Micromanaging cardiac regeneration:Targeted delivery of micro RNAs for cardiac repair and regeneration

The loss of cardiomyocytes during injury and disease can result in heart failure and sudden death, while the adult heart has a limited capacity for endogenous regeneration and repair. Current stem cell-based regenerative medicine approaches modestly improve cardiomyocyte survival, but offer neglectable cardiomyogenesis. This has prompted the need for methodological developments that crease de novo cardiomyocytes. Current insights in cardiac development on the processes and regulatory mechanisms in embryonic cardiomyocyte differentiation provide a basis to therapeutically induce these pathways to generate new cardiomyocytes. Here, we discuss the current knowledge on embryonic cardiomyocyte differentiation and the implementation of this knowledge in state-ofthe-art protocols to the direct reprogramming of cardiac fibroblasts into de novo cardiomyocytes in vitro and in vivo with an emphasis on micro RNA-mediated reprogramming. Additionally, we discuss current advances on state-of-theart targeted drug delivery systems that can be employed to deliver these micro RNAs to the damaged cardiac tissue. Together, the advances in our understanding of cardiac development, recent advances in micro RNAbased therapeutics, and innovative drug delivery systems, highlight exciting opportunities for effective therapies for myocardial infarction and heart failure.

Nampt is involved in DNA double-strand break repair

DNA double-strand break(DSB) is the most severe form of DNA damage,which is repaired mainly through high-fidelity homologous recombination(HR) or error-prone non-homologous end joining(NHEJ).Defects in the DNA damage response lead to genomic instability and ultimately predispose organs to cancer.Nicotinamide phosphoribosyltransferase(Nampt),which is involved in nicotinamide adenine dinucleotide metabolism,is overexpressed in a variety of tumors.In this report,we found that Nampt physically associated with CtIP and DNA-PKcs/Ku80,which are key factors in HR and NHEJ,respectively.Depletion of Nampt by small interfering RNA(siRNA) led to defective NHEJ-mediated DSB repair and enhanced HR-mediated repair.Furthermore,the inhibition of Nampt expression promoted proliferation of cancer cells and normal human fibroblasts and decreased β-galactosidase staining,indicating a delay in the onset of cellular senescence in normal human fibroblasts.Taken together,our results suggest that Nampt is a suppressor of HR-mediated DSB repair and an enhancer of NHEJ-mediated DSB repair,contributing to the acceleration of cellular senescence.

CELLULAR SUBSTANCE EXUDATION AND SEED VIGOUR

In this paper, seeds of pinus koraiensis which has a characteristic of deep dormancy were selected as an experiment material, and the relation of cellular substance exudation to seed vigour is discussed based on the dormant state, the different measuring parts and the imbibed state of seeds before testing, as well as on the respiration of embryo and endosperm. The major measured results arc as follows: (1) After soaking for 24h, the dry embryo conductivity of sccdlot L is greater that than of sccdlot H: (2) The substance exudation of dry embryo of sccdlot H is less than that of sccdlot L; (3) After seeds imbibed, the substance exudation of dormant embryo of sccdlot H is more than that of sccdlot L; (4) After germination hastening treatment, the substance exudation of H embryos is greater than that of L embryos; (5) After artificially accelerated ageing treatment, the embryo conductivity of imbibed seeds has a positive correlation with seed vigour.

推拿治疗骨骼肌损伤的分子生物学机制研究进展

骨骼肌损伤是人们生活中时常发生的一类疾患,严重者可造成肢体活动障碍。推拿治疗骨骼肌损伤类疾病有显著疗效,通过检索近5年来推拿治疗急慢性骨骼肌损伤的相关基础实验文献,对推拿治疗骨骼肌损伤的分子生物学机制研究进展进行总结、归纳,从调控肌卫星细胞、相关生长因子及炎性因子、信号通路、细胞自噬等方面进行综述,以期为临床治疗骨骼肌损伤提供有力的理论依据,并对骨骼肌损伤的研究提供新思路。

Proteomic Alterations in Human Dermal Fibroblasts under Photo-Induced Pollution Caused by Excessive Solar Irradiations such as Infra-Red, Blue Light, UVA and UVB

Background: The skin serves as the first line of defense for the human body. Direct sunlight contains damaging radiations that can speed up the ageing process of the skin, resulting in wrinkles, leathery skin, dark patches, and solar elastosis. Objectives: To evaluate the effect of multiple solar irradiation related factors at the protein level in human dermal fibroblast (HDF). The overall effect of individual solar irradiations such as Infrared A (IRA), blue light (BL), UVA, and UVB on HDF cells and the extent of molecular level aberrations to be assessed and compared against each. Methods: Label-free quantitative proteomics (MS/MS) approach has been adopted in this study to observe the protein level changes induced in the HDF cells through various exposures of full light sources. Following that, downstream insilico analysis has been carried out. Results: In this study, it is demonstrated all the four different solar irradiations significantly contribute to the molecular degeneration of skin cells through various mechanisms. This study confirms that BL down-regulates DNA repair proteins and the skin cells-HDF stimulate the histone proteins as a response mechanism to maintain the chromosomal integrity. Conclusions: The proteomics experiment carried out in the current study intends to support the future sun care products based on full light protection technology that can be custom designed to provide complete protection from the solar radiation. Similar technology could enhance the further investigations for deeper understanding of induction, mode of action, and prevention of skin damage from extensive solar irradiation.

腺病毒介导的p33^(ING1b)过表达显著促进衰老细胞的DNA损伤修复

p33ING1b是一个较晚发现的肿瘤抑制基因ING1的主要表达形式,但是它在细胞衰老过程中的作用特别是对衰老细胞DNA损伤修复的影响还没有被阐明.本研究首先用2BS细胞构建了细胞衰老模型,通过RTPCR和Western印迹技术证实p33ING1b在衰老细胞中的表达水平下调;然后,通过构建和包装包含p33ING1b基因的腺病毒,将p33ING1b导入年轻和衰老细胞中并使其过表达,用HCR(hostcellreactivation,宿主细胞复活)方法检测年轻细胞和衰老细胞DNA损伤修复能力.实验表明,相对于年轻细胞,p33ING1b过表达使衰老细胞的DNA的损伤修复能力显著增加,说明p33ING1b在衰老细胞中的表达下调与衰老细胞DNA损伤修复能力的下降有关,也进一步证实了p33ING1b在细胞衰老过程中起着十分重要的作用.

胚胎型仿生电路中具有自修复性能的存储器设计

胚胎型仿生电路是一种芯片级容错数字电路,其工作机制为汲取生物体生长过程的灵感从而使得数字系统具有自主容错能力。该电路是由二维电子细胞阵列组成,文中分析了这种数字电路的结构和容错机制,讨论了细胞的主要组成部件的设计,并基于海明码(Hamming Code)为细胞中的存储器设计了一种具有自检测和自修复能力的结构。最后,以4×4乘法器为应用实例,通过仿真实验验证了细胞中存储器的自诊断、自修复能力和该仿生电路的自修复能力。

DNA损伤修复机制和糖尿病造成的动脉粥样硬化

动脉粥样硬化及其所引起的心肌梗死、脑卒中、冠状动脉粥样硬化性心脏病(冠心病)等是导致老年人病死率增加的重要原因。DNA损伤是激活DNA损伤修复路径导致细胞早衰的重要原因,而动脉粥样硬化中存在DNA损伤及DNA损伤修复机制参与的证据。糖尿病作为心血管疾病危险因素具有导致DNA损伤,从而加速血管老化的作用。该文综述了动脉粥样硬化疾病中DNA损伤和DNA双链损伤修复机制的研究进展,从而为防治动脉粥样硬化疾病提供新的思路。

基于三维多胞结构的汽车吸能盒优化设计

为改善汽车吸能盒在低速碰撞情况下的力学表现,将一种新型具有负泊松比效应的多胞结构设计为汽车前纵梁的吸能盒.通过对新型负泊松比多胞结构形状参数的研究,确立了多胞结构中特定的元胞几何参数及元胞层数作为优化变量,结构质量以及所吸收的能量作为优化目标.首先通过最优拉丁超立方的方法在变量空间内进行样本点的选取并采用ABAQUS进行有限元仿真计算,然后由Isight软件根据样本点的计算结果对优化变量与优化目标建立三阶响应面模型,最终采用NCGA对响应面模型进行优化.将优化结果进行RCAR(Research Council for Automobile Repairs)标准模型仿真计算,结果验证了这一新型负泊松比吸能盒可以在较小的质量下满足RCAR低速碰撞标准.

外泌体在组织修复及抗瘢痕治疗中的研究进展

促进皮肤创面愈合、减少瘢痕形成是皮肤科及整形外科的治疗重心。近年来研究发现,外泌体(EXOs)作为细胞与细胞之间的通信工具参与了旁分泌作用,并被发现在多种病理生理过程及疾病进程中发挥着重要作用,逐渐成为肿瘤免疫领域及再生医学领域研究的热点。外泌体可促进创面修复,通过抑制早期炎症反应、促进血管生成和细胞增殖、调控胶原重塑来抑制瘢痕形成,为皮肤创面修复提供了一个全新的促愈合方法。外泌体在创面修复及抗瘢痕治疗中具有广阔的应用前景,有望为创伤修复及抗瘢痕治疗开拓新路径。

胃息肉及胃癌组织中PMS2、MSH6、C-met的表达水平及其临床应用价值

目的对比分析胃息肉及胃癌组织中错配修复基因PMS2、MSH6、细胞间质表皮转化因子(C-met)的表达及其在胃息肉向胃癌转化中的预测价值。方法选取2017年7月至2019年12月安徽理工大学第一附属医院收治的143例胃息肉患者及45例胃癌患者作为研究对象,对比胃息肉及胃癌组织中PMS2、MSH6、C-met的表达水平及其相关性,建立PMS2、MSH6、C-met的受试者工作特征曲线(ROC曲线),分析其在胃息肉向胃癌转化中的预测价值。结果不同病理类型胃息肉及胃癌组织中PMS2、MSH6、C-met阳性表达率比较差异有统计学意义(P<0.01),其中PMS2、MSH6的阳性表达率比较,胃癌组织<腺瘤性息肉<胃底腺息肉<增生性息肉<炎性息肉;C-met阳性表达率比较,胃癌组织>腺瘤性息肉>胃底腺息肉>增生性息肉>炎性息肉。Spearman相关分析结果显示,PMS2、MSH6、C-met表达水平与胃息肉病理类型及病变严重程度呈显著相关性(r=-0.324、r=-0.319、r=0.298,均P<0.001),且PMS2表达与MSH6表达呈正相关(r=0.796,P<0.001),PMS2、MSH6表达与C-met表达呈负相关(r=-0.492、r=-0.483,均P<0.001);ROC曲线分析结果显示,PMS2预测胃息肉向胃癌转化的灵敏度为83.3%、特异度为74.8%,MSH6预测胃息肉向胃癌转化的灵敏度为82.5%、特异度为73.6%,C-met预测胃息肉向胃癌转化的灵敏度为77.8%,特异度为71.2%。结论PMS2、MSH6、C-met表达与胃息肉病理类型及病变严重程度显著相关,可能参与不同病理类型胃息肉向胃癌的发生发展,明确胃息肉的病理类型并检测PMS2、MSH6、C-met表达水平对防治胃息肉向胃癌转化具有重要意义。

7050铝合金内部沿晶微裂纹热塑性修复的元胞自动机模拟

根据7050铝合金单道次热压缩变形实验数据,对建立微裂纹修复的元胞自动机(CA)模型所需相关参数进行辨识和计算。利用Microsoft Visual C++平台编制了包含拓扑变形机制、位错密度演变机制、动态再结晶动力学机制的沿晶微裂纹热塑性修复的微观组织CA演化规则。针对裂纹表面和母相晶界的不同特征,提出再结晶过程中表面能和晶界能驱动下不同的晶粒长大方式。CA模拟结果表明:一定条件下的热塑性变形和动态再结晶可完全修复材料内部微裂纹,且裂纹愈合过程中出现的分段愈合特征与实验结果相吻合,但裂纹愈合的形貌演化取决于裂纹形态、裂纹表面形核率和形核位置、新晶粒长大方向与速度。

存在共因失效的复杂可修系统可靠性评估

鉴于传统方法在处理存在由部件选择性失效传播引起的共因失效的复杂可修系统可靠性与可用性评估问题时的缺陷,提出一种基于元胞自动机思想的蒙特卡洛模拟方法用以评估存在共因失效的复杂可修系统的可靠性。该方法首先将系统转化成二终端网络,然后基于问题的基本假设去模拟不同时刻下网络各边对应的状态值,利用元胞自动机并行搜索的优势判断每次模拟过程中不同时刻下网络的连通性,从而推导出计算系统可靠性、瞬时可用性、区间可用性、系统平均维修时间以及系统单位时间平均维修次数的具体算法。最后,通过算例对算法进行了说明。

外泌体在再生修复及抗衰老领域的研究进展

如何修复各类疾病引起的组织器官损伤是再生医学的研究热点。近年来,干细胞凭借其分泌活性生物成分的功能,成为治疗中的主力。其作用机制是其旁分泌作用可调节再生修复能力。这种分泌型再生环境的重要构件就是外泌体——一种直径为40~150 nm的囊泡物质,可介导蛋白质和核酸跨细胞界限的转移运输。本文对基于干细胞的修复如何向外泌体过渡,以及外泌体的各种功能和机制进行综述。

腹腔镜下胃十二指肠球部溃疡穿孔修补术与开腹手术的比较研究

目的:探讨腹腔镜下胃十二指肠球部溃疡穿孔修补术与开腹手术对患者机体的影响作用机制。方法:2008年8月-2013年5月江苏省盐城市第三人民医院普外科行胃、十二指肠球部溃疡穿孔修补术患者58例,其中30例行腹腔镜下胃、十二指肠球部溃疡穿孔修补术,28例行开腹胃十二指肠球部溃疡穿孔修补术,分析两组患者的临床资料及实验数据。结果:1)术后肠功能恢复时间、住院时间、术后抗生素使用时间等方面,腹腔镜组明显优于开腹组。2)腹腔镜组患者外周血WBC计数、CRP水平等炎症指标水平显著低于开腹组。3)ELISA检测显示,腹腔镜组患者血清IL-6和TNF-α炎症因子水平明显低于开腹组。4)腹腔镜手术对患者T淋巴细胞亚群分布影响小于开腹组,表明腹腔镜组患者机体细胞免疫状态较稳定。结论:腹腔镜下行胃十二指肠球部溃疡修补术对机体造成轻微的创伤,对脏器干扰小,全身炎症反应程度轻,对机体细胞免疫功能干扰少,并发症少,更有利于患者的恢复,是一种安全有效的手术方式。

肝受体同系物1对大鼠急性胰腺炎细胞模型中腺泡细胞损伤修复的影响及其机制

目的探讨肝受体同系物1(NR5A2)对大鼠急性胰腺炎(AP)细胞模型中腺泡细胞损伤修复的影响及其机制。方法将大鼠胰腺腺泡细胞系AR42J细胞分为模型组和正常对照组,模型组予100 nmol/L雨蛙素刺激24 h构建体外AP模型,正常对照组予相同体积的磷酸盐缓冲液培养24 h。取对数生长期的AR42J细胞分为对照组、沉默NR5A2组(KD组)和对照慢病毒感染组(LV-control组)。KD组用慢病毒感染AR42J细胞,对照组不处理,LV-control组感染相同体积的对照慢病毒载体。慢病毒感染96 h后,对照组、KD组和LV-control组均予2%胎牛血清饥饿12 h,100 nmol/L雨蛙素刺激细胞24 h,分别设为正常模型组(CAE组)、沉默NR5A2+雨蛙素组(KC组)和对照慢病毒+雨蛙素组(LV-control+CAE组)。定量逆转录聚合酶链反应检测白细胞介素1β(IL-1β)、IL-6、肿瘤坏死因子α(TNF-α)的m RNA表达量,比色法检测细胞淀粉酶的活性,蛋白质印迹法检测NR5A2和核因子κB P65的表达,细胞增殖实验检测细胞的增殖情况。结果模型组IL-1β、IL-6、TNF-αm RNA及淀粉酶表达量均高于正常对照组(均P <0.001),体外AP模型构建成功。模型组NR5A2 m RNA及蛋白表达量均低于正常对照组,核因子κB P65表达量高于正常对照组(均P <0.05)。慢病毒感染96 h后,KD组NR5A2 m RNA及蛋白表达量均低于对照组和LV-control组[(0.47±0.07)比(1.00±0.07)、(1.00±0.08),(0.39±0.10)比(1.01±0.08)、(1.04±0.20)](均P <0.05)。雨蛙素刺激24 h后,KC组IL-1β、IL-6、TNF-αm RNA及淀粉酶表达量均高于CAE组及LV-control+CAE组(均P <0.05)。KC组Ed U阳性百分比低于对照组、CAE组及LV-control+CAE组[(7.97±0.29)%比(71.70±1.64)%、(51.63±0.90)%、(45.37±1.31)%](P <0.001)。KC组核因子κB P65表达量高于CAE组和LV-control+CAE组(P <0.001)。结论在体外AP细胞模型中,NR5A2的表达降低可以加重腺泡细胞的炎症反应,抑制腺泡细胞的增殖和再生,影响腺泡细胞的损伤修复,其机制可能与上调核因子κB的表达有关。

体细胞重编程的转化医学研究

脑血管疾病、痴呆、糖尿病、恶性肿瘤、骨退行性病等重大临床疾患的发病率、患病率、病死率和致残率居高不下,细胞保护与细胞损伤修复药物、策略和方法的转化研发、应用与推广一直停滞不前或进展过缓应是其重要原因之一。本研究通过医学、生物学、数据库构建、程序编写、软件研制、统计分析及管理工程等多个领域专业人员的通力合作,对2012年诺贝尔生理学或医学奖两位获奖者关于"成熟细胞可以被重编程而多能化"的原始研究及其被引用的大规模复杂信息数据做整体定量对比和局部关联解析,探讨体细胞重编程研究的临床应用前景和实现策略,发现两位获奖者原创性研究及其影响在时间、学科、科学和技术等多个层面与角度上差异具有统计学意义,揭示和证明了加强与加快转化医学和转化神经科学研究的时代意义、紧迫需求、重要方向、目标与路径及我国医学科研管理体系因此所面临的重要挑战。

腹腔镜胃十二指肠溃疡穿孔修补术与传统开腹手术的疗效及细胞免疫功能的影响比较

目的:观察比较腹腔镜胃十二指肠溃疡穿孔修补术与传统开腹手术的临床疗效以及细胞免疫功能的影响。方法:随机选择2015年1-12月本院进行胃十二指肠穿孔治疗患者60例,根据来诊时间序列号单号为观察组,双号为对照组,每组各30例。观察组患者行腹腔镜胃十二指肠溃疡穿孔修补术,对照组患者行开腹手术。观察两组患者手术时间、术中出血量、肠蠕动恢复时间、住院时间、感染、肠粘连等术后并发症情况以及CD3^+、CD4^+、C反应蛋白(CRP)在术前、术后第1、3、5天的变化。结果:观察组患者手术时间明显长于对照组,但是术中出血量、肠蠕动恢复时间、住院时间以及并发症发生情况均明显少于对照组,两组比较差异均有统计学意义(P<0.05)。两组患者CD3^+、CD4^+手术前后比较差异均无统计学意义(P>0.05),但是观察组术后1、7 d明显高于对照组,两组比较差异均有统计学意义(P<0.05)。两组患者术后CRP均有所升高,但对照组升高的更为明显,两组比较差异有统计学意义(P<0.05)。结论:腹腔镜十二指肠溃疡穿孔修补术的临床疗效优于传统开腹手术,且其对患者细胞免疫功能的影响则明显更低,值得临床推广应用。

DLX2基因诱导细胞成骨及分化的机制研究

DLX2基因位于第2号染色体长臂,可参与机体多种生长发育过程。该基因在成骨与成软骨形成诱导中的作用引起学者们的广泛关注。目前对DLX2基因在各不同类型细胞的成骨与成软骨分化中所涉及的分子及信号通路已有一定研究,但对于其中涉及的不同分子与信号通路间的交互作用及具体作用机制尚未阐明。因此,深入探究DLX2基因与各成骨与成软骨信号分子通路间的交联,可以进一步明确和重新认识该基因在人体组织学骨愈合再生过程中的作用及具体机制,为今后临床开发新的骨修复治疗方法提供理论依据和新思路。

Modification of tubular chitosan-based peripheral nerve implants: applications for simple or more complex approaches

Surgical treatment of peripheral nerve injuries is still a major challenge in human clinic.Up to now,none of the well-developed microsurgical treatment options is able to guarantee a complete restoration of nerve function.This restriction is also effective for novel clinically approved artificial nerve guides.In this review,we compare surgical repair techniques primarily for digital nerve injuries reported with relatively high prevalence to be valuable attempts in clinical digital nerve repair and point out their advantages and shortcomings.We furthermore discuss the use of artificial nerve grafts with a focus on chitosan-based nerve guides,for which our own studies contributed to their approval for clinical use.In the second part of this review,very recent future perspectives for the enhancement of tubular(commonly hollow)nerve guides are discussed in terms of their clinical translatability and ability to form three-dimensional constructs that biomimick the natural nerve structure.This includes materials that have already shown their beneficial potential in in vivo studies like fibrous intraluminal guidance structures,hydrogels,growth factors,and approaches of cell transplantation.Additionally,we highlight upcoming future perspectives comprising co-application of stem cell secretome.From our overview,we conclude that already simple attempts are highly effective to increase the regeneration supporting properties of nerve guides in experimental studies.But for bringing nerve repair with bioartificial nerve grafts to the next level,e.g.repair of defects>3 cm in human patients,more complex intraluminal guidance structures such as innovatively manufactured hydrogels and likely supplementation of stem cells or their secretome for therapeutic purposes may represent promising future perspectives.