Skip to content

Next-Generation Pharmacotherapy for Depressive Disorders: From Novel Compounds to Optimized Use of Available Drugs.

Fan Bu, Lan Qin, Zhengchi Lou, Yanfang Xie, Shaojian Zhang, Lile Xiong, Yi Wen

Drug design, development and therapy January 1, 2026 Peer reviewed DOI: 10.2147/dddt.s609327 via PubMed

Summary

Depressive disorders, particularly treatment-resistant depression (TRD) and bipolar depression, often do not respond to existing antidepressants. This review highlights new pharmacotherapy options such as NMDA receptor modulators, neuroactive steroid therapies like brexanolone and zuranolone, and psychedelic-assisted treatments. It emphasizes the importance of optimizing existing treatments through strategies like drug repurposing and personalized medication management to enhance outcomes for diverse patient populations.

Study at a glance

Design narrative review
Population patients with depressive disorders, including treatment-resistant depression and bipolar depression
Key finding Progress in depression pharmacotherapy relies on both developing new drugs and improving the use of existing treatments.

Abstract

Depressive disorders remain a major source of disability worldwide, and many patients do not achieve sustained remission despite the availability of multiple antidepressant options. Unmet needs are particularly evident in treatment-resistant depression (TRD) and bipolar depression, where delayed onset of action, incomplete response, relapse, residual functional impairment, and tolerability limitations reduce the practical value of conventional monoaminergic strategies. This clinically oriented narrative review examines next-generation pharmacotherapy for depressive disorders from a drug-centered and mechanism-informed perspective. A targeted literature search was conducted across major biomedical and psychological databases and was supplemented by regulatory documents, prescribing information, pharmacogenomic recommendations, and selected real-world evidence. Representative next-generation approaches include N-methyl-D-aspartate (NMDA) receptor modulators and other rapid-acting agents, dextromethorphan-bupropion, multimodal antidepressants, neuroactive steroid-related therapies such as brexanolone and zuranolone, psychedelic-assisted pharmacotherapy, kappa-opioid receptor antagonists, and bipolar-relevant mood-stabilizing pharmacotherapies. The review also discusses mechanism-informed optimization of available drugs, including repurposing, augmentation, rational combination pharmacotherapy, dose and sequencing strategies, maintenance-oriented prescribing, and measurement-based care. Pharmacogenomics, pharmacokinetic/pharmacodynamic variability, and clinical stratification are considered as practical components of precision pharmacotherapy. Current evidence suggests that progress in depression pharmacotherapy depends not only on developing new compounds, but also on improving treatment selection, sequencing, monitoring, tolerability management, and sustained use in heterogeneous clinical populations. A next-generation framework should therefore integrate novel drug classes with improved use of established agents, while remaining sensitive to differences among unipolar depression, bipolar depression, and TRD.

Tags

Comments

No comments yet.

Log in to comment