Cardiac resident macrophages: Spatiotemporal distribution, development, physiological functions, and their translational potential on cardiac diseases

Cardiac resident macrophages (CRMs) are the main population of cardiac immune cells. The role of these cells in regeneration, functional remodeling, and repair after cardiac injury is always the focus of research. However, in recent years, their dynamic changes and contributions in physiological states have a significant attention. CRMs have specific phenotypes and functions in different cardiac chambers or locations of the heart and at different stages. They further show specific differentiation and development processes. The present review will summarize the new progress about the spatiotemporal distribution, potential developmental regulation, and their roles in cardiac development and aging as well as the translational potential of CRMs on cardiac diseases. Of course, the research tools for CRMs, their respective advantages and disadvantages, and key issues on CRMs will further be discussed.

An emerging role for Hippo-YAP signaling in cardiovascular development

The Hippo signaling pathway was originally discovered in Drosophila and shown to be critical for organ size control and tumorigenesis. This pathway consists of a cascade of kinases and several adaptors that lead to the phosphorylation and inhibition, through nuclear exclusion, of the transcriptional cofactor Yorkie in Drosophila or YAP （yes associated protein） in mammals. Recent studies demonstrate that cardiac-specific deletion of the Hippo pathway kinase Mst （STE20-1ike protein kinases） co-activator WW45 （WW domain-containing adaptor 45）, Mstl, Mst2, or Lats2 （large tumor suppressor homologue 2） in mice result in over-grown hearts with elevated cardiomyocyte proliferation. Consistent with these observations, over-expression of YAP in the mouse embryonic heart increases heart size and promotes cardiac regeneration and contractility after myocardial infarction by inducing cardiomyocyte proliferation, whereas deletion of YAP in the mouse heart impedes cardiomyocyte proliferation, causing myocardial hypoplasia and embryonic or premature lethality. YAP has also been shown to play an important role in the vascular system. Specific-deletion of YAP from vascular smooth muscle cells in mice results in aberrant development of large arteries with a hypoplastic arterial wall phenotype. Hippo-YAP signaling cross-talks with other signaling pathways such as IGF （insulin-like growth factor） and Wnt signaling to promote heart growth by increasing expression of cell cycle genes. The purpose of this review is to summarize these recent findings and discuss potential diagnostic or therapeutic strategies in cardiovascular system based on manipulating the Hippo-YAP signaling.

基于胚胎干细胞模型的Cry1Ab蛋白发育毒性

目的:通过胚胎干细胞发育毒性评价模型研究Cry1Ab蛋白对于细胞增殖和分化能力的影响,以评估其发育毒性。方法:设置Cry1Ab蛋白7个剂量组(31.25、62.50、125.00、250.00、320.00、1 000.00、2 000.00μg/L),以5-氟尿嘧啶(5-fluorouracil, 5-FU)为阳性对照,以磷酸缓冲盐溶液(phosphate buffer saline, PBS)为溶剂对照,分别处理小鼠胚胎干细胞D3(embryonic stem cell line D3,ES-D3)和小鼠成纤维细胞3T3。通过CCK-8法检测细胞活性,计算受试物对于不同细胞的增殖半抑制浓度(50%inhibition concentration of growth and viability, IC_(50))。设置Cry1Ab蛋白5个剂量组(125.00、250.00、320.00、1 000.00、2 000.00μg/L),设置溶剂对照(PBS),同时以5-FU为受试物进行模型验证,分别处理细胞后,通过拟胚胎体(embryonic bodies, EBs)培养法诱导ES-D3分化出心肌细胞;镜下观察EBs生长情况并测量其第3天和第5天的直径,观察并记录同批次EBs分化出搏动心肌细胞的比例,计算受试物的心肌分化半抑制浓度(50%inhibition concentration of differentiation, ID50),根据发育毒性判别函数对受试物的胚胎发育毒性进行分类;收集培养终点的EBs样本,进行实时定量聚合酶链式反应(real-time quantitative po-lymerase chain reaction, qPCR),检测心肌分化相关标志物(Oct3/4、GATA-4、Nkx2.5和β-MHC)的mRNA表达情况。结果:5-FU的IC_(50,3T3)为46.37μg/L,IC_(50,ES)为32.67μg/L,ID_(50,ES)为21.28μg/L,根据判别函数结果将5-FU分类为强胚胎毒性物质。不同浓度的Cry1Ab蛋白处理组的3T3细胞和ES-D3细胞活性与对照组相比差异均无统计学意义(P>0.05)。与对照组相比,Cry1Ab蛋白处理组分化第3天和第5天的EBs直径差异无统计学意义(P>0.05),EBs形态也未见明显差异;不同浓度Cry1Ab蛋白处理组的心肌分化率与对照组相比差异无统计学意义(P>0.05)。5-FU使β-MHC、Nkx2.5和GATA-4的mRNA表达水平降低(P<0.05),且具有剂量依赖趋势(P<0.05),而与细胞多能性相关的标志物Oct3/4 mRNA表达水平则呈升高趋势(P<0.05);Cry1Ab蛋白处理组的成熟心肌标志物β-MHC、心肌早期分化标志物Nkx2.5和GATA-4、多能性相关标志物Oct3/4的mRNA表达水平与对照组相比差异均无统计学意义(P>0.05)。结论:本实验模型中未观察到31.25~2 000.00μg/L的Cry1Ab蛋白具有发育毒性。

妊娠糖尿病母鼠其胎儿心脏P38 MAPK的表达及意义

目的:了解p38丝裂原活化蛋白激酶(p38 mitogen-activated protein kinase,P38 MAPK)在妊娠糖尿病(gestational diabetes mellitus,GDM)母鼠胎儿心脏中的表达规律,旨在探讨其与妊娠期糖尿病母鼠其婴儿发育异常的内在联系。方法:取成年雌性SD大鼠随机分成两组,通过阴道涂片确定怀孕后分别注射链脲佐菌素(streptozoto-cin,STZ)及柠檬酸-柠檬酸钠缓冲液,建立GDM组和对照组,给药后72 h隔天测血糖及体质量。两组大鼠分别于孕后第12、15、19 d随机抽取剖宫,进行胎鼠心脏取材,HE染色观察心脏组织病理变化,免疫组化检测P38 MAPK的蛋白表达量,荧光定量PCR方法检测心脏组织P38 MAPK mRNA的表达。结果:①对照组子鼠心脏发育情况正常,未见心肌壁异常增厚、房室间隔病理性缺损及动脉圆锥干畸形等异常情况。高倍镜下可见心肌细胞呈椭圆形,胞浆丰富,核大,形态规则,染色均匀。GDM组12、15、19 d均可见子鼠心脏发育异常,包括室间隔缺损、圆锥干发育畸形、心肌异常肥厚及心腔扩大等,高倍镜下可见12、15 d心肌细胞结构较清晰,细胞肿胀,胞浆溶解,胞核形态尚规则,细胞结构不清。19 d细胞可见胞浆溶解,成片的无结构区,胞核形态不规则。②第12、15、19 d GDM组p38MAPK蛋白在胎鼠心肌细胞胞浆中的表达显著增强,与相应时间点的对照组相比均明显增高,在GDM组中,以第12 d的表达最强。③第12、15、19 d GDM组胎鼠心脏组织中p38 MAPK mRNA的相对表达量明显高于相应时间点的对照组。结论:妊娠糖尿病母鼠其胎鼠心脏发育异常的发生率明显升高。p38 MAPK蛋白及mRNA在妊娠糖尿病胎鼠孕12、15、19 d三个观察点的心脏表达水平明显增高,提示其可能参与妊娠糖尿病致心脏发育异常的过程。

双酚AP对斑马鱼心脏发育毒性作用研究

双酚AP(BPAP)是一种环境内分泌干扰物,在环境及人体中均有所分布。之前的研究阐述了双酚类似物BPAF对斑马鱼发育和心脏环化的影响及其潜在机制,但BPAP对心脏发育的毒性作用及其作用机制尚未阐明。该课题将斑马鱼胚胎暴露于不同浓度的BPAP,利用荧光显微技术与荧光定量PCR等方法,对染毒后96 h内的斑马鱼胚胎和幼鱼的孵化、心脏发育形态、心脏发育相关的4个心脏转录因子(Gata4、Hand2、Nkx2.5、Tbx5)的表达以及心肌细胞活性氧水平等4个方面进行研究,旨在研究BPAP对斑马鱼心脏发育毒性。实验结果表明,BPAP引起斑马鱼胚胎孵化率下降、死亡率升高、心率降低以及心脏环化障碍等,且与BPAP的剂量相关。深入研究表明,BPAP能诱导斑马鱼胚胎以及幼鱼心肌细胞氧化应激以及下调心脏发育有关的转录因子Gata4、Hand2、Nkx2.5、Tbx5。由此可知,BPAP影响斑马鱼胚胎发育和心脏环化障碍,通过诱导心肌细胞的氧化应激和下调心脏发育相关的转录因子。

香加皮对斑马鱼发育毒性及心脏毒性的影响

目的探讨香加皮水提液对斑马鱼的发育毒性及不同暴露时间药物对心脏毒性的影响。方法参照经济合作与发展组织推荐的方法,将受精后6小时(6 hour-post-fertilization,6 hpf)胚胎暴露在含有不同浓度香加皮水溶液的24孔板中,分别在24、48、72、96 hpf阶段测定胚胎/幼鱼的自主抽动次数、心率、孵化率、死亡率等指标。随后,使用不同浓度的香加皮水溶液处理发育至48、72、96 hpf的斑马鱼24小时,通过死亡率确定不同暴露阶段对斑马鱼心脏毒性的影响。结果各暴露组24 hpf自主抽动次数增加、48 hpf心率以及72 hpf孵化率显著降低,与正常对照组相比均有显著性差异(P<0.05);24 hpf低浓度给药组胚胎发育迟缓、眼点未发育、头部偏小或未发育,高浓度组发育畸形或停留在体节期;48 hpf胚胎卵黄囊畸形、黑色素生成抑制、尾芽未脱落;72 hpf幼鱼出现身体弯曲、心包水肿、卵黄囊畸形等中毒症状。不同发育阶段斑马鱼急性毒性暴露实验结果表明:香加皮对48、72、96 hpf斑马鱼的半数致死浓度(LC_(50))分别为:0.866 mg/m L、0.693 mg/m L和0.843mg/m L。结论香加皮对斑马鱼具有明显的发育毒性和心脏毒性,且48 hpf斑马鱼非常适合进行心脏毒性药物筛选。

不同发育时期小鼠心肌MyoG基因的表达分析

肌细胞生成素MyoG基因一直是肌肉研究中的一个热点基因,其在肌肉中的表达水平对该肌肉的生长发育至关重要。试验通过HE染色、免疫组织化学和q PCR技术研究了不同发育阶段小鼠心肌中MyoG的表达差异。结果表明,MyoG在幼年、性成熟、体成熟和老年4个时期的小鼠心肌胞质中均有表达,且其随着年龄增长逐渐下降,尤其在老年鼠中表达显著降低。结果提示,MyoG基因在心脏中的表达与心肌生长发育密切相关。

Overlapping Cardiac Programs in Heart Development and Regeneration

Gaining cellular and molecular insights into heart development and regeneration will likely provide new therapeutic targets and opportunities for cardiac regenerative medicine,one of the most urgent clinical needs for heart failure.Here we present a review on zebrafish heart development and regeneration,with a particular focus on early cardiac progenitor development and their contribution to building embryonic heart,as well as cellular and molecular programs in adult zebrafish heart regeneration.We attempt to emphasize that the signaling pathways shaping cardiac progenitors in heart development may also be redeployed during the progress of adult heart regeneration.A brief perspective highlights several important and promising research areas in this exciting field.

极低出生体重儿心脏迷走神经张力和学龄期发育结局的相关性分析

目的探讨极低出生体重儿(VLBWI)心脏迷走神经张力和学龄期发育结局的相关性分析。方法选择2007年5月至2010年5月中山大学附属第八医院重症监护病房收治的VLBWI患儿60例进行分析,于33~35周孕龄进行呼吸性窦性心律失常(RSA)成熟评分,并记录其他生理指标,探讨其与学龄期发育结局的相关性分析。结果学龄期发育结局与出生后3年的发育结局密切相关,多元回归分析结果显示,VLBWIRSA成熟程度与学龄期的社交能力相关。结论通过RSA测量可早期评估中枢神经系统自我调节能力及预测学龄期发育结局。

Comparison of developmental toxicity of different surface modified CdSe/ZnS QDs in zebrafish embryos

Quantum dots(QDs)are new types of nanomaterials.Few studies have focused on the effect of different surface modified QDs on embryonic development.Herein,we compared the in vivo toxicity of Cd Se/Zn S QDs with carboxyl(-COOH)and amino(-NH 2)modification using zebrafish embryos.After exposure,the two Cd Se/Zn S QDs decreased the survival rate,hatching rate,and embryo movement of zebrafish.Moreover,we found QDs attached to the embryo membrane before hatching and the eyes,yolk and heart after hatching.The attached amount of carboxyl QDs was more.Consistently,the Cd content in embryos and larvae was higher in carboxyl QD-treatment.We further observed that the two QDs caused zebrafish pericardial edema and cardiac dysfunction.In line with it,both carboxyl and amino QDs upregulated the transcription levels of cardiac development-related genes,and the levels were higher in carboxyl QD-treated groups.Furthermore,the chelator of Cd^2+diethylene triamine pentacetate acid could partially rescued the developmental toxicity caused by the two types of QDs suggesting that both the nature of QDs and the release of Cd^2+contribute to the developmental toxicity.In conclusion,the two Cd Se/ZnS QDs have developmental toxicity and affect the cardiac development,and the carboxyl QDs is more toxic possibly due to the higher affinity and more release to embryos and larvae.Our study provides new knowledge that the surface functional modification of QDs is critical on the development on aquatic species,which is beneficial to develop and applicate QDs more safely and environmentfriendly.

不同寄主植物桑寄生水提物对斑马鱼胚胎心脏发育毒性及机制研究

目的 研究不同寄主植物桑寄生Taxilli Herba水提物对斑马鱼胚胎心脏发育毒性及其机制,为桑寄生用药安全提供理论依据。方法 以受精后6 h(6 h post fertilization,6 hpf)正常发育的斑马鱼胚胎为动物模型,将桑树Morus alba、柳树Salix babylonica、油茶Camellia oleifera、夹竹桃Nerium indicum、苦楝Melia azedarach和漆树Toxicodendron trichocarpum 6种寄主植物桑寄生水提物各设置低、中、高3个药物浓度,分别处理斑马鱼胚胎,检测72 hpf孵化仔鱼的心脏形态、心率、心包面积、静脉窦(sinus venosus,SV)和动脉球(bulbus arteriosus,BA)间距、超氧化物歧化酶(superoxide dismutase,SOD)和过氧化氢酶(catalase,CAT)活性、心肌细胞的凋亡情况以及氧化应激相关酶基因[SOD1、CAT、谷胱甘肽S-转移酶2(glutathione S-transferase 2,GSTP2)]、心脏发育相关基因[GATA结合蛋白5(GATA binding protein 5,GATA5)、NK2同源框5(NK2 homeobox 5,NKX2.5)、肌球蛋白重链6(Myosin,heavy chain 6,MYH6)]及心肌细胞凋亡相关基因[B淋巴细胞瘤-2(B-cell lymphoma-2,Bcl-2)、Bcl-2相关X蛋白(Bcl-2 associated X protein,Bax)]的表达水平。结果 与空白组比较,除桑树寄主桑寄生外,其他5种桑寄生水提物处理的斑马鱼胚胎均出现不同程度的心包水肿、心率降低、心包面积和SV-BA间距增大(P<0.05、0.01),SOD和CAT活性降低(P<0.05、0.01),SOD1、CAT、GSTP2、GATA5、NKX2.5、MYH6的表达表现出明显的上调或下调(P<0.05、0.01)。夹竹桃、苦楝和漆树3种寄主桑寄生还观察到心肌细胞凋亡,Bcl-2表达和Bcl-2/Bax值明显降低(P<0.05、0.01)。结论 桑寄生对斑马鱼胚胎心脏发育毒性具有明显的寄主相关性,除桑树寄主桑寄生外,其他5种寄主桑寄生均表现出不同程度的心脏发育毒性,寄主植物不同,毒性机制也不同。

妊娠期糖尿病胎鼠心脏T-同源盒转录因子表达研究

目的探讨T-同源盒转录因子5(TBX-5)在母鼠妊娠糖尿病(GDM)胎鼠心脏中的分布、表达规律及其在胎鼠心脏发育异常中的作用。方法将成年SD雌鼠随机分成GDM组和对照组,通过阴道涂片确定怀孕后分别注射链脲佐菌素(STZ)及柠檬酸-柠檬酸钠缓冲液(PBS)制备GDM模型,于孕0、3、6、9、12、15、19天对母鼠进行尾静脉采血测血糖,并分别于孕后第12、15、19天进行胎鼠心脏取材,HE染色观察心脏组织病理变化,免疫组化检测TBX-5的表达并进行半定量检测。结果与对照组相比,GDM组胎鼠出现液化吸收胎、死胎、畸心胎的例数增多(P<0.01)。在大体观及高倍镜下,GDM组12、15、19天胎鼠心脏发育异常比例多于对照组(P<0.01)。在正常对照组及GDM组各亚组中,TBX-5均在第12天时表达最强,明显高于15、19天(P<0.01)。TBX-5在15天及19天时的表达无明显差别(P>0.05)。孕12、15、19天GDM组TBX-5在心肌细胞表达显著增强,与相应时间点的对照组相比均明显增高(P<0.01)。结论 TBX-5蛋白在妊娠糖尿病母鼠孕12、15、19天三个观察点胎鼠心脏的表达水平明显增高,提示其过度表达可能与妊娠期糖尿病致胎鼠心脏畸形的发生存在关联。

三氯乙烯的心脏发育毒性

我国先天性心脏病位居出生缺陷疾病的首位。除遗传因素外,环境因素也是先天性心脏病的重要诱因。三氯乙烯是分布广泛的环境有机污染物,流行病学研究显示其与先天性心脏病存在相关性。动物实验和体外实验也发现,三氯乙烯可引起心脏畸形,并干扰人胚胎干细胞向心肌细胞的分化。目前三氯乙烯心脏发育毒性的分子机制尚不明确。本综述从流行病学研究、动物实验、体外实验以及分子机制等方面探讨三氯乙烯心脏发育毒性的研究进展。

彩色多普勒超声联合胎儿NT检查在双胎妊娠胎儿发育畸形诊断

目的探讨彩色多普勒超声脐带动脉搏动指数(UA)、脑动脉搏动指数(MCA)联合胎儿颈后透明带心血管参数(NT)在双胎妊娠胎儿发育畸形诊断中的应用价值。方法随机选取孕中期双绒毛膜双羊膜双胎妊娠(病例来源:2016年4月~2017年4月)120例,均行产前彩色多普勒超声UA、MCA、NT检测。以最终尸检核查和妊娠结局随访结果作为胎儿畸形诊断的金标准,对比发育正常胎儿与发育畸形胎儿彩超UA、MAC和NT的差异,采用ROC曲线法分析单纯彩超UA、单纯彩超MAC、单纯超声NT及三者联合诊断胎儿发育畸形的敏感度、特异度、准确度。结果本组120例病例的尸检核查及随访(分娩后1年)结果显示,102例双胎胎儿发育均完全正常,15例双胎之一发育异常,3例双胎发育均异常,胎儿发育畸形率为8.75%。发育畸形胎儿的彩超UA、MAC和NT均高于发育正常胎儿(P<0.05)。以彩超UA、MAC联合NT诊断双胎妊娠胎儿发育畸形的准确度、敏感度、特异度(85.98%、87.11%、88.93%)高于单纯彩超UA诊断(73.48%、75.43%、68.43%)、单纯彩超MAC诊断(74.63%、73.09%、70.18%)和单纯超声NT诊断(74.12%、73.54%、71.35%)(P<0.05)。结论双胎妊娠的胎儿发育畸形风险较高,与正常发育双胎妊娠胎儿相比,发育畸形双胎妊娠胎儿的彩超UA、MAC和NT值均相对较高,超声UA、MCA联合NT检查在双胎妊娠胎儿发育畸形诊断中具有较高价值,且明显优于单纯彩超UA、单纯彩超MAC、单纯超声NT的诊断效能。

Zebrafish Foxc1a controls ventricular chamber maturation by directly regulating wwtr1 and nkx2.5 expression

Chamber maturation is a significant process in cardiac development. Disorders of this crucial process lead to a range of congenital heart defects. Foxc1a is a critical transcription factor reported to regulate the specification of cardiac progenitor cells. However, little is known about the role of Foxc1a in modulating chamber maturation. Previously, we reported that foxc1a-null zebrafish embryos exhibit disrupted heart structures and functions. In this study, we observe that ventricle structure and cardiomyocyte proliferation are abolished during chamber maturation in foxc1a-null zebrafish embryos. To observe the endogenous localization of Foxc1a in the hearts of living embryos, we insert eyfp at the foxc1a genomic locus using TALEN. Analysis of the knockin zebrafish show that foxc1a is widely expressed in ventricular cardiomyocytes during chamber development. Cardiac RNA sequencing analysis reveals the downregulated expression of the Hippo signaling effector wwtr1. Dual-luciferase and chromatin immunoprecipitation assays reveal that Foxc1a can bind directly to three sites in the wwtr1 promoter region. Furthermore, wwtr1m RNA overexpression is sufficient to reverse the ventricle defects during chamber maturation. Conditional overexpression of nkx2.5 also partially rescues the ventricular defects during chamber development. These findings demonstrate that wwtr1 and nkx2.5 are direct targets of Foxc1a during ventricular chamber maturation.

环境内分泌干扰物暴露引起心脏发育毒性的研究进展

环境内分泌干扰物(EDCs)普遍存在于各种生活场景中,可结合机体中的不同受体,干扰内分泌系统正常功能而引发各组织器官病变。本文对环境中常见几类EDCs暴露致心脏形态结构生长畸形和心功能异常,以及其有关机制包括氧化应激、炎症反应、信号转导、心脏发育相关转录调控因子表达改变、受体介导途径和细胞凋亡等的研究状况进行综述,了解EDCs致心脏发育毒性的过程及其暴露对心脏发育的影响程度,为EDCs的毒性机制研究及防治心脏相关疾病提供理论基础和研究方向。