3,4-Diaminopyridine (or 3,4-DAP) is an organic compound with the formula C₅H₃N(NH₂)₂. It is formally derived from pyridine by substitution of the 3 and 4 positions with an amino group.

With the International Nonproprietary Name amifampridine, it is used as a drug, predominantly in the treatment of a number of rare muscle diseases. In Europe, the phosphate salt of amifampridine has been licenced as Firdapse (BioMarin Pharmaceutical) in 2010 as an orphan drug.^[3]

Uses[edit]

3,4-Diaminopyridine is used for the treatment of Lambert-Eaton myasthenic syndrome (LEMS). In Lambert-Eaton syndrome, acetylcholine release is inhibited as antibodies meant to target characteristic cancers target Ca²⁺ channels on the prejunctional membrane instead. 3,4-Diaminopyridine works by blocking potassium channel efflux in nerve terminals so that action potential duration is increased. Ca²⁺ channels can then be open for a longer time and allow greater acetylcholine release to stimulate muscle at the end plate. A 2005 systematic review from the Cochrane Collaboration found some data favouring its use in LEMS.^[4]

It is also used to treat many of the congenital myasthenic syndromes, particularly those with defects in choline acetyltransferase, downstream kinase 7, and those where any kind of defect causes "fast channel" behaviour of the acetylcholine receptor.^[5]

3,4-Diaminopyridine has also been proposed for the treatment of multiple sclerosis, but a 2002 systematic review found that there was little unbiased data to support its use in MS.^[6]

Cost[edit]

The licensing of 3,4-diaminopyridine in 2010 led to a sharp increase in price for the drug. In some cases, this has led to hospitals using an unlicenced form rather than the licensed agent, as the price difference proved prohibitive. The drug company has been criticised for licencing the drug on the basis of previously conducted research, and yet charging exorbitantly for it.^[7] A group of UK neurologists and pediatricians have petitioned to prime minister David Cameron in an open letter to review the situation.^[8] The company has responded that it submitted the licensing request at the suggestion of the French government, and points out that the increased cost of a licensed drug also means that it is monitored by regulatory authorities (e.g. for uncommon side-effects), a process that was previously not present.^[9] In 2010, company scientists published evidence that amifampridine should be the first-line treatment for LEMS.^[10]

3,4-DAP has been provided free of charge for in excess of 12 years by Jacobus Pharmaceutical of New Jersey through Orphan Drug Status which requires careful monitoring by the prescribing physician. Jacobus is involved in clinical trials to receive FDA approval before the company mentioned above (Biomarin) which has charged exorbitant amounts for its version of 3,4-DAP (Firdapse) which, if it differs at all from the Jacobus DAP, only differs in adding a stability component. Anyone considering participating in a clinical trial for Biomarin (now out-licensed to Catalyst Pharmaceutical Partners, Inc. in the US) should review materials about Biomarin's pricing in the global market and Jacobus' past generous behavior before deciding to join the Biomarin clinical trials rather than the Jacobus ones.

See also[edit]

• 4-Aminopyridine

References[edit]