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Allergen-induced fluctuation in CC chemokine receptor 3 expression on bone marrow CD34+ cells from asthmatic subjects: significance for mobilization of haemopoietic progenitor cells in allergic inflammation

机译：变应原诱导哮喘受试者骨髓CD34 +细胞CC趋化因子受体3表达的波动：在过敏性炎症中动员造血祖细胞的意义

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There is increasing evidence that primitive progenitors migrate from the bone marrow (BM) via the peripheral circulation to tissue sites where they undergo in situ differentiation to provide a continued source of effector cells, such as eosinophils, during an allergic inflammatory response. To study mechanisms of progenitor cell mobilization in allergic reactions, we investigated fluctuations in the expression of the eotaxin receptor, CC chemokine receptor 3 (CCR3), on CD34⁺ cells from stable asthmatics following allergen (i.e. antigen) challenge. BM aspirates were taken from seven early responder (ER) and 10 dual responder (DR) asthmatics who, following antigen challenge developed only an early bronchoconstrictor response and an early and late- bronchoconstrictor response, respectively. Expression of CCR3 was detected on primitive (CD34⁺ cells) and eosinophil-lineage committed progenitors (CD34⁺ interleukin-5 receptor alpha-subunit⁺ cells) by flow cytometry and confirmed by co-localization of CCR3 messenger RNA to CD34 immunopositive cells using in situ hybridization. When preantigen levels were compared to 24-hr postantigen levels, significant increases in BM CD34⁺ CCR3⁺ cells were detected in DR, who also developed a significant sputum and blood eosinophilia and increased methacholine airway responsiveness. In contrast, a significant attenuation of BM CD34⁺ CCR3⁺ cells was observed in ER. In a dose-dependent manner eotaxin, but not interleukin (IL)-5, stimulated CD34⁺ progenitor cell migration in vitro. This migrational response to eotaxin was abrogated by anti-CCR3 monoclonal antibody and primed by preincubation with IL-5. We propose that fluctuations in CCR3 expression on human BM CD34⁺ cells may facilitate chemokine-mediated progenitor cell mobilization to the peripheral circulation and the resultant development of pulmonary eosinophilia, a cardinal feature of asthma.

机译：越来越多的证据表明原始祖细胞通过外周循环从骨髓（BM）迁移到组织部位，在过敏性炎症反应过程中，它们会原位分化以提供效应细胞（如嗜酸性粒细胞）的持续来源。为了研究在过敏反应中祖细胞动员的机制，我们研究了过敏原（即抗原）后稳定哮喘患者CD34 ^{+ 细胞上嗜酸性粒细胞趋化因子受体CC趋化因子受体3（CCR3）表达的变化。挑战。 BM抽吸物是从7名早期反应者（ER）和10位双重反应者（DR）的哮喘患者中抽取的，他们在抗原攻击后分别分别产生了早期的支气管收缩反应和早期和晚期的支气管收缩反应。在原始细胞（CD34 ^{+ ）和嗜酸性粒细胞定型祖细胞（CD34 ^{+ interleukin-5 receptor alpha-subunit ^{+ ）上检测到CCR3的表达。细胞）通过流式细胞仪检测，并通过原位杂交将CCR3信使RNA与CD34免疫阳性细胞共定位。当将抗原前水平与抗原后24小时水平进行比较时，在DR中检测到BM CD34 ^{+ CCR3 ^{+ 细胞的显着增加，他们也出现了明显的痰液和血液嗜酸性粒细胞增多和乙酰甲胆碱气道反应性增强。相反，在ER中观察到BM CD34 ^{+ CCR3 ^{+ 细胞的显着衰减。嗜酸细胞活化趋化因子以剂量依赖的方式刺激CD34 ^{+ 祖细胞的体外迁移，但不是白介素（IL）-5。通过抗CCR3单克隆抗体消除了对嗜酸性粒细胞趋化因子的迁移反应，并通过与IL-5预温育进行了预激。我们认为，人BM CD34 ^{+ 细胞上CCR3表达的波动可能促进趋化因子介导的祖细胞动员至外周循环，并由此导致肺嗜酸性粒细胞增多，这是哮喘的主要特征。}}}}}}}}}}

著录项

期刊名称 Immunology
作者
Roma Sehmi; Sandra Dorman; Adrian Baatjes; Rick Watson; Ronan Foley; Sun Ying; Douglas S Robinson; A Barry Kay; Paul M OByrne; Judah A Denburg;
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作者单位

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年(卷),期 2003(109),4
年度 2003
页码 536–546
总页数 11
原文格式 PDF
正文语种
中图分类免疫学;
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专利

1. Expression of stromal cell-derived factor-1/pre-B cell growth-stimulating factor receptor, CXC chemokine receptor 4, on CD34+ human bone marrow cells is a phenotypic alteration for committed lymphoid progenitors. [J] . Ishii T, Nishihara M, Ma F, The Journal of Immunology: Official Journal of the American Association of Immunologists . 1999,第7期

机译：CD34 +人骨髓细胞上基质细胞衍生因子-1 /前B细胞生长刺激因子受体CXC趋化因子受体4的表达是定型淋巴祖细胞的表型改变。
2. Expression of Stromal Cell-Derived Factor-1/Pre-B Cell Growth-Stimulating Factor Receptor, CXC Chemokine Receptor 4, on CD34+ Human Bone Marrow Cells Is a Phenotypic Alteration for Committed Lymphoid Progenitors [J] . Takefumi Ishii, Masamichi Nishihara, Feng Ma, The journal of immunology . 1999,第7期

机译：基质细胞衍生因子-1 /前B细胞生长刺激因子受体，CXC趋化因子受体4在CD34 +人骨髓细胞上的表达是所致淋巴祖细胞的表型改变。
3. Treatment with anti-CC chemokine receptor 3 monoclonal antibody or dexamethasone inhibits the migration and differentiation of bone marrow CD34 progenitor cells in an allergic mouse model. [J] . Ben S, Li X, Xu F, Allergy . 2008,第9期

机译：用抗CC趋化因子受体3单克隆抗体或地塞米松治疗可抑制变态小鼠模型中骨髓CD34祖细胞的迁移和分化。
4. Estrogen Receptor Expression Profile of Disseminated Epithelial Tumor Cells in Bone Marrow of Breast Cancer Patients [C] . Nina Ditsch, Michaela Rolle, Michael Untch, International Meeting on Molecular Staging on Cancer . 2003

机译：乳腺癌患者骨髓中散发性上皮细胞雌激素受体表达谱
5. Beta-Adrenergic Receptor Mediated Transcriptional Dysregulation in Hematopoietic Stem and Progenitor Cells Leads to Bone Marrow Erythroid Suppression in Multiple Myeloma Patients - ex vivo Investigations [D] . Subramaniam, Vimal. 2021

机译：β-肾上腺素能受体介导的造血干细胞和祖细胞中的转录失调导致多发性骨髓瘤患者的骨髓红细胞抑制 - 以外的研究
6. Allergen-induced increases in IL-5 receptor alpha-subunit expression on bone marrow-derived CD34+ cells from asthmatic subjects. A novel marker of progenitor cell commitment towards eosinophilic differentiation. [O] . R Sehmi, L J Wood, R Watson, 1997

机译：过敏原诱导的哮喘受试者骨髓来源的CD34 +细胞上IL-5受体α亚基表达的增加。祖细胞致力于嗜酸性细胞分化的新标记。
7. Allergen-induced fluctuation in CC chemokine receptor 3 expression on bone marrow CD34+ cells from asthmatic subjects: significance for mobilization of haemopoietic progenitor cells in allergic inflammation [O] . Sehmi, Roma, Dorman, Sandra, Baatjes, Adrian, 2003

机译：变应原诱导哮喘受试者骨髓CD34 +细胞CC趋化因子受体3表达的波动：在过敏性炎症中动员造血祖细胞的意义

Allergen-induced fluctuation in CC chemokine receptor 3 expression on bone marrow CD34+ cells from asthmatic subjects: significance for mobilization of haemopoietic progenitor cells in allergic inflammation

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