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鉴定血液和皮肤人类树突状细胞的谱系关系和新型标记物。

Identification of lineage relationships and novel markers of blood and skin human dendritic cells.

机构信息

Westmead Millennium Institute, Westmead, New South Wales 2145, Australia.

出版信息

J Immunol. 2013 Jan 1;190(1):66-79. doi: 10.4049/jimmunol.1200779. Epub 2012 Nov 26.

DOI:10.4049/jimmunol.1200779
PMID:23183897
Abstract

The lineage relationships and fate of human dendritic cells (DCs) have significance for a number of diseases including HIV where both blood and tissue DCs may be infected. We used gene expression profiling of human monocyte and DC subpopulations sorted directly from blood and skin to define the lineage relationships. We also compared these with monocyte-derived DCs (MDDCs) and MUTZ3 Langerhans cells (LCs) to investigate their relevance as model skin DCs. Hierarchical clustering analysis showed that myeloid DCs clustered according to anatomical origin rather than putative lineage. Plasmacytoid DCs formed the most discrete cluster, but ex vivo myeloid cells formed separate clusters of cells both in blood and in skin. Separate and specific DC populations could be determined within skin, and the proportion of CD14(+) dermal DCs (DDCs) was reduced and CD1a(+) DDCs increased during culture, suggesting conversion to CD1a(+)-expressing cells in situ. This is consistent with origin of the CD1a(+) DDCs from a local precursor rather than directly from circulating blood DCs or monocyte precursors. Consistent with their use as model skin DCs, the in vitro-derived MDDC and MUTZ3 LC populations grouped within the skin DC cluster. MDDCs clustered most closely to CD14(+) DDCs; furthermore, common unique patterns of C-type lectin receptor expression were identified between these two cell types. MUTZ3 LCs, however, did not cluster closely with ex vivo-derived LCs. We identified differential expression of novel genes in monocyte and DC subsets including genes related to DC surface receptors (including C-type lectin receptors, TLRs, and galectins).

摘要

人类树突状细胞 (DCs) 的谱系关系和命运对包括 HIV 在内的许多疾病具有重要意义,因为血液和组织中的 DC 都可能被感染。我们使用直接从血液和皮肤中分选的单核细胞和 DC 亚群的基因表达谱来定义谱系关系。我们还将其与单核细胞来源的树突状细胞 (MDDC) 和 MUTZ3 朗格汉斯细胞 (LC) 进行比较,以研究它们作为模型皮肤 DC 的相关性。层次聚类分析表明,髓系 DC 根据解剖起源而不是推测的谱系聚类。浆细胞样 DC 形成了最离散的簇,但在外周血和皮肤中的髓系细胞形成了独立的细胞簇。可以在皮肤内确定单独和特定的 DC 群体,并且 CD14(+) 真皮 DC (DDC) 的比例在培养过程中降低,CD1a(+) DDC 增加,表明在原位转化为表达 CD1a(+) 的细胞。这与 CD1a(+) DDC 来源于局部前体而不是直接来自循环血液 DC 或单核细胞前体的观点一致。与它们作为模型皮肤 DC 的用途一致,体外衍生的 MDDC 和 MUTZ3 LC 群体在皮肤 DC 簇内分组。MDDC 与 CD14(+) DDC 聚类最接近;此外,还在这两种细胞类型之间确定了 C 型凝集素受体表达的共同独特模式。然而,MUTZ3 LC 与体外衍生的 LC 聚类不密切。我们在单核细胞和 DC 亚群中鉴定了新型基因的差异表达,包括与 DC 表面受体相关的基因(包括 C 型凝集素受体、TLR 和半乳糖凝集素)。

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