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Recent advances in the detection of bone marrow micrometastases: A promising area for research or just another false hope? A review of the literature.

机译:骨髓微转移酶检测的最新进展:一个有希望的研究领域还是另一个错误的希望?文献综述。

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摘要

The presence of early disseminated tumor cells (DTC), otherwise termed micrometastases or minimal residual disease, in the bone marrow (BM), or other secondary compartments, such as the blood and the lymph nodes, is the main reason for recurrence of patients with early stage epithelial cancers after "curative" resection of the primary tumor. There is increasing evidence, that the detection of DTC in BM aspirates may provide additional and independent prognostic information and aid in the stratification of these patients for adjuvant clinical treatment. However, the clinical relevance of micrometastases has not yet been firmly established. In addition, the molecular events and interactions that prevail in early metastatic disease and determine the formation or not of overt metastases remain poorly understood. The methods currently used for the detection of micrometastatic cells include extremely sensitive immunocytochemical and molecular assays, often in conjunction with enrichment techniques for the purification of tumor cells and additional increase of their sensitivity. Nevertheless, the specificity of these methods is mostly inadequate. After the impressive advances of molecular cytogenetics, a highly accurate and global assessment of the genetic status of tumors is now possible. Therefore, the greatest challenge of our time is the application of these novel technologies for the clarification of the key molecular events that initiate metastatic spread. This will further enable us to identify the highly specific and sensitive diagnostic and prognostic markers as well as the therapeutic targets which are so urgently needed.
机译:骨髓(BM)或其他次级隔室(例如血液和淋巴结)中存在早期播散的肿瘤细胞(DTC),也称为微转移或极少的残留疾病,是复发性DPS患者的主要原因。 “根治性”切除原发肿瘤后的早期上皮癌。越来越多的证据表明,在BM抽吸物中检测DTC可能会提供更多且独立的预后信息,并有助于对这些患者进行分层以进行辅助临床治疗。然而,微转移的临床相关性尚未得到牢固确立。另外,在早期转移性疾病中普遍存在并决定是否形成明显转移的分子事件和相互作用仍然知之甚少。当前用于检测微转移细胞的方法包括极其敏感的免疫细胞化学和分子测定,通常与用于纯化肿瘤细胞的富集技术结合并进一步提高其敏感性。然而,这些方法的特异性大多是不足的。在分子细胞遗传学取得令人瞩目的进步之后,现在可以对肿瘤的遗传状态进行高度准确和全面的评估。因此,我们时代最大的挑战是应用这些新技术来阐明引发转移扩散的关键分子事件。这将使我们能够识别出高度特异性和敏感性的诊断和预后标志物以及急需的治疗目标。

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