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首页> 外文期刊>Neurosurgical focus >Liquid biopsies for the diagnosis and surveillance of primary pediatric central nervous system tumors: a review for practicing neurosurgeons
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Liquid biopsies for the diagnosis and surveillance of primary pediatric central nervous system tumors: a review for practicing neurosurgeons

机译:液体活组织检查诊断和监测原发性小儿中枢神经系统肿瘤:练习神经外科的综述

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OBJECTIVE Primary brain tumors are the most common cause of cancer-related deaths in children and pose difficult questions for the treating physician regarding issues such as the risk/benefit of performing a biopsy, the accuracy of monitoring methods, and the availability of prognostic indicators. It has been recently shown that tumor-specific DNA and proteins can be successfully isolated in liquid biopsies, and it may be possible to exploit this potential as a particularly useful tool for the clinician in addressing these issues. METHODS A review of the current literature was conducted by searching PubMed and Scopus. MeSH terms for the search included “liquid biopsy,” “brain,” “tumor,” and “pediatrics” in all fields. Articles were reviewed to identify the type of brain tumor involved, the method of tumor DNA/protein analysis, and the potential clinical utility. All articles involving primary studies of pediatric brain tumors were included, but reviews were excluded. RESULTS The successful isolation of circulating tumor DNA (ctDNA), extracellular vesicles, and tumor-specific proteins from liquid biopsies has been consistently demonstrated. This most commonly occurs through CSF analysis, but it has also been successfully demonstrated using plasma and urine samples. Tumor-related gene mutations and alterations in protein expression are identifiable and, in some cases, have been correlated to specific neoplasms. The quantity of ctDNA isolated also appears to have a direct relationship with tumor progression and response to treatment. CONCLUSIONS The use of liquid biopsies for the diagnosis and monitoring of primary pediatric brain tumors is a foreseeable possibility, as the requisite developmental steps have largely been demonstrated. Increasingly advanced molecular methods are being developed to improve the identification of tumor subtypes and tumor grades, and they may offer a method for monitoring treatment response. These minimally invasive markers will likely be used in the clinical treatment of pediatric brain tumors in the future.
机译:目标原发性脑肿瘤是儿童癌症相关死亡的最常见原因,对治疗医生构成困难的问题,了解诸如进行活检的风险/益处,监测方法的准确性以及预后指标的可用性等问题。最近已经表明,肿瘤特异性DNA和蛋白质可以成功地分离在液体活组织检查中,并且可以将这种潜力作为临床医生提供的特别有用的工具中,以解决这些问题。方法通过搜索PubMed和Scopus来进行当前文献的审查。用于搜索的网格术语包括“液体活检,”“脑,”肿瘤“肿瘤”和“儿科”在所有领域。综述文章以鉴定所涉及的脑肿瘤类型,肿瘤DNA /蛋白质分析的方法,以及潜在的临床效用。包括涉及对儿科脑肿瘤的初步研究的所有文章,但除了征收的评论。结果一直证明,循环肿瘤DNA(CTDNA),细胞外囊泡和肿瘤特异性蛋白的成功分离已经证明。这通常是通过CSF分析发生的,但也已经通过血浆和尿液样本成功地证明。肿瘤相关的基因突变和蛋白质表达的改变是可识别的,在某些情况下,与特定的肿瘤相关。分离的CTDNA的数量也似乎与肿瘤进展和对治疗的反应具有直接关系。结论使用液体活组织检查对原发性小儿脑肿瘤的诊断和监测是可预见的可能性,因为必要的发育步骤在很大程度上已经证明。正在开发越来越先进的分子方法以改善肿瘤亚型和肿瘤等级的鉴定,并且它们可以提供用于监测治疗响应的方法。这些微创标志物可能在未来进行小儿脑肿瘤的临床治疗中使用。

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