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首页> 外文期刊>Xenotransplantation >Pig peripheral blood mononuclear cells are directly associated with the thrombotic microangiopathy that complicates the induction of chimerism in pig-to-baboon xenotransplantation.
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Pig peripheral blood mononuclear cells are directly associated with the thrombotic microangiopathy that complicates the induction of chimerism in pig-to-baboon xenotransplantation.

机译:猪外周血单核细胞与血栓性微血管病变直接相关,血栓性微血管病变使猪到狒狒异种移植中嵌合现象的诱导复杂化。

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The infusion of large numbers of porcine cells into primates in order to induce specific immunologic tolerance by mixed hematopoietic chimerism, results in thrombotic microangiopathy that can be fatal. For this reason, it is important to study in vitro the interaction of primate endothelial cells with pig cells. We show that pig peripheral blood mononuclear cells (p-PBMC) activate human endothelial cells (hECs) through direct contact. Thus, when endothelial cells are cultured in the presence of p-PBMC, overexpression of VCAM-1 and E-selectin adhesion molecules occurs within 3 h of culture and continues for at least 9 h. The co-culture of p-PBMC and hECs also results in an important adhesion of human platelets to both types of cell. Thus, viewed with the microscope, platelets aggregate above the endothelial cells and also around the pig cells. We present data that suggest that the presence of p-PBMC may be more important with regard to the increase of platelet adhesion to the endothelial cells than the activation alone of the cells. Our results also show that p-PBMC, and not the activated endothelia or the culture supernatant of activated hECs, are able to activate the coagulation cascade because they are able to generate thrombin when added to defibrinated human plasma. Overall, these findings suggest that p-PBMC are of primary importance for the development of the thrombotic disorders that occur in primates transplanted with pig progenitor cells.
机译:为了通过混合的造血嵌合体诱导特异性的免疫耐受,向灵长类动物中注入大量的猪细胞会导致血栓性微血管病变,这可能是致命的。因此,重要的是在体外研究灵长类内皮细胞与猪细胞的相互作用。我们显示,猪外周血单个核细胞(p-PBMC)通过直接接触激活人内皮细胞(hECs)。因此,当在p-PBMC存在下培养内皮细胞时,VCAM-1和E-选择素粘附分子的过度表达会在培养的3小时内发生,并持续至少9小时。 p-PBMC和hEC的共培养还导致人血小板对两种类型细胞的重要粘附。因此,用显微镜观察,血小板在内皮细胞上方以及猪细胞周围聚集。我们提供的数据表明,p-PBMC的存在可能对血小板与内皮细胞粘附的增加比单独激活细胞更为重要。我们的结果还表明,p-PBMC而非活化的内皮细胞或活化的hECs的培养上清液能够活化凝血级联反应,因为当它们添加到去纤维化的人血浆中时,它们能够产生凝血酶。总体而言,这些发现表明,p-PBMC对于发生在移植有猪祖细胞的灵长类动物中发生的血栓形成疾病至关重要。

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