基于组学的生物信息学分析在Alzheimer’s病生物标志物研究中的应用进展

Alzheimer’s病(AD)是一种引起认知下降的慢性神经退行性疾病,是痴呆的最常见原因,严重危害老年人的生命健康。目前,AD的发病机制尚不清楚,临床发现患病时多已进展至中后期,且缺乏早期的诊疗手段。基于组学的生物信息学分析方法是一个新兴的研究领域,可以揭示神经元退变、凋亡等生物学过程,对探索AD的发病机制及寻找早期的诊疗手段至关重要。本文就基于组学的生物信息学技术在AD生物标志物研究中的应用进行综述。

轻度Alzheimer’s病患者血浆氨水平对脑脊液β-淀粉样蛋白含量及认知功能的影响

目的探讨轻度Alzheimer’s病(AD)患者血浆氨水平对CSFβ-淀粉样蛋白(Aβ)含量及认知功能的影响。方法以本院收治的108例轻度AD患者(MMSE≥16分)和47名志愿者(正常对照组)为研究对象,行认知功能评估及血浆氨检测。轻度AD患者根据血浆氨水平分为血浆氨正常组(ADA-组)、血浆氨升高组(ADA+组)。检测AD患者CSF的Aβ42、Aβ40、总tau和磷酸化tau水平并进行比较。结果与正常对照组比较,ADA-组及ADA+组MMSE、蒙特利尔认知评估量表(MoCA)评分显著降低(均P<0.001),ADA-组MoCA评分显著高于ADA+组(P<0.001)。ADA+组血浆氨水平显著高于ADA-组及正常对照组(均P<0.001)。ADA+组Aβ42、Aβ40水平显著低于ADA-组(t=2.29,P=0.024;t=2.72,P=0.008)。ADA+组血浆氨水平与MoCA评分(r=-0.47,P<0.001)及CSF Aβ42水平(r=-0.63,P<0.001)呈显著负相关。CSF Aβ42水平在血浆氨水平和认知功能之间存在显著中介效应,中介效应占总效应的百分比为45.94%。结论部分AD患者存在血浆氨升高,高血氨可能通过降低CSF Aβ42水平,导致Aβ42沉积形成斑块,使认知障碍进一步加重。

多奈哌齐治疗Alzheimer’s病有效血药浓度及影响因素

多奈哌齐(DNP)是治疗轻中度Alzheimer’s病(AD)的一线用药,有效的药物浓度是提高大脑皮质乙酰胆碱含量、改善认知的关键。DNP治疗轻中度AD患者的疗效和血药浓度密切相关,推荐剂量下,给药剂量越高,效果越显著。影响多奈哌齐血药浓度及治疗效果的因素主要包括载脂蛋白E、肝药酶CYP 2D6、肝药酶CYP 3A4、年龄、雌激素受体、肝功能、肾功能、对氧化酶、丁酰胆碱酯酶、乙酰胆碱受体亚基及血药浓度检测手段等。本文就血药浓度的监测及影响因素的研究进展进行探讨,以期为临床合理、精准及个体化用药提供参考。

Alzheimer’s病患者血清miR-182表达水平的变化及临床意义

目的探讨血清标记物miR-182在Alzheimer’s病(AD)患者血清中的含量变化及临床意义。方法收集40例首诊AD患者美金刚治疗前后的血清样本,并以40名健康志愿者作为对照。AD组于治疗前后,健康对照组于入组时采用荧光定量PCR技术检测血清miR-182表达水平,ROC曲线评价血清miR-182表达水平对AD诊断的敏感度和特异度。采用MMSE和蒙特利尔认知评估量表(MoCA)量表评价AD患者治疗前后的认知功能,并检测患者血清脑源性神经营养因子(BDNF)水平,分析血清miR-182表达水平与MMSE、MoCA评分和BDNF的相关性。结果 AD组及健康对照组治疗前血清miR-182的表达水平差异具有统计学意义(z=-7.612,P<0.01)。AD组患者治疗后血清miR-182表达水平显著低于治疗前(z=-4.302,P<0.05)。AD组治疗后MMSE评分及MoCA评分显著高于治疗前(z=-2.382,z=-2.401;均P<0.05)。血清miR-182表达水平与MMSE和MoCA量表评分呈负相关(r=-0.546,r=-0.581;均P<0.01)。ROC曲线显示,血清miR-182曲线下面积分别为0.904(95%CI:0.846-0.963,P<0.01),灵敏度为89.1%,特异度为80.0%。初诊AD患者血清miR-182表达水平与BDNF水平呈现负相关(r=-0.762,P<0.01)。结论 miR-182作为血清学标记物,可较好的应用于AD的临床诊断与病情评估,在AD发病中起重要作用。

SNHG14在Alzheimer’s病患者血清中表达及其与神经细胞自噬相关性研究

目的检测SNHG14在Alzheimer’s病(AD)患者血清中的表达水平及在小鼠神经元细胞系HT-22细胞中敲低SNHG14后对细胞自噬相关基因表达的影响。方法取50例AD患者(AD组)血清和50例正常对照者(正常对照组)血清的总RNA,并逆转录为cDNA,实时荧光定量PCR检测其中SNHG14的相对表达水平,并分析其与患者临床参数之间的相关性;在小鼠神经元细胞系HT-22细胞中敲低SNHG14后,检测细胞中自噬相关蛋白5(ATG5)表达情况。结果AD组血清中SNHG14的表达水平[(45.33±7.04)×10-4]明显低于正常对照组[(74.07±9.63)×10-4],差异具有统计学意义(t=2.410,P=0.0178)。AD组血清中SNHG14表达水平与患者年龄(P=0.370)、吸烟(P=0.276)、性别(P=0.778)均无明显相关性。神经元细胞HT-22中敲低SNHG14后细胞自噬相关基因ATG5表达较正常对照组明显下降,差异具有统计学意义(t=3.049,P=0.038)。结论SNHG14在AD患者血清中的表达下调,其参与病发病可能的机制为调节神经元细胞自噬。

SORL1、EPHA1基因多态性与新疆维吾尔族及汉族Alzheimer’s病的相关性研究

目的研究新疆地区汉族、维吾尔族Alzheimer’s病(AD)患者SORL1基因、EPHA1基因多态性,探讨SORL1基因及EPHA1基因多态性与AD的相关性。方法应用PCR测序技术对新疆地区131例散发AD患者(维吾尔族72例、汉族59例)以及128例对照者(维吾尔族63例、汉族65例)进行SORL1基因及EPHA1基因7个SNP位点rs1699102、rs1010159、rs2282649、rs3824968、rs11767557、rs1525119、rs10233030基因多态性分析。结果SORL1基因中rs1699102、rs1010159、rs2282649、rs3824968病例组和对照组比较差异无统计学意义(均P>0.05)。EPHA1基因型rs11767557、rs1525119、rs10233030位点分布在病例组和对照组之间差异无统计学意义(均P>0.05)。SORL1基因的rs1010159、rs2282649、rs3824968单倍体在维吾尔族AD患者与汉族AD患者比较中差异有统计学意义(均P<0.05),EPHA1基因中rs1525119、rs10233030形成单体型在维吾尔族AD患者与汉族AD患者比较中差异有统计学意义(均P<0.05)。结论SORL1基因的4个SNP位点及EPHA1基因的3个SNP位点与新疆AD患者发生无明显相关性。

神经胶质细胞及其在Alzheimer’s病中的作用

目的 综述神经胶质细胞 ,特别是星型胶质细胞、小胶质细胞在Alzheimer’s病发病机制中的异常活化。方法 根据国内外文献 ,较全面介绍了胶质细胞在中枢神经系统中和Alzheimer’s病的重要作用。结果与结论 神经胶质细胞构成中枢神经系统 (CNS)微环境 ,异常活化的胶质细胞可以分泌细胞因子 ,补体 ,氧自由基 ,启动炎症反应 ,进一步加剧Alzheimer’s病神经元损伤和神经的变性。神经胶质细胞的异常活化可能是AD的发病机制之一。

Alzheimer’s病相关癫痫的研究进展

轻度认知障碍或Alzheimer’s病(AD)的患者容易出现癫痫发作和临床表现不明显的异常神经电活动,这可能与认知能力下降有关。与年龄相匹配的认知正常人群相比,AD患者癫痫发作的患病率亦有所增加。本文综述了近年来有关AD患者发生癫痫样发作/癫痫的研究,以便临床医生警惕性提高,防止漏诊和误诊。

764-3对Alzheimer’s病样大鼠的治疗作用

向大鼠侧脑室内注射聚集态的β 淀粉样多肽 (Aβ 2 5 35 ) 15mmol后 ,动物在三种行为试验中都出现学习记忆障碍 ,同时海马和大脑皮层的胆碱乙酰转移酶 (ChAT)活性下降。这表明应用Aβ 2 5 35脑室内注射造成Alzheimer’s病动物模型的可行性。 76 4 3于手术后早期多次给药 (2mg/ 0 5mL 每天 1次i p )明显改善Aβ 2 5 35所致的学习记忆缺陷 ,并使海马的ChAT回升。本文又首次报告Aβ 2 5 35引起前脑多个脑区的一氧化氮合酶(NOS)表达上调 ,76 4 3拮抗此反应。结果提示 76 4 3的作用机制与其在脑内提高ChAT活性和抑制病理性的NOS表达有关。

血管周围间隙与Alzheimer’s病相关性的研究

Alzheimer’s病(AD)是一种渐进性神经系统变性病。近年来发现小血管病在AD患者中广泛存在并参与AD的病理过程。血管周围间隙(PVS)是蛛网膜下腔小动静脉穿过脑实质时形成的围绕在血管周围的腔隙,为脑小血管病的影像学表现形式之一。本文对PVS中CSF-组织间液循环通路、PVS内β样淀粉蛋白清除机制以及PVS扩张的形成因素进行阐述,探讨PVS扩张对AD的发展及认知功能的影响。PVS与AD相关性的研究可能对AD药物治疗的研发提供一定指导意义。

等电聚焦双向电泳法分析Alzheimer’s病脑皮质蛋白

目的 :利用等电聚焦双向电泳法 (2 DE)研究Alzheimer’s病 (AD)患者脑皮质蛋白的生化改变 ,并探讨该方法的重复性和可靠性。方法 :利用 2 DE分析AD患者和健康对照者的额、颞叶皮质蛋白 ;通过 2 DE计算机分析系统对结果进行定性、定量分析。结果 :2 DE图谱可识别蛋白或多肽 80 0余种 ,发现 31个电泳点在实验组和对照组有显著性量性差异 ,有两种未鉴别蛋白在AD脑出现频率较高。结论 :所采用的2 DE具有较高的重复性和良好的分辨率。AD脑蛋白的改变以量变为特点。

高血压及降压药与Alzheimer’s病的关系

痴呆有许多病因,最常见的为Alzheimer’s病(AD)和血管性痴呆(VD)。VD继发于脑血管病,而AD为神经变性类型痴呆,这两种疾病常会共存。有强力证据;表明两者可为连续疾病谱系,提示血管性危险因素与AD存在关联。AD为慢性进行性神经变性病,临床表现为进行性记忆下降,其不断进展。

Sorl1 knockout inhibits expression of brain-derived neurotrophic factor:involvement in the development of late-onset Alzheimer's disease

Sortilin-related receptor 1(SORL1)is a critical gene associated with late-onset Alzheimer’s disease.SORL1 contributes to the development and progression of this neurodegenerative condition by affecting the transport and metabolism of intracellularβ-amyloid precursor protein.To better understand the underlying mechanisms of SORL1 in the pathogenesis of late-onset Alzheimer s disease,in this study,we established a mouse model of SorI1 gene knockout using cluste red regularly inters paced short palindro mic repeats-associated protein 9 technology.We found that Sorl1-knocko ut mice displayed deficits in learning and memory.Furthermore,the expression of brain-derived neurotrophic factor was significantly downregulated in the hippocampus and co rtex,and amyloidβ-protein deposits were observed in the brains of 5orl1-knockout mice.In vitro,hippocampal neuronal cell synapses from homozygous Sorl1-knockout mice were impaired.The expression of synaptic proteins,including Drebrin and NR2B,was significantly reduced,and also their colocalization.Additionally,by knocking out the Sorl1 gene in N2a cells,we found that expression of the N-methyl-D-aspartate receptor,NR2B,and cyclic adenosine monophosphate-response element binding protein was also inhibited.These findings suggest that SORL1 participates in the pathogenesis of late-onset Alzheimer s disease by regulating the N-methyl-D-aspartate receptor NR2B/cyclic adenosine monophosphate-response element binding protein signaling axis.

Genetic and epigenetic targets of natural dietary compounds as anti-Alzheimer's agents

Alzheimer’s disease is a progressive neurodegenerative disorder and the most common cause of dementia that principally affects older adults.Pathogenic factors,such as oxidative stress,an increase in acetylcholinesterase activity,mitochondrial dysfunction,genotoxicity,and neuroinflammation are present in this syndrome,which leads to neurodegeneration.Neurodegenerative pathologies such as Alzheimer’s disease are considered late-onset diseases caused by the complex combination of genetic,epigenetic,and environmental factors.There are two main types of Alzheimer’s disease,known as familial Alzheimer’s disease(onset<65 years)and late-onset or sporadic Alzheimer’s disease(onset≥65 years).Patients with familial Alzheimer’s disease inherit the disease due to rare mutations on the amyloid precursor protein(APP),presenilin 1 and 2(PSEN1 and PSEN2)genes in an autosomaldominantly fashion with closely 100%penetrance.In contrast,a different picture seems to emerge for sporadic Alzheimer’s disease,which exhibits numerous non-Mendelian anomalies suggesting an epigenetic component in its etiology.Importantly,the fundamental pathophysiological mechanisms driving Alzheimer’s disease are interfaced with epigenetic dysregulation.However,the dynamic nature of epigenetics seems to open up new avenues and hope in regenerative neurogenesis to improve brain repair in Alzheimer’s disease or following injury or stroke in humans.In recent years,there has been an increase in interest in using natural products for the treatment of neurodegenerative illnesses such as Alzheimer’s disease.Through epigenetic mechanisms,such as DNA methylation,non-coding RNAs,histone modification,and chromatin conformation regulation,natural compounds appear to exert neuroprotective effects.While we do not purport to cover every in this work,we do attempt to illustrate how various phytochemical compounds regulate the epigenetic effects of a few Alzheimer’s disease-related genes.

Circadian rhythm disruption and retinal dysfunction:a bidirectional link in Alzheimer’s disease?

Dysfunction in circadian rhythms is a common occurrence in patients with Alzheimer’s disease.A predominant function of the retina is circadian synchronization,carrying information to the brain through the retinohypothalamic tract,which projects to the suprachiasmatic nucleus.Notably,Alzheimer’s disease hallmarks,including amyloid-β,are present in the retinas of Alzheimer’s disease patients,followed/associated by structural and functional disturbances.However,the mechanistic link between circadian dysfunction and the pathological changes affecting the retina in Alzheimer’s disease is not fully understood,although some studies point to the possibility that retinal dysfunction could be considered an early pathological process that directly modulates the circadian rhythm.

Activation of autophagy by Citri Reticulatae Semen extract ameliorates amyloid-beta-induced cell death and cognition deficits in Alzheimer’s disease

Amyloid-beta-induced neuronal cell death contributes to cognitive decline in Alzheimer’s disease.Citri Reticulatae Semen has diverse beneficial effects on neurodegenerative diseases,including Parkinson’s and Huntington’s diseases,however,the effect of Citri Reticulatae Semen on Alzheimer’s disease remains unelucidated.In the current study,the anti-apoptotic and autophagic roles of Citri Reticulatae Semen extract on amyloid-beta-induced apoptosis in PC12 cells were first investigated.Citri Reticulatae Semen extract protected PC12 cells from amyloid-beta-induced apoptosis by attenuating the Bax/Bcl-2 ratio via activation of autophagy.In addition,Citri Reticulatae Semen extract was confirmed to bind amyloid-beta as revealed by biolayer interferometry in vitro,and suppress amyloid-beta-induced pathology such as paralysis,in a transgenic Caenorhabditis elegans in vivo model.Moreover,genetically defective Caenorhabditis elegans further confirmed that the neuroprotective effect of Citri Reticulatae Semen extract was autophagy-dependent.Most importantly,Citri Reticulatae Semen extract was confirmed to improve cognitive impairment,neuronal injury and amyloid-beta burden in 3×Tg Alzheimer’s disease mice.As revealed by both in vitro and in vivo models,these results suggest that Citri Reticulatae Semen extract is a potential natural therapeutic agent for Alzheimer’s disease via its neuroprotective autophagic effects.

Nanomaterials-mediated lysosomal regulation:a robust protein-clearance approach for the treatment of Alzheimer’s disease

Alzheimer’s disease is a debilitating,progressive neurodegenerative disorder characterized by the progressive accumulation of abnormal proteins,including amyloid plaques and intracellular tau tangles,primarily within the brain.Lysosomes,crucial intracellular organelles responsible for protein degradation,play a key role in maintaining cellular homeostasis.Some studies have suggested a link between the dysregulation of the lysosomal system and pathogenesis of neurodegenerative diseases,including Alzheimer’s disease.Restoring the normal physiological function of lysosomes hold the potential to reduce the pathological burden and improve the symptoms of Alzheimer’s disease.Currently,the efficacy of drugs in treating Alzheimer’s disease is limited,with major challenges in drug delivery efficiency and targeting.Recently,nanomaterials have gained widespread use in Alzheimer’s disease drug research owing to their favorable physical and chemical properties.This review aims to provide a comprehensive overview of recent advances in using nanomaterials(polymeric nanomaterials,nanoemulsions,and carbon-based nanomaterials)to enhance lysosomal function in treating Alzheimer’s disease.This review also explores new concepts and potential therapeutic strategies for Alzheimer’s disease through the integration of nanomaterials and modulation of lysosomal function.In conclusion,this review emphasizes the potential of nanomaterials in modulating lysosomal function to improve the pathological features of Alzheimer’s disease.The application of nanotechnology to the development of Alzheimer’s disease drugs brings new ideas and approaches for future treatment of this disease.

Diet and physical activity influence the composition of gut microbiota,benefit on Alzheimer's disease

Alzheimer's disease is a neurodegenerative disease with complex etiology.Gut microbiota influences the gutbrain axis,which may affect pathways related to the pathogenesis of Alzheimer's disease.Additionally,diet and physical activity are likely to affect the pathology of Alzheimer's disease as well as the gut microbiota.This demonstrates that it may be possible to prevent or halt the progression of Alzheimer's disease by regulating the gut microbiota using diet and physical activity strategies.Therefore,the present study reviews the association between these two interventions and gut microbiota in the human body.It also summarizes how these two interventions benefit Alzheimer's disease.Furthermore,the primary limitations of these two interventions are discussed and promising strategies are proposed,which may be beneficial to further study and develop the intervening measure for the progression of Alzheimer's disease.

Neural stem cells promote neuroplasticity: a promising therapeutic strategy for the treatment of Alzheimer’s disease

Recent studies have demonstrated that neuroplasticity,such as synaptic plasticity and neurogenesis,exists throughout the normal lifespan but declines with age and is significantly impaired in individuals with Alzheimer’s disease.Hence,promoting neuroplasticity may represent an effective strategy with which Alzheimer’s disease can be alleviated.Due to their significant ability to self-renew,differentiate,and migrate,neural stem cells play an essential role in reversing synaptic and neuronal damage,reducing the pathology of Alzheimer’s disease,including amyloid-β,tau protein,and neuroinflammation,and secreting neurotrophic factors and growth factors that are related to plasticity.These events can promote synaptic plasticity and neurogenesis to repair the microenvironment of the mammalian brain.Consequently,neural stem cells are considered to represent a potential regenerative therapy with which to improve Alzheimer’s disease and other neurodegenerative diseases.In this review,we discuss how neural stem cells regulate neuroplasticity and optimize their effects to enhance their potential for treating Alzheimer’s disease in the clinic.

Environmental enrichment in combination with Bifidobacterium breve HNXY26M4 intervention amplifies neuroprotective benefits in a mouse model of Alzheimer's disease by modulating glutamine metabolism of the gut microbiome

The gut microbiota-brain axis has emerged as a novel target for Alzheimer's disease(AD),a neurodegenerative disease characterised by behavioural and cognitive impairment.However,most previous microbiome-based intervention studies have focused on single factors and yielded only modest cognitive improvements.Here,we proposed a multidomain intervention strategy that combined Bifidobacterium breve treatment with environmental enrichment(EE)training.In this study,we found that compared with EE or B.breve treatment alone,B.breve intervention combined with EE amplified its neuroprotective effects on AD mice,as reflected by improved cognition,inhibited neuroinflammation and enhanced synaptic function.Moreover,using microbiome and metabolome profiling,we found that the combination of B.breve and EE treatment restored AD-related gut microbiota dysbiosis and reversed microbial metabolite changes.Finally,by integrating behavioural and neurological data with metabolomic profiles,we revealed that the underlying mechanism may involve the modulation of microbiota-derived glutamine metabolism via gut-brain interactions.Collectively,combined B.breve intervention with EE treatment can alleviate AD-related cognitive impairment and improve brain function by regulating glutamine metabolism of the gut microbiome.Our findings provide a promising multidomain intervention strategy,with a combination of dietary microbiome-based and lifestyle-targeted interventions,to promote brain function and delay the progression of AD.