Lu L, Shen R N, Zhou S Z, Srivastava C, Harrington M, Miyazawa K, Wu B, Lin Z H, Ruscetti S, Broxmeyer H E
Department of Medicine (Hematology/Oncology), Indiana University School of Medicine, Indianapolis 46202-5121.
Int J Hematol. 1991 Apr;54(2):117-24.
Mice infected with the polycythemia-inducing strain of the Friend virus complex (FVC-P) have been used as a leukemic mouse model. In the present study, purified iron-saturated human lactoferrin (LF) and recombinant murine (rmu) interferon-gamma (IFN-gamma), alone or in combination, were used to influence disease progression in virally infected mice. DBA/2 mice were injected i.v. with FVC-P, and were treated s.c. with 100 micrograms LF at day 7, and/or rmuIFN-gamma at 5 x 10(4) units/day for 3 days beginning at day 6 after viral infection. Mice were assessed for survival, and also 14 days after virus inoculation, the mice were killed and spleen extracts were assessed for spleen focus forming virus (SFFV) titers by spleen focus forming unit (SFFU) assay, SFFV mRNA and genomic DNA expression, and natural killer (NK) cell activity. Treatment with LF or rmuIFN-gamma alone had little or no effect on SFFU numbers or SFFV mRNA or genomic DNA expression. However, dramatically decreased SFFV titers and levels of SFFV mRNA and genomic DNA were observed in mice treated with the combination of LF and rmuIFN-gamma. NK cell activity decreased by FVC-P was returned to normal levels by LF and rmuIFN-gamma. The combined treatment also enhanced the survival rates of FVC-P-infected mice. The results suggest synergistic suppressive effects of LF with rmuIFN-gamma on disease progression in FVC-P-infected mice. This information might be of significance as a potential therapy for patients with leukemia and those infected with retroviruses.
感染了弗瑞德病毒复合体(FVC-P)的红细胞增多症诱导株的小鼠已被用作白血病小鼠模型。在本研究中,单独或联合使用纯化的铁饱和人乳铁蛋白(LF)和重组鼠(rmu)干扰素-γ(IFN-γ)来影响病毒感染小鼠的疾病进展。给DBA/2小鼠静脉注射FVC-P,并在病毒感染后第7天皮下注射100微克LF,和/或从病毒感染后第6天开始,以5×10⁴单位/天的剂量皮下注射rmuIFN-γ,持续3天。评估小鼠的存活率,并且在病毒接种后14天,处死小鼠,通过脾集落形成单位(SFFU)测定法评估脾提取物中的脾集落形成病毒(SFFV)滴度、SFFV mRNA和基因组DNA表达,以及自然杀伤(NK)细胞活性。单独用LF或rmuIFN-γ治疗对SFFU数量或SFFV mRNA或基因组DNA表达几乎没有影响。然而,在联合使用LF和rmuIFN-γ治疗的小鼠中,观察到SFFV滴度以及SFFV mRNA和基因组DNA水平显著降低。FVC-P导致降低的NK细胞活性通过LF和rmuIFN-γ恢复到正常水平。联合治疗还提高了FVC-P感染小鼠的存活率。结果表明LF与rmuIFN-γ对FVC-P感染小鼠疾病进展具有协同抑制作用。该信息作为白血病患者和逆转录病毒感染者的潜在治疗方法可能具有重要意义。
