A Clinical Trial to Prevent New Onset Diabetes After Transplantation

预防移植后新发糖尿病的临床试验

• 批准号: 8677880
• 负责人: Akinlolu Oluseun Ojo
• 金额: $ 45.29万
• 依托单位: UNIVERSITY OF MICHIGAN AT ANN ARBOR
• 依托单位国家: 美国
• 财政年份: 2011
• 资助国家: 美国
• 起止时间: 2011-09-09 至 2017-05-30
• 项目状态: 已结题
• 来源: https://reporter.nih.gov/project-details/8677880
• 关键词: Adrenal Cortex Hormones; Allogenic; Allografting; Anorexia; Austria; Behavior Therapy; Beta Cell; Biological Preservation; Calcineurin inhibitor; Cardiovascular system; Cell physiology; Chronic; Clinical; Clinical Trials; Controlled Clinical Trials; Counseling; Cyclosporine; Deterioration; Development; Diabetes Mellitus; Diagnosis; Diet; Dietary intake; Disease remission; Dose; Enrollment; Event; Exhibits; Fleming Method Relaxation; General Hospitals; General Population; Glucose; Glucose Intolerance; Glycosylated hemoglobin A; Health; Health system; Homeostasis; Hyperglycemia; Hypoglycemia; Hypoglycemic Agents; Immunosuppression; Immunosuppressive Agents; Impaired fasting glycaemia; Incidence; Inferior; Injectable; Insulin; Insulin Resistance; Isophane Insulin; Kidney Transplantation; Lead; Maintenance Therapy; Medical; Metabolic; Metabolic stress; Michigan; Minority; Modeling; Newly Diagnosed; Non-Insulin-Dependent Diabetes Mellitus; Onset of illness; Operative Surgical Procedures; Oral; Participant; Patients; Peripheral; Pharmaceutical Preparations; Plasma; Population Heterogeneity; Postoperative Period; Prevalence; Procedures; Randomized; Randomized Clinical Trials; Regimen; Rejuvenation; Relative Risks; Rest; Risk; Risk Reduction; Safety; Sample Size; Secondary to; Stress; Structure of beta Cell of islet; Tacrolimus; Taiwan; Testing; Therapeutic Intervention; Time; Transplant Recipients; Transplantation; Universities; Uremia; arm; basal insulin; cardiovascular disorder risk; cell injury; cytotoxic; diabetic; economic outcome; fasting plasma glucose; follow-up; glucose metabolism; glycemic control; health care service utilization; hepatic gluconeogenesis; impaired glucose tolerance; improved; non-diabetic; open label; prevent; standard of care

DESCRIPTION (provided by applicant): Immediately following allogeneic kidney transplantation, the pancreatic beta-cell mass is relentlessly punished by four counterregulatory metabolic factors namely: (1) gluconeogenic surgery-related stress; (2) exogenous glucocortocoid-induced peripheral insulin resistance and hepatic gluconeogenesis; (3) direct beta-cell injury by the calcineurin inhibitor (cyclosporine or tacrolimus) and; (4) increased dietary caloric load secondary to the abrogation of chronic uremia-related anorexia. Consequent to this metabolic engagement, 45-80% of new kidney transplant recipients (KTRs) will manifest persistent reversible hyperglycemia, 30% will maintain chronic impaired glucose intolerance and 15-20% will succumb to new onset diabetes after transplantation (NODAT) by the end of the first post transplant year. NODAT is a form type 2 diabetes mellitus that afflicts up to 30% of kidney transplant recipients who survive through the third post transplant year. NODAT is associated with increased risk for post transplant cardiovascular events, higher health care utilization and dramatically inferior kidney graft and patient survival. The offending determinants of NODAT are largely unavoidable because calcineurin inhibitors are the mainstay immunosuppressive drug for kidney transplantation, 70-80% of KTRs are treated initially high dose corticosteroid followed by low dose maintenance therapy and improved dietary intake is a desired benefit of kidney transplantation. Evidence shows that the state of glucotoxicity induced by persistent hyperglycemia causes continuous decline in pancreatic beta-cell function during the early period of development of type 2 diabetes mellitus. More recently, protection of beta-cells by aggressive lowering of hyperglycemia with early initiation of insulin therapy has shown promise in inducing remission of newly diagnosed type 2 diabetes mellitus in the general population. We posit that early use of insulin therapy in previously non-diabetic KTRs who exhibit abnormal glucose metabolism immediately after kidney transplantation will enable the discontinuation of anti-diabetic therapy during the subsequent follow-up and will result in a reduced incidence of NODAT. We have completed a proof-of-concept clinical trial, using basal insulin during the immediate post-transplant period in 50 KTRs. The prevalence of NODAT at 12 months was reduced by 65%. We now propose to conduct a safety and efficacy open-label, block-randomized clinical trial in a diverse population of KTRs to test the primary hypothesis that an early NPH insulin regimen will reduce the incidence of NODAT from 15% to 10% without a significant difference in the risk of detectable hypoglycemia between the experimental and the control arms of the study. A sample size of 180 KTRs has a 90% power to detect a 30% risk reduction for NODAT at one-year post transplantation after protecting one interim analysis with the O'Brien-Fleming method. The study would be conducted at the University of Michigan Health System (n=90) and the Medical University of Vienna 'General Hospital' (n=90). Participants will be enrolled over a 24 months period with a minimum follow-up of 24 months post randomization.

描述（由申请人提供）：在同种异体肾移植后，胰腺β细胞团立即受到四种反调节代谢因素的无情惩罚，即：（1）促血管生成的手术相关应激;（2）外源性糖皮质激素诱导的外周胰岛素抵抗和肝血管生成;（3）钙调磷酸酶抑制剂直接损伤β细胞。（环孢霉素或他克莫司）和（4）继发于消除慢性尿毒症相关厌食症的饮食热量负荷增加。与这种代谢参与相一致，45-80%的新肾移植受者（KTR）将表现出持续的可逆性高血糖症，30%将维持慢性葡萄糖耐受不良受损，15-20%将在移植后第一年结束时死于移植后新发糖尿病（NODAT）。NODAT是一种2型糖尿病，困扰着多达30%的肾移植受者，他们在移植后第三年存活。NODAT与移植后心血管事件的风险增加、更高的卫生保健利用率和显著降低的肾移植和患者生存率相关。NODAT的不利决定因素在很大程度上是不可避免的，因为钙调磷酸酶抑制剂是肾移植的主要免疫抑制药物，70-80%的KTR最初接受高剂量皮质类固醇治疗，随后接受低剂量维持治疗，改善饮食摄入是肾移植的期望益处。有证据表明，在2型糖尿病发展的早期阶段，持续高血糖诱导的葡萄糖毒性状态导致胰腺β细胞功能持续下降。最近，通过早期开始胰岛素治疗积极降低高血糖症来保护β细胞已显示出在一般人群中诱导新诊断的2型糖尿病缓解的前景。我们认为，在肾移植后立即显示糖代谢异常的既往非糖尿病KTR中，早期使用胰岛素治疗将使随后随访期间的抗糖尿病治疗停止，并将导致NODAT发生率降低。我们已经完成了一项概念验证临床试验，在50个KTR中，在移植后立即使用基础胰岛素。12个月时NODAT的患病率降低了65%。我们现在建议在不同的KTR人群中进行一项安全性和有效性的开放标签、区组随机临床试验，以检验主要假设，即早期NPH胰岛素方案将使NODAT的发生率从15%降低至10%，而研究的实验组和对照组之间可检测到的低血糖风险无显著差异。在用O 'Brien-Fleming方法进行一次中期分析后，180个KTR的样本量具有90%的把握度来检测移植后一年NODAT风险降低30%。本研究将在密歇根大学卫生系统（n=90）和维也纳医科大学“综合医院”（n=90）进行。受试者将在24个月内入组，随机化后至少随访24个月。