While all epilepsy drugs carry a warning about an increased risk of suicidal behavior, it may only be certain newer medications that are connected to the hazard, a study published Monday suggests.

In a study of 44,300 UK patients who used epilepsy drugs between 1990 and 2005, researchers found an increased risk of suicide, attempted suicide or “self-harm” only among current users of certain newer medications that have previously been linked to a risk of depression.

Those drugs include topiramate (Topamax), tiagabine (Gabitril), levetiracetam (Keppra) and vigabatrin (Sabril).

The findings, published in the journal Neurology, add to a debate about the Food and Drug Administration’s decision, in 2008, to require all epilepsy medications to carry a warning about the risk of suicidal behavior.

The move arose from the findings of an FDA “meta-analysis” of 199 clinical trials testing 11 different epilepsy medications. That analysis, which combined the results of all the trials, found that patients receiving medication had a higher rate of suicidal thoughts and behavior during the study periods than those given a placebo — 0.4 percent, versus 0.2 percent.

The analysis was not, however, able to distinguish whether the risk was associated with any particular drugs. And critics argued that requiring all epilepsy medications to carry a suicide warning was too broad a measure, as the drugs are not all alike.

These latest findings offer some support for that contention. But they do not mean that the drugs implicated in this study are the only ones connected to suicide risk, according to the researchers and others who reviewed the study.

For one, the findings are based on a review of information from a database — a study design that cannot prove cause-and-effect.

Moreover, there were only a small number of documented suicides, suicide attempts or instances of self-harm (self-inflicted injuries without a clear intent of suicide), according to Dr. Frank Andersohn and his colleagues at Charite-University Medical Center in Berlin.

The researchers found 453 cases among all 44,300 patients, based on a UK database of electronic medical records.

They then attempted to look at the risk of suicidal behavior and self-harm according to different categories of epilepsy drug. Topiramate, tiagabine, levetiracetam and vigabatrin were grouped together as newer drugs with a “high” risk of depression — based on the fact that in clinical trials, more than 1 percent of patients using the drugs developed depression.

Another group included four newer medications considered to have a low depression risk: gabapentin (Neurontin), lamotrigine (Lamictal), oxcarbazepine (Trileptal) and pregabalin (Lyrica). The other two groups were barbiturates and older epilepsy drugs like valproate (Depakine, Epilim) and carbamazepine (Carbatrol, Tegretol).

Overall, the researchers found a three-fold higher risk of suicidal behavior or self-harm among current users of the group including topiramate, tiagabine, levetiracetam and vigabatrin, as compared with patients who had not used any epilepsy medication in the past year.

However, the numbers, again, were small.

There were only two cases each among current users of topiramate, levetiracetam and vigabatrin, and none among tiagabine users.

The findings, therefore, need to be “interpreted with caution” and confirmed in future studies, Andersohn and his colleagues write.

The results also differ from those of a study published in April in the Journal of the American Medical Association. In that study, researchers found that new users of gabapentin, lamotrigine, oxcarbazepine and tiagabine had a higher suicide risk than those on topiramate — one of the drugs linked to an increased risk in this latest study.

An editorial published with the study agrees that the research is a “good initial attempt” at looking at a complicated question, but more work is needed.

Epilepsy itself is linked to a higher-than-average risk of depression and suicide, pointed out Dr. Josemir W. Sander of the University College London in the UK, one of the editorial authors. That, he told Reuters Health in an email, can make it hard to “disentangle” the potential effects of epilepsy medications themselves.

“The fact that each study into this issue seems to come up with different answers just confirms my belief that this does not have an easy answer,” Sander said.

A limitation of the current study is that it lacked detailed descriptions of patients’ epilepsy type and any co-existing psychiatric disorders, according to Sander.

There is “no doubt,” he explained, that there are many different subgroups of people with epilepsy, and certain patients are more vulnerable to any increased risk of suicidal behavior linked to medications.

For now, Sander said, it is important for people with epilepsy to have a psychiatric evaluation before starting a new drug — a step the FDA has advised doctors to take.

Indeed, the key message for people with epilepsy is that the most important factor in their risk of suicidal thoughts or behavior is whether they have a history, or a family history, of depression or anxiety, according to Dr. Andres Kanner, a professor of neurological sciences at Rush Medical College in Chicago, and chair of the American Epilepsy Society’s task force on the psychiatric aspects of epilepsy.

Certain epilepsy medications may facilitate the development of suicidal thoughts and behavior in vulnerable people, Kanner told Reuters Health, but any risk linked to a drug itself would be small.

“Make sure your doctor knows if you have a history of depression or anxiety,” Kanner advised, noting that that includes a personal or family history. The doctor can then consider that in the overall management of a patient’s epilepsy.

Going forward, Sander said there remains an “urgent” need for clinical trials looking at individual epilepsy drugs in different subgroups of patients, to get a clearer picture of each medication’s full risk “profile.”

The study was funded by drugmaker Bayer Schering Pharma, and two co-authors on the work have served as consultants for Novartis and Sanofi-Aventis — makers of two of the medications not linked to suicide risk in this study.

Sander and his co-author on the editorial have ties to several makers of epilepsy drugs — including ones that were and were not linked to suicide risk in this study. The companies include UCB (maker of Keppra), Pfizer (Neurontin) and GlaxoSmithKline (Lamictal).

Kanner has also received research support from various companies that make epilepsy drugs.

Source: Reuters

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Actavis Group, the international generic pharmaceuticals company, today announced the launch of the antiepileptic drug Topiramate in the UK, Germany, France and Switzerland. The product was launched on day one as the originator’s patent expired on 25 September. Actavis was first to market in all four countries.

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Topiramate is used to treat epilepsy and will be sold in tablets of 25mg, 50mg, 100mg and 200mg. Topiramate is the generic equivalent of Janssen-Cilaq’s Topamax® / Epitomax®.

According to IMS Health, Janssen-Cilag’s product had sales of approximately ?? mln for the 12 months ended June 2009 in the four countries of UK, Germany, France and Switzerland.

Topiramate Actavis was developed by Actavis’ R&D in Iceland and in produced by Actavis in Hafnarfjordur, Iceland.

Actavis has already launched Topiramate in other countries where no patent protection was in place, including Portugal in 2007.

Source: LivePharma

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In a posting to the FDA’s website on Tuesday, the agency indicated that it approved updated labelling for more than 20 anti-epileptic drugs, which will warn about an increased risk of suicidal thoughts or behaviour associated with use of the treatments.

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The US regulator said it had been working with the manufacturers of the drugs “to better understand the suicidality risk” since issuing two safety alerts last year, including one in December announcing that the companies would be required to update the labels.

The changes apply to all anti-epileptic treatments, except those approved solely for short-term use, the FDA added. The drugmakers have also been required to develop comprehensive medication guides for patients, some of which have already been approved, while the remainder should be available by the end of the year. Guides already approved include those for Pfizer’s Lyrica (pregabalin), GlaxoSmithKline’s Lamictal (lamotrigine), UCB’s Keppra (levetiracetam), Johnson & Johnson’s Topamax (topiramate), and Eisai’s Zonegran (zonisamide).

Pfizer commented that “it worked closely with the FDA to update the labelling for its antiepileptic medicines,” and indicated that the warning “applies to all medicines in the anti-epileptic class.”

Source: FirstWord

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Researching drugs for neurological drugs can be a very dicey affair, considering the mushrooming R&D costs and expensive failures, especially in the case of orphan neurological disorders. Aashruti Kak provides an update on the status of drug development across neurological disorders

Hundreds of millions of people worldwide are affected by neurological disorders. Due to the incredibly high global prevalence of these disorders the scope of research in the neurology segment is infinite for researchers and highly profitable for pharmaceutical companies.

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As per Ramaraju Nallaparaju, Consultant, Healthcare Consulting, Datamonitor, India, in 2007, the global neurology market was worth $34.5 billion. Of the seven major markets, which account for 74 per cent ($25.5 billion) of the global market, US market was the largest with 64.5 per cent share ($16,434 million). The five European countries (France, Germany, Italy, Spain and the UK) had 27 per cent ($6,882 million) and JapanUS and the five EU markets have shown strong growth over the period 2004-07. However, with a CAGR of only 0.5 per cent , the Japanese market has remained flat over the same period. The top five neurological drugs companies-as measured in terms of 2007 revenues in the seven major markets-account for just over 43per cent of the total $34.50 billion 2007 neurological drug sales. accounted for 8.5 per cent ($2,178 million). Both the

“The central nervous system (CNS) market in India is estimated to be around Rs 1,200 crore ($275 million), with major players in this segment being Sun Pharmaceuticals, Torrent Pharma, Abbot India, and Lundbeck India. Other players which are making major inroads into this market are Intas Pharmaceuticals, Micro and Sanofi-Synthelabo India, USV and Elder Pharmaceuticals,” says Nallaparaju.

Common disorders

Common neurological disorders include epilepsy, Alzheimer’s disease and other dementias, Parkinson’s disease, multiple sclerosis, insomnia, cerebrovascular diseases including stroke, migraine and other headache disorders, neuroinfections, brain tumours, traumatic disorders of the nervous system such as brain trauma, and neurological disorders as a result of malnutrition. The existing therapies for the some of the disorders are as follows:

Epilepsy-Epilepsy can be controlled with medication, but not cured, although surgery may be considered in difficult cases. There are about 12-14 drugs available in the market to treat epilepsy, which is characterised by recurrent unprovoked seizures-transient signs and/or symptoms due to abnormal, excessive or synchronous neuronal activity in the brain. “Sodium valproate, carbamazepine, phenytoin, lamotrigine, topiramate and leveritacetam (last three being newer drugs) are some of the most commonly used treatments. These drugs may work for some and not for others. Often even the newer drugs fail,” says Dr Joy Desai, Consultant Neurologist, Jaslok Hospital, Mumbai.

Multiple sclerosis (MS)-MS is an auto immune brain targeted inflammatory disease in which the body’s immune system changes and identifies the brain structures as being foreign, and therefore it attacks it. “MS may cause attacks that may lead to numbness is limbs, paralysis, visual, urinary or speech problems. So during the acute attack you are supposed to suppress it by giving an immunosuppressant, which commonly is intravenous (IV) steroids, which helps for the time being but after a few months the attacks recur someplace else in the body,” informs Desai. Every attack leaves behind a disability which may be profound and may disallow a person from normal vision, imbalance etc. He adds, “To make sure that these recurring attacks die down you need an immunomodulator, which modulates the immune system such that it stops attacking itself too often. In the case of MS, immunomodulators that are currently in use are interferons.”

Alzheimer’s disease-The basic reason why Alzheimer’s disease occurs is due to the depletion of a chemical called acetylcholine in the fundamental circuits that sub serve memory registration and retrieval. And if you supplement a drug that can augment the amount of acetylcholine in the brain then memory improves. “There is no absolute cure, but there are three medications that have been licensed for treatment to help their symptoms of the disease-rivastigmine, donepezil, galantamine,” says Desai. Aricept (donepezil hydrochloride), produced by Eisai and co-marketed with Pfizer, was the first drug to be licensed in the UK specifically for Alzheimer’s disease, followed by Exelon (rivastigmine) by Novartis Pharmaceuticals, Reminyl (galantamine), co-developed by Shire Pharmaceuticals and the Janssen Research Foundation, and Ebixa (memantine), produced by Merz and marketed in Europe by Lundbeck, which is the newest of the Alzheimer’s drugs.

Parkinson’s disease-Treatment for Parkinson’s has evolved considerably over the last three decades. Existing treatments day can improve symptoms, delay onset of total physical dependence, hence delaying morbidity and mortality, which result due to progressive immobility. Levodopa (also called L-dopa) is the most commonly prescribed and most effective medication for controlling the symptoms of Parkinson’s disease, particularly bradykinesia (slow movement) and rigidity. L-dopa is taken in combination with carbidopa (Sinemet) to increase its effectiveness and prevent or lessen side effects. Other treatments are dopamine agonists (Parlodel, Permax, Requip, Mirapex)-that activate dopamine receptor-taken alone or in combination with sinemet. Requip and Mirapex are newer medications, which are safer and more effective than the older drugs, Parlodel and Permax. Symmetrel, anticholinergics (artane, cogentin), eldepryl or deprenyl, Tasmar and Comtan (COMT Inhibitors) are other treatments for Parkinson’s.

Orphan neurological disorders-Amyotrophic lateral sclerosis (ALS/Motor neuron disease) and Huntington’s disease (HD) are two orphan neurological disorders. ALS, also known as Lou Gehrig’s disease and Maladie de Charcot, is a progressive neurodegenerative disease associated with the loss of upper and lower motor neurons. “Sanofi-Aventis’s Rilutek (riluzole) is the leading drug for ALS. Rilutek accounted for 84 per cent of the total ALS market value in 2006, across the seven major markets. Other drug classes, such as antidepressants and antispasm agents, are prescribed to treat specific symptoms and co-morbidities,” informs Nallaparaju.

HD, on the other hand, is an autosomal dominant, inherited, neurodegenerative, neuropsychiatry disease which gives rise to progressive motor, cognitive and behavioral symptoms. Nallaparaju says, “Current pharmacological therapy of HD is limited to the management or alleviation of associated neurobehavioral or movement abnormalities. The market is almost entirely composed of off-label prescribing of narcoleptics, antidepressants and anti-Parkinson’s drugs. Due to the comparatively cheap and highly genericised nature of these drug classes, the value in the six major markets (US, France, Germany, Italy, Spain and the UK) reached only $24 million in 2007.”

Top 10 neurological brands in the seven major markets (based on the last three quarter sales in 2006) are-Aricept for Alzheimer’s (patent expiring in 2010); Topamax for epilepsy (patent expiring in 2008); Lamictal for epilepsy (patent expiring in 2008); Ambien for insomnia (patent expired); Depakote for epilepsy (patent expiring in 2008); Avonex for MS (patent expiring in 2013); Lyrica for epilepsy (patent expiring in 2018), Copaxone for MS (patent expiring in 2014); Imitrex for migraine (patent expiring in 2008); and Kepprafor epilepsy (patent expiring in 2008. With some drug patents expiring this year and in the near future, the prospects of getting cheaper, and hence, more accessibility are bright.

“Among the top 10 neurological brands across the seven major markets, the leading drug class is anticonvulsants (Topamax, Lamictal, Depakote, Lyrica and Keppra). These are also approved for a number of psychiatric and pain indications, which significantly broadens their target patient population,” says Nallaparaju. Among the anticonvulsants, Pfizer’s Lyrica is the fastest growing neurological drug with a CAGR of approximately 400 per cent (2004-2007) and it sustained this rapid growth in 2006-07 with an annual growth of 50.7 per cent . “Five of the top 10 products are getting off-patent this year. With formulation and development expertise, global presence, and competitive pricing, Indian companies are poised to target the $8.8 billion market of these five drugs getting genericised,” he adds.

Current ongoing research

“For epilepsy, we are doing clinical research for new drugs, mostly because there are patients that need them following the failure of standard treatments. These trials are sponsored by UCB,” reveals Desai. “We have a new anti-epileptic drug called brivaracetam (generic), which is a new compound developed by UCB. Right now we are doing phase III for brivaracetam for epilepsy patients who are not responding to standard treatment,” he adds. The drug may be put up for FDA licensing in 2010, so it might come into the market internationally by 2011. Johnson & Johnson is also developing a drug called carisbamate that it thinks is very promising, which may hit the market by 2010.

For MS there are newer immunomodulators that may be available two or three years from now. “There is a monoclonal antibody (mAb) called tysabri (natalizumab), which is undergoing studies in Europe and the US. Initially, when the drug was developed, there were two patients who had a very disastrous side effect and died-a condition called progressive multifocal leukoencephalopathy (PML). It has not happened again but it can be considered as a possible side effect. In all likelihood the drug will still get licensed,” says Desai.

There is a vaccine that is being studied for Alzheimer’s-beta amyloid vaccine. There is an abnormal deposition of a protein called beta amyloid (present in many structures of the nervous system) which, in Alzheimer’s, goes under a structural change and gets deposited as a pathological process and forms what is known as neuritic plaque. So to target this part of the pathology researchers are trying to target a vaccine which can block the beta amyloid from getting deposited in the brain. However, according to a recent study by researchers in University of California (in the Journal of Neuroscience), the vaccine does what it is designed to do-clear beta-amyloid plaques from the brain-but does not seem to help restore lost learning and memory abilities, hence the need for complementary treatments that would be able to address the complexity of Alzheimer’s disease.

Another significant development in Alzheimer’s R&D is the recent liscencing deal between Pfizer and Medivation (a San Fransisco based biopharmaceutical company) to co-develop and market Medivation’s drug Dimebon for Alzheimer’s and Huntington’s disease, which is currently in phase III trials. The results from the study should be out by 2010.

In mid 2007, a study featured in the journal Nature stated that a team of researchers at Northwestern University’s Feinberg School of Medicine had found that isradipine, a drug widely used for hypertension and stroke, could restore dopamine neurons to their original healthy state in mice, hence benefiting susceptible cases of Parkinson’s as well as those who are already affected by the disease. Another drug has been very recently found to slow the progression of Parkinson’s. Researchers from Newcastle University found that rasagiline (also known as Azilect) can slow the development of the disease if given at an early stage. Both the above mentioned studies cannot be termed as conclusive; however, they do raise expectations of a new treatment for the disease.

There any other known and promising neurological drugs as well that are currently undergoing clinical trials in various companies.

Issues and trends

There are quite a few issues and limitations that pharma companies face in the R&D of neurological drugs across disorders. “Considering that among the top 10 products five of them are getting off-patent this year, new drug launches in the same therapy classes of these drugs are bound to get affected,” reveals Nallaparaju. He continues, “The reduced cash flow (from lower revenue realisation) will adversely affect investments in R&D. There are chances of potential failure in the clinical trials, and availability of limited patient population (for recruiting in trials) of ALS and Huntington’s disease.” Additionally, he says that since novel therapies like cell therapy/gene therapy for Parkinson’s disease are still in initial stages of development, it is likely that there would be regulatory resistance to the acceptance of such novel therapies.

There have also been controversies regarding the teratogenicity of some of the neurological drugs. For instance, carbamazepine has a potential teratogenic risk. A number of reports have described a slight increase in the risk of major congenital abnormalities, especially neural tube defects, among children of mothers with epilepsy treated with carbamazepine during pregnancy. If women are treated with a combination of carbamazepine and other anti-epileptic drugs, particularly sodium valproate, there is an increased risk without any doubt.

A new trend that is surfacing is the overlap of neurology and psychiatry, because of which there may be a dual approach required/implemented soon to deal with neurological disorders. “Because some of the psychiatric drugs are being used off-label in neurological disorders, this is quite possible. Also, some psychiatric drugs will be used in these conditions for the co-morbidities that the patients may be present with,” says Nallaparaju.

Desai concurs, ” Most of the anti epileptics are being used by psychiatrists to treat bipolar mood disorder based on the theory that bipolar depression is a sort of limbic epilepsy (epilepsy of emotions).” For example, sodium valproate is used off-licence by specialists as a mood stabiliser for treating people with the psychiatric illness, bipolar affective disorder. This use is not licensed, but the medicine has been shown to be effective for controlling episodes of mania in this condition, and for helping prevent future episodes of ill health. To understand better cases like how sodium valproate works as a mood stabiliser in bipolar disorder, neurologists and psychiatrists ought to work together.

Unmet needs

Globally, about 94 companies are developing products for various neurological disorders. From amongst them, some Indian companies like Glenmark are developing drugs for indications like migraine (pipeline drug-GRC6211). Glenmark has partnered with Eli-Lilly for development deals. Suven Life sciences has also partnered with Eli-Lilly.

As neurological disorders are age-related, an increasing ageing population will drive the growth of the market, and hence the R&D. The following indications posses high levels of unmet needs:

Alzheimer’s disease affects approximately 24 million people worldwide today, with the number predicted to reach 40 million by 2020. Further, current therapy has a modest symptomatic effect and does not significantly modify the course of this progressive neuro-degenerative disorder

There is a significant need for an MS treatment with superior efficacy to current therapies with a less invasive and less time-consuming route of administration. There is also an unmet need for primary-progressive and secondary-progressive MS indications

There is also need for a reduced dosing frequency or a less invasive therapy with good patient compliance

In novel therapies for Parkinson’s like cell therapy/gene therapy, initial studies have shown significant results in slowing the progression of the disease, this area needs to be explored more extensively.

Searching for the ‘Ideal’

“Philosophically, I think most disease cannot be reversed, you can only buy time. The key to developing new drugs for these disorders is to know what goes wrong and try to formulate a fix,” says Desai. He adds, “The problem in degenerative disease is that we only know what happens as an end result, but we haven’t yet understood what initiates it. If one can find the initiative event that triggers the disease chain, we can come close to finding a better treatment if not a cure.”

Each drug is different. Desai says, “We need a medication that can be given orally and at the same time can pass the blood brain barrier and reach the nervous system to the target because the target is itself protected by the blood brain barrier.” Another attribute can be that the drug should be specifically targeted, act only at the site where it is needed, for example it should only augment acetylcholine in the brain where it is needed and not else where in the body and produce side effects. “A drug that can reach the nervous system without losing its potency and has minimum side effects is what you are looking for,” he says. Unfortunately, neurological diseases are so many that it will be difficult to form a common umbrella to give attributes to a drug and call it ‘ideal’.

Source: Express Healthcare

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