Saha S, Wiese D, Badin J, Beutler T, Nora D, Ganatra B K, Desai D, Kaushal S, Nagaraju M, Arora M, Singh T
Department of Anatomy, Michigan State University, McLaren Regional Medical Center, Flint, USA.
Ann Surg Oncol. 2000 Mar;7(2):120-4. doi: 10.1007/s10434-000-0120-z.
Sentinel lymph node (SLN) mapping for melanoma and breast cancer has greatly enhanced the identification of micrometastases in many patients, thereby upstaging a subset of these patients. The purpose of this study was to see if SLN mapping technique could be used to identify SLNs in colorectal cancer and to assess its impact on pathological staging and treatment.
At the time of surgery, 1 ml of Lymphazurin 1% was injected subserosally around the tumor without injecting into the lumen. The first to fourth blue nodes identified were considered the SLNs, which have the highest probability to contain metastases. A standard oncological resection of the bowel was then performed. Multilevel microsections of the SLNs, including a detailed pathological examination of the entire specimen, was performed.
SLN was successfully identified in 85 (98.8%) of 86 patients. In 85 patients, there were 1,367 (16 per patient) lymph nodes examined, of which 140 (1.6 per patient) were identified as SLNs. In 53 (95%) of 56, of whom the SLNs were without metastases (negative), all other non-SLNs also were negative. In 29 (34% of 85) patients, SLNs were positive for metastases; in 14 of the 29 patients, other non-SLNs also were positive in addition to the SLNs. In the other 15 of the 29 patients (18% of 85 patients), SLNs were the only site of metastases, and all other non-SLNs were negative. In 7 patients (8.2% of 85 patients), micrometastases were identified only in 1 or 2 of the 10 sections of a single SLN. In five of seven patients, such micrometastases were detected by hematoxylin and eosin staining and immunohistochemistry; in the other two patients, it was detected only by immunohistochemistry. In patients with negative SLNs, the rate of occurrence of micrometastases in non-SLNs was 5 (0.4%) of 1,184 lymph nodes.
SLN mapping can be performed easily in colorectal cancer patients, with an accuracy of more than 95%. The identification of submicroscopic lymph node metastases by this technique may have upstaged these patients (18%) from stage I/II to stage III disease, who may then benefit from further adjuvant chemotherapy.
黑色素瘤和乳腺癌的前哨淋巴结(SLN)定位极大地提高了许多患者微转移灶的识别率,从而使部分患者分期上调。本研究的目的是探讨SLN定位技术能否用于识别结直肠癌的SLN,并评估其对病理分期和治疗的影响。
手术时,在肿瘤周围浆膜下注射1%的亚甲蓝1ml,不注入肠腔。最先发现的4个蓝色淋巴结被视为SLN,其转移可能性最高。然后进行标准的肠道肿瘤切除手术。对SLN进行多级切片,包括对整个标本进行详细的病理检查。
86例患者中有85例(98.8%)成功识别出SLN。85例患者共检查了1367个淋巴结(平均每例16个),其中140个(平均每例1.6个)被确定为SLN。56例SLN无转移(阴性)的患者中,53例(95%)所有其他非SLN也为阴性。29例(85例中的34%)患者的SLN有转移;这29例患者中,14例的其他非SLN除SLN外也有转移。29例患者中的另外15例(85例患者中的18%),SLN是唯一的转移部位,所有其他非SLN均为阴性。7例患者(85例患者中的8.2%),仅在单个SLN的10个切片中的1个或2个切片中发现微转移。7例患者中的5例,苏木精-伊红染色和免疫组化检测到这种微转移;另外2例患者仅通过免疫组化检测到。SLN阴性的患者中,非SLN微转移的发生率为1184个淋巴结中的5个(0.4%)。
结直肠癌患者中SLN定位操作简便,准确率超过95%。通过该技术识别亚显微镜下淋巴结转移可能使这些患者(18%)分期从I/II期上调至III期,进而可能从进一步的辅助化疗中获益。
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