Pollock J L, Westervelt P, Kurichety A K, Pelicci P G, Grisolano J L, Ley T J
Washington University School of Medicine, Division of Bone Marrow Transplantation, Department of Internal Medicine, St. Louis, MO 63110, USA.
Proc Natl Acad Sci U S A. 1999 Dec 21;96(26):15103-8. doi: 10.1073/pnas.96.26.15103.
Acute promyelocytic leukemia (APML) most often is associated with the balanced reciprocal translocation t(15;17) (q22;q11.2) and the expression of both the PML-RARalpha and RARalpha-PML fusion cDNAs that are formed by this translocation. In this report, we investigated the biological role of a bcr-3 isoform of RARalpha-PML for the development of APML in a transgenic mouse model. Expression of RARalpha-PML alone in the early myeloid cells of transgenic mice did not alter myeloid development or cause APML, but its expression significantly increased the penetrance of APML in mice expressing a bcr-1 isoform of PML-RARalpha (15% of animals developed APML with PML-RARalpha alone vs. 57% with both transgenes, P < 0.001). The latency of APML development was not altered substantially by the expression of RARalpha-PML, suggesting that it does not behave as a classical "second hit" for development of the disease. Leukemias that arose from doubly transgenic mice were less mature than those from PML-RARalpha transgenic mice, but they both responded to all-trans retinoic acid in vitro. These findings suggest that PML-RARalpha drives the development of APML and defines its basic phenotype, whereas RARalpha-PML potentiates this phenotype via mechanisms that are not yet understood.
急性早幼粒细胞白血病(APML)最常与平衡的相互易位t(15;17) (q22;q11.2)以及由该易位形成的PML-RARα和RARα-PML融合cDNA的表达相关。在本报告中,我们在转基因小鼠模型中研究了RARα-PML的一种bcr-3亚型在APML发生发展中的生物学作用。单独在转基因小鼠的早期髓系细胞中表达RARα-PML并不会改变髓系发育或导致APML,但它的表达显著增加了在表达PML-RARα的bcr-1亚型的小鼠中APML的发生率(仅表达PML-RARα时15%的动物发生APML,而同时表达两个转基因时为57%,P < 0.001)。RARα-PML的表达并未显著改变APML发生的潜伏期,这表明它在该疾病的发生中并非作为经典的“二次打击”。来自双转基因小鼠的白血病比来自PML-RARα转基因小鼠的白血病成熟度更低,但它们在体外对全反式维甲酸均有反应。这些发现表明,PML-RARα驱动APML的发生并定义其基本表型,而RARα-PML通过尚未明确的机制增强了这种表型。