Rejection of human islets and human HLA-A2.1 transgenic mouse islets by alloreactive human lymphocytes in immunodeficient NOD-scid and NOD-Rag1(null)Prf1(null) mice.

Banuelos SJ; Shultz LD; Greiner DL; Burzenski LM; Gott B; Lyons BL; Rossini AA; Appel MC

首页> 外文期刊>Clinical immunology: The official journal of the Clinical Immunology Society >Rejection of human islets and human HLA-A2.1 transgenic mouse islets by alloreactive human lymphocytes in immunodeficient NOD-scid and NOD-Rag1(null)Prf1(null) mice.

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Rejection of human islets and human HLA-A2.1 transgenic mouse islets by alloreactive human lymphocytes in immunodeficient NOD-scid and NOD-Rag1(null)Prf1(null) mice.

机译：免疫缺陷的NOD-scid和NOD-Rag1（null）Prf1（null）小鼠中的同种反应性人淋巴细胞排斥人胰岛和人HLA-A2.1转基因小鼠胰岛。

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Immunodeficient NOD mice engrafted with human peripheral blood mononuclear cells (PBMCs) were used in two models of human islet allograft rejection. Model one: human PBMCs were engrafted into chemically diabetic NOD-scid mice bearing established subrenal human islet allografts. Inflammation and often complete islet allograft rejection were observed. Model 2 incorporated three key advances. First, we developed a new immunodeficient recipient, NOD-RagI(null)Prf1(null) mice. Second, graft-lymphocyte interactions were optimized by intrasplenic co-transplantation of islets and human PBMC. Third, NOD-scid islets expressing human HLA-A2.1 were used as allograft targets. Diabetic NOD-RagI(null)Prf1(null) recipients of HLA-A2.1 transgenic mouse islets, alone or co-engrafted with HLA-A2-positive human PBMC, exhibited durable graft survival and euglycemia. Contrastingly, co-transplantation with HLA-A2-negative human PBMC led to islet graft rejection without evidence of graft-vs.-host disease (GVHD). We propose that diabetic NOD-RagI(null)Prf1(null) mice co-engrafted with HLA-A2 mouse transgenic islets and allogeneic human PBMC provide an effective in vivo model of human islet allograft rejection.

机译：植入了人类外周血单核细胞（PBMC）的免疫缺陷NOD小鼠被用于两种人类胰岛同种异体移植排斥模型。模型一：将人PBMCs移植入带有已建立的肾下人胰岛的同种异体的化学性糖尿病NOD-scid小鼠中。观察到炎症和经常完全胰岛排斥反应。模型2包含了三个主要方面。首先，我们开发了一种新的免疫缺陷受体，NOD-RagI（null）Prf1（null）小鼠。其次，通过胰岛和人PBMC的脾内共移植来优化移植物-淋巴细胞的相互作用。第三，将表达人HLA-A2.1的NOD-scid胰岛用作同种异体移植靶。单独或与HLA-A2阳性人类PBMC共移植的HLA-A2.1转基因小鼠胰岛的糖尿病NOD-RagI（无效）Prf1（无效）受体表现出持久的移植物存活率和血糖正常。相反，与HLA-A2阴性的人PBMC共移植导致胰岛移植排斥反应，而没有移植物抗宿主病（GVHD）的证据。我们建议与HLA-A2小鼠转基因胰岛和同种异体人类PBMC共移植的糖尿病NOD-RagI（null）Prf1（null）小鼠提供了有效的体内人类胰岛异体移植排斥模型。

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《Clinical immunology: The official journal of the Clinical Immunology Society》 |2004年第3期|共11页
作者
Banuelos SJ; Shultz LD; Greiner DL; Burzenski LM; Gott B; Lyons BL; Rossini AA; Appel MC;
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正文语种 eng
中图分类临床医学;
关键词
Human; NOD; Laboratory mice; Allografting; Homologous Grafts;

机译：人;NOD;实验室小鼠;同种异体移植;同源移植;

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1. Rejection of human islets and human HLA-A2.1 transgenic mouse islets by alloreactive human lymphocytes in immunodeficient NOD-scid and NOD-Rag1(null)Prf1(null) mice. [J] . Banuelos SJ, Shultz LD, Greiner DL, Clinical immunology: The official journal of the Clinical Immunology Society . 2004,第3期

机译：免疫缺陷的NOD-scid和NOD-Rag1（null）Prf1（null）小鼠中的同种反应性人淋巴细胞排斥人胰岛和人HLA-A2.1转基因小鼠胰岛。
2. Human Immune System Development and Rejection of Human Islet Allografts in Spontaneously Diabetic NOD-Rag1~(null) IL2rγ~(null) Ins2~(Akita)Mice [J] . Michael A. Brehm, Rita Bortell, Philip dilorio, Diabetes . 2010,第9期

机译：自发性糖尿病NOD-Rag1〜（null）IL2rγ〜（null）Ins2〜（Akita）小鼠的人体免疫系统发育和同种异体移植排斥反应
3. Alloimmune Injury and Rejection of Human Skin Grafts on Human Peripheral Blood Lymphocyte-Reconstituted Non-Obese Diabetic Severe Combined Immunodeficient beta(2)-Microglobulin-Null Mice. [J] . Turgeon NA, Banuelos SJ, Shultz LD, Experimental Biology and Medicine: Journal of the Society for Experimental Biology and Medicine . 2003,第9期

机译：同种异体免疫损伤和人类皮肤移植对人外周血淋巴细胞重构的非肥胖糖尿病严重联合免疫缺陷的β（2）-微球蛋白-空小鼠的排斥反应。
4. Inhibition of Human Islet Amyloid Polypeptide Aggregation and Membrane Damage in β-Islet Celt Mimics [C] . Brenan Wilson, Deborah L. Heyl American Peptide Symposium . 2011

机译：β-islet Celt模拟中的人胰岛淀粉样蛋白多肽聚集和膜损伤的抑制作用
5. Tumor-specific human primary T cells engineered to overexpress IL-2, IL-7, IL-15, or IL-21 confer varying degrees of tumor rejection and xenogeneic graft-versus-host disease in an immunodeficient mouse model. [D] . Markley, John Charles. 2009

机译：经过工程改造以过度表达IL-2，IL-7，IL-15或IL-21的肿瘤特异性人类原代T细胞可在免疫缺陷小鼠模型中赋予不同程度的肿瘤排斥反应和异种移植物抗宿主病。
6. Correction: Ex Vivo Expanded Human Regulatory T Cells Delay Islet Allograft Rejection via Inhibiting Islet-Derived Monocyte Chemoattractant Protein-1 Production in CD34+ Stem Cells-Reconstituted NOD-scid IL2rγnull Mice [O] . -1

机译：更正：体内扩增的人类调节性T细胞通过抑制CD34 +干细胞重构的NOD-scidIL2rγnull小鼠中胰岛来源的单核细胞趋化蛋白1的产生来延迟胰岛同种异体移植的排斥反应。
7. Ex vivo expanded human regulatory T cells delay islet allograft rejection via inhibiting islet-derived monocyte chemoattractant protein-1 production in CD34+ stem cells-reconstituted NOD-scid IL2rγnull mice. [O] . Fang Xiao, Liang Ma, Min Zhao, 2014

机译：离体扩增的人调节性T细胞通过抑制CD34 +干细胞重构的NOD-scidIL2rγnull小鼠中的胰岛衍生的单核细胞趋化蛋白-1产生来延迟胰岛同种异体移植排斥。

Rejection of human islets and human HLA-A2.1 transgenic mouse islets by alloreactive human lymphocytes in immunodeficient NOD-scid and NOD-Rag1(null)Prf1(null) mice.

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