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Home - Pharmacology - Observational Evidence Fills the Gaps in Cardio-Oncology Therapeutics

Pharmacology

Observational Evidence Fills the Gaps in Cardio-Oncology Therapeutics

Last updated: February 27, 2026 4:09 am
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Observational Evidence Fills the Gaps in Cardio-Oncology Therapeutics

A recent editorial in *Heart* underscores a critical evidence gap in the pharmacotherapy of acute myocardial infarction (AMI) for patients with active cancer. Historically, these patients have been excluded from the randomized clinical trials that established the safety and efficacy profiles of key antithrombotic drugs and revascularization strategies. This leaves clinicians with significant uncertainty regarding optimal drug dosing, the balance of bleeding risk versus ischemic benefit, and the management of complex drug–drug interactions common in this population. The article argues that high-quality observational studies are now essential to build the therapeutic framework for this growing patient group, who may represent up to 5% of AMI cases.

Why it might matter to you: This highlights a frontier in personalized medicine where standard pharmacokinetic and pharmacodynamic models may not apply, demanding a nuanced approach to therapeutic drug monitoring and dose-response. For pharmacologists, it identifies a pressing need to study drug metabolism and receptor binding in the context of cancer biology and its treatments to mitigate adverse drug reactions and toxicity. This work directly informs the design of future clinical trials aimed at establishing safe therapeutic windows for cardiovascular drugs in oncological patients.

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