Prepulse inhibition (PPI) of tactile startle response in recombinant congenic strains of mice:QTL mapping and comparison with acoustic PPI

Prepulse inhibition （PPI） of the startle response is a psychophysiological measure of sensorimotor gating believed to be cross-modal between different sensory systems. We analyzed the tactile startle response （TSR） and PPI of TSR （tPPI）, using light as a prepulse stimulus, in the mouse strains A/J and C57BL/6J and 36 recombinant congenic strains derived from them. Parental strains were significantly different for TSR, but were comparable for tPPI. Among the congenic strains, variation for TSR was significant in both genetic backgrounds, but that of tPPI was significant only for the C57BL/6J background. Provisional mapping for loci modulating TSR and tPPI was carried out. Using mapping data from our previous study on acoustic startle responses （ASR） and PPI of ASR （aPPI）, no common markers for aPPI and tPPI were identified. However, some markers were significantly associated with both ASR and TSR, at least in one genetic background. These results indicate cross-modal genetic regulation for the startle response but not for PPI, in these mouse strains.

Prepulse inhibition deficits in antipsychotic-na-ve first-episode schizophrenia:a meta-analysis

Objective:Published studies have found prepulse inhibition(PPI)in schizophrenia is impaired,suggesting PPI may be a biomarker of schizophrenia.We aim to examine whether PPI deficits exist in antipsychotic-na-ve,first-episode schizophrenia,and evaluate the effect size of PPI deficits between patients and healthy controls.Methods:The effect size of PPI deficits was evaluated for PPI%by calculating standard mean differences(SMDs)between patients with antipsychotic-na-ve,first-episode schizophrenia and healthy controls.Results:Twelve studies met the inclusion criteria,consisting390antipsychotic-na-ve,first-episode schizophrenia and406healthy controls.The effect sizes of76dB PPI in60ms and120ms interstimulus interval(ISI)were-0.19and-0.41respectively,and the76dB PPI overall effect size was-0.30.The effect sizes of85/86dB PPI in30ms,60ms and120ms ISI were-0.25,-0.42and-0.59respectively,and the85/86dB PPI overall effect size was-0.46.One study were excluded due to heterogeneity in the85/86dB,120ms ISI group,the pooled effect size of the PPI differences between patient group and health control dropped to-0.42,and the overall effect size changed to-0.39.There were no statistical differences in startle magnitude(overall effect size=-0.18)and habituation%(overall effect size=-0.17)between patients and healthy controls.Conclusions:Antipsychotic-na-ve,first-episode schizophrenia patients exhibit robust and reliable deficits in PPI,85/86dB PPI deficit was more severe than76dB PPI,and85/86dB,60-ms ISI PPI was more likely to be a biomarker for schizophrenia,it suggested that the parameters of PPI are particularly significant to affect the effect size so that should be interpreted with cautions in the future studies.

No Correlation between <i>AVPR</i>1A Promoter Polymorphisms and Prepulse Inhibition in Patients with Nocturnal Enuresis

Introduction: A correlation between AVPR1A promoter polymorphisms and prepulse inhibition (PPI) of startle reflexes has been described in healthy adults. Many children with nocturnal enuresis (NE) have a reduced PPI and treatment with desamino arginine vasopressin (dDAVP), a ligand of the arginine vasopressin receptor 1A (AVPR1A), and both improve clanical symptoms and significantly increase PPI. Methods: In 17 children (median 9.1 years, range 6.4-17.3) with NE, promoter repeats within the RS1 and RS3 regions of AVPR1A were quantified and correlated to PPI (native and age-adjusted). Results: No direct correlation was found between the number of promoter repeats at RS1 and PPI (correlation coefficient—0.240, p = 0.346) or RS3 and PPI (correlation coefficient—0.0192, p = 0.936), with no change through age-adjustment of PPI. The different RS3 length subgroups did not show differences in PPI, nor did differentiation of NE according to clinical subtype or treatment response to dDAVP show differences in the number of promoter repeats. Conclusion: The missing reproducibility of the correlation between AVPR1A promoter polymorphisms and PPI in a group with wide range of PPI suggests a more complex interaction. Therefore, further investigations are needed to analyze this very plausible interaction. Conditions with a reduced PPI, such as enuresis, schizophrenia or autism, are particularly interesting for this research.

Roles of 5-HT2 receptors in effects of DOM,ketamine and methamphetamine on prepulse inhibition in Sprague Dawley rats

OBJECTIVE Prepulse inhibition(PPI)of the acoustic startle response provides a measure of sensorimotor gating system mecha⁃nisms,which is known to be impaired in schizo⁃phrenia patients.We assessed the effects of the 5-HT2A/2C receptor agonist(±)2,5-dimethoxy-4-methylamphetamine(DOM),the NMDA receptor antagonist ketamine,the dopamine receptor ago⁃nist methamphetamine(Meth)on PPI and the startle magnitude in SD rats.METHODS AND RESULTS Systemic administration of the three compounds all dose-dependently reduced PPI.However,as far as startle magnitude,only DOM at the doses of 3 mg·kg-1 reduced that,while both ketamine and Meth did not change the startle magnitudes.Furthermore,to determine whether 5-HT2A receptor mediate this effect,the non-spe⁃cific 5-HT2 receptor antagonist cyproheptadine,specific 5-HT2A receptor antagonist ketanserin and specific 5-HT2C receptor antagonist SB242084 were tested.Cyproheptadine,ketan⁃serin and SB242084 did not alter startle ampli⁃tude by themselves in SD rats and only ketanserin slightly increased PPI at higher dose(3 mg·kg-1).PPI impairment induced by DOM was restored by pretreatment of cyproheptadine(1 mg·kg-1)and ketanserin(1 mg·kg-1),while not by pretreat⁃ment of SB242084(1 mg·kg-1).Damage of PPI induced by ketamine and Meth was not reversed by cyproheptadine(1 and 5 mg·kg-1).CONCLU⁃SION The receptor mechanisms underlying the disruption of PPI caused by DOM,ketamine and Meth were different from each other,at least 5-HT2A receptor was not the junction receptor for which the three chemicals acted.

惊跳反射前脉冲抑制在听觉领域的研究进展

惊跳反射前脉冲抑制(prepulse inhibition,PPI)是一种复杂的听觉行为反应,为评估人类和实验动物的听觉门控系统提供了有价值的方法。其神经通路涉及中枢听觉皮层,因此对于探究动物及人类(尤其是婴幼儿)听觉皮层的发育变化具有重要意义。本文对PPI在听觉科学领域近年来的研究进行总结,并探讨今后的发展趋势。

Discovery of Chrysoeriol,a PI3K-AKT-mTOR Pathway Inhibitor with Potent Antitumor Activity against Human Multiple Myeloma Cells in vitro

This study was designed to determine the impact of chrysoeriol on proliferation and cell cycle progression in the human multiple myeloma cell lines RPMI 8226 and KM3,and its related molecular mechanisms.Chryseoriol was identified by using the phosphorylated AKT-specific cytoblot high throughput assay.CCK-8 assay was employed to examine the growth inhibition rate and IC 50 (48 h) in peripheral blood mononuclear cells (PBMNCs),RPMI 8226 and KM3 cells treated with chrysoeriol at various concentrations.Cells were labeled with 5-6-carboxyfluorescein diacetate succinimidyl ester (CFSE),and the proliferation dynamics was detected by flow cytometry and analyzed with ModFit software.The cell cycles of RPMI 8226 and KM3 cells were measured by flow cytometry when the IC 50 concentration of chrysoeriol was adopted.The alterations in cell-cycle related proteins (Cyclin B1,Cyclin D1,p21) and proteins in PI3K-AKT-mTOR pathway were determined by Western blot analysis.The results showed the proliferation of multiple myeloma cells was significantly inhibited by chrysoeriol,resulting in cell cycle arrest in G 2 /M phase.Chrysoeriol could significantly reduce the expression of p-AKT (s473) and p-4eBP1 (t37/46) protein,meanwhile enhanced Cyclin B1 and p21 protein expression.Similar effects were not observed in PBMNCs from normal donors.It was concluded that chrysoeriol was a selective PI3K-AKT-mTOR pathway inhibitor.It restrained the proliferation of human multiple myeloma cells,but didn’t affect proliferation of PBMNCs from normal donors.It might exhibit the cell cycle regulatory effect via the inhibition of PI3K-AKT-mTOR signal pathway.

Panax notogiseng saponin inhibits ischemia-induced apoptosis by activating PI3K/Akt signal pathway in cardiomyocytes

The panax notoginseng saponin(PNS) had been clinically used for the treatment of cardiovascular diseases and stroke in China.It had been demonstrated that PNS could protect cardiomyocytes from injury induced by ischemi- a,but the underlying molecular mechanisms of this protective effect were still unclear.This study was aimed to investigate the protective effect and molecular mechanisms of PNS on apoptosis in H9c2 cells in vitro and rat myocardial ischemia injury model in vivo.Annexin-V/PI assay shew that PNS could protect H9c2 cells from apoptosis induced by serum, glucose and oxygen deprivation(SGOD) in a dose-dependent manner.However,the anti-apoptotic effect of PNS was reversed by LY294002,a specific PI3K inhibitor.This antiapoptotic effect of PNS was confirmed by JC-1,a specific probe of mitochondrial membrane potential staining.PNS could significantly increase phos-Akt in H9c2 cells by Western blot assays and its effect could be inhibited by LY294002.Furthermore,PNS could improve ischemic-induced left ventricular function as reflected by EF,LVDd and LVDs.PNS could also inhibited cellular apoptosis in myocardial tissues in ischemic rats by TUNEL assay.PNS administration also increased the expression of phos-Akt in rat ischemic myocardial tissues.These results suggested that PNS could protect myocardial cells from apoptosis induced by ischemia in vitro model and in vivo model through activating-PI3K/Akt signal pathway which may be meaningful for further understanding the molecular mechanisms of cardiac protection of PNS.And the results might be useful in treatment of myocardial ischemia in future.

Acoustic startle reflex and pre-pulse inhibition in tinnitus patients

Gap induced pie-pulse inhibition(Gap-PPI) of acoustic startle reflex has been used as a measurement of tinnitus in animal models.However,whether this test is sensitive to detect tinnitus in humans is still unclear.Based on the testing procedure used in animal studies,a human subject testing method was formulated and conducted to investigate if a similar result could be found in tinnitus patients.Audiologic and tinnitus assessments and acoustic startle reflex measurements were performed on seven tinnitus subjects and nine age matched subjects without tinnitus.There was no significant difference found between the control and tinnitus group on the Gap-PPl across the frequencies evaluated.The amplitude of the startle response in the tinnitus group with normal hearing thresholds was significantly higher than the control group and those with tinnitus and hearing loss.This preliminary result suggests that hyperexcitability in the central auditory system may be involved in tinnitus.There was no correlation between hearing thresholds and the increased amplitude of startle response.

儿童精神分裂症前脉冲抑制特征及三年随访

目的初步探讨儿童精神分裂症前脉冲抑制(prepulse inhibition,PPI)特征,并随访其变化。方法纳入56例儿童精神分裂症患者和38名健康儿童,应用事件相关脑电仪,采用单独强刺激和弱刺激+强刺激范式,进行PPI检测。患儿组于治疗后第1年、第2年和第3年进行PPI随访。结果基线时,在Cz点,患儿组比对照组单独强刺激的惊跳反射潜伏期延长[(97.00±13.02)ms vs.(86.02±11.10)ms,P<0.01],患儿组比对照组弱刺激+强刺激的惊跳反射潜伏期延长[(97.01±20.02)ms vs.(84.01±17.02)ms,P<0.01]、波幅增高[(47.01±21.00)μV vs.(39.00±12.01)μV,P<0.01],患儿组PPI比值低于对照组(43.02%±37.21%vs.66.00%±32.01%,P<0.01)。未发现患儿组PPI各指标与PANSS量表总分、各因子分有统计学相关性(P>0.05)。患儿组在治疗后的第1年、第2年和第3年进行PPI检测,Cz点惊跳反射波幅、PPI比值与治疗前比较差异无统计学意义(P>0.05)。结论儿童精神分裂症患者PPI存在异常,随访提示PPI变异可能是儿童精神分裂症患者的属性标志,此初步结论有待于临床中进一步证实。

儿童首发精神分裂症患者和正常儿童前脉冲抑制的对照研究

目的·采用前脉冲抑制(prepulse inhibition,PI)新技术评价儿童首发精神分裂症(childhood onset schizophrenia,COS)患者感觉门控及其变异特点。方法·应用事件相关电位仪,采用单独强刺激和弱刺激+强刺激范式,对56例COS患者和38名正常儿童(normal children,NC)进行PI检测,并用阳性和阴性症状量表(Positive and Negative Syndrome Scale,PANSS)、社会功能缺陷筛选量表(Social Disability Screening Schedule,SDSS)、社会支持量表(Social Adjustment Rating Scale,SSRS)、家庭负担会谈量表(Family Interview Schedule,FIS)等4个量表对COS患者进行综合评估。结果·比对上述量表形成的社会客观支持度与社会支持量标准值[(8±2)分],COS组数值为(10±3)分,两者差异具有统计学意义(P=0.007)。未发现PI与PANSS量表总分、各因子分的相关性(均P>0.05)。COS组比NC组单独强刺激的惊跳反射潜伏期延长[NC组为(86±11)ms,COS组为(97±13)ms,P=0.001]。COS组比NC组弱刺激+强刺激的惊跳反射波幅增高,潜伏期延长[NC组波幅为(39±12)μV,COS组波幅为(47±21)μV,P=0.007;NC组潜伏期为(84±17)ms,COS组(97±20)ms,P=0.003]。COS组PI抑制率低于NC组[NC组抑制率为(66±32)%,COS组抑制率为(43±37)%,P=0.000]。结论·COS患者同成人精神分裂症一样存在PI异常。PI变化可能是反映COS患者激越情绪变化的生物学标记的结果。

Impaired prepulse inhibition of acoustic startle in Chinese patients with first-episode, medication-naive schizophrenia

Background Patients with schizophrenia have prominent abnormality in information processing that can be observed by measures of prepulse inhibition （PPI） of acoustic startle reflex and PPI deficits have been considered as a candidate endophenotypic marker of schizophrenia. However, there has been little information on PPI and related measures in Chinese patients with schizophrenia. The research was to explore the deficits of acoustic startle reflex that might exist in Chinese patients with schizophrenia. Methods Startle response to acoustic stimuli, habituation, and PPI were examined in 31 Chinese patients with first-episode, medication-naive schizophrenia and 30 age-and sex-matched healthy Chinese controls. At the same day of startle testing, psychopathological symptoms of the patients were assessed with the Positive and Negative Syndrome Scale （PANSS）. Results Compared with healthy controls, patients exhibited the significant reduction in startle response and PPI deficits at 60 milliseconds （ms） intervals （PP160, P 〈0.05） but not at 30 or 120 ms intervals. Furthermore, there was a relatively strong correlation between PPI60 （P 〈0.05） and scores of positive scale of PANSS in patients with schizophrenia. Conclusion Our findings confirmed impaired PPI in Chinese patients with schizophrenia and suggested that a relationship between sensorimotor gating deficits and clinical symptoms of patients with schizophrenia might exist.

Differences in P50 and prepulse inhibition of the startle reflex between male smokers and non-smokers with first episode schizophrenia without medical treatment

Backgorund Nicotine may improve schizophrenia patient＇s cognitive deficit symptoms.This study was to explore the chronic effects of smoking on prepulse inhibition of the startle reflex （PPI） and P50 in the patients with first-episode schizophrenia （FES）.Methods The event-related potentials （ERP） recording and analysis instrument made by Brain Products,Germany,was used to detect PPI and P50 in 49 male FES patients （FES group,n=21 for smokers and n=28 for non-smokers） and 43 normal male controls （control group,n=19 for smokers and n=24 for non-smokers）.Results Compared with normal controls,the FES group had prolonged PPI latency when elicited by single stronger stimulus （P ＜0.05）; the FES group had prolonged PPI latency and increased PPI amplitude （P ＜0.05,0.01） when elicited by weak and strong stimuli.The FES group had lower PPI inhibition rate than normal controls （P ＜0.05）.Compared with normal controls,the FES group had increased P50-S2 amplitude and increased amplitude ratio S2/S1 （both P ＜0.05）.In the control group,the smokers had a tendency of increase in P50-S2 amplitude （P ＞0.05） and shorter P50-S2 latency （P ＜0.05） than the non-smokers.The smokers had higher PPI amplitude than the non-smokers （P ＜0.05）.In the FES group,the smokers had higher P50-S1 amplitude,shorter P50-S2 latency,and higher amplitude ratio S2/S1 than the non-smokers （P ＜0.05,0.01）.The smokers had higher PPI amplitude than the non-smokers （P ＜0.05）.Conclusions There is obvious PPI and P50 deficits in schizophrenic patients.However,these deficits are relatively preserved in the smokers compared with the non-smokers,which suggests that long-term smoking might partially improve the sensory gating in schizophrenic patients.Whether this conclusion can be deduced to female patients requires further follow-ups.

助孕3号方防治大鼠自然流产的机理研究

目的:研究助孕3号方防治肾虚、脾虚型大鼠自然流产的机理。方法:(1)以羟基脲与米非司酮(RU486)建立肾虚加黄体抑制模型,利血平与RU486建立脾虚加黄体抑制模型。(2)观察助孕3号方对病证结合模型大鼠孕酮(P)分泌、蜕膜孕激素受体(PR)和雌激素受体(ER)的影响;酶联免疫法检测血清卵泡刺激素、雌二醇和P,免疫组化法检测蜕膜PR,光镜观察子宫、卵巢的形态学改变。(3)助孕3号方对大鼠离体与在体子宫兴奋性的影响,采用水提液与含药血清进行离体子宫兴奋试验。结果:(1)助孕3号方能提高肾虚加黄体抑制与脾虚加黄体抑制模型大鼠蜕膜PR阳性率,与单纯黄体抑制模型组比较差异均有显著性(P<0.05)。(2)助孕3号方水提液和含药血清均能降低离体子宫肌条收缩的强度(P<0.05),在体子宫兴奋试验提示助孕3号组子宫收缩强度显著下降(P<0.05)。结论:补肾和补肾健脾中药保胎的主要作用环节是提高靶细胞PR以及对子宫平滑肌的舒缓作用。

磷缓解水鳖镉毒害的生理研究

研究了 Cd对水鳖生理生化过程的影响及 Pi对 Cd胁迫的缓解作用。结果显示 ,Cd能抑制水鳖的代谢和生长 ,使叶绿素含量与光合速率下降 ,呼吸速率与可溶性糖含量增加 ,POD活性增强 ;当加入 0 .6 mmol/L Pi后 ,能相对减轻 Cd造成的毒害 ,表现出 Pi对

精神分裂症感觉门控电位P50和惊跳反射弱刺激抑制的相关性

目的:探讨精神分裂症患者感觉门控电位P50和惊跳反射弱刺激抑制(PPI)的特征以及两者的相关性。方法:选取符合美国精神障碍诊断与统计手册第4版(DSM-IV)的精神分裂症患者78例,正常对照90例,使用阳性和阴性症状量表(PANSS)评定精神分裂症患者的临床精神病理症状;使用脑电生理记录仪,采用听觉条件(S1)-测试(S2)刺激范式进行P50检测;使用SR-HLAB惊跳反射监控系统测查听觉惊跳反射。结果:精神分裂症组的S1波幅低于对照组[(2.9±1.7)μV vs.(3.7±2.0)μV,P<0.05];S2波幅高于对照组[(2.0±1.2)μV vs.(1.4±1.5)μV,P<0.001];P50抑制率比值(S2/S1)精神分裂症组高于对照组[(0.8±0.5)vs.(0.4±0.4),P<0.001],P50抑制率差值(S1-S2)低于对照组[(0.9±1.7)vs.(2.3±1.8),P<0.001]。精神分裂症组的惊跳反射的波幅低于对照组[(1037.5±1048.6)ms vs.(1367.7±952.3)ms,P<0.001],习惯化百分比亦低于对照组[(33.9±20.8)%vs.(48.8±34.7)%,P=0.002];精神分裂症组的PPI60和PPI120均低于对照组[(24.1±9.1)%vs.(29.8±11.5)%,P=0.020;(31.2±10.1)%vs.(42.6±15.4)%,P<0.001]。在精神分裂症组中,P50各项分析指标与PPI各项分析指标间的相关性无统计学意义(P>0.05),P50与PPI各项分析指标与PANSS总分、PANSS阳性症状总分、PANSS阴性症状总分间的相关性无统计学意义(P>0.05);在对照组中,惊跳反射的波幅与s1波幅与s2波幅呈正相关(r=0.28、0.27,均P<0.05)。结论:精神分裂症患者可能存在感觉门控的缺陷,P50和PPI缺陷与临床精神病理症状的严重程度可能无关,反映感觉门控的两种测量模式P50和PPI间可能无相关性,二者可能相互独立。

氟哌啶醇对MK-801致小鼠高活动性与前脉冲抑制损害的作用☆

目的观察氟哌啶醇对谷氨酸功能低下小鼠模型表现出的高活动性及前脉冲抑制（prepulse inhibition，PPI）损害的作用。方法昆明种小鼠152只分组（n=8或n=10）进行下述对照观察：观察不同剂量氟哌啶醇（0．03、0．1、0．3mg／kg）腹腔注射对昆明种小鼠探究行为和自主活动的影响；以0．25mg／kgMK-801诱导小鼠自主活动增加，观察上述剂量氟哌啶醇对MK-801致小鼠高活动性的影响；以0．5mg／kgMK-801诱导小鼠PPI损害，观察氟哌啶醇（0．1、0．3、1mg／kg）对基线水平PPI以及MK-801损害后PPI的作用。结果与对照组比较，氟哌啶醇剂量为0．1mg/kg和0．3mg／kg时，小鼠的探究行为及自主活动总路程减少（P〈0．05）；但剂量为0．03mg／kg时，对小鼠的探究行为及自主活动均无影响（P〉0．05）。氟哌啶醇剂量为0．1—0．3mg／kg时，呈剂量依赖性抑制由MK一801引起的自主活动增加（F=27．23，P〈0．01），0．1mg／kg的氟哌啶醇的抑制程度为22％（P〈0．01），0．3mg,／kg的氟哌啶醇的抑制程度为65％（P〈0．001）。氟哌啶醇（0．1、0．3、1mg／kg）呈剂量依赖性增强了基线的PPI（F=9．06，P〈0．001），增加程度分别为44％（P〈0．05）、60％（P=0．001）和61％（P=0．001）。只有剂量为1mg／kg时抑制了MK-801引起的PPI损害（P〈0．05）。结论氟哌啶醇非特异性地抑制了谷氨酸功能低下小鼠模型表现出的高活动性与PPI损害。

精神分裂症患者听觉惊跳反射抑制与儿茶酚-O-甲基转移酶基因Val158Met多态性的相关性

目的:探讨精神分裂症患者儿茶酚-O-甲基转移酶(COMT)第158位密码子从缬氨酸到蛋氨酸的多态性(Vall58Met)与听觉惊跳反射抑制(PPI)的关系。方法:选取符合美国精神障碍诊断与统计手册第4版(DSM-IV)的精神分裂症患者178例,正常对照190例,使用SR-HLAB惊跳反射监控系统测查听觉惊跳反射,其分析指标包括:惊跳反射的反应波幅(SR);惊跳反射的适应性(HAB);时间间隔(LI)为30 ms、60 ms、120 ms时的听觉刺激惊跳反射弱刺激抑制(PPI30%、PPI60%、PPI120%);应用聚合酶链反应和限制性片段长度多态性的方法,分析精神分裂症组与对照组COMT Vall58Met基因型与等位基因分布频率。结果:精神分裂症组的波幅(SR)低于对照组[(563±460)mVvs.(695±447)m V,P<0.05],适应性(HAB)低于对照组[(32±46)vs.(48±33),P<0.01],差异有统计学意义;精神分裂症组与对照组之间PPI差异有统计学意义(F=7.15,P<0.05),组与时间间隔的交互作用差异有统计学意义(F=5.57,P<0.05),进一步分析发现精神分裂症组的%PPI120低于对照组[(27±5)vs.(35±3),P<0.05]。2组间COMT基因型和等位基因分布有统计学意义(χ~2=8.16、11.74,均P<0.05)。COMT三种基因型对HAB%的主效应有统计学意义(F=3.07,P<0.05);分组和COMT基因型对SR,HAB%,%PPI120的交互作用无统计学意义(F=1.64、2.87、2.26,均P>0.05)。结论:COMT基因Vall58Met多态性可能与精神分裂症的适应性有关,但与精神分裂症PPI缺陷可能无关。

对听感觉运动门控自上而下调节的动物模型和神经机制

对惊反射的前脉冲抑制是减少干扰影响、保护脑内信息加工的重要机制。它既是研究感觉运动门控的模型,也是探究精神分裂症机制的模型。前脉冲抑制可被选择性注意和情绪等高级认知活动所调节。本论文工作围绕着恐惧条件化和知觉空间分离去掩蔽(空间选择性注意)对听觉前脉冲抑制多层次化的自上而下调节,在大鼠行为模型、神经通路、神经电生理机制等几个层次上开展了系统性研究,并引入了精神分裂症的神经发育模型,证实早期社会隔离饲养对前脉冲抑制注意调节的破坏影响。本论文研究成果不仅对认识正常情况下脑在复杂刺激场景中的信息加工机制有重要意义,以感觉运动门控认知调节功能缺失为基础的动物模型也将推动精神分裂症心理学和神经生物学机制的研究。

不同注意形式调节听感觉门控的神经机制

前脉冲抑制(prepulse inhibition,PPI)是听感觉门控的测量模型,反映了听觉系统的早期信息选择功能。尽管PPI的主要神经环路位于脑干,研究发现PPI可以被注意自上而下调节。然而,已有研究并未区分不同注意(特征注意和空间注意)对PPI的特异性调节,并且神经机制方面的研究集中于听皮层区域,仍缺乏对皮层下机制的探讨。在以往研究的成果基础之上,借助听觉信息加工的双通路模型,采用行为测量、脑电和脑成像技术,揭示特征和空间两种注意调节PPI的神经活动在听觉系统中的层次性神经表达。包括1)建立特征注意和空间注意调节PPI的统一行为模型,考察两种注意调节PPI的时间动态性异同;2)两种注意调节PPI的脑干分离机制,即前脉冲刺激包络和精细结构成分加工在注意调节PPI中的作用差异;3)两种注意调节PPI的关键脑区和脑网络差异。

不同月龄精神分裂症模型小鼠前脉冲抑制行为的异常

目的研究不同月龄精神分裂症模型小鼠的前脉冲抑制(prepulse inhibition,PPI)改变。方法将小鼠按照月龄分为青年、中年和老年组,按小清蛋白(parvalbumin,PV)阳性的γ-氨基丁酸能神经元中精神分裂症风险基因Erbb4基因型分为精神分裂症模型(PV-Erbb4-/-)小鼠和正常对照(PV-Erbb4+/+)小鼠,用前脉冲抑制实验检测PPI效率(PPI%),前脉冲刺激为74 dB、78 dB和86 dB,用一般线性回归分析Erbb4基因型和年龄对PPI%的交互作用。结果前脉冲刺激为78 d B和86 dB时,Erbb4基因型和年龄对PPI强度的交互作用有统计学意义(P<0.05),正常对照(PV-Erbb4+/+)小鼠老年组PPI%比青年组更小(78 dB:β=-13.61,P=0.02;86 dB:β=-10.58,P=0.03)。结论年龄和Erbb4基因型对PPI的影响存在交互作用,正常对照小鼠PPI随年龄增加而减小,而精神分裂症模型小鼠变化方向相反。