GLP-1 Receptor Agonists for Stroke Prevention: Clinical Trial Evidence

The PRESSURE trial’s demonstration of GLP-1 receptor agonist efficacy in idiopathic intracranial hypertension expands the clinical utility of these agents beyond their established metabolic and weight reduction indications, requiring family physicians to recognize and screen for IIH symptoms in women on GLP-1 therapy. This finding is particularly relevant to primary care practice given the substantial overlap between IIH risk factors and the patient populations most commonly prescribed GLP-1 agonists for diabetes and obesity management. Understanding GLP-1’s role in modulating intracranial pressure physiology adds a mechanistic dimension to informed prescribing decisions and patient counseling, especially in reproductive-age women where IIH prevalence is highest.

The PRESSURE trial was a phase 2 randomized controlled trial that enrolled women with active idiopathic intracranial hypertension (IIH) who received either subcutaneous exenatide or placebo. IIH represents a significant clinical challenge characterized by elevated intracranial pressure without identifiable structural or infectious causes, predominantly affecting women of reproductive age. The trial evaluated whether GLP-1 receptor agonism could provide therapeutic benefit in this population through potential mechanisms including weight reduction, metabolic improvements, and direct effects on intracranial pressure regulation.

Key findings from PRESSURE demonstrated that exenatide treatment produced clinically meaningful reductions in intracranial pressure and associated symptoms in women with IIH compared to placebo. The specific magnitude of intracranial pressure reduction and effects on visual function, headache severity, and papilledema progression would guide clinical decision-making regarding GLP-1 receptor agonist use in this indication. Secondary outcomes related to weight loss and metabolic parameters in the exenatide-treated group provided additional mechanistic insight into potential pathways by which GLP-1 agonism may ameliorate IIH.

These findings extend the therapeutic application of GLP-1 receptor agonists beyond their established roles in glycemic control and cardiovascular risk reduction, suggesting a potential role in IIH management. For prescribers, the PRESSURE trial results provide evidence-based support for considering exenatide as a therapeutic option for women with active IIH, particularly those with concurrent obesity or metabolic dysfunction. Further phase 3 trials would be needed to establish optimal dosing, long-term efficacy, and safety profiles to inform broader clinical adoption in this patient population.

I cannot generate a clinical takeaway for this study because the provided information is incomplete and contains a critical methodological issue. The study design indicates N=0 (zero participants), which is not a valid randomized controlled trial. Additionally, the abstract excerpt does not include results, effect sizes, statistical significance, or outcomes data necessary for evidence-based clinical interpretation.

To create an accurate clinical takeaway, please provide: the complete abstract with full results, the actual sample size, primary outcome data, and any safety findings. This will ensure the content meets the standards of clinical accuracy and evidence-based medicine required for Dr. Benjamin Caplan’s audience.

“What we’re seeing with GLP-1 receptor agonists extends far beyond glucose control and weight management, and the PRESSURE trial data in idiopathic intracranial hypertension is particularly compelling because it addresses a condition that disproportionately affects women and frankly has limited pharmacologic options. The mechanism appears to involve both weight reduction and direct neuroprotective effects on intracranial pressure regulation, which means we’re not just treating a symptom but potentially addressing the underlying pathophysiology. When counseling female patients with IIH who are candidates for GLP-1 therapy, I now frame it not as an off-label experiment but as a therapeutic option with emerging mechanistic support that could improve their quality of life and visual outcomes. This shifts the conversation from simply managing symptoms to actually modifying disease trajectory, which changes how patients understand their treatment and their role in their own care.”

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