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首页> 外文期刊>Transplantation: Official Journal of the Transplantation Society >In vivo bioluminescence imaging of transplanted islets and early detection of graft rejection.
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In vivo bioluminescence imaging of transplanted islets and early detection of graft rejection.

机译:胰岛的体内生物发光成像和移植物排斥的早期检测。

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摘要

BACKGROUND: Bioluminescence imaging (BLI) modalities are being developed to monitor islet transplant mass and function in vivo. The aim of this study was to use the BLI system to determine how the change in functional islet mass correlated to metabolic abnormalities during the course of alloimmune rejection in a murine transplant model. METHODS: Islets obtained from a transgenic mouse strain (FVB/NJ-luc) that constitutively expressed firefly luciferase were transplanted to various implantation sites of syngeneic wild-type FVB/NJ or allogeneic Balb/C streptozotocin-induced diabetic recipients. In vivo graft luminescent signals were repeatedly measured after transplantation using the BLI system and related to blood glucose levels and graft site histologic findings. RESULTS: The BLI signals were detected in as few as 10 islets implanted in the renal subcapsular space, intrahepatic, intraabdominal, and subcutaneous locations. There was a linear relationship between the number of islets transplanted and luminescence intensity. In isografts, stable luminescence intensity signals occurred within 2 weeks of transplantation and remained consistent on a long-term basis (18 months) after transplantation. In allografts, after normoglycemia was achieved and stable luminescence intensity occurred, graft bioluminescent intensity progressively decreased several days before permanent recurrence of hyperglycemia as a result of histologically proven rejection ensued. CONCLUSIONS: Bioluminescence imaging is a sensitive method for tracking the fate of islets after transplantation and is a useful method to detect early loss of functional islet mass caused by host immune responses even before overt metabolic dysfunction is evident. Bioluminescence imaging holds promise for use in designing and testing interventions to prolong islet graft survival.
机译:背景:正在开发生物发光成像(BLI)模式以监测胰岛移植的体内质量和功能。这项研究的目的是使用BLI系统确定在小鼠移植模型的同种免疫排斥反应过程中功能性胰岛质量的变化与代谢异常之间的关系。方法:将由组成型表达萤火虫荧光素酶的转基因小鼠品系(FVB / NJ-luc)获得的胰岛移植到同基因野生型FVB / NJ或同种异体Balb / C链脲佐菌素诱导的糖尿病受体的各个植入位点。移植后使用BLI系统反复测量体内移植物发光信号,并与血糖水平和移植部位组织学发现相关。结果:在植入肾下囊间隙,肝内,腹内和皮下位置的胰岛中仅检测到10个胰岛,就检测到BLI信号。胰岛移植的数目与发光强度之间存在线性关系。在同种异体移植物中,稳定的发光强度信号在移植后2周内发生,并在移植后的长期(18个月)内保持一致。在同种异体移植物中,达到正常血糖水平并出现稳定的发光强度后,由于组织学上证实的排斥反应,在高血糖永久性复发之前数天,移植物的生物发光强度逐渐降低。结论:生物发光成像是一种追踪移植后胰岛命运的灵敏方法,并且是检测宿主免疫反应引起的功能性胰岛早期丢失的有用方法,甚至可以在明显的代谢功能障碍未发现之前就进行检测。生物发光成像有望用于设计和测试干预措施以延长胰岛移植物的存活。

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