目的探讨艾滋病相关淋巴结病中浆细胞的变化与艾滋病患者机体免疫和病理发展变化的关系。方法采用免疫组织化学法检测10例艾滋病相关淋巴结病患者淋巴结组织中CD138、CD21、Ki-67的表达情况。结果 (1)艾滋病相关淋巴结病中,CD138+浆细胞在淋巴结各区域广泛表达,HIV+组高于HIV-组(P0.05)。(2)CD138+浆细胞在艾滋病相关淋巴结病各个时期呈倒"V"字形发展变化过程。(3)艾滋病相关淋巴结病中CD138+浆细胞数与CD4数呈显著负相关(r=-0.77,P=0.009)。(4)在艾滋病相关淋巴结病中有5%的CD138+浆细胞表达Ki-67。结论浆细胞与艾滋病相关淋巴结病的发生发展密切相关。

We have tracked the in vivo migration and have identified in vivo correlates of cytotoxic T-lymphocyte (CTL) activity in HIV-seropositive subjects infused with autologous gene-marked CD8+ HIV-specific CTL. The number of circulating gene-marked CTL ranged from 1.6 to 3.5% shortly after infusion to less than 0.5% 2 weeks later. Gene-marked CTL were present in the lymph node at 4.5- to 11-fold excess and colocalized within parafollicular regions of the lymph node adjacent to cells expressing HIV tat fusion transcripts, a correlate of virus replication. The CTL clones expressed the CCR5 receptor and localized among HIV-infected cells expressing the ligands MIP-1α and MIP-1β, CC-chemokines produced at sites of virus replication. Aggregates of apoptotic cells and cells expressing granzyme-B localized within these same sites. In contrast, lymph node sections from untreated HIV-seropositive subjects, all with significant viral burden (> 50,000 HIV RNA copies/mL plasma), showed no CC-chemokine expression and exhibited only sporadic and randomly distributed cells expressing granzymes and/or apoptotic cells. These studies show that the infused CTL specifically migrate to sites of HIV replication and retain their antigen-specific cytolytic potential. Moreover, these studies provide a methodology that will facilitate studies of both the magnitude and functional phenotype of Ag-specific CD8+ T cells in vivo.