Literature DB >> 30115023

Impact of childhood trauma on sensory gating in patients with first-episode schizophrenia.

Xian-Bin Li1, Qi-Jing Bo1, Qing Tian1, Ning-Bo Yang1, Zhen Mao1, Wei Zheng2, Yu-Jie Wen1, Chuan-Yue Wang3.   

Abstract

BACKGROUND: Childhood trauma (CT) has been found to contribute to the onset of schizophrenia and auditory sensory gating deficit is a leading endophenotype for schizophrenia. However, the association between the CT and sensory gating in first-episode schizophrenia remains elusive.
METHODS: Fifty-six patients and 49 age and sex-matched healthy controls were assessed using the Childhood Trauma Questionnaire-Short Form (CTQ-SF) for CT and Positive and Negative Syndrome Scale (PANSS) for symptoms severity. Sensory gating was tested using the modified paradigm, perceived spatial separation-induced prepulse inhibition (PSS-PPI), and the perceived spatial co-location PPI (PSC-PPI or classical PPI).
RESULTS: Comparing with healthy controls, the patients had significantly higher score on sexual abuse (t = 2.729, p < 0.05), lower PSS- PPI, % (ISI = 120 ms and ISI = 60 ms) (t = - 3.089, - 4.196, p < 0.05). Univariate analysis revealed the absence of a significant correlation among CT, PPI paradigms and symptoms. However, multiple linear regression analyses demonstrated the CTQ-SF total was negatively associated with PSS PPI (ISI = 120 ms) (p = 0.018).
CONCLUSION: The current study illustrates that the impact of CT on sensory gating in patients with first-episode schizophrenia, and thus we conclude that CT may be a risk factor to the occurrence of schizophrenia through its impact on sensory gating.

Entities:  

Keywords:  Childhood trauma; Schizophrenia; Sensory gating

Mesh:

Year:  2018        PMID: 30115023      PMCID: PMC6097339          DOI: 10.1186/s12888-018-1807-7

Source DB:  PubMed          Journal:  BMC Psychiatry        ISSN: 1471-244X            Impact factor:   3.630


Background

Schizophrenia can be understood as a complex illness of adaptation to social context. Although heritability is often emphasized, the fact that occurrence is associated with environmental factors such as childhood trauma (CT) suggests that exposure to life stress may play an important role in developing “social” brain during sensitive periods [1]. Childhood adversities, particularly exposure to multiple adversities involving hostility, threat, and CT (emotional, physical, and sexual abuse; emotional and physical neglect) have been found to contribute to the onset of psychiatric disorder including schizophrenia [2-4]. Auditory sensory gating deficit is a leading endophenotype for schizophrenia [5]. The prepulse inhibition (PPI) is the weakening of acoustic startle reflex (ASR) when a weaker sensory stimulus precedes the startling stimulus [6], which is considered as a good indicator of sensory gating [7]. PPI impairment has been found to always be associated with core features of schizophrenia, such as aggressive behavior [8] and positive symptoms [9, 10], and relatively stable across treatment conditions [11]. It is also considered as an early sign or residual symptom of schizophrenia [12, 13]. The social isolation rat model shares some similarities with the humans experiencing CT and some neurobiological changes in socially isolated rats can mimic characteristics of schizophrenia, therefore it can serve as a model of schizophrenia [14]. Studies show that socially isolated rats exhibit increased level of ASR and produce specific deficits in PPI [6, 15]. Furthermore, exposure to CT during puberty was associated with increased risk for neuropsychiatric disorders through PPI deficit in rats [16]. In the previously study, we found sexual abuse can be a predisposing factor that affects sensorimotor gating in the patients with chronic schizophrenia [17]. To date, the association between the ASR, PPI and CT in first-episode schizophrenia has not been explored. Therefore, we aimed to examine the relationship between CT, ASR and PPI in Chinese patients diagnosed with first-episode schizophrenia in the current study.

Methods

Subjects

All participants were inpatients or outpatients of Beijing Anding Hospital, Capital Medical University in Beijing, China. The inclusion criteria were: (1) Met the diagnostic criteria of first-episode (less than 60 months) schizophrenia based on the Structured Clinical Interview for DSM-IV (SCID) [18]; (2) Had been clinically stable for > 12 weeks; (3) had a IQ above 80 on the Wechsler Adult Intelligence Scale (CWAIS) [19] and were able to read, comprehend and sign the consent. Patients were excluded if they were clinically unstable. In addition, 49 individuals without severe mental disorders or current substance use (included nicotine abuse) were recruited from the same geographical areas to serve as healthy controls for the PPI test battery and CTQ assessment (Controls’ age mean ± SD: 26.2 ± 3.9; years of education mean ± SD:14.0 ± 2.3). The protocol of this study was revised and approved by the ethics committee of Beijing Anding Hospital, Beijing, China. We followed the Declaration of Helsinki while we conducting the research. Each patient signed an informed written consent, an overseeing mental health expert have ruled that all adult patients and participants have been capable of ethically and medically consenting for their participation in the research. In the case of members of this study may not be capable of providing ethical consent for their participation, we would provide a legal guardian or representative to provide consent to participate in their stead. A total of 62 eligible patients between the age of 16 and 65 years old were initially enrolled, however, 10 patients (10.7%) dropped out from the study.

Assessment of childhood trauma questionnaire – Short form (CTQ-SF)

We used the CTQ-SF to screen for CT in our patient and the healthy controls. The CTQ-SF is a 28-item retrospective self-report survey of CT experiences, which has five categories for children 12 years and older [20]. The five subscales included were emotional abuse (EA), physical abuse (PA), sexual abuse (SA), emotional neglect (EN) and physical neglect (PN). Each subscale contains five items [21]. The Chinese version of CTQ-SF has been shown to have good validity and reliability [22].

Assessment of psychiatric symptomatology and demographic features

We used the Positive and Negative Symptoms Scale (PANSS) to evaluate the symptom of the patients [23]. Furthermore, we used locally-developed data collection tables to collect demographic characteristics (age at onset, age of first treatment seeking, the duration of untreated psychosis).

Assessment of startle reflex

Apparatus

The experiments was conducted in a sound shielded room, and the temperature and humidity was comfortable. Two Ag/AgCl electrodes (diameter, 0.4 cm; resistance <5kΩ) were positioned on below and lateral to the right eye, over the orbicularis oculi muscle. Acoustic startle reflection was measured as the eyeblink component from EMG activity (filtering, 100–1000 Hz; amplifying, 10,000). Acoustic signals were delivered binaurally through Sennheiser HD 600 headphone. Acoustic sound intensity were calibrated by AUDit and System 824 audiometer calibration (Larson Davis, USA).

Testing procedure

A new designed paradigm was used in PPI testing. The prepulse sound (acoustic intensity, 65 dB SPL; duration, 150 ms; broadband white noise) was performed from headphones with interaural leading time differences at each ear onset delay 3 ms (left ear leading or right ear leading). Moreover, the background noise (acoustic intensity 60 dB SPL from 0 to 10 kHz) was presented in this testing as a masker (interaural leading time differences, 3 ms), and the background noise was contributed to a fused noise-masker signal between prepulse sound (target sound) and the background noise (masker). As a result of precedence effect, two types of perceived spatial relationships were generated: perceptual spatial separation PPI (PSS PPI) and perceptual spatial co-location PPI (PSC PPI). A trial performed a prepulse stimuli, followed by a startling pulse stimuli of 104 dB SPL broadband white nosie for 40 ms. Two lead inter-stimulus interval (ISI) (prepulse onset to pulse onset) were used (60 ms, 120 ms). Then a new trial started in a random time (15 to 25 s). Thus, four trial combinations (PSC PPI or PSS PPI * ISI 120 ms or 60 m’s) were performed in the experiment. We described the detailed measurement procedures in our other published articles (Fig. 1) [24].
Fig. 1

Schematic illustration of the prepulse inhibition paradigm. In a block design (7 min), a background wideband noise was continuously delivered as the masker (left leading or right leading), 7 trials contained the startling (pulse) sound alone, and 20 trials contained the prepulse (left leading or right leading) 120 ms or 60 ms preceding the startling (pulse) noise. Trials in each block were presented randomly with the inter-trial interval about 20 s. Note: RNRP (RNLP): right leading masking with prepulse co-location (separation); LNLP (LNRP): left leading masking with prepulse co-location (separation). We have published this paradigm in our privous paper ([24])

Schematic illustration of the prepulse inhibition paradigm. In a block design (7 min), a background wideband noise was continuously delivered as the masker (left leading or right leading), 7 trials contained the startling (pulse) sound alone, and 20 trials contained the prepulse (left leading or right leading) 120 ms or 60 ms preceding the startling (pulse) noise. Trials in each block were presented randomly with the inter-trial interval about 20 s. Note: RNRP (RNLP): right leading masking with prepulse co-location (separation); LNLP (LNRP): left leading masking with prepulse co-location (separation). We have published this paradigm in our privous paper ([24])

Statistical analysis

We used student’s t-test to compare the startle activity, PPI and CT in patients and healthy controls. Spearman’s correlation was used to evaluate the correlation among symptoms, PPI and CT. In addition, a multiple linear regression analysis was conducted to investigate the association between childhood trauma and PPI. We used the Statistical Package of Social Sciences (SPSS, version 16.0) to conduct the statistical analyses.

Results

Demographics features and CT

This study included 56 patients with first-episode schizophrenia (22 males and 34 females) with an average age 25.9 ± 6.8 years (). The duration of untreated psychosis was 20.33 ± 18.14 months (1 to 60). Forty-nine healthy controls were recruited from the same geographical areas. The patients had higher score of SA than health controls (actual scores 6.47 vs 5.50, t = 2.729, p < 0.05). The patients had lower PSS PPI (both ISI = 120 ms, ISI = 60 ms) than healthy controls (t = − 3.089, − 4.196, p < 0.05, respectively). Demographic data and clinical features of the enrolled patients are summarized in Table 1.
Table 1

Demographic and clinical characteristics of schizophrenia patients and controls

Schizophrenia patients (N = 56)Controls (N = 49)X2/t P
Gender, M/F22/3425/241.4420.245
Age, years25.90 ± 6.8026.21 ± 3.90− 0.2740.785
Education, years13.18 ± 3.2414.12 ± 3.27−1.3720.173
DUP, months29.92 ± 29.63
Drug-naïve/ on medication24/32
Risperidone 10
Paliperidone 6
Olanzapine 7
Aripiprazole 6
Quetiapine 3
On medication>2w/<2w11/21
PANSS
 Total82.28 + 22.32
 Positive22.57 ± 7.17
 Negative19.25 ± 9.33
 General Psychopathology43.02 ± 5.57
Childhood trauma
 Total42.89 ± 11.6038.60 ± 8.861.9190.058
 Emotional abuse7.97 ± 3.227.00 ± 2.481.5890.116
 Physical abuse6.11 ± 2.156.26 ± 2.08− 0.3140.754
 Sexual abuse6.47 ± 2.135.50 ± 1.062.7290.008
 Emotional neglect12.83 ± 5.0410.97 ± 3.941.9100.060
 Physical neglect9.87 ± 3.168.86 ± 2.311.6790.097
PPI index
 Startle77.41 ± 36.8274.73 ± 30.330.3220.748
 PPI (ISI = 120 ms), %
  PSC PPI20.20 ± 25.8627.77 ± 20.31−1.3210.191
  PSS PPI21.06 ± 23.1337.82 ± 20.58−3.0890.003
 PPI (ISI = 60 ms), %
  PSC PPI19.98 ± 19.6028.45 ± 18.57−1.7480.086
  PSS PPI21.03 ± 17.6641.07 ± 19.56−4.1960.000

DUP duration of untreatment psychosis, PANSS Positive and Negative Syndrome Scale, PSC PPI perceived spatial co-location PPI, PSS PPI perceived spatial separation

Demographic and clinical characteristics of schizophrenia patients and controls DUP duration of untreatment psychosis, PANSS Positive and Negative Syndrome Scale, PSC PPI perceived spatial co-location PPI, PSS PPI perceived spatial separation

Correlations among CT, sensory gating and symptoms

There were no significant correlation among CT, PPI and symptoms after the multiple comparison correction (Table 2). Furthermore, we did not observe significant associations between CT and PPI after the multiple comparison correction (Table 3).
Table 2

The relationship among childhood trauma, PPI, and symptoms of schizophrenia

PositiveNegativeGeneral PsychopathologyPANSS Total
Childhood trauma
 Emotional abuse0.0020.060−0.126−0.038
 Physical abuse0.3170.1430.1860.312
 Sexual abuse−0.0380.1980.1240.149
 Emotional neglect0.456 (0.005)0.075−0.2590.131
 Physical neglect0.2840.399 (0.018)0.0710.455 (0.008)
 Total score0.366 (0.036)0.185−0.1320.220
PPI index
 Startle−0.113−0.340− 0.011−0.210
 PSC PPI120−0.373−0.185− 0.131−0.240
 PSS PPI120−0.466 (0.004)−0.231− 0.302−0.403
 PSC PPI60−0.216−0.191− 0.136−0.223
 PSS PPI60−0.290−0.322− 0.207−0.369

PSC PPI perceived spatial co-location PPI, PSS PPI perceived spatial separation, PPI prepulse inhibition

Table 3

The relationship between the specific of CT and PPI in first-episode schizophrenia

StartlePSC PPI120PSS PPI120PSC PPI60PSS PPI60
Emotional abuse0.194−0.268− 0.139−0.591 (0.006)−0.236
Physical abuse−0.1190.024−0.507 (0.019)−0.146− 0.206
Sexual abuse−0.0360.021−0.289− 0.239−0.354
Emotional neglect−0.287−0.064− 0.203−0.370− 0.193
Physical neglect0.016−0.053−0.258− 0.338−0.371
Total score−0.112−0.095− 0.378−0.495 (0.026)− 0.394

PSC PPI perceived spatial co-location PPI, PSS PPI perceived spatial separation PPI, CT childhood trauma, PPI prepulse inhibition

The relationship among childhood trauma, PPI, and symptoms of schizophrenia PSC PPI perceived spatial co-location PPI, PSS PPI perceived spatial separation, PPI prepulse inhibition The relationship between the specific of CT and PPI in first-episode schizophrenia PSC PPI perceived spatial co-location PPI, PSS PPI perceived spatial separation PPI, CT childhood trauma, PPI prepulse inhibition

Regression analyses for CT subtypes, demographic features and PSS PPI

The multiple linear regression analyses showed that total score of CTQ-SF was negatively correlated with PSS PPI (ISI = 120 ms) (p = 0.018) (Table 4). We did not identify any type of trauma significantly correlated with either PSC PPI or PSS PPI (ISI = 60 ms) (data not shown).
Table 4

Multiple linear regression analyzing the impact of demographics, childhood trauma on PSS PPI (ISI = 120 ms)

PPI subscaleOdds ratio95% CI p
PSS PPI
 Constant71.1083.660~ 70.8140.011
  Childhood trauma−1.542−2.775~ − 0.3090.018
  DUP0.4310.021~ 0.8400.041

R2 = 0.531, Adjusted R2 = 0.452, F = 6.784, P = 0.011

DUP the duration of untreatment psychosis, Dependent variables: continuous and normally distributed: Independent variables: Categorical variable: sex: 1. male 2. female; Smoke history: 1.No 2.Yes; the rest of variable are continuous: age, dup, education years; PSS PPI perceived spatial separation prepulse inhibition;

Multiple linear regression analyzing the impact of demographics, childhood trauma on PSS PPI (ISI = 120 ms) R2 = 0.531, Adjusted R2 = 0.452, F = 6.784, P = 0.011 DUP the duration of untreatment psychosis, Dependent variables: continuous and normally distributed: Independent variables: Categorical variable: sex: 1. male 2. female; Smoke history: 1.No 2.Yes; the rest of variable are continuous: age, dup, education years; PSS PPI perceived spatial separation prepulse inhibition;

Discussion

We examined the effect of CT on PPI in patients with first-episode schizophrenia (course of illness was less than 60 months). Overall, the patients had significantly higher score on SA and had more PPI deficit than healthy controls. More importantly, we found that CT was negatively correlated with PPI in the regression analysis. CT has been demonstrated to have an impact on adult mental health, and exposure to early trauma has been linked to many psychopathologies, including schizophrenia [4]. In the current study, we found that patients with first-episode schizophrenia experienced higher level of SA. A number of studies in a range of samples attest to a link between childhood SA and psychosis, and SA before the age of 16 was strongly associated with schizophrenia, particularly if it involved non-consensual sexual intercourse [25]. A possible mechanism may be demonstrated via a neurodevelopmental model. Effects of SA on neurodevelopmental growth of the individual may give rise to neurocognitive deficits, further leading to the occurrence of schizophrenia [26]; We also found the patients had more severe PPI deficit than healthy controls, which is consistent with findings of other studies [7, 9, 27]. In the current study, we observed a negative correlation between CTQ-SF total and PSS PPI in patients. Evidence from animal studies may shed some light on the mechanism of exposure to traumatizing experiences on startle response and psychotic symptoms. One study, based on an experimental animal model, found that early life adversity during puberty was associated with increased risk for mental illness through sensory gating deficits [16]. Other study found that social isolation tend to have effects on PPI in rats [28]. Moreover, CT was associated with increased startle response in human [29]. Our findings showed that CT was indeed associated with sensory gating in first-episode schizophrenia, which attributed to the impact of early life adversity on neurodevelopment [26]. CT in humans shares some similarities with the socially isolated rat. At the behavioral level, social isolation induces hyperlocomotion, and dysfunctions in conditioned learning, reversal learning, and memory. [30]. At the endophenotype level, social isolation induces abnormalities in startle reflex and PPI. Moreover, social isolation causes changes of neurotransmitters, such as the increase of dopamine in the nucleus accumbens, the amygdala and other brain regions in the limbic system, the decrease of dopamine in medial prefrontal cortex, the decrease of 5-HT in the nucleus accumbens and the hippocampus, and changes of glutamine in the prefrontal cortex [30]. The proposed traumagenic neurodevelopmental model of schizophrenia shares similarities between the impact of CT on the brain development and the neurological abnormalities found in schizophrenia [26]. And, PPI is an important index which can reflect sensory gating function and the neurodevelopment [7]. So, we speculated that CT in human may be the risk factors to the occurrence of schizophrenia through its effects on sensory gating, and CT could cause a gene-environment interaction that result in the expression of schizophrenic symptoms. This study has a few limitations: (1) The current study was a case-control study, a follow up study may be needed in the future to test the effect of CT on the development of sensory gating. (2). Psychotropic drugs with sedative effect have effects on PPI. In this study, 32 patients have taken drugs, which may have some influence on the results. (3). CT is deeply associated with both child factor and parental factor (for example parents’ neurodevelopmental disorder or psychiatric disease). Furthermore, it is suggested that subjects with sub-clinical autistic traits might have impaired sensory gating from birth. Unfortunately, we have not collected the information about developmental course, thus the possibilities that schizophrenic patients might have comorbid developmental disorders (especially ASD), which lead to impaired sensory gating observed in patients group.

Conclusion

The patients with first-episode schizophrenia experienced a higher level of SA and deficit of sensory gating. Furthermore CT have effects on sensory gating, which may be contribute to the onset of schizophrenia.
  26 in total

1.  The environment and schizophrenia.

Authors:  Jim van Os; Gunter Kenis; Bart P F Rutten
Journal:  Nature       Date:  2010-11-11       Impact factor: 49.962

2.  Impaired prepulse inhibition of acoustic startle in schizophrenia.

Authors:  A Parwani; E J Duncan; E Bartlett; S H Madonick; T R Efferen; R Rajan; M Sanfilipo; P B Chappell; S Chakravorty; S Gonzenbach; G N Ko; J P Rotrosen
Journal:  Biol Psychiatry       Date:  2000-04-01       Impact factor: 13.382

3.  Sensory gating event-related potentials and oscillations in schizophrenia patients and their unaffected relatives.

Authors:  Mei-Hua Hall; Grantley Taylor; Dean F Salisbury; Deborah L Levy
Journal:  Schizophr Bull       Date:  2010-04-02       Impact factor: 9.306

4.  Impact of childhood trauma on sensorimotor gating in Chinese patients with chronic schizophrenia.

Authors:  Xianbin Li; Qing Tian; Qijing Bo; Guangping Zhang; Wei Zheng; Yujie Wen; Yilang Tang; Chuanyue Wang
Journal:  Psychiatry Res       Date:  2018-01-31       Impact factor: 3.222

5.  Stress in puberty unmasks latent neuropathological consequences of prenatal immune activation in mice.

Authors:  Sandra Giovanoli; Harald Engler; Andrea Engler; Juliet Richetto; Mareike Voget; Roman Willi; Christine Winter; Marco A Riva; Preben B Mortensen; Joram Feldon; Manfred Schedlowski; Urs Meyer
Journal:  Science       Date:  2013-03-01       Impact factor: 47.728

6.  Prepulse inhibition of acoustic startle in subjects with schizophrenia treated with olanzapine or haloperidol.

Authors:  Erica Duncan; Sandor Szilagyi; Marion Schwartz; Alena Kunzova; Shobhit Negi; Toby Efferen; Eric Peselow; Subhajit Chakravorty; Myrsini Stephanides; James Harmon; Dragana Bugarski-Kirola; Stephen Gonzenbach; John Rotrosen
Journal:  Psychiatry Res       Date:  2003-08-30       Impact factor: 3.222

7.  The Relationship of Common Risk Variants and Polygenic Risk for Schizophrenia to Sensorimotor Gating.

Authors:  Panos Roussos; Stella G Giakoumaki; Chrysoula Zouraraki; John F Fullard; Vasiliki-Eirini Karagiorga; Eva-Maria Tsapakis; Zoe Petraki; Larry J Siever; Todd Lencz; Anil Malhotra; Cleanthe Spanaki; Panos Bitsios
Journal:  Biol Psychiatry       Date:  2015-06-27       Impact factor: 13.382

Review 8.  Top-down modulation of prepulse inhibition of the startle reflex in humans and rats.

Authors:  Liang Li; Yi Du; Nanxin Li; Xihong Wu; Yanhong Wu
Journal:  Neurosci Biobehav Rev       Date:  2009-02-11       Impact factor: 8.989

9.  Deficits of perceived spatial separation induced prepulse inhibition in patients with schizophrenia: relationships to symptoms and neurocognition.

Authors:  Ning-Bo Yang; Qing Tian; Yu Fan; Qi-Jing Bo; Liang Zhang; Liang Li; Chuan-Yue Wang
Journal:  BMC Psychiatry       Date:  2017-04-11       Impact factor: 3.630

Review 10.  Schizophrenia.

Authors:  Michael J Owen; Akira Sawa; Preben B Mortensen
Journal:  Lancet       Date:  2016-01-15       Impact factor: 79.321

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Journal:  Schizophr Bull       Date:  2020-12-01       Impact factor: 9.306

2.  Detection of Schizophrenia Cases From Healthy Controls With Combination of Neurocognitive and Electrophysiological Features.

Authors:  Qing Tian; Ning-Bo Yang; Yu Fan; Fang Dong; Qi-Jing Bo; Fu-Chun Zhou; Ji-Cong Zhang; Liang Li; Guang-Zhong Yin; Chuan-Yue Wang; Ming Fan
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