Chiral switch

The word "chiral switch" was introduced by Agranat and Caner in 1999.[1] Chiral switches are chiral drugs that are already approved as racemates but that have been re-developed as single enantiomers.[2][3] The term chiral switching has been coined to describe the development of single enantiomers from racemate drugs. For example, levofloxacin is a chiral switch of racemic ofloxacin. The essential principle of a chiral switch is that there is a change in the status of chirality.[4] In general, the term chiral switch is preferred over racemic switch because the switch is usually happening from a racemic drug to the corresponding single enantiomer(s). It is important to understand that chiral switches are treated as a selection invention.[5] A selection invention is an invention that selects a group of new members from a previously known class on the basis of superior properties.[6] To express the pharmacological activities of each of the chiral twins of a racemic drug two technical terms have been coined eutomer and distomer.[7][8] The member of the chiral twin that has greater physiological activity is referred to as the eutomer and the other one with lesser activity is referred to as distomer. The eutomer/distomer ratio is called the eudisimic ratio and reflects the degree of enantioselectivity of the biological activity.[9]

In case of stereoselectivity in action only one of the components in the racemic mixture is truly active (eutomer). The other isomer, the distomer, should be regarded as impurity or isomeric ballast[10] not contributing to the effects aimed at. It is well documented that the pharmacologically inactive isomer (distomer) may contribute to the toxic or adverse effects of the drugs. There is a wide spectrum of possibilities of distomer actions, many of which are confirmed experimentally.[11][12] Sometimes the single enantiomer version lacks certain side-effects that the racemate exhibits. And where the two enantiomers are sufficiently different in pharmacological effects, it may be possible to get a patent on one or both isomers (for instance, as in the case of propoxyphene). The chiral twins of propoxyphene are separately sold by Eli Lilly and company. Dextropropoxyphene is an analgesic agent (Darvon) and levopropoxyphene an effective antitussive (Novrad).[13][14] Interestingly the reversed trade names of the drugs, DARVON and NOVRAD, also reflect the chemical mirror-image relationship. A positive consequence of this redesigning approach is that it has given a new life to an old drug, minimizing or avoiding the undesirable side-effect profile. Whether to go in for a chiral switch is normally made on a case-by-case basis. A pragmatic solution could be in favor of a decision-tree approach, incorporating various factors such as pharmacodynamic, pharmacokinetic, toxicological profile of the enantiomers, enantiomer-enantiomer interaction potential, safety, efficacy, risk-benefit ratio, chiral inversion, distomer liability, physicochemical properties, cost of separation and production, quality control criteria, marketing edge, etc.[15][16][17][18]

The chiral-switch concept


The chiral switch concept[19] is illustrated in the diagram. This chiral switch is from (±)-ibuprofen to (S)-(+)-ibuprofen (dexibuprofen). The nonsteroidal anti-inflammatory drug (NSAID) ibuprofen was the first chiral drug of the NSAID class to be switched to the single-enantiomer version in 1994. The switch was done based on the fact that the (S)-ibuprofen, the eutomer, was over 100-fold more potent as an inhibitor of cycloxygenase-1 (COX-1) enzyme than (R)-ibuprofen.[20] Moreover, ibuprofen, when administered as the racemate, the active (R)-enantiomer undergoes partial unidirectional chiral inversion (approximately 60%) to the (S)-enantiomer. Therefore, the use of the single (S)-ibuprofen was expected to give faster onset of action at a lower dosage.[21]

The chiral-switch concept

Rationale for switching

There are several possible potential benefits to chiral switching or chiral specific drugs.[22] These include:

  1. An improved (less complex, more selective) pharmacodynamic profile
  2. A higher therapeutic index (improved safety margin)
  3. Less complex pharmacokinetic profile, less complex drug interactions
  4. Less complex relationship between plasma concentration and effect  
  5. More rational therapeutic drug monitoring
  6. Expose the patient to less body load and thus reduce metabolic/renal/hepatic drug load

The chiral switching approach has sometimes resulted in failures and disappointments.[23]

Regulatory environment

The roles of regulatory agencies also continue to evolve with respect to the development of chiral switches. An interesting concept brought up in the FDA policy is that of "bridging studies".[24][25] [26][27] When a sponsor/innovator seeks to develop a single enantiomer from a racemic drug, the regulatory agencies demand them to conduct bridging studies. Bridging studies are tests (pharmacological and toxicological evaluations) to connect what is known about the already approved racemate and what is unknown about the single enantiomer under study, without going back to square one as for a completely new chemical entity. The intent of the bridging studies is to make sure that the companies are not scarifying some protective effect conferred by the other" isomer when they develop a chiral drug as single enantiomer rather than a racemate. "Bridging" procedure will help to reduce the number of studies required on the "new" enantiopure drug.[28]

Launched chiral switches

Chiral switch, a re-engineering approach, has enabled in the remarketing of a number of racemic drugs as chiral specific enantiomer products. Chiral switching strategy is the way most blockbuster drugs have entered the market as enantiopure drugs. But the alternate route is de novo (anew) synthesis of chiral specific drugs.[29] The chiral switches may have the same, very similar, therapeutic indications as the original racemic drug. But, there are instances where new indications for the old drug have been reported. The table below gives a brief list of launched chiral switches.[30]

Racemic drug Chiral switch (Unichiral drugs)[31][32] Pharmacological action Main benefit(s) claimed
Ibuprofen (S)-(+)-Ibuprofen; Dexibuprofen Anti-inflammatory Faster onset; low adverse effect profile
Ofloxacin (S)-(-)-Ofloxacin; Levofloxacin Antibactereial increased potency
Ketoprofen (S)-(+)-Ketoprofen; Dexketoprofen Anti-inflammatory Faster onset
Salbutamol/ Albuterol (R)-(-)-Albuterol; Levalbuterol Bronchodialator Reduction in side effects; improved tolerability profile
Omeprazole (S)-(-)-Omepazole; Esomeprazole Proton pump inhibitor Increased activation; less variable metabolism
Bupivacaine (S)-(-)-Bupivacaine; Levobupivacine Local anethetic Decreased risk of cardiotoxicity
Cetrizine (R )-(-)-Cetrizine; Levocetirizine Antihistamine Increased potency; decreased side-effects
Citalopram (S)-(-)-Citalopram; Escitalopram Antidepressant Faster onset of action; reduction in side effects and improved tolerability profile
Ketamine (S)-Ketamine Anaesthetic Increased potency and tolerance; faster recovery

Failed/aborted chiral switches

The re-evaluation of single enantiomers not without problems. The chiral switches of fluoxetine and fenfluramine are classical examples.[33] The development of (R )-fluoxetine was terminated after patients developed abnormal heart rhythms. The chiral switch of fenfluramine, dexfenfluramine was withdrawn from world marker due to pulmonary hypertension. The table below enumerates couple of chiral switches aborted or withdrawn due stereochemically engineered toxicity.

Racemic drug Chiral switch Pharmacological action Comments
Fluoxetine (R)-Fluoxetine Antidepressant Significant increase in QTC ; Abnormal heart rhythms; Aborted the program[34]
Fenfluramine (S)-Fenfluramine; Dexphenfluramine Antiobesity Valvular heart disease and Pulmonary hypertension; withdrawn worldwide,1997.[35][36]
Labetalol Dilevalol Beta blocker Increased hepatotoxicity[37]
Propranolol S(-)-Propranolol Beta blocker Unexpected reduction of beta-blocking activity[37]

Evergreening

"Evergreening" refers to the various strategies whereby owners (innovators/sponsors) of pharmaceutical products use patent laws and minor drug modifications to extend their monopoly privileges on the drug.[38] An enantiomer patent is another form of evergreening based on a chiral switch strategy.[39] Single-enantiomer drugs represent more than 50% of the top-selling 100 drugs worldwide.[40] There are some studies which go to suggest that drug companies employ chiral switching for life-cycle management/patent protection of the parent racemic drug and also as a marketing strategy.[41] Pharmaceutical companies support evergreening practices.[42] Some chiral switches are performed to re-start the patent clock for a medication without reducing side effects or improving efficacy.[43] A high price can then continue to be charged for a medication. [43] Examples include citalopram and escitalopram, and omeprazole and esomeprazole. In both these medications, proposed theoretical benefits were used to market the enantiopure drugs, without any clinical trials being conducted to provide evidence that the racemic drugs improved patient centered outcomes. [43]

Metabolite switches

This idea, drug to metabolite switching, is an extension of the chiral switch concept. The purpose of the switching is to develop an active metabolite which will be devoid of the side-effects and have an improved therapeutic profile compared to the parent drug. Some examples of metabolite switches,[44] (including those in the market and others under investigation) include terfenadine to fexofenadine; astemizole to norastemizole; loratadine to desmethylloratadine, halofantrine to desbutylhalofantrine, and cisapride to norcisapride. The following table lists some examples of drug to metabolite switches.

Original drug Metabolite switch Pharmacological action Main claimed benefit(s)
Terfenadine Fexofenadine Antihistaminic Decreased cardiotoxicity
Astemizole Norastemisole Antihistaminic Increased potency; decreased cardiotoxicity
Loratidine Demethyltoratidine Antihistaminic Increased potency
Halofantrine Desbutythalofantrine Antimalarial Decreased cardiotoxicity
Cisapride Norcisapride Prokinetic Increased efficacy; decreased cardiotoxicity
Acetanilide Paracetamol Analgesic Does not cause methemoglobinemia
Phenacetin Not carcinogenic
Risperidone Paliperidone Antipsychotic Less variability of effect; less sedation[45]

See also

References

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