Eo S K, Kumaraguru U, Rouse B T
Laboratory of Viral Immunology, Department of Microbiology, University of Tennessee, Knoxville, TN 37996, USA.
J Immunol. 2001 Oct 1;167(7):3592-9. doi: 10.4049/jimmunol.167.7.3592.
Lymphotoxin alpha-deficient (LTalpha-/-) mice, which lack lymph nodes and possess a disorganized spleen, develop dysfunctional CD8+ T cells upon HSV infection and readily succumb to herpes encephalitis. Such mice do develop apparently normal peptide-specific CD8+ T cell responses, as measured by MHC class I tetramer staining, but the majority of cells fail to become cytotoxic or express peptide-induced IFN-gamma production. In the present study, we demonstrate that functional defects of CD8+ T cells in LTalpha-/- mice can be largely rectified by the administration of plasmid DNA encoding CCR7 ligands before HSV infection. Treated mutant mice developed increased peptide-specific cytotoxic responses, enhanced numbers of CD8+ T cells capable of producing IFN-gamma, as well as improved resistance to HSV challenge. The corrective effect of chemokine treatment appeared to result from improved dendritic cell-mediated Ag presentation. Thus, a major consequence of the treatment was an increase in splenic dendritic cell number in CCR7 ligand-treated LTalpha-/- mice with such splenocyte populations showing improved APC activity in vitro. Our results document that functional defects of CD8+ T cells can be corrected, and indicate the value of plasmid vector encoding appropriate chemokines to achieve such immunotherapy.
缺乏淋巴结且脾脏结构紊乱的淋巴毒素α缺陷(LTα-/-)小鼠,在感染单纯疱疹病毒(HSV)后会产生功能失调的CD8+ T细胞,并易患疱疹性脑炎。通过MHC I类四聚体染色测量,此类小鼠确实会产生明显正常的肽特异性CD8+ T细胞反应,但大多数细胞无法成为细胞毒性细胞或表达肽诱导的γ干扰素产生。在本研究中,我们证明,在HSV感染前给予编码CCR7配体的质粒DNA,可在很大程度上纠正LTα-/-小鼠中CD8+ T细胞的功能缺陷。经治疗的突变小鼠产生了增强的肽特异性细胞毒性反应,能够产生γ干扰素的CD8+ T细胞数量增加,并且对HSV攻击的抵抗力也有所提高。趋化因子治疗的纠正作用似乎源于树突状细胞介导的抗原呈递的改善。因此,治疗的一个主要结果是CCR7配体治疗的LTα-/-小鼠脾脏树突状细胞数量增加,此类脾细胞群体在体外显示出改善的抗原呈递细胞活性。我们的结果证明CD8+ T细胞的功能缺陷可以得到纠正,并表明编码适当趋化因子的质粒载体在实现这种免疫治疗方面的价值。
