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The detection and significance of melanoma micrometastases in sentinel nodes.

机译:前哨淋巴结中黑色素瘤微转移的检测及其意义。

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Sentinel node (SN) biopsy in melanoma patients is an accurate and minimally invasive method of staging and determining prognosis in patients with early-stage disease, and of identifying those patients who may benefit from complete regional lymph node dissection. Careful identification, removal and pathological assessment of SNs is critical to the accuracy of the technique and deficiencies in any of these steps may result in a false-negative biopsy. Pathologists should examine multiple sections from each SN, stained routinely with haematoxylin-eosin and immunohistochemically for melanoma-associated antigens. However, the most appropriate staining and sectioning protocol is not clear from the available evidence. While it appears that more extensive sectioning protocols detect more melanoma, failure rates and false-negative rates of the procedure do not appear to be significantly worse than with less extensive sampling protocols. Micromorphometrical parameters of melanoma deposits in SNs (such as their size, maximal tumour penetrative depth, microanatomical location and percentage nodal cross-sectional area) have been shown to be predictive of regional non-SN involvement and of clinical outcome. Classifying and measuring these parameters can be difficult, depending on the nature and distribution of the tumour deposits in the SN. Because the positive SNs have been removed in all patients included in studies assessing the clinical significance of tiny SN melanoma micrometastases, the likely therapeutic effect of the SN biopsy itself and/or any complete lymph node dissection, as well as lead time bias, are important confounding factors that must be considered when interpreting these studies. Limited data from some retrospective studies with relatively short follow-up suggest that some melanoma metastases may not be clinically relevant, but other studies imply a likely clinical significance of even very small SN metastases. Until there is unequivocal evidence from prospective randomised clinical trials with long term follow-up for the prognostic significance (or lack thereof) of very small SN tumour deposits, it is probably prudent to treat patients with such deposits as SN-positive.
机译:黑色素瘤患者的前哨淋巴结活检是一种准确,微创的分期和确定早期疾病患者预后的方法,可用于识别可能从区域淋巴结清扫中受益的患者。对SN进行仔细的识别,去除和病理评估对于该技术的准确性至关重要,而任何这些步骤中的缺陷都可能导致假阴性的活检。病理学家应检查每个SN的多个切片,常规用苏木精-曙红染色,并用免疫组织化学方法检查黑色素瘤相关抗原。但是,根据现有证据尚不清楚最合适的染色和切片方案。虽然似乎更广泛的切片方案可以检测到更多的黑色素瘤,但该方法的失败率和假阴性率似乎并不比不那么广泛的采样方案差得多。 SN中黑色素瘤沉积物的微观形态参数(例如其大小,最大肿瘤穿透深度,显微解剖学位置和淋巴结横截面面积百分比)已显示出区域性非SN参与和临床结局的预测。根据SN中肿瘤沉积物的性质和分布,很难对这些参数进行分类和测量。因为在研究中评估了微小SN黑色素瘤微转移的临床意义的所有患者中均去除了阳性SN,所以SN活检本身和/或任何完整的淋巴结清扫的可能的治疗效果以及前置时间偏差很重要。解释这些研究时必须考虑的混杂因素。一些随访时间相对较短的回顾性研究的有限数据表明,某些黑色素瘤转移可能与临床无关,但其他研究暗示即使很小的SN转移也可能具有临床意义。除非有长期随访的前瞻性随机临床试验明确证据显示极小的SN肿瘤沉积物的预后意义(或缺乏),否则谨慎对待具有SN阳性沉积物的患者。

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