recurrence, and survival.
Double immunostaining for CD34 and αSMA was conducted on 53 breast cancer cases that were thoroughly characterized in relation to clinicopathologic data. Double immunostaining for CD34 and αSMA demonstrated different distribution patterns of both markers in normal and breast cancer tissues. DIA data about αSMA tumor cell density, intensity, tumor score, and histological score were correlated with clinicopathological factors.
We delineated three unique breast cancer subgroups based on αSMA tumor scores: a 9.43% low-expressing subgroup (αSMA_TS, score 4), a 35.07% medium-expressing subgroup (αSMA_TS, scores 5 and 6), and a 55.5% high-expressing subgroup (αSMA_TS, scores 7 and 8). Stromal immature vessels and tertiary lymphoid structures (TLS) exhibited a strong correlation with αSMA_TS, whereas recurrence, perineural, and lymphovascular invasion strongly influenced the αSMA_TS and αSMA_TS subgroups. The αSMA_TS subgroup demonstrated the most heterogeneity with the influence of αSMA-expressing breast cancer cells on tumor size, nodal status, perineural and lymphovascular invasion, menopausal status, recurrence, and survival. Most of the cases from the αSMA_TS subgroup had Luminal B and Luminal B-HER2 phenotypes, while triple-negative breast cancer (TNBC) represented one-third of all cases in the αSMA_TS subgroup.
αSMA-expressing breast cancer cells variably affect malignant growth, invasion, and recurrence, highly contingent upon their density and expression intensity. The current investigation identified an αSMA_TS BC subgroup that appears to promote invasiveness, recurrence, and survival in breast cancer. Our data indicate that αSMA BC-expressing cells play a dual role in BC progression, contingent upon their percentage and expression intensity; however, further research is required to elucidate the factors and mechanisms responsible for their accumulation and/or transdifferentiation in malignant breast tissue.
α平滑肌肌动蛋白(αSMA)已在恶性肿瘤中得到广泛研究,主要涉及其在肿瘤基质内癌相关成纤维细胞(CAF)中的表达。显微镜检查表明,αSMA的表达不仅局限于肿瘤基质区室,也存在于一部分肿瘤细胞中,并且这种表达与来自肺、肝或卵巢恶性肿瘤的恶性细胞侵袭性增强表型相关。关于乳腺癌(BC)细胞中肌动蛋白表达的信息匮乏,且由于文献中的矛盾发现,其对临床病理特征的影响仍不明确。
利用数字图像分析(DIA)方法检测乳腺癌细胞中的αSMA肿瘤评分,并严格分析αSMA肿瘤评分值对临床病理参数的不同影响,尤其关注肿瘤细胞侵袭性、复发和生存情况。
对53例乳腺癌病例进行CD34和αSMA双重免疫染色,并根据临床病理数据进行全面特征分析。CD34和αSMA双重免疫染色显示了这两种标志物在正常和乳腺癌组织中的不同分布模式。关于αSMA肿瘤细胞密度、强度、肿瘤评分和组织学评分的DIA数据与临床病理因素相关联。
我们根据αSMA肿瘤评分划定了三个独特的乳腺癌亚组:一个低表达亚组(αSMA_TS,评分为4),占9.43%;一个中等表达亚组(αSMA_TS,评分为5和6),占35.07%;一个高表达亚组(αSMA_TS,评分为7和8),占55.5%。基质未成熟血管和三级淋巴结构(TLS)与αSMA_TS密切相关,而复发、神经周围和淋巴管浸润强烈影响αSMA_TS及αSMA_TS亚组。αSMA_TS亚组表现出最大的异质性,即表达αSMA的乳腺癌细胞对肿瘤大小 nodal status、神经周围和淋巴管浸润、绝经状态、复发和生存有影响。αSMA_TS亚组中的大多数病例具有Luminal B和Luminal B-HER2表型,而三阴性乳腺癌(TNBC)占αSMA_TS亚组所有病例的三分之一。
表达αSMA的乳腺癌细胞对恶性生长、侵袭和复发有不同影响,这高度取决于它们的密度和表达强度。当前研究确定了一个αSMA_TS BC亚组,该亚组似乎促进乳腺癌的侵袭性、复发和生存。我们的数据表明,表达αSMA的BC细胞在BC进展中起双重作用,这取决于它们的百分比和表达强度;然而,需要进一步研究以阐明导致它们在恶性乳腺组织中积累和/或转分化的因素和机制。 (注:“nodal status”原文未翻译,可能是输入有误,若为“淋巴结状态”等,可按正确内容替换)
