内毒素对疣、低γ球蛋白血症、感染和骨髓疏松综合征模型小鼠的临床和血液学影响。

Shamik Majumdar, Ji-Liang Gao, Sergio M Pontejo, Karl Balabanian, Françoise Bachelerie, Philip M Murphy
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引用次数: 0

摘要

疣、低γ球蛋白血症、感染和骨髓增生症(WHIM)综合征免疫缺陷是由常染色体显性功能获得性CXCR4突变引起的,该突变可促进由成熟白细胞骨髓滞留引起的严重泛白细胞减少症。因此,WHIM患者会出现反复的细菌感染;然而,败血症并不常见。为了研究这种临床二分法,我们用LPS刺激WHIM模型小鼠。WHIM和野生型(WT)小鼠的LD50相似,LPS诱导的WT小鼠急性淋巴细胞减少是不依赖于Cxcr4的。相比之下,在WHIM小鼠中,LPS不影响循环T细胞水平,但B细胞水平异常增加,这是由于选择性的、细胞内在的和Cxcr4 WHIM等位基因依赖性的Cxcr4高晚期前B细胞的出现,这种模式被大肠杆菌感染所复制。在WT和WHIM小鼠中,CXCR4拮抗剂AMD3100迅速增加循环淋巴细胞水平,然后在随后的LPS处理后迅速收缩。因此,LPS诱导的淋巴细胞减少与CXCR4无关,WHIM突变不会增加临床LPS敏感性。异常WT不依赖于Cxcr4,但Cxcr4依赖于whad, LPS对晚期b前细胞动员的促进作用揭示了变体受体的独特信号通路。
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Clinical and Hematologic Effects of Endotoxin in Warts, Hypogammaglobulinemia, Infections, and Myelokathexis Syndrome Model Mice.

Warts, hypogammaglobulinemia, infections, and myelokathexis (WHIM) syndrome immunodeficiency is caused by autosomal dominant gain-of-function CXCR4 mutations that promote severe panleukopenia caused by bone marrow retention of mature leukocytes. Consequently, WHIM patients develop recurrent bacterial infections; however, sepsis is uncommon. To study this clinical dichotomy, we challenged WHIM model mice with LPS. The LD50 was similar in WHIM and wild-type (WT) mice, and LPS induced acute lymphopenia in WT mice that was Cxcr4 independent. In contrast, in WHIM mice, LPS did not affect circulating T cell levels, but the B cell levels anomalously increased because of selective, cell-intrinsic, and Cxcr4 WHIM allele-dependent emergence of Cxcr4high late pre-B cells, a pattern that was phenocopied by Escherichia coli infection. In both WT and WHIM mice, the CXCR4 antagonist AMD3100 rapidly increased circulating lymphocyte levels that then rapidly contracted after subsequent LPS treatment. Thus, LPS-induced lymphopenia is CXCR4 independent, and a WHIM mutation does not increase clinical LPS sensitivity. Anomalous WT Cxcr4-independent, but Cxcr4 WHIM-dependent, promobilizing effects of LPS on late pre-B cell mobilization reveal a distinct signaling pathway for the variant receptor.

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