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Immune Activation: Contribution to AIDS-Associated Non-Hodgkin Lymphoma

机译:免疫激活:对艾滋病相关的非霍奇金淋巴瘤的贡献

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HIV infection is associated with a greatly elevated risk for the development of non-Hodgkin lymphoma (NHL), which while diminished, remains elevated in the highly active antiretroviral therapy (HAART) era. Chronic B cell activation, driven by contact with HIV virions, B cell-stimulatory cytokines, viruses (EBV, HPV, HCV), and by high levels of antigenic stimulation occurs in HIV infected persons, and it is seen at even higher levels in those who go on to develop AIDS-NHL. Evidence from multiple studies indicates that elevated serum levels of several B cell-stimulatory cytokines and biomarkers are seen preceding AIDS-NHL, as well as in immunocompetent persons that develop NHL. Phenotypic changes in circulating B cells also are seen preceding AIDS-NHL, including the expression of AICDA, and of cell-surface molecules and miRNA that are associated with activated B cells. HAART only partially normalizes the immune system of treated HIV+ persons as they still show clear evidence for ongoing inflammation and immune activation in, even those who show complete suppression of HIV viremia. Together, this provides ample evidence to support the notion that chronic activation of B cells contributes to the genesis of B cell lymphomas.
机译:HIV感染与非霍奇金淋巴瘤(NHL)发展的风险大大相关,虽然减少,但在高度活跃的抗逆转录病毒疗法(HAART)时代仍保持升高。慢性B细胞激活是由与HIV病毒体接触,B细胞刺激性细胞因子,病毒(EBV,HPV,HCV)驱动的,并且在HIV感染者中发生了高水平的抗原刺激,并且在这些抗原感染者中发生,并且在这些抗原感染者中发生,在这些抗原感染者中,在这些抗原感染者中,在这些抗原感染者中,在这些抗原感染者中,在这些抗原感染者中,在这些抗原感染者中,在这些抗原感染者中,在这些抗原感染者中,在这些抗原刺激中也可以在较高的水平中看到这些抗原刺激。继续开发艾滋病-NHL的人。来自多项研究的证据表明,在AIDS-NHL之前,还可以看到几种B细胞刺激性细胞因子和生物标志物的血清水平升高,以及发展NHL的免疫能力的人。在AIDS-NHL之前,还可以看到循环B细胞的表型变化,包括AICDA的表达,与活化B细胞相关的细胞表面分子和miRNA。 Haart仅部分将治疗的HIV+人的免疫系统归一化,因为他们仍然显示出明确的炎症和免疫激活的证据,即使是那些完全抑制HIV病毒血症的人。总之,这提供了充分的证据,以支持B细胞的慢性激活有助于B细胞淋巴瘤的发生。

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