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巴雷特食管相关腺癌的预后、治疗现状及前瞻性创新:文献综述

Current state of prognostication, therapy and prospective innovations for Barrett's-related esophageal adenocarcinoma: a literature review.

作者信息

Mittal Sumeet K, Abdo Joe, Adrien Malika P, Bayu Binyam A, Kline Jay R, Sullivan Molly M, Agrawal Devendra K

机构信息

Norton Thoracic Institute, St. Joseph's Hospital and Medical Center, Dignity Health, Phoenix, AZ, USA.

Stella Diagnostics, Inc., Salt Lake City, UT, USA.

出版信息

J Gastrointest Oncol. 2021 Aug;12(4):1197-1214. doi: 10.21037/jgo-21-117.

Abstract

OBJECTIVE

Barrett's esophagus (BE) is the only known precursor to esophageal adenocarcinoma (EAC), which has one of the lowest 5-year survival rates in oncology. The reasons for poor survival are twofold: the large majority of diagnoses are in advanced stages (~80%) and limited treatment options, with a deficit of biology-guided therapies. As a rapidly growing public health concern with poor prognosis, research into the molecular progression for BE and novel therapeutics for EAC currently has high clinical utility. Review of the literature reveals that innovative analysis of metaplastic progression from BE to EAC at a molecular level can shed light on the underlying transformative probabilities of BE into malignant pathologies and may impact current of future therapeutic modalities for management of these diseases.

BACKGROUND

EAC is the fastest increasing cancer in the United States with a 600% increase over the past 25 years. This cancer arises from dysplastic tissue of BE, a complication of gastroesophageal reflux disease (GERD). Chronic acid and bile reflux in the distal esophagus initiates a metaplastic conversion of normal squamous epithelium to premalignant intestinalized columnar epithelium. Patients with BE have a 125-fold higher risk of cancer compared to the general population.

METHODS

We critically reviewed the current status of BE monitoring, and subsequent therapeutic strategies being used in patients who have progressed to cancer. Also, new diagnostic tools and therapeutic candidates for BE-related EAC are discussed. Highly-targeted searches of databases containing recent original peer-reviewed papers were utilized for this review.

CONCLUSIONS

Novel and well-described biomarkers analyzed in the patient's diseased tissue will provide for more powerful diagnostics, but also possess the potential to develop strategies for personalized management and identify targets for intervention to either cease disease progression or treat BE and/or EAC. Since millions of Americans develop BE without progressing to cancer, there is a critical need to identify the small percentage of Barrett's patients who possess hallmarks of disease progression or carcinogenesis with novel screening techniques. Incorporation of such tools into standard screening protocols for BE surveillance and/or therapy would be critical to detect malignant transformations before clinically obvious cancer ever develops.

摘要

目的

巴雷特食管(BE)是食管腺癌(EAC)唯一已知的癌前病变,而食管腺癌是肿瘤学中5年生存率最低的疾病之一。生存率低的原因有两方面:绝大多数诊断为晚期(约80%)且治疗选择有限,缺乏生物学指导的疗法。作为一种预后不良且迅速引起公众健康关注的疾病,对BE的分子进展及EAC新型疗法的研究目前具有很高的临床应用价值。文献综述表明,从分子水平对BE向EAC的化生进展进行创新性分析,能够揭示BE转变为恶性病变的潜在可能性,并可能影响当前或未来这些疾病的治疗方式。

背景

EAC是美国发病率增长最快的癌症,在过去25年中增长了600%。这种癌症起源于BE的发育异常组织,BE是胃食管反流病(GERD)的一种并发症。远端食管的慢性酸和胆汁反流引发正常鳞状上皮向癌前肠化生柱状上皮的化生转变。与普通人群相比,BE患者患癌风险高125倍。

方法

我们严格审查了BE监测的现状以及用于进展为癌症患者的后续治疗策略。此外,还讨论了与BE相关的EAC的新诊断工具和治疗候选方案。本综述利用对包含近期经同行评审的原始论文的数据库进行的高度针对性搜索。

结论

在患者病变组织中分析的新型且描述详尽的生物标志物将提供更强大的诊断方法,同时也有可能制定个性化管理策略并确定干预靶点,以阻止疾病进展或治疗BE和/或EAC。由于数百万美国人患BE但未进展为癌症,因此迫切需要通过新型筛查技术识别出一小部分具有疾病进展或致癌特征的巴雷特患者。将此类工具纳入BE监测和/或治疗的标准筛查方案对于在临床明显癌症发生之前检测恶性转化至关重要。

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