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肢端雀斑样痣黑色素瘤在BRAF基因第15外显子中存在肿瘤内异质性,其突变不同于V600E/V600K。

Acral Lentiginous Melanomas Harbour Intratumor Heterogeneity in BRAF Exon 15, With Mutations Distinct From V600E/V600K.

作者信息

Fernandes Mariana, Barcelos Denise, Comodo Andréia Neves, Guimarães Daiane Pereira, Lopes Carapeto Fernando Cintra, Cardili Leonardo, de Sousa Morães Lais, Cerutti Ap Janete, Landman Ap Gilles

机构信息

Department of Pathology, Universidade Federal de São Paulo, São Paulo, Brazil.

Department of Morphology and Genetics, Federal University of São Paulo, São Paulo, Brazil.

出版信息

Am J Dermatopathol. 2019 Oct;41(10):733-740. doi: 10.1097/DAD.0000000000001418.

Abstract

The choice of appropriate therapeutic strategies may be influenced by intratumor heterogeneity and makes cancer treatment considerably more challenging. We aimed to evaluate the heterogeneity of BRAF exon 15 mutations in different areas of acral lentiginous melanoma (ALM). The entire exon 15 was sequenced in 4 different areas of paraffin-embedded samples from 26 patients with ALM. A total of 26 of 49 cases of ≥1 mm in depth of ALM identified by clinical, anatomical, and pathological data fulfilled the inclusion and exclusion criteria for this study. Tumors had a mean Breslow depth of 7.2 mm and an average mitotic index of 3 mitosis/mm. Mutations distinct from the common V600E and V600K were detected in 31%, and intratumor heterogeneity was observed in 31% of samples. Interestingly, 63.5% of all mutations had been previously associated with cancer. Most (62.5%) of the missense BRAF exon 15 mutations found in the ALM samples examined here were deemed "detrimental" for protein function according to at least 2 functional prediction programs, and 3 mutations (37.5%) were predicted to be "neutral," with no effect on protein function. BRAF exon 15 mutations were detected frequently in ALM and displayed heterogeneity, a finding to be further investigated.

摘要

合适治疗策略的选择可能受肿瘤内异质性影响,这使得癌症治疗更具挑战性。我们旨在评估肢端雀斑样痣黑素瘤(ALM)不同区域BRAF外显子15突变的异质性。对26例ALM患者石蜡包埋样本的4个不同区域进行了整个外显子15的测序。根据临床、解剖学和病理学数据确定的49例深度≥1mm的ALM病例中,共有26例符合本研究的纳入和排除标准。肿瘤的平均Breslow深度为7.2mm,平均有丝分裂指数为3个有丝分裂/mm。在31%的样本中检测到不同于常见V600E和V600K的突变,31%的样本观察到肿瘤内异质性。有趣的是,所有突变中有63.5%以前与癌症相关。根据至少2个功能预测程序,在此处检测的ALM样本中发现的大多数(62.5%)错义BRAF外显子15突变被认为对蛋白质功能“有害”,3个突变(37.5%)被预测为“中性”,对蛋白质功能无影响。BRAF外显子15突变在ALM中频繁检测到并表现出异质性,这一发现有待进一步研究。

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