Tumor-infiltrating lymphocytes are the key determinants of pathological features associated with pathogenic BRCA variants in high-grade serous ovarian carcinoma.

IF 3.1 3区医学 Q1 MEDICINE, GENERAL & INTERNAL

Frontiers in Medicine Pub Date : 2025-06-03 eCollection Date: 2025-01-01 DOI:10.3389/fmed.2025.1555883

Dang H Nguyen-Phan, Tin Dang, Anh N Dang, Loc T H Huynh, Phuong T B Nguyen, Vu Q Tran, Hanh T T Ngo, Thao T P Doan, Tu A Thai, Chien-Chin Chen

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引用次数: 0

Abstract

Background: High-grade serous ovarian carcinoma (HGSOC), an aggressive cancer associated with pathogenic BRCA variants, causes genomic instability and sensitivity to poly (ADP-ribose) polymerase inhibitors. Identifying pathogenic BRCA variants is crucial for the treatment of HGSOC; however, genetic testing is expensive and time-consuming. This study aimed to explore pathological features, particularly the presence of tumor-infiltrating lymphocytes (TILs), as potential surrogates to streamline patient selection for genetic testing.

Methods: We retrospectively analyzed 58 cases of HGSOC with known BRCA variant profiles. Tumors were categorized as TIL-positive or TIL-negative based on the presence of > 40 or ≤ 40 intraepithelial lymphocytes in a single high-power field (HPF), respectively. Key pathological features, including solid, endometrioid, and transitional (SET) architecture patterns; necrosis; and mitotic activity, were evaluated within these subgroups. Statistical analyses were used to determine the associations between these features and BRCA variant status.

Results: In TIL-negative HGSOCs, SET patterns were strongly associated with pathogenic or likely pathogenic BRCA variants (p = 0.028), emerging as the most reliable morphological marker in this group. In TIL-positive HGSOCs, low mitotic activity (≤7 mitotic figure per 10 HPFs) was significantly correlated with pathogenic BRCA variants (p = 0.0002), underscoring its diagnostic significance. Necrosis and mitotic activity in TIL-negative cases and SET patterns in TIL-positive cases were not significantly associated with pathogenic BRCA variants. Combined analysis of both TIL subgroups diluted these associations, underscoring the significance of stratifying cases by the immune context.

Discussion: The presence of TILs affects the diagnostic value of pathological features for BRCA variant status in HGSOC. Regarding pathogenic BRCA variants, SET patterns and low mitotic activity were identified as critical markers in TIL-negative tumors and TIL-positive tumors, respectively. These associations likely stem from interactions among genomic instability, immune response, and tumor growth. Our framework leverages these insights to prioritize high-risk cases for genetic testing, thereby optimizing resource allocation.

Conclusion: The presence of TILs is critical for understanding the association between pathological features and pathogenic BRCA variants in HGSOC. To improve pathogenic BRCA variant prediction, optimize genetic testing, and guide tailored intervention, our framework integrates immune context and morphological markers. This approach is especially useful in resource-limited settings and can enhance diagnostic efficiency and clinical decision-making.

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肿瘤浸润淋巴细胞是高级别浆液性卵巢癌中与致病性BRCA变异相关的病理特征的关键决定因素。

背景：高级别浆液性卵巢癌（HGSOC）是一种与致病性BRCA变异相关的侵袭性癌症，导致基因组不稳定和对聚adp核糖聚合酶抑制剂的敏感性。鉴定致病性BRCA变异对治疗HGSOC至关重要；然而，基因检测既昂贵又耗时。本研究旨在探讨病理特征，特别是肿瘤浸润淋巴细胞（til）的存在，作为简化患者基因检测选择的潜在替代品。方法：我们回顾性分析了58例已知BRCA变异谱的HGSOC。根据单个高倍视场（HPF）中存在bbb40或≤40上皮内淋巴细胞将肿瘤分为til阳性或til阴性。主要病理特征，包括实性、子宫内膜样和过渡性（SET）结构模式；坏死;有丝分裂活性，在这些亚组中进行评估。统计分析用于确定这些特征与BRCA变异状态之间的关联。结果：在til阴性的hgsoc中，SET模式与致病性或可能致病性BRCA变异密切相关（p = 0.028），是该组中最可靠的形态学标记。在til阳性的HGSOCs中，低有丝分裂活性（每10个hfs≤7个有丝分裂图）与致病性BRCA变异显著相关（p = 0.0002），强调其诊断意义。til阴性病例的坏死和有丝分裂活性以及til阳性病例的SET模式与致病性BRCA变异无显著相关性。对两个TIL亚组的综合分析淡化了这些关联，强调了按免疫背景对病例进行分层的重要性。讨论：TILs的存在影响HGSOC中BRCA变异状态的病理特征的诊断价值。对于致病性BRCA变异，SET模式和低有丝分裂活性分别被确定为til -阴性肿瘤和til -阳性肿瘤的关键标志物。这些关联可能源于基因组不稳定性、免疫反应和肿瘤生长之间的相互作用。我们的框架利用这些见解来优先考虑基因检测的高风险病例，从而优化资源分配。结论：TILs的存在对于理解HGSOC的病理特征与致病性BRCA变异之间的关系至关重要。为了提高BRCA致病性变异预测，优化基因检测，指导量身定制的干预，我们的框架整合了免疫背景和形态标记。这种方法在资源有限的情况下特别有用，可以提高诊断效率和临床决策。

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来源期刊

Frontiers in Medicine Medicine-General Medicine

CiteScore

5.10

自引率

5.10%

发文量

3710

审稿时长

12 weeks

期刊介绍： Frontiers in Medicine publishes rigorously peer-reviewed research linking basic research to clinical practice and patient care, as well as translating scientific advances into new therapies and diagnostic tools. Led by an outstanding Editorial Board of international experts, this multidisciplinary open-access journal is at the forefront of disseminating and communicating scientific knowledge and impactful discoveries to researchers, academics, clinicians and the public worldwide. In addition to papers that provide a link between basic research and clinical practice, a particular emphasis is given to studies that are directly relevant to patient care. In this spirit, the journal publishes the latest research results and medical knowledge that facilitate the translation of scientific advances into new therapies or diagnostic tools. The full listing of the Specialty Sections represented by Frontiers in Medicine is as listed below. As well as the established medical disciplines, Frontiers in Medicine is launching new sections that together will facilitate - the use of patient-reported outcomes under real world conditions - the exploitation of big data and the use of novel information and communication tools in the assessment of new medicines - the scientific bases for guidelines and decisions from regulatory authorities - access to medicinal products and medical devices worldwide - addressing the grand health challenges around the world