Expression of iNOSmRNA to prevent cardiac allograft vasculopathy after heart transplantation in rat

Objective Develop the model of post-transplant cardiac allograft vasculopathy (CAV) and prevent or treat CAV through Expression of iNOSmRNA.Methods Rat model of heterotopic heart transplantation was developed and three groups were divided as following: Comparison group, CsA group, iNSOmRNA group. Hearts were harvested at post-operative two weeks and four weeks and CAV was detected by immunohitochemical technique and in situ hybridization technique.Results iNOSmRNA group had no CAV develpment and synthetizing vast NO.Conclusion Expression of iNOSmRNA can prevent CAV development.

Early detection of cardiac allograft vasculopathy and chronic rejection after heart transplantation-Report of one case

Objective To study clinically the feasibility of early diagnosis of cardiac allograft vascularopathy(CAV) and chronic rejection. Methods A 13-year-old female patient with dilated cardiomy-opathy received orthotopic heart transplantation for advanced heart failure, and subsequent immunosuppressive therapy including cyclosporine, prednisone and mofetil, and a mondily close follow-up. Coronary angiography and left ventricular endomyocardial biopsy (EMB) was perormed 9 months after the operation. Results The clinical and follow-up data of the case showed that cardiac or systemic nonspecific symptoms such as exertional chest discomfort, palpitation, fatigue or fever of unknown reasons were the first and ignorable clinical symptoms, and found disappeared after dosage addition of cyclinsporine, which indicated a early clinical manifestations of rejection or vasculopathy. While persistent sinus tachycardia on electrocadiogram, decreased left ventricular ejection fraction(from 64% -68% down to 47% - 50% ),

Coronary microvasculopathy in heart transplantation: Consequences and therapeutic implications

Despite the progress made in the prevention and treatment of rejection of the transplanted heart, cardiac allograft vasculopathy(CAV) remains the main cause of death in late survival transplanted patients. CAV consists of a progressive diffuse intimal hyperplasia and the proliferation of vascular smooth muscle cells, ending in wall thickening of epicardial vessels, intramyocardial arteries(50-20 μm), arterioles(20-10 μm), and capillaries(< 10 μm). The etiology of CAV remains unclear; both immunologic and non-immunologic mechanisms contribute to endothelial damage with a sustained inflammatory response. The immunological factors involved are Human Leukocyte Antigen compatibility between donor and recipient, alloreactive T cells and the humoral immune system. The non-immunological factors are older donor age, ischemia-reperfusion time, hyperlipidemia and CMV infections. Diagnostic techniques that are able to assess microvascular function are lacking. Intravascular ultrasound and fractional flow reserve, when performed during coronary angiography, are able to detect epicardial coronary artery disease but are not sensitive enough to assess microvascular changes. Some authors have proposed an index of microcircula-tory resistance during maximal hyperemia, which is calculated by dividing pressure by flow(distal pressure multiplied by the hyperemic mean transit time). Non-invasive methods to assess coronary physiology are stress echocardiography, coronary flow reserve by transthoracic Doppler echocardiography, single photon emission computed tomography, and perfusion cardiac magnetic resonance. In this review, we intend to analyze the mechanisms, consequences and therapeutic implications of microvascular dysfunction, including an extended citation of relevant literature data.

Persistent Epstein-Barr viral load in Epstein-Barr viral na?ve pediatric heart transplant recipients:Risk of late-onset post-transplant lymphoproliferative disease

AIM To examine the risk of late-onset post-transplant lymphoproliferative disorder(PTLD) in the presence of persisting high Epstein-Barr virus(EBV) in EBV na?ve pediatric heart transplant(HT) recipients. METHODS A retrospective review of the medical records of the 145 pediatric HT recipients who had serial EBV viral load monitoring at our center was performed. We defined EBV naive patients whose EBV serology either IgM or IgG in the blood were negative at the time of HT and excluded passive transmission from mother to child in subjects less than 6 mo of age. RESULTS PTLD was diagnosed in 8 out of 145 patients(5.5%); 6/91(6.5%) in those who were EBV seropositive and 2/54(3.7%) in the EBV na?ve group at the time of HT(P = 0.71). We found 32/145(22%) patients with persistently high EBV load during continuing follow-up; 20/91(22%) in EBV seropositive group vs 12/54(22%) in EBV na?ve group(P = 0.97). There was no significant association between pre-HT serostatus and EBV load after transplant(P > 0.05). In the EBV seropositive group, PTLD was diagnosed in 15%(3/20) of patients with high EBV vs 4.2%(3/71) of patients with low or undetectable EBV load(P = 0.14) whereas in EBV na?ve patients 8.3%(1/12) of those withhigh EBV load and 2.3%(1/42) with low or undetectable EBV load(P = 0.41). There was a highly significant association between occurrence of PTLD in those with high EBV load and duration of follow up(4.3 ± 3.9 years) after HT by Cochran-Armitage test for the entire cohort(P = 0.005). At least one episode of acute rejection occurred in 72%(23/32) of patients with high EBV vs 36%(41/113) patients with low or undetectable EBV after HT(P < 0.05). CONCLUSION There is an association between persistently high EBV load during post-HT follow up and the occurrence of late-onset PTLD in pediatric HT recipients irrespective of serostatus at the time of transplant. The occurrence of allograft rejection increased in patients with high EBV load presumably due to reduction in immunosuppression.

Mechanical Thrombectomy in Post-Transplant Heart

Coronary allograft vasculopathy (CAV) is an accelerated form of coronary artery disease that is responsible for significant mortality after cardiac transplantation. We report a case of CAV with significant thrombus burden which was managed with mechanical thrombectomy. Both aspiration and mechanical thrombectomy can be safely done in cardiac transplant recipients and may be considered in order to minimize exposure to coronary artery bypass procedure. This is especially valuable in emergency circumstances.

小鼠颈部同种异体心脏移植模型学习曲线分析

目的探讨小鼠颈部同种异体心脏移植模型建立的学习曲线特点。方法回顾性分析课题组行60只小鼠颈部同种异体心脏移植模型制备的资料,分别记录手术过程中移植总时间、受体准备时间、供体准备时间、动静脉套管制成时间、供体心血管连接时间,采用累积和(CUSUM)分析法及最佳拟合曲线获取各阶段移植手术的学习曲线中渡过学习期所需最小手术样本数。以学习曲线最长手术阶段的最小手术样本数作为界限将小鼠分为学习阶段组和成熟阶段组,比较各组手术时间及手术失败率的差异。结果60只小鼠完成颈部心脏移植,移植总时间为(119.80±43.17)min,受体准备时间为(76.43±26.46)min,供体准备时间为(29.85±9.82)min,动静脉套管制成时间为(32.10±21.62)min,供体心血管连接时间为(17.47±8.43)min。对CUSUM学习曲线进行拟合,采用三次方时拟合度最高,各阶段手术时间学习曲线所对应的最小手术样本数依次是受体手术25,供体手术19,动静脉套管制成29,供体心血管连接24,手术全过程25。以学习曲线最长的手术阶段(动脉套管制成)的最小样本数29为分界点分为两组,与学习阶段组相比,成熟阶段组移植总时间[(156.80±32.80)min对(85.06±9.45)min]、受体准备时间[(95.41±18.89)min对(50.94±7.45)min]、供体准备时间[(37.03±9.51)min对(23.13±2.95)min]、动静脉套管制成时间[(50.41±16.65)min对(14.97±5.74)min]、供体心血管连接时间[(24.38±7.16)min对(11.00±1.55)min],均明显减少,差异有统计学意义(P<0.01)。成熟阶段组手术失败率较学习阶段组明显降低(48.28%对9.68%,P=0.0013)。结论建立小鼠颈部同种异体心脏移植模型的学习曲线在各手术阶段略有差异,手术样本数达29以后技术基本成熟。手术技术成熟后手术时间及成功率都会有明显改善。

NBD多肽预处理的树突状细胞延长移植心存活时间的实验研究

目的探讨NBD多肽预处理的供体源性树突状细胞(DC)在诱导心脏移植免疫耐受中的作用及可能机制。方法体外培养供体源性BALB/c小鼠骨髓树突状细胞并以NBD多肽预处理(NBD多肽-DC,在小鼠心脏移植前7 d,将NBD多肽-DC输至受者C57BL/6小鼠体内。应用Cu-T建立小鼠颈部异位心脏移植模型,观察心脏移植物存活时间,病理分析检测排斥反应程度,混合淋巴细胞反应(MLR)测定受者脾脏T细胞对供者同种抗原的反应性,并用ELISA方法测定受者血清Th1型细胞因子(IFN-γ和IL-12)和Th2型细胞因子(IL-4和IL-10)水平的变化。结果NBD多肽-DC可使移植心脏存活天数延长至(21.83±3.54)d,较PBS对照组的(6.66±1.21)d明显延长(P<0.01),降低排斥反应病理分级(Stanford 1～2级),能诱导受者脾脏T细胞的抗原特异性低反应性,使受者小鼠血清INF-γ和IL-12水平显著降低(P<0.01),而IL-4和IL-10水平明显升高(P<0.01)。结论NBD多肽预处理的供体源性DC能够诱导针对移植供者产生的特异性免疫耐受现象,其机制可能与诱导受者T细胞的抗原特异性低反应性及Th1/Th2免疫偏移有关。

左旋精氨酸抑制大鼠心脏移植术后移植物血管病的研究

目的 探讨左旋精氨酸 (L Arg)预防和治疗心脏移植术后移植物血管病的作用。 方法 建立大鼠异位心脏移植动物模型 ,观察给与L Arg、一氧化氮合酶 (NOS)抑制药物左旋精氨酸甲酯 (L NAME)后不同时间移植心脏冠状血管的改变。结果 L Arg组大鼠无移植物血管病 (CAV)的形成和一氧化氮 (NO)能大量合成 ,L NAME组大鼠有CAV形成。结论 NOS抑制药物L NAME加重移植后移植物血管病病变 ,L Arg可以预防和减轻移植后移植物血管病的病变 。

同种异体心肺联合移植术一例

于１９９２年２月９日为１例原发性肺动脉高压并进行性心力衰竭垂危患者作了心肺联合移植术。方法全麻、中低温、全心肺转流下进行同种异体全心肺联合移植术。结果术中顺利，心脏自动复跳，血流动力学稳定，血液分析正常。患者术后１３０分钟后神志清醒，第３天拔去胸腔引流管，第４天出现血氧饱和度急速下降，第１７天多器官功能衰竭死亡。结论缺乏监测手段和心肺联合移植经验，将严重全身性霉菌感染误诊为排斥反应。

内源性应激损伤对移植后大鼠心脏病变的影响(英文)

目的:应激效应在多种心脏疾病的发生、发展中发挥重要作用。本研究探讨在心脏移植后慢性排斥反应期,是否存在应激效应对心肌和冠状动脉的损伤。方法:采用Ono模型建立大鼠心脏移植,采用蛋白质组技术比较同基因移植与异基因移植后2周、8周左室心脏组织的蛋白质变化,通过基质辅助激光解吸电离飞行时间质谱(MALDI-TOF-MS)分析获得肽质量指纹图谱,经Matrix Science查询软件搜索获得匹配的蛋白质。结果:异基因移植心脏在术后2周即出现血管内膜增厚[(2.07%±0.93%)vs.(27.58%±11.14%),P<0.01)],在术后8周更明显[(2.34%±1.06%)vs.(72.29%±20.57%),P<0.01)];蛋白质组学技术分析左室心肌,发现了45个差异表达的蛋白质;通过数据库鉴定得到37种蛋白质,其中9个与应激和损伤相关蛋白质,进一步使用Western印迹验证了其中的2个。结论:移植后心肌持续受到应激效应的损伤可能是大鼠心脏移植后冠状动脉病变发生发展的一个重要原因。

大鼠腹腔心脏移植术后移植物血管病模型的建立

目的探讨建立大鼠腹腔心脏移植物血管病动物模型的方法。方法将40只W istar大鼠和40只SD大鼠随机配对分为对照组和实验组,建立大鼠的异位心脏移植;对照组不注射环孢霉素A(C sA),实验组腹腔注射小剂量的C sA,两组分别于移植术后2周和4周切取移植心脏,在光学显微镜下观察移植心脏冠状血管的改变。结果对照组术后2周和4周冠状血管内膜无变化;实验组术后2周冠状血管内膜增厚,4周后冠状血管内膜成同心圆样改变,管腔明显狭窄,出现移植后移植物血管病改变。结论该模型是一种可靠的移植物血管病的动物模型。

应用彩色多谱勒超声心动图监测心脏移植术后排斥反应

目的 评价超声心动图在监测心脏移植术后急性排斥反应中的作用。方法 采用Accuson型彩色多谱勒超声心动图诊断仪，应用M型超声观察室壁厚度及活动度、有无心包积液；应用B型超声观察各房室腔大小；用脉冲多谱勒频谱测E峰峰值流速、A峰峰值流速及E/A值，连续观察120 d后行心内膜心肌活检（EMB）。结果 超声心动图连续监测4个半月未发现排斥反应征象，心脏结构、功能正常。结论 动态应用超声心动图监测心脏移植后早期急性排斥反应的发生具有安全、迅速、无创、无并发症的优点，同EMB相比有明显优越性。

茵陈五苓散对小鼠心脏移植排斥反应的抑制作用

目的探讨中药茵陈五苓散对大鼠心脏移植排斥反应抑制作用的效果及机制。方法将实验动物随机分为两组,即对照组与实验组,腹部触诊观察移植心脏存活时间,移植7天后部分心脏做病理检查,取脾脏行脾细胞培养,并检测脾细胞培养液中白细胞介素(IL)2、4、6及干扰素(IFN)-γ的浓度。结果与对照组相比,实验组心脏移植物存活时间明显延长(P<0.05),病理显示明显抑制了心脏移植物血管病变,且脾细胞培养液中IL-2、IL-4、IL-6浓度无差别,但IFN-γ的浓度明显降低(P<0.05)。结论茵陈五苓散能明显地延长大鼠心脏移植物的存活时间。

同种心脏移植急性排斥反应机制研究进展

同种原位心脏移植已成为临床治疗终末期心脏病的有效方法 ,供心保存、外科手术技术、术后感染已不再是阻碍心脏移植成功的最主要因素。影响心脏移植成败 ,术后病人的生存期以及生存质量的主要因素是术后免疫排斥反应。因此 ,对心脏移植急性排斥反应的发生机制的研究便显得尤为重要。本文就其基本理论 ,目前研究现状及进展进行探讨和综述。

同种瓣的生物活性与耐久性

液氮保存的同种瓣具有生物活性 ,在临床应用中显示了良好的近中期效果 ,但长期耐久性还有待提高。研究表明 ,同种瓣的供者来源、热缺血时间、灭菌时间和温度、灭菌液的配方、保存方法均能影响瓣膜的生物活性。有活性的同种瓣临床应用效果和使用寿命明显优于无活性的同种瓣 ,在移植后能诱发机体产生供体特异性的体液免疫和细胞免疫反应。瓣膜中存活的成纤维细胞和移植免疫反应与同种瓣耐久性的关系目前意见尚未统一。同种瓣植入的手术方式、供者瓣膜尺寸、宿主因素 (年龄、体重、健康状态 )等均能影响同种瓣的耐久性。

大鼠腹腔异位心脏移植及移植物血管病模型的建立

目的探讨建立大鼠腹腔异位心脏移植及移植物血管病模型的方法和意义。方法将健康Witar大鼠和SD大鼠,建立腹腔异位心脏移植模型。分对照组、实验组和同系移植组,实验组腹腔注射CsA,对照组和同系移植组注射生理盐水。术后15、60d切取供心,观测移植物冠状血管的病理变化。结果大鼠腹腔异位心脏移植成功建立,手术成活率90%。实验组术后15d出现冠状血管内膜增厚,60d出现明显的移植物血管病理改变。结论建立Witar大鼠和SD大鼠腹腔异位心脏移植,可复制出移植物血管病病理变化,是一种理想的移植物血管病实验模型。

大鼠异位移植心脏的心肌、血管病变观察与研究

目的 :探讨在心脏移植中心肌及血管病变的发生和发展情况 ,为预防和治疗移植排斥反应提供理论依据。方法 :采用颈部心脏移植模型 ,用供体脾细胞 (SPC)和环磷酰胺 (CP)预处理受体 ,H E、Masson三色、VanGieson和免疫组化平滑肌细胞染色 ,对移植心脏的浸润细胞 ,心肌纤维化和移植心脏动脉硬化进行分析研究。结果 :经SPC和CP预处理后 ,移植心脏的存活时间明显延长 ,炎性细胞浸润 ,心肌纤维化和心脏动脉硬化明显减轻。结论 :①急性排斥反应时 ,移植心脏内大量炎性细胞浸润 ;②炎性细胞浸润是由心外膜心肌开始逐渐向心内膜方向发展 ;③SPC和CP联合预处理 ,可以预防和减缓移植心脏心肌纤维化和心脏动脉硬化。

肝细胞生长因子对大鼠心脏移植细胞凋亡的影响

目的探讨肝细胞生长因子(HGF)对大鼠心脏移植后细胞凋亡的影响。方法建立大鼠异位心脏移植模型,将32只受体SD大鼠随机分为两组:对照组术后注射生理盐水1 ml.kg-1.d-1;实验组术后15 d注射HGF50μg.kg-1.d-1。用HE染色和TUNEL技术检测移植心脏切片进行排斥反应的病理分级,计算凋亡指数,并观察移植存活时间。结果与对照组比较,HGF能明显减少心肌细胞凋亡(P<0.05),减轻移植物的组织损伤,延长移植物存活时间(P<0.05)。结论外源性HGF能抑制移植心脏细胞凋亡,发挥抗排斥反应作用,显著延长移植物存活时间。

心脏移植的发展现状和新挑战

心脏移植是终末期心力衰竭患者的首选治疗。供者不足一直以来都是限制心脏移植数量增长的主要问题,随着新技术的不断更新和引入,供者池被不断扩大,比如使用年龄较大的供者、丙型肝炎病毒感染的供者、毒品过量致死的供者或心脏死亡器官捐献(DCD)供者的心脏等。与此同时,高龄、多器官功能不全、机械循环支持及人类白细胞抗原抗体致敏受者的比例近几年明显增加。供者数量的不足、受者状况的复杂化、免疫抑制治疗的个体化管理和远期移植物血管病的防治等都是心脏移植领域面临的挑战。本文通过概述现今全球在扩大供者库、提高受者质量、加强排斥反应的诊治和心脏移植物血管病变的预防等方面的新进展,以期有助于改善在等待或已经接受心脏移植的终末期心力衰竭患者的生存时间和生活质量。

同种异体心脏移植长期存活(附1例报告)

目的 介绍我院首例同种异体原位心脏移植术的围手术期处理及排斥反应监测、治疗经验。方法 切取供体（24岁男性脑死亡者）心脏并原位移植给受体（43岁女性终末期扩张性心肌病患者），并在术后进行严格的监护治疗和随防。供心手术历时50 min，移植心脏热缺血时间为0 min，冷缺血时间为70 min；受体手术历时290 min，体外循环总时间123 min，主动脉阻断73 min。术后采用FK 506，骁悉及泼尼松行免疫抑制治疗，同时用彩色多普勒超声心动图监测排斥反应。结果 患者现已健康生存160 d，心、肝、肾功能正常。结论 心脏移植是治疗终末期心脏病的最有效方法，术后处理是确保心脏移植成功的关键。