优化新生脉散方调控β1-AR/cAMP/PKA/CREB信号通路对心力衰竭大鼠心肌纤维化的影响

目的 基于β1-AR/cAMP/PKA/CREB信号通路探讨优化新生脉散方对心力衰竭大鼠心肌纤维化的影响。方法 50只SD大鼠随机分为假手术组10只和手术组40只,采用左冠状动脉前降支结扎法建立心力衰竭大鼠模型。将成模大鼠随机分为模型组、卡托普利组和中药低、高剂量组,每组8只,给药组分别予相应药物灌胃4周。超声心动图测定大鼠左室射血分数(LVEF)、左室短轴缩短率(LVFS),测定心、肺质量并计算心、肺脏器系数,组织病理学观察心肌纤维化程度,ELISA测定血清N端脑利钠肽前体(NT-ProBNP)及心肌组织环磷酸腺苷(cAMP)、Ⅰ型胶原(ColⅠ)、Ⅲ型胶原(ColⅢ)含量,免疫组化检测心肌组织β1肾上腺素受体(β1-AR)、cAMP阳性表达,Western blot检测心肌组织β1-AR/cAMP/PKA/CREB信号通路相关蛋白表达。结果 与假手术组比较,模型组大鼠LVEF、LVFS明显降低(P<0.01),心、肺脏器系数明显升高(P<0.01);心肌细胞数目减少、胶原容积分数升高、Ⅰ/Ⅲ型胶原纤维占比增加(P<0.01),血清NT-ProBNP和心肌组织ColⅠ、ColⅢ含量明显升高,心肌组织cAMP含量明显降低(P<0.01),心肌组织β1-AR和cAMP阳性表达明显降低(P<0.01),β1-AR、腺苷酸环化酶(AC)1、cAMP、p-蛋白激酶A(PKA)、p-环磷腺苷反应元件结合蛋白(CREB)蛋白表达明显降低,p-Smad2、ColⅠ、ColⅢ、α平滑肌肌动蛋白(α-SMA)蛋白表达明显升高(P<0.05,P<0.01)。与模型组比较,给药组不同程度增加大鼠LVEF、LVFS,降低心、肺脏器系数;增加心肌细胞数目、减少胶原容积分数和Ⅰ/Ⅲ型胶原纤维占比,下调血清NT-ProBNP和心肌组织ColⅠ、ColⅢ含量,上调cAMP含量,增加心肌组织β1-AR和cAMP阳性表达,上调β1-AR、AC1、cAMP、p-PKA、p-CREB蛋白表达,抑制p-Smad2、ColⅠ、ColⅢ、α-SMA蛋白表达,其中中药高剂量组和卡托普利组作用更明显(P<0.01,P<0.05)。结论 优化新生脉散方能减轻心力衰竭大鼠心肌纤维化程度,改善心肌肥厚和重构,增加左心室收缩力,其机制可能与激活β1-AR/cAMP/PKA/CREB信号通路有关。

复心合剂对慢性充血性心力衰竭患者淋巴细胞β_1-AR mRNA表达的影响及临床观察

目的:评价具有温阳复心、活血利水作用的复心合剂对慢性心力衰竭(CHF)心阳虚衰证患者淋巴细胞β1-AR mRNA表达的影响及临床治疗效果。方法:60例慢性心力衰竭心阳虚衰证患者,随机分为对照组(缬沙坦组)30例、治疗组(复心合剂组)30例,经6周治疗后,观察患者外周血淋巴细胞β1-AR mRNA表达、6min步行试验(6MWT)、脑钠肽(BNP)及生活质量评分的变化,观察复心合剂改善心衰患者的临床疗效。结果两组心衰患者外周血淋巴细胞β1-AR mRNA表达量较治疗前明显提高(P<0.01);患者6WMT距离较治疗前明显增加(P<0.01),且6WMT心功能分级较治疗前明显改善(P<0.01);患者血浆BNP水平较治疗前明显降低(P<0.01);明尼苏达心力衰竭生活质量评分较治疗前明显降低(P<0.01),患者生活质量明显改善。结论复心合剂能提高心衰患者外周血淋巴细胞β1-AR mRNA的表达,并有效提高CHF患者运动耐量,降低血浆BNP水平,改善生活质量。

分别阻断β_1-和β_2-AR对小鼠胰岛素低血糖休克的影响

分别阻断小鼠 β1 和 β2 AR后进行了加速胰岛素低血糖休克的研究。结果表明 ,对照组的休克率为 4 7 3 % ,潜伏期为 (1 64 8± 3 1 9)min ;阻断 β1 AR组的休克率增加到 74 % (P <0 0 0 5 ) ,潜伏期减少到(1 4 3 8± 4 5 6)min (P <0 0 5 ) ;阻断 β2 AR组的休克率降低到 1 5 3 % (P <0 0 0 5 ) ,潜伏期为 (1 4 9 3±4 9 1 )min (P >0 2 )。证明阻断 β1 AR可加速小鼠的胰岛素低血糖休克 ,而阻断 β2

血清NY-ESO-1自身抗体和MMP1联合检测对食管鳞状细胞癌的诊断价值

目的:探讨血清基质金属蛋白酶-1(matrix metalloproteinase-1,MMP1)和纽约食管鳞状细胞癌抗原-1(New York esophageal squamous cell carcinoma 1,NY-ESO-1)自身抗体联合检测在食管鳞状细胞癌中的诊断意义。方法:应用酶联免疫吸附实验检测120例食管鳞状细胞癌患者和120例正常对照血清中MMP1和NY-ESO-1自身抗体的表达水平,采用受试者工作特征(receiver operating characteristic,ROC)曲线评价诊断效能。结果:血清MMP1和NY-ESO-1自身抗体在食管鳞状细胞癌患者中的表达均明显高于正常对照[(8.070±5.738)ng/mL vs(4.331±3.137)ng/mL,Z=6.214,P<0.001;0.463±0.571 vs 0.156±0.086,Z=5.210,P<0.001]。ROC曲线显示,当血清MMP1为最佳诊断临界值10.586 ng/mL时,其在诊断食管鳞状细胞癌的曲线下面积(area under the ROC curve,AUC)为0.732(95%CI:0.671~0.787),敏感度为24.2%,特异度为95.0%。NY-ESO-1自身抗体诊断食管鳞状细胞癌AUC为0.695(95%CI:0.632~0.752),敏感度为33.0%,特异度为95.0%。MMP1和NY-ESO-1自身抗体联合检测诊断食管鳞状细胞癌的AUC为0.800(95%CI:0.744~0.849),敏感度为47.5%,特异度为95.0%。结论:血清MMP1和NY-ESO-1自身抗体联合检测可能有助于提高食管鳞状细胞癌的诊断效能。

Location-based prediction model for Crohn’s disease regarding a novel serological marker,anti-chitinase 3-like 1 autoantibodies

BACKGROUND Defective neutrophil regulation in inflammatory bowel disease(IBD)is thought to play an important role in the onset or manifestation of IBD,as it could lead to damage of the intestinal mucosal barrier by the infiltration of neutrophils in the inflamed mucosa and the accumulation of pathogens.Like neutrophils in the context of innate immune responses,immunoglobulin A(IgA)as an acquired immune response partakes in the defense of the intestinal epithelium.Under normal conditions,IgA contributes to the elimination of microbes,but in connection with the loss of tolerance to chitinase 3-like 1(CHI3L1)in IBD,IgA could participate in CHI3L1-mediated improved adhesion and invasion of potentially pathogenic microorganisms.The tolerance brake to CHI3L1 and the occurrence of IgA autoantibodies to this particular target,the exact role and underlying mechanisms of CHI3L1 in the pathogenesis of IBD are still unclear.AIM To determine the predictive potential of Ig subtypes of a novel serological marker,anti-CHI3L1 autoantibodies(aCHI3L1)in determining the disease phenotype,therapeutic strategy and long-term disease course in a prospective referral cohort of adult IBD patients.METHODS Sera of 257 Crohn’s disease(CD)and 180 ulcerative colitis(UC)patients from a tertiary IBD referral center of Hungary(Division of Gastroenterology,Department of Internal Medicine,Faculty of Medicine,University of Debrecen)were assayed for IgG,IgA,and secretory IgA(sIgA)type aCHI3L1 by enzyme-linked immunosorbent assay using recombinant CHI3L1,along with 86 healthy controls(HCONT).RESULTS The IgA type was more prevalent in CD than in UC(29.2%vs 11.1%)or HCONT(2.83%;P<0.0001 for both).However,sIgA subtype aCHI3L1 positivity was higher in both CD and UC patients than in HCONT(39.3%and 32.8%vs 4.65%,respectively;P<0.0001).The presence of both IgA and sIgA aCHI3L1 antibodies was associated with colonic involvement(P<0.0001 and P=0.038,respectively)in patients with CD.Complicated disease behavior at sample procurement was associated with aCHI3L1 sIgA positivity(57.1%vs 36.0%,P=0.009).IgA type aCH3L1 was more prevalent in patients with frequent relapse during the disease course in the CD group(46.9%vs 25.7%,P=0.005).In a group of patients with concomitant presence of pure inflammatory luminal disease and colon involvement at the time of diagnosis,positivity for IgA or sIgA type aCH3L1 predicted faster progression towards a complicated disease course in time-dependent models.This association disappeared after merging subgroups of different disease locations.CONCLUSION CHI3L1 is a novel neutrophil autoantigenic target in IBD.The consideration of antibody classes along with location-based prediction may transform the future of serology in IBD.

Enzyme-linked immunosorbent assay of 3 Screen Islet Cell Autoantibody in patients with autoimmune thyroid disease

BACKGROUND In recent years,the emergence of multiplex technology that can simultaneously measure multiple anti-islet autoantibodies has become particularly valuable for the staging and early diagnosis of immune-mediated type 1 diabetes(T1D).While it has been established that 20%-30%of T1D patients suffer from autoimmune thyroid disease(AITD),there is limited available data regarding the presence of anti-islet autoantibodies in AITD patients.Among commercially available anti-islet autoantibodies,glutamic acid decarboxylase 65 autoantibodies(GADAs)are often the first marker measured in general clinical practice.AIM To investigate the frequency of anti-islet autoantibodies in AITD patients.METHODS Our study involved four hundred ninety-five AITD patients,categorized into three distinct groups:AITD with T1D(n=18),AITD with phenotypic type 2 diabetes(T2D)(n=81),and AITD without diabetes(n=396),and the enzyme-linked immunosorbent assay(ELISA)was employed to determine the frequencies of 3 Screen Islet Cell Autoantibody(3 Screen ICA),GADA,insulinoma-associated antigen-2 autoantibodies(IA-2As),and zinc transporter 8 autoantibodies(ZnT8As)within these groups.RESULTS The frequency of 3 Screen ICA in AITD patients with T1D,T2D,and those without diabetes were 88.9%,6.2%,and 5.1%,respectively,with no significant difference seen between the latter two groups.Notably,the frequency of 3 Screen ICA was 11.1%higher in AITD patients with T1D,1.3%higher in AITD patients with T2D,and 1.1%higher in AITD patients without diabetes compared to GADA,respectively.Furthermore,12.5%,20.0%,and 20.0%of the 3 Screen ICA-positive patients were negative for GADA.Additionally,1.3%of the AITD patients who tested negative for 3 Screen ICA in both the AITD with T2D and non-diabetic AITD groups were found to be positive for individual autoantibodies.Among the 3 Screen ICA-positive patients,there was a significantly higher proportion of individuals with multiple autoantibodies in AITD patients with T1D compared to those without diabetes(37.5%vs 5.0%,P<0.05).However,this proportion was similar to that in AITD patients with T2D(20.0%).Nevertheless,there was no significant difference in 3 Screen ICA titers between AITD patients with T1D and those without diabetes(436.8±66.4 vs 308.1±66.4 index).Additionally,no significant difference in 3 Screen ICA titers was observed between Graves’disease and Hashimoto’s thyroiditis in any of the groups.CONCLUSION Our findings reveal that some AITD patients without diabetes exhibit 3 Screen ICA titers comparable to those in AITD patients with T1D.Thus,3 Screen ICA outperforms GADA in identifying latent anti-islet autoantibody-positive individuals among AITD patients.

β_1-AR/CMC-UPLC/MS联用的分析方法筛选辛夷中的活性成分

目的建立高表达的β_1肾上腺素受体细胞膜色谱法(β_1-AR/CMC)与超高效液相-质谱(UPLC/MS)离线联用(β_1-AR/CMC-Offline-UPLC/MS)的分析方法,并从辛夷中筛选对β_1-AR具有抑制作用的活性成分。方法建立β_1-AR/CMC-Offline-UPLC/MS分析方法;采用阳性对照药物美托洛尔(Meto)和阴性对照药物地西泮(DZ)考察分析方法的可行性;用所建立的分析方法分离、筛选、鉴定辛夷提取物中的活性成分。结果建立并验证了β_1-AR/CMC-Offline-UPLC/MS分析方法,并以β_1-AR/CMC系统对辛夷95%乙醇提取物中的活性成分进行筛选,经UPLC/MS鉴定保留组分为辛夷脂素。结论本课题所建立的β_1-AR/CMC-Offline-UPLC/MS分析方法具有灵敏度高、特异性强、稳定性高、分析速度快的特点,能够用于从辛夷中筛选对β1-AR具有抑制作用的活性成分。

良性前列腺增生合并慢性前列腺炎组织中SIgA、α1-AR的表达与意义

目的:了解良性前列腺增生(BPH)合并慢性前列腺炎(CP)组织中SIgA、α1-AR的表达及意义。方法:将62例行经尿道前列腺等离子电切组织标本,根据术前前列腺按摩液(EPS)常规、经直肠前列腺B超、血清前列腺特异抗原(PSA)、国际前列腺症状评分(IPSS)、临床症状以及有无慢性骨盆疼痛综合征以及术后组织病理检查结果分为单纯BPH、BPH合并慢性前列腺炎两组。采用免疫组化、RT-PCR等实验方法研究两组前列腺组织中SIgA、α1-AR的表达。结果:62例患者中30例为BPH合并慢性前列腺炎,32例为单纯BPH,通过对患者一般资料对比和对实验结果进行统计学分析,合并慢性前列腺炎的BPH患者SIgA、α1-AR表达显著高于单纯BPH患者(0.380 8±0.144 3 vs 0.295 4±0.008 4;0.440 5±0.104 1 vs 0.383 2±0.013 6),差异有统计学意义(P<0.05)。结论:SIgA、α1-AR在BPH合并慢性前列腺炎患者中的表达上调,提示慢性前列腺炎与BPH可能有一定的内在联系,炎症反应可能是BPH的一个致病因素,与BPH的病理发展过程有关。

良性前列腺增生合并慢性前列腺炎组织中sIgA、α_1-AR的表达与意义

目的探讨良性前列腺增生与良性前列腺增生合并前列腺炎患者组织中s Ig A、α1-AR表达的意义。方法选取2014年1月至2015年1月在大连市友谊医院泌尿外科就诊的70例患者,根据诊断结果的不同,36例单纯良性前列腺增生(BPH)患者为BPH组,34例并慢性前列腺炎(CP)患者CP组,取两组病理进行免疫组化实验比较两组患者s Ig A、α1-AR。结果 CP组s Ig A、α1-AR值明显高于BPH组,差异有统计学意义(P<0.05)。结论良性前列腺增生合并慢性前列腺炎患者组织中s Ig A、α1-AR的表达明显高于单纯良性前列腺增生患者,提示慢性前列腺炎可能与BPH可能有一定联系,BPH的一个致病因素之一可能是炎性反应,与BPH的病理发展过程有关。

正常与心力衰竭大鼠心脏抗β_1受体自身抗体生物效应的比较研究

目的 :对比观察正常与病理性心脏 β1 受体自身抗体的生物效应。方法 :分级盐析法结合离子交换层析法分离提纯正常无抗体组、β1 受体生理性抗体组及 β1 受体病理性抗体组大鼠血清中的 Ig G,应用乳鼠心肌细胞培养技术及放射免疫分析方法 ,观察各组自身抗体及 β1 受体单克隆抗体对培养乳鼠心肌细胞跳动频率和大鼠心室肌细胞c AMP产生量的影响。结果 :在正常大鼠血清中 ,抗 β1 受体自身抗体的阳性率与抗体滴度均显著低于病理性抗体组大鼠阳性血清的阳性率和抗体滴度。生理性抗体、病理性抗体和单克隆抗体均表现出激动剂样生物学效应 ,且具有浓度依赖性。但是 ,在相近抗体浓度条件下 ,生理性抗体对心率和 c

抗β_1肾上腺素能受体抗体在鼠巨细胞病毒性心肌炎中的作用

目的探讨抗β1肾上腺素能受体抗体在鼠巨细胞病毒性心肌炎中的作用。方法用酶联免疫吸附试验方法检测巨细胞病毒性心肌炎小鼠血清中抗β1肾上腺素能受体抗体滴度,石蜡病理切片计算心肌病理积分,生物信号采集处理系统记录心电图。结果实验组小鼠心肌炎发病率为69.4%,死亡率为11.11%。实验组小鼠血清抗β1肾上腺素能受体抗体滴度和阳性率比对照组高(P<0.01),小鼠血清抗β1肾上腺素能受体抗体滴度与心肌病变程度和心电图改变密切相关(r分别为0.93、0.90)。结论抗β1肾上腺素能受体抗体可能参与鼠巨细胞病毒性心肌炎的发病过程。

慢性心力衰竭患者血清β_1肾上腺素能受体自身抗体的浓度与心功能的相关性研究

目的分析慢性心力衰竭(chronic heart failure,CHF)患者血清抗β1肾上腺素能受体(beta 1-adrenergic receptor,β1-AR)自身抗体浓度及其与患者心功能指标的相关性。方法选择CHF患者78例,正常体检者82例作为对照组,测定抗β1-AR自身抗体浓度、左心室射血分数(left ventricular ejection fraction,LVEF),进行6min步行试验(six-minute walking test,6MWT)以评价患者心功能,并研究抗体浓度与心功能指标的相关性。结果CHF患者抗β1-AR自身抗体浓度显著升高(P<0.05),与走距(r=0.43,P<0.05)及LVEF(r=0.51,P<0.05)呈正相关。结论CHF患者血清抗β1-AR自身抗体浓度的增高可能是患者心功能恶化的重要因素,该抗体浓度可协助判断CHF患者的心功能及预后。

烟雾吸入伤大鼠肺组织α_1-AR的变化与哌唑嗪保护作用的实验研究

目的 探讨α1肾上腺素受体 (α1-AR)在烟雾吸入伤大鼠肺组织变化与哌唑嗪对烟雾吸入伤的保护作用。方法 采用大鼠烟雾吸入伤模型致伤大鼠 ,干湿重法测定肺组织含水量 ,伊文斯蓝法测定肺微量血管通透性 (PMVP) ,放射受体分析法测定肺组织α1-AR的变化。结果 烟雾吸入致伤后大鼠PMVP增大 ,2h达显著水平 ,6h达高峰 ,2 4h仍显著高于正常 ;肺含水量伤后 2h明显升高 ,6h达非常显著水平 ,2 4h达高峰 ;肺组织α1-AR密度于烟雾致伤后 2、4、6及 2 4h显著升高 ,但亲和力除伤后 2h升高之外 ,无明显变化。相关分析显示 ,肺组织α1-AR密度的升高与PMVP增大呈显著正相关。腹腔给予α1-AR阻断剂哌唑嗪 0 5、1 5及 3 0mg/kg能明显降低PMVP及肺水含量 ,减轻肺损伤。结论 大鼠烟雾吸入性肺损伤的发病机制与α1-AR密度升高有关 ,哌唑嗪对烟雾吸入伤具有一定保护作用。

Cl^-通道阻断剂对A10细胞α_1-AR介导的Ca^(2+)内流的影响

目的 :在胚胎大鼠主动脉平滑肌细胞 (A10 ) ,探讨Cl- 通道与Ca2 + 内流的关系及酪氨酸磷酸化对Ca2 + 内流的作用。方法 :采用Fura 2荧光探针双波长测定胞浆游离Ca2 + 浓度 ([Ca2 + ]i)。结果 :Ca2 +通道阻断剂nifedipine和SK&F96 36 5可阻止肾上腺素 (Adr)触发的Ca2 + 内流 ;氯通道阻断剂niflumicacid(NFA)和furosemide呈浓度依赖性抑制Ca2 + 内流。在Ca2 + 内流被SK&F96 36 5最大限度抑制后 ,NFA和furosemide可进一步抑制Ca2 + 内流 ;而Ca2 +内流被NFA和furosemide分别最大抑制 2 8%和 35 %后 ,SK&F96 36 5也可进一步抑制Ca2 + 内流达 5 3%和5 2 %。genistein呈浓度依赖性抑制Ca2 + 内流 ;vana date浓度依赖性促进Ca2 + 内流。结论 :在A10细胞 ,肾上腺素受体触发的Ca2 + 内流涉及电压依赖性Ca2 + 通道 (VDC)和受体操纵性Ca2 + 通道 (ROC) ;氯通道参与了VDC及ROC介导的Ca2 + 内流 ;蛋白酪氨酸磷酸化的水平影响Ca2 + 内流。

慢性心力衰竭患者心脏β_1受体自身抗体与心功能及QTcd的相关性分析

目的通过β1肾上腺素受体自身抗体水平的检测,分析其与心功能及心电图表现的相关性,并观察β受体阻滞剂卡维地洛的治疗作用。方法65例慢性心力衰竭患者采用酶联免疫法测定患者血清中β1受体自身抗体水平,据此分为β1受体自身抗体阳性组(β1阳性组)30例和β1受体自身抗体阴性组(β1阴性组)35例,采用超声心动图测量左室舒张末径,左室收缩末径和左室射血分数进行心功能检测,常规12导心电图测量QTcd值。在血管紧张素转换酶抑制剂、利尿剂和洋地黄制剂治疗基础上加用β受体阻滞剂卡维地洛,随访半年。结果(1)治疗前β1阳性组左室舒张末径显著大于β1阴性组〔(66.01±5.47)vs(63.07±5.64)mm;P<0.05)〕,左室收缩末径大于β1阴性组〔(54.24±8.43)vs(50.72±6.12)mm;P=0.052)〕,左室射血分数显著低于β1阴性组〔(32.16±9.00)vs(36.64±8.20)%;P<0.05)〕。治疗后两组左室舒张末径、收缩末径均较治疗前显著减小(P<0.01),左室射血分数较治疗前提高(P<0.01)。β1阳性组左室舒张末径、收缩末径和左室射血分数与β1阴性组无差异(P>0.05)。(2)治疗前β1阳性组心率显著高于β1阴性组〔(94±14)vs(87±16)次/min;P<0.05)〕,β1阳性组QTcd值显著大于β1阴性组〔(71.14±34)vs(58.33±14)ms;P<0.05)〕,治疗后两组心率及血压均较治疗前显著减低(P<0.01),β1阳性组QTcd值较治疗前显著减低(P<0.05),β1阳性组心率和QTcd值与β1阴性组无显著差异(P>0.05)。结论β1受体自身抗体阳性者心功能较差且QTcd值长,β受体阻滞剂可以抑制心肌重构,改善心功能,减小QT离散度,提示β1受体自身抗体参与心力衰竭的病理生理过程,阳性者可能临床预后差。

β1-AR在大鼠室性心律失常中的作用机理研究

观察β1-肾上腺素能受体(β1-AR)的缺失对诱发大鼠室性心律失常的影响;探讨β1-AR在室性心律失常发生中的作用。方法:选用20;只体重300g左右大鼠;随机分为对照组(Con;组)、实验组(β1-AR组);每组各10只;β1-AR组大鼠敲除β1肾上腺素能受体基因;Con组大鼠为同基因野生型(WT)大鼠(β1+/+β2+/+β3+/+);分别测量Con组和β1-AR组两组大鼠的血压、心率并记录;采用单导管技术对野生型大鼠(Con组)和实验组(β1-AR组)大鼠进行电生理检测;记录Con组和β1-AR组大鼠标准体表心电图、心内电生理参数和室性心律失常诱发率情况;结果:1、与Con组大鼠相比;β1-AR组大鼠平均心率降低;血压下降(p<0.05);2、体表心电图显示;与Con组大鼠相比;β1-AR组大鼠QT间期延长(p<0.05);但QTc两组无明显差异(P>0.05);3、心内电生理检查结果显示:与Con组大鼠相比;β1-AR组大鼠心室有效不应期(VRP)延长;(p<0.05)。4、心律失常诱导结果显示;与Con组大鼠相比;β1-AR组大鼠诱发室性心律失常的概率显著降低。结论:β1-AR基因缺失可降低大鼠血压及心率;延长心室复极时间和心室有效不应期;同时室性心律失常发生率显著降低;这表明β1肾上腺素能受体在室性心律失常的发生中起重要作用;为β1受体阻滞剂在室性心律失常的药物治疗靶点提供科学依据。

Autoantibodies to apolipoprotein A-1 as a biomarker of cardiovascular autoimmunity

Immune-driven inflammation plays an important part inatherogenesis and is therefore believed to be key to thedevelopment of cardiovascular disease(CVD), whichis currently the leading cause of death in the Westernworld. By fulfilling some of the Koch postulates, athero-genesis has even been proposed to be considered as anautoimmune disease, raising the hope that CVD couldbe prevented by immunomodulation. Nevertheless,the role of the immune system and autoimmune reac-tions in atherosclerosis appear to be a double edged-sword, with both pro-atherogenic and anti-atherogenicattributes. Hence, if immunomodulation is to becomea therapeutic option for atherosclerosis and CVD, it willbe crucial to correctly identify patients who might ben-efit from targeted suppression of deleterious autoim-mune responses. This could be achieved, for example, by the detection of disease-associated autoantibodies. In this work, we will review the currently available clini-cal, in vitro, and animal studies dedicated to autoan-tibodies against apolipoprotein A-1(anti-apoA-1 IgG), the major proteic fraction of high density lipoprotein. Current clinical studies indicate that high levels of anti-apoA-1 IgG are associated with a worse cardiovascular prognosis. In addition, in vitro and animal studies indi-cate a pro-inflammatory and pro-atherogenic role, sup-porting the hypothesis that these autoantibodies may play a direct causal role in CVD, and furthermore that they could potentially represent a therapeutic target for CVD in the future.

外周血单个核细胞TFAM、GDF-15、淋巴细胞β1-AR的mRNA对近期MACE的预测效能

目的探究外周血单个核细胞(PBMCs)线粒体转录因子A(TFAM)、生长分化因子-15(GDF15)、淋巴细胞β1肾上腺素受体(β1-AR)的mRNA对近期主要心血管不良事件(MACE)的预测效能。方法选取延安大学附属医院2017年4月~2019年10月CHF患者127例作为研究对象,分析外周血指标与心肌重构指标[左心房内径(LAP)、左室后壁厚度(LVPW)、左室舒张末内径(LVEDD)、左室质量指数(LVMI)、左室重构指数(LVRI)]、LVEF相关性及对MACE的预测价值。结果PBMCs中TFAM、淋巴细胞β1-AR mRNA相对含量与LAP、LVPW、LVEDD、LVMI呈负相关,与LVRI、LVEF呈正相关,GDF-15 mRNA相对含量与LAP、LVPW、LVEDD、LVMI呈正相关,与LVRI、LVEF呈负相关(P<0.05);随访3个月,发生MACE组PBMCs中TFAM、淋巴细胞β1-AR mRNA相对含量低于未发生MACE组,GDF15 mRNA高于未发生MACE组(P<0.05);PBMCs中TFAM、GDF-15、淋巴细胞β1-AR mRNA相对含量联合预测MACE的AUC值为0.889,大于任一指标单独预测。结论CHF患者PBMCs中TFAM、GDF-15、淋巴细胞β1-AR mRNA表达异常,在其病理变化中发挥重要作用,且表达水平与MACE发生关系密切,可能成为CHF新的标志物及治疗靶点。

Design,synthesis and biological estimation of 1-(benzoxazole-2-yl)piperazine and 4-(benzoxazole-2-yl)piperidine derivatives as potentialα_1-AR antagonists

1-(benzoxazole-2-yl ) 的二个系列 piperazine (哌啶加重的 8a 鈥搃) 和 4-(benzoxazole-2-yl )(10a 鈥搃) 被设计，综合并且为他们的伪 1 评估了 -AR 对抗活动。在 vitro 的生物试金显示 10h 显示出稍微更强壮的伪 1 -AR 对抗活动到我们的铅混合物的 1。