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Human embryonic stem cell (hES) derived dendritic cells are functionally normal and are susceptible to HIV-1 infection

机译:人类胚胎干细胞(hES)衍生的树突状细胞功能正常,容易感染HIV-1

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Background Human embryonic stem (hES) cells hold considerable promise for cell replacement and gene therapies. Their remarkable properties of pluripotency, self-renewal, and tractability for genetic modification potentially allows for the production of sizeable quantities of therapeutic cells of the hematopoietic lineage. Dendritic cells (DC) arise from CD34+ hematopoietic progenitor cells (HPCs) and are important in many innate and adaptive immune functions. With respect to HIV-1 infection, DCs play an important role in the efficient capture and transfer of the virus to susceptible cells. With an aim of generating DCs from a renewable source for HIV-1 studies, here we evaluated the capacity of hES cell derived CD34+ cells to give rise to DCs which can support HIV-1 infection. Results Undifferentiated hES cells were cultured on S17 mouse bone marrow stromal cell layers to derive CD34+ HPCs which were subsequently grown in specific cytokine differentiation media to promote the development of DCs. The hES derived DCs (hES-DC) were subjected to phenotypic and functional analyses and compared with DCs derived from fetal liver CD34+ HPC (FL-DC). The mature hES-DCs displayed typical DC morphology consisting of veiled stellate cells. The hES-DCs also displayed characteristic phenotypic surface markers CD1a, HLA-DR, B7.1, B7.2, and DC-SIGN. The hES-DCs were found to be capable of antigen uptake and stimulating na?ve allogeneic CD4+ T cells in a mixed leukocyte reaction assay. Furthermore, the hES-DCs supported productive HIV-1 viral infection akin to standard DCs. Conclusion Phenotypically normal and functionally competent DCs that support HIV-1 infection can be derived from hES cells. hES-DCs can now be exploited in applied immunology and HIV-1 infection studies. Using gene therapy approaches, it is now possible to generate HIV-1 resistant DCs from anti-HIV gene transduced hES-CD34+ hematopoietic progenitor cells.
机译:背景技术人类胚胎干(hES)细胞在细胞替代和基因治疗方面具有广阔的前景。它们具有出色的多能性,自我更新和易于遗传修饰的特性,可潜在地产生相当数量的造血谱系治疗细胞。树突状细胞(DC)来自CD34 +造血祖细胞(HPC),在许多先天性和适应性免疫功能中起重要作用。关于HIV-1感染,DC在有效捕获病毒并将其转移到易感细胞中起重要作用。为了从可再生资源产生DC进行HIV-1研究,我们在这里评估了hES细胞衍生的CD34 +细胞产生可支持HIV-1感染的DC的能力。结果将未分化的hES细胞培养在S17小鼠骨髓基质细胞层上,得到CD34 + HPC,其随后在特定的细胞因子分化培养基中生长以促进DC的发育。对源自hES的DC(hES-DC)进行表型和功能分析,并与源自胎儿肝脏CD34 + HPC的DC(FL-DC)进行比较。成熟的hES-DC表现出典型的DC形态,由被遮盖的星状细胞组成。 hES-DC还显示了特征表型表面标记CD1a,HLA-DR,B7.1,B7.2和DC-SIGN。在混合白细胞反应试验中,发现hES-DCs能够吸收抗原并刺激幼稚的同种CD4 + T细胞。此外,hES-DC支持类似于标准DC的生产性HIV-1病毒感染。结论支持hvs-1感染的表型正常和功能正常的DC可以来自hES细胞。 hES-DCs现在可以用于应用免疫学和HIV-1感染研究。使用基因治疗方法,现在有可能从抗HIV基因转导的hES-CD34 +造血祖细胞中产生HIV-1抗性DC。

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