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Ordeals, poisons, and a ‘punishment from God’: a short global history of rivastigmine and other dementia treatments

Pharmaceutical roots is a content series from LGC Mikromol investigating and outlining the natural origins of pharmaceutical substances, and offering a deeper dive into their uses, risks, and mechanisms of action.

 

We supply an ISO 17034-accredited API and several impurity products for rivastigmine and other acetylcholinase inhibitors. For more information, please scroll to the bottom of this article.

 

Although the history of dementia is “probably as old as mankind itself”, the condition has evolved to become a modern-day scourge. According to the World Health Organisation (WHO), around 55 million individuals across the planet have the illness, the world’s seventh most deadly disease. WHO adds that the global cost of direct and informal care for people with dementia is already around $1.3 trillion per year and - with the elderly population  increasing in nearly every country – it will require close to $3 trillion to look after an anticipated 78 million sufferers by 2030.

 

History

 

Even before it had a name, humans were familiar with dementia. As early as 2000 BC, the ancient Egyptians “were already aware that memory declines as people age.” Pythagoras (570-495 BC) classified human lifespans into six stages, identifying senescence (age 63-79) and old age (80-plus) as the phases when some could be expected to degenerate in mind. Hippocrates (460-347 BC) believed that cognitive disorder resulted from brain injury, whereas the Roman philosopher Cicero believed that dementia was not an inevitable consequence of ageing, but more a question of willpower. “Pugnandum, tamquam contra morbum sic contra senectutem", he wrote, meaning: “We have to fight against ageing, as we do against a disease”. The word ‘dementia’ also has its roots in Latin, and is a composite of ‘de’ (meaning a loss or deprivation), ‘ment’ (meaning ‘mind’) and ‘ia’ (indicating a condition).

After the fall of the Roman Empire, religious notions of sin and punishment meant senility was often regarded as a punishment from God. And it was only in the early 20th century, when scientific advances allowed us to look inside the brain, that doctors realised diseases could cause this mental deterioration. In 1906, German psychiatrist Dr Alois Alzheimer used a microscope to examine the brain of Auguste Deter, a 50-year-old woman who had died after experiencing dementia-like symptoms, and found microscopic plaques and tangles. These clumps and deposits, made from proteins later known as amyloid and tau, are now recognised as the hallmarks of Alzheimer’s disease and many other forms of dementia. In the present day, WHO defines dementia as “a syndrome – usually of a chronic or progressive nature – that leads to deterioration in cognitive function… beyond what might be expected from the usual consequences of biological ageing.” Consciousness is not affected, WHO says, adding that cognitive impairment is “commonly accompanied, and occasionally preceded, by changes in mood, emotional control, behaviour, or motivation.”

 

Rivastigmine and its relatives

 

Although there is currently no cure for dementia, a family of drugs called cholinesterase inhibitors (also called acetylcholinase inhibitors, or AChEs) can alleviate symptoms – particularly in the early stages of the disease. Rivastigmine, donepezil, galantamine, and physostigmine are all part of the AChE family that have been used to treat Alzheimer’s and other forms of dementia, although they also have a wide range of other uses – both therapeutic and malignant.

 

Hippomane-Mancinella

Physostigmine

Physostigmine is an alkaloid found naturally in both the Calabar bean (Physostigma venenosum) and the Manchineel Tree (Genus Hippomane) – a.k.a. “the most dangerous tree in the world .” The Caribbean Manchineel’s sweet-scented apple-like fruits have been blamed for “poisoning Spanish conquistadores, shipwrecked sailors, and present-day tourists” and its sap also used by Carib Indians to poison their arrows. Meanwhile, the similarly toxic Calabar bean was used in ancient Africa as an ordeal to prove or disprove a person’s guilt (if the accused vomited within half an hour, they were innocent, but if they perished they were guilty). Perhaps not surprisingly, physostigmine’s not inconsiderable side effects rendered it unsuitable for treating Alzheimer’s, although it is still widely prescribed as a treatment for glaucoma and anticholinergic toxicity.

 

Galanthus-nivalis

Galantamine

In 1947, Soviet scientists N.F. Proskurnina and L.Y. Areshknina reported the discovery of previously unknown alkaloids in the common snowdrop (Galanthus nivalis) and named the compound galantamine. Used as a neuromuscular drug in the 1960s, galantamine demonstrated positive effects on impaired human cognition in the late 1970s, although Cold War-era supply issues prevented its systematic development as an Alzheimer’s drug until the 1990s. The achievement of full chemical synthesis enabled supply to be increased by an order of magnitude, and by 2001 galantamine was launched onto the market in the US and Europe (as Reminyl, or Razadyne).

 

Donepezil

A derivative of tacrine, an early cholinesterase inhibitor whose use has now been discontinued, donepezil delays the progressive worsening of cognitive symptoms of Alzheimer's disease, and was first approved for sale (as Aricept) in the US in 1996, with Canada, the European Union, and many other countries following soon afterwards. According to one survey, “most studies convey that this drug can provide a modest benefit on cognition, behavior, and (daily) activities… in (cases of) both moderate and severe AD, contributing to slow down disease progression and, to a lesser extent, to delay institutionalization.”

 

Rivastigmine

A semi-synthetic derivative of physostigmine, rivastigmine was developed by a team led by Dr Marta Weinstock-Rosin, of Hebrew University in Israel. Weinstock-Rosin, who as a child narrowly escaped to Britain from Nazi Germany in 1939 and emigrated to Israel 30 years later, won the Israel Prize for medicine for her discovery. After being sold to Novartis by the university’s technology transfer company, Yissum, rivastigmine was marketed under the brand name Exelon as a treatment for Alzheimer’s, and brought in more than $1 billion in revenues in the year 2013 alone.

 

 

Mechanism of action

In the brains of dementia sufferers, there are low levels of acetylcholine, a chemical that helps send signals between nerve cells. Donepezil, rivastigmine and galantamine all work in a similar way – by preventing acetylcholinesterase from breaking down acetylcholine, which may ease symptoms of Alzheimer’s disease temporarily. Rivastigmine is a carbamate derivative that is structurally related to physostigmine, but not to donepezil and tacrine. The precise mechanism has not been fully determined, but it is suggested that rivastigmine binds reversibly with and deactivates chlolinesterase (e.g. acetylcholinesterase, butyrylcholinesterase), preventing the hydrolysis of acetylcholine, and increasing its concentration at cholinergic synapses. The anticholinesterase activity of rivastigmine is relatively specific for brain acetylcholinesterase and butyrylcholinesterase compared with those in peripheral tissues.

Synthesis

rivastigmine-synthesis

 

 

 

API

Rivastigmine Hydrogen Tartrate

rivastigmine-hydrogen-tartrate

 

Impurities

Name

Impurity

Product Type

Pack Size

3-[(1RS)-1-(Dimethylamino)ethyl]phenyl Dimethylcarbamate

Impurity

By-product

100mg

3-[(1R)-1-(Dimethylamino)ethyl]phenyl N-Ethyl-N-methylcarbamate Hydrogen Tartrate ((R)-Rivastigmine Hydrogen Tartrate)

Impurity

By-product

25mg

3-[(1S)-1-(Dimethylamino)ethyl]phenol (Dimetol)

Impurity

Degradation product; Intermediate

25mg

3-Acetylphenyl Ethyl(methyl)carbamate

Impurity

Degradation product; Intermediate

25mg

3-[(1RS)-1-(Dimethylamino)ethyl]phenyl Dimethylcarbamate Hydrochloride

Impurity

By-product

25mg

3-Nitrophenyl Ethyl(methyl)carbamate

Impurity

 

25mg

1-(3-Methoxyphenyl)ethan-1-ol

Impurity

Intermediate

25mg

3-((1RS)-1-Aminoethyl)phenyl N-Ethyl-N-methylcarbamate

Impurity

Degradation product

100mg

3-[(1RS)-1-[[Ethyl(methyl)carbamoyl]amino]ethyl]phenyl N-Ethyl-N-methylcarbamate

Impurity

 

25mg

3-((1RS)-1-Aminoethyl)phenyl 4-Methylbenzenesulfonate

Impurity

Intermediate

100mg

1-(3-Methoxyphenyl)ethan-1-one

Impurity

Intermediate

100mg

(S)-N,N-Dimethyl-1-[3-(4-nitrophenoxy)phenyl]ethanamine

Impurity

 

100mg

3-[(1S)-1-(Dimethylamino)ethyl]phenyl Diethylcarbamate

Impurity

By-product

100mg

(S)-1-[3-[(Ethyl(methyl)carbamoyl)oxy]phenyl]-N,N,N-trimethylethanaminium Chloride

Impurity

 

25mg

2-[(1RS)-1-(Dimethylamino)ethyl]phenyl N-Ethyl-N-methylcarbamate ((RS)-Rivastigmine 2-Isomer)

Impurity

By-product

100mg

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