Reinders Marlies E J, Bank Jonna R, Dreyer Geertje J, Roelofs Helene, Heidt Sebastian, Roelen Dave L, Al Huurman Volkert, Lindeman Jan, van Kooten Cees, Claas Frans H J, Fibbe Wim E, Rabelink Ton J, de Fijter Johan W
J Transl Med. 2014 Dec 10;12:331. doi: 10.1186/s12967-014-0331-x.
Kidney transplantation has improved survival and quality of life for patients with end-stage renal disease. Despite excellent short-term results due to better and more potent immunosuppressive drugs, long-term survival of transplanted kidneys has not improved accordingly in the last decades. Consequently there is a strong interest in immunosuppressive regimens that maintain efficacy for the prevention of rejection, whilst preserving renal structure and function. In this respect the infusion of mesenchymal stromal cells (MSCs) may be an interesting immune suppressive strategy. MSCs have immune suppressive properties and actively contribute to tissue repair. In experimental animal studies the combination of mammalian target of rapamycin (mTOR) inhibitor and MSCs was shown to attenuate allo immune responses and to promote allograft tolerance. The current study will test the hypothesis that MSC treatment, in combination with the mTOR inhibitor everolimus, facilitates tacrolimus withdrawal, reduces fibrosis and decreases the incidence of opportunistic infections compared to standard tacrolimus dose.
METHODS/DESIGN: 70 renal allograft recipients, 18-75 years old, will be included in this Phase II, open label, randomized, non-blinded, prospective, single centre clinical study. Patients in the MSC treated group will receive two doses of autologous bone marrow derived MSCs IV (target 1,5 x 10(6), Range 1-2 x 10(6) million MSCs per/kg body weight), 7 days apart, 6 and 7 weeks transplantation in combination with everolimus and prednisolone. At the time of the second MSC infusion tacrolimus will be reduced to 50% and completely withdrawn 1 week later. Patients in the control group will receive everolimus, prednisolone and standard dose tacrolimus. The primary end point is to compare fibrosis by quantitative Sirius Red scoring of MSC treated and untreated groups at 6 months compared to 4 weeks post-transplant. Secondary end points include: composite end point efficacy failure (Biopsy Proven Acute Rejection, graft loss or death); renal function and proteinuria; opportunistic infections; immune monitoring and "subclinical" cardiovascular disease groups by assessing echocardiography in the different treatment groups.
This study will provide information whether MSCs in combination with everolimus can be used for tacrolimus withdrawal, and whether this strategy leads to preservation of renal structure and function in renal recipients.
NCT02057965.
肾移植改善了终末期肾病患者的生存率和生活质量。尽管由于更好、更强效的免疫抑制药物带来了出色的短期效果,但在过去几十年中,移植肾的长期存活率并未相应提高。因此,人们对既能维持预防排斥反应的疗效,又能保护肾脏结构和功能的免疫抑制方案有着浓厚兴趣。在这方面,间充质基质细胞(MSC)的输注可能是一种有趣的免疫抑制策略。MSC具有免疫抑制特性,并积极参与组织修复。在实验动物研究中,雷帕霉素靶蛋白(mTOR)抑制剂与MSC的联合使用显示可减轻同种异体免疫反应并促进同种异体移植耐受。本研究将检验以下假设:与标准他克莫司剂量相比,MSC治疗联合mTOR抑制剂依维莫司可促进他克莫司撤减、减少纤维化并降低机会性感染的发生率。
方法/设计:本II期、开放标签、随机、非盲、前瞻性、单中心临床研究将纳入70名年龄在18至75岁之间的肾移植受者。MSC治疗组的患者将接受两剂静脉注射的自体骨髓来源的MSC(目标剂量为每千克体重1.5×10⁶,范围为1至2×10⁶个MSC),间隔7天,在移植后6周和7周时与依维莫司和泼尼松龙联合使用。在第二次输注MSC时,他克莫司将减至50%,并在1周后完全停用。对照组的患者将接受依维莫司、泼尼松龙和标准剂量的他克莫司。主要终点是在移植后6个月与4周时,通过对MSC治疗组和未治疗组进行定量天狼星红评分来比较纤维化情况。次要终点包括:复合终点疗效失败(活检证实的急性排斥反应、移植肾丢失或死亡);肾功能和蛋白尿;机会性感染;通过评估不同治疗组的超声心动图进行免疫监测和“亚临床”心血管疾病分组。
本研究将提供关于MSC与依维莫司联合使用是否可用于撤减他克莫司,以及该策略是否能在肾移植受者中保留肾脏结构和功能的信息。
NCT02057965。
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