Calpains抑制剂对离体大鼠海马脑组织切片CA1区神经元缺氧/复氧性损伤的影响

目的研究Calpains抑制剂PD150606对离体大鼠海马脑组织切片CA1区神经元缺氧性损伤的 影响。方法将大鼠海马脑组织切片随机分为单纯缺氧(Con)组(n=6)、PD150606(PD)组(n=10)、二甲亚枫 (DMSO)组(n=8)。Con组的海马脑组织切片应用正常的人工脑脊液(aCSF)在37℃孵育60分钟,而PD组、DM- SO组的海马脑组织切片分别给用含有50μmol／L的PD150606或O.3％DMSO的aCSF孵育60分钟,所有脑片 均缺氧5分钟,复氧60分钟。分别记录用药前及缺氧前膜电位、缓慢去极化的速率、快速去极化时间及快速去极 化的幅度、复氧60分钟神经元的膜电位及神经元对细胞内注入电流及对Schaffer旁路刺激的反应。计算复氧60 分钟海马CA1区PI阳性神经元细胞数。结果PD组神经元的快速去极化时间为(299±43)秒,显著高于DMSO 组的(24.6±73)秒和Con组的(257±25)秒(P均<0.05);PD组8例在复氧60分钟后膜电位逐渐恢复到基础值 水平,并对细胞注入电流及经Schaffer旁路刺激可以产生高幅度、持续时间短的动作电位。此外,PD组海马CA1 区PI阳性神经元死亡数量为(78±15)个／mm,明显少于DMSO组的(180+22)个／mm和Con组的(198±20)个 ／mm(P均<0.05)。结论PD150606可以显著减轻大鼠海马CA1区神经元缺氧性损伤,减少缺氧／复氧后神经 元的死亡,促进复氧后神?

线粒体calpains与细胞凋亡关系的研究进展

calpains是一类由Ca2+激活的内源性半胱氨酸蛋白酶。尽管先前研究认为calpains是一种胞质酶,最近研究发现μ-calpain、m-calpain、calpain10以及内源性抑制剂calpastatin也同时存在于线粒体中,在caspase依赖型和非依赖型细胞凋亡通路中均发挥着重要的作用。calpain除了与caspase相互作用外,还可剪切凋亡相关蛋白如Bcl-2、Bax、Bid等,促进Cyt-C、AIF的释放,从而参与调控细胞凋亡的病理过程。calpains作为潜在的治疗靶点,研究线粒体calpains与细胞凋亡通路的关系具有重大意义。

慢性阻塞性肺疾病模型大鼠骨骼肌中Calpains的表达

目的:探讨Calpains在慢性阻塞性肺疾病(COPD)大鼠骨骼肌萎缩中的作用。方法:40只健康雄性Wistar大鼠随机分为COPD模型组及对照组,模型组采用气管内注入脂多糖加香烟烟雾染毒法建立大鼠COPD模型,HE染色法观察肺组织及骨骼肌(趾长伸肌、膈肌)组织的病理学改变;分别采用免疫组化和RT-PCR法测定骨骼肌组织中Calpains(μ-Calpain和m-Calpain)蛋白及mRNA的表达。结果:在COPD模型组大鼠观察到骨骼肌萎缩,对照组大鼠未见骨骼肌萎缩。与对照组比较,COPD模型组大鼠趾长伸肌及膈肌中μ-Calpain和m-Calpain蛋白及m-Calpain mRNA表达增强(P<0.05),而μ-Calpain mRNA的表达差异无统计学意义(P>0.05)。结论:Calpains在COPD模型大鼠骨骼肌中表达上调,可能参与COPD模型大鼠骨骼肌萎缩。

Long-term application of diethylstilbestrol upregulates expressions of μ-and m-calpains in pituitary intermediate lobe of female Wistar rats

BACKGROUND： During formation of prolactin neoplasia, how cells and its structure in adenohypophysis affect prolactin cells should be further studied. Intermediate lobe can be regarded as a driving region to release prolactin （PRL） and may promote formation of prolactin neoplasia in pituitary anterior lobe. OBJECTIVE： To observe the effect of diethylstilbestrol （DES） on the expressions of μ and m-calpains in pituitary intermediate lobe of female Wistar rats. DESIGN： Observational contrast animal study. SETTING： Beijing Neurosurgical Institute. MATERIALS： A total of 21 female Wistar rats, 3 weeks old weighing 70-80 g were housed with free access to tap water and standard pellet food. They were kept in a CL-grade condition, at （24±1）℃ and a humidity of （55±5）%, and with a 12 hours day-night cycle. Caprine anti-μ- and m-calpains antibodies were provided by Santa Cruz Biotechnology, CA, USA; rabbit-anti-PRL antibodies by Dako, Denmark; rabbit-anti-ACTH antibody by Boster Company, Wuhan. METHODS： The experiment was carried out in Pathophysiological Department and Animal Laboratory, Beijing Neurosurgical Institute from August 2006 to January 2007. ① Rats were randomly divided into groups with 7 in each group, including vehicle control group, in which rats were injected intraperitoneally with sun-flower seed oil （1 mL/kg, twice a week） for 16 weeks; DES group, where animals were administered with DES （5 mg/kg, twice a week） for 16 weeks; DES ＋ vehicle control group, in which DES was administered for 12 weeks at the same dose with those in DES group, and then was discontinued and replaced by sun-flower seed oil （1 mL/kg, twice a week） for the following 4 weeks. ② At 16 weeks later, pituitary tissue was dealt with HE staining and PRL immunohistochemical examination to observe evoke of tumor; meanwhile, immunohistochemical examination was used to observe expression of PRL of pituitary anterior lobe, expressions of μ- and m-calpains of pituitary intermediate lobe and distribution of adrenocorticotropin. MAIN OUTCOME MEASURES： ① Expression of PRL of pituitary anterior lobe, expressions of μ- and m-calpains of pituitary intermediate lobe and distribution of adrenocorticotropin. ② Morphological observation of pituitary tissue. RESULTS： All 21 rats were involved in the final analysis. ① Results of immunohistochemical examination： Morphological changes of neoplasia in DES group were strongly positive to PRL, and this suggested that formation of prolactin adenoma was observed in pituitary tissue. As compared with vehicle control group, expression of adrenoeorticotropic hormone （ACTH） was increased in both DES group and DES ＋ vehicle control group. In addition, expressions of μ- and m-calpains in pituitary intermediate lobe were higher in DES group than that in vehicle control group. Otherwise, expressions of m-calpains in pituitary intermediate lobe was decreased in DES ＋ vehicle control group, but expression of μ-calpains was still increased. ② Morphological observation of pituitary tissue： Gland tubes were orderly arranged in rats in vehicle control group. Anterior pituitary gland in rats of DES group demonstrated an apparent disappearance of gland tubes and a relatively large-scaled vasculature formation, namely the vascular lake lined by tightly arranged endothelial cells. Local integrated tumor cell arrangements were also detected. In addition, the border between the IL and the anterior lobe was locally blurred. The definite tumor-like changes in pituitary tissueswere confirmed in 6 of 7 female Wistar rats in DES group, and one spontaneous occurrence of tumor formation was found in vehicle control group. In DES ＋ vehicle control group, DES withdrawal led to the subtile emergence of gland tube cavity, although tumor-like cells still existed in 4 of 7 rats, suggesting occurrence of the tumor regression due to the withdrawal of DES. CONCLUSION： A long-term application of DES can enhance the expressions of ubiquitours neutral cysteine protease in pituitary intermediate lobe and this suggests that both of them play a key role in release of hormone and formation of prolactin neoplasia through directly promoting PRL expression and release of neighboring pituitary intermediate lobe.

Calpains与心房颤动的关系

心房颤动 (简称房颤 )的发生发展是一个十分复杂的过程 ,有多种机制参与其中。大量研究表明 ,钙超载是房颤发病的主要机制之一。calpains是一类钙离子依赖性的中性蛋白酶 ,广泛存在于机体的各组织中 ,参与多种生理病理过程。近年来研究表明 ,calpains激活后能够部分降解收缩蛋白 ,引起心肌收缩功能下降 ,并影响心肌细胞结构和通道蛋白水平 ,与房颤心房电重构和结构重构有关。

尿沉渣中钙信号相关mRNA作为IgA肾病足细胞损伤无创性指标的研究

IgA肾病(IgA nephropathy,IgAN)是目前最常见的原发性慢性肾小球疾病,5%~25%的IgAN患者10年内进展为终末期肾脏病(end-stage renal disease,ESRD),需行肾脏替代治疗^([1])。近年来,足细胞在IgAN中,致病作用受到更多关注,足细胞损伤与蛋白尿及IgAN病情进展正相关^([2])。

BmCalpains are involved in autophagy and apoptosis during metamorphosis and after starvation in Bombyx mori

Apoptosis and autophagy play crucial roles during Bombyx mori metamorphosis and in response to various adverse conditions, including starvation. Recently, calpain, one of the major intracellular proteases, has been reported to be involved in apoptosis and autophagy in mammals. BmATG5 and BmATG6 have been identified to mediate apoptosis following autophagy induced by 20-hydroxyecdysone and starvation in B. mori. However, B. mori calpains and their functions remain unclear. In this study, phylogenetic analysis of calpains from B. mori, Drosophila melanogaster and Homo sapiens were performed and the results showed distinct close relationships of BmCalpain-A/B with DmCalpain- A/B, BmCalpain-C with DmCalpain-C, and BmCalpain-7 with HsCalpain-7. Then, the expression profiles of BmCalpains were analyzed by quantitative real-time polymerase chain reaction, and results showed that expression ofBmCalpain-A/B, BmCalpain-C and BmCalpain-7 was significantly increased during B. mori metamorphosis and induced in the fat body and midgut of starved larvae, which is consistent with the expression profiles ofBmAtgS, BmAtg6 and BmCaspase-1. Moreover, the apoptosis-associated cleavage of BmATG6 in Bm-12 cells was significantly enhanced when BmCalpain-A/B and BmCalpain-7 were induced by starvation, and was partially inhibited by the inhibitor of either calpain or caspase, but completely inhibited when both types of inhibitors were applied together. Our results indicated that BmCalpains, including BmCalpain-A/B, -C and -7, may be involved in autophagy and apoptosis during B. mori metamorphosis and after starvation, and may also contribute to the apoptosis-associated cleavage of BmATG6.

The regulatory role of Pin1 in neuronal death

Regulated cell death predominantly involves apoptosis,autophagy,and regulated necrosis.It is vital that we understand how key regulatory signals can control the process of cell death.Pin1 is a cis-trans isomerase that catalyzes the isomerization of phosphorylated serine or threonine-proline motifs of a protein,thereby acting as a crucial molecular switch and regulating the protein functionality and the signaling pathways involved.However,we know very little about how Pin1-associated pathways might play a role in regulated cell death.In this paper,we review the role of Pin1 in regulated cell death and related research progress and summarize Pin1-related pathways in regulated cell death.Aside from the involvement of Pin1 in the apoptosis that accompanies neurodegenerative diseases,accumulating evidence suggests that Pin1 also plays a role in regulated necrosis and autophagy,thereby exhibiting distinct effects,including both neurotoxic and neuroprotective effects.Gaining an enhanced understanding of Pin1 in neuronal death may provide us with new options for the development of therapeutic target for neurodegenerative disorders.

维生素E对帕金森病模型细胞的抗凋亡作用及其机制

目的:探讨维生素E(VE)对1-甲基-4-苯基-吡啶离子(MPP+)诱导的神经元凋亡的保护作用及其可能机制。方法:用重组鼠神经生长因子(nerve growth factor,NGF)对大鼠PC12细胞株进行诱导分化,加入500μmol/L的MPP+制成帕金森病细胞凋亡模型,再给予不同浓度的VE处理细胞;Hoechst 33342染色后通过荧光显微镜观察各组细胞形态;应用流式细胞术观察各组细胞的凋亡率和坏死率;采用蛋白质印迹法检测各组细胞中细胞周期依赖蛋白激酶5(cyclin-dependent kinase 5,CDK5)、calpains的表达。结果:给予NGF后第2天可见PC12细胞突起数量增多、长度变长,细胞胞体变大、形态不规则;随着VE浓度升高,细胞凋亡率明显下降(P<0.01);VE浓度为200μmol/L时细胞活性最高(P<0.01),细胞核固缩和碎裂现象最少见。随着VE浓度升高,PC12细胞内CKD5、calpains的表达逐渐下降。结论:VE通过抑制细胞凋亡通路中calpains通路,在帕金森病细胞模型中发挥神经元保护作用。

电刺激对牛背最长肌中钙激活酶活性及嫩度的影响

通过对中国杂交黄牛(鲁西黄牛×西门塔尔)牛背最长肌中Calpains活性及剪切力值的分析,研究了电刺激对牛背最长肌宰后成熟过程中Calpains活性及牛肉嫩度的影响。结果表明:电刺激显著提高了μ-calpain的活性(P<0.05),降低了calpastatin对μ-calpain的抑制作用,提高了牛背最长肌的嫩度,缩短了牛肉的成熟时间;但电刺激仅在宰后成熟1h,显著提高了m-calpain的活性(P<0.05);宰后成熟24h、3d,与对照组之间差异不显著(P>0.05),试验结果证实,电刺激通过对Calpains体系的影响,改变了牛肉的成熟速度,显著的改善了牛肉的嫩度。

In Silico Evaluation of the Potential Interference of Boceprevir, Calpain Inhibitor II, Calpain Inhibitor XII, and GC376 in the Binding of SARS-CoV-2 Spike Protein to Human Nanobody Nb20

Virtual screening can be a helpful approach to propose treatments for COVID-19 by developing inhibitors for blocking the attachment of the virus to human cells. This study uses molecular docking, recovery time and dynamics to analyze if potential inhibitors of main protease (Mpro) of SARS-CoV-2 can interfere in the attachment of nanobodies, specifically Nb20, in the receptor binding domain (RBD) of SARS-CoV-2. The potential inhibitors are four compounds previously identified in a fluorescence resonance energy transfer (FRET)-based enzymatic assay for the SARS-CoV-2 Mpro: Boceprevir, Calpain Inhibitor II, Calpain Inhibitor XII, and GC376. The findings reveal that Boceprevir has the higher affinity with the RBD/Nb20 complex, followed by Calpain Inhibitor XII, GC376 and Calpain Inhibitor II. The recovery time indicates that the RBD/Nb20 complex needs a relatively short time to return to what it was before the presence of the ligands. For the RMSD the Boceprevir and Calpain Inhibitor II have the shortest interaction times, while Calpain Inhibitor XII shows slightly more interaction, but with significant pose fluctuations. On the other hand, GC376 remains stably bound for a longer duration compared to the other compounds, suggesting that they can potentially interfere with the neutralization process of Nb20.

反复离心运动对大鼠骨骼肌损伤和蛋白质降解机制的影响

目的:探讨连续离心运动训练对骨骼肌中Calpain和Ubiquitin含量的影响及其与骨骼肌损伤之间的关系;方法:雄性SD大鼠29只随机分为对照组、离心训练后即刻组、24h组和7天组。训练组大鼠连续进行7天的下坡跑运动,分别在末次训练后即刻,24h和第7天取股四头肌,测定股四头肌的超微结构、血清LDH和CK活性以及骨骼肌中Calpain-1、Calpain-2和Ubiquitin含量;结果:1)7天离心训练后即刻和24h,股四头肌超微结构的损伤性变化呈渐进性加重,离心训练后24h组出现明显的肌丝坏死。训练后第7天仍不能完全恢复。血清CK和LDH活性的变化与大鼠股四头肌超微结构的变化相一致。2)与对照组相比,末次训练后即刻骨骼肌中Calpain-1、Calpain-2和Ubiquitin含量均显著升高;训练后24h,Calpain-1和Calpain-2含量进一步升高,其中,Calpain-1显著高于对照组和训练后24h组,Calpain-2虽显著高于对照组,但与训练后即刻组相比无显著性差异;而Ubiquitin含量显著低于训练后即刻组。训练后第7天,Calpain-1和Calpain-2含量显著低于训练后24h组,但仍然高于对照组;而Ubiquitin含量虽高于训练后24h组和对照组,但无显著性差异;结论:1)连续的离心运动可能对骨骼肌纤维的损伤产生一定的累加作用;2)短期连续的离心训练后,骨骼肌中Calpain和Ubiquitin的动态变化几乎与骨骼肌超微结构的动态变化相一致。离心运动训练导致骨骼肌中Calpain和Ubiquitin含量的增加,可能是导致骨骼肌累积性损伤的重要机制。

银杏二萜内酯葡胺注射液通过下调calpain信号通路抑制脑缺血神经细胞凋亡

研究银杏二萜内酯葡胺注射液(diterpene ginkgolides meglumine injection DGMI)对缺氧缺糖/复氧(oxygen-glucose deprivation/reoxygenation,OGD/R)损伤的人神经母细胞瘤细胞SH-SY5Y凋亡的抑制作用及其机制。采用试剂盒、Fluo-3 AM法、Western blot检测SH-SY5Y细胞氧糖剥离损伤4h后,与药物一起复氧1h细胞乳酸脱氢酶(LDH)的漏出量、caspase-3/7酶活力、细胞质中核小体含量、胞浆游离钙离子浓度以及calpain、cleaved caspase-12蛋白量的变化。结果显示DGMI能极显著降低OGD/R损伤的SH-SY5Y细胞LDH的漏出量,抑制caspase-3/7酶活性,减少细胞核核小体的释放量,下调细胞内游离钙离子浓度、calpain和cleaved caspase-12蛋白量,抑制calpain凋亡信号通路保护神经细胞。DGMI对OGD/R诱导的SH-SY5Y细胞凋亡具有显著的抑制作用,其作用机制可能与抑制细胞内Ca^(2+)/calpain/caspase-12/capase-3信号通路有关。

Calpain10基因多态性与中国人2型糖尿病遗传易感性的相关性研究

目的 了解 Calpain 10基因对中国汉族人 2型糖尿病遗传易感性的影响。方法 采用病例对照研究方法 ;以聚合酶链式反应 -限制性内切酶长度多态性 (PCR- RFL P)技术 ,对 2 11例 2型糖尿病患者及 12 7例正常对照 Calpain10基因 SNP4 3及 SNP19多态性进行基因分型。结果 同对照组相比 ,SNP4 3的 G等位基因频率在 2型糖尿病人群中显著升高 (91.9% vs 85 .8% ,P=0 .0 1)。但 SNP19位点等位基因频率在上述两组中的频率分布无显著差异。此外 ,本研究还观察到在正常对照组中 ,SNP4 3GG基因型与体重指数和腰 -臀围比值增加相关。结论 Calpain 10基因 SNP4 3位点 G等位基因可直接或与其他糖尿病基因相互作用决定汉族人

Calpain对细胞骨架蛋白tau降解作用的研究(英文)

Calpain是钙依赖性中性蛋白酶 ,根据其对钙敏感性的不同 ,可分为m 和 μ calpain两型 .分别用不同浓度CaCl2 溶液孵育Wistar大鼠脑皮质匀浆液 ,并用蛋白质印迹和定量图像分析技术检测不同亚型calpain对tau蛋白的降解作用 .研究发现 :在 3 7℃用 1mmol/LCa2 + 孵育底物 15min ,可见tau蛋白明显降解 ,并在分子质量为 2 9ku处出现tau蛋白降解片段 ;当Ca2 + 浓度为 5mmol/L时 ,tau蛋白几乎全部被降解 ;这种tau蛋白降解可被calpain特异性抑制剂完全逆转 .进一步的研究发现 ,分别用 μ calpain抑制剂 (0 0 5μmol/Lcalpastatin) ,m calpain抑制剂 (10 0 μmol/LcalpaininhibitorⅣ )或总calpain抑制剂 (552 μmol/Lcalpeptin)与 1mmol/LCa2 + 共同孵育Wistar大鼠脑皮质匀浆液 ,Ca2 + 激活的tau蛋白降解分别被抑制8 6% ,92 5%和 97 8% .结果表明一定浓度的Ca2 + 可同时激活 μ calpain和m calpain ,这两种亚型calpain均参与降解tau蛋白 ,但m calpain的作用比 μ

calpain与细胞凋亡

calpain是钙激活中性蛋白酶,属于半胱氨酸蛋白水解酶超家族成员。是由分子量为80KD的催化亚单位和分子量为30KD的调解亚单位组成的异二聚体。研究最多的是calpain1和2,它们又称μ-calpain和m-calpain。calpain被认为与细胞骨架重塑、信号转导途径、调控细胞周期、基因表达调控、某些凋亡途径以及长程增强效应等有关。calpain参与了细胞凋亡,而calpain抑制剂可以阻止细胞的凋亡。

血管性痴呆小鼠海马CA1区CalpainⅠ表达的变化

目的探讨脑缺血—再灌注后不同时期血管性痴呆(VD)小鼠海马CA1区病理改变及CalpainⅠ表达的变化。方法243只雄性昆明小鼠随机分为假手术组(99只)和模型组(144只),VD动物模型采用双侧颈总动脉反复缺血—再灌注合并尾端放血的方法制备;分别于造模后第4周、6周和8周测试小鼠的学习和记忆成绩,HE染色观察小鼠海马CA1区正常神经元计数,免疫组化方法观察CalpainⅠ的表达。结果造模后4周、6周和8周时模型组小鼠的学习、记忆成绩均明显劣于假手术组小鼠(P<0.05)。假手术组海马CA1区单位面积正常神经元计数分别为(102±15)个、(108±11)个和(101±12)个;模型组分别为(65±19)个、(21±3)个和(50±11)个,较假手术组均显著降低(P<0.05),其中以造模后6周损害最严重,较模型组造模后4、8周时也显著减少(P<0.05)。假手术组造模后4周、6周和8周时小鼠海马CA1区CalpainⅠ的平均OD值分别是0.030±0.003、0.031±0.003和0.029±0.003;模型组CalpainⅠ的平均OD值分别是0.099±0.009、0.121±0.010和0.115±0.010,较假手术组均显著增高(P<0.05),尤以术后6周时增高明显。结论脑缺血—再灌注6周时海马CA1区神经元损害最严重,CalpainⅠ参与了脑缺血—再灌注后小鼠VD的发生。

日本血吸虫Calpain的DNA疫苗诱导小鼠免疫保护性研究

目的 研究日本血吸虫中国大陆株Calpain的DNA疫苗对Balb/c小鼠的免疫保护性作用。方法 大量制备pVAC质粒DNA和pVAC -CalpainDNA疫苗 ,Balb/c小鼠 5 0只 ,随机均分为对照组和实验组 ,对照组每只小鼠的股四头肌注射接种 10 μgpVAC质粒DNA ,实验组以同样方式注射 10 μgpVAC -CalpainDNA疫苗 ,第 3周加强免疫一次。第 4周每只小鼠经腹部皮肤感染 ( 2 5± 1)条尾蚴 ,感染 6周后剖杀 ,从门静脉灌流收集计成虫数、碎脾计T淋巴细胞总数、从各鼠肝脏的同一部位切下小块肝组织 ,置 5 %KOH溶液消化后 ,计算每克肝组织虫卵数 ,比较减虫率、减雌率和减卵率。于免疫前、第一次免疫后 2周和感染后 2周分别从尾静脉采血 ,用ELISA测定抗体水平。结果 与对照组相比 ,实验组获得 36.84%的减虫率、36.36%的减雌率和 43.31%的减卵率 ,感染后实验组小鼠IgG抗体水平升高幅度大于对照组 ,对照组T淋巴细胞数显著多于实验组。结论 CalpainDNA疫苗可诱导小鼠产生较好的免疫保护作用 。

E-64d对大鼠视网膜缺血再灌注损伤中Calpain和Caspase-3表达的调控作用

目的探讨E-64d(半胱氨酸蛋白酶抑制剂及钙激活中性蛋白酶抑制剂)在大鼠视网膜缺血再灌注损伤(RIRI)中对Calpain/Caspase-3表达的调节作用。方法将80只SD大鼠随机分为正常组、视网膜缺血再灌注组、对照组和E-64d治疗组,并分为1、3、6、24、72h5个时间段。通过前房穿刺加压法制成RIRI动物模型,采用Western-blot以及RT-PCR方法测定在大鼠RIRI模型中的Calpian、Caspase-3蛋白和mRNA表达情况。结果缺血再灌注24hm-Calpain、Caspase-3蛋白的表达缺血再灌注组较正常组上升,而E-64d组表达与正常组相似,比缺血再灌注组下降。E-64d能下调视网膜缺血再灌注后m-Calpain/Calpastatin的mRNA比值,在24h与缺血组有显著统计学差异。结论E-64d能降低视网膜缺血再灌注时m-Calpain、Caspase-3蛋白的表达,调控m-Calpain和Calpastatin的mRNA比值。

过敏毒素C5a通过Calpain途径致VEC凋亡损伤

目的探索C5a是否与LPS、毒源性大肠杆菌O157产生的外毒素—V毒素(verotoxin)具有相似的可以导致血管内皮细胞(VEC)凋亡的作用。方法流式细胞仪检测细胞凋亡发生率,首先探讨rhC5a刺激的质量浓度,分别为0.2μg/mL、0.5μg/mL、1μg/mL和1.5μg/mL刺激12 h检测VEC凋亡发生率;在rhC5a质量浓度均为1μg/mL条件下,时间分别为2 h、6 h、12 h、18 h和24 h,检测VEC凋亡发生率。Western blot方法检测凋亡相关蛋白。结果在rhC5a质量浓度为0.2μg/mL、0.5μg/mL、1μg/mL和1.5μg/mL刺激12 h诱导的凋亡发生率分别为4.58%、7.87%、17.94%和19.03%。在确定rhC5a质量浓度1μg/mL的条件下,VEC发生凋亡呈时间依赖关系,在2 h、6 h、12 h、18 h和24 h的时相,细胞凋亡发生率分别为4.58%、12.78%、18.12%、19.08%和19.96%。rhC5a刺激VEC细胞,calpain-2蛋白表达呈时间依赖性,而calpain-1蛋白的表达为浓度依赖性。结论C5a可以导致VEC细胞发生凋亡,calpain参与了这类细胞的凋亡进程。