Hoatlin M E, Kozak S L, Lilly F, Chakraborti A, Kozak C A, Kabat D
Department of Biochemistry and Molecular Biology, Oregon Health Sciences University, Portland 97201-3098.
Proc Natl Acad Sci U S A. 1990 Dec;87(24):9985-9. doi: 10.1073/pnas.87.24.9985.
The leukemogenic membrane glycoprotein (gp55) encoded by Friend spleen focus-forming virus appears to bind to erythropoietin receptors (EpoR) sto stimulate erythroblastosis [Li, J.-P., D'Andrea, A.D., Lodish, H.F. & Baltimore, D. (1990) Nature (London) 343, 762-764]. To directly compare the effects of gp55 with erythropoietin (Epo), we produced retrovirions that encode either gp55, Epo, or EpoR. After infection with EpoR virus, interleukin 3-dependent DA-3 cells bound 125I-labeled Epo and grew without interleukin 3 in the presence of Epo. These latter cells, but not parental DA-3 cells, became factor-independent after superinfection either with Epo virus or with Friend spleen focus-forming virus. In addition, Epo virus caused a disease in mice that mimicked Friend erythroleukemia. Although Fv-2r homozygotes are susceptible to all other retroviral diseases, they are resistant to both Epo viral and Friend viral erythroleukemias. These results indicate that both gp55 and Epo stimulate EpoR and that the Fv-2 gene encodes a protein that controls response to these ligands. However, the Fv-2 protein is not EpoR because the corresponding genes map to opposite ends of mouse chromosome 9. These results have important implications for understanding signal transduction by EpoR and the role of host genetic variation in controlling susceptibility to an oncogenic protein.
弗瑞德脾脏集落形成病毒编码的致白血病膜糖蛋白(gp55)似乎能与促红细胞生成素受体(EpoR)结合,从而刺激成红细胞增多症[李,J.-P.,丹德利亚,A.D.,洛迪什,H.F. & 巴尔的摩,D.(1990年)《自然》(伦敦)343,762 - 764]。为了直接比较gp55与促红细胞生成素(Epo)的作用,我们制备了编码gp55、Epo或EpoR的逆转录病毒颗粒。用EpoR病毒感染后,依赖白细胞介素3的DA - 3细胞结合了125I标记的Epo,并在有Epo存在的情况下无需白细胞介素3就能生长。这些细胞,而非亲本DA - 3细胞,在用Epo病毒或弗瑞德脾脏集落形成病毒再次感染后变得不依赖因子。此外,Epo病毒在小鼠中引发了一种类似于弗瑞德红细胞白血病的疾病。尽管Fv - 2r纯合子对所有其他逆转录病毒疾病敏感,但它们对Epo病毒和弗瑞德病毒引起的红细胞白血病均有抗性。这些结果表明,gp55和Epo都能刺激EpoR,且Fv - 2基因编码一种控制对这些配体反应的蛋白质。然而,Fv - 2蛋白不是EpoR,因为相应基因定位于小鼠9号染色体的两端。这些结果对于理解EpoR的信号转导以及宿主基因变异在控制对致癌蛋白易感性中的作用具有重要意义。