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金丝雀痘病毒(ALVAC)和痘苗病毒嗜性的比较分析显示,ALVAC对单核细胞系人类细胞具有更受限且更具偏好性的嗜性。

Comparative analysis of tropism between canarypox (ALVAC) and vaccinia viruses reveals a more restricted and preferential tropism of ALVAC for human cells of the monocytic lineage.

作者信息

Yu Qigui, Jones Brad, Hu Ningjie, Chang Hong, Ahmad Sidrah, Liu Jun, Parrington Mark, Ostrowski Mario

机构信息

Hawaii AIDS Clinical Research Program, Department of Medicine, University of Hawaii at Manoa, Honolulu, HI, USA.

出版信息

Vaccine. 2006 Sep 29;24(40-41):6376-91. doi: 10.1016/j.vaccine.2006.06.011. Epub 2006 Jun 30.

Abstract

The poxviruses including canarypox (ALVAC) and vaccinia viruses are promising vaccine vectors in humans, but little is known about their biology in human cells. Using recombinant enhanced green fluorescence protein (EGFP)-expressing ALVAC and vaccinia viruses, we have focused here on a side-by-side comparison of ALVAC and vaccinia virus tropism for cells from human peripheral blood and bone marrow. Both ALVAC and vaccinia viruses showed a strong bias towards monocyte infection. ALVAC minimally infected CD19+ B cells and was unable to infect ex vivo NK cells and T lymphocytes, whereas vaccinia virus could infect B lymphocytes and NK cell populations. Vaccinia virus was also able to infect T lymphocytes at low, but detectable levels that could be enhanced upon their activation. The observed preferential infection of ALVAC or vaccinia virus to monocytes was the result of preferential binding to this population, rather than lineage-specific differences in the expression of viral genes. Moreover, the level of CD14 expression on monocytes correlated with their preference to be infected with ALVAC or vaccinia virus. Both ALVAC and vaccinia viruses could infect immature monocyte derived dendritic cells (MDDCs), but only ALVAC infection induced their subsequent maturation. Vaccinia virus, however, showed greater tropism for mature MDDCs compared to ALVAC. Infection in human bone marrow cultures showed that ALVAC infection was restricted to a myelomonocytoid cell-specific CD33(+) cell population, while vaccinia virus showed a strong, but not exclusive, preference for these cells. These findings have implications in terms of choosing optimal pox virus derived vectors as vaccines in terms of reducing clinical reactogenicity and inducing dendritic cell (DC) maturation.

摘要

包括金丝雀痘病毒(ALVAC)和痘苗病毒在内的痘病毒是很有前景的人类疫苗载体,但人们对它们在人类细胞中的生物学特性了解甚少。我们使用表达重组增强型绿色荧光蛋白(EGFP)的ALVAC和痘苗病毒,在此重点对ALVAC和痘苗病毒对人外周血和骨髓细胞的嗜性进行了并列比较。ALVAC和痘苗病毒都表现出对单核细胞感染的强烈偏好。ALVAC极少感染CD19+ B细胞,且无法感染离体NK细胞和T淋巴细胞,而痘苗病毒能够感染B淋巴细胞和NK细胞群体。痘苗病毒也能够以较低但可检测到的水平感染T淋巴细胞,且在T淋巴细胞激活后感染水平会增强。观察到的ALVAC或痘苗病毒对单核细胞的优先感染是优先结合该群体的结果,而非病毒基因表达上的谱系特异性差异。此外,单核细胞上CD14的表达水平与其被ALVAC或痘苗病毒感染的偏好相关。ALVAC和痘苗病毒都能够感染未成熟的单核细胞衍生树突状细胞(MDDC),但只有ALVAC感染会诱导其随后成熟。然而,与ALVAC相比,痘苗病毒对成熟MDDC表现出更强的嗜性。在人骨髓培养物中的感染显示,ALVAC感染局限于骨髓单核细胞样细胞特异性的CD33(+)细胞群体,而痘苗病毒对这些细胞表现出强烈但并非排他性的偏好。这些发现对于选择最佳的痘病毒衍生载体作为疫苗以降低临床反应原性和诱导树突状细胞(DC)成熟具有重要意义。

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