降钙素基因相关肽参与缺血预处理减轻肾损伤的迟发保护作用

继１９８６年Ｍｕｒｙ等发现多次短暂的缺血再灌流（Ｉｓｃｈｅｍｉｃｒｅｐｅｒｆｕｓｉｏｎ,ＩＲ）的刺激,可使心肌在即后经历的长时性ＩＲ中得到保护而提出缺血预处理（Ｉｓｃｈｅｍｉｃｐｒｅｃｏｎｄｉｔｉｏｎｉｎｇ,ＩＰＣ）的概念以后,Ｍａｒｂｅｒ等表明ＩＰ...     

SMT对大鼠在体心脏缺血-再灌注损伤超微结构的保护作用

目的：研究ＳＭＴ对心脏缺血－再灌注损伤（ＩＲＩ）心肌超微结构的影响。方法：ＳＤ大鼠１８只,体重３２０￣３８０ｇ,随机分为三组：①缺血－再灌注组（ＩＲ）：夹闭冠状动脉左前降支６０ｍｉｎ,松夹２０ｍｉｎ。②缺血－再灌注＋ＳＭＴ组（ＳＭＴ）：再灌注前５ｍｉｎ,股静脉注射ｉＮＯＳ抑制剂Ｓ－ｍｅｔｈｙｌｉｓｏｔｈｉｏｕｒｅａ ｓｕｌｆａｔｅ（ＳＭＴ ５ｍｇ／ｋｇ ｗ）,余同ＩＲ组;③对照组（Ｃ）：暴露心脏后     

缺血-再灌注时大鼠心脏Gi蛋白α亚基的变化

本工作研究了心肌缺血－再灌注时,受体－腺苷酸环化酶细胞膜信号转导系统中Ｇ蛋白含量及功能的变化。采用免疫印迹法和放射免疫法分别测定大鼠心脏Ｇｉα２,Ｇｉα３和Ｇｓα的含量及腺苷酸环化酶的活性。结果显示缺血－再灌注时心功能明显损伤;心脏Ｇｓα无明显变化;心肌细胞膜Ｃｉα２和Ｇｉα３含量分别升高３７．４％（Ｐ〈０．０１）和４２．４％（Ｐ〈０．０１）;胞浆内Ｇｉα２和Ｇｉα３含量无明显变化;缺血心肌腺苷酸     

部分裸子植物叶片总蛋白分析

采用ＳＤＳ－ ＰＡＧＥ 技术, 分析了红豆杉科（Ｔａｘａｃｅａｅ） 植物南方红豆杉（ Ｔａｘｕｓ ｃｈｉｎｅｎｓｉｓｖａｒ－ ｍａｉｒｅｉ （Ｌｅｍｅｅ ｅｔ Ｌｅｖｌ－） Ｃｈｅｎｇ ｅｔ Ｌ－Ｋ－Ｆｕ） 、穗花杉（ Ａｍｅｎｔｏｔａｘｕｓ ａｒｇｏｔａｅｎｉａ （Ｈａｎｃｅ） Ｐｉｌ ｇｅｒ） 、云南穗花杉（ Ａ－ ｙｕｎｎａｎｅｎｓｉｓ Ｌｉ） 、白豆杉（ Ｐｓｅｕｄｏｔａｘｕｓｃｈｉｅｎｉｉ（Ｃｈｅｎｇ） Ｃｈｅｎｇ） 以及三尖杉科（Ｃｅｐｈａｌｏｔａｘａｃｅａｅ） 、植物三尖杉（ Ｃｅｐｈａｌｏｔａｘｕｓ ｆｏｒｔｕｎｅｉ Ｈｏｏｋ－ｆ－） 、粗榧（ Ｃ－ｓｉｎｅｎｓｉｓ （Ｒｅｈｄ－ｅｔＷｉｌｓ－） Ｌｉ） 、海南粗榧（ Ｃ－ｈａｉｎａｎｅｎｓｉｓ Ｌｉ） 、篦子三尖杉（ Ｃ－ｏｌｉｖｅｒｉ Ｍａｓｔ－） 和罗汉松科（Ｐｏｄｏｃａｒｐａｃｅａｅ） 、植 物罗汉松 （ Ｐｏｄｏｃａｒｐｕｓ ｍａｃｒｏｐｈｙｌｌｕｓ （ Ｔｈｕｎｂ－ ） Ｄ－Ｄｏｎ） 、鸡毛 松（ Ｐ－ｉｍｂｒｉｃａｔｕｓ Ｂｌ－） 、竹柏（ Ｐ－ ｎａｇｉ（Ｔｈｕｎｂ－） Ｚｏｌｌ） 、陆均松（ Ｄａｃｒｙｄｉｕｍ ｐｉｅｒｒｅｉ Ｈｉｃｋｅｌ） 共１２ 种植物的叶片蛋白, 在蛋白质水平上采用     

ATP敏感性钾通道在预缺血对麻醉家兔缺血心肌保护中的作用

在氨基甲酸乙酯和戊巴比妥钠两种不同麻醉的家兔心肌缺血－再灌注模型,观察了ＡＴＰ敏感性钾通道开发剂ｃｒｏｍａｋｌｉｍ（Ｃｒｏ）和预缺血（ＩＰ）对血流动力学和心肌梗塞范围的影响,旨在阐明ＫＡＴＰ通道是否与ＩＰ对ＩＲ心肌的保护机制。     

壁山县农田生态系统中氮肥利用与平衡的研究

壁山县农田生态系统中氮肥利用与平衡的研究何新华（云南师范大学生物系,昆明６５００９２）ＮＢａｌａｎｃｅｉｎＡｇｒｏｅｃｏｓｙｓｔｅｍｏｆＢｉｓｈａｎＣｏｕｎｔｙａｆｔｅｒＡｐｐｌｙｉｎｇＮｉｔｒｏｇｅｎｏｕｓＦｅｒｔｉｌｉｚｅｒｓ￥ＨｅＸｉｎｈｕａ（Ｄｅｐａｒｔ－ｍｅｎｔｏｆＢｉｏｌｏｇｙＹｕｎｎａｎＮｏｒｍａｌＵｎｉｖｅｒｓｉｔｙ,Ｋｕｎｍｉｎｇ,６５００９２）．ＣｈｉｎｅｓｅＪｏｕｒｎａｌｏｆＥｃｏｌｏｇｙ,１９９３,１２（５）：２９－３５。Ｔｈｅｉｎｐｕｔａｎｄｏｕｔｐｕｔｏｆｎｉｔｒｏｇｅｎａｎｄｇｒａｉｎｙｉｅｌｄｄｕｒｉｎｇ１９４９－１９８０ｉｎＢｉｓｈａｎＣｏｕｎｔｙａｒｅａｎａｌｙｓｅｄ．Ｔｈｅｒｅｓｕｌｔｓｓｈｏｗｔｈａｔｎｉｔｒｏｇｅｎｃｏｎｓｕｍｐｔｉｏｎｉｓｈｉｇｈｅｒｔｈａｎｉｔｓａｃｃｕｍｕｌａｔｉｏｎ（－３１．６％,＋１４．０％）ａｎｄｔｈｅｒａ－ｔｉｏｏｆｏｒｇａｎｉｃ－Ｎｔｏｃｈｅｍｌｃａｌ－Ｎｉｓｏｂｖｉｏｕｓｌｙｉｎｄｉｓｏｒｄｅｒ（２．００：０．６７）．Ｉｔｉｓｓｕｇｇｅｓｔｅｄｔｈａｔｎｉｔｒｏｇｅｎｂａｌ－ａｎｃｅｃａｎｂｅｍａｉｎｔａｉｎｅｄｔｈｒｏｕｇｈｐｌａ     

B.thuringiensis穿梭载体的构建及cry1C基因的表达

以ＵＣ１９为母体,克隆了Ｂｔ ｋｅｎ－Ａｇ（Ｂ。．ｔｈｒｕｉｎｇｉｅｎｓｉｓ ｓｕｂｓｐ．ｋｅｎｙａｅ Ａｇ）的复制起始区（～１．６ｋｂ）、ｐＵＣ４Ｋ的ａｐｈ１基因,构建成穿梭载体ｐＨＶ－１,ｐＨＶ－１在Ｅ．ｃｏｌｉ中经１００个世代,质粒保持率在８０％以Ｂｔｉ ４Ｑ８（Ｂ．ｔｈｕｒｉｎｇｉｅｎｓｉｓ ｓｕｂｓｐ．ｉｓｒａｅｌｅｎｓｉｓ ４Ｑ８）中经４０个世代,质粒保持率在８０％以上,将Ｂ．ｌｉｃｈ     

朝鲜淫羊藿的化学成分（Ⅱ）

从朝鲜淫羊藿的地上部分分离到七个成分（Ⅰ、Ⅱ、Ⅲ、Ⅳ、Ⅴ、Ⅵ、Ⅶ）。经ＵＶ,ＩＲ,＾１Ｈ－ＮＭＲ,＾１３Ｃ－ＮＭＲ,ＭＳ及化学方法鉴定了它们的结构,分别是ｉｃａｒｉｔｉｎ－３－Ｏ－ａ－Ｌ－ｒｈａｍｎｏｐｙｒａｎｏｓｉｄｅ（Ⅰ）,ｓａｇｉｔｔａｔｏｓｉｄｅ Ａ（Ⅱ）,ｓａｇｉｔｔａｔｏｓｉｄｅ Ｂ（Ⅲ）,３,５,７－ｔｒｉｈｙｄｒｏｘｙｌ－４＾１－ｍｅｔｈｏｘｙ１－８－ｐｒｅｎｙ１－ｆｌａｖｏｎｅ－     

土壤微生物生物量周转的估算

土壤微生物生物量周转的估算高云超,朱文珊,陈文新（北京农业大学生物学院,１０００９４）ＥｓｔｉｍａｔｉｏｎｆｏｒＢｉｏｍａｓｓａｎｄＴｕｒｎｏｖｅｒｏｆＳｏｉｌＭｉｃｒｏｏｒｇａｎｉｓｍｓ￥ＧａｏＹｕｎｃｈａｏ;ＺｈｕＷｅｎｓｈａｎ;ＣｈｅｎＷｅｎｘｉｎ（ＣｏｌｌｅｇｅｏｆＢｉｏｌｏｇｉｃａｌＳｃｉｅｎｃｅｓ,ＢｅｉｊｉｎｇＡｇｒｉｃｕｌｔｕｒａｌＵｎｉｖｅｒｓｉｔｙ,Ｂｅｉｊｉｎｇ１０００９４）．ＣｈｉｎｅｓｅＪｏｕｒ－ｎａｌｏｆＥｃｏｌｏｇｙ,１９９３,１２（６）：６－１０。Ｔｏｏｂｔａｉｎｓｏｍｅｉｎｆｏｒｍａｔｉｏｎａｂｏｕｔｔｒａｎｓｆｏｒｍａｔｉｏｎｏｆｍｉｎｅｒａｌｎｕｔｒｉｅｎｔｓｂｙｓｏｉｌｍｉｃｒｏｏｒｇａｎｉｓｍｓ,ｗｅｈａｖｅｍｅａｓｕｒｅｄｔｈｅａｍｏｕｎｔａｎｄｔｕｒｎｏｖｅｒｒａｔｅｏｆｓｏｉｌｒｎｉｃｒｏｂｉａｌｂｉｏｍａｓｓｉｎｎｏ－ｔｉｌｌａｇｅ,ｄｉｒｅｃｔｄｒｉｌｌｉｎｇａｎｄｐｌｏｗ－ｉｎｇｓｏｉｌｓ．Ｍｉｃｒｏｂｉａｌｂｉｏｒｎａｓｓｉｎｎｏ－ｔｉｌｌａｇｅｔｏｐｓｏｉｌｉｓ５１．７％ａｎｄ２６．０％ｈｉｇｈｅｒｔｈａｎｔｈｏｓｅｉｎｐｌｏｗｉｎｇａｎｄｄｉｒｅｃ     

肾素-血管紧张素系统不参与肝缺血再灌注损伤中的作用

以往实验证实,肾素－血管紧张素系统（ｒｅｎｉｎａｎｇｉｏｔｅｎｓｉｏｎｓｙｓｔｅｍ,ＲＡＳ）在心肌缺血再灌注损伤中起一定的作用。但是否参与肝缺血再灌注损伤（ｈｅｐａｔｉｃｉｓｈｅｍｉａｒｅｐｅｒｆｕｓｉｏｎｉｎｊｕｒｙ,ＨＩＲＩ）的形成,至今国内外...     

下肢骨骼肌缺血后处理对兔缺血/再灌注心肌坏死和凋亡的影响

目的:探讨在体情况下,骨骼肌缺血后处理对兔缺血/再灌注心肌坏死和凋亡的影响。方法:新西兰大白兔36只,随机分成3组(每组随机选取6只进行梗死范围的测定,另外6只进行凋亡测定):①假手术组(Sham组);②缺血/再灌注组(I/R组);③远端后处理组(RPostC组)。在缺血前、后及再灌注60 min、120 min分别抽血测定肌酸激酶(CK),乳酸脱氢酶(LDH)的活性。采用伊文思兰(evans blue)和三苯基氯化四氮唑(TTC)染色方法确定心肌缺血区范围以及心肌坏死区范围。用Tunel法检测兔心肌缺血区细胞凋亡情况,免疫组织化学方法检测心肌缺血区蛋白caspase-3、Bcl-2及Bax的表达。结果:RPostC组心肌坏死程度、再灌注末CK活性较I/R组明显减低。RPostC组缺血区心肌Tunel阳性指数显著低于I/R组(21.79%±1.07%vs35.81%±1.10%,P<0.05)。而RPostC组缺血区心肌细胞caspase-3阳性指数显著低于I/R组(25.03%±1.16%vs39%±2.43%,P<0.05)。与Sham组比较,I/R组及RPostC组Bax蛋白表达指数、Bcl-2蛋白表达指数均升高;但RPostC组的Bax/Bcl-2比值降低,而I/R组的Bax/Bcl-2比值升高。与I/R组相比较,RPostC组Bax蛋白表达指数及Bax/Bcl-2比值显著降低,Bcl-2表达指数显著升高,差异均有统计学意义。结论:远端后处理能够明显的减少缺血/再灌注心肌细胞的坏死和凋亡,其减轻心肌细胞凋亡的机制可能与抑制促凋亡基因caspase-3的活化及Bcl-2表达的上调有关。     

Local Arginase Inhibition during Early Reperfusion Mediates Cardioprotection via Increased Nitric Oxide Production

Consumption of L-arginine contributes to reduced bioavailability of nitric oxide (NO) that is critical for the development of ischemia-reperfusion injury. The aim of the study was to determine myocardial arginase expression and activity in ischemic-reperfusion myocardium and whether local inhibition of arginase within the ischemic myocardium results in increased NO production and protection against myocardial ischemia-reperfusion. Anesthetized pigs were subjected to coronary artery occlusion for 40 min followed by 4 h reperfusion. The pigs were randomized to intracoronary infusion of vehicle (n = 7), the arginase inhibitor N-hydroxy-nor-L-arginine (nor-NOHA, 2 mg/min, n = 7), the combination of nor-NOHA and the NO synthase inhibitor N^G-monomethyl-L-arginine (L-NMMA, 0.35 mg/min, n = 6) into the jeopardized myocardial area or systemic intravenous infusion of nor-NOHA (2 mg/min, n = 5) at the end of ischemia and start of reperfusion. The infarct size of the vehicle group was 80±4% of the area at risk. Intracoronary nor-NOHA reduced infarct size to 46±5% (P<0.01). Co-administration of L-NMMA abrogated the cardioprotective effect mediated by nor-NOHA (infarct size 72±6%). Intravenous nor-NOHA did not reduce infarct size. Arginase I and II were expressed in cardiomyocytes, endothelial, smooth muscle and poylmorphonuclear cells. There was no difference in cytosolic arginase I or mitochondrial arginase II expression between ischemic-reperfused and non-ischemic myocardium. Arginase activity increased 2-fold in the ischemic-reperfused myocardium in comparison with non-ischemic myocardium. In conclusion, ischemia-reperfusion increases arginase activity without affecting cytosolic arginase I or mitochondrial arginase II expression. Local arginase inhibition during early reperfusion reduces infarct size via a mechanism that is dependent on increased bioavailability of NO.     

刺槐素对大鼠心肌缺血再灌注损伤的保护作用与机制研究

摘要 目的：探讨刺槐素对大鼠心肌缺血再灌注损伤(MIRI)的作用以及可能的作用机制。方法：对24只Sprague-Dawley (SD)大鼠进行随机分组,分为：假手术组、模型组、刺槐素给药组、刺槐素+AG490给药组,每组6只,通过结扎冠状动脉左前降支,缺血30 min,再灌注120 min复制心肌缺血再灌注损伤模型。利用氯化三苯基四氮唑测定心肌梗死面积,紫外分光光度计和酶联免疫法检测血清中肌酸激酶同工酶（CK-MB）、乳酸脱氢酶（LDH）的活性,蛋白印迹法分别检测心肌组织中Bcl-2、Bax、Stat3和p-Stat3蛋白相对表达水平。结果：与假手术组比较,模型组大鼠血清中CK-MB、LDH活性明显升高（P＜0.01）,心肌梗死面积百分比显著增加（P＜0.01）,p-Stat3/Stat3比率、Bcl-2/Bax比率显著下降（P＜0.01）;与模型组相比,刺槐素给药组中CK-MB、LDH的活性,以及心肌梗死面积百分比显著降低（P＜0.01）,Bcl-2/Bax比率和p-Stat3/Stat3比率显著提高（P＜0.05）。然而在刺槐素+AG490药物组中刺槐素对于受损心肌的保护作用被AG490消除。结论：刺槐素可减轻MIRI大鼠心肌损伤,发挥心肌保护作用,其机制可能与活化Jak2/Stat3信号通路进而抑制心肌细胞凋亡有关。     

Balanced expression of mitochondrial apoptosis regulatory proteins correlates with long-term survival of cardiac allografts

Abnormal regulation of apoptosis is observed in ischemic injury and may contribute to the pathogenesis of atherosclerosis. However, its role in cardiac allograft vasculopathy (CAV), the fundamental lesion of chronic rejection (CR) in heart transplantation, remains uncertain. To clarify this issue, apoptosis was quantitated in myocardium and coronary arteries from 5 cardiac allograft donors (NL) and explanted hearts of 24 patients with ischemic cardiomyopathy (IsCM) and 15 patients with CR. Tissue samples were analyzed via end-labeling fragmented DNA [via deoxynucleotidyl transferase-mediated dUTP nick end-labeling (TUNEL)] and immunoblotting for activated caspase-3 and -9. Myocyte apoptosis assessed by TUNEL was similarly increased over NL (0.21%) in both the CR (0.88%; P < 0.01) and IsCM (0.88%; P < 0.01) groups. Activated caspase-9 levels were significantly higher in CR (14.7%) compared with IsCM (6.9%; P < 0.01) and NL (0%) groups, whereas activated caspase-3 levels were similarly elevated in both CR and IsCM (7.8 and 6.5% vs. 0% in NL; P < 0.01 and P < 0.05) groups. Expression of myocardial Bcl-2 and Bax was increased in CR compared with both NL (Bax, 4.3-fold; P < 0.01; Bcl-2, 5.9-fold; P < 0.01) and IsCM (IsCM: Bax, 2.2-fold; P < 0.05; Bcl-2, 3.2-fold; P < 0.01) groups. The rate of apoptosis and the Bcl-2/Bax ratio independently correlated to graft survival in CR (activation of caspase-9: r = 0.87; P < 0.01; Bcl-2/Bax: r = 0.57; P = 0.05). Compared with native atherosclerosis, coronary arteries with CAV showed more medial apoptosis (7.8-fold; P < 0.01) and higher Bcl-2 levels (5.1-fold; P < 0.01) with lower Bax levels (threefold; P < 0.05) in the intima. These results indicate that abnormal Bcl-2 and Bax expression in myocardium and coronary arteries of cardiac allografts with CR is distinct from that in IsCM and suggest that balancing Bcl-2 to Bax in transplanted hearts promotes long-term graft survival.     

Cardioprotective effect of rosuvastatin in vivo is dependent on inhibition of geranylgeranyl pyrophosphate and altered RhoA membrane translocation

Hydroxymethyl glutaryl (HMG)-coenzyme A (CoA) reductase inhibitors (statins) protect the myocardium against ischemia-reperfusion injury via a mechanism unrelated to cholesterol lowering. Statins may inhibit isoprenylation and thereby prevent activation of proteins such as RhoA. We hypothesized that statins protect the myocardium against ischemia-reperfusion injury via a mechanism involving inhibition of geranylgeranyl pyrophosphate synthesis and translocation of RhoA to the plasma membrane. Sprague-Dawley rats were given either the HMG-CoA reductase inhibitor rosuvastatin, geranylgeranyl pyrophosphate dissolved in methanol, the combination of rosuvastatin and geranylgeranyl pyrophosphate, rosuvastatin and methanol, or distilled water (control) by intraperitoneal injection for 48 h before ischemia-reperfusion. Animals were anesthetized and either subjected to 30 min of coronary artery occlusion followed by 2 h of reperfusion where at infarct size was determined, or the expression of RhoA protein was determined in cytosolic and membrane fractions of nonischemic myocardium. There were no significant differences in hemodynamics between the control group and the other groups before ischemia or during ischemia and reperfusion. The infarct size was 80 +/- 3% of the area at risk in the control group. Rosuvastatin reduced infarct size to 64 +/- 2% (P<0.001 vs. control). Addition of geranylgeranyl pyrophosphate (77 +/- 2%, P<0.01 vs. rosuvastatin) but not methanol (65 +/- 2%, not significant vs. rosuvastatin) abolished the cardioprotective effect of rosuvastatin. Geranylgeranyl pyrophosphate alone did not affect infarct size per se (84 +/- 2%). Rosuvastatin increased the cytosol-to-membrane ratio of RhoA protein in the myocardium (P<0.05 vs. control). These changes were abolished by addition of geranylgeranyl pyrophosphate. We conclude that the cardioprotection and the increase of the RhoA cytosol-to-membrane ratio induced by rosuvastatin in vivo are blocked by geranylgeranyl pyrophosphate. The inhibition of geranylgeranyl pyrophosphate formation and subsequent modulation of cytosol/membrane-bound RhoA are of importance for the protective effect of statins against myocardial ischemia-reperfusion injury.     

人参皂甙 Rb1对大鼠缺血再灌注心肌细胞Bcl-2、Bax、Bad、Fas基因表达的影响

目的观察人参皂甙Rb1对缺血再灌注心肌细胞Bcl-2、Bax、Bad、Fas基因表达的影响.方法结扎/松解Wistar大鼠左冠状动脉前降支,建立大鼠缺血再灌注动物模型,免疫组化法检测Bcl-2、Bax、Bad、Fas基因的蛋白表达,并利用图象分析系统测量蛋白阳性表达区域平均光密度值,进行定量分析.结果缺血再灌注组及Rb1治疗组Bcl-2、Bax、Bad、Fas基因的表达较假手术组明显增加(P<0.05), Rb1治疗组Bcl-2的表达与缺血再灌注组比较无明显差异(P>0.05),而Bax、Bad、Fas的表达明显下降(P<0.05),人参皂甙Rb1治疗组Bcl-2/Bax、Bcl-2/Bad以及Bcl-2/Fas比值均较假手术组与缺血再灌注组明显增加.结论人参皂甙Rb1治疗可以抑制缺血再灌注心肌细胞中促凋亡基因Bax、Bad、Fas的表达,并使Bcl-2/Bax、Bcl-2/Bad以及Bcl-2/Fas比值增加.     

心肌缺血预适应循环血中微囊泡对大鼠心肌I/R损伤的作用

目的：研究心肌缺血预适应（IPC）大鼠循环血中微囊泡（MVs）对大鼠在体心肌缺血/再灌注（I/R）损伤的作用及相关机制。方法：反复短暂结扎/松开大鼠冠状动脉左前降支建立大鼠IPC模型,自腹主动脉取血,超速离心法分离循环血中的IPC-MVs,并对其进行流式鉴定。建立在体大鼠心肌I/R模型,股静脉注射IPC-MVs 7 mg/kg。HE染色观察心肌形态学变化,TTC染色检测心肌梗死范围,TUNEL染色检测心肌细胞凋亡率。比色法测定血清乳酸脱氢酶（LDH）活力,分光光度法测定心肌组织caspase 3活力,Western blot法检测心肌组织Bcl-2、Bax蛋白表达水平。结果：流式细胞术检测IPC-MVs浓度为4380±745个/μl。与I/R组比较,IPC-MVs能够减轻I/R大鼠心肌组织损伤,缩小心肌梗死范围（P<0.01）,减少心肌细胞凋亡数量（P<0.01）,明显降低血清LDH活力（P<0.01）,降低心肌组织caspase 3活力（P<0.01）,升高Bcl-2蛋白表达（P<0.01）,降低Bax蛋白表达（P<0.01）,升高Bcl-2/Bax比值（P<0.01）。结论：IPC-MVs显著减轻大鼠在体心肌I/R损伤,通过上调心肌组织中Bcl-2的蛋白表达,下调Bax的蛋白表达,升高Bcl-2/Bax比值,降低caspase 3活力而发挥心肌保护作用。     

急性力竭运动后小鼠肾细胞凋亡水平的变化及牛磺酸的保护作用

为探讨急性力竭运动后小鼠(Mus musculus)肾细胞凋亡水平的时相性变化及牛磺酸对肾的保护作用,将56只雄性小鼠随机分为对照组、力竭运动组(分为运动后即刻组、12h组、24 h组和48 h组)及牛磺酸运动组(分为12h组和24 h组),每小组8只,一次性力竭游泳运动后检测肾细胞凋亡水平、Bcl-2和Bax蛋白表达、一氧化氮(NO)含量及结构型一氧化氮合酶(cNOS)、诱导型一氧化氮合酶(iNOS)活性的变化.结果显示,力竭运动后各组小鼠肾细胞凋亡水平呈先升高后下降的趋势,其中运动后24 h组的凋亡水平达峰值(P＜0.05).与对照组相比,运动各组Bax表达均显著增强(P＜0.05).除运动后即刻组外,运动各组Bcl-2表达显著减弱(P＜0.05).各组Bax/Bcl-2比值显著升高,并在运动后24 h达峰值(P＜0.01),后出现下降趋势.小鼠力竭游泳后24 h和48 h肾组织NO含量显著高于对照组(P＜0.05),同时iNOS活性升高(P＜0.01),cNOS活性无显著性变化.相比同时刻运动组,牛磺酸运动组小鼠肾细胞凋亡水平、Bax表达及Bax/Bcl-2比值、iNOS活性显著降低(P＜0.05),Bcl-2表达显著升高(P＜0.05).以上结果表明,急性力竭运动可导致肾细胞凋亡的发生,iNOS、Bax、Bcl-2水平及Bax/Bcl-2比值可能在肾细胞凋亡的发生过程中发挥重要的介导作用.牛磺酸可通过调控iNOS活性及Bax/Bcl-2比值,抑制急性力竭运动后小鼠肾细胞凋亡的发生.     

Lactate accumulation rather than ATP depletion predicts ischemic myocardial necrosis: implications for the development of lethal myocardial injury

In ischemia, the myocardial metabolic status determines the expansion of necrosis. Decreased ATP levels and increased lactate contents in ischemic myocardium undergoing lethal injury are known to be related to the expansion of irreversible damage. However, their individual contributions have not yet been firmly established. Using two differently effective protocols of ischemic preconditioning (IP short and IP long), ischemic cardioplegic arrest (CP) and their combination (IP+CP) to directly influence the metabolic status of porcine myocardium, graded preservations in ATP content and decreases in lactate accumulation during 45 min ischemia could be achieved (control: ATP, 0.15+/-0.03; lactate, 60.53+/-4.89 micromol/g wet weight; IP short, 0.33+/-0.10/27.42+/-3.90; IP long, 0.60+/-0.10/17.49+/-2.14; CP, 0.98+/-0.12/11.82+/-0.96; IP+CP, 2.24+/-0.28/10.88+/-0.89; all P<0.001 vs. control). At the same time, a graded reduction of myocardial necrosis was observed (90.0+/-3.1 vs. 31.7+/-4.55 vs. 5.05+/-2.1 vs. 0.0 [isolated patchy necroses] vs. none). Regression analysis revealed only a weak correlation of infarct size and ATP preservation (r=0.567). In fact, there was a biphasic relation: with ATP levels above 1 micromol/g wet weight, no infarction occurred. ATP levels below this threshold value were associated with steep increase in infarct size. However, even for this latter range, the regression coefficient remained low (r=0.654). Instead, over the entire range, there was a close, rectilinear correlation of infarct size and lactate accumulation (r=0.939). These data indicate that lactate accumulation rather than ATP depletion determines the development of lethal myocardial injury. However, the biphasic relation between ATP depletion and infarct size suggests the latter to play a permissive role, since above a threshold value of 1 micromol/g wet weight neither substantial lactate accumulation nor infarction was observed. Below this threshold, however, infarct size increased as lactate accumulated.