Functional analysis of the NUP98-CCDC28A fusion protein

PetitA.; RaguC.; SolerG.OttolenghiC.SchluthC.Radford-WeissI.Schneider-MaunouryS.CallebautI.DastugueN.DrabkinH.A.BernardO.A.RomanaS.Penard-LacroniqueV.

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Functional analysis of the NUP98-CCDC28A fusion protein

机译：NUP98-CCDC28A融合蛋白的功能分析

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Background The nucleoporin gene NUP98 is rearranged in more than 27 chromosomal abnormalities observed in childhood and adult, de novo and therapy-related acute leukemias of myeloid and T-lymphoid origins, resulting in the creation of fusion genes and the expression of chimeric proteins. We report here the functional analysis of the NUP98-coiled-coil domain-containing protein 28A (NUP98-CCDC28A) fusion protein, expressed as the consequence of a recurrent t(6;11)(q24.1;p15.5) translocation. Design and Methods To gain insight into the function of the native CCDC28A gene, we collected information on any differential expression of CCDC28A among normal hematologic cell types and within subgroups of acute leukemia. To assess the in vivo effects of the NUP98-CCDC28A fusion, NUP98- CCDC28A or full length CCDC28A were retrovirally transduced into primary murine bone marrow cells and transduced cells were next transplanted into sub-lethally irradiated recipient mice. Results Our in silico analyses supported a contribution of CCDC28A to discrete stages of murine hematopoietic development. They also suggested selective enrichment of CCDC28A in the French-American-British M6 class of human acute leukemia. Primary murine hematopoietic progenitor cells transduced with NUP98-CCDC28A generated a fully penetrant and transplantable myeloproliferative neoplasm-like myeloid leukemia and induced selective expansion of granulocyte/macrophage progenitors in the bone marrow of transplanted recipients, showing that NUP98-CCDC28A promotes the proliferative capacity and self-renewal potential of myeloid progenitors. In addition, the transformation mediated by NUP98-CCDC28A was not associated with deregulation of the Hoxa-Meis1 pathway, a feature shared by a diverse set of NUP98 fusions. Conclusions Our results demonstrate that the recurrent NUP98-CCDC28A is an oncogene that induces a rapid and transplantable myeloid neoplasm in recipient mice. They also provide additional evidence for an alternative leukemogenic mechanism for NUP98 oncogenes.

机译：背景核孔蛋白基因 NUP98 在儿童和成人、新发和治疗相关的髓系和 T 淋巴系起源的急性白血病中观察到的超过 27 种染色体异常中重排，导致融合基因的产生和嵌合蛋白的表达。我们在这里报告了 NUP98 卷曲螺旋结构域包含蛋白 28A （NUP98-CCDC28A）融合蛋白的功能分析，该蛋白表达为复发性 t（6;11）（Q24.1;p15.5）易位。设计和方法为了深入了解天然CCDC28A基因的功能，我们收集了有关正常血液细胞类型和急性白血病亚组内CCDC28A差异表达的信息。为了评估 NUP98-CCDC28A 融合的体内效应，将 NUP98 CCDC28A或全长CCDC28A逆病毒转导到原代小鼠骨髓细胞中，然后将转导细胞移植到亚致死性辐照的受体小鼠中。结果我们的计算机分析支持CCDC28A对小鼠造血发育的离散阶段的贡献。他们还建议选择性富集法美英M6类人类急性白血病的CCDC28A。用NUP98-CCDC28A转导的原代小鼠造血祖细胞产生完全渗透和可移植的骨髓增生性肿瘤样髓系白血病，并诱导移植受者骨髓中粒细胞/巨噬细胞祖细胞的选择性扩增，表明NUP98-CCDC28A促进了髓系祖细胞的增殖能力和自我更新潜力。此外，NUP98-CCDC28A介导的转化与Hoxa-Meis1通路的失调无关，Hoxa-Meis1通路是多种NUP98融合所共有的特征。结论结果表明，复发性NUP98-CCDC28A是一种癌基因，可诱导受体小鼠快速且可移植的髓系肿瘤。它们还为 NUP98 癌基因的替代白血病机制提供了额外的证据。

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《Haematologica》 |2012年第3期|379-387|共9页
作者
PetitA.; RaguC.; SolerG.OttolenghiC.SchluthC.Radford-WeissI.Schneider-MaunouryS.CallebautI.DastugueN.DrabkinH.A.BernardO.A.RomanaS.Penard-LacroniqueV.;
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作者单位

Assistance Publique-H?pitaux de Paris-AP-HP, Laboratoire d'Hématologie Biologique, H?pital Necker;

Laboratoire de Biologie du Développement, CNRS/Université Paris 6 UMR7622, Paris, France;

IMPMC-UMR7590, CNRS, Université Paris 6, Paris, FranceLaboratoire d'Hématologie, H?pital Purpan, Toulouse, FranceDivision of Hematology-Oncology, Medical University of South Carolina, Charleston, SC, United StatesINSERM U985, Institut Gustave Roussy, Villejuif, France, Université Paris Sud-11, Villejuif, FranceINSERM U985, Institut Gustave Roussy, Villejuif, France, AP-HP, Laboratoire de HistologieINSERM U985, Institut Gustave Roussy, Villejuif, France, Department d'Hématologie pédiatrique etINSERM U985, Institut Gustave Roussy, Villejuif, France, Center for Regenerative Medicine, HarvardINSERM U985, Institut Gustave Roussy, Villejuif, France, Université Paris Descartes, Paris, FranceINSERM U985, Institut Gustave Roussy, Villejuif, France;

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正文语种意大利语
中图分类血液及淋巴系疾病;
关键词
Mouse model; NUP98 fusions; T-ALL;

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Functional analysis of the NUP98-CCDC28A fusion protein

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