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评估新辅助化疗后乳腺癌的肿瘤负荷、组织学变化及免疫格局:来自50例病例的见解

Evaluating the Tumor Burden, Histological Changes, and Immune Landscape of Breast Cancer Post-neoadjuvant Chemotherapy: Insights From 50 Cases.

作者信息

Rajesh Arasi, Gurusamy Dharma Saranya, Manikkam Rajalakshmi

机构信息

Pathology, Government Medical College, Tuticorin, IND.

Pathology, Government Medical College, Virudhunagar, IND.

出版信息

Cureus. 2025 Mar 8;17(3):e80258. doi: 10.7759/cureus.80258. eCollection 2025 Mar.

Abstract

Breast cancer is a heterogeneous disease with variable responses to neoadjuvant chemotherapy (NACT). Evaluating the histopathological and immune changes in post-NACT breast cancer specimens is crucial for understanding treatment response and guiding further management. This study aims to assess tumor burden using the Residual Cancer Burden (RCB) index, examine histological alterations, evaluate immune activity through tumor-infiltrating lymphocytes (TILs), and analyze proliferative capacity via Ki-67 expression in post-NACT breast cancer specimens. A cross-sectional study of 50 modified radical mastectomy (MRM) specimens post-NACT was conducted. The histopathological analysis included tumor regression changes, stromal and cellular alterations, and nodal involvement. Immune response was assessed by quantifying TILs, and proliferation was measured using the Ki-67 index. Statistical correlations were made between clinicopathological parameters, TILs, and Ki-67 expression. Residual disease was detected in 39 cases (78%), and 11 cases (22%) had no residual disease. Among the 39 cases with residual disease, the majority were classified as RCB II (22 cases, 56%), 16 cases (41%) were classified as RCB III, and one case (3%) was classified as RCB I. Common histological changes post-NACT included fibrosis in 31 cases (62%), necrosis in 19 cases (38%), and infiltration by foamy histiocytes in 16 cases (32%). Malignant epithelial cells more frequently exhibited foamy cytoplasm (16 cases (41%) vs. two cases (5%); p=0.0003), hyperchromatic nucleus (26 cases (67%) vs. six cases (15%); p=0.0001), and prominent nucleoli (26 cases (67%) vs. four cases (10%); p=0.0001) compared to benign cells. Among the 39 cases with residual disease, low TIL and high Ki-67 expression were observed in 20 cases (51%), while 12 cases (32%) showed high TIL and low Ki-67. Residual tumors with high TIL and high Ki-67 (four cases, 10%) and low TIL and low Ki-67 (three cases, 8%) were less common. A significant inverse relationship was found between TIL levels and Ki-67 expression (p=0.0002), as tumors with low TIL were more likely to have high Ki-67 expression (20 cases, 51%), whereas those with high TIL more frequently exhibited low Ki-67 expression (12 cases, 32%). Post-NACT evaluation of tumor burden, immune landscape, and proliferation provides valuable prognostic insights. Integrating RCB, TILs, and Ki-67 into routine pathological assessment may aid patient stratification and guide personalized treatment strategies. Further large-scale studies are needed to validate these findings and improve therapeutic decision-making in breast cancer management.

摘要

乳腺癌是一种异质性疾病,对新辅助化疗(NACT)的反应各不相同。评估NACT后乳腺癌标本的组织病理学和免疫变化对于了解治疗反应和指导进一步治疗至关重要。本研究旨在使用残余癌负担(RCB)指数评估肿瘤负荷,检查组织学改变,通过肿瘤浸润淋巴细胞(TILs)评估免疫活性,并通过NACT后乳腺癌标本中Ki-67的表达分析增殖能力。对50例NACT后的改良根治性乳房切除术(MRM)标本进行了横断面研究。组织病理学分析包括肿瘤消退变化、基质和细胞改变以及淋巴结受累情况。通过量化TILs评估免疫反应,使用Ki-67指数测量增殖情况。对临床病理参数、TILs和Ki-67表达进行了统计学相关性分析。39例(78%)检测到残留疾病,11例(22%)无残留疾病。在39例有残留疾病的病例中,大多数被分类为RCB II(22例,56%),16例(41%)被分类为RCB III,1例(3%)被分类为RCB I。NACT后常见的组织学变化包括31例(62%)纤维化、19例(38%)坏死和16例(32%)泡沫组织细胞浸润。与良性细胞相比,恶性上皮细胞更常表现出泡沫状细胞质(16例(41%)对2例(5%);p=0.0003)、核深染(26例(67%)对6例(15%);p=0.0001)和明显核仁(26例(67%)对4例(10%);p=0.0001)。在39例有残留疾病的病例中,20例(51%)观察到低TIL和高Ki-67表达,而12例(32%)表现为高TIL和低Ki-67。高TIL和高Ki-67的残留肿瘤(4例,10%)和低TIL和低Ki-67的残留肿瘤(3例,8%)较少见。发现TIL水平与Ki-67表达之间存在显著负相关(p=0.0002),因为TIL低的肿瘤更可能具有高Ki-67表达(20例,51%),而TIL高的肿瘤更常表现为低Ki-67表达(12例,32%)。NACT后对肿瘤负荷、免疫格局和增殖的评估提供了有价值的预后见解。将RCB、TILs和Ki-67纳入常规病理评估可能有助于患者分层并指导个性化治疗策略。需要进一步的大规模研究来验证这些发现并改善乳腺癌管理中的治疗决策。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ff62/11890627/18ecd1d6dd94/cureus-0017-00000080258-i01.jpg

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