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胎盘组织中的 Hofbauer 细胞通过诱导免疫调节细胞因子限制 HIV-1 的复制,并可能抵消母婴传播(MTCT)。

Placental Hofbauer cells limit HIV-1 replication and potentially offset mother to child transmission (MTCT) by induction of immunoregulatory cytokines.

机构信息

Department of Pediatrics and Children's Healthcare of Atlanta, Emory University, Atlanta, GA 30322, USA.

出版信息

Retrovirology. 2012 Dec 5;9:101. doi: 10.1186/1742-4690-9-101.

Abstract

BACKGROUND

Despite readily detectable levels of the HIV-1 (co)-receptors CD4, CCR5 and DC-SIGN on placental macrophages (Hofbauer Cells [HCs]), the rate of HIV-1 infection in utero in the absence of interventions is only 7% of exposed infants. Here, we examine the replication kinetics of human HCs to the primary isolate HIV-1BaL. We also determined the infectivity of HIV-1-exposed HCs by co-culturing with isolated cord and peripheral blood mononuclear cells [CBMCs, PBMCs]. To understand the limiting nature of HCs to HIV-1 replication, we examined the effect of endogenously secreted cytokines on replication kinetics.

RESULTS

HCs have reduced ability to replicate HIV-1 in vitro (p < 0.01) and to transmit virus to CBMCs and PBMCs (p < 0.001 for both) compared to standard infections of MDMs. HCs were shown to release HIV-1 particles at levels comparable to MDMs, however exhibit significant decreases in viral transcription (gag and env), which may account for lower levels of HIV-1 replication. Un-stimulated HCs constitutively express significantly higher levels of regulatory cytokines, IL-10 and TGF-β, compared to MDMs (p < 0.01), which may contribute to immunoregulatory predominance at the placenta and possibly account for down-regulation of HIV-1 replication and infectivity by HCs. We further demonstrate that these regulatory cytokines inhibit HIV-1 replication within HCs in vitro.

CONCLUSION

HCs have reduced ability to replicate and disseminate R5-tropic HIV-1BaLin vitro and potentially offset mother to child transmission (MTCT) of HIV-1 by the induction of immunoregulatory cytokines. Despite the potential for migration and infectivity, HCs are not present in the neighboring fetal circulation. These results implicate HCs as important mediators of protection at the feto-maternal interface during ongoing HIV-1 exposure.

摘要

背景

尽管胎盘巨噬细胞(Hofbauer 细胞[HCs])上可检测到 HIV-1(共)受体 CD4、CCR5 和 DC-SIGN 的水平,但在没有干预措施的情况下,宫内 HIV-1 感染的发生率仅为暴露婴儿的 7%。在这里,我们研究了人 HCs 对原发性 HIV-1BaL 分离株的复制动力学。我们还通过与分离的脐带和外周血单核细胞[CBMCs,PBMCs]共培养来确定 HIV-1 暴露的 HCs 的感染性。为了了解 HCs 对 HIV-1 复制的限制性质,我们研究了内源性分泌细胞因子对复制动力学的影响。

结果

与 MDM 的标准感染相比,HCs 在体外复制 HIV-1 的能力降低(p<0.01),并且向 CBMCs 和 PBMCs 传播病毒的能力也降低(两者均为 p<0.001)。HCs 释放 HIV-1 颗粒的水平与 MDMs 相当,但病毒转录(gag 和 env)显著下降,这可能导致 HIV-1 复制水平降低。与 MDMs 相比,未受刺激的 HCs 持续表达显著更高水平的调节细胞因子,IL-10 和 TGF-β(p<0.01),这可能有助于胎盘处的免疫调节优势,并可能解释 HCs 下调 HIV-1 复制和感染性的原因。我们进一步证明,这些调节细胞因子在体外抑制 HCs 中的 HIV-1 复制。

结论

HCs 在体外复制和传播 R5 嗜性 HIV-1BaL 的能力降低,并且通过诱导免疫调节细胞因子,可能抵消 HIV-1 的母婴传播(MTCT)。尽管存在迁移和感染性,但 HCs 不存在于邻近的胎儿循环中。这些结果表明 HCs 是在持续 HIV-1 暴露期间胎儿-母体界面保护的重要介质。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/47f0/3524025/3e8dbafd440d/1742-4690-9-101-1.jpg

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