鼻窦肠型腺癌中的肿瘤萌芽、p53 和 DNA 错配修复标记物:一项回顾性研究证实了肿瘤萌芽的不良预后影响

Cancers Pub Date : 2024-05-16 DOI:10.3390/cancers16101895
Sebastiano Puccio, Giuseppe Azzarello, Valeria Maffeis, Licia Laurino, Edoardo Mairani, Federica Conte, Nicola Tessari, Diego Cazzador, Elisabetta Zanoletti, Doriano Politi, Enzo Emanuelli, Giacomo Spinato, Simonetta Ausoni
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摘要

鼻窦肠型腺癌(ITAC)是一种非常罕见的、与职业密切相关的肿瘤,在组织学上与结直肠癌(CRC)非常相似。在后者中,肿瘤萌芽(TB)被广泛认为是一个负面的预后参数。本研究旨在评估 TB 在 ITAC 中的预后作用,并将其与该疾病的其他已确定或新出现的生物标志物(如 p53 和 DNA 错配修复(MMR)系统缺陷状态/微卫星不稳定性(MSI))相关联。我们回顾性分析了意大利北部两家医疗机构治疗的 32 例 ITAC 诊断患者的连续标本。我们对手术标本进行了肺结核评估(低-中-高);通过免疫组化对 p53 表达和 MMR 蛋白进行了评估。我们利用临床数据和患者的预后对结果进行了回顾性分层。根据萌芽计数,患者被分为两组:中/高萌芽(>4 TB)和低萌芽(≤4 TB)。与低芽数患者相比,高芽数(>4)患者的复发和死亡风险更高,中位生存期分别为 13 个月和 54 个月。在多变量分析中,将结核病、治疗和分期作为协变量考虑,结核病成为一个独立的预后因素,不受疾病分期或接受的治疗类型的影响。作为预后生物标志物的 p53 状态没有影响,也没有发现 MMR 蛋白发生改变。本研究的结果为肺结核在 ITAC 中的预后作用提供了进一步的重要证据,并强调了在临床实践中使用肺结核进行更大规模的多中心研究的必要性。
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Tumor Budding, p53, and DNA Mismatch Repair Markers in Sinonasal Intestinal-Type Adenocarcinoma: A Retrospective Study Supports the Adverse Prognostic Impact of Tumor Budding
Sinonasal intestinal-type adenocarcinoma (ITAC) is a very rare, closely occupational-related tumor with strong histological similarities to colorectal cancer (CRC). In the latter, tumor budding (TB) is widely recognized as a negative prognostic parameter. The aim of this study was to evaluate the prognostic role of TB in ITAC and to correlate it with other established or emerging biomarkers of the disease, such as p53 and deficient DNA mismatch repair (MMR) system status/microsatellite instability (MSI). We retrospectively analyzed 32 consecutive specimens of patients with ITAC diagnosis treated in two institutions in Northern Italy. We reviewed surgical specimens for TB evaluation (low-intermediate/high); p53 expression and MMR proteins were evaluated via immunohistochemistry. Results were retrospectively stratified using clinical data and patients’ outcomes. According to bud counts, patients were stratified into two groups: intermediate/high budding (>4 TB) and low budding (≤4 TB). Patients with high TB (>4) have an increased risk of recurrence and death compared to those with low TB, with a median survival of 13 and 54 months, respectively. On multivariate analysis, considering TB, therapy, and stage as covariates, TB emerged as an independent prognostic factor net of the stage of disease or type of therapy received. No impact of p53 status as a biomarker of prognosis was observed and no alterations regarding MMR proteins were identified. The results of the present work provide further significant evidence on the prognostic role of TB in ITAC and underline the need for larger multicenter studies to implement the use of TB in clinical practice.
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