Reduced mesencephalic astrocyte-derived neurotrophic factor expression by mutant androgen receptor contributes to neurodegeneration in a model of spinal and bulbar muscular atrophy pathology

Spinal and bulbar muscular atrophy is a neurodegenerative disease caused by extended CAG trinucleotide repeats in the androgen receptor gene,which encodes a ligand-dependent transcription facto r.The mutant androgen receptor protein,characterized by polyglutamine expansion,is prone to misfolding and forms aggregates in both the nucleus and cytoplasm in the brain in spinal and bulbar muscular atrophy patients.These aggregates alter protein-protein interactions and compromise transcriptional activity.In this study,we reported that in both cultured N2a cells and mouse brain,mutant androgen receptor with polyglutamine expansion causes reduced expression of mesencephalic astrocyte-de rived neurotrophic factor.Overexpressio n of mesencephalic astrocyte-derived neurotrophic factor amelio rated the neurotoxicity of mutant androgen receptor through the inhibition of mutant androgen receptor aggregation.Conversely.knocking down endogenous mesencephalic astrocyte-derived neurotrophic factor in the mouse brain exacerbated neuronal damage and mutant androgen receptor aggregation.Our findings suggest that inhibition of mesencephalic astrocyte-derived neurotrophic factor expression by mutant androgen receptor is a potential mechanism underlying neurodegeneration in spinal and bulbar muscular atrophy.

Functions of nuclear factor Y in nervous system development,function and health

Nuclear factor Y is a ubiquitous heterotrimeric transcription factor complex conserved across eukaryotes that binds to CCAAT boxes,one of the most common motifs found in gene promoters and enhancers.Over the last 30 years,research has revealed that the nuclear factor Y complex controls many aspects of brain development,including differentiation,axon guidance,homeostasis,disease,and most recently regeneration.However,a complete understanding of transcriptional regulatory networks,including how the nuclear factor Y complex binds to specific CCAAT boxes to perform its function remains elusive.In this review,we explore the nuclear factor Y complex’s role and mode of action during brain development,as well as how genomic technologies may expand understanding of this key regulator of gene expression.

The effects of exercise interventions on brain-derived neurotrophic factor levels in children and adolescents:a meta-analysis

Brain-derived neurotrophic factor is a crucial neurotrophic factor that plays a significant role in brain health. Although the vast majority of meta-analyses have confirmed that exercise interventions can increase brain-derived neurotrophic factor levels in children and adolescents, the effects of specific types of exercise on brain-derived neurotrophic factor levels are still controversial. To address this issue, we used meta-analytic methods to quantitatively evaluate, analyze, and integrate relevant studies. Our goals were to formulate general conclusions regarding the use of exercise interventions, explore the physiological mechanisms by which exercise improves brain health and cognitive ability in children and adolescents, and provide a reliable foundation for follow-up research. We used the Pub Med, Web of Science, Science Direct, Springer, Wiley Online Library, Weipu, Wanfang, and China National Knowledge Infrastructure databases to search for randomized controlled trials examining the influences of exercise interventions on brain-derived neurotrophic factor levels in children and adolescents. The extracted data were analyzed using Review Manager 5.3. According to the inclusion criteria, we assessed randomized controlled trials in which the samples were mainly children and adolescents, and the outcome indicators were measured before and after the intervention. We excluded animal experiments, studies that lacked a control group, and those that did not report quantitative results. The mean difference(MD;before versus after intervention) was used to evaluate the effect of exercise on brain-derived neurotrophic factor levels in children and adolescents. Overall, 531 participants(60 children and 471 adolescents, 10.9–16.1 years) were included from 13 randomized controlled trials. Heterogeneity was evaluated using the Q statistic and I^(2) test provided by Review Manager software. The meta-analysis showed that there was no heterogeneity among the studies(P = 0.67, I^(2) = 0.00%). The combined effect of the interventions was significant(MD = 2.88, 95% CI: 1.53–4.22, P < 0.0001), indicating that the brain-derived neurotrophic factor levels of the children and adolescents in the exercise group were significantly higher than those in the control group. In conclusion, different types of exercise interventions significantly increased brain-derived neurotrophic factor levels in children and adolescents. However, because of the small sample size of this meta-analysis, more high-quality research is needed to verify our conclusions. This metaanalysis was registered at PROSPERO(registration ID: CRD42023439408).

Telencephalic stab wound injury induces regenerative angiogenesis and neurogenesis in zebrafish:unveiling the role of vascular endothelial growth factor signaling and microglia

After brain damage,regenerative angiogenesis and neurogenesis have been shown to occur simultaneously in mammals,suggesting a close link between these processes.However,the mechanisms by which these processes interact are not well understood.In this work,we aimed to study the correlation between angiogenesis and neurogenesis after a telencephalic stab wound injury.To this end,we used zebrafish as a relevant model of neuroplasticity and brain repair mechanisms.First,using the Tg(fli1:EGFP×mpeg1.1:mCherry)zebrafish line,which enables visualization of blood vessels and microglia respectively,we analyzed regenerative angiogenesis from 1 to 21 days post-lesion.In parallel,we monitored brain cell proliferation in neurogenic niches localized in the ventricular zone by using immunohistochemistry.We found that after brain damage,the blood vessel area and width as well as expression of the fli1 transgene and vascular endothelial growth factor(vegfaa and vegfbb)were increased.At the same time,neural stem cell proliferation was also increased,peaking between 3 and 5 days post-lesion in a manner similar to angiogenesis,along with the recruitment of microglia.Then,through pharmacological manipulation by injecting an anti-angiogenic drug(Tivozanib)or Vegf at the lesion site,we demonstrated that blocking or activating Vegf signaling modulated both angiogenic and neurogenic processes,as well as microglial recruitment.Finally,we showed that inhibition of microglia by clodronate-containing liposome injection or dexamethasone treatment impairs regenerative neurogenesis,as previously described,as well as injury-induced angiogenesis.In conclusion,we have described regenerative angiogenesis in zebrafish for the first time and have highlighted the role of inflammation in this process.In addition,we have shown that both angiogenesis and neurogenesis are involved in brain repair and that microglia and inflammation-dependent mechanisms activated by Vegf signaling are important contributors to these processes.This study paves the way for a better understanding of the effect of Vegf on microglia and for studies aimed at promoting angiogenesis to improve brain plasticity after brain injury.

Age-related driving mechanisms of retinal diseases and neuroprotection by transcription factor EB-targeted therapy

Retinal aging has been recognized as a significant risk factor for various retinal disorders,including diabetic retinopathy,age-related macular degeneration,and glaucoma,following a growing understanding of the molecular underpinnings of their development.This comprehensive review explores the mechanisms of retinal aging and investigates potential neuroprotective approaches,focusing on the activation of transcription factor EB.Recent meta-analyses have demonstrated promising outcomes of transcription factor EB-targeted strategies,such as exercise,calorie restriction,rapamycin,and metformin,in patients and animal models of these common retinal diseases.The review critically assesses the role of transcription factor EB in retinal biology during aging,its neuroprotective effects,and its therapeutic potential for retinal disorders.The impact of transcription factor EB on retinal aging is cell-specific,influencing metabolic reprogramming and energy homeostasis in retinal neurons through the regulation of mitochondrial quality control and nutrient-sensing pathways.In vascular endothelial cells,transcription factor EB controls important processes,including endothelial cell proliferation,endothelial tube formation,and nitric oxide levels,thereby influencing the inner blood-retinal barrier,angiogenesis,and retinal microvasculature.Additionally,transcription factor EB affects vascular smooth muscle cells,inhibiting vascular calcification and atherogenesis.In retinal pigment epithelial cells,transcription factor EB modulates functions such as autophagy,lysosomal dynamics,and clearance of the aging pigment lipofuscin,thereby promoting photoreceptor survival and regulating vascular endothelial growth factor A expression involved in neovascularization.These cell-specific functions of transcription factor EB significantly impact retinal aging mechanisms encompassing proteostasis,neuronal synapse plasticity,energy metabolism,microvasculature,and inflammation,ultimately offering protection against retinal aging and diseases.The review emphasizes transcription factor EB as a potential therapeutic target for retinal diseases.Therefore,it is imperative to obtain well-controlled direct experimental evidence to confirm the efficacy of transcription factor EB modulation in retinal diseases while minimizing its risk of adverse effects.

Brain-derived neurotrophic factor signaling in the neuromuscular junction during developmental axonal competition and synapse elimination

During the development of the nervous system,there is an overproduction of neurons and synapses.Hebbian competition between neighboring nerve endings and synapses performing different activity levels leads to their elimination or strengthening.We have extensively studied the involvement of the brain-derived neurotrophic factor-Tropomyosin-related kinase B receptor neurotrophic retrograde pathway,at the neuromuscular junction,in the axonal development and synapse elimination process versus the synapse consolidation.The purpose of this review is to describe the neurotrophic influence on developmental synapse elimination,in relation to other molecular pathways that we and others have found to regulate this process.In particular,we summarize our published results based on transmitter release analysis and axonal counts to show the different involvement of the presynaptic acetylcholine muscarinic autoreceptors,coupled to downstream serine-threonine protein kinases A and C(PKA and PKC)and voltage-gated calcium channels,at different nerve endings in developmental competition.The dynamic changes that occur simultaneously in several nerve terminals and synapses converge across a postsynaptic site,influence each other,and require careful studies to individualize the mechanisms of specific endings.We describe an activity-dependent balance(related to the extent of transmitter release)between the presynaptic muscarinic subtypes and the neurotrophin-mediated TrkB/p75NTR pathways that can influence the timing and fate of the competitive interactions between the different axon terminals.The downstream displacement of the PKA/PKC activity ratio to lower values,both in competing nerve terminals and at postsynaptic sites,plays a relevant role in controlling the elimination of supernumerary synapses.Finally,calcium entry through L-and P/Q-subtypes of voltage-gated calcium channels(both channels are present,together with the N-type channel in developing nerve terminals)contributes to reduce transmitter release and promote withdrawal of the most unfavorable nerve terminals during elimination(the weakest in acetylcholine release and those that have already become silent).The main findings contribute to a better understanding of punishment-rewarding interactions between nerve endings during development.Identifying the molecular targets and signaling pathways that allow synapse consolidation or withdrawal of synapses in different situations is important for potential therapies in neurodegenerative diseases.

The cGAS-STING-interferon regulatory factor 7 pathway regulates neuroinflammation in Parkinson's disease

Interferon regulatory factor 7 plays a crucial role in the innate immune response.However,whether interferon regulatory factor 7-mediated signaling contributes to Parkinson's disease remains unknown.Here we report that interferon regulatory factor 7 is markedly up-regulated in a 1-methyl-4-phenyl-1,2,3,6-tetrahydropyridine-induced mouse model of Parkinson's disease and co-localizes with microglial cells.Both the selective cyclic guanosine monophosphate adenosine monophosphate synthase inhibitor RU.521 and the stimulator of interferon genes inhibitor H151 effectively suppressed interferon regulatory factor 7 activation in BV2 microglia exposed to 1-methyl-4-phenylpyridinium and inhibited transformation of mouse BV2 microglia into the neurotoxic M1 phenotype.In addition,si RNA-mediated knockdown of interferon regulatory factor 7 expression in BV2 microglia reduced the expression of inducible nitric oxide synthase,tumor necrosis factorα,CD16,CD32,and CD86 and increased the expression of the anti-inflammatory markers ARG1 and YM1.Taken together,our findings indicate that the cyclic guanosine monophosphate adenosine monophosphate synthase-stimulator of interferon genes-interferon regulatory factor 7 pathway plays a crucial role in the pathogenesis of Parkinson's disease.

联合凉膈散治疗脓毒症ARDS的疗效及其对血清CC-16、Ang-2、vWF的影响

目的研究联合凉膈散治疗脓毒症急性呼吸窘迫综合征(ARDS)的疗效及其对血清Clara细胞分泌蛋白-16(CC-16)、血管生成-2(Ang-2)、血管性血友病因子(vWF)的影响。方法前瞻性选择2021年7月至2023年6月在河北省沧州中西医结合医院治疗的脓毒症ARDS患者98例,按照随机数字表法将其分为试验组与对照组,每组各49例。对照组行常规对症治疗,试验组行常规对症治疗+凉膈散治疗。比较两组治疗7 d后临床疗效;两组治疗7 d后机械通气时间、入住ICU时间;治疗前及治疗7 d后病情严重程度[急性生理学与慢性健康状况评分Ⅱ(APACHEⅡ)]、血气分析指标[动脉血氧分压(PaO_(2))、氧合指数(PaO_(2)/FiO_(2))及动脉血氧饱和度(SaO_(2))]、血清CC-16、Ang-2、vWF水平。结果试验组总有效率为91.84%,高于对照组(73.47%),差异有统计学意义(P<0.05)。试验组机械通气时间、入住ICU时间分别为(5.62±0.58)、(8.76±0.90)d,均小于对照组[(8.94±0.92)、(13.87±1.53)d],差异均有统计学意义(P<0.05)。治疗7 d后,试验组APACHEⅡ评分为(9.79±1.04)分,低于对照组[(13.59±1.57)分],PaO_(2)、PaO_(2)/FiO_(2)、SaO_(2)分别为(94.29±9.65)mmHg、(326.08±35.86)mmHg、1.03±0.12,均高于对照组[(80.38±8.42)mmHg、(268.69±28.75)mmHg、0.88±0.09],差异均有统计学意义(P<0.05)。治疗7 d后,试验组血清CC-16、Ang-2、vWF水平分别为(42.73±4.45)ng/L、2083(1879,2205)pg/mL、(4.95±0.52)μg/mL,均低于对照组[(49.35±5.14)ng/L、2749(2562,3075)pg/mL、(5.53±0.58)μg/mL],差异均有统计学意义(P<0.05)。结论联合凉膈散治疗脓毒症ARDS可改善患者症状,缩短其恢复时间,改善患者血气分析指标,降低血清CC-16、Ang-2、vWF水平,疗效显著。

VWF、AT-Ⅲ、凝血因子对慢加急性肝衰竭的临床预测价值

目的探讨VWF、AT-Ⅲ、凝血因子对慢加急性肝衰竭(acute-on-chronic liver failure,ACLF)患者的临床预测价值。方法回顾性分析2021年9月至2023年5月昆明医科大学第二附属医院消化内科收治的111例肝硬化患者的临床资料,并计算Child-Pugh评分、MELD评分、MELD-NA评分。分析影响ACLF的相关因素,并评估VWF、AT-Ⅲ、凝血因子对ACLF的预测价值。结果与低MELD组相比,高MELD组IL-6、PCT、CRP、VWF水平升高,差异有统计学意义(P<0.05),而凝血因子Ⅷ水平升高差异无统计学意义(Z=0.169,P=0.866);凝血因子Ⅱ、Ⅴ、Ⅶ、Ⅸ、Ⅹ、Ⅺ、Ⅻ和AT-Ⅲ水平降低,差异有统计学意义(P<0.05)。患者的IL-6、PCT、CRP、VWF、AT-Ⅲ和凝血因子Ⅱ、Ⅴ、Ⅶ、Ⅷ、Ⅸ、Ⅹ、Ⅺ、Ⅻ水平在不同Child-Pugh分级中的差异有统计学意义(P<0.05)。单变量分析中,PCT、CRP、VWF、AT-Ⅲ和凝血因子Ⅱ、Ⅶ、Ⅸ、Ⅹ、Ⅺ、Ⅻ与ACLF发生相关(P<0.05)。多因素分析显示,VWF、AT-Ⅲ为ACLF是否发生的独立危险因素(P均<0.05)。AT-Ⅲ、VWF诊断效能ROC曲线分析,AT-Ⅲ的AUC值为0.873(P<0.001),敏感度为94.1%,特异度为73.1%;VWF的AUC值为0.699(P=0.002),敏感度为65.4%,特异度为79.6%。结论肝硬化患者的IL-6、PCT、CRP、VWF、AT-Ⅲ和凝血因子Ⅱ、Ⅴ、Ⅶ、Ⅷ、Ⅸ、Ⅹ、Ⅺ、Ⅻ水平在不同Child-Pugh分级中存在差异;肝硬化患者MELD评分增大,IL-6、PCT、CRP、VWF水平升高,凝血因子Ⅱ、Ⅴ、Ⅶ、Ⅸ、Ⅹ、Ⅺ、Ⅻ和AT-Ⅲ水平降低;AT-Ⅲ、VWF是ACLF的独立危险因素,可一定程度预测ACLF的发生,为ACLF的诊断提供依据。

重度创伤性颅脑损伤后凝血功能障碍患者血浆α2-抗纤溶酶、vWF及ET-1水平及其影响因素分析

目的探讨重度创伤性颅脑损伤(TBI)后凝血功能障碍患者血浆α2-抗纤溶酶(α2-AP)、血管性血友病因子(vWF)及内皮素-1(ET-1)水平变化及影响因素。方法回顾性分析2021年1月—2022年12月南阳市第一人民医院神经外科和新乡市中心医院神经外科收治的106例重度TBI患者。其中男性58例,女性48岁;年龄32~60岁,平均43.7岁。根据TBI后24 h内是否发生凝血功能障碍分为凝血正常组(74例)和凝血障碍组(32例)。比较两组重度TBI患者临床资料和入院次日清晨的凝血功能指标及血浆α2-AP、vWF、ET-1水平;Pearson相关性分析重度TBI后凝血功能障碍患者血浆α2-AP、vWF、ET-1水平与凝血功能指标的关系;Logistic回归性分析影响重度TBI患者发生凝血功能障碍的危险因素;受试者工作特征(ROC)曲线分析血浆α2-AP、vWF、ET-1水平对重度TBI患者发生凝血功能障碍的预测价值。结果两组患者年龄、入院GCS、入院头部最高AIS和入院时平均MAP比较,差异有统计学意义[(45.4±5.7)岁vs.(42.8±4.2)岁、(6.7±1.1)分vs.(7.2±0.9)分、(4.6±0.8)分vs.(3.7±0.6)分、(84.1±11.2)mmHg vs.(91.0±9.7)mmHg],P<0.05。凝血障碍组TBI患者PT、APTT和INR等凝血功能指标水平和血浆α2-AP、vWF、ET-1水平高于凝血正常组,纤维蛋白原(FIB)水平低于凝血正常组[(27.9±3.4)s vs.(12.0±1.9)s、(66.4±5.8)s vs.(36.2±2.3)s、1.6±0.2 vs.1.0±0.1、(67.8±8.2)mg/L vs.(19.3±2.4)mg/L、(162.5±24.6)%vs.(94.8±10.4)%、(65.1±5.2)mg/L vs.(41.6±3.9)mg/L、(2.6±0.3)g/L vs.(3.9±0.5)g/L,差异有统计学意义(P<0.05)。Pearson相关性分析,重度TBI后凝血功能障碍患者血浆α2-AP、vWF、ET-1与PT呈强正相关(r=0.723、0.528、0.586,P<0.05),与APTT呈强正相关(r=0.646、0.572、0.585,P<0.05),与INR呈强正相关(r=0.592、0.507、0.548,P<0.05),与FIB呈强负相关(r=-0.653、-0.672、-0.526,P<0.05);Logistic回归分析显示,入院时GCS降低(OR=2.593,95%CI:1.018~6.606,P<0.05)、α2-AP水平升高(OR=3.019,95%CI:1.107~8.236,P<0.05)和vWF水平升高(OR=2.729,95%CI:1.028~7.243,P<0.05)为重度TBI患者发生凝血功能障碍的相关危险因素;ROC曲线显示,α2-AP、vWF、ET-1预测重度TBI患者发生凝血功能障碍的AUC分别为0.887(95%CI:0.805~0.969,P<0.05)、0.828(95%CI:0.734~0.922,P<0.05)和0.807(95%CI:0.695~0.918,P<0.05),联合检测的AUC为0.912(95%CI:0.854~0.970,P<0.05),灵敏度为91.67%,特异度为87.14%。结论重度TBI后凝血功能障碍患者血浆α2-AP、vWF和ET-1水平均显著升高,其中血浆α2-AP、vWF水平升高为重度TBI患者发生凝血功能障碍的相关危险因素。

血清vWF、Treg相关细胞因子在急性白血病患儿危险分层及疗效评估中的价值

目的探究血清血管性血友病因子(vWF)、调节性T细胞(Treg)相关细胞因子[转化生长因子-β(TGF-β)、白介素-10(IL-10)、白介素-35(IL-35)]在急性白血病(AL)患儿危险分层及疗效评估中的价值,为AL患儿临床诊疗提供参考。方法选取2020年2月至2022年8月郑州大学第三附属医院收治的78例AL患儿,根据CCLG-ALL-2018方案危险分层分为低危组(39例)、中危组(21例)、高危组(18例)3个亚组,分别比较不同类型、不同危险分层患儿血清vWF、TGF-β、IL-10、IL-35水平,并进行相关性分析。AL患儿均接受规范化治疗,根据治疗1 a疗效评估结果分为临床有效组(完全缓解+部分缓解,62例)、临床无效组(未缓解,16例),分别比较两组治疗2、6个月血清vWF、TGF-β、IL-10、IL-35水平,分析其对AL患儿疗效的预测价值。结果低危组血清vWF、IL-10、IL-35水平低于中危组,中危组血清vWF、IL-10、IL-35水平低于高危组(P<0.05);低危组血清TGF-β水平高于中危组,中危组血清TGF-β水平高于高危组(P<0.05);Spearman相关系数法分析显示,血清vWF、IL-10、IL-35与AL患儿危险分层呈正相关,血清TGF-β与AL患儿危险分层呈负相关(P<0.05);78例AL患儿经1 a治疗后有28例完全缓解、34例部分缓解,计入临床有效组(62例),16例未缓解,计入临床无效组(16例)。治疗2、6个月临床有效组血清vWF、IL-10、IL-35水平均低于临床无效组,血清TGF-β水平高于临床无效组,差异有统计学意义(P<0.05);治疗2、6个月各血清指标联合预测AL患儿临床无效的曲线下面积分别为0.875、0.933(P<0.05)。结论血清vWF、TGF-β、IL-10、IL-35与AL患儿危险分层及疗效有关,动态监测血清vWF、Treg相关细胞因子有利于病情及疗效评估。

Significant risk factors for intensive care unit-acquired weakness:A processing strategy based on repeated machine learning

BACKGROUND Intensive care unit-acquired weakness(ICU-AW)is a common complication that significantly impacts the patient's recovery process,even leading to adverse outcomes.Currently,there is a lack of effective preventive measures.AIM To identify significant risk factors for ICU-AW through iterative machine learning techniques and offer recommendations for its prevention and treatment.METHODS Patients were categorized into ICU-AW and non-ICU-AW groups on the 14th day post-ICU admission.Relevant data from the initial 14 d of ICU stay,such as age,comorbidities,sedative dosage,vasopressor dosage,duration of mechanical ventilation,length of ICU stay,and rehabilitation therapy,were gathered.The relationships between these variables and ICU-AW were examined.Utilizing iterative machine learning techniques,a multilayer perceptron neural network model was developed,and its predictive performance for ICU-AW was assessed using the receiver operating characteristic curve.RESULTS Within the ICU-AW group,age,duration of mechanical ventilation,lorazepam dosage,adrenaline dosage,and length of ICU stay were significantly higher than in the non-ICU-AW group.Additionally,sepsis,multiple organ dysfunction syndrome,hypoalbuminemia,acute heart failure,respiratory failure,acute kidney injury,anemia,stress-related gastrointestinal bleeding,shock,hypertension,coronary artery disease,malignant tumors,and rehabilitation therapy ratios were significantly higher in the ICU-AW group,demonstrating statistical significance.The most influential factors contributing to ICU-AW were identified as the length of ICU stay(100.0%)and the duration of mechanical ventilation(54.9%).The neural network model predicted ICU-AW with an area under the curve of 0.941,sensitivity of 92.2%,and specificity of 82.7%.CONCLUSION The main factors influencing ICU-AW are the length of ICU stay and the duration of mechanical ventilation.A primary preventive strategy,when feasible,involves minimizing both ICU stay and mechanical ventilation duration.

Are TrkB receptor agonists the right tool to fulfill the promises for a therapeutic value of the brain-derived neurotrophic factor?

Brain-derived neurotrophic factor signaling via its receptor tro pomyosin receptor kinase B regulates several crucial physiological processes.It has been shown to act in the brain,promoting neuronal survival,growth,and plasticity as well as in the rest of the body where it is involved in regulating for instance aspects of the metabolism.Due to its crucial and very pleiotro pic activity,reduction of brain-derived neurotrophic factor levels and alterations in the brain-derived neurotrophic factor/tropomyosin receptor kinase B signaling have been found to be associated with a wide spectrum of neurological diseases.Howeve r,because of its poor bioavailability and pharmacological properties,brain-derived neurotrophic factor itself has a very low therapeutic value.Moreover,the concomitant binding of exogenous brain-derived neurotrophic factor to the p75 neurotrophin receptor has the potential to elicit several unwanted and deleterious side effects.Therefo re,developing tools and approaches to specifically promote tropomyosin receptor kinase B signaling has become an important goal of translational research.Among the newly developed tools are different categories of tropomyosin receptor kinase B receptor agonist molecules.In this review,we give a comprehensive description of the diffe rent tro pomyosin receptor kinase B receptor agonist drugs developed so far and of the res ults of their application in animal models of several neurological diseases.Moreover,we discuss the main benefits of tropomyosin receptor kinase B receptor agonists,concentrating especially on the new tropomyosin receptor kinase B agonist antibodies.The benefits observed both in vitro and in vivo upon application of tropomyosin receptor kinase B receptor agonist drugs seem to predominantly depend on their general neuroprotective activity and their ability to promote neuronal plasticity.Moreover,tro pomyosin receptor kinase B agonist antibodies have been shown to specifically bind the tropomyosin receptor kinase B receptor and not p75 neurotrophin receptor.Therefore,while,based on the current knowledge,the tropomyosin receptor kinase B receptor agonists do not seem to have the potential to reve rse the disease pathology per se,promoting brainderived neurotrophic factor/tro pomyosin receptor kinase B signaling still has a very high therapeutic relevance.

舒肝化癥方对肝纤维化模型大鼠VEGF、CTGF、CD31及vWF表达的影响及其相关性研究

目的:以四氯化碳(CCl_(4))致大鼠肝纤维化为研究对象,研究舒肝化癥方(SGHZD)对大鼠肝纤维化血瘀证的影响及机理,分析血管内皮生长因子(VEGF)、结缔组织生长因子(CTGF)、血小板-内皮细胞黏附分子(CD31)及血管性血友病因子(vWF)在SGHZD抗肝纤维化过程中的表达及其相关性。方法:SPF级SD大鼠,雄性,54只,按随机原则分成空白组、模型组(2.0 mg/kg 40%CCl_(4)橄榄油溶液+等量的0.9%的生理盐水)、阳性对照组(2.0 mg/kg 40%CCl_(4)橄榄油溶液+0.2 mg/kg秋水仙碱溶液)、SGHZD高剂量组(2.0 mg/kg 40%CCl_(4)橄榄油溶液+29.52g/kgSGHZD)、SGHZD中剂量组(2.0 mg/kg 40%CCl_(4)橄榄油溶液+14.76 g/kgSGHZD)和SGHZD低剂量组(2.0 mg/kg 40%CCl_(4)橄榄油溶液+7.38 g/kgSGHZD),各9只。造模时间为8周,每周2次,从造模第2天起,用药治疗每天1次,治疗8周,实验期间动态监测所有大鼠的生理情况,马松染色(Masson)对肝组织病理形态学变化和胶原纤维沉积情况进行观察,实时荧光定量聚合酶链式反应(Real-time PCR)检测VEGF、CTGF、CD31、vWF mRNA的表达水平,Western blot检测VEGF,CTGF,CD31,vWF的蛋白表达。结果:与空白组相比,模型组大鼠整体状况明显下降,Masson染色结果显示大鼠汇管区和中央静脉区形成假小叶,并伴有纤维间隔形成,胶原纤维沉积增多且有显著意义(P<0.05);RT-qPCR、Western blot结果显示,VEGF、CTGF、CD31、vWF mRNA和蛋白表达均上升(P<0.05);与模型组相比,阳性对照组和SGHZD组各剂量Masson染色显示胶原纤维沉积明显减少,纤维间隔程度减轻,差异有统计学意义(P<0.05),RT-qPCR、Western blot结果显示VEGF、CTGF、CD31、vWF mRNA及蛋白的表达量均下降,但以阳性对照组及中药高剂量组效果最好(P均<0.05);将Masson染色胶原容积分数分别与VEGF、CTGF、CD31及vWF蛋白表达进行相关性分析,发现VEGF、CTGF、CD31及vWF在肝纤维化的形成过程中随着肝纤维化程度加重其表达上调,而在SGHZD抗肝纤维化过程中随着胶原容积分数减少其表达减少;对VEGF、CTGF、CD31及vWF蛋白表达进行相关性分析,发现VEGF、CTGF、CD31及vWF在肝纤维化的形成发展中和SGHZD抗肝纤维化的过程中均呈显著正相关。结论:SGHZD对CCl_(4)所致肝纤维化大鼠有显著疗效,其作用机理可能与VEGF、CTGF、CD31及vWF的表达、病理性血管生成、肝窦毛细血管化及肝纤维化血瘀证相关。

Hepatocyte growth factor promotes retinal pigment epithelium cell activity through MET/AKT signaling pathway

AIM:To explore the effects of hepatocyte growth factor(HGF)on retinal pigment epithelium(RPE)cell behaviors.METHODS:The human adult retinal pigment epithelial cell line-19(ARPE-19)were treated by HGF or mesenchymalepithelial transition factor(MET)inhibitor SU11274 in vitro.Cell viability was detected by a Cell Counting Kit-8 assay.Cell proliferation and motility was detected by a bromodeoxyuridine incorporation assay and a wound healing assay,respectively.The expression levels of MET,phosphorylated MET,protein kinase B(AKT),and phosphorylated AKT proteins were determined by Western blot assay.The MET and phosphorylated MET proteins were also determined by immunofluorescence assay.RESULTS:HGF increased ARPE-19 cells’viability,proliferation and migration,and induced an increase of phosphorylated MET and phosphorylated AKT proteins.SU11274 significantly reduced cell viability,proliferation,and migration and decreased the expression of MET and AKT proteins.SU11274 suppressed HGF-induced increase of viability,proliferation,and migration in ARPE-19 cells.Additionally,SU11274 also blocked HGF-induced phosphorylation of MET and AKT proteins.CONCLUSION:HGF enhances cellular viability,proliferation,and migration in RPE cells through the MET/AKT signaling pathway,whereas this enhancement is suppressed by the MET inhibitor SU11274.HGF-induced MET/AKT signaling might be a vital contributor of RPE cells survival.

The roles of macrophage migration inhibitory factor in retinal diseases

Macrophage migration inhibitory factor(MIF),a multifunctional cytokine,is secreted by various cells and participates in inflammatory reactions,including innate and adaptive immunity.There are some evidences that MIF is involved in many vitreoretinal diseases.For example,MIF can exacerbate many types of uveitis;measurements of MIF levels can be used to monitor the effectiveness of uveitis treatment.MIF also alleviates trauma-induced and glaucoma-induced optic nerve damage.Furthermore,MIF is critical for retinal/choroidal neovascularization,especially complex neovascularization.MIF exacerbates retinal degeneration;thus,anti-MIF therapy may help to mitigate retinal degeneration.MIF protects uveal melanoma from attacks by natural killer cells.The mechanism underlying the effects of MIF in these diseases has been demonstrated:it binds to cluster of differentiation 74,inhibits the c-Jun N-terminal kinase pathway,and triggers mitogen-activated protein kinases,extracellular signal-regulated kinase-1/2,and the phosphoinositide-3-kinase/Akt pathway.MIF also upregulates Toll-like receptor 4 and activates the nuclear factor kappa-B signaling pathway.This review focuses on the structure and function of MIF and its receptors,including the effects of MIF on uveal inflammation,retinal degeneration,optic neuropathy,retinal/choroidal neovascularization,and uveal melanoma.

Spatial-temporal differentiation and influencing factors of rural settlements in mountainous areas: an example of Liangshan Yi Autonomous Prefecture, Southwestern China

Rural settlement is the basic spatial unit for compact communities in rural area. Scientific exploration of spatial-temporal differentiation and its influencing factors is the premise of spatial layout rationalization. Based on land use data of Liangshan Yi Autonomous Prefecture(hereinafter referred to as Liangshan Prefecture) in Sichuan Province, China from 1980 to 2020, compactness index, fractal dimension, imbalance index, location entropy and the optimal parameters-based geographical detector(OPGD) model are used to analyze the spatial-temporal evolution of the morphological characteristics of rural settlements, and to explore the influence of natural geographical factors, socioeconomic factors, and policy factors on the spatial differentiation of rural settlements. The results show that:(1) From 1980 to 2020, the rural settlements area in Liangshan Prefecture increased by 15.96 km^(2). In space, the rural settlements are generally distributed in a local aggregation, dense in the middle and sparse around the periphery. In 2015, the spatial density and expansion index of rural settlements reached the peak.(2) From 1980 to 2020, the compactness index decreased from 0.7636 to 0.7496, the fractal dimension increased from 1.0283 to 1.0314, and the fragmentation index decreased from 0.1183 to 0.1047. The spatial morphological structure of rural settlements tended to be loose, the shape contour tended to be complex, the degree of fragmentation decreased, and the spatial distribution was significantly imbalanced.(3) The results of OPGD detection in 2015 show that the influence of each factor is slope(0.2371) > traffic accessibility(0.2098) > population(0.1403) > regional GDP(0.1325) > elevation(0.0987) > poverty alleviation(0). The results of OPGD detection in 2020 show that the influence of each factor is slope(0.2339) > traffic accessibility(0.2198) > population(0.1432) > regional GDP(0.1219) > poverty alleviation(0.0992) > elevation(0.093). Natural geographical factors(slope and elevation) are the basic factors affecting the spatial distribution of rural settlements, and rural settlements are widely distributed in the river valley plain and the second half mountain area. Socioeconomic factors(traffic accessibility, population, and regional GDP) have a greater impact on the spatial distribution of rural settlements, which is an important factor affecting the spatial distribution of rural settlements. Policy factors such as poverty alleviation relocation have an indispensable impact on the spatial distribution of rural settlements. The research results can provide decisionmaking basis for the spatial arrangement of rural settlements in Liangshan Prefecture, and optimize the implementation of rural revitalization policies.

Predictors of Bleeding from Esophageal Varices: The Role of Factor VII and von Willebrand Factor (vWF)

Objectives: Bleeding from gastroesophageal varices is the most serious and life-threatening complication of cirrhosis and accounts for 10% of all cases of bleeding from the upper GI tract. It is essential to identify and treat those patients at the highest risk because each episode of variceal hemorrhage carries a 20 percent to 30 percent risk of death, and up to 70 percent of patients who do not receive treatment die within one year of the initial bleeding episode. The aim of this study is to determine the clinical predictors of bleeding esophageal varices and study the role of F VII (factor VII) and vWF (von willebrand factor) in predicting bleeding in patients with eosphogeal varices. Methods: A case control study was done on all patients with esophageal varices admitted at Sohag and Qena faculty of medicine hospitals from January 2012 to August 2013. Various clinical, laboratory and endoscopic variables were tested to determine the predictors of esophageal bleeding. Results: Among 300 patients with esophageal varices, 80 percent was due to hepatitis C virus (HCV), 18 percent was due to hepatitis B virus (HBV), and 2 percent had both HCV and HBV. As an etiologic factor for their liver disease, hemoglobin was 10.12 ± 2.26 g/l, platelet count 135.55 ± 65.94 × l09/l, prothrombin time 14.1 ± 0.92 second, albumin 2.88 ± 0.71 g/dl, ALT 48.25 ± 24.15 u/l, total bilirubin 1.92 ± 1.36 mg/dl. Factor VII was 27.4 ± 8.92 percent and vWF was 188.33 ± 13.66 IU/dl. Splenomegaly was reported 79.6 percent, 90.3 percent had ascites. 35 percent had grade III esophageal varices, 29 percent had four-column esophageal varices on endoscopy, 13.7 percent had concomitant gastric varices and 38.3 percent had portal hypertensive gastropathy. Platelet count, presence of red color sign, the number of columns of esophageal varices, presence of portal gastropathy on eosphagogastroduodenoscopy (EGD) showed a significant positive correlation with bleeding. There is a significant decrease of FVII and a significant increase of vWF in bleeding group in comparison with non bleeding group. Conclusion: Thrombocytopenia, presence of encephalopathy and endoscopic findings of large varices, presence of red color sign, and portal hypertensive gastropathy were found to be predictors of esophageal variceal bleeding. Increase of vWF and decrease of FVII are laboratory predictors of esophageal variceal bleeding.

Biological factors driving colorectal cancer metastasis

Approximately 20%of colorectal cancer(CRC)patients present with metastasis at diagnosis.Among Stage I-III CRC patients who undergo surgical resection,18%typically suffer from distal metastasis within the first three years following initial treatment.The median survival duration after the diagnosis of metastatic CRC(mCRC)is only 9 mo.mCRC is traditionally considered to be an advanced stage malignancy or is thought to be caused by incomplete resection of tumor tissue,allowing cancer cells to spread from primary to distant organs;however,increa-sing evidence suggests that the mCRC process can begin early in tumor development.CRC patients present with high heterogeneity and diverse cancer phenotypes that are classified on the basis of molecular and morphological alterations.Different genomic and nongenomic events can induce subclone diversity,which leads to cancer and metastasis.Throughout the course of mCRC,metastatic cascades are associated with invasive cancer cell migration through the circulatory system,extravasation,distal seeding,dormancy,and reactivation,with each step requiring specific molecular functions.However,cancer cells presenting neoantigens can be recognized and eliminated by the immune system.In this review,we explain the biological factors that drive CRC metastasis,namely,genomic instability,epigenetic instability,the metastatic cascade,the cancer-immunity cycle,and external lifestyle factors.Despite remarkable progress in CRC research,the role of molecular classification in therapeutic intervention remains unclear.This review shows the driving factors of mCRC which may help in identifying potential candidate biomarkers that can improve the diagnosis and early detection of mCRC cases.

vWF:Ag国产试剂盒的性能验证研究

目的评价国产vWF:Ag(胶乳免疫比浊法)试剂盒在进口血凝检测系统上的检测性能。方法共收集2023年4月至7月北京友谊医院西城院区157例住院患者和40例表观健康人员的枸橼酸钠抗凝血浆样本。vWF:Ag试剂检测质控在靶值宣称的范围内,再进行试剂的性能验证。选取vWF:Ag国产试剂质控品进行精密度评价;选取北京九强公司的工作校准品进行正确度验证;选取高、低值临床样本进行线性范围评价;选取表观健康人群样本进行参考区间验证;选取50例高、中、低值均匀分布临床样本,将国产试剂和进口试剂的结果进行比对,并计算两者相关性和相对偏差;对国产试剂盒对干扰物质(直接胆红素、间接胆红素、血红蛋白、脂肪乳)的抗干扰性能进行验证。结果vWF:Ag国产试剂高、中、低3个质控浓度的批内精密度CV、批间精密度CV和总精密度CV均<10%。正确度两个水平的工作校准品与靶值的偏倚分别为-2.0%和3.3%,均<±10%。线性范围相关系数大于0.995,偏差<±15%,验证的线性范围为10%~253%。O型血人群参考范围为47.8%~138.5%、非O型血人群参考范围为76.5%~163.0%,验证通过。干扰物质胆红素≤40mg/dL,血红蛋白≤150mg/dL,脂肪乳≤600mg/dL,回收率在90%~110%之间,相对偏差<±10%,满足试剂要求。结论在沃芬全自动血凝分析仪ACL TOP500检测系统上,vWF:Ag(胶乳免疫比浊法)国产试剂盒性能良好,符合实验室检测质量要求,满足临床检测需求。