Saroufim Maya, Habib Robert H, Gerges Rita, Saab Jad, Loya Asif, Amr Samir S, Sheikh Salwa, Satti Mohammad, Oberkanins Christian, Khalifeh Ibrahim
American University of Beirut Medical Center, Beirut, Lebanon.
Weill-Cornell Medical Center, New York, NY, United States.
Exp Mol Pathol. 2014 Dec;97(3):315-20. doi: 10.1016/j.yexmp.2014.09.008. Epub 2014 Sep 16.
Selective BRAF inhibitors have shown dramatic results with regard to improving outcome in patients with melanoma. Testing the BRAF status in matched primary and metastatic melanomas to optimize individual targeted therapy is not well investigated.
Extended BRAF testing using PCR for 9 mutations and VE1 immunohistochemistry for BRAF V600E detection on 95 lesions including 40 primary melanomas with their matched metastases (n = 42), recurrences (n = 9) and second primaries (n = 4) was performed. Nine patients had multiple metastases.
V600E was the only identified mutation type; 35.4% of primary vs. 18.9% of metastatic melanomas. The overall primary-metastatic BRAF status discordance rate was 32.3% using PCR and 27.5% with immunohistochemistry, and was significantly more frequent in primary lesions with mutant BRAF (67%). Males and patients with metastasis to lymph nodes were less likely to be discordant compared to females and those with metastasis to other sites (p = 0.023). Discordant BRAF mutation status was predicted by multivariate binary logistic regression: the presence of a mutant BRAF in the primary melanoma [OR (95% C.I.) = 23.4 (2.4-229.7)] and female gender [OR = 10.6 (1.08-95)]. Inter-metastases BRAF concordance was 100% (6 comparisons).
A high discordant rate implies the need for clinical trials addressing the response to targeted therapy in patients with discordant BRAF statuses between their primary and metastatic lesions.
选择性BRAF抑制剂在改善黑色素瘤患者的预后方面已显示出显著效果。对于在匹配的原发性和转移性黑色素瘤中检测BRAF状态以优化个体化靶向治疗的研究尚不充分。
对95个病灶进行了扩展BRAF检测,采用PCR检测9种突变,并采用VE1免疫组化检测BRAF V600E,其中包括40例原发性黑色素瘤及其匹配的转移灶(n = 42)、复发灶(n = 9)和第二原发性肿瘤(n = 4)。9例患者有多个转移灶。
V600E是唯一鉴定出的突变类型;原发性黑色素瘤中为35.4%,转移性黑色素瘤中为18.9%。使用PCR检测时,原发性-转移性BRAF状态的总体不一致率为32.3%,免疫组化检测时为27.5%,在BRAF突变的原发性病灶中更为常见(67%)。与女性以及有其他部位转移的患者相比,男性和有淋巴结转移的患者出现不一致的可能性较小(p = 0.023)。通过多因素二元逻辑回归预测BRAF突变状态不一致:原发性黑色素瘤中存在BRAF突变[比值比(95%置信区间)= 23.4(2.4 - 229.7)]以及女性性别[比值比 = 10.6(1.08 - 95)]。转移灶之间的BRAF一致性为100%(6次比较)。
高不一致率意味着需要开展临床试验,以研究原发性和转移性病灶BRAF状态不一致的患者对靶向治疗的反应。
