Djordjevic P B, Lalic N, Bumbasirevic V, Jotic A, Paunovic I, Colovic R, Lalic K, Raketic N, Nikolic D, Zamaklar M, Rajkovic N, Lukic L J, Dimitrijevic-Sreckovic V, Dragasevic M, Popovic S, Gostiljac D, Canovic F, Markovic I
Institut for Endocrinology, Diabetes, and Metabolic Diseases, Belgrade, Serbia and Montenegro.
Transplant Proc. 2005 Dec;37(10):4440-5. doi: 10.1016/j.transproceed.2005.10.050.
Previous studies have suggested that the multiple transplants might be equally metabolically efficient to a single regimen for human adult islets. The aim of this study was to compare immunological and metabolic parameters after each of the two regimens of human fetal islets (HFI). Group A single transplants (n = 9) had 180 +/- 20 x 1000 HFI equivalents (IEQs) implanted via a single intramuscular injection. In group B multiple transplants (n = 8) islets were implanted by three consecutive injections of 60 +/- 10 x 1000 IEQs at 7-day intervals. We analyzed the immunological parameters of CD4/CD8 T lymphocyte ratios; islet cell antibodies (ICAs) and insulin antibodies (IAs). We estimated insulin secreting capacity (ISC) as the metabolic parameter. We observed that the CD4+/CD8+ T-cell ratio increased, peaking on day 90, in similar fashion in both groups: day -1: A = 1.18 +/- 0.03 versus B = 1.19 +/- 0.04; on day 90: A = 1.79 +/- 0.09, versus B = 1.75 +/- 0.08 (P = NS) immediately before the decrease in C-peptide levels. Thereafter the ratios rapidly decreased without statistical differences. The levels of ICAs did not change. The levels of IAs, which were increased before transplant, then decreased without statistical differences between the groups. The values of ISC increased after transplant and then decreased similar to the T-cell ratio. Our results demonstrated that regimens of multiple and single HFIs did not show differences in the kinetics of the immunological response presumably mediating graft destruction. The CD4/CD8 ratio increased as the C-peptide level decreased, peaking on day 90 at the time of a decrease in C-peptide. These results may be useful for clinical studies of HFIs for type 1 diabetic patients.
先前的研究表明,对于成人胰岛移植,多次移植在代谢效率上可能与单次移植方案相当。本研究的目的是比较两种人胎儿胰岛(HFI)移植方案后的免疫和代谢参数。A组单次移植(n = 9)通过单次肌肉注射植入180±20×1000个HFI等效物(IEQs)。B组多次移植(n = 8)通过每隔7天连续三次注射60±10×1000个IEQs来植入胰岛。我们分析了CD4/CD8 T淋巴细胞比率、胰岛细胞抗体(ICA)和胰岛素抗体(IA)的免疫参数。我们将胰岛素分泌能力(ISC)作为代谢参数进行评估。我们观察到,两组中CD4+/CD8+ T细胞比率均升高,在第90天达到峰值,且方式相似:第-1天:A组=1.18±0.03,B组=1.19±0.04;第90天:紧接C肽水平下降之前,A组=1.79±0.09,B组=1.75±0.08(P=无显著性差异)。此后,该比率迅速下降,无统计学差异。ICA水平未发生变化。移植前升高的IA水平随后下降,两组间无统计学差异。ISC值在移植后升高,然后与T细胞比率类似地下降。我们的结果表明,多次和单次HFI移植方案在可能介导移植物破坏的免疫反应动力学方面未显示出差异。CD4/CD8比率随着C肽水平下降而升高,在C肽下降时的第90天达到峰值。这些结果可能对1型糖尿病患者的HFI临床研究有用。
