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首页> 外文期刊>Science Advances >The clonal repopulation of HSPC gene modified with anti–HIV-1 RNAi is not affected by preexisting HIV-1 infection
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The clonal repopulation of HSPC gene modified with anti–HIV-1 RNAi is not affected by preexisting HIV-1 infection

机译:用抗HIV-1 RNAi改性HSPC基因的克隆重新灌注不受预先存在的HIV-1感染的影响

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Despite advances in hematopoietic stem/progenitor cell (HSPC) transplant for HIV-1–infected patients, the impact of a preexisting HIV-1 infection on the engraftment and clonal repopulation of HSPCs remains poorly understood. We have developed a long terminal repeat indexing-mediated integration site sequencing (LTRi-Seq) method that provides a multiplexed clonal quantitation of both anti–HIV-1 RNAi (RNA interference) gene-modified and control vector-modified cell populations, together with HIV-1–infected cells—all within the same animal. In our HIV-1–preinfected humanized mice, both therapeutic and control HSPCs repopulated efficiently without abnormalities. Although the HIV-1–mediated selection of anti–HIV-1 RNAi-modified clones was evident in HIV-1–infected mice, the organ-to-organ and intra-organ clonal distributions in infected mice were indistinguishable from those in uninfected mice. HIV-1–infected cells showed clonal patterns distinct from those of HSPCs. Our data demonstrate that, despite the substantial impact of HIV-1 infection on CD4sup+/sup T cells, HSPC repopulation remains polyclonal, thus supporting the use of HSPC transplant for anti-HIV treatment.
机译:尽管造血茎/祖细胞(HSPC)移植对HIV-1感染的患者进行了进展,但预先存在的HIV-1感染对HSPCS的植入和克隆重新迁移的影响仍然很清楚。我们开发了一个长终端重复索引介导的集成站点测序(LTRI-SEQ)方法,提供抗HIV-1 RNAi(RNA干扰)基因改性和对照矢量改性细胞群的多路复用克隆定量。 HIV-1感染的细胞 - 全部在同一动物内。在我们的HIV-1-预先预留的人源化小鼠中,治疗和对照HSPCS有效地重新灌注,没有异常。虽然HIV-1介导的抗HIV-1 RNAI改性克隆的选择在HIV-1感染的小鼠中明显明显,但感染小鼠的器官与器官和器官克隆分布在未感染的小鼠中难以区分。 HIV-1感染的细胞显示出与Hspcs中不同的克隆模式。我们的数据表明,尽管HIV-1感染对CD4 + T细胞的显着影响,但HSPC refopulation仍然是多克隆的,因此支持HSPC移植用于抗HIV治疗的使用。

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