Garlan Fanny, Blanchet Benoit, Kramkimel Nora, Puszkiel Alicja, Golmard Jean-Louis, Noe Gaelle, Dupin Nicolas, Laurent-Puig Pierre, Vidal Michel, Taly Valerie, Thomas-Schoemann Audrey
INSERM UMR-S1147, CNRS SNC5014, Equipe Labélisée Ligue Contre le Cancer, Université Paris Descartes, Centre Université Paris Sorbonne Cité, Universitaire des Saints-Pères, Paris, France.
Assistance Publique des Hôpitaux de Paris, Unité Fonctionnelle de Pharmacocinétique et Pharmacochimie, Hôpital Cochin, Paris, France.
Target Oncol. 2017 Jun;12(3):365-371. doi: 10.1007/s11523-017-0491-8.
Circulating tumor DNA (ctDNA) has been reported as a prognostic marker in melanoma. In BRAF V600-mutant melanoma, a plasma under-exposure to vemurafenib could favor emerging resistance but no biological data are available to support this hypothesis.
We aimed to investigate the relationship between vemurafenib plasma concentrations and the ctDNA plasma concentration during follow-up of BRAF-mutated melanoma patients.
Eleven patients treated with single-agent vemurafenib for advanced BRAF V600-mutant melanoma were analyzed in an exploratory monocentric study. The vemurafenib plasma concentration was measured by liquid chromatography. ctDNA was extracted from plasma samples and the ctDNA concentration was evaluated using picoliter droplet-based digital PCR with Taqman detection probes targeting the BRAF p.V600E/K mutation and wild-type BRAF sequences.
At baseline, plasma ctDNA was detectable in 72% (n = 8/11) of patients and the ctDNA concentration decreased in 88% of these patients (n = 7/8) from day (D) 0 to D15 after vemurafenib initiation. During follow-up, an increased ctDNA concentration was detected in nine patients: in five patients, the first increase in ctDNA concentrations followed a decrease in vemurafenib concentrations. More interestingly, an inverse correlation between vemurafenib concentration and ctDNA concentrations was demonstrated (p = 0.026). The ctDNA concentration at baseline was associated with overall survival (hazard ratio = 2.61, 95% CI 1.04-6.56; p = 0.04).
This study demonstrates the relevance of vemurafenib plasma monitoring during the follow-up of metastatic melanoma patients. Plasma drug monitoring and ctDNA concentrations could be combined to monitor tumor evolution in melanoma patients treated with anti-BRAF therapies.
循环肿瘤DNA(ctDNA)已被报道为黑色素瘤的一种预后标志物。在BRAF V600突变的黑色素瘤中,血浆中维莫非尼暴露不足可能会促进耐药性的出现,但尚无生物学数据支持这一假设。
我们旨在研究BRAF突变的黑色素瘤患者随访期间维莫非尼血浆浓度与ctDNA血浆浓度之间的关系。
在一项探索性单中心研究中,分析了11例接受单药维莫非尼治疗的晚期BRAF V600突变黑色素瘤患者。通过液相色谱法测量维莫非尼血浆浓度。从血浆样本中提取ctDNA,并使用基于皮升液滴的数字PCR和靶向BRAF p.V600E/K突变及野生型BRAF序列的Taqman检测探针评估ctDNA浓度。
基线时,72%(n = 8/11)的患者血浆ctDNA可检测到,其中88%(n = 7/8)的患者在维莫非尼开始使用后的第0天到第15天ctDNA浓度下降。随访期间,9例患者检测到ctDNA浓度升高:5例患者中,ctDNA浓度首次升高发生在维莫非尼浓度下降之后。更有趣的是,维莫非尼浓度与ctDNA浓度之间存在负相关(p = 0.026)。基线时的ctDNA浓度与总生存期相关(风险比 = 2.61,95% CI 1.04 - 6.56;p = 0.04)。
本研究证明了在转移性黑色素瘤患者随访期间监测维莫非尼血浆浓度的相关性。血浆药物监测和ctDNA浓度可结合起来监测接受抗BRAF治疗的黑色素瘤患者的肿瘤进展。
