Minimizing tacrolimus decreases the risk of new-onset diabetes mellitus after liver transplantation

AbstractAIM： To investigate the impact of minimum tacrolimus（TAC） on new-onset diabetes mellitus （NODM） afterliver transplantation （LT）.METHODS： We retrospectively analyzed the data of973 liver transplant recipients between March 1999and September 2014 in West China Hospital LiverTransplantation Center. Following the exclusion ofineligible recipients, 528 recipients with a TAC-dominantregimen were included in our study. We calculatedand determined the mean trough concentration ofTAC （cTAC） in the year of diabetes diagnosis in NODMrecipients or in the last year of the follow-up in non-NODM recipients. A cutoff of mean cTAC value forpredicting NODM 6 mo after LT was identified usinga receptor operating characteristic curve. TAC-relatedcomplications after LT was evaluated by χ^2 test, andthe overall and allograft survival was evaluated usingthe Kaplan-Meier method. Risk factors for NODM afterLT were examined by univariate and multivariate Cox regression.RESULTS： Of the 528 transplant recipients, 131（24.8%） developed NODM after 6 mo after LT, andthe cumulative incidence of NODM progressivelyincreased. The mean cTAC of NODM group recipientswas significantly higher than that of recipients in thenon-NODM group （7.66 ± 3.41 ng/mL vs 4.47 ± 2.22ng/mL, P 〈 0.05）. Furthermore, NODM group recipientshad lower 1-, 5-, 10-year overall survival rates （86.7%,71.3%, and 61.1% vs 94.7%, 86.1%, and 83.7%, P 〈0.05） and allograft survival rates （92.8%, 84.6%, and75.7% vs 96.1%, 91%, and 86.1%, P 〈 0.05） thanthe others. The best cutoff of mean cTAC for predictingNODM was 5.89 ng/mL after 6 mo after LT. Multivariateanalysis showed that old age at the time of LT （〉 50years）, hypertension pre-LT, and high mean cTAC （≥5.89 ng/mL） after 6 mo after LT were independent riskfactors for developing NODM. Concurrently, recipientswith a low cTAC （〈 5.89 ng/mL） were less likely tobecome obese （21.3% vs 30.2%, P 〈 0.05） or todevelop dyslipidemia （27.5% vs 44.8%, P 〈0.05）,chronic kidney dysfunction （14.6% vs 22.7%, P 〈 0.05）,and moderate to severe infection （24.7% vs 33.1%, P〈 0.05） after LT than recipients in the high mean cTACgroup. However, the two groups showed no significantdifference in the incidence of acute and chronicrejection, hypertension, cardiovascular events and newonsetmalignancy.CONCLUSION： A minimal TAC regimen can decreasethe risk of long-term NODM after LT. Maintaining a cTACvalue below 5.89 ng/mL after LT is safe and beneficial.

New-onset diabetes mellitus after kidney transplantation:Current status and future directions

A diagnosis of new-onset diabetes after transplantation(NODAT) carries with it a threat to the renal allograft,as well as the same short-and long-term implications of type 2 diabetes seen in the general population.NODAT usually occurs early after transplantation,and is usually diagnosed according to general population guidelines.Non-modifiable risk factors for NODAT include advancing age,African American,Hispanic,or South Asian ethnicity,genetic background,a positive family history for diabetes mellitus,polycystic kidney disease,and previously diagnosed glucose intolerance.Modifiable risk factors for NODAT include obesity and the metabolic syndrome,hepatitis C virus and cytomegalovirus infection,corticosteroids,calcineurin inhibitor drugs(especially tacrolimus),and sirolimus.NODAT affects graft and patient survival,and increases the incidence of post-transplant cardiovascular disease.The incidence and impact of NODAT can be minimized through pre-and post-transplant screening to identify patients at higher risk,including by oral glucose tolerance tests,as well as multi-disciplinary care,lifestyle modification,and the use of modified immunosuppressive regimens coupled with glucose-lowering therapies including oral hypoglycemic agents and insulin.Since NODAT is a major cause of post-transplant morbidity and mortality,measures to reduce its incidence and impact have the potential to greatly improve overall transplant success.

IGF2 ApaI A/G Polymorphism Evaluated in ESRD Individuals as a Biomarker to Identify Patients with New Onset Diabetes Mellitus after Renal Transplant in Asian Indians

Insulin like growth factors2 (IGF2) regulates pancreatic β-cell renewal and apoptosis, which in turn plays a role in altering insulin activity and glucose homeostasis. Polymorphisms in IGF2 gene have been associated with altered levels of IGF2. Hence, ApaI polymorphism in exon 9 of IGF2 (rs#680) gene was assessed in patients with end stage renal disease (ESRD) to identify individuals at risk of developing new onset diabetes mellitus (NODM) in Asian Indians. Isolated DNA was used for PCR&RFLP based genotyping of IGF2 ApaI polymorphism which was carried out in 364 individuals these included 140 patients who had undergone renal transplant, 42 of which developed new onset diabetes mellitus after renal transplant and 224 healthy control volunteers. In the present study NODM or post transplant diabetes mellitus (PTDM) showed a significant association with G allele and AG genotype when compared with the Non-NODM ESRD patients after transplant (OR 2.081, 95% CI = 1.191 - 3.634, p = 0.01 and OR 3.188, 95% CI = 1.498 - 6.785, p = 0.002) ESRD patients with healthy controls also showed an association with G allele and AG genotype (OR 1.512, 95% CI = 1.060 - 2.155, p = 0.02 and OR 2.235, 95% CI = 1.453 - 3.438, p = 0.0002). IGF2 could be used as a biomarker to identify individuals at high risk of developing NODM, it would be a valuable asset in selecting appropriate immunosuppressive regimens for individuals undergoing transplant. Present study shows the importance of IGF2 ApaI polymorphism in assessing the risk of NODM in ESRD individuals in Asian Indians with ESRD.

New-onset diabetes after kidney transplantation:Incidence and associated factors

AIM To determine the incidence and associated factors of new-onset diabetes after transplantation(NODAT) in a Portuguese central hospital. METHODS This single-center retrospective study involved consecutive adult nondiabetic transplant recipients, who had undergone kidney transplantation between January 2012 and March 2016. NODAT was diagnosed according to the criteria of the American Diabetes Association. Data were collected from an institutional database of the Nephrology and Kidney Transplantation Department(Santa Maria Hospital, Lisbon, Portugal) and augmented with data of laboratorial parameters collected from the corresponding patient electronic medical records. Exclusion criteria were preexisting diabetes mellitus, missing information and follow-up period of less than 12 mo. Data on demographic and clinical characteristics as well as anthropometric and laboratorial parameters were also collected. Patients were divided into two groups: With and without NODAT-for statistical comparison.RESULTS A total of 156 patients received kidney transplantduring the study period, 125 of who were included in our analysis. NODAT was identified in 27.2% of the patients(n = 34; 53% female; mean age: 49.5 ± 10.8 years; median follow-up: 36.4 ± 2.5 mo). The incidence in the first year was 24.8%. The median time to diagnosis was 3.68 ± 5.7 mo after transplantation, and 76.5% of the patients developed NODAT in the first 3 mo. In the group that did not develop NODAT(n = 91), 47% were female, with mean age of 46.4 ± 13.5 years and median follow-up of 35.5 ± 1.6 mo. In the NODAT group, the pretransplant fasting plasma glucose(FPG) levels were significantly higher [101(96.1-105.7) mg/d L vs 92(91.4-95.8) mg/d L, P = 0.007] and pretransplant impaired fasting glucose(IFG) was significantly more frequent(51.5% vs 27.7%, P = 0.01). Higher pretransplant FPG levels and pretransplant IFG were found to be predictive risk factors for NODAT development [odds ratio(OR): 1.059, P = 0.003; OR: 2.772, P = 0.017, respectively]. CONCLUSION NODAT incidence was high in our renal transplant recipients, particularly in the first 3 mo posttransplant, and higher pretransplant FPG level and IFG were risk factors.

Simultaneous pancreas-kidney transplantation for end-stage renal failure in type 1 diabetes mellitus: Current perspectives

Type 1 diabetes mellitus(T1DM)is one of the important causes of chronic kidney disease(CKD)and end-stage renal failure(ESRF).Even with the best available treatment options,management of T1DM poses significant challenges for clinicians across the world,especially when associated with CKD and ESRF.Substantial increases in morbidity and mortality along with marked rise in treatment costs and marked reduction of quality of life are the usual consequences of onset of CKD and progression to ESRF in patients with T1DM.Simultaneous pancreas-kidney transplant(SPK)is an attractive and promising treatment option for patients with advanced CKD/ESRF and T1DM for potential cure of these diseases and possibly several complications.However,limited availability of the organs for transplantation,the need for long-term immunosuppression to prevent rejection,peri-and post-operative complications of SPK,lack of resources and the expertise for the procedure in many centers,and the cost implications related to the surgery and postoperative care of these patients are major issues faced by clinicians across the globe.This clinical update review compiles the latest evidence and current recommendations of SPK for patients with T1DM and advanced CKD/ESRF to enable clinicians to care for these diseases.

New onset hypertension after transplantation

It has been reported that up to 90%of organ transplant recipients have suboptimal blood pressure control.Uncontrolled hypertension is a well-known culprit of cardiovascular and overall morbidity and mortality.In addition,rigorous control of hypertension after organ transplantation is a crucial factor in prolonging graft survival.Nevertheless,hypertension after organ transplantation encompasses a broader range of causes than those identified in non-organ transplant patients.Hence,specific management awareness of those factors is mandated.An in-depth understanding of hypertension after organ transplantation remains a debatable issue that necessitates further clarification.This article provides a comprehensive review of the prevalence,risk factors,etiology,complications,prevention,and management of hypertension after organ transplantation.

Simultaneous liver, pancreas-duodenum and kidney transplantation in a patient with hepatitis B cirrhosis, uremia and insulin dependent diabetes mellitus

Simultaneous liver,pancreas-duodenum,and kidney transplantation has been rarely reported in the literature. Here we present a new and more efficient en bloc technique that combines classic orthotopic liver and pancreas-duodenum transplantation and heterotopic kidney transplantation for a male patient aged 44 years who had hepatitis B related cirrhosis,renal failure,and insulin dependent diabetes mellitus(IDDM). A quadruple immunosuppressive regimen including induction with basiliximab and maintenance therapy with tacrolimus,mycophenolate mofetil,and steroids was used in the early stage post-transplant. Postoperative recovery was uneventful and the patient was discharged on the 15 th postoperative day with normal liver and kidney function. The insulin treatment was completely withdrawn 3 wk after operation,and the blood glucose level remained normal. The case findings support that abdominal organ cluster and kidney transplantation is an effective method for the treatment of end-stage liver disease combined with uremia and IDDM.

Statin use and risk of diabetes mellitus

The 3-hydroxy-methylglutaryl coenzyme A reductase inhibitors, statins, are widely used in the primary and secondary prevention of cardiovascular diseases to lower serum cholesterol levels. As type 2 diabetes mellitus is accompanied by dyslipidemia, statins have a major role in preventing the long term complications in diabetes and are recommended for diabetics with normal low density lipoprotein levels as well. In 2012, United States Food and Drug Administration released changes to statin safety label to include that statins have been found to increase glycosylated haemoglobin and fasting serum glucose levels. Many studies done on patients with cardiovascular risk factors have shown that statins have diabetogenic potential and the effect varies as per the dosage and type used. The various mechanisms for this effect have been proposed and one of them is downregulation of glucose transporters by the statins. The recommendations by the investigators are that though statins can have diabetogenic risk, they have more long term benefits which can outweigh the risk. In elderly patients and those with metabolic syndrome, as the risk of diabetes increase, the statins should be used cautiously. Other than a subset of population with risk for diabetes; statins still have long term survival benefits in most of the patients.

Importance of genetic polymorphisms in liver transplantation outcomes

Although,liver transplantation serves as the only curative treatment for patients with end-stage liver diseases,it is burdened with complications,which affect survival rates.In addition to clinical risk factors,contribution of recipient and donor genetic prognostic markers has been extensively studied in order to reduce the burden and improve the outcomes.Determination of single nucleotide polymorphisms(SNPs)is one of the most important tools in development of personalized transplant approach.To provide a better insight in recent developments,we review the studies published in the last three years that investigated an association of recipient or donor SNPs with most common issues in liver transplantation:Acute cellular rejection,development of new-onset diabetes mellitus and non-alcoholic fatty liver disease,hepatocellular carcinoma recurrence,and tacrolimus concentration variability.Reviewed studies confirmed previously established SNP prognostic factors,such as PNPLA3 rs738409 for nonalcoholic fatty liver disease development,or the role of CYP3A5 rs776746 in tacrolimus concentration variability.They also identified several novel SNPs,with a reasonably strong association,which have the potential to become useful predictors of post-transplant complications.However,as the studies were typically conducted in one center on relatively low-to-moderate number of patients,verification of the results in other centers is warranted to resolve these limitations.Furthermore,of 29 reviewed studies,28 used gene candidate approach and only one implemented a genome wide association approach.Genome wide association multicentric studies are needed to facilitate the development of personalized transplant medicine.

Pancreatic transplantation: Brief review of the current evidence

Kidney transplantation is the treatment of choice for management of end-stage renal disease.However,in diabetic patients,the underlying metabolic disturbance will persist and even may get worse after isolated kidney transplantation.Pancreatic transplantation in humans was first introduced in 1966.The initial outcome was disappointing.However,this was changed after the improvement of surgical techniques together with better patient selection and the availability of potent and better-tolerated immune-suppression like cyclosporine and induction antibodies.Combined kidney and pancreas transplantation will not only solve the problem of organ failure,but it will also stabilise or even reverse the metabolic complications of diabetes.Combined kidney and pancreas transplantation have the best long term outcome in diabetic cases with renal failure.Nevertheless,at the cost of an initial increase in morbidity and risk of mortality.Other transplantation options include pancreas after kidney transplantation and islet cell transplantation.We aim by this work to explore various options which can be offered to a diabetic patient with advanced chronic kidney disease.Our work will provide a simplified,yet up-to-date information regarding the different management options for those diabetic chronic kidney failure patients.

阿托伐他汀诱导的MIN6细胞铁死亡及相关机制研究

目的:探讨阿托伐他汀(atorvastatin,Ator)是否可诱导小鼠胰岛β细胞株MIN6细胞发生铁死亡,并探讨其可能的作用机制。方法:将MIN6细胞分为对照组、Ator组、Ator+凋亡抑制剂(Z-VAD-FMK)组、Ator+坏死抑制剂(necrostatin-1,Nec-1)组和Ator+铁死亡抑制剂(ferrostatin-1,Fer-1)组。采用CCK-8法检测细胞活力;透射电镜观察细胞超微结构;荧光显微镜观察活性氧(reactive oxygen species,ROS)和Fe^(2+)水平;酶联免疫吸附试验(enzyme-linked immuno sorbent assay,ELISA)检测丙二醛(malondialdehyde,MDA)和还原型谷胱甘肽(glutathione,GSH)含量;实时荧光定量PCR法(quantitative real-time PCR,RT-qPCR)检测凋亡基因半胱氨酸蛋白酶3(caspase-3)、坏死基因受体结合丝氨酸苏氨酸激酶3(receptor-interacting serine threonine kinase 3,Ripk3)、铁死亡相关基因长链酯酰辅酶A合成酶4(acyl-coA synthetase long-chain family member 4,Acsl4)、前列腺素内过氧化物合酶2(prostaglandin-endoperoxide synthase 2,Ptgs2)和谷胱甘肽过氧化物酶4(glutathione peroxidase 4,Gpx4)的mRNA表达水平;Western blot检测4-羟基壬烯醛(4-hydroxynonenal,4-HNE)和GPX4的蛋白表达水平。结果:与Ator组相比,Ator+Z-VAD-FMK组和Ator+Fer-1组细胞存活率更高(P均<0.01)。透射电镜下Ator组细胞可见凋亡、铁死亡和自噬相关的形态学特征。与对照组相比,Ator组细胞Fe^(2+)相对荧光强度、MDA水平和ROS相对水平均升高,GSH含量下降;caspase-3、Acsl4、Ptgs2的mRNA及4-HNE的蛋白表达增加(P均<0.05),GPX4的mRNA和蛋白表达减少(P<0.05)。与Ator组相比,Ator+Fer-1组Fe^(2+)相对荧光强度、MDA水平和ROS相对水平均下降,GSH含量上升;Acsl4的mRNA表达减少,Gpx4的mRNA表达增加(P均<0.05);4-HNE的蛋白表达减少而GPX4的蛋白表达增加,但差异无统计学意义。结论:Ator可能通过抑制甲羟戊酸途径下调GPX4表达,诱导MIN6细胞发生铁死亡。

胰腺囊性肿瘤患者行胰体尾切除术后新发糖尿病预后因素的初步探讨

目的探讨胰腺囊性肿瘤患者行胰体尾切除术后新发糖尿病(new-onset diabetes mellitus,NODM)的预后因素。方法回顾分析2010年1月~2019年12月我院92例胰腺囊性肿瘤行腹腔镜胰体尾切除的临床资料,根据入选和排除标准,共纳入74例,按照术后随访期间是否发生NODM分为NODM组(n=26)和糖代谢正常组(n=48),采用单因素分析胰腺囊性肿瘤患者行腹腔镜胰体尾切除术后NODM的预后因素。P<0.05认为差异有显著性,OR>4认为有潜在临床意义的NODM预后因素。结果26例胰腺囊性肿瘤行胰体尾切除术后NODM(35.1%),确诊NODM中位时间为9个月(3~56个月)。单因素分析显示颈部胰腺离断颈部(OR=11.000,P=0.000)、有糖尿病家族史(OR=5.000,P=0.004)和BMI≥25.0(OR=4.333,P=0.007)是术后NODM的预后因素。结论胰腺囊性肿瘤行胰体尾切除时应尽可能保留更多的胰腺组织,避免在颈部离断胰腺,BMI≥25.0和糖尿病家族史的患者术后应密切关注糖代谢情况。

高血压患者衰弱分期及衰弱指数对新发糖尿病发生的影响

目的:探索衰弱分期及衰弱指数(frailty index,FI)对高血压患者新发糖尿病的影响。方法:本研究为单中心回顾性队列研究,入选符高血压患者953例。据FI将患者分为三组:衰弱组(FI>0.21)、衰弱前期组(0.10<FI≤0.21)、健康组(FI≤0.10)。研究的主要终点是新发糖尿病。通过多元Cox回归分析探究衰弱分期对新发糖尿病的影响,并绘制Kaplan-Meier曲线及限制性立方样条(RCS)曲线直观反映FI与新发糖尿病之间的关系,同时进行了亚组分析。结果:随着衰弱程度的加重,患者新发糖尿病的发生率显著增高(P<0.001)。Kaplan-Meier曲线表明衰弱组、衰弱前期组患者新发糖尿病的风险显著高于无衰弱组。调整混杂因素后的多元Cox回归的结果显示,与无衰弱组相比,衰弱组(HR=3.14,95%CI:1.50~6.58,P=0.002)显著升高了患者新发糖尿病风险,是新发糖尿病的独立危险因素;而衰弱前期组(HR=1.88,95%CI:0.95~3.74,P=0.071)差异无统计学意义。RCS曲线表明FI与新发糖尿病的关系是线性的,新发糖尿病风险随着FI的上升而增加。亚组分析结果表明各亚组与衰弱分期之间对结局的影响并无显著的交互作用。结论:在高血压患者中,衰弱是新发糖尿病的独立危险因素,FI与新发糖尿病风险呈线性正相关。

肾移植术后新发糖尿病危险因素分析

目的探讨肾移植术后新发糖尿病(new-onset diabetes mellitus after renal transplantation,NODAT)的危险因素。方法术前未患糖尿病接受同种尸体肾移植的患者706例,根据入选时有否NODAT分为NODAT组和非NODAT组。统计NODAT发生率,对两组患者可能存在的NODAT危险因素[糖尿病家族史、年龄、性别、体重指数、透析方式与时间、术后使用含他克莫司(FK506)免疫抑制方案例数、急性排斥反应发生次数]进行组间单因素分析。结果 706例术前非糖尿病的肾移植术后患者中,发生NODAT78例,非NODAT患者628例,NODAT发生率为11%。单因素分析结果显示,NODAT组的患者年龄、术前糖尿病家族史、术后使用含FK506免疫抑制方案例数、急性排斥发生次数,均显著高于非NODAT组(P﹤0.05～P<0.01)。结论患者年龄大、有糖尿病家族史、术后使用含FK506的免疫抑制方案、急性排斥发生次数多是引发NODAT的危险因素。

不同免疫抑制方案对肾移植术后糖尿病发病率的影响

为探讨不同免疫抑制方案对肾移植术后糖尿病 (PTDM)发病率的影响 ,根据不同免疫抑制方案把4 2 9例肾移植患者分为三组 ,定期监测患者用药情况、生化指标、环孢素 A(Cs A )浓度、FK50 6 浓度 ,随访时间至少6个月。结果 :PTDM发病率为强的松 +Cs A+硫唑嘌呤 (1组 ) 11.8% ,强的松 +霉酚酸酯 (MMF) +Cs A(2组 )6 .4 % ,强的松 +MMF+FK50 6 (3组 ) 4 .2 % ,三组之间存在显著差异 ,2组排斥反应率和平均激素用量明显低于 1组。认为肾移植术后不同免疫抑制方案下 PTDM的发病率不同 ,小剂量 Cs A或 FK50 6 联合 MMF的免疫抑制方案可以降低

西罗莫司转换钙调磷酸蛋白酶抑制剂治疗肾移植术后糖尿病

目的评价西罗莫司(SRL)转换钙调磷酸蛋白酶抑制剂(CNI)治疗肾移植术后糖尿病的安全性及疗效。方法回顾性分析我院近10年321例肾移植术后患者,其中有34例(10.59%)诊断为肾移植术后糖尿病,按治疗方案分为3组:A组(14例)为标准化的CNI减量方案,B组(12例)为SRL转换CNI药物方案,C组(10例)为口服降糖药物,所有患者均辅助饮食及运动疗法。当餐后血糖超过14.0 mmol/L时,餐前均辅助皮下注射短效胰岛素治疗并维持治疗,并规律随访5年。结果所有入组患者诊断肾移植术后糖尿病时血糖平均13.02±1.74 mol/L,3组间无显著性差异(P>0.05)。经辅助治疗6月后,A、B、C组患者血糖分别平均下降至8.05±2.45、7.45±2.44和9.30±3.89 mmol/L。经调整胰岛素剂量12月后A组和B组患者血糖均降至正常,但日均胰岛素用量,A组患者明显多于B组(P<0.05)。SRL组转换时的肌酐165.1±61.8 mmol/L,转换5年后肌酐150.0±53.0 mmol/L(P<0.05);CNI减量组治疗前肌酐152.0±43.0 mmol/L,5年后肌酐是145.9±53.0 mmol/L;C组患者肾功能没有在治疗中获益,治疗后肌酐上升。A组患者5年生存率人/肾分别是100%和75%,与B组患者人/肾生存率83.4%和68%,两组无显著性差异(P>0.05),C组患者5年生存率分别是71.8%和52.4%,明显低于A组和B组。结论肾移植术后行SRL转换CNI药物有利于改善肾移植术后糖尿病且不增加排斥风险。

肾移植术后糖尿病发病率与危险因素

目的:探讨肾移植术后糖尿病(post-transplantation diabetes mellitus,PTDM)的发病率及危险因素。方法:567例术前无糖尿病的肾移植患者入组,回顾性调查患者性别、移植时年龄、体重、体重指数(BMI)、透析时间、移植前空腹血糖等一般临床资料及移植后1,3,6,12,24个月的免疫抑制方案、空腹血糖等实验室检测结果。根据美国糖尿病协会的诊断标准将患者分为PTDM组和对照组(移植后非糖尿病组),采用t检验和χ~2检验统计两组间上述各变量的差异,采用logistic回归分析发生PTDM的危险因素。结果:PTDM发病率为24.2%(137/567),男性(OR=1.813,P=0.009)、移植时年龄>45岁(OR=2.528,P<0.001)、移植时体重>65 kg(OR=2.445,P<0.001)、移植时BMI>24 kg·m^(-2)(OR=1.819,P=0.005)、术后1,3,6,12,24个月的环孢素日剂量及血浓度均与PTDM的发生显著相关。结论:男性、移植时年龄>45岁、体重>65kg、BMI>24及较高的环孢素日剂量和血浓度是发生PTDM的危险因素。

他克莫司血药浓度及相关基因多态性与心脏移植术后新发糖尿病的相关性

目的探讨他克莫司血药浓度及相关基因多态性与心脏移植术后新发糖尿病(NODAT)的相关性。方法拟纳入移植术前无糖尿病的心脏移植受者。收集患者资料并检测rs2237895、rs5215、rs2276706和rs8450四个单核苷酸多态性(SNPs)位点。根据美国糖尿病协会(ADA)诊断标准判断NODAT。采用多元logistic回归分析他克莫司血药浓度对NODAT的影响,并建立NODAT风险预测模型。结果共纳入101例心脏移植受者,其中NODAT 31例(30.7%)。NODAT组他克莫司剂量校正浓度(C 0/D)显著高于非NODAT组(139.3比96.0,P=0.025)。他克莫司C 0/D≥110 ng·mL-1/(mg·kg-1·d-1)[OR=4.52,95%CI(1.63,12.53),P=0.004]、年龄≥45岁[OR=4.99,95%CI(1.65,15.10),P=0.005]和体质量指数(BMI)≥25 kg·(m 2)-1[OR=3.70,95%CI(1.38,9.93),P=0.009]是NODAT的独立危险因素。在NODAT风险预测模型中加入他克莫司C 0/D≥110 ng·mL-1/(mg·kg-1·d-1)使风险预测模型的AUROC提高到0.788(P<0.001)。结论他克莫司C 0/D[≥110 ng·mL-1/(mg·kg-1·d-1)]、年龄(≥45岁)和BMI[≥25 kg·(m 2)-1]是NODAT发生的独立危险因素。基于以上危险因素建立的NODAT风险预测模型具有较好的预测效能,可便捷地初步筛选出心脏移植术后NODAT的高危人群,以便及时干预,预防NODAT的发生。

胰肾联合移植治疗胰岛素依赖型糖尿病及终末期肾病的实验与临床研究

目的：探讨在我国进行胰肾联合移植（ＳＰＫＴ）的可行方法，并应用于临床。方法：在８０余次尸体供者腹腔多脏器联合摘取及动物实验的基础上，在临床施行ＳＰＫＴ３例，胰十二指肠移植于右髂窝，肾脏移植于左髂窝，腹主动脉与肠系膜上动脉袖片与髂外动脉端－侧吻合，门静脉与髂外静脉端－侧吻合，胰腺外分泌引流采用经膀胱途径。结果：１例已存活８个月，术后未用胰岛素，胰肾功能良好，无并发症，已恢复正常生活和工作；１例术后４７天死于脑出血，死亡时胰肾功能良好；１例术后４９天胰腺动脉血栓形成，死于坏死性胰腺炎。结论：ＳＰＫＴ是治疗糖尿病并发终末期肾病的一种切实可行的有效方法，它将成为治疗该病的一种安全、有效、常规治疗方法。

合并不同糖尿病病程的胰腺癌患者临床特征及相关危险因素对胰腺癌发病年龄的影响

目的分析胰腺癌(pancreatic cancer,PC)合并糖尿病(diabetes mellitus,DM)患者的临床特征及不同因素对PC发病年龄的影响。方法 1985年1月至2014年10月北京协和医院收治的PC合并DM且符合一定纳入标准的患者,先分析总体人群基本特征,再根据不同DM病程,将总体人群分为新发DM组(病程≤2年)和长病程DM组(病程>2年),分析不同亚组的临床特征、肿瘤特征、既往疾病史及用药情况,并分析不同因素包括性别、生活方式、家族史、既往史、用药情况对PC发病年龄的影响。结果共327例PC合并DM患者纳入本研究。总体人群及按病程分组人群中男性比例均较高,且发病年龄较女性更低[(60.2±9.5)岁比(65.7±8.5)岁,P<0.001]。新发DM组较长病程DM组PC发病年龄更低[(60.6±9.5)岁比(64.4±9.0)岁,P<0.001],有DM家族史者比例更低(13.8%比24.3%,P=0.016),平均体重下降程度更明显(9.0 kg比5.0 kg,P=0.003),空腹血糖水平更低(8.2 mmol/L比9.1 mmol/L,P=0.003),肿瘤平均直径更大(4.0 cm比3.5 cm,P=0.007),胰岛素和降压药的使用比例均较低(41.9%比71.3%,P<0.001;32.9%比49.6%,P=0.004)。男性(P<0.001)、吸烟(P<0.001)、饮酒(P<0.001)、有DM家族史(P=0.048)、使用二甲双胍(P=0.046)的患者PC发病年龄更低,而服用阿卡波糖者PC发病年龄更高(P=0.042)。结论无DM家族史、伴体重明显下降、有吸烟、饮酒史的新发DM患者,可能是患PC的高危人群,需格外警惕,注意早期筛查。