Fosamax (alendronate sodium)

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FOSAMAX
Fosamax prescription drug, tablet form
Formula:	C4H13NO7P2
Molar Mass:	249.097 g/mol
INN:	Alendrotnic Acid
USAN:	Alendronate sodium
IUPAC:	4-amino-1-hydroxybutylidene) bisphosphonic acid monosodium salt trihydrate

Fosamax (Alendronate Sodium or Alendronic Acid) is a pharmaceutical drug administered to prevent and treat osteodegenerative diseases such as Osteoporosis. Functioning as a nitrogen-containing, second generation bisphosphonate, Fosamax binds to hydroxyapatite in bone and promotes apoptosis in osteoclasts (cells specialized in skeletal breakdown), thereby delaying the degradation of bone tissue. While incorporated in bone matrix, alendronate is not pharmacologically active, thus, it must be continuously administered to suppress osteoclasts on newly formed resorption surfaces ^[1].

Contents 1 History 2 Structural Highlights [2] 3 Function 4 Mechanism 5 Side Effects [6] 6 References 7 Contributors and Editors

History

Fosamax has been in use since September 29,1995 after gaining Food and Drug Administraion (FDA) approval. The drug obtained FDA clearance based on data from five clinical trials, lasting two years, involving 1,827 postmenopausal women with osteoporosis in 16 different countries. The trials showed a significant increase in bone mineral density at the spine, hip, and other sites. Overall, the drug reduced the number of women with new spinal fractures by 48%, the total number of new spinal fractures by 63%, and reduced overall height loss by 35%. Today, the drug remains in circulation in caplet and liquid forms and attainable at most pharmaceutical distribution centers with eligible prescription.

Structural Highlights ^[2]

spinqualitylabelsall models Crystal Structure of human FPPS in complex with pamidronate Show:Asymmetric Unit Biological Assembly Drag the structure with the mouse to rotate   Export Animated Image Structure of Fosamax As a bisphosphonate, Fosamax is a synthetic analog of pyrophosphate, containing two protonated phosphorus oxyanions. Each oxyanion is attached to a hydroxyl group, and at least one hydroxyl group is bounded to sodium. When exposed to solution, Fosamax may form ionic bond(s) with other metal cations such as magnesium. The central carbon is also attached to a hydroxyl group as well as a three-carbon chain leading up to an amino group.

Function

Functioning as a nitrogen-containing, second generation bisphosphonate, Fosamax binds to hydroxyapatite in bone and promotes apoptosis in osteoclasts (cells specialized in skeletal breakdown), thereby slowing the degradation of bone tissue^[3]. Furthermore, alendronic acid binds to and inhibits the activity of farnesyl pyrophosphate synthase, an enzyme catalyzes a step in a biochemical pathway essential for homeostatic regulation of osteoclastic activity.

Mechanism

Fosamax inhibits farnesyl pyrophosphate synthase (FPS or FPPS), one of the enzymes found in the mevalonic acid pathway, which produces isoprenoid compounds that are essential for post-translational modification of small guanosine triphosphate (GTP)-binding proteins, such as Rho, Ras, and Rab. Inhibition of this process interferes with osteoclast function and survival ^[4]. The net negative charge of alendronic acid is thought to bind to three aspartate residues while also forming electrostatic interactions with Magnesium cofactors, binding in competition with other aminobisphosphates such as pamidronate and risedronate. ^[5].

Side Effects ^[6]

Common side effects of Fosamax include gas, constipation, heartburn, diarrhea, bloating, nausea, vomiting, stomach pain, joint pain or swelling, swelling in your hands or feet, dizziness, headache, eye pain, back pain, or weakness. Serious side effects of Fosamax include severe pain (joints, bone, muscle, jaw, back or heartburn), chest pain, difficulty swallowing, bloody stools, eye pain, skin blisters, and swelling of the face, tongue, or throat.

References

1. ↑ Fosamax: Uses, Dosage & Side Effects - Drugs.com. (2016, November 3).Fosamax: Uses, Dosage & Side Effects - Drugs.com. Retrieved November 14, 2016, from https://www.drugs.com/fosamax.html
2. ↑ Protein Data Bank in Europe: Bringing Structure to Biology, from http://www.ebi.ac.uk/pdbe/entry/pdb/2F89
3. ↑ Drake, Matthew T., Bart L. Clarke, and Sundeep Khosla. "Bisphosphonates: Mechanism of Action and Role in Clinical Practice." Mayo Clinic Proceedings 83, no. 9 (2008): 1032-045. doi:10.4065/83.9.1032.
4. ↑ Alendronic acid. (2005, June 13), from http://www.drugbank.ca/drugs/DB00630#bond-15126
5. ↑ http://www.pnas.org/content/96/1/133.full.pdf
6. ↑ Common Side Effects of Fosamax (Alendronate Sodium) Drug Center - RxList. (2015, August 26). RxList. Retrieved November 14, 2016, from http://www.rxlist.com/fosamax-side-effects-drug-center.htm

Contributors and Editors

Floro, Alyssa Jewel D. Kidd, Justin M. Samady, Osna M.</font>