Tufariello J M, Cho S, Horwitz M S
Department of Microbiology, Albert Einstein College of Medicine, Bronx, NY 10461.
Proc Natl Acad Sci U S A. 1994 Nov 8;91(23):10987-91. doi: 10.1073/pnas.91.23.10987.
The adenovirus (Ad) 14.7-kDa protein, which is called "14.7K," has been shown to function as a general inhibitor of tumor necrosis factor alpha (TNF) cytolysis in tissue culture assays, and the effect of this antagonism on viral pathogenesis in vivo has recently been explored. In infections of immunocompetent BALB/c mice, we have shown previously that Ad type 2 (Ad2) 14.7K, when cloned into a vaccinia virus (VV) vector in combination with the gene for murine TNF, is able to counteract much of the attenuating effect of TNF on VV virulence. In the present study we utilized VV constructs expressing various combinations of Ad 14.7K and TNF in infections of T- and B-cell-deficient C.B-17 severe combined immunodeficient (SCID) mice to determine whether these cells are directly necessary for 14.7K's reversal of TNF-mediated viral attenuation. The mice were infected by the intranasal route, and mortality, morbidity, histopathology, and virus replication in selected organs were evaluated at various times after infection. We found that, in the SCID murine pneumonia model, neither the attenuation by TNF nor its reversal by Ad 14.7K require the participation of T or B lymphocytes or their secreted products. SCID mice infected with VV expressing both 14.7K and TNF [VV 14.7(+)/TNF] were generally well clinically for the first 7-10 days after infection; however, they developed a subacute or chronic illness, succumbing to diseminated VV infection at least 3 weeks earlier than mice infected with VV expressing TNF alone [VV 14.7(-)/TNF]. Animals infected with VV 14.7(+)/TNF were shown to have higher initial titers of virus and delayed clearance from the lungs as well as more rapid spread of virus to internal organs than animals infected with VV 14.7(-)/TNF. SCID mice infected intranasally with VV without TNF showed a dramatic increase in acute disease and succumbed within the first 1-2 weeks after infection, independent of Ad 14.7K expression.
腺病毒(Ad)的14.7 kDa蛋白,即所谓的“14.7K”,在组织培养试验中已被证明可作为肿瘤坏死因子α(TNF)细胞溶解的一般抑制剂,并且最近已经探索了这种拮抗作用对体内病毒发病机制的影响。在免疫活性BALB/c小鼠的感染中,我们之前已经表明,当将Ad2 14.7K克隆到痘苗病毒(VV)载体中并与鼠TNF基因结合时,它能够抵消TNF对VV毒力的许多减弱作用。在本研究中,我们利用表达Ad 14.7K和TNF各种组合的VV构建体感染T细胞和B细胞缺陷的C.B-17严重联合免疫缺陷(SCID)小鼠,以确定这些细胞对于14.7K逆转TNF介导的病毒减弱是否直接必要。小鼠通过鼻内途径感染,并在感染后的不同时间评估死亡率、发病率、组织病理学以及选定器官中的病毒复制情况。我们发现,在SCID小鼠肺炎模型中,TNF的减弱作用及其被Ad 14.7K的逆转作用均不需要T淋巴细胞或B淋巴细胞或它们分泌的产物参与。感染表达14.7K和TNF的VV [VV 14.7(+)/TNF]的SCID小鼠在感染后的最初7 - 10天通常临床状况良好;然而,它们会发展为亚急性或慢性疾病,比单独感染表达TNF的VV [VV 14.7(-)/TNF]的小鼠至少提前3周死于播散性VV感染。与感染VV 14.7(-)/TNF的动物相比,感染VV 14.7(+)/TNF的动物显示出更高的初始病毒滴度、从肺部清除病毒的延迟以及病毒向内部器官的更快传播。经鼻内感染不含TNF的VV的SCID小鼠急性疾病显著增加,并在感染后的前1 - 2周内死亡,与Ad 14.7K的表达无关。
