Panel-based next-generation sequencing identifies prognostic and actionable genes in childhood acute lymphoblastic leukemia and is suitable for clinical sequencing

被引:8
作者
Ishida, Hisashi [1 ]
Iguchi, Akihiro [2 ]
Aoe, Michinori [3 ]
Takahashi, Takahide [3 ]
Tamefusa, Kosuke [1 ]
Kanamitsu, Kiichiro [1 ]
Fujiwara, Kaori [1 ]
Washio, Kana [1 ]
Matsubara, Takehiro [4 ]
Tsukahara, Hirokazu [1 ]
Sanada, Masashi [5 ]
Shimada, Akira [1 ]
机构
[1] Okayama Univ Hosp, Dept Pediat Pediat Hematol & Oncol, Kita Ku, 2-5-1 Shikatacho, Okayama 7008558, Japan
[2] Hokkaido Univ Hosp, Dept Pediat, Sapporo, Hokkaido, Japan
[3] Okayama Univ Hosp, Div Med Support, Okayama, Japan
[4] Okayama Univ Hosp, Dept BioBank, BioRepository BioMarker Anal Ctr, Okayama, Japan
[5] Natl Hosp Org, Nagoya Med Ctr, Clin Res Ctr, Nagoya, Aichi, Japan
关键词
Leukemia; Pediatric; ALL; Molecular genetics; Precision medicine; STEM-CELL TRANSPLANTATION; IKZF1; DELETION; JAPAN ASSOCIATION; GENOMIC LANDSCAPE; MEDICAL GENETICS; CREBBP MUTATIONS; AMERICAN-COLLEGE; 1ST RELAPSE; RISK; CHILDREN;
D O I
10.1007/s00277-018-3554-8
中图分类号
R5 [内科学];
学科分类号
1002 ; 100201 ;
摘要
Acute lymphoblastic leukemia (ALL) is the most common malignancy in children. Although the cure rate of ALL has greatly improved, a considerable number of patients suffer from relapse of leukemia. Therefore, ALL remains the leading cause of death from cancer during childhood. To improve the cure rate of these patients, precisely detecting patients with high risk of relapse and incorporating new targeted therapies are urgently needed. This study investigated inexpensive, rapid, next-generation sequencing of more than 150 cancer-related genes for matched diagnostic, remission, and relapse samples of 17 patients (3months to 15years old) with relapsed ALL. In this analysis, we identified 16 single-nucleotide variants (SNVs) and insertion/deletion variants and 19 copy number variants (CNVs) at diagnosis and 28 SNVs and insertion/deletion variants and 22 CNVs at relapse. With these genetic alterations, we could detect several B cell precursor ALL patients with high-risk gene alterations who were not stratified into the highest-risk group (5/8, 62.5%). We also detected potentially actionable genetic variants in about half of the patients (8/17, 47.1%). Among them, we found that one patient harbored germline TP53 mutation as a secondary finding. This inexpensive, rapid method can be immediately applied as clinical sequencing and could lead to better management of these patients and potential improvement in the survival rate in childhood ALL.
引用
收藏
页码:657 / 668
页数:12
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