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卡波西样血管内皮瘤的外显子序列分析:推定驱动突变的鉴定

Exome sequence analysis of Kaposiform hemangioendothelioma: identification of putative driver mutations.

作者信息

Egashira Sho, Jinnin Masatoshi, Harada Miho, Masuguchi Shinichi, Fukushima Satoshi, Ihn Hironobu

机构信息

Faculty of Life Sciences, Kumamoto University - Kumamoto, Japan.

出版信息

An Bras Dermatol. 2016 Nov-Dec;91(6):748-753. doi: 10.1590/abd1806-4841.20165026.

Abstract

BACKGROUND

: Kaposiform hemangioendothelioma is a rare, intermediate, malignant tumor. The tumor's etiology remains unknown and there are no specific treatments.

OBJECTIVE

: In this study, we performed exome sequencing using DNA from a Kaposiform hemangioendothelioma patient, and found putative candidates for the responsible mutations.

METHOD

: The genomic DNA for exome sequencing was obtained from the tumor tissue and matched normal tissue from the same individual. Exome sequencing was performed on HiSeq2000 sequencer platform.

RESULTS

: Among oncogenes, germline missense single nucleotide variants were observed in the TP53 and APC genes in both the tumor and normal tissue. As tumor-specific somatic mutations, we identified 81 candidate genes, including 4 nonsense changes, 68 missense changes and 9 insertions/deletions. The mutations in ITGB2, IL-32 and DIDO1 were included in them.

CONCLUSION

: This is a pilot study, and future analysis with more patients is needed to clarify: the detailed pathogenesis of this tumor, the novel diagnostic methods by detecting specific mutations, and the new therapeutic strategies targeting the mutation.

摘要

背景

卡波西样血管内皮瘤是一种罕见的、中间型恶性肿瘤。该肿瘤的病因尚不清楚,且没有特异性治疗方法。

目的

在本研究中,我们使用一名卡波西样血管内皮瘤患者的DNA进行外显子组测序,发现了可能的致病突变候选基因。

方法

用于外显子组测序的基因组DNA取自肿瘤组织以及同一患者的配对正常组织。外显子组测序在HiSeq2000测序平台上进行。

结果

在癌基因中,肿瘤组织和正常组织的TP53和APC基因均存在种系错义单核苷酸变异。作为肿瘤特异性体细胞突变,我们鉴定出81个候选基因,包括4个无义突变、68个错义突变和9个插入/缺失突变。其中包括ITGB2、IL-32和DIDO1基因的突变。

结论

这是一项初步研究,需要对更多患者进行进一步分析,以阐明:该肿瘤的详细发病机制、通过检测特定突变的新型诊断方法以及针对该突变的新治疗策略。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4276/5193184/f52e9d89ab56/abd-91-06-0748-g01.jpg

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