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CD200 表达标记人类 AML 中的白血病干细胞。

CD200 expression marks leukemia stem cells in human AML.

机构信息

Princess Margaret Cancer Centre, University Health Network, Toronto, ON, Canada.

Department of Medicine, Schulich School of Medicine and Dentistry, Western University, London, ON, Canada.

出版信息

Blood Adv. 2020 Nov 10;4(21):5402-5413. doi: 10.1182/bloodadvances.2020001802.

Abstract

The leukemia stem cell (LSC) populations of acute myeloid leukemia (AML) exhibit phenotypic, genetic, and functional heterogeneity that contribute to therapy failure and relapse. Progress toward understanding the mechanistic basis for therapy resistance in LSCs has been hampered by difficulties in isolating cell fractions that enrich for the entire heterogeneous population of LSCs within individual AML samples. We previously reported that CD200 gene expression is upregulated in LSC-containing AML fractions. Here, we show that CD200 is present on a greater proportion of CD45dim blasts compared with more differentiated CD45high cells in AML patient samples. In 75% (49 of 65) of AML cases we examined, CD200 was expressed on ≥10% of CD45dim blasts; of these, CD200 identified LSCs within the blast population in 9 of 10 (90%) samples tested in xenotransplantation assays. CD200+ LSCs could be isolated from CD200+ normal HSCs with the use of additional markers. Notably, CD200 expression captured both CD34- and CD34+ LSCs within individual AML samples. Analysis of highly purified CD200+ LSC-containing fractions from NPM1-mutated AMLs, which are commonly CD34-, exhibited an enrichment of primitive gene expression signatures compared with unfractionated cells. Overall, our findings support CD200 as a novel LSC marker that is able to capture the entire LSC compartment from AML patient samples, including those with NPM1 mutation.

摘要

急性髓系白血病 (AML) 的白血病干细胞 (LSC) 群体表现出表型、遗传和功能异质性,这导致了治疗失败和复发。尽管在理解 LSCs 治疗耐药的机制基础方面取得了一些进展,但由于难以从单个 AML 样本中分离出富含整个 LSC 异质群体的细胞分数,这一进展受到了阻碍。我们之前报道过 CD200 基因表达在含 LSC 的 AML 分数中上调。在这里,我们表明 CD200 存在于 AML 患者样本中比分化程度更高的 CD45high 细胞更多的 CD45dim blasts 上。在我们检查的 75%(65 例中的 49 例)AML 病例中,CD200 在≥10%的 CD45dim blast 上表达;在 10 个接受异种移植试验的样本中,其中 9 个(90%)中 CD200 鉴定了 blast 群体中的 LSCs。可以使用额外的标记物从 CD200+正常 HSCs 中分离出 CD200+ LSCs。值得注意的是,CD200 表达在单个 AML 样本中捕获了 CD34-和 CD34+ LSCs。对富含 NPM1 突变的 AML 中高度纯化的 CD200+ LSC 包含分数的分析表明,与未分级细胞相比,原始基因表达特征得到了富集。总的来说,我们的研究结果支持 CD200 作为一种新的 LSC 标志物,能够从 AML 患者样本中捕获整个 LSC 区室,包括那些具有 NPM1 突变的样本。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5fcb/7656934/a05c58611924/advancesADV2020001802absf1.jpg

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