Role of lipids in the control of autophagy and primary cilium signaling in neurons

The brain is,after the adipose tissue,the organ with the greatest amount of lipids and diversity in their composition in the human body.In neurons,lipids are involved in signaling pathways controlling autophagy,a lysosome-dependent catabolic process essential for the maintenance of neuronal homeostasis and the function of the primary cilium,a cellular antenna that acts as a communication hub that transfers extracellular signals into intracellular responses required for neurogenesis and brain development.A crosstalk between primary cilia and autophagy has been established;however,its role in the control of neuronal activity and homeostasis is barely known.In this review,we briefly discuss the current knowledge regarding the role of autophagy and the primary cilium in neurons.Then we review the recent literature about specific lipid subclasses in the regulation of autophagy,in the control of primary cilium structure and its dependent cellular signaling in physiological and pathological conditions,specifically focusing on neurons,an area of research that could have major implications in neurodevelopment,energy homeostasis,and neurodegeneration.

Mechano-Sensing by Endothelial Primary Cilium

Introduction Primary cilium is a non-motile microstructure,protruding from cell surface of most mammalian cells.It was previously thought to be vestigial.However,recent studies indicate that it may serve as one of the most vital mechanosensors for many types of cells such as epithelial and endothelial cells and osteocytes.Protruding from the apical membrane,the primary cilium can directly sense subtle variation of mechanical forces exerted on the cell and then transduce the mechanical cues into biochemical signals into the cell,although the mechanism remain elusive.Vascular endothelial cells(ECs)lining the inner wall of our blood vessels are continuously exposed to the blood flow.In order to maintain proper functions for the cardiovascular system,ECs should have a variety of mechano-sensors and transducers to sense the blood flow change and adjust the vessel size and transport across the vessel wall accordingly.Among more than a dozen recognized EC mechano-sensors,the primary cilium has drawn more and more attention recently.Primary cilium on endothelial cells is essential for the homeostasis of vessels.It is reported to be prevalent in areas of disturbed flow where atherosclerosis and intracranial aneurysm usually occur.Deficiencies of primary cilia may promote atherosclerosis,endothelial-to-mesenchymal transition(EndoMT)and loss of direction orientation,to name a few.Therefore understanding why the primary cilia are necessary to maintain the homeostasis of blood vessels and how will help us develop better treatment strategies for the common cardiovascular diseases.Dimension and structure of primary cilium Primary cilium is reported to be shorter than 8 in length and about 0.2 in diameter.The length of primary cilium varies in different cell types and under different conditions.The major structural components of the primary cilium include basal body,ciliary axoneme(consisting of nine doublet microtubules),ciliary membrane,transition zone,basal feet,and striated rootlets.Each part of the primary cilium is essential and has specific function.Current methods investigating the EC primary cilium as a mechano-sensor:Immunostaining and imaging techniques have been used to investigate the molecular mechanisms by which EC primary cilium serves as a mechano-sensor and transducer.It has been found that various proteins locate on the primary cilium,working together to maintain the function of primary cilium.Some proteins function as ion-channels,mediating Ca2+entry into the primary cilium.Some are involved in the cascade signal pathway.Others are related to the assembly and maintenance of primary cilium.Briefly,the flow induces the deflection of the EC primary cilium,which triggers calcium increase via opening of the PC2 cation channel that is responsible for calcium ion influx.This PC2 cation channel is localized to the primary cilium and is assumed to be stretch-activated.The resulting change in the intracellular calcium concentration then regulates numerous molecular activities inside the cell that contribute to vessel homeostasis.In addition to triggering calcium release,another mechanism has also been found in blood-pressure maintenance in the vasculature,where the vessel diameter is regulated by endothelial primary cilia through adjusting nitric oxide production.So far,little is known about the mechanical mechanism behind this deflection-triggered o-pening of signaling pathways.For example,what is the flow induced bending behavior and force distribution? What is the threshold value of stretch/defection for activating a corresponding signaling pathway? These all remain to be answered.In combination of image data and experiments,several computational models have been established to answer these questions.However,the current models are not able to include the complex structure of primary cilium and the model predictions are limited.Future studies With the development of super high resolution optical microscopy,more detailed images for the structural(molecular)components of EC primary cilia will be revealed,especially when the ECs are alive and the forces are known.Combining these experimental observations with more sophisticated mathematical models will elucidate the mechano-sensing mechanism of EC primary cilia,as the force and stress distribution on cilium along with other mechanical properties are still beyond the capability of experimental approaches due to the scales of the quantities involved.By using numerical approaches,much more detailed dynamic information can be obtained.

Pathologically relevant aldoses and environmental aldehydes cause cilium disassembly via formyl group-mediated mechanisms

Carbohydrate metabolism disorders(CMDs),such as diabetes,galactosemia,and mannosidosis,cause ciliopathy-like multiorgan defects.However,the mechanistic link of cilia to CMD complications is still poorly understood.Herein,we describe significant cilium disassembly upon treatment of cells with pathologically relevant aldoses rather than the corresponding sugar alcohols.Moreover,environmental aldehydes are able to trigger cilium disassembly by the steric hindrance effect of their formyl groups.Mechanistic studies reveal that aldehydes stimulate extracellular calcium influx across the plasma membrane,which subsequently activates the calmodulin-Aurora A-histone deacetylase 6 pathway to deacetylate axonemal microtubules and triggers cilium disassembly.In vivo experiments further show that Hdac6 knockout mice are resistant to aldehyde-induced disassembly of tracheal cilia and sperm flagella.These findings reveal a previously unrecognized role for formyl group-mediated cilium disassembly in the complications of CMDs.

中间体残体与初级纤毛的关系及其在肿瘤生长中的作用

最新研究表明,初级纤毛细胞外发生途径与一种特殊细胞器—中间体残体相关。中间体残体是细胞有丝分裂末期中间体脱落形成的点状细胞器,中间体残体形成后在细胞表面移动,当与中心体在细胞表面靠近后,调节中心体在其母中心粒的顶端形成初级纤毛。初级纤毛可作为抑制肿瘤发生的细胞器,并在多种肿瘤中丢失,研究发现中间体残体在肿瘤细胞中聚集影响初级纤毛的发生。更重要的是,中间体残体和初级纤毛在肿瘤细胞中均通过自噬途径降解,中间体残体还可以将肿瘤信号通路因子传递给初级纤毛进而影响肿瘤细胞的发生发展。本文综述了中间体残体和初级纤毛的基本结构及形成过程,详细阐述了中间体残体调控初级纤毛发生的具体机制,探讨及展望了中间体残体调控初级纤毛形成在肿瘤发生发展和靶向治疗中的作用及研究趋势。

A cilium-independent role for intraflagellar transport 88 in regulating angiogenesis

Endothelial cilia are microtubule-based hair-like protrusions in the lumen of blood vessels that function as fluid mechanosensors to regulate vascular hemodynamics. However, the functions of endothelial cilia in vascular development remain controversial. In this study, depletion of several key proteins responsible for ciliogenesis allows us to identify a cilium-independent role for intraflagellar transport 88(IFT88) in mammalian angiogenesis. Disruption of primary cilia by heat shock does not affect the angiogenic process. However, depletion of IFT88 significantly inhibits angiogenesis both in vitro and in vivo. IFT88 mediates angiogenesis by regulating the migration, polarization, proliferation, and oriented division of vascular endothelial cells. Further mechanistic studies demonstrate that IFT88 interacts with c-tubulin and microtubule plus-end tracking proteins and promotes microtubule stability. Our findings indicate that IFT88 regulates angiogenesis through its actions in microtubule-based cellular processes, independent of its role in ciliogenesis.

Control of the Hedgehog pathway by compartmentalized PKA in the primary cilium

The Hedgehog(Hh)signaling is one of the essential signaling pathways during embryogenesis and in adults.Hh signal transduction relies on primary cilium,a specialized cell surface organelle viewed as the hub of cell signaling.Protein kinase A(PKA)has been recognized as a potent negative regulator of the Hh pathway,raising the question of how such a ubiquitous kinase specifically regulates one signaling pathway.We reviewed recent genetic,molecular and biochemical studies that have advanced our mechanistic understanding of PKA’s role in Hh signaling in vertebrates,focusing on the compartmentalized PKA at the centrosome and in the primary cilium.We outlined the recently developed genetic and optical tools that can be harvested to study PKA activities during the course of Hh signal transduction.

中国大鲵机械感受器的超微结构

首次以透射电镜研究了大鲵成体 (实验材料共两条 )皮肤侧线器官中机械感受器即表面神经丘和陷器官的超微结构 ,并在这两种感受器官之间进行了比较。它们都由三种细胞组成 :周围的套细胞 ,底部的支持细胞以及中央的感觉细胞 ;且感觉细胞的游离面均有一根动纤毛和几十根静纤毛。但这两种器官在大小、各种细胞的数量、形状和排列上不同 ,尤其是表面神经丘感觉细胞游离面纤毛具有双向极性 ,而陷器官体现为多向极性 ;表面神经丘的突触球集中分布于一个特殊的感觉细胞 。

低频脉冲电磁场对大鼠成骨细胞骨形成的影响及作用机制

目的观察低频脉冲电磁场(PEMFs)对大鼠成骨细胞(ROBs)骨形成的影响,探讨了环磷酸腺苷(cAMP)/蛋白激酶A (PKA)/环磷腺苷效应结合蛋白(CREB)信号通路的作用机制。方法取新生Wistar大鼠颅骨,通过多次酶消化法获得ROBs并进行传代融合。采用50 Hz 0. 6 m T PEMFs处理3、6、9 d后,检测ROBs内的碱性磷酸酶(ALP)浓度;处理0、15、30、60、90、120 min后,检测ROBs内骨形成相关因子(RUNX2)和成骨相关转录因子(OSX)蛋白表达,cAMP浓度,p-PKA、p-CREB和CREB蛋白表达。观察p-CREB核转位情况。采用RNA干扰法干扰IFT88后,检测ROBs内RUNX2、OSX、p-PKA和p-CREB蛋白表达情况。结果 PEMFs处理ROBs 3、6、9 d后,ALP活性值分别为24. 356±4. 911、37. 688±2. 151和39. 922±5. 486,均明显高于相应对照组的18. 531±2. 401 (P=0. 0121)、33. 675±4. 366 (P=0. 0324)和36. 574±1. 339 (P=0. 0134)。PEMFs处理30 (P=0. 0042和P=0. 0058)、60 (P=0. 0097和P=0. 0079)、90 min (P=0. 0083和P=0. 0098)时,ROBs内的RUNX2和OSX活性均显著高于未处理组; PEMFs处理30(P=0. 0012)和60 min (P=0. 0035)时,ROBs内的cAMP浓度明显高于未处理时; PEMFs处理15 (P=0. 0018)、30 (P=0. 0087)、90 (P=0. 0250)和120 min (P=0. 0350)时,ROBs内的p-PKA水平明显高于未处理组; PEMFs处理15 (P=0. 0075)、30 (P=0. 0017)、60 (P=0. 0074)和90 min (P=0. 0096)时,ROBs内的p-CREB水平明显高于未处理组。PEMFs处理ROBs 15 min后,CREB发生磷酸化并聚集于细胞核内。将PKA、p-PKA与初级纤毛共定位染色,结果发现p-PKA定位于初级纤毛上。RNA干扰去除初级纤毛后,干扰组的p-PKA (F=78. 602,P=0. 0270)和p-CREB (F=76. 082,P=0. 0089)蛋白表达量及RUNX2 (F=41. 064,P=0. 0230)和OSX (F=57. 524,P=0. 0310)蛋白表达量均明显低于未干扰组。结论 PEMFs可能是通过初级纤毛相关的cAMP/PKA/CREB信号通路促进ROBs骨形成。

初级纤毛与Wnt信号通路相关性研究进展

初级纤毛是一类以微管为基础结构的细胞器,其来源于细胞的母中心粒,锚定在细胞膜并如"天线"般突出细胞表面。作为细胞感受器,初级纤毛从环境中接受各种信号,传导至细胞内引起细胞反应。近期的研究表明,初级纤毛对与胚胎发育密切相关的Wnt信号通路的传导起重要作用。纤毛的损害可造成Wnt信号通路的异常,并引起胚胎中多类脏器一系列的病理改变,导致初级纤毛相关疾病的发生。文章主要阐述了初级纤毛与Wnt/β-catenin、Wnt/PCP通路及初级纤毛相关疾病之间的关系,并对初级纤毛相关疾病的治疗进行了初步探讨。对初级纤毛与Wnt信号通路关系的深入研究将有助于人们对该类疾病的进一步诊断和治疗。

纤毛中Hedgehog信号调控机制研究进展

纤毛是多种信号通路的重要调节者,对Hedgehog(Hh)信号通路也起着至关重要的调控作用。研究表明Hh信号通路与鞭毛内转运密切相关,遗传学与细胞生物学的相关研究也表明了Hh信号对初级纤毛有依赖性。Hh信号通路的核心元件都定位于纤毛上,并通过鞭毛内转运实现其对信号刺激的应答,最终影响Hh基因的转录,而精子鞭毛的结构与纤毛类似,纤毛疾病也会造成精子鞭毛运动功能障碍。纤毛不动综合征等纤毛结构与功能的异常都会影响Hh通路,其诸多调节因子如Foxj1等对纤毛形成机制有重要意义,也为治疗不育症及避孕等相关措施研究提供了新思路。文章对纤毛中Hh信号调控机制研究进展进行综述。

MEMS矢量水听器定位误差分析与测试

针对一种纤毛式微机械电子(MEMS)矢量水听器的工作原理进行分析,通过分析得出该矢量微传感器的定位误差主要来源于纤毛柱体的偏差。通过有限元仿真分析得出纤毛柱体的偏差对矢量水听器在两个方向上的灵敏度有较大影响,理论计算出在纤毛偏移下2个轴向灵敏度度误差为9.74%。对水听器结构进行轴向灵敏度测试,测出x向灵敏度为0.683mV/g(其中g为重力加速度),y向灵敏度为0.755mV/g,两个方向上灵敏度相对误差为9.5%,与仿真结果接近。

一氧化碳和尼古丁对大鼠气管粘膜表面结构影响的扫描电镜观察

用香烟雾中的一氧化碳和尼古丁作用于幼年大鼠后，以扫描电镜观察了气管粘膜表面结构的变化。发现一氧化碳及尼古丁均使气管粘膜上皮表面的纤毛肿胀增粗、密度降低、出现倒伏和脱落；并促使杯状细胞增生。另外一氧化碳和尼古丁混合作用时出现了大面积的纤毛粘着和局部出现聚集成群的杯状细胞。

桉柠蒎的药理作用与临床评价

目的评价桉柠蒎的药理作用及临床应用。方法收集和查找文献资料,从药理作用、药动学、国内外临床研究、用法与用量、药物不良反应5个方面全面评价桉柠蒎。结果详细地评价了桉柠蒎的作用机理及临床应用。结论桉柠蒎是粘液溶解性祛痰药,可解除粘液纤毛清除系统障碍,全面恢复粘液纤毛清除系统功能,重建整个系统的清除防御机制,打破炎症的恶性循环,从根本上治疗鼻炎、支气管炎等气道炎性反应。

枇杷和葡萄果实的表面微细结构及其发育过程

扫描电镜观察表明，枇杷果实仅有一层表皮细胞，表皮着生的气孔和纤毛基部均由环形脊所包围．气孔的分化在果实开始膨大前即已完成，而纤毛可以在幼果膨大过程中持续分化产生．成熟纤毛呈卷曲丝状，平均最大直径为（２３．５８±１．９９）μｍ．葡萄果皮由三层表皮细胞构成，角质层较厚，其上未见气孔．幼果表面的蜡质层由不连续的垂直蜡质小片构成，随着果实的发育，蜡质小片增厚变宽，不断生长，最后相互连接，形成致密的蜂窝状结构．

MEMS仿生矢量水听器二次集成的误差分析测试

由中北大学研制的MEMS仿生矢量水听器具有低频、高灵敏度等性能特点,但由于纤毛柱体采用二次集成工艺集成在MEMS微结构上,常出现纤毛二次集成倾斜偏差,而且,该偏差严重影响到矢量水听器两轴输出的一致性,即灵敏度的一致性和指向性的对称性。为此研究了纤毛倾斜偏差对MEMS矢量水听器性能的影响。首先,理论上分析水听器工作原理和二次集成工艺的误差来源。然后,在通过激光显微镜等设备得出二次集成误差的基础上,通过ANSYS有限元分析方法分析得出纤毛的倾斜偏差对水听器的灵敏度影响很大,理论上计算出两个轴灵敏度误差为8.7%。因此,提出了通过优化二次集成工艺,从而减少两轴输出的不一致性。最后,采用矢量水听器校准系统测试改进前和改进后的水听器。结果表明:纤毛二次集成过程的倾斜偏差引起两轴输出的不一致(两轴灵敏度相对误差约为9.0%),改进后的水听器可以显著减小二次集成带来的误差。

鼻渊舒口服液对实验性鼻窦炎大鼠鼻粘膜的超微结构的影响

目的:观察鼻渊舒口服液对实验性鼻窦炎大鼠鼻粘膜的超微结构的影响。方法:运用透射电镜观察正常大鼠,实验性急性化脓性鼻窦炎大鼠和用鼻渊舒口服液灌胃治疗的实验性急性化脓性鼻窦炎大鼠的鼻粘膜的超微结构。结果:正常大鼠鼻粘膜的粘膜上皮纤毛结构正常,内质网和线粒体丰富;模型组大鼠鼻粘膜的纤毛大多倒伏、断裂、排列紊乱,胞浆内内质网和线粒体重度扩张;用鼻渊舒口服液治疗后的大鼠鼻粘膜上皮可见短纤毛,线粒体和内质网轻度扩张。结论:鼻粘膜纤毛清除系统的受损,在急性鼻窦炎的发生,发展上起着重要作用;鼻渊舒口服液可让受损的鼻粘膜上皮修复再生,为临床治疗提供了参考依据。

从苍蝇与物面的触粘看尺度效应

苍蝇与光滑硬物体接触时,靠腿上纤毛与物体表面产生吸附作用,在JKR接触理论下,得出考虑表面能作用时的粘附力表达式,结果表明苍蝇与物面的触粘和脱离界定了其纤毛的尺度范围,该尺度范围与扫描电镜观察的结果相一致。

仿生水听器设计、制造与测试

根据仿生鱼类侧线细胞纤毛原理,设计、制造并测试了一种新型双纤毛压阻水听器,用于检测水下声信号。与传统的压电水听器相比,这种水听器具有体积小和矢量性的优点。利用聚氨酯仿生细胞壁作为透声帽,利用硅油模拟细胞液和压阻微梁模拟感觉纤毛三层拾振结构,从而提高纤毛式水听器的可靠性。封装以后的纤毛式水听器采用振动台和矢量水听器校准系统进行测试,测得谐振频率为2.03 kHz,灵敏度可达-180 dB,具有余弦"8"字指向性。

丹参喷鼻剂的黏膜毒性评价

目的:考察丹参喷鼻剂的黏膜毒性。方法:选用家兔、蟾蜍和大鼠作为动物模型,观察丹参喷鼻剂对家兔眼黏膜及分泌物、对蟾蜍上颚纤毛摆动持续时间和大鼠鼻黏膜细胞形态的影响。结果:丹参喷鼻剂对家兔眼黏膜有可逆的轻微刺激性;蟾蜍丹参喷鼻剂组和生理盐水组的上颚纤毛运动停止时间无显著性差异;低剂量组大鼠鼻黏膜上皮基本完整、纤毛整齐,与生理盐水组无显著性差异。结论:丹参喷鼻剂安全有效。

初级纤毛在骨组织力学信号传导中的作用

骨组织不断接受力学刺激并保持骨形成和骨吸收的动态平衡。目前,人们仍不清楚骨组织如何感知力学刺激。越来越多的研究表明初级纤毛可能是骨组织力学刺激感受器,并将细胞外的力学刺激信号转化为细胞内的生化信息,最终骨组织实现其结构的重塑。在此,本文将对初级纤毛研究现状进行综述,并预测初级纤毛未来的研究趋势,为利用初级纤毛来防治骨质疏松症打下基础。