Increased excitatory amino acid transporter 2 levels in basolateral amygdala astrocytes mediate chronic stress–induced anxiety-like behavior

The conventional perception of astrocytes as mere supportive cells within the brain has recently been called into question by empirical evidence, which has revealed their active involvement in regulating brain function and encoding behaviors associated with emotions.Specifically, astrocytes in the basolateral amygdala have been found to play a role in the modulation of anxiety-like behaviors triggered by chronic stress. Nevertheless, the precise molecular mechanisms by which basolateral amygdala astrocytes regulate chronic stress–induced anxiety-like behaviors remain to be fully elucidated. In this study, we found that in a mouse model of anxiety triggered by unpredictable chronic mild stress, the expression of excitatory amino acid transporter 2 was upregulated in the basolateral amygdala. Interestingly, our findings indicate that the targeted knockdown of excitatory amino acid transporter 2 specifically within the basolateral amygdala astrocytes was able to rescue the anxiety-like behavior in mice subjected to stress. Furthermore, we found that the overexpression of excitatory amino acid transporter 2 in the basolateral amygdala, whether achieved through intracranial administration of excitatory amino acid transporter 2agonists or through injection of excitatory amino acid transporter 2-overexpressing viruses with GfaABC1D promoters, evoked anxiety-like behavior in mice. Our single-nucleus RNA sequencing analysis further confirmed that chronic stress induced an upregulation of excitatory amino acid transporter 2 specifically in astrocytes in the basolateral amygdala. Moreover, through in vivo calcium signal recordings, we found that the frequency of calcium activity in the basolateral amygdala of mice subjected to chronic stress was higher compared with normal mice.After knocking down the expression of excitatory amino acid transporter 2 in the basolateral amygdala, the frequency of calcium activity was not significantly increased, and anxiety-like behavior was obviously mitigated. Additionally, administration of an excitatory amino acid transporter 2 inhibitor in the basolateral amygdala yielded a notable reduction in anxiety level among mice subjected to stress. These results suggest that basolateral amygdala astrocytic excitatory amino acid transporter 2 plays a role in in the regulation of unpredictable chronic mild stress-induced anxiety-like behavior by impacting the activity of local glutamatergic neurons, and targeting excitatory amino acid transporter 2 in the basolateral amygdala holds therapeutic promise for addressing anxiety disorders.

Sodium-dependent glucose transporter 2 inhibitors effects on myocardial function in patients with type 2 diabetes and asymptomatic heart failure

BACKGROUND Sodium-dependent glucose transporter 2 inhibitors(SGLT2i)have shown efficacy in reducing heart failure(HF)burden in a very heterogeneous groups of patients,raising doubts about some contemporary assumptions of their mechanism of action.We previously published a prospective observational study that evaluated mechanisms of action of SGLT2i in patients with type 2 diabetes who were in HF stages A and B on dual hypoglycemic therapy.Two groups of patients were included in the study:the ones receiving SGLT2i as an add-on agent to metformin and the others on dipeptidyl peptidase-4 inhibitors as an add-on to metformin due to suboptimal glycemic control.AIM To evaluate the outcomes regarding natriuretic peptide,oxidative stress,inflammation,blood pressure,heart rate,cardiac function,and body weight.METHODS The study outcomes were examined by dividing each treatment arm into two subgroups according to baseline parameters of global longitudinal strain(GLS),N-terminal pro-brain natriuretic peptide,myeloperoxidase(MPO),high-sensitivity C-reactive protein(hsCRP),and systolic and diastolic blood pressure.To evaluate the possible predictors of observed changes in the SGLT2i arm during follow-up,a rise in stroke volume index,body mass index(BMI)decrease,and lack of heart rate increase,linear regression analysis was performed.RESULTS There was a greater reduction of MPO,hsCRP,GLS,and blood pressure in the groups with higher baseline values of mentioned parameters irrespective of the therapeutic arm after 6 months of follow-up.Significant independent predictors of heart rate decrease were a reduction in early mitral inflow velocity to early diastolic mitral annular velocity at the interventricular septal annulus ratio and BMI,while the predictor of stroke volume index increase was SGLT2i therapy itself.CONCLUSION SGLT2i affect body composition,reduce cardiac load,improve diastolic/systolic function,and attenuate the sympathetic response.Glycemic control contributes to the improvement of heart function,blood pressure control,oxidative stress,and reduction in inflammation.

The sexually dimorphic expression of glutamate transporters and their implication in pain after spinal cord injury

In addition to the loss of motor function,~60% of patients develop pain after spinal cord injury.The cellular-molecular mechanisms are not well understood,but the data suggests that plasticity within the rostral,epicenter,and caudal penumbra of the injury site initiates a cellularmolecular interplay that acts as a rewiring mechanism leading to central neuropathic pain.Sprouting can lead to the formation of new connections triggering abnormal sensory transmission.The excitatory glutamate transporters are responsible for the reuptake of extracellular glutamate which makes them a critical target to prevent neuronal hyperexcitability and excitotoxicity.Our previous studies showed a sexually dimorphic therapeutic window for spinal cord injury after treatment with the selective estrogen receptor modulator tamoxifen.In this study,we investigated the anti-allodynic effects of tamoxifen in male and female rats with spinal cord injury.We hypothesized that tamoxifen exerts anti-allodynic effects by increasing the expression of glutamate transporters,leading to reduced hyperexcitability of the secondary neuron or by decreasing aberrant sprouting.Male and female rats received a moderate contusion to the thoracic spinal cord followed by subcutaneous slow-release treatment of tamoxifen or matrix pellets as a control(placebo).We used von Frey monofilaments and the“up-down method”to evaluate mechanical allodynia.Tamoxifen treatment decreased allodynia only in female rats with spinal cord injury revealing a sexdependent effect.The expression profile of glutamatergic transporters(excitatory amino acid transporter 1/glutamate aspartate transporter and excitatory amino acid transporter 2/glutamate transporter-1)revealed a sexual dimorphism in the rostral,epicenter,and caudal areas of the spinal cord with a pattern of expression primarily on astrocytes.Female rodents showed a significantly higher level of excitatory amino acid transporter-1 expression while male rodents showed increased excitatory amino acid transporter-2 expression compared with female rodents.Analyses of peptidergic(calcitonin gene-related peptide-α)and non-peptidergic(isolectin B4)fibers outgrowth in the dorsal horn after spinal cord injury showed an increased calcitonin gene-related peptide-α/isolectin B4 ratio in comparison with sham,suggesting increased receptive fields in the dorsal horn.Although the behavioral assay shows decreased allodynia in tamoxifen-treated female rats,this was not associated with overexpression of glutamate transporters or alterations in the dorsal horn laminae fibers at 28 days post-injury.Our findings provide new evidence of the sexually dimorphic expression of glutamate transporters in the spinal cord.The dimorphic expression revealed in this study provides a therapeutic opportunity for treating chronic pain,an area with a critical need for treatment.

Drosophila models used to simulate human ATP1A1 gene mutations that cause Charcot-Marie-Tooth type 2 disease and refractory seizures

Certain amino acids changes in the human Na^(+)/K^(+)-ATPase pump,ATPase Na^(+)/K^(+)transporting subunit alpha 1(ATP1A1),cause Charcot-Marie-Tooth disease type 2(CMT2)disease and refractory seizures.To develop in vivo models to study the role of Na^(+)/K^(+)-ATPase in these diseases,we modified the Drosophila gene homolog,Atpα,to mimic the human ATP1A1 gene mutations that cause CMT2.Mutations located within the helical linker region of human ATP1A1(I592T,A597T,P600T,and D601F)were simultaneously introduced into endogenous Drosophila Atpαby CRISPR/Cas9-mediated genome editing,generating the Atpα^(TTTF)model.In addition,the same strategy was used to generate the corresponding single point mutations in flies(Atpα^(I571T),Atpα^(A576T),Atpα^(P579T),and Atpα^(D580F)).Moreover,a deletion mutation(Atpα^(mut))that causes premature termination of translation was generated as a positive control.Of these alleles,we found two that could be maintained as homozygotes(Atpα^(I571T)and Atpα^(P579T)).Three alleles(Atpα^(A576T),Atpα^(P579)and Atpα^(D580F))can form heterozygotes with the Atpαmut allele.We found that the Atpαallele carrying these CMT2-associated mutations showed differential phenotypes in Drosophila.Flies heterozygous for Atpα^(TTTF)mutations have motor performance defects,a reduced lifespan,seizures,and an abnormal neuronal morphology.These Drosophila models will provide a new platform for studying the function and regulation of the sodium-potassium pump.

Sodium-dependent glucose transporter 2 inhibitors:Transforming diabetic cardiomyopathy management

This article addresses the substantial findings of a study on sodium-dependent glucose transporter 2 inhibitors(SGLT2is)and their effects on myocardial function in patients with type 2 diabetes and asymptomatic heart failure.The editorial explores the broader implications of the study findings for clinical practice,thus highlighting the pivotal role of SGLT2is in improving cardiac function,reducing oxidative stress,and attenuating inflammation.It emphasizes the importance of early intervention with SGLT2is in preventing the progression of diabetic cardio-myopathy;hence,these inhibitors have the potential to transform the manage-ment of asymptomatic heart failure in patients with diabetes.

Crosslink among cyclin-dependent kinase 9,ATP binding cassette transporter G2 and Beclin 1 in colorectal cancer

Colorectal cancer(CRC)ranks third in the number of cancers mainly because of the inability to diagnose it at an early stage.The pathogenesis of CRC is complicated,which is the result of the complex interaction of multiple genetic and environmental factors.Currently,one of the main treatments for CRC is chemotherapy.But the primary cause of CRC treatment failure is drug resistance.The expression of cyclin-dependent kinase 9(CDK9)was correlated with elevated autophagy levels in colon cancer,and high expression of CDK9 indicates a poor prognosis in CRC.The incidence of autophagy and the expressions of Beclin 1 and ATP binding cassette transporter G2 are different in left and right colon cancer,and autophagy may be involved in the occurrence of chemotherapy resistance.In this article,the roles of CDK9,ATP binding cassette transporter G2 and Beclin 1 in CRC were elucidated,emphasizing the linkages among them and providing potential therapeutic targets of CRC.

Discharge mode and particle transport in radio frequency capacitively coupled Ar/O_(2) plasma discharges

Simulations are conducted on capacitively coupled Ar/O_(2)mixed gas discharges employing a one-dimensional fluid coupled with an electron Monte Carlo(MC)model.The research explores the impact of different O_(2)ratio and pressures on the discharge characteristics of Ar/O_(2)plasma.At a fixed Ar/O_(2)gas ratio,with the increasing pressure,higher ion densities,as well as a slight increase in electron density in the bulk region can be observed.The discharge remains dominated by the drift-ambipolar(DA)mode,and the flux of O(3P)at the electrode increases with the increasing pressure due to higher background gas density,while the fluxes of O(1D)and Ardecrease due to the pronounced loss rate.With the increasing proportion of O_(2),a change in the dominant discharge mode from a mode to DA mode can be detected,and the O_(2)-associated charged particle densities are significantly increased.However,Ar+density shows a trend of increasing and then decreasing,while for neutral fluxes at the electrode,Arflux decreases,and O(3P)flux increases with the reduced Ar gas proportion,while trends in O(1D)flux show slight differences.The evolution of the densities of the charged particle and the neutral fluxes under different discharge parameters are discussed in detail using the ionization characteristics as well as the transport properties.Hopefully,more comprehensive understanding of Ar/O_(2)discharge characteristics in this work will provide a valuable reference for the industry.

不同矿浆温度下Ca^(2+)、Mg^(2+)对黄铁矿可浮性的影响

这是一篇矿物加工工程领域的论文。通过单矿物浮选实验、浮选溶液化学、Zeta电位、XPS,研究了不同矿浆温度下Ca^(2+)、Mg^(2+)对黄铁矿浮选效果的影响机理,结果表明:低温能够明显抑制黄铁矿的浮选,且温度降低能够明显弱化Ca^(2+)、Mg^(2+)对黄铁矿浮选的抑制作用。当矿浆温度从20℃降至5℃时,矿浆中带电粒子运动速度减慢,Zeta电位增大,生成氢氧化钙镁沉淀的临界pH值增大,纯水矿浆中黄铁矿表面的FeO/OH的比例减小,Ca^(2+)、Mg^(2+)矿浆中黄铁矿表面FeO/OH含量的降低幅度减小,减少了黄铁矿表面的氧化程度和活性吸附位点,减少了Ca^(2+)、Ca(OH)+,Mg^(2+)和Mg(OH)+等离子在黄铁矿表面的吸附;但低温并不改变Ca^(2+)、Mg^(2+)在黄铁矿表面的存在形式和吸附状态,pH值为9时,钙镁均以Ca^(2+)、Ca(OH)+、Mg^(2+)、Mg(OH)+的形式存在并吸附在黄铁矿表面。

利用CRISPR/Cas9系统创制水稻品种GW2基因的突变体

培育具有育种价值的GW2基因编辑的水稻优异新品种在水稻育种中具有重要意义,利用CRISPR/Cas9基因编辑技术,以生产上广泛推广应用的13份水稻品种为材料,对粒质量基因(GW2)进行定向性状改良,通过农杆菌转化创制出一批无T-DNA元件的水稻非转基因GW2突变纯合株系。结果表明:13份T0代水稻转基因中,有28.0%~59.1%植株的GW2基因发生了突变,纯合突变株数量占总突变株数量的35.0%,双等位突变株数量占总突变株数量的14.2%,杂合突变株数量占总突变株数量的50.8%。此外,不同水稻品种发生的突变类型也略有不同。对13份T2代非转基因水稻GW2突变纯合株进行千粒质量性状的考种分析。与对应的野生型亲本品种相比,纯合突变水稻植株的千粒质量显著提高10.81%~58.22%。本研究结果极大地丰富了GW2的突变类型,为不同水稻品种的高产稳产创造了重要的种质资源,同时也为利用基因编辑提高水稻产量提供了有价值的育种信息。

尼莫地平对脊髓损伤大鼠脊髓组织Ca^(2+)及细胞焦亡的影响

目的研究尼莫地平(Nimodipine)对脊髓损伤(SCI)大鼠及脊髓组织Ca^(2+)及细胞焦亡的影响。方法将36只SD雄性大鼠按照随机数表法分为假手术组(Sham组)、脊髓损伤组(SCI组)和SCI+Ca^(2+)抑制剂尼莫地平组(Nimodipine组)各12只。脊髓撞击法制备大鼠SCI模型,BBB评分评估大鼠运动功能,荧光探针检测脊髓组织Ca^(2+)含量,酶联免疫吸附法检测白介素1β(IL-1β)及白介素18(IL-18)含量,蛋白免疫印迹检测细胞焦亡相关蛋白NOD样受体蛋白3(NLRP3)及半胱氨酸/天冬氨酸蛋白酶1(Caspase-1)的表达水平。结果与Sham组比较,SCI组大鼠BBB评分降低,差异有统计学意义(P<0.05);与Sham组比较,SCI组大鼠Ca^(2+)(18.92±3.60)、IL-1β[(383.66±45.42)pg/mL]、IL-18[(364.21±38.23)pg/mL]含量和NLRP3(0.93±0.19)、Caspase-1(0.98±0.08)的表达水平明显增加,差异均有统计学意义(P<0.05);与SCI组比较,Nimodipine组大鼠1 d、3 d、7 d的BBB评分稍增高,但差异均无统计学意义(P>0.05),而14 d、21 d及28 d大鼠BBB评分明显增高,差异均有统计学意义(P<0.05);与SCI组比较,Nimodipine组大鼠Ca^(2+)(11.73±4.31)、IL-1β[(292.93±28.48)pg/mL]、IL-18[(279.81±22.52)pg/mL]含量和NLRP3(0.79±0.18)及Caspase-1(0.63±0.10)的表达水平明显减少,差异均有统计学意义(P<0.05)。结论尼莫地平可能通过抑制Ca^(2+)来改善SCI大鼠的细胞焦亡及运动功能。

富里酸和Ca^(2+)共存对嗜酸性氧化亚铁硫杆菌介导生成次生高铁矿物的影响

为揭示富里酸和Ca^(2+)共存对嗜酸性氧化亚铁硫杆菌(Acidithiobacillus ferrooxidans)氧化酸性矿山废水(AMD)中的Fe^(2+)和形成次生高铁矿物的影响,分析了pH、Fe^(2+)氧化率、铁沉淀率以及次生高铁矿物矿相、基团等相关指标。结果表明,Ca^(2+)确实具有提高嗜酸性氧化亚铁硫杆菌氧化Fe^(2+)的能力。低质量浓度(0.2 g/L)的富里酸对嗜酸性氧化亚铁硫杆菌活性的提高具有促进作用,高质量浓度(0.4 g/L)的富里酸具有抑制作用,而增加Ca^(2+)反过来能够减弱高浓度富里酸对嗜酸性氧化亚铁硫杆菌的抑制作用。对形成的次生高铁矿物进行X射线衍射(XRD)和傅立叶红外光谱(FTIR)分析,结果表明高浓度富里酸促进了另一次生高铁矿物草黄铁矾的生成。

利用CRISPR/Cas9构建敲除小鼠模型研究PPP2R3A基因对心脏功能的影响

目的 应用CRISPR/Cas9技术构建蛋白磷酸2调节亚基B″家族α亚型(PPP2R3A)基因敲除小鼠,从分子水平及组织水平上研究PPP2R3A缺失对心脏的影响。方法 将Cas9 mRNA和两个靶向PPP2R3A第3外显子翻译起始密码子附近区域的单导向RNA微注射到C57BL/6小鼠受精卵中。小鼠出生后取其基因组DNA进行聚合酶链反应(PCR)和测序以鉴定基因型,鉴定后,基因PPP2R3A缺失型小鼠为KO组,野生型C57BL/6小鼠为WT组(雄性3只,雌性2只)。小鼠心脏组织经甲醛固定并制成切片后分别进行苏木素-伊红(HE)染色和免疫组织化学染色。提取小鼠心脏组织总RNA和蛋白,应用荧光定量PCR和Western印迹验证基因敲除小鼠的有效性和检测互作蛋白表达。结果 获得F1代PPP2R3A杂合小鼠,PCR和测序结果表明突变小鼠的基因型存在113 bp的缺失突变。与WT组相比,KO组心脏组织中PPP2R3A mRNA和蛋白表达量明显下降(均P<0.05),参与心脏发育的G蛋白信号转导调控因子(RGS)19表达量明显升高(P<0.05)。PPP2R3A蛋白表达受损引起了心脏组织病理学变化。结论 PPP2R3A在体内可能通过与RGS19蛋白互作来参与心脏的发育并对心脏功能产生影响。

川芎嗪抑制ROCK的表达降低模拟失重大鼠血管Ca^(2+)敏感性

研究失重条件下血管平滑肌收缩性、Ca^(2+)敏感性及其调控通路RhoA-ROCK蛋白表达的变化,以及川芎嗪干预对其的影响。大鼠尾部悬吊模拟失重,在机体前、后部分别选取颈总动脉和肠系膜上动脉。在模拟失重大鼠颈总动脉中,由苯肾上腺素(PHE)或KCl诱发的血管收缩性和Ca^(2+)敏感性增强,RhoA激酶2(ROCK II)的表达、肌球蛋白磷酸酶靶亚基1(MYPT1)和肌球蛋白调节轻链(MLC)的磷酸化水平均上升,血管孵育Y-27632(ROCK特异性抑制剂)后可降低以上变化。模拟失重大鼠灌饲川芎嗪亦可降低以上变化。模拟失重后,大鼠肠系膜上动脉的收缩性和Ca^(2+)敏感性、ROCK II的表达、MYPT1和MLC的磷酸化水平降低,血管孵育Y-27632对以上变化无明显作用。模拟失重大鼠灌饲川芎嗪亦对以上变化无明显作用。结果表明,由RhoA-ROCK调控的血管平滑肌Ca^(2+)敏感性的变化可能是失重条件下机体前后部血管收缩性发生区域性重塑的关键因素。川芎嗪可抑制ROCK蛋白的表达,降低血管平滑肌升高的Ca^(2+)敏感性,从而纠正失重条件下机体前部血管收缩性的增强,但对失重条件下机体后部血管收缩性的减弱无恢复作用。

乳腺癌患者HER2、CA153表达与声触诊组织成像定量技术参数的相关性分析

目的:分析乳腺癌患者人表皮生长因子受体2(HER2)、糖类抗原153(CA153)表达与声触诊组织成像定量(VTIQ)技术参数的相关性。方法:选取2018年5月至2020年5月合肥市第三人民医院收治的80例女性乳腺癌患者,其中世界卫生组织(WHO)分期Ⅰ期14例、Ⅱ期22例、Ⅲ期31例、Ⅳ期13例;另选取同时间段收治的53例女性乳腺良性疾病患者为对照。所有患者先行常规超声检查,随后进入超声VTIQ成像模式获得剪切波速度(SWV)均值参数;采用免疫组织化学法检测乳腺组织中HER2表达,采用罗氏E411电化学发光免疫分析仪检测血清CA153水平;采用Pearson法分析乳腺癌患者血清CA153水平与SWV均值的相关性。结果:与良性患者比较,乳腺癌患者VTIQ技术参数SWV均值、血清CA153水平及HRR2阳性表达率均显著升高,差异有统计学意义(F=39.107,78.353,P<0.05);与乳腺癌Ⅰ+Ⅱ期患者比较,乳腺癌Ⅲ、Ⅳ期患者VTIQ技术参数SWV均值、血清CA153水平、HRR2阳性表达率均显著升高,差异有统计学意义(t=2.685、3.556、8.326、10.455,P<0.05);与乳腺癌Ⅲ期比较,乳腺癌Ⅳ期患者VTIQ技术参数SWV均值、血清CA153水平、HRR2阳性表达率均显著升高,差异有统计学意义(t=4.632、8.659,P<0.05)。与HER2阴性表达乳腺癌患者SWV均值比较,HER2阳性表达乳腺癌患者SWV均值升高,差异有统计学意义(χ^(2)=59.751,P<0.05)。乳腺癌患者血清CA153水平与SWV均值呈正相关(r=0.501,P<0.05)。结论:乳腺癌患者VTIQ参数SWV均值与乳腺癌患者生物标志物HER2、CA153表达水平密切相关。

电针对糖尿病模型大鼠海马CA3区神经元Nrf2、HO-1和PSD95表达的影响

目的观察电针对糖尿病模型大鼠海马CA3区核因子E2相关因子(Nrf2)、血红素氧合酶(HO-1)与突触后致密蛋白95(PSD95)表达变化,探讨电针保护糖尿病神经系统损伤的可能机制。方法将雄性Wistar大鼠随机分为正常组、载体组、糖尿病组和电针组,每组8只。采用链脲佐菌素腹腔注射法制备糖尿病大鼠模型。造模成功1周后,电针组电针刺激一侧“足三里”及“胰俞”穴,30分钟/次,1次/天,连续4周。血糖仪检测大鼠空腹血糖水平;尼氏染色法观察大鼠海马CA3区神经元形态;免疫组织化学染色法检测大鼠海马CA3区的Nrf2、HO-1与PSD95的蛋白表达。结果空腹血糖检测结果显示,与正常组和载体组比较,糖尿病组血糖水平升高(P<0.05);与糖尿病组比较,电针组血糖水平降低(P<0.05)。尼氏染色结果显示,与正常组和载体组比较,糖尿病组海马CA3区神经元层次减少,胞核固缩;与糖尿病组比较,电针组海马CA3区神经元层次增加,形态改善。免疫组织化学染色结果显示,与正常组和载体组比较,糖尿病组海马CA3区Nrf2、HO-1与PSD95蛋白表达降低(P<0.05);与糖尿病组比较,电针组海马CA3区Nrf2、HO-1与PSD95蛋白表达升高(P<0.05),且与正常组和载体组表达水平相接近(P>0.05)。结论电针可上调糖尿病模型大鼠海马CA3区Nrf2、HO-1与PSD95的表达,提示其可能通过抑制氧化应激和改善突触可塑性发挥对其对神经元的保护作用。

基于SiO_(2)@CA微球的非晶结构色涂层的制备及光学性能

目的制备基于SiO_(2)@CA微球的非晶结构色涂层,并得到调控结构色颜色的方法,作为功能包装或智能包装的潜在应用。方法将咖啡酸(CA)与SiO_(2)微球在CuCl_(2)和NaBO_(3)·4H_(2)O的催化下产生活性氧(ROS),使CA迅速氧化为具有强黏附性的聚咖啡酸(PCA)包覆SiO_(2)微球,即SiO_(2)@CA复合微球,然后将该复合微球与无水乙醇组成的悬浮液喷涂于亲水化的玻璃基片表面,从而制得非晶结构色涂层。采用FT-IR、XPS、TGA、SEM等对SiO_(2)@CA复合微球及其结构色涂层进行表征,研究CA含量、CuCl_(2)/CA的质量比和NaBO_(3)·4H_(2)O/CA的质量比对复合微球的形貌及结构色涂层光学性能的影响。结果在CA质量分数为5%、CuCl_(2)/CA的质量比为12∶和NaBO_(3)·4H_(2)O/CA的质量比为64∶的制备条件下可以得到适宜的SiO_(2)@CA复合微球及结构色涂层。结论采用CA可有效提高所制备非晶结构色涂层颜色的对比度,实现颜色调控。

膜诱导技术结合Ca(OH)_(2)-PMMA治疗节段性骨缺损的研究进展

节段性骨缺损是一种负担较大、治疗具有挑战性的疾病,其病因包括创伤、感染、肿瘤等。目前骨缺损的重建方法主要有血管化骨移植、骨搬运以及膜诱导技术(Masquelet技术)等。而血管化自体骨移植虽然被认为是重建大尺寸骨缺损的金标准,但其具有专业性要求高、治疗周期长、过程复杂等局限性,而膜诱导技术因简单、高效及可靠等特性被广泛应用于骨缺损的治疗。膜诱导技术通过两次手术获取具有生物效应的诱导膜,促进缺损部位新骨的生长和愈合,是目前国内外公认的治疗节段性骨缺损的有效方法。本文将概述骨缺损的现状,介绍临界尺寸骨缺损的概念,探讨及思考在膜诱导技术中结合聚甲基丙烯酸甲酯氢氧化钙混合物[Ca(OH)_(2)-PMMA]新型材料应用于节段性骨缺损治疗的临床意义。

基于第一性原理计算Ca掺杂MoS_(2)对焊接气体的吸附性能

工业焊接的过程中会产生焊接废气例如CO、NO_(2)和CH_(4),这些气体会对工作人员的身心健康造成威胁,为解决这种废气吸附的需求,此文用基于密度泛函理论的第一性原理方法,搭建了Ca掺杂MoS_(2)的模型,用Dmol3模块研究掺杂后的电子结构,并计算了Ca-MoS_(2)吸附CO、CH_(4)和NO_(2)三种气体的态密度、电荷转移、吸附能、电子密度差等参数.结果表明Ca-MoS_(2)对于CH_(4)是一种物理吸附,主要是范德华力作用,而Ca-MoS_(2)吸附CO和NO_(2)是一种化学吸附,存在较强的吸附能力.此类掺杂有望制成新的气敏传感器等有益结果,该工作具有一定意义.

CRISPR/Cas9技术高效制备山羊SOCS2基因编辑胚胎

旨在设计、筛选高效编辑山羊胚胎生长负调控因子SOCS2基因的sgRNA,为通过SOCS2基因编辑创制快长型山羊奠定技术基础。本研究利用在线网站对山羊SOCS2基因SH2结构域保守序列设计2条sgRNA,构建表达载体,体外转录获得sgRNA及Cas9 mRNA;体外检测sgRNA+Cas9蛋白切割靶DNA的效率;在此基础上将屠宰场山羊卵巢分离培养的442个孤雌胚胎进行分组,2个试验组显微注射sgRNA和Cas9 mRNA混合物,对照组注射超纯水,以单个囊胚全基因组DNA扩增产物为模板,PCR扩增靶区域并测序鉴定,发生编辑的样本进行T-A克隆测序检测编辑形式;根据在线网站预测,每条sgRNA选择5个错配数最少的潜在脱靶位点进行脱靶检测。结果表明,在SOCS2基因83和96号氨基酸密码子附近区域获得2条sgRNA并成功构建表达载体,体外转录获得高质量sgRNA和Cas 9 mRNA;两条sgRNA均可引导Cas9蛋白在体外完全切割靶DNA;SOCS2-sg-83对胚胎的编辑效率为94.1%,160个T-A克隆中有152个在靶位点出现插入、缺失或替换,概率为95.0%,其中81.3%发生了移码突变,9.4%的克隆缺失83号氨基酸密码子,累计90.6%的克隆实现了SOCS2基因功能性敲除;SOCS2-sg-96对胚胎的编辑效率为50.0%,80个T-A克隆中有70个在靶位点出现插入、缺失或替换,概率为87.5%,移码突变概率为75.0%,5.0%的克隆缺失了96号氨基酸密码子,累计80.0%的克隆实现了SOCS2基因功能性敲除。另外,在所有已编辑胚胎中均未发现脱靶。综上,SOCS2-sg-83可实现山羊胚胎SOCS2基因的高效、精准编辑和敲除,为高效制备SOCS2基因敲除山羊,培育快长型肉用山羊奠定了技术基础。

黄腐酸对Ca(NO_(3))_(2)胁迫下菜薹幼苗生长及生理生化特性的影响

土壤次生盐渍化会严重影响菜薹的产量及品质,黄腐酸作为一种全水溶性的有机物质,对缓解植物盐胁迫具有积极作用。本研究以金秋红二号红菜薹为试验材料,探究在Ca(NO_(3))_(2)胁迫下外源施用黄腐酸对菜薹幼苗生长发育和生理生化指标的影响。结果表明,与15 mmol/L Ca(NO_(3))_(2)(CK)相比,80 mmol/L Ca(NO_(3))_(2)处理显著抑制了菜薹的生长,而与80 mmol/L Ca(NO_(3))_(2)处理相比,80 mmol/L Ca(NO_(3))_(2)+100μmol/L黄腐酸处理可以显著缓解Ca(NO_(3))_(2)对菜薹的抑制作用,促进菜薹幼苗的生长,增加菜薹幼苗的净光合速率及气孔导度。同时与80 mmol/L Ca(NO_(3))_(2)处理相比,80 mmol/L Ca(NO_(3))_(2)+100μmol/L黄腐酸处理可以显著降低菜薹幼苗叶片相对电导率和丙二醛含量,减少O_(2)·^(-)、H_(2)O_(2)的积累,增强抗氧化酶(超氧化物歧化酶、过氧化氢酶、抗坏血酸酶)活性。上述结果表明,外源施用黄腐酸可以通过提高菜薹的光合和抗氧化能力来缓解Ca(NO_(3))_(2)胁迫,本研究结果可为黄腐酸在缓解蔬菜盐胁迫中的应用提供理论依据。