Data-driven biological subtypes of depression: systematic review of biological approaches to depression subtyping

亚型 重性抑郁障碍 荟萃分析 萧条(经济学) 心理信息 临床心理学 人口 非典型忧郁症 生物标志物 梅德林 心理学 生物信息学 医学 生物 内科学 遗传学 心情 程序设计语言 经济 宏观经济学 环境卫生 生物化学 计算机科学
作者
Lian Beijers,Klaas J. Wardenaar,Hanna M. van Loo,Robert A. Schoevers
出处
期刊:Molecular Psychiatry [Springer Nature]
卷期号:24 (6): 888-900 被引量:221
标识
DOI:10.1038/s41380-019-0385-5
摘要

Research into major depressive disorder (MDD) is complicated by population heterogeneity, which has motivated the search for more homogeneous subtypes through data-driven computational methods to identify patterns in data. In addition, data on biological differences could play an important role in identifying clinically useful subtypes. This systematic review aimed to summarize evidence for biological subtypes of MDD from data-driven studies. We undertook a systematic literature search of PubMed, PsycINFO, and Embase (December 2018). We included studies that identified (1) data-driven subtypes of MDD based on biological variables, or (2) data-driven subtypes based on clinical features (e.g., symptom patterns) and validated these with biological variables post-hoc. Twenty-nine publications including 24 separate analyses in 20 unique samples were identified, including a total of ~ 4000 subjects. Five out of six biochemical studies indicated that there might be depression subtypes with and without disturbed neurotransmitter levels, and one indicated there might be an inflammatory subtype. Seven symptom-based studies identified subtypes, which were mainly determined by severity and by weight gain vs. loss. Two studies compared subtypes based on medication response. These symptom-based subtypes were associated with differences in biomarker profiles and functional connectivity, but results have not sufficiently been replicated. Four out of five neuroimaging studies found evidence for groups with structural and connectivity differences, but results were inconsistent. The single genetic study found a subtype with a distinct pattern of SNPs, but this subtype has not been replicated in an independent test sample. One study combining all aforementioned types of data discovered a subtypes with different levels of functional connectivity, childhood abuse, and treatment response, but the sample size was small. Although the reviewed work provides many leads for future research, the methodological differences across studies and lack of replication preclude definitive conclusions about the existence of clinically useful and generalizable biological subtypes.
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