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常规影像学检查结合 31 基因表达谱检测可较无监测影像学研究的患者更早地检测到黑色素瘤,且转移瘤负荷降低。

Routine imaging guided by a 31-gene expression profile assay results in earlier detection of melanoma with decreased metastatic tumor burden compared to patients without surveillance imaging studies.

机构信息

Department of Dermatology, Feinberg School of Medicine, Northwestern University, 676 N. St. Clair Street, Suite 1765, Chicago, IL, 60611, USA.

Department of Plastic Surgery, Cleveland Clinic Lerner Research Institute, Cleveland, OH, USA.

出版信息

Arch Dermatol Res. 2023 Oct;315(8):2295-2302. doi: 10.1007/s00403-023-02613-6. Epub 2023 Mar 28.

DOI:10.1007/s00403-023-02613-6
PMID:36977840
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10676305/
Abstract

Patients with early-stage disease typically have a good prognosis, but still have a risk of recurrence, even with negative sentinel lymph node biopsy (SLNB). This study explores the utility of routine imaging to detect metastases in patients with negative SLNB but high-risk 31 gene expression profile (31-GEP) scores. We retrospectively identified melanoma patients with negative SLNBs. Patients with high-risk GEP results were placed in the experimental group and patients without GEP testing were placed in the control group. Among both cohorts, recurrent melanoma groups were identified. The tumor burden at the time of recurrence and the time to recurrence were compared between experimental group patients with routine imaging and control group patients without imaging schedules. We identified 327 control patients and 307 experimental patients, of which 14.1% versus 20.5% had melanoma recurrence, respectively. Of the patients with recurrent melanoma, those in the experimental group were older (65.75 versus 59.20), had higher Breslow depths (3.72 mm versus 3.31 mm), and had advanced tumor staging (89.5% versus 71.4% of patients presenting clinical stage ≥ II) compared to the control group at primary diagnosis. However, melanoma recurrence was detected earlier (25.50 months versus 35.35 months) in the experimental group at a lower overall tumor burden (73.10 mm versus 27.60 mm). A higher percentage of experimental patients started immunotherapy when offered (76.3% and 67.9%). Patients who received routine imaging after high-risk GEP test scores had an earlier recurrence diagnosis with lower tumor burden, leading to better clinical outcomes.

摘要

患有早期疾病的患者通常预后良好,但即使前哨淋巴结活检(SLNB)阴性,仍有复发的风险。本研究探讨了在 SLNB 阴性但 31 基因表达谱(31-GEP)评分高风险的患者中,常规影像学检查检测转移的效用。我们回顾性地确定了 SLNB 阴性的黑色素瘤患者。GEP 结果高风险的患者被置于实验组,没有进行 GEP 检测的患者被置于对照组。在这两个队列中,都确定了复发性黑色素瘤组。比较了实验组常规影像学检查患者和对照组无影像学检查计划患者的复发时肿瘤负担和复发时间。我们确定了 327 名对照组患者和 307 名实验组患者,其中分别有 14.1%和 20.5%的患者出现黑色素瘤复发。在复发性黑色素瘤患者中,实验组患者年龄更大(65.75 岁比 59.20 岁),Breslow 深度更高(3.72mm 比 3.31mm),且在初诊时肿瘤分期更晚(89.5%比 71.4%的患者为临床分期≥Ⅱ期)。然而,实验组患者的黑色素瘤复发更早(25.50 个月比 35.35 个月),总肿瘤负担更低(73.10mm 比 27.60mm)。在实验组中,更多的患者在提供免疫治疗时开始接受治疗(76.3%和 67.9%)。在高风险 GEP 测试评分后接受常规影像学检查的患者更早地诊断出复发,且肿瘤负担更低,从而获得更好的临床结局。

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