MYCN is a novel oncogenic target in pediatric T-cell Acute Lymphoblastic Leukemia

被引：25

作者：

Astolfi, Annalisa ^{[1
,2
]}

Vendemini, Francesca ^{[2
]}

Urbini, Milena ^{[1
,2
]}

Melchionda, Fraia ^{[2
]}

Masetti, Riccardo ^{[2
]}

Franzoni, Monica ^{[2
]}

Libri, Virginia ^{[2
]}

Serravalle, Salvatore ^{[2
]}

Togni, Marco ^{[2
]}

Paone, Giuseppina ^{[2
]}

Montemurro, Luca ^{[2
]}

Bressanin, Daniela ^{[3
]}

Chiarini, Francesca ^{[4
]}

Martelli, Alberto M. ^{[3
]}

Tonelli, Roberto ^{[5
]}

Pession, Andrea ^{[1
,2
]}

机构：

[1] Univ Bologna, Giorgio Prodi Canc Res Ctr, Bologna, Italy

[2] Univ Bologna, S Orsola Malpighi Hosp, Pediat Oncol & Hematol Unit Lalla Seragnoli, Bologna, Italy

[3] Univ Bologna, Dept Biomed & Neuromotor Sci, Bologna, Italy

[4] Natl Res Council IOR, Inst Mol Genet, Bologna, Italy

[5] Univ Bologna, Dept Pharm & Biotechnol, Bologna, Italy

来源：

ONCOTARGET | 2014年 / 5卷 / 01期

关键词：

pediatric T-ALL; MYCN; peptide nucleic acid; TAL1; HUMAN NEUROBLASTOMA-CELLS; PEPTIDE NUCLEIC-ACID; N-MYC; C-MYC; GENE-EXPRESSION; COPY-NUMBER; INHIBITION; NOTCH1; DNA; RHABDOMYOSARCOMAS;

D O I：

10.18632/oncotarget.1337

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

MYCN is an oncogene frequently overexpressed in pediatric solid tumors whereas few evidences suggest his involvement in the pathogenesis of haematologic malignancies. Here we show that MYCN is overexpressed in a relevant proportion (40 to 50%) of adult and pediatric T-cell acute lymphoblastic leukemias (T-ALL). Focusing on pediatric T-ALL, MYCN-expressing samples were found almost exclusively in the TAL1-positive subgroup. Moreover, TAL1 knockdown in T-ALL cell lines resulted in a reduction of MYCN expression, and TAL1 directly binds to MYCN promoter region, suggesting that TAL1 pathway activation could sustain the up-regulation of MYCN. The role of MYCN in T-ALL was investigated by peptide nucleic acid (PNA-MYCN)-mediated transcriptional silencing of MYCN and by siRNAs. MYCN knockdown in T-ALL cell lines resulted in a reduction of cell viability, up to 50%, while no effect was elicited with a mismatch PNA. The inhibitory effect of PNA-MYCN on cell viability was due to a significant increase in apoptosis. PNA-MYCN treatment in pediatric T-ALL samples reduced cell viability of leukemic cells from patients with high MYCN expression, while no effect was obtained in MYCN-negative blast cells. These results showed that MYCN is frequently overexpressed in pediatric T-ALL and suggested his role as a candidate for molecularly-directed therapies.

引用

页码：120 / 130

页数：11

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