Justus Liebig University Giessen and Philipps University Marburg, Center for Mind, Brain and Behavior (CMBB), Giessen and Marburg, Germany
Department of Psychotherapy and Psychosomatics, Justus Liebig University Giessen, Giessen, Germany.
BMJ Open. 2020 Dec 17;10(12):e040123. doi: 10.1136/bmjopen-2020-040123.
Success rates of psychotherapy in post-traumatic stress disorder related to childhood maltreatment (PTSD-CM) are limited.
Observer-blind multicentre randomised clinical trial (A-1) of 4-year duration comparing enhanced methods of STAIR Narrative Therapy (SNT) and of trauma-focused psychodynamic therapy (TF-PDT) each of up to 24 sessions with each other and a minimal attention waiting list in PTSD-CM. Primary outcome is severity of PTSD (Clinician-Administered PTSD Scale for DSM-5 total) assessed by masked raters. For SNT and TF-PDT, both superiority and non-inferiority will be tested. Intention-to-treat analysis (primary) and per-protocol analysis (secondary). Assessments at baseline, after 10 sessions, post-therapy/waiting period and at 6 and 12 months of follow-up. Adult patients of all sexes between 18 and 65 years with PTSD-CM will be included. Continuing stable medication is permitted. To be excluded: psychotic disorders, risk of suicide, ongoing abuse, acute substance related disorder, borderline personality disorder, dissociative identity disorder, organic mental disorder, severe medical conditions and concurrent psychotherapy. To be assessed for eligibility: n=600 patients, to be e randomly allocated to the study conditions: n=328. Data management, randomisation and monitoring will be performed by an independent European Clinical Research Infrastructure Network (ECRIN)-certified data coordinating centre for clinical trials (KKS Marburg). Report of AEs to a data monitoring and safety board. Complementing study A-1, four inter-related add-on projects, including subsamples of the treatment study A-1, will examine (1) treatment integrity (adherence and competence) and moderators and mediators of outcome (B-1); (2) biological parameters (B-2, eg, DNA damage, reactive oxygen species and telomere shortening); (3) structural and functional neural changes by neuroimaging (B-3) and (4) cost-effectiveness of the treatments (B-4, costs and utilities).
Approval by the institutional review board of the University of Giessen (AZ 168/19). Following the Consolidated Standards of Reporting Trials statement for non-pharmacological trials, results will be reported in peer-reviewed scientific journals and disseminated to patient organisations and media.
DRKS 00021142.
针对与儿童期虐待相关的创伤后应激障碍(PTSD-CM)的心理治疗成功率有限。
一项为期 4 年的、观察者盲法、多中心随机临床试验(A-1),比较了强化 STAIR 叙事治疗(SNT)和创伤聚焦心理动力学治疗(TF-PDT)的疗效,每组治疗均不超过 24 次,同时与最小关注的等待名单进行比较。主要结局是通过盲法评估者评估 PTSD 的严重程度(DSM-5 总临床医生管理 PTSD 量表)。对于 SNT 和 TF-PDT,均将进行优势和非劣效性检验。意向治疗分析(主要)和符合方案分析(次要)。在基线、10 次治疗后、治疗后/等待期以及 6 个月和 12 个月随访时进行评估。纳入患有 PTSD-CM 的所有性别为 18 至 65 岁的成年患者。允许继续稳定用药。排除标准:精神病性障碍、自杀风险、持续虐待、急性物质相关障碍、边缘型人格障碍、分离性身份障碍、器质性精神障碍、严重的医疗状况和同时进行的心理治疗。将对 600 名符合条件的患者进行评估,以随机分配至研究条件:n=328。数据管理、随机化和监测将由欧洲临床研究基础设施网络(ECRIN)认证的临床试验数据协调中心(KKS Marburg)执行。不良事件报告给数据监测和安全委员会。补充研究 A-1,包括治疗研究 A-1 的子样本,将进行四项相互关联的附加项目,以检查(1)治疗完整性(依从性和能力)以及结局的调节剂和介质(B-1);(2)生物参数(B-2,例如 DNA 损伤、活性氧和端粒缩短);(3)神经影像学的结构和功能神经变化(B-3);(4)治疗的成本效益(B-4,成本和效用)。
经吉森大学机构审查委员会批准(AZ 168/19)。根据非药物试验的统一报告标准声明,结果将在同行评议的科学期刊上报告,并传播给患者组织和媒体。
DRKS 00021142。
