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Ellenbroek, B.A. (1993) Treatment of schizophrenia: A clinical and preclinical evaluation of neuroleptic drugs. Pharmacology & Therapeutics, 57, 1-78.
- Listed: 2 June 2026 22 h 16 min
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Ellenbroek, B.A. (1993) Treatment of schizophrenia: A clinical and preclinical evaluation of neuroleptic drugs. Pharmacology & Therapeutics, 57, 1-78.
**Ellenbroek, B.A. (1993) Treatment of schizophrenia: A clinical and preclinical evaluation of neuroleptic drugs. Pharmacology & Therapeutics, 57, 1-78.**
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When the name *Ellenbroek* appears in the annals of psychiatric research, it signals a pivotal moment in the evolution of schizophrenia treatment. In 1993, B.A. Ellenbroek published a comprehensive review titled *“Treatment of schizophrenia: A clinical and preclinical evaluation of neuroleptic drugs”* in *Pharmacology & Therapeutics*. This landmark paper, spanning 78 pages, bridged the gap between laboratory discoveries and bedside practice, offering clinicians and researchers a clear roadmap for the next generation of antipsychotic medication.
### Why This Study Still Matters
Even three decades later, the core insights from Ellenbroek’s work remain relevant to mental health professionals, pharmacologists, and anyone interested in the science of **schizophrenia**. The article systematically compared first‑generation (typical) neuroleptics with emerging second‑generation (atypical) agents, dissecting their mechanisms of action, side‑effect profiles, and therapeutic efficacy. By integrating **clinical trials** with **preclinical animal models**, Ellenbroek provided a rare, holistic view of how neuroleptic drugs influence dopamine pathways, glutamate transmission, and neuroplasticity.
### Clinical Evaluation: From Hospital Wards to Real‑World Settings
Ellenbroek’s clinical section highlighted key trials that measured symptom reduction using the Positive and Negative Syndrome Scale (PANSS) and the Brief Psychiatric Rating Scale (BPRS). The review emphasized:
1. **Efficacy** – Typical neuroleptics like haloperidol showed robust control of positive symptoms (hallucinations, delusions) but fell short on negative symptoms (social withdrawal, flat affect).
2. **Safety** – Extrapyramidal side effects (EPS) and tardive dyskinesia were major concerns, prompting the search for drugs with a better tolerability profile.
3. **Patient adherence** – The paper argued that side‑effect burden directly impacts medication compliance, a critical factor in long‑term outcomes.
These findings helped shape prescribing guidelines that still influence today’s **antipsychotic medication** strategies.
### Preclinical Evaluation: The Lab Bench Perspective
On the preclinical front, Ellenbroek examined rodent and primate studies that explored drug binding affinities, receptor occupancy, and behavioral outcomes. Notably, the review underscored the importance of:
– **D2 receptor antagonism** as the cornerstone of antipsychotic action.
– **Serotonin 5‑HT2A antagonism** in newer agents, which appeared to mitigate EPS while improving mood and cognition.
– **Neuroprotective effects**, suggesting that some neuroleptics might modulate oxidative stress and neuroinflammation—areas that modern researchers are revisiting with renewed interest.
By correlating these laboratory results with clinical data, Ellenbroek demonstrated how **pharmacology** can predict real‑world drug performance, a principle that continues to guide **drug development** pipelines.
### The Legacy: From 1993 to Today
Fast forward to 2024, and the landscape of schizophrenia treatment has expanded to include **long‑acting injectable (LAI) antipsychotics**, **partial dopamine agonists**, and **glutamatergic modulators**. Yet, the framework Ellenbroek established—evaluating both clinical efficacy and preclinical mechanisms—remains the gold standard for assessing new therapies.
Researchers now build upon her methodology by incorporating **genomic biomarkers**, **neuroimaging**, and **digital phenotyping** to personalize treatment. The original quote, a citation in countless subsequent papers, serves as a reminder that rigorous, dual‑track evaluation is essential for advancing **mental health care**.
### Takeaway for Clinicians and Readers
– **Holistic assessment**: When choosing an antipsychotic, consider both symptom control and side‑effect burden.
– **Evidence‑based practice**: Trust studies that integrate clinical outcomes with preclinical insights, just as Ellenbroek did.
– **Future directions**: Stay informed about emerging neuroleptic agents that target novel pathways beyond dopamine.
In sum, Ellenbroek’s 1993 review is more than a historical reference; it is a living document that continues to inform **schizophrenia treatment**, inspire **pharmacological innovation**, and guide clinicians toward safer, more effective **neuroleptic drug** regimens. By revisiting this seminal work, we honor the past while charting a clearer, evidence‑driven future for patients living with schizophrenia.
—
*Keywords: schizophrenia treatment, neuroleptic drugs, antipsychotic medication, clinical evaluation, preclinical evaluation, dopamine antagonism, serotonin 5‑HT2A, side effects, patient adherence, mental health research, pharmacology, therapeutic strategies.*
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