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BRAF抑制剂与IFNα联合应用于BRAF突变型黑色素瘤的抗肿瘤活性

Antitumor Activity of BRAF Inhibitor and IFNα Combination in BRAF-Mutant Melanoma.

作者信息

Sabbatino Francesco, Wang Yangyang, Scognamiglio Giosuè, Favoino Elvira, Feldman Steven A, Villani Vincenzo, Flaherty Keith T, Nota Sjoerd, Giannarelli Diana, Simeone Ester, Anniciello Anna M, Palmieri Giuseppe, Pepe Stefano, Botti Gerardo, Ascierto Paolo A, Ferrone Cristina R, Ferrone Soldano

出版信息

J Natl Cancer Inst. 2016 Feb 5;108(7). doi: 10.1093/jnci/djv435. Print 2016 Jul.

DOI:10.1093/jnci/djv435

PMID:26851802

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC4948304/

Abstract

BACKGROUND

BRAF(V600E)-mediated MAPK pathway activation is associated in melanoma cells with IFNAR1 downregulation. IFNAR1 regulates melanoma cell sensitivity to IFNα, a cytokine used for the adjuvant treatment of melanoma. These findings and the limited therapeutic efficacy of BRAF-I prompted us to examine whether the efficacy of IFNα therapy of BRAF(V600E) melanoma can be increased by its combination with BRAF-I.

METHODS

BRAF/NRAS genotype, ERK activation, IFNAR1, and HLA class I expression were tested in 60 primary melanoma tumors from treatment-naive patients. The effect of BRAF-I on IFNAR1 expression was assessed in three melanoma cell lines and in four biopsies of BRAF(V600E) metastases. The antiproliferative, pro-apoptotic and immunomodulatory activity of BRAF-I and IFNα combination was tested in vitro and in vivo utilizing three melanoma cell lines, HLA class I-MA peptide complex-specific T-cells and immunodeficient mice (5 per group for survival and 10 per group for tumor growth inhibition). All statistical tests were two-sided. Differences were considered statistically significant when the P value was less than .05.

RESULTS

The IFNAR1 level was statistically significantly (P < .001) lower in BRAF(V600E) primary melanoma tumors than in BRAF wild-type tumors. IFNAR1 downregulation was reversed by BRAF-I treatment in the three melanoma cell lines (P ≤ .02) and in three out of four metastases. The IFNAR1 level in the melanoma tumors analyzed was increased as early as 10 to 14 days following the beginning of the treatment. These changes were associated with: 1) an increased susceptibility in vitro of melanoma cells to the antiproliferative (P ≤ .04), pro-apoptotic (P ≤ .009) and immunomodulatory activity, including upregulation of HLA class I antigen APM component (P ≤ .04) and MA expression as well as recognition by cognate T-cells (P < .001), of BRAF-I and IFNα combination and 2) an increased survival (P < .001) and inhibition of tumor growth of melanoma cells (P < .001) in vivo by BRAF-I and IFNα combination.

CONCLUSIONS

The described results provide a strong rationale for the clinical trials implemented in BRAF(V600E) melanoma patients with BRAF-I and IFNα combination.

摘要

背景

BRAF（V600E）介导的MAPK通路激活在黑色素瘤细胞中与IFNAR1下调相关。IFNAR1调节黑色素瘤细胞对IFNα的敏感性，IFNα是一种用于黑色素瘤辅助治疗的细胞因子。这些发现以及BRAF抑制剂（BRAF-I）有限的治疗效果促使我们研究BRAF-I与IFNα联合使用是否能提高BRAF（V600E）黑色素瘤的IFNα治疗效果。

方法

对60例未经治疗的原发性黑色素瘤患者的肿瘤进行BRAF/NRAS基因型、ERK激活、IFNAR1和HLA I类表达检测。在三种黑色素瘤细胞系和四例BRAF（V600E）转移灶活检中评估BRAF-I对IFNAR1表达的影响。利用三种黑色素瘤细胞系、HLA I类-MA肽复合物特异性T细胞和免疫缺陷小鼠（每组5只用于生存实验，每组10只用于肿瘤生长抑制实验）在体外和体内测试BRAF-I与IFNα联合使用的抗增殖、促凋亡和免疫调节活性。所有统计检验均为双侧检验。当P值小于0.05时，差异被认为具有统计学意义。

结果

BRAF（V600E）原发性黑色素瘤肿瘤中的IFNAR1水平在统计学上显著低于BRAF野生型肿瘤（P < 0.001）。在三种黑色素瘤细胞系（P ≤ 0.02）和四例转移灶中的三例中，BRAF-I治疗可逆转IFNAR1下调。在治疗开始后10至14天，分析的黑色素瘤肿瘤中的IFNAR1水平即升高。这些变化与以下情况相关：1）黑色素瘤细胞在体外对BRAF-I与IFNα联合使用的抗增殖（P ≤ 0.04）、促凋亡（P ≤ 0.009）和免疫调节活性的敏感性增加，包括HLA I类抗原APM成分上调（P ≤ 0.04）和MA表达以及同源T细胞识别（P < 0.001）；2）BRAF-I与IFNα联合使用在体内可提高黑色素瘤细胞的生存率（P < 0.001）并抑制肿瘤生长（P < 0.001）。

结论

上述结果为在BRAF（V600E）黑色素瘤患者中开展BRAF-I与IFNα联合使用的临床试验提供了有力依据。

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BRAF抑制剂与IFNα联合应用于BRAF突变型黑色素瘤的抗肿瘤活性

Antitumor Activity of BRAF Inhibitor and IFNα Combination in BRAF-Mutant Melanoma.

作者信息

出版信息

BACKGROUND

METHODS

RESULTS

CONCLUSIONS

背景

方法

结果

结论

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