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I 型干扰素的动力学和性别特异性反应的微异质性。

Microheterogeneity in the Kinetics and Sex-Specific Response to Type I IFN.

机构信息

Department of Life Sciences, Ben-Gurion University of the Negev, Beer-Sheva, Israel.

Department of Immunology, Blavatnik Institute, Harvard Medical School, Boston, MA.

出版信息

J Immunol. 2024 Jul 1;213(1):96-104. doi: 10.4049/jimmunol.2300453.

Abstract

The response to type I IFNs involves the rapid induction of prototypical IFN signature genes (ISGs). It is not known whether the tightly controlled ISG expression observed at the cell population level correctly represents the coherent responses of individual cells or whether it masks some heterogeneity in gene modules and/or responding cells. We performed a time-resolved single-cell analysis of the first 3 h after in vivo IFN stimulation in macrophages and CD4+ T and B lymphocytes from mice. All ISGs were generally induced in concert, with no clear cluster of faster- or slower-responding ISGs. Response kinetics differed between cell types: mostly homogeneous for macrophages, but with far more kinetic diversity among B and T lymphocytes, which included a distinct subset of nonresponsive cells. Velocity analysis confirmed the differences between macrophages in which the response progressed throughout the full 3 h, versus B and T lymphocytes in which it was rapidly curtailed by negative feedback and revealed differences in transcription rates between the lineages. In all cell types, female cells responded faster than their male counterparts. The ISG response thus seems to proceed as a homogeneous gene block, but with kinetics that vary between immune cell types and with sex differences that might underlie differential outcomes of viral infections.

摘要

I 型干扰素的反应涉及到典型 IFN 特征基因(ISGs)的快速诱导。目前尚不清楚在细胞群体水平上观察到的严格控制的 ISG 表达是否正确代表了单个细胞的一致反应,还是掩盖了基因模块和/或反应细胞的某些异质性。我们对来自小鼠的巨噬细胞和 CD4+T 和 B 淋巴细胞在体内 IFN 刺激后的头 3 小时进行了时间分辨的单细胞分析。所有的 ISGs 通常都协同诱导,没有明显的更快或更慢反应的 ISG 簇。细胞类型之间的反应动力学不同:巨噬细胞的反应大多是同质的,但 B 和 T 淋巴细胞的反应动力学多样性要大得多,其中包括一组明显的无反应细胞。速度分析证实了巨噬细胞之间的差异,在巨噬细胞中,反应在整个 3 小时内持续进行,而 B 和 T 淋巴细胞的反应则被负反馈迅速阻断,并揭示了不同谱系之间转录率的差异。在所有细胞类型中,雌性细胞的反应速度都比雄性细胞快。因此,ISG 反应似乎是作为一个同质的基因块进行的,但在免疫细胞类型之间的动力学有所不同,并且存在性别差异,这可能是病毒感染的不同结果的基础。

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