Impact of pre-trauma recreational drug use on mental health outcomes among survivors of the Israeli Nova Festival terrorist attack

IF 73.3 1区 医学 Q1 Medicine World Psychiatry Pub Date : 2024-09-16 DOI:10.1002/wps.21254
Nitsa Nacasch, Tal Malka, Joseph Zohar, Yarden V. Dejorno, Gal Levi, Raz Gross, Mark Weiser, Hagit Cohen
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We hypothesized that the pre-trauma use of psychostimulants or hallucinogens would be significantly associated with the severity of peri-traumatic dissociation, anxiety, depression, and acute stress disorder (ASD) symptoms in survivors of the attack.</p>\n<p>Two hundred thirty-two survivors sought assistance at the Chaim Sheba Medical Center and underwent clinical evaluation. They were considered for this study if they had no severe physical injuries; no first-degree family member killed during the attack; and no history of mental disorders, including post-traumatic stress disorder (PTSD).</p>\n<p>Of the 232 survivors screened for the study, 126 met the above criteria and provided informed consent to participate. However, two of them who reported using hallucinogenic mushrooms, and one who reported using ketamine prior to the traumatic event, were excluded from the analysis, due to the small sample size for these drugs, leaving a sample of 123 participants. Their mean age (±SE) was 28.4±0.7 years; 75 of them (60.9%) were male; 68.9% were never married, and 68.2% were holding a high-school degree or equivalent.</p>\n<p>Seventy-one of them (57.7%) reported using psychoactive drugs at the festival – 12 only alcohol, nine only lysergic acid (LSD), seven only 3,4-methylenedioxymethamphetamine (MDMA), six only cannabis, three only methylmethcathinone (MMC), 15 various drug combinations including alcohol, and 19 various drug combinations excluding alcohol.</p>\n<p>All participants completed several questionnaires, assessing peri-traumatic dissociation (Peritraumatic Dissociative Experiences Questionnaire, PDEQ), post-traumatic anxiety (Generalized Anxiety Disorder-7, GAD-7; and Visual Analog Scale for Anxiety, VAS-A), depression (Patient Health Questionnaire-9, PHQ-9), and ASD symptoms (Posttraumatic Diagnostic Scale, PDS-5).</p>\n<p>Both the GAD-7 scores and the PDS-5 hyperarousal scores were significantly higher in the drug-user than in the drug-free group (p&lt;0.05 and p&lt;0.008, respectively). The scores of most participants were above the clinical threshold for these instruments (&gt;10 for GAD-7 in 70.4%, and &gt;28 for PDS-5 in 81.3% of the participants), indicating a very high level of anxiety- and hyperarousal-related symptoms in both groups. Both the PDEQ and PHQ-9 scores were higher in the drug-user than in the drug-free group, but the differences were not significant. No significant differences were found between the groups in the VAS-A, total PDS-5, and PDS-5 subscales. The VAS-A scores of 51.9% of the participants were higher than 6, which is the clinical threshold for this instrument.</p>\n<p>A multiple regression analysis was performed on the scores of the PDEQ, PHQ-9, GAD-7, PDS-5 (total and subscales), and VAS-A questionnaires, employing nine sets of independent variables related to drug use, gender and age (see supplementary information).</p>\n<p>The multiple regression model for the PDEQ scores was statistically significant (p=0.018). The severity of peri-traumatic dissociation was significantly correlated with alcohol consumption prior to the event (β=0.25, p&lt;0.008), but not with the consumption of any other drug. Consuming alcohol prior to the traumatic event, as compared with consuming other drugs, significantly increased the likelihood of experiencing peri-traumatic dissociation (PDEQ score = 24.8±2.0 vs. 19.3±1.0, p&lt;0.015).</p>\n<p>The model for the PHQ-9 scores was statistically significant (p=0.02). The severity of depressive symptoms was significantly correlated with alcohol consumption prior to the event (β=0.32, p&lt;0.001), but not with the consumption of any other drug. Consuming alcohol prior to the event, as compared with consuming other drugs, significantly increased the likelihood of depressive symptoms (PHQ-9 score = 18.7±1.8 vs. 13.8±0.6, p&lt;0.0015).</p>\n<p>The model for the GAD-7 scores was statistically significant (p=0.04). The severity of anxiety symptoms was significantly correlated with alcohol consumption prior to the event (β=0.29, p&lt;0.002). Consuming alcohol, as compared with consuming other drugs prior to the event, significantly increased the likelihood of anxiety (GAD-7 score = 16.3±1.0 vs. 12.7±0.6, p&lt;0.004). None of the other drugs consumed prior to the event significantly affected symptoms of anxiety.</p>\n<p>The model for the PDS-5 arousal-hyperactivity scores was statistically significant (p=0.03). The severity of arousal and hyperactivity symptoms was significantly correlated with alcohol (β=0.24, p&lt;0.011) and MMC (β=0.24, p&lt;0.011) consumption prior to the traumatic event. Both alcohol and MMC consumption significantly increased the likelihood of experiencing arousal and hyperactivity symptoms, as compared with the consumption of other drugs.</p>\n<p>The multiple regression analysis of the PDEQ dissociation score with VAS-A, GAD-7, PHQ-9, and PDS-5 subscale scores, including gender and age, was statistically significant (p=0.0001). Experiencing peri-traumatic dissociation was significantly correlated with the VAS-A score (β=0.31, p&lt;0.02) and with the PDS-5 mood score (β=0.28, p&lt;0.045).</p>\n<p>A mediation analysis showed that pre-trauma alcohol consumption positively predicted PDS-5 mood scores (β=0.15, p=0.03), PDS-5 arousal scores (β=0.16, p=0.015), PDS-5 intrusive scores (β=0.23, p=0.001), GAD-7 anxiety scores (β=0.20, p=0.0015), PHQ-9 depression scores (β=0.24, p=0.00025), and PDEQ peri-traumatic dissociation scores (β=0.20, p=0.01). With the introduction of the peri-traumatic dissociation variable into the model as a potential mediator, the association between alcohol consumption and PDS-5 mood, PDS-5 intrusive, GAD-7 anxiety and PHQ-9 depressive scores became less significant (p&lt;0.04, p&lt;0.015, p&lt;0.015 and p&lt;0.02, respectively). This finding suggests that peri-traumatic dissociation partially mediated the association between alcohol consumption and mood, intrusion, anxiety and depressive symptoms.</p>\n<p>So, in marked contrast to our expectations, we found that only pre-trauma alcohol consumption, with or without other drugs, significantly increased the risk of peri-traumatic dissociation, anxiety, depression, and ASD symptoms.</p>\n<p>Alcohol consumption exerts various effects on brain functions and behavior, ranging from anxiolytic and mild disinhibitory effects to sedation, motor incoordination, altered memory and emotional processing<span><sup>1, 2</sup></span>. Therefore, pre-trauma alcohol consumption may have interfered with the cognitive, emotional and physiological processes necessary to cope with the traumatic event. The previously available evidence on the effect of pre-trauma alcohol use on the development of post-traumatic symptomatology was mixed<span><sup>3-7</sup></span>.</p>\n<p>Importantly, the traumatic event was prolonged (participants had to run and hide for 8-20 hours until they were rescued). Therefore, the survivors may have experienced a hangover, which could have increased their anxiety and traumatic stress<span><sup>8</sup></span>.</p>\n<p>We also found that peri-traumatic dissociation significantly increased the likelihood of subsequent anxiety and mood symptoms in participants who consumed alcohol. Peri-traumatic dissociation can potentially disrupt the processing and integration of traumatic memories, which may impede recovery and increase the probability of developing post-traumatic disorders, because trauma-related memories persist in a fragmented and unprocessed state<span><sup>9</sup></span>.</p>\n<p>The Nova massacre provides a unique opportunity to study how pre-trauma drug consumption affects post-trauma mental health outcomes. Yet, our study is not devoid of limitations. First, as in all naturalistic studies, the sample size is constrained. Second, we relied only on the reports of the participants on their consumption of drugs, rather than on measurements of blood concentrations and data regarding the actual quantities of the consumed substances, which hampers a more nuanced understanding of the correlation between drug consumption and the observed outcomes.</p>\n<p>Nonetheless, this study presents novel insights into the relationship between pre-trauma alcohol consumption and increased vulnerability to peri-traumatic dissociation, anxiety, depression, and ASD symptoms. Given the widespread prevalence of alcohol consumption in social gatherings – and the increasing occurrence of sexual assaults, physical assaults and vehicular accidents – these findings can have a social and clinical interest. Moreover, since alcohol is a compound with a known pharmacology and mode of action, they can be relevant to the elucidation of the biology of response to traumatic experiences.</p>","PeriodicalId":23858,"journal":{"name":"World Psychiatry","volume":"36 1","pages":""},"PeriodicalIF":73.3000,"publicationDate":"2024-09-16","publicationTypes":"Journal Article","fieldsOfStudy":null,"isOpenAccess":false,"openAccessPdf":"","citationCount":"0","resultStr":null,"platform":"Semanticscholar","paperid":null,"PeriodicalName":"World Psychiatry","FirstCategoryId":"3","ListUrlMain":"https://doi.org/10.1002/wps.21254","RegionNum":1,"RegionCategory":"医学","ArticlePicture":[],"TitleCN":null,"AbstractTextCN":null,"PMCID":null,"EPubDate":"","PubModel":"","JCR":"Q1","JCRName":"Medicine","Score":null,"Total":0}
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Abstract

On October 7, 2023, about 4,000 civilians attending the Nova open-air music festival in southern Israel were the victims of a sudden terrorist attack. They had to swiftly react to the attack by running and hiding for extended periods of time to protect their lives.

At the time of the attack, a significant proportion of these people were under the influence of various recreational drugs. We hypothesized that the pre-trauma use of psychostimulants or hallucinogens would be significantly associated with the severity of peri-traumatic dissociation, anxiety, depression, and acute stress disorder (ASD) symptoms in survivors of the attack.

Two hundred thirty-two survivors sought assistance at the Chaim Sheba Medical Center and underwent clinical evaluation. They were considered for this study if they had no severe physical injuries; no first-degree family member killed during the attack; and no history of mental disorders, including post-traumatic stress disorder (PTSD).

Of the 232 survivors screened for the study, 126 met the above criteria and provided informed consent to participate. However, two of them who reported using hallucinogenic mushrooms, and one who reported using ketamine prior to the traumatic event, were excluded from the analysis, due to the small sample size for these drugs, leaving a sample of 123 participants. Their mean age (±SE) was 28.4±0.7 years; 75 of them (60.9%) were male; 68.9% were never married, and 68.2% were holding a high-school degree or equivalent.

Seventy-one of them (57.7%) reported using psychoactive drugs at the festival – 12 only alcohol, nine only lysergic acid (LSD), seven only 3,4-methylenedioxymethamphetamine (MDMA), six only cannabis, three only methylmethcathinone (MMC), 15 various drug combinations including alcohol, and 19 various drug combinations excluding alcohol.

All participants completed several questionnaires, assessing peri-traumatic dissociation (Peritraumatic Dissociative Experiences Questionnaire, PDEQ), post-traumatic anxiety (Generalized Anxiety Disorder-7, GAD-7; and Visual Analog Scale for Anxiety, VAS-A), depression (Patient Health Questionnaire-9, PHQ-9), and ASD symptoms (Posttraumatic Diagnostic Scale, PDS-5).

Both the GAD-7 scores and the PDS-5 hyperarousal scores were significantly higher in the drug-user than in the drug-free group (p<0.05 and p<0.008, respectively). The scores of most participants were above the clinical threshold for these instruments (>10 for GAD-7 in 70.4%, and >28 for PDS-5 in 81.3% of the participants), indicating a very high level of anxiety- and hyperarousal-related symptoms in both groups. Both the PDEQ and PHQ-9 scores were higher in the drug-user than in the drug-free group, but the differences were not significant. No significant differences were found between the groups in the VAS-A, total PDS-5, and PDS-5 subscales. The VAS-A scores of 51.9% of the participants were higher than 6, which is the clinical threshold for this instrument.

A multiple regression analysis was performed on the scores of the PDEQ, PHQ-9, GAD-7, PDS-5 (total and subscales), and VAS-A questionnaires, employing nine sets of independent variables related to drug use, gender and age (see supplementary information).

The multiple regression model for the PDEQ scores was statistically significant (p=0.018). The severity of peri-traumatic dissociation was significantly correlated with alcohol consumption prior to the event (β=0.25, p<0.008), but not with the consumption of any other drug. Consuming alcohol prior to the traumatic event, as compared with consuming other drugs, significantly increased the likelihood of experiencing peri-traumatic dissociation (PDEQ score = 24.8±2.0 vs. 19.3±1.0, p<0.015).

The model for the PHQ-9 scores was statistically significant (p=0.02). The severity of depressive symptoms was significantly correlated with alcohol consumption prior to the event (β=0.32, p<0.001), but not with the consumption of any other drug. Consuming alcohol prior to the event, as compared with consuming other drugs, significantly increased the likelihood of depressive symptoms (PHQ-9 score = 18.7±1.8 vs. 13.8±0.6, p<0.0015).

The model for the GAD-7 scores was statistically significant (p=0.04). The severity of anxiety symptoms was significantly correlated with alcohol consumption prior to the event (β=0.29, p<0.002). Consuming alcohol, as compared with consuming other drugs prior to the event, significantly increased the likelihood of anxiety (GAD-7 score = 16.3±1.0 vs. 12.7±0.6, p<0.004). None of the other drugs consumed prior to the event significantly affected symptoms of anxiety.

The model for the PDS-5 arousal-hyperactivity scores was statistically significant (p=0.03). The severity of arousal and hyperactivity symptoms was significantly correlated with alcohol (β=0.24, p<0.011) and MMC (β=0.24, p<0.011) consumption prior to the traumatic event. Both alcohol and MMC consumption significantly increased the likelihood of experiencing arousal and hyperactivity symptoms, as compared with the consumption of other drugs.

The multiple regression analysis of the PDEQ dissociation score with VAS-A, GAD-7, PHQ-9, and PDS-5 subscale scores, including gender and age, was statistically significant (p=0.0001). Experiencing peri-traumatic dissociation was significantly correlated with the VAS-A score (β=0.31, p<0.02) and with the PDS-5 mood score (β=0.28, p<0.045).

A mediation analysis showed that pre-trauma alcohol consumption positively predicted PDS-5 mood scores (β=0.15, p=0.03), PDS-5 arousal scores (β=0.16, p=0.015), PDS-5 intrusive scores (β=0.23, p=0.001), GAD-7 anxiety scores (β=0.20, p=0.0015), PHQ-9 depression scores (β=0.24, p=0.00025), and PDEQ peri-traumatic dissociation scores (β=0.20, p=0.01). With the introduction of the peri-traumatic dissociation variable into the model as a potential mediator, the association between alcohol consumption and PDS-5 mood, PDS-5 intrusive, GAD-7 anxiety and PHQ-9 depressive scores became less significant (p<0.04, p<0.015, p<0.015 and p<0.02, respectively). This finding suggests that peri-traumatic dissociation partially mediated the association between alcohol consumption and mood, intrusion, anxiety and depressive symptoms.

So, in marked contrast to our expectations, we found that only pre-trauma alcohol consumption, with or without other drugs, significantly increased the risk of peri-traumatic dissociation, anxiety, depression, and ASD symptoms.

Alcohol consumption exerts various effects on brain functions and behavior, ranging from anxiolytic and mild disinhibitory effects to sedation, motor incoordination, altered memory and emotional processing1, 2. Therefore, pre-trauma alcohol consumption may have interfered with the cognitive, emotional and physiological processes necessary to cope with the traumatic event. The previously available evidence on the effect of pre-trauma alcohol use on the development of post-traumatic symptomatology was mixed3-7.

Importantly, the traumatic event was prolonged (participants had to run and hide for 8-20 hours until they were rescued). Therefore, the survivors may have experienced a hangover, which could have increased their anxiety and traumatic stress8.

We also found that peri-traumatic dissociation significantly increased the likelihood of subsequent anxiety and mood symptoms in participants who consumed alcohol. Peri-traumatic dissociation can potentially disrupt the processing and integration of traumatic memories, which may impede recovery and increase the probability of developing post-traumatic disorders, because trauma-related memories persist in a fragmented and unprocessed state9.

The Nova massacre provides a unique opportunity to study how pre-trauma drug consumption affects post-trauma mental health outcomes. Yet, our study is not devoid of limitations. First, as in all naturalistic studies, the sample size is constrained. Second, we relied only on the reports of the participants on their consumption of drugs, rather than on measurements of blood concentrations and data regarding the actual quantities of the consumed substances, which hampers a more nuanced understanding of the correlation between drug consumption and the observed outcomes.

Nonetheless, this study presents novel insights into the relationship between pre-trauma alcohol consumption and increased vulnerability to peri-traumatic dissociation, anxiety, depression, and ASD symptoms. Given the widespread prevalence of alcohol consumption in social gatherings – and the increasing occurrence of sexual assaults, physical assaults and vehicular accidents – these findings can have a social and clinical interest. Moreover, since alcohol is a compound with a known pharmacology and mode of action, they can be relevant to the elucidation of the biology of response to traumatic experiences.

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以色列新星音乐节恐怖袭击幸存者创伤前使用娱乐性药物对心理健康结果的影响
2023 年 10 月 7 日,约 4000 名参加以色列南部诺瓦露天音乐节的平民成为一场突如其来的恐怖袭击的受害者。在袭击发生时,这些人中有相当一部分受到了各种娱乐性药物的影响。我们假设,创伤前使用精神兴奋剂或致幻剂与袭击幸存者创伤前分离、焦虑、抑郁和急性应激障碍(ASD)症状的严重程度有显著关联。在经过筛选的 232 名幸存者中,有 126 人符合上述标准,并在知情的情况下同意参与研究。然而,其中有两名幸存者表示在创伤事件发生前曾使用致幻蘑菇,一名幸存者表示在创伤事件发生前曾使用氯胺酮,由于这些药物的样本量较小,因此被排除在分析之外。他们的平均年龄(±SE)为 28.4±0.7 岁;其中 75 人(60.9%)为男性;68.9% 的人从未结过婚,68.2% 的人拥有高中或同等学历。他们中有 71 人(57.7%)称在音乐节上使用了精神药物--12 人只饮酒,9 人只服用麦角酸(LSD),7 人只服用 3,4-亚甲二氧基甲基苯丙胺(MDMA),6 人只服用大麻,3 人只服用甲卡西酮(MMC),15 人服用包括酒精在内的各种混合药物,19 人服用不包括酒精在内的各种混合药物。所有参与者都填写了几份问卷,评估创伤前分离体验(创伤前分离体验问卷,PDEQ)、创伤后焦虑(广泛性焦虑症-7,GAD-7;焦虑视觉模拟量表,VAS-A)、抑郁(患者健康问卷-9,PHQ-9)和 ASD 症状(创伤后诊断量表,PDS-5)。用药组的 GAD-7 评分和 PDS-5 过度焦虑评分均显著高于未用药组(分别为 p&lt;0.05 和 p&lt;0.008)。大多数参与者的得分都高于这些工具的临床阈值(70.4% 的参与者 GAD-7 得分为 10,81.3% 的参与者 PDS-5 得分为 28),这表明两组参与者的焦虑和过度焦虑相关症状都非常严重。吸毒者组的 PDEQ 和 PHQ-9 分数均高于未吸毒者组,但差异不显著。在 VAS-A、PDS-5 总分和 PDS-5 分量表方面,两组之间没有发现明显差异。51.9%的参与者的VAS-A得分高于6分,这是该工具的临床阈值。对PDEQ、PHQ-9、GAD-7、PDS-5(总分和分量表)和VAS-A问卷的得分进行了多元回归分析,采用了九组与吸毒、性别和年龄相关的自变量(见补充信息)。创伤前解离的严重程度与事件发生前的饮酒量有显著相关性(β=0.25,p&lt;0.008),但与其他任何药物的消费无关。与服用其他药物相比,在创伤事件发生前饮酒会明显增加创伤前解离的可能性(PDEQ 分数 = 24.8±2.0 vs. 19.3±1.0,p&lt;0.015)。PHQ-9 分数模型具有统计学意义(p=0.02)。抑郁症状的严重程度与事件发生前的饮酒量显著相关(β=0.32,p&lt;0.001),但与其他任何药物的摄入量无关。与服用其他药物相比,事件发生前饮酒会明显增加出现抑郁症状的可能性(PHQ-9 评分 = 18.7±1.8 vs. 13.8±0.6,p&lt;0.0015)。焦虑症状的严重程度与事件发生前的饮酒量明显相关(β=0.29,p&lt;0.002)。与活动前服用其他药物相比,活动前饮酒会明显增加焦虑的可能性(GAD-7 评分 = 16.3±1.0 vs. 12.7±0.6,p&lt;0.004)。事件发生前服用的其他药物均未对焦虑症状产生明显影响。PDS-5唤醒-过度活跃评分模型具有统计学意义(p=0.03)。唤醒和多动症状的严重程度与创伤事件前的酒精摄入量(β=0.24,p&lt;0.011)和 MMC 摄入量(β=0.24,p&lt;0.011)明显相关。
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来源期刊
World Psychiatry
World Psychiatry Nursing-Psychiatric Mental Health
CiteScore
64.10
自引率
7.40%
发文量
124
期刊介绍: World Psychiatry is the official journal of the World Psychiatric Association. It aims to disseminate information on significant clinical, service, and research developments in the mental health field. World Psychiatry is published three times per year and is sent free of charge to psychiatrists.The recipient psychiatrists' names and addresses are provided by WPA member societies and sections.The language used in the journal is designed to be understandable by the majority of mental health professionals worldwide.
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