Analysis of the potential biological value of pyruvate dehydrogenase E1 subunitβin human cancer

BACKGROUND The pyruvate dehydrogenase E1 subunitβ(PDHB)gene which regulates energy metabolism is located in mitochondria.However,few studies have elucidated the role and mechanism of PDHB in different cancers.AIM To comprehensive pan-cancer analysis of PDHB was performed based on bioinformatics approaches to explore its tumor diagnostic and prognostic value and tumor immune relevance in cancer.In vitro experiments were performed to examine the biological regulation of PDHB in liver cancer.METHODS Pan-cancer data related to PDHB were obtained from the Cancer Genome Atlas(TCGA)database.Analysis of the gene expression profiles of PDHB was based on TCGA and Genotype Tissue Expression Dataset databases.Cox regression analysis and Kaplan-Meier methods were used to assess the correlation between PDHB expression and survival prognosis in cancer patients.The correlation between PDHB and receiver operating characteristic diagnostic curve,clinicopathological staging,somatic mutation,tumor mutation burden(TMB),microsatellite instability(MSI),DNA methylation,and drug susceptibility in pan-cancer was also analyzed.Various algorithms were used to analyze the correlation between PDHB and immune cell infiltration and tumor chemotaxis environment,as well as the co-expression analysis of PDHB and immune checkpoint(ICP)genes.The expression and functional phenotype of PDHB in single tumor cells were studied by single-cell sequencing,and the functional enrichment analysis of PDHB-related genes was performed.The study also validated the level of mRNA or protein expression of PDHB in several cancers.Finally,in vitro experiments verified the regulatory effect of PDHB on the proliferation,migration,and invasion of liver cancer.RESULTS PDHB was significantly and differently expressed in most cancers.PDHB was significantly associated with prognosis in patients with a wide range of cancers,including kidney renal clear cell carcinoma,kidney renal papillary cell carcinoma,breast invasive carcinoma,and brain lower grade glioma.In some cancers,PDHB expression was clearly associated with gene mutations,clinicopathological stages,and expression of TMB,MSI,and ICP genes.The expression of PDHB was closely related to the infiltration of multiple immune cells in the immune microenvironment and the regulation of tumor chemotaxis environment.In addition,single-cell sequencing results showed that PDHB correlated with different biological phenotypes of multiple cancer single cells.This study further demonstrated that down-regulation of PDHB expression inhibited the proliferation,migration,and invasion functions of hepatoma cells.CONCLUSION As a member of pan-cancer,PDHB may be a novel cancer marker with potential value in diagnosing cancer,predicting prognosis,and in targeted therapy.

丙酮酸脱氢酶E1α亚单位缺陷导致Leigh综合征

Leigh综合征是由于线粒体呼吸链能量代谢障碍所导致的遗传性疾病,丙酮酸脱氢酶E1浕亚单位(pyruvate dehydrogenase complex E1 alpha subunit,PDHA1)缺陷是导致Leigh综合征的常见原因之一。该研究通过PDHA1基因分析首次确诊了1例中国患者。该患儿1岁后运动发育落后,无力,肌张力低下,肌腱反射消失,发热、感冒时间歇性加重,智力发育正常。肌电图检查、腓肠肌病理活检结果提示神经性损害。3岁时脑MRI扫描未见异常,5岁时脑MRI呈现双侧苍白球对称性损害,符合Leigh综合征表现。经基因分析证实患者及其母亲PDHA1基因外显子3存在C214T突变,导致丙酮酸脱氢酶复合物活性下降。经过维生素B1、辅酶Q10、左旋肉碱及低碳水化合物饮食治疗后,患儿运动能力显著改善,现在8岁,正常就学。PDHA1缺陷为X连锁遗传性疾病,表型复杂,临床诊断困难,该患儿以无力为主要表现,经基因诊断确诊。

丙酮酸脱氢酶E1α亚单位、转录激活反应RNA结合蛋白1在表皮生长因子受体突变晚期非小细胞肺癌中的表达及对患者预后的影响

目的探讨丙酮酸脱氢酶E1α亚单位(PDHA1)、转录激活反应RNA结合蛋白1(TARBP1)在表皮生长因子受体(EGFR)突变晚期非小细胞肺癌(NSCLC)中的表达及对患者预后的影响。方法取95例接受靶向治疗的EGFR突变晚期NSCLC患者的肿瘤组织,免疫组化法检测PDHA1、TARBP1蛋白的表达情况,并分析其与患者临床特征的关系。随访3年,记录患者的总生存率,NSCLC患者预后的影响因素采用Cox风险比例回归模型分析。结果95例NSCLC患者肿瘤组织中,PDHA1阳性表达率为45.26%,阴性表达率为54.74%;TARBP1阳性表达率为74.74%,阴性表达率为25.26%。分化程度为中低分化、淋巴结转移NSCLC患者肿瘤组织中PDHA1蛋白的阳性表达率较低、TARBP1蛋白的阳性表达率较高。至随访结束,95例NSCLC患者病死67例,生存28例。PDHA1阳性表达患者总生存率为44.2%,明显高于PDHA1阴性表达患者的17.3%(P﹤0.01);TARBP1阳性表达患者的总生存率为18.3%,明显低于TARBP1阴性表达患者的62.5%(P﹤0.01)。多因素Cox回归分析结果显示,分化程度为中低分化、有淋巴结转移、PDHA1表达阴性、TARBP1表达阳性均是NSCLC患者预后的独立危险因素(P﹤0.05)。结论接受靶向治疗的EGFR突变晚期NSCLC患者肿瘤组织中PDHA1阴性表达率较低、TARBP1阳性表达率较高,且PDHA1阴性表达、TARBP1阳性表达患者的预后较差。

琥珀酸脱氢酶B和丙酮酸脱氢酶激酶1在鼻咽癌组织中的表达及其临床意义

目的:探讨琥珀酸脱氢酶(SDH)B和丙酮酸脱氢酶激酶(PDK)1在鼻咽癌组织中的表达及其临床意义。方法:采用免疫组化法检测78例鼻咽癌组织及35例鼻咽黏膜慢性炎症组织中SDHB和PDK1的表达情况,运用x2检验分析SDHB和PDK1表达与鼻咽癌患者临床病理因素的关系,运用Kaplan-Meter法分析其与预后的关系。结果:SDHB和PDK1在鼻咽癌组织中阳性表达率分别为39.7%(31/78)和53.8%(42/78),而在鼻咽黏膜慢性炎症组织中为62.9%(22/35)和20.0%(7/35),SDHB和PDK1表达均与鼻咽癌复发、颈部淋巴结转移相关(P<0.05),与患者性别、年龄等无显著相关(P>0.05)。K-M生存曲线提示SDHB阳性表达和PDK1阴性表达者的生存率分别高于SDHB阴性表达和PDK1阳性表达者,多因素Cox回归分析显示,T分级、临床分期、复发是影响鼻咽癌患者预后的独立因素,SDHB和PDK1表达不能作为影响鼻咽癌预后的独立因素。结论:SDHB和PDK1表达在鼻咽癌的发展、淋巴结转移、复发中起着重要作用,并可能对预后有影响,但SDHB和PDK1表达不是影响预后的独立因素。

维生素B_(1)在中枢认知功能中的作用研究进展

维生素B_(1),又称为硫胺素,是影响脑能量代谢的关键物质。硫胺素的代谢物焦磷酸硫胺素是糖酵解、三羧酸循环及磷酸戊糖旁路的三种关键酶(丙酮酸脱氢酶复合体、α-酮戊二酸脱氢酶复合体和转酮醇酶)的辅因子。脑内硫胺素水平以及硫胺素依赖酶的活性和表达会影响脑内能量代谢,进而影响中枢神经系统的认知功能。补充硫胺素对中枢神经认知功能异常有改善作用。本文对近年来相关的研究进展进行综述,以阐明脑内硫胺素缺乏及硫胺素依赖酶的功能与表达的损伤对中枢认知功能的影响,为脑能量代谢障碍的相关研究提供参考。

非小细胞肺癌组织中PDHA1、GBP1的表达及临床意义

目的探讨非小细胞肺癌(NSCLC)组织中丙酮酸脱氢酶复合物E1α亚单位(PDHA1)和鸟苷酸结合蛋白1(GBP1)的表达及临床意义。方法选取山东省烟台市烟台山医院2016年1月至2017年10月84例NSCLC患者为研究对象,比较其癌组织及癌旁组织中PDHA1与GBP1的表达情况。根据患者癌组织中PDHA1的表达情况将其分为PDHA1阳性组(30例)和PDHA1阴性组(54例),再根据GBP1的表达情况将其分为GBP1阳性组(58例)和GBP1阴性组(26例)。随访3年,采用生存曲线分析PDHA1与GBP1表达与患者预后的关系。结果NSCLC患者癌组织中PDHA1表达低于癌旁组织,GBP1表达高于癌旁组织,差异有统计学意义(P<0.05)。84例NSCLC患者均随访成功,无失访病例。随访3年内,共有31例死亡。PDHA1阳性组3年生存率高于PDHA1阴性组,GBP1阳性组3年生存率低于GBP1阴性组,差异有统计学意义(P<0.05)。结论PDHA1在NSCLC组织中低表达,GBP1在其中高表达,二者有望成为新的NSCLC预后评估的分子标志物。

巨噬细胞PDHA1基因敲除对非酒精性脂肪性肝病小鼠肝细胞凋亡的影响

目的:探讨巨噬细胞丙酮酸脱氢酶E1 α1亚基(pyruvate dehydrogenase E1 subunit alpha 1), PDHA1在同型半胱氨酸(homocysteine, Hcy)诱导的小鼠非酒精性脂肪性肝病(non-alcoholic fatty liver disease, NAFLD)中对肝细胞凋亡的作用。方法:随机选取6周龄体重相近的PDHA1基因正常野生型小鼠和巨噬细胞特异性PDHA1基因敲除(PDHA1^(iΔMΦ/iΔMΦ))小鼠各12只,均分别给予普通饮食和高Hcy饮食喂养12周后用于后续实验。应用琼脂糖凝胶电泳技术对PDHA1^(iΔMΦ/iΔMΦ)小鼠进行基因鉴定;Western blot检测两种基因型小鼠骨髓巨噬细胞PDHA1蛋白表达;使用全自动生化分析仪检测小鼠血清Hcy和丙氨酸转氨酶(alanine aminotransferase, ALT)水平;试剂盒检测肝组织上清液甘油三酯(triglyceride, TG)和ALT水平;苏木精-伊红(hematoxylin-eosin, HE)染色观察小鼠肝组织结构改变;qRT-PCR和Western blot检测小鼠肝组织中凋亡相关指标Bax和caspase-3的mRNA和蛋白表达。结果:PDHA1^(iΔMΦ/iΔMΦ)小鼠均表达Lyz2-Cre及PDHA1-flox,且巨噬细胞中PDHA1蛋白表达减少(P<0.05),表明巨噬细胞特异性PDHA1敲除小鼠模型构建成功。高Hcy饮食组PDHA1^(iΔMΦ/iΔMΦ)小鼠血清Hcy水平升高(P<0.05),表明高Hcy血症模型构建成功。高Hcy饮食组小鼠肝组织上清液TG和ALT水平显著升高(P<0.05),且巨噬细胞中PDHA1敲除后,血清及肝组织中ALT水平升高更为显著。HE染色结果表明,高Hcy饮食使小鼠肝脏发生脂肪变性,巨噬细胞中PDHA1基因敲除可加重肝细胞的变性坏死。PDHA1^(iΔMΦ/iΔMΦ)组凋亡相关指标Bax和caspase-3表达均显著升高(P<0.05)。结论:抑制小鼠巨噬细胞中PDHA1表达,可促进高Hcy饮食诱导的NAFLD小鼠模型中肝细胞的凋亡,这可能是加重NAFLD肝损伤的其中一个机制。

Catalytic domain of PDC-E2 contains epitopes recognized by antimitochondrial antibodies in primary biliary cirrhosis

AIM:To search for further immunodominant peptides of the pyruvate dehydrogenase complex E2-component (PDC-E2) recognized by antimitochondrial antibodies (AMA) in primary biliary cirrhosis (PBC). METHODS:Sera from 95 patients with PBC were tested by enzyme-linked immunosorbent assay against 33 synthetic overlapping peptides (25 amino acids; aa) covering the entire length of the E2-subunit of PDC-E2. Furthermore,the inner lipoyl peptide 167-184 was used in an unlip oylated and a lipoylated form as well as coupled to ovalbumin. Sera from 11 AMA negative/ANA posit ive PBC patients,63 patients with other liver disorders and 22 healthy blood donors served as controls.RESULTS:Of the 95 PBC-sera,74% reacted with the peptide 475-499 and 58% with the pept ide 407-431 located within the catalytic domain of PDC-E2. Patients with other disorders or healthy controls were positive in only up to 18%. Antibodies to the unlipoylatedand lip oylated pept ide 167-184 within the inner lipoyl domain were found in only 5% and 11% of the PBC sera,respectively; using ovalbumin-coupled peptides,the incidence increased up to 57% (unlipoylated form). CONCLUSION:Peptides within the catalytic site of PDC-E2 rather than the previously reported lipoyl binding peptide 167-184 may represent major immunodomin ant epitopes recognized by AMA in PBC.

New insights into the pathogenesis of primary biliary cholangitis asymptomatic stage

Primary biliary cholangitis(PBC)is a chronic cholestatic progressive liver disease and one of the most important progressive cholangiopathies in adults.Damage to cholangiocytes triggers the development of intrahepatic cholestasis,which progresses to cirrhosis in the terminal stage of the disease.Accumulating data indicate that damage to biliary epithelial cells[(BECs),cholangiocytes]is most likely associated with the intracellular accumulation of bile acids,which have potent detergent properties and damaging effects on cell membranes.The mechanisms underlying uncontrolled bile acid intake into BECs in PBC are associated with pH change in the bile duct lumen,which is controlled by the bicarbonate(HCO3-)buffer system“biliary HCO3-umbrella”.The impaired production and entry of HCO3-from BECs into the bile duct lumen is due to epigenetic changes in expression of the X-linked microRNA 506.Based on the growing body of knowledge on the molecular mechanisms of cholangiocyte damage in patients with PBC,we propose a hypothesis explaining the pathogenesis of the first morphologic(ductulopenia),immunologic(antimitochondrial autoantibodies)and clinical(weakness,malaise,rapid fatigue)signs of the disease in the asymptomatic stage.This review focuses on the consideration of these mechanisms.

高通量测序揭示原发性胆汁性胆管炎患者的T细胞受体图谱特征

目的揭示原发性胆汁性胆管炎(primary biliary cholangitis,PBC)患者T细胞受体(T cell receptor,TCR)图谱特征,并揭示大肠埃希菌(Escherichia coli,E.coli)的丙酮酸脱氢酶复合体E2亚基(pyruvate dehydrogenase complex E2,PDC-E2)抗原在PBC疾病的分子模拟机制。方法采用多重聚合酶链反应和免疫组库测序技术分析PBC患者和健康对照者的CD4^(+)和CD8^(+)记忆性TCRβ链互补决定区3(complementarity determining region 3,CDR3)序列的多样性、氨基酸组成及疏水性、共有CDR3序列。体外诱导和扩增人PDC-E2_(163-176)(人PDC-E2)抗原相关T细胞和E.coli PDC-E2_(31-44/134-147/235-248)(E.coli PDC-E2)抗原相关T细胞,通过免疫组库测序技术鉴定人(和E.coli)PDC-E2抗原相关TCRβCDR3图谱,并分析其丰度变化。结果PBC患者组和健康对照组间的CD4^(+)记忆性T细胞、CD8^(+)记忆性T细胞TCRβCDR3免疫图谱多样性相似,D50指数[CD4^(+)记忆性T细胞:0.028±0.019比0.034±0.015;CD8^(+)记忆性T细胞:(1.86±2.70)×10^(-3)比(4.62±3.89)×10^(-4)]、Shannon指数(CD4^(+)记忆性T细胞:9.473±1.346比9.734±0.933;CD8^(+)记忆性T细胞:6.197±1.519比5.436±1.629)、Gini指数(CD4^(+)记忆性T细胞:0.786±0.048比0.760±0.036;CD8^(+)记忆性T细胞:0.920±0.047比0.939±0.025)等差异均无统计学意义(P均>0.05)。PBC组和健康对照组CD4^(+)记忆性T细胞和CD8^(+)记忆性T细胞间共有CDR3序列百分比差异无统计学意义[(6.47±1.43)%比(6.21±3.18)%;t=-0.21,P=0.84]。健康对照组和PBC组中序列长度为13、14、15的CDR3分子第6位和第7位氨基酸的组成频率中部分存在显著差异,疏水氨基酸组成频率近似。通过细胞培养和免疫组库测序鉴定了一系列人PDC-E2和E.coli PDC-E2抗原刺激后丰度显著上升的TCR序列。结论该研究鉴定出PBC疾病的TCR图谱特征,从TCR这个新视角阐述了E.coli在PBC疾病中的分子模拟机制。

原发性胆汁性肝硬化患者血清AMA-M2及其靶抗原检测的阳性率对比

目的:针对PBC患者血清同时选用国产和进口两种试剂盒检测AMA-M2及其靶抗原:丙酮酸脱氢酶复合体E2亚单位(PDC-E2)及抗M2-3E等免疫指标,并对其敏感性进行对比,观察两种试剂盒检测有无差异及3个指标之间的敏感性。方法:对51例PBC确诊患者的血清标本,采用上海丰翔生物公司及欧蒙公司的ELISA试剂盒对待测血清分别进行了AMA-M2、抗M2-3E、PDC-E2等指标的检测,进行阳性率的比较。结果:51例患者血清标本中,国产试剂盒检测AMA-M2、抗M2-3E、PDC-E2的阳性率分别为72.5%、90.2%、72.5%,进口试剂盒检测AMA-M2、抗M2-3E、PDC-E2的阳性率分别为78.4%、92.2%、82.4%,经统计软件处理得到的结果P>0.05,无明显的统计学差异。针对42例AMA阳性的患者进行AMA-M2、抗M2-3E、PDC-E2检测时,国产试剂盒检测的阳性率分别为85.7%、95.2%和78.6%,进口试剂盒检测的阳性率分别为95.2%、100%、95.2%,经统计软件处理后得出P>0.05,两种试剂盒检测无明显的差别。结论:使用进口和国产两种试剂盒检测AMA-M2、PDC-E2、抗M2-3E的阳性率无明显的统计学差异。AMA-M2、PDC-E2、抗M2-3E 3个指标中阳性率最高的是抗M2-3E,AMA-M2和PDC-E2差异无统计学意义。

Dichloroacetic acid and rapamycin synergistically inhibit tumor progression

Mammalian target of rapamycin(mTOR)controls cellular anabolism,and mTOR signaling is hyperactive in most cancer cells.As a result,inhibition of mTOR signaling benefits cancer patients.Rapamycin is a US Food and Drug Administration(FDA)-approved drug,a specific mTOR complex 1(mTORC1)inhibitor,for the treatment of several different types of cancer.However,rapamycin is reported to inhibit cancer growth rather than induce apoptosis.Pyruvate dehydrogenase complex(PDHc)is the gatekeeper for mitochondrial pyruvate oxidation.PDHc inactivation has been observed in a number of cancer cells,and this alteration protects cancer cells from senescence and nicotinamide adenine dinucleotide(NAD^(+))exhaustion.In this paper,we describe our finding that rapamycin treatment promotes pyruvate dehydrogenase E1 subunit alpha 1(PDHA1)phosphorylation and leads to PDHc inactivation dependent on mTOR signaling inhibition in cells.This inactivation reduces the sensitivity of cancer cells'response to rapamycin.As a result,rebooting PDHc activity with dichloroacetic acid(DCA),a pyruvate dehydrogenase kinase(PDK)inhibitor,promotes cancer cells'susceptibility to rapamycin treatment in vitro and in vivo.