Journal Article Summary
The article investigates the interactions between two specific enzymes, cytochrome P450 2B6 and 2B4, and the drug amlodipine. Understanding how these enzymes metabolize drugs is important because they play a crucial role in drug metabolism and can influence how effectively medications work in the body. The study aims to clarify how certain residues in the enzymes' substrate access channels affect their ability to process amlodipine, which could have implications for drug efficacy and safety.
The researchers used advanced absorbance spectroscopy to study how amlodipine binds to P450 2B4 and 2B6. They found that both enzymes can bind two molecules of amlodipine, indicating a complex interaction. Mutations in specific residues of the enzymes significantly affected their catalytic efficiency, suggesting that these residues are important for the enzymes' function. The study revealed that certain mutations led to a marked decrease in the enzymes' ability to metabolize typical substrates, highlighting the role of these residues in drug metabolism.
However, the study has limitations, including the focus on laboratory conditions that may not fully replicate the complexities of human metabolism. Additionally, the findings are based on specific mutations and may not encompass all variations in the enzymes. Patients and caregivers should discuss any concerns about drug interactions or metabolism with healthcare professionals, especially if they are taking medications that are metabolized by cytochrome P450 enzymes, as this can affect drug effectiveness and safety.
Medical Safety Note
This journal article summary is provided for educational purposes only and is not medical advice. Always consult a licensed healthcare professional before starting, stopping, or changing any medication.
Article Cited
- Jang Hyun-Hee, Davydov Dmitri R., Lee Ga-Young, Yun Chul-Ho, Halpert James R.. THE ROLE OF CYTOCHROME P450 2B6 AND 2B4 SUBSTRATE ACCESS CHANNEL RESIDUES PREDICTED BASED ON CRYSTAL STRUCTURES OF THE AMLODIPINE COMPLEXES†. Archives of biochemistry and biophysics 2014. DOI: 10.1016/j.abb.2014.01.008. PMID: 24445070. PMCID: PMC4030592.
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