存在睡眠呼吸异常的慢病患者呼吸影响心率变异性的初步分析*

目的: 基于整体整合生理学医学理论提出的呼吸引起循环指标变异的假说,分析研究存在睡眠呼吸异常的慢病患者睡眠期间呼吸和心率变异之间的相关关系。方法: 纳入存在睡眠呼吸异常且呼吸暂停低通气指数（AHI）≥15次/小时的慢病患者11例,签署知情同意书后完成标准化症状限制性极限运动的心肺运动试验（CPET）和睡眠呼吸监测,计算分析病人睡眠期间波浪式呼吸（OB）期与正常平稳呼吸期的呼吸鼻气流、心电图R-R间期心率变异的规律。结果: 存在睡眠呼吸异常的慢病患者CPET峰值摄氧量（Peak VO₂）和无氧阈（AT）为（70.8±13.6）%pred和（71.2±6.1）%pred;CPET有5例存在运动诱发的波浪式呼吸（EIOB）,6例为呼吸不稳定,提示整体功能状态低于正常人。本组慢病患者AHI为每小时（28.8±10.0）次,睡眠呼吸异常总时间占睡眠总时间的比值为（0.38±0.25）;OB周期的平均时间长度为（51.1±14.4）s。本组慢病患者正常平稳呼吸期的呼吸周期数与心率变异周期数的比值（B-n/HRV-B-n）为1.00±0.04,每个呼吸周期节律的心率变异平均幅度（HRV-B-M）为（2.64±1.59） bpm,虽然低于正常人（P<0.05）,但却与无睡眠呼吸异常的慢病患者相似（P>0.05）;HRV-B-M的变异度CV（HRV-B-M的SD/x）为( 0.33±0.11）,期间血氧饱和度（SpO₂）虽略低,但并无明显规律性下降与上升。本组慢病患者的OB期间呼吸周期数与心率变异周期数（OB-B-n/OB-HRV-B-n）比值为（1.22±0.18）,OB期每个呼吸周期节律的心率变异平均幅度（OB-HRV-B-M）为（3.56±1.57）bpm及其变异度（OB-CV =OB-HRV-B-M的SD/x）为（0.59±0.28）,每个OB周期节律的心率变异平均幅度（OB-HRV-OB-M）为（13.75±4.25）bpm,OB期间低通气时SpO₂出现明显的下降,OB期间SpO₂平均变异幅度（OB-SpO₂-OB-M）为（4.79±1.39）%,OB期的OB-B-n/OB-HRV-B-n比值、OB-HRV-OB-M比其正常平稳呼吸期对应指标显著增大（P<0.01）。OB-HRV-B-M虽然与正常平稳呼吸期HRV-B-M相比差异无统计学意义（P>0.05）,但其变异度OB-CV却显著增大（P<0.01）。结论: 睡眠呼吸异常的慢病患者OB期的心率变异幅度大于其正常平稳呼吸期,当呼吸模式发生改变时心率变异也发生明显改变,其平稳呼吸期的呼吸周期数与心率变异周期数的比值与正常人以及无睡眠呼吸异常的慢病患者相同,证实心率变异为呼吸源性;而其OB期间心率变异周期数相对于呼吸周期减少直接源于此时的低通气或者呼吸暂停,心率变异也是呼吸源性。     

柚皮苷通过P2X7受体减轻HIV-1包膜糖蛋白gp120导致大鼠神经功能损害的的作用及机制

人类免疫缺陷病毒-1(Human immunodeficiency virus-1,HIV-1)包膜糖蛋白gp120能够引起大鼠出现学习记忆障碍的行为学改变并增加海马中P2X7受体的表达;柚皮苷对gp120引起的行为学改变及P2X7表达增多具有改善作用。为了研究柚皮苷通过减少P2X7受体表达减轻gp120导致大鼠神经功能损害的作用及机制,本实验选择SD大鼠并分为假手术操作的对照组、脑室注射gp120的gp120组、脑室注射gp120及不同剂量柚皮苷灌胃的柚皮苷组、脑室注射BzATP的BzATP组、脑室注射gp120、BzATP及90mg/kg柚皮苷灌胃的90mg/kg/d柚皮苷+BzATP组。Morris水迷宫检测逃避潜伏期及错误次数,TUNEL法检测海马中细胞凋亡率,Elisa法检测海马中肿瘤坏死因子-α(Tumor necrosis factor-α,TNF-α)、白介素-1β(Interleukin-1β,IL-1β)、白介素-6(Interleukin-6,IL-6)的含量,Western blot检测海马中P2X7受体的表达。结果显示:与对照组比较,gp120组大鼠的逃避潜伏期延长,错误次数及海马中细胞凋亡率、TNF-α、IL-1β、IL-6的含量、P2X7受体的表达水平增加(P<0.05);与gp120组比较,不同剂量柚皮苷组大鼠的逃避潜伏期缩短,错误次数及海马中细胞凋亡率、TNF-α、IL-1β、IL-6的含量、P2X7受体的表达水平减少(P<0.05);与90mg/kg/d柚皮苷组比较,90mg/kg/d柚皮苷+BzATP组大鼠的逃避潜伏期延长,错误次数及海马中细胞凋亡率、TNF-α、IL-1β、IL-6的含量、P2X7受体的表达水平增加(P<0.05)。本研究的结果表明柚皮苷减轻HIV-1包膜糖蛋白gp120诱导的神经功能损害,这一作用与抑制海马组织中P2X7受体表达并减轻炎症反应及细胞凋亡有关。创新在于首次阐明了柚皮苷减轻HIV-1包膜糖蛋白gp120诱导神经功能损害的分子机制。在gp120引起大鼠行为学改变及海马组织中细胞凋亡、炎症反应激活的过程中,柚皮苷通过抑制P2X7受体的表达来改善行为学改变、抑制细胞凋亡及炎症反应的激活。     

滇西并流河谷区土壤酶活性化学计量学特征与环境因子的关系

横断山河谷区具有极高的景观异质性,气候与植被类型多样化程度较高。为探讨土壤C、N、P、S四种生物元素在滇西怒江、澜沧江、金沙江及元江并流河谷区的区域循环特征,在各河谷的森林、草地、农田中分别取浅层(0～10 cm)土样,测定了土壤中C、N、P、S的循环酶,即β-葡萄糖苷酶(BG)、N-乙酰-β-D-氨基葡萄糖苷酶(NAG)、酸性磷酸酶(AP)、硫酸脂酶(SU)活性,分析了土壤酶活性及其化学计量学特征与环境因素之间的关系。结果表明: 不同流域和不同土地类型下AP、NAG活性均有显著差异;4种酶活性之间均呈显著正相关,BG、NAG、SU活性由东南向西北随采样点的海拔升高而逐渐升高;在各流域土壤中,酶活性的生态化学计量比均为AP∶SU > BG∶SU > NAG∶SU > BG∶NAG > BG∶AP > NAG∶AP;与各流域内的林地和草地相比,农田土壤BG∶NAG较高,而NAG∶AP较低(元江流域除外);农田土壤中AP∶SU、BG∶SU、NAG∶SU在元江流域小于草地和林地,在澜沧江流域和金沙江流域则大于林地而小于草地。土壤酶活性及其化学计量学特征受到土壤理化性质、气候及区位的综合影响,其中土壤理化性质的影响最大。农业活动对C∶N∶P相关酶化学计量学特征具有显著影响,降低了土壤中N分解酶与其他酶活性的计量比,表现为增加了BG∶NAG,降低了NAG∶AP,农业活动对其他酶化学计量学特征的影响较小。     

Crumbs proteins stabilize the cone mosaics of photoreceptors and improve vision in zebrafish

Although the unique organization of vertebrate cone mosaics was first described long ago,both their underlying molecular basis and physiological significance are largely unknown.Here,we demonstrate that Crumbs proteins,the key regulators of epithelial apical polarity,establish the planar cellular polarity of photoreceptors in zebrafish.Via heterophilic Crb2a-Crb2b interactions,the apicobasal polarity protein Crb2b restricts the asymmetric planar distribution of Crb2a in photoreceptors.The planar polarized Crumbs proteins thus balance intercellular adhesions and tension between photoreceptors,thereby stabilizing the geometric organization of cone mosaics.Notably,loss of Crb2b in zebrafish induces a nearsightedness-like phenotype in zebrafish accompanied by an elongated eye axis and impairs zebrafish visual perception for predation.These data reveal a detailed mechanism for cone mosaic homeostasis via previously undiscovered apical-planar polarity coordination and propose a pathogenic mechanism for nearsightedness.     

Sustainability of SARS-CoV-2 Induced Humoral Immune Responses in COVID-19 Patients from Hospitalization to Convalescence Over Six Months

Virologica Sinica - Understanding the persistence of antibody in convalescent COVID-19 patients may help to answer the current major concerns such as the risk of reinfection, the protection period...     

PML Suppresses Influenza Virus Replication by Promoting FBXW7 Expression

Virologica Sinica - Influenza A viruses (IAV) are responsible for seasonal flu epidemics, which can lead to high morbidity and mortality each year. Like other viruses, influenza virus can hijack...     

Congestive heart failure in COX2 deficient rats

Non-steroidal anti-inflammatory drugs (NSAIDs) inhibit prostaglandin (PG) formation by targeting cyclooxygenase (COX) 1 and 2.Long-term use of NSAIDs that selectively inhibit COX2 increases the risk for thrombotic events,cardiac failure,and hypertension.However,the underlying mechanisms remain unclear.In this study,COX1- and COX2-deficient rats were created via Cas9/RNA-mediated gene targeting.DNA genotyping and Western blot analysis confirmed successful generation of COX1~(-/-)and COX2~(-/-)rats.Adult COX1~(-/-)rats grew normally,while more than 70%of COX2~(-/-)rats after wean died within 2 months.Echocardiography showed markedly reduced left ventricular ejection fraction and fractional shortening in adult COX2~(-/-)rats compared to those in wildtype (WT) controls.Histological analysis revealed accumulation of inflammatory cells and severe interstitial and perivascular fibrosis in COX2~(-/-)cardiac tissues.Moreover,cardiac ATP and acetyl-Co A production was dramatically decreased in COX2~(-/-)rats.Consistently,the expression of genes related to mitochondrial oxidation,such as those that encode for subunits of pyruvate dehydrogenase complex and acyl Co A dehydrogenases,were downregulated,while glycolytic hexokinase 1 (HK1) was upregulated in COX2~(-/-)heart tissues.These observations indicate that COX2-deficient rats developed spontaneously heart failure,likely as a result of dysregulated cardiac energy metabolism.     

Th2 polarization in target organs is involved in the alleviation of pathological damage mediated by transplanting granulocyte colony-stimulating factor-primed donor T cells

Acute graft-versus-host disease(a GVHD) is caused by allo-activated donor T cells infiltrating target organs. As a regulator of immune function, granulocyte colony-stimulating factor(G-CSF) has been demonstrated to relieve the a GVHD reaction.However, the role of G-CSF-primed donor Tcells in specific target organs is still unknown. In this study, we employed a classical MHC-mismatched transplantation mouse model(C57BL/6 into BALB/c) and found that recipient mice transplanted with GCSF-primed T cells exhibited prolonged survival compared with that of the PBS-treated group. This protective function against GVHD mediated by G-CSF-primed donor T cells was further confirmed by decreased clinical and pathological scores in this a GVHD mouse model, especially in the lung and gut. Moreover, we found that Tcells polarized towards Th2 cells and regulatory T cells were increased in specific target organs. In addition, G-CSF treatment inhibited inducible co-stimulator(ICOS) expression and increased the expression of tolerance-related genes in recipient mice. Our study provides new insight into the immune regulatory effects of G-CSF on T cell-mediated a GVHD, especially for its precise regulation in GVHD target organs.     

聚多巴胺的表面修饰功能在组织工程的应用进展*

聚多巴胺作为贻贝的仿生材料,可由多巴胺在碱性环境中自发形成。由于其较好的黏附特性以及组织相容性,在生命科学等领域有着广泛的应用。将聚多巴胺对材料进行表面修饰,既可以保护材料免受强氧化剂、酸碱等外界的侵蚀,也可以通过表面改性赋予材料新的功能,使其在各领域发挥更好的作用。对聚多巴胺的制备原理、生物性能,以及近年来在组织工程领域(骨组织、软骨组织、硬脑膜组织、血管组织、耳组织)的运用进行综述,以期为后续聚多巴胺作为组织工程黏附材料的研究提供参考。