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多参数流式细胞术分析人脾在研究患者血浆来源 EVs 中的应用。

Multiparameter Flow Cytometry Analysis of the Human Spleen Applied to Studies of Plasma-Derived EVs From Patients.

机构信息

ISGlobal, Hospital Clinic - Universitat de Barcelona, Barcelona, Spain.

IGTP: Germans Trias i Pujol Research Institute, Barcelona, Spain.

出版信息

Front Cell Infect Microbiol. 2021 Mar 1;11:596104. doi: 10.3389/fcimb.2021.596104. eCollection 2021.

Abstract

The spleen is a secondary lymphoid organ with multiple functions including the removal of senescent red blood cells and the coordination of immune responses against blood-borne pathogens, such as malaria parasites. Despite the major role of the spleen, the study of its function in humans is limited by ethical implications to access human tissues. Here, we employed multiparameter flow cytometry combined with cell purification techniques to determine human spleen cell populations from transplantation donors. Spleen immuno-phenotyping showed that CD45 cells included B (30%), CD4 T (16%), CD8 T (10%), NK (6%) and NKT (2%) lymphocytes. Myeloid cells comprised neutrophils (16%), monocytes (2%) and DCs (0.3%). Erythrocytes represented 70%, reticulocytes 0.7% and hematopoietic stem cells 0.02%. Extracellular vesicles (EVs) are membrane-bound nanoparticles involved in intercellular communication and secreted by almost all cell types. EVs play several roles in malaria that range from modulation of immune responses to vascular alterations. To investigate interactions of plasma-derived EVs from Plasmodium vivax infected patients (PvEVs) with human spleen cells, we used size-exclusion chromatography (SEC) to separate EVs from the bulk of soluble plasma proteins and stained isolated EVs with fluorescent lipophilic dyes. The integrated cellular analysis of the human spleen and the methodology employed here allowed in vitro interaction studies of human spleen cells and EVs that showed an increased proportion of T cells (CD4+ 3 fold and CD8+ 4 fold), monocytes (1.51 fold), B cells (2.3 fold) and erythrocytes (3 fold) interacting with PvEVs as compared to plasma-derived EVs from healthy volunteers (hEVs). Future functional studies of these interactions can contribute to unveil pathophysiological processes involving the spleen in vivax malaria.

摘要

脾脏是一个具有多种功能的次级淋巴器官,包括清除衰老的红细胞和协调针对血液传播病原体(如疟原虫)的免疫反应。尽管脾脏具有重要作用,但由于获取人类组织涉及伦理问题,其功能在人类中的研究受到限制。在这里,我们采用多参数流式细胞术结合细胞纯化技术,从移植供体中确定人类脾脏细胞群体。脾脏免疫表型显示 CD45 细胞包括 B(30%)、CD4 T(16%)、CD8 T(10%)、NK(6%)和 NKT(2%)淋巴细胞。髓样细胞包括中性粒细胞(16%)、单核细胞(2%)和 DC(0.3%)。红细胞占 70%,网织红细胞占 0.7%,造血干细胞占 0.02%。细胞外囊泡(EVs)是参与细胞间通讯的膜结合纳米颗粒,几乎所有细胞类型都能分泌 EVs。EVs 在疟疾中发挥多种作用,从调节免疫反应到血管改变。为了研究来自间日疟原虫感染患者的血浆衍生 EVs(PvEVs)与人脾脏细胞的相互作用,我们使用分子筛层析(SEC)将 EVs 与大量可溶性血浆蛋白分离,并使用荧光亲脂性染料对分离的 EVs 进行染色。这里使用的人类脾脏综合细胞分析和方法学允许进行人脾脏细胞和 EVs 的体外相互作用研究,结果显示与来自健康志愿者的血浆衍生 EVs(hEVs)相比,与 PvEVs 相互作用的 T 细胞(CD4+增加 3 倍,CD8+增加 4 倍)、单核细胞(增加 1.51 倍)、B 细胞(增加 2.3 倍)和红细胞(增加 3 倍)的比例增加。这些相互作用的未来功能研究可以有助于揭示间日疟原虫感染中涉及脾脏的病理生理过程。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/afd7/7957050/dcbeb036cdb4/fcimb-11-596104-g001.jpg

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