Xadago back on track in the US
Xadago (safinamide) for PD is back on track in the US as the FDA has informed the company and its partners Zambon and US WorldMeds that no further clinical studies will be required for Xadago’s US NDA resubmission. A complete response letter issued by the regulators on 29 March had requested clinical evaluation of the possible effect of safinamide on potential abuse liability and dependence/withdrawal effects as required by the Controlled Substance Staff (CSS) in the Center for Drug Evaluation and Research (CDER) at the FDA; no further efficacy or safety data for Xadago in patients with PD has been requested. Newron had subsequently submitted additional preclinical abuse liability studies and additional analyses of the clinical data as requested by CSS following on-going dialogue with the agency.
Newron now aims to re-submit Xadago’s NDA by end November and anticipates US approval mid 2017. This outcome is positive in our view as we had raised concerns that additional trials could be required and, as such, had placed our valuation under review while we awaited further clarity from the company post discussions with CSS on the revised approval timelines for Xadago in the US, to understand the magnitude of the slippage. Our concerns have now abated but we have revised our US Xadago expectations to a launch mid-2017 from H216 to reflect the need to re-submit the NDA file.
Safinamide is a reversible MAO-B inhibitor
Safinamide has multiple mechanisms of action, with reversible inhibition of MAO-B (monoamine oxidase), which blocks the enzyme responsible for breaking down dopamine, inhibition of dopamine uptake, and inhibition of glutamate release. PD is characterised by progressive loss of dopaminergic neurons within the basal ganglia in the brain, leading to a decline in dopamine levels. Since dopamine plays a critical role in movement and co-ordination, a reduction in its levels leads to the characteristic and progressive features of PD; tremor, slowness of movement and rigidity. The current mainstay of drug treatment is limited to oral therapies such as levodopa (L-DOPA), dopamine agonists (DA) and monoamine oxidase-B inhibitors (MAOI), which aim to increase or substitute for dopamine. However, over time the benefits of drug treatment diminish (L-DOPA provides symptomatic relief of around three to five years. Importantly treatment with L-DOPA can lead to the unpleasant axillary effects of motor fluctuations (ON/OFF effect) and involuntary movements known as L-DOPA induced dyskinesia (LD). Safinamide helps to restore dopamine levels in the brain (by inhibiting dopamine enzymatic breakdown), thereby improving the patient's symptoms.
Safinamide is used as an add-on to L-DOPA therapy
Safinamide is being positioned as an add-on rather than a monotherapy treatment in PD, given that it can be used in combination with DA’s in early PD and with L-DOPA in mid- to late-stage patients. This means patients can remain on safinamide throughout their life, without physicians having to switch treatment with disease progression, which in our view would facilitate its use. Exhibit 2 highlights the clinical impact of safinamide as an add-on therapy at various stages of PD.
Both DAs and L-DOPA are now generic, hence expensive drug combinations should not be an issue or barrier to safinamide’s use. Both DAs and L-DOPA are well established in treating PD, hence the biggest competition to safinamide, in our view, will likely be new drugs with unique or novel mechanisms of action; however, the majority of such candidates are at an earlier stage of development.
Exhibit 2: Xadago offers benefits in PD across the disease spectrum as add on therapy
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Source: Newron presentation
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Regional partnerships in place to maximise value
Safinamide was partnered with Meiji Seika in Japan/Asia, with Zambon in all other regions during 2012 and with US WorldMeds as a sublicence from Zambon for the US market in 2016. Zambon is a private Italian company with 2014 reported group turnover of €601m, with the pharmaceutical division contributing 88% and the chemicals division 12%. The main focus of the pharma division is respiratory, pain management and women’s health. Zambon does not have a significant pharmaceutical sales presence in the US and hence the drug was sub-licensed to US WorldMeds in the US to maximise safinamide’s potential. Newron is eligible for regulatory related milestone payments from Zambon (we assume US approval) and for double-digit royalties on sales. As part of any sub-licensing, Newron could be eligible for around 25-30% of milestone payments and 50% of royalties. Financial terms with Meiji Seika have not been disclosed; the Phase III study has been initiated in Japan. To date, partner Zambon has launched Xadago in nine EU countries (Germany, Spain, Italy, Belgium, Denmark, Sweden, the UK, the Netherlands, Luxembourg) and Norway and Switzerland. We expect further launches in Europe in 2016.
US WorldMeds: Xadago a neat fit into the portfolio
Commercial partner, Zambon, has sublicensed the US commercialisation Xadago (safinamide) to US WorldMeds. Under the agreement’s terms, Zambon will give Newron a share of undisclosed upfront, milestone and royalty payments made by US WorldMeds in addition to a milestone payment on FDA approval (we estimate €9m, which we include in our 2017 forecasts).
US WorldMeds is a Kentucky-based pharmaceutical company that markets a number of specialty products including a treatment for PD (notably Apokyn) for the acute treatment of intermittent ‘off’ episodes). If approved, Xadago would fit neatly into WorldMeds’ portfolio as it would be indicated for use as add on to levodopa in mid- to late-stage PD. WorldMeds plans to focus more than 60 sales representatives on launching Xadago in the US, which we now assume in H217 on the basis of an approval in H117.
We forecast global peak sales of €450m in PD
In the US there are 1-1.5 million PD patients; we estimate around 80% of PD patients receive treatment, suggesting a total treated PD patient population of around one million (taking the mid-way point). There is a similar-sized market in Europe and a smaller market of around 250,000 in Japan. Safinamide could be used to treat all stages of PD and we assume can reach peak penetration of 10% of treated PD patients six years after launch. We assume a price of $7/day in the US and €3.7/day in Europe and Japan (around a 20% discount to the US price assumption), which compares favourably to other PD products, including rasagiline (which will go generic in 2017). We continue to forecast peak Xadago sales of €450m in PD, which comprises ex-US peak sales of €200m based on use only in the mid-late stage PD patients, a group which represents 75-80% of the PD market. In the US, our peak sales are €250m where we continue to include both the early and mid- to late-stage patients. Our royalty rate forecasts are around 12-13%.
In our view, the closest comparable (and competitor) for Xadago/safinamide is Azilect (rasagiline), an MAO-B inhibitor that is used as monotherapy and as an add-on to L-DOPA. Azilect is sold by Teva and Lundbeck and generated sales of $650m in 2014; it will go generic in 2017. In contrast to other MAO-B inhibitors, safinamide does not appear to have a tyramine interaction, hence avoiding any dietary restrictions (such as cheese and red wine).
Dyskinesia could expand the market opportunity
A subset analysis of a previous clinical trial (study 018) found that safinamide could improve dyskinesia in patients with moderate dyskinesia at baseline. This could present an attractive and differentiated market opportunity for safinamide. Safinamide is thought to improve dyskinesia owing to inhibition of glutamate release, with glutamate expression associated with dyskinesia. Although L-DOPA is an effective treatment for PD, its use is associated with the development of dyskinesia. The ability to improve dyskinesia could therefore allow for potentially earlier use of L-DOPA in PD and to expand the market opportunity for safinamide.
The subset analysis revealed that the third of patients who scored a four or higher on the dyskinesia rating scale at the beginning of the study reported an improvement of 24% on 100mg of safinamide (added to L-DOPA) versus placebo. There were no significant differences, however, for patients on 50 mg of safinamide.
Further studies evaluating safinamide’s impact on dyskinesia will depend on partner Zambon and sub-licenser US WorldMeds intentions for its development. We believe a single six-month treatment study assessing patients with higher grade dyskinesia could be sufficient to file for a label extension for safinamide. We highlight that the dyskinesia label extension would differentiate safinamide from all other classes of PD drug treatments.
We include a risk-adjusted contribution for safinamide in dyskinesia, assuming peak sales of €350m until there is more clarity on the potential magnitude of benefit. It is estimated that dyskinesia affects around 40% of PD patients treated with L-DOPA for four to six years, with limited treatment options aside from L-DOPA dosing adjustment. With around one million PD patients in each of the US and Europe, this represents a large opportunity. We assume the safinamide label could be expanded to include dyskinesia following a single clinical trial, which could potentially start once approval has been granted in the US and could lead to potential launch in 2020.
Evenamide (NW-3509) Phase II data potential Q416
Evenamide (NW-3509) is an internally developed asset that originates from Newron’s ion channel discovery platform. It is a novel, new generation, oral, antipsychotic drug in development for schizophrenia that acts through pathways that are not targeted by available antipsychotic drugs. Given the lack of novel treatments for this chronic, debilitating condition, positive Phase II data confirming proof of concept would be welcomed by the market. Evenamide is being evaluated in the first instance as a potential add-on therapy to antipsychotics for treating schizophrenia.
Schizophrenia is a chronic and severe mental disorder involving a breakdown in the relation between thought, emotion and behaviour, leading to faulty perception and the inability to function normally. Signs and symptoms can vary. Generally symptoms are classified into three categories:
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Positive symptoms include hallucinations, delusions, thought disorders, movement disorders
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Negative symptoms include flat effect (reduced expression of emotion), social withdrawal, lack of interest in everyday activities
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Cognitive symptoms include trouble focusing, poor ‘executive functioning’ and problems with ‘working memory’
Drug treatments for schizophrenia focus on eliminating symptoms; the current mainstay of which are antipsychotic drugs (‘typical antipsychotics’ were developed in the 1950’s examples include haloperidol, chlorpromazine and fluphenazine; ‘atypical antipsychotics’ were developed in the 1990s, examples include aripiprazole (BMS’s Abilify), olanzapine (Lilly’s Zyprexa), quetiapine (AstraZeneca’s Seroquel) and risperidone (Risperdal). The first generation of typical anti-psychotics were hampered with significant neurological side effects including in some cases non-reversible tardive dyskinesia. The newer generation of ‘atypical antipsychotics improved on the side effect profile, however, long-term drug treatment of schizophrenia has its limitations; the NCBI (US National Center for Biotechnology) estimates that 25-33% of patients are treatment resistant.
Novel mode of action enables reduced hyper-excited neuronal activity
Evenamide functions as a sodium channel modulator, which regulates the hyperexcitability of neurons. This means that evenamide may normalise the activity of neurons that are firing too rapidly or at an abnormal rate; many schizophrenia patients exhibit abnormal excitability of neurons in certain regions of the brain. This abnormal excitability translates into high levels of glutamate, which may be responsible for many symptoms of schizophrenia. Thus, modulation of hyperexcitability could reduce psychotic symptoms such as hallucinations and delusions, especially when used as an add-on to available antipsychotic treatments. Importantly the addition of evenamide as an adjunct to antipsychotics could reduce antipsychotic-induced side effects and enable patients to take a lower dose of the concurrent anti-psychotic. Evenamide importantly has a fast onset of action and has demonstrated high bioavailability in the brain. Evenamide is patent protected in the US and other territories until around 2028, excluding any extensions.
Early data show evenamide could have utility as add-on therapy
A Phase I safety study including doses of evenamide up to 30mg has completed in 54 healthy volunteers; the drug was generally well tolerated. Evenamide has shown benefits in preclinical models of psychosis, mania, depression, anxiety and cognition. In particular, improved effects were noted with the combination of evenamide with either haloperidol or risperidone (both typically used to treat schizophrenia) in a preclinical model, shown in Exhibit 3. Evenamide could therefore have utility as an add-on treatment to antipsychotics in patients with schizophrenia who are experiencing breakthrough symptoms despite being on standard of care.
Exhibit 3: Preclinical data demonstrating the improved effect from the combination of NW-3509 with typical antipsychotics
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Source: Newron. Note: PPI or prepulse inhibition deficit is an excessive startle response, which is typically associated with schizophrenia; it results in an inability to recognise weak stimuli which is thought to lead to the typical symptoms of schizophrenia (including hallucinations and delusions).
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Phase II POC is expected to read out Q416
A Phase II study is ongoing (enrolment started January 2016), assessing evenamide as an add-on therapy for reducing positive symptoms and psychotic worsening in patients with schizophrenia experiencing breakthrough symptoms while on adequate doses of risperidone or aripiprazole; data could become available in Q416. This is a double-blind, placebo controlled, four-week in/outpatient study evaluating 15-25mg of evenamide (twice daily) in a minimum of 90 patients across study centres based in the US and India.
We forecast conservative evenamide peak sales of €380m
Newron estimates that the antipsychotic market is worth around $23bn, suggesting that evenamide could have significant potential. However, until proof-of-concept data are available, estimating the potential market opportunity for evenamide is not straightforward given its potential would be dependent on the breadth of clinical trials conducted. For the purposes of our valuation, we include base-case assumptions, which conservatively assume that evenamide could achieve peak sales of c €380m, representing only c 2% of the current market. Although we have limited visibility on the timing and terms of any potential out-licensing, we continue to assume standard terms including a double-digit royalty on sales, commensurate with an asset out-licensed with proof-of-concept data. Given the size of this market, evenamide’s potential could be significantly larger than our current estimate. Given the potential size of the market and scope of development, Newron plans to out-license this asset and a deal could come after the Phase II is complete; this should maximise deal terms although Newron would be prepared to partner sooner if suitable deal terms were offered.
Sarizotan the first orphan drug for RS
Sarizotan is a highly selective serotonin (5-HT1a) and dopamine (D2) antagonist that in preclinical studies demonstrated activity in normalising the abnormal breathing patterns in animal models of RS. In July 2015 the FDA designated orphan drug status to sarizotan for the treatment of RS. It was in-licensed from Merck KGaA in 2011 and was previously examined as a treatment for PD by Merck KGaA but failed in two Phase III trials in 2006.
Rett syndrome: A rare genetic disorder
RS is a rare, genetic neurodevelopmental disorder that generally affects girls. This severe brain disorder arises from a non-inherited genetic mutation (X-linked methyl CpG-binding protein 2). The mutation causes severe disability and a reduction life expectancy. Symptoms include impaired brain function, leading to issues with a number of functions, including breathing, swallowing, problems with muscles and co-ordination, and seizures. There is no curative treatment for RS and current treatment is therefore more symptomatic.
RS affects between one in every 10,000 to 15,000 female births (source: US NIH), with Newron estimating that there are around 36,000 RS patients in the US and Europe. Children with RS will generally develop normally until one to two years of age, when development will slow and regress. Given the infrequency of RS, precise mortality rates are difficult to establish. However, life expectancy is generally thought to be less than the general population. According to the IRSF (International Rett Syndrome Foundation) sudden death occurs in around 25% of RS patients, with studies speculating that possible causes could include respiratory failure and apnoea, owing to an underlying disorder in the heart’s electrical activity. Research suggests that RS is associated with a prolonged QT interval1 (a measure of the heart’s electrical activity). Boys born with RS usually die shortly after birth; as males have only one chromosome (XY) versus females (XX) and thus the disease is more fatal.
Sarizotan demonstrated utility in RS-related apnoea in animal models
Sarizotan is not being developed to address the underlying cause of RS but as a potential treatment for these life-threatening breathing disorders. Approximately 70% of patients with RS demonstrate respiratory abnormalities (eg apnoea, hyperventilation, respiratory dysrhythmia). It is postulated that the breathing disturbance in RS is related to neuronal hyperactivity in the brainstem. In preclinical studies, sarizotan has demonstrated reduced apnoea and corrected irregular breathing in RS mouse models. These data are shown in Exhibit 4. On the left, the RS mouse model shows recurring instances of apnoea, which are corrected when treated with sarizotan, with apnoea overall reduced by 70-85%. It is this profile which has encouraged Newron to pursue pivotal development of sarizotan in RS. Newron received sarizotan’s IND approval by FDA in May 2016.
Exhibit 4: Sarizotan reduced apnoea and breathing irregularities in preclinical studies
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STARS pivotal Phase III sarizotan study has begun
STARS (Sarizostan Treatment of Apneas in Rett Syndrome), a potentially pivotal clinical study to evaluate breathing disorders associated with RS has now begun; the first US study centre initiated is the Rush Medical Center, Chicago. STARS is a global study that will recruit around 129 RS patients (three groups of 43) aged 13 and over. Two doses of sarizotan will be investigated (5mg and 10mg, twice daily), which will be compared to placebo. Efficacy will be assessed via a measure of respiratory function (using an at-home monitor); the primary endpoint of the study is the reduction in the number of clinically significant apnoea (>10seconds) episodes at 24 weeks. After 24 weeks, all patients will be switched to receive sarizotan and will be followed for a further 48 weeks. Newron has sought advice from both regulators and key opinion leaders in the design of this study.
Although RS is a rare condition, diagnosed patients are generally included on patient registries and are known by patient advocacy groups and physicians who work in the RS field. Newron is working with these groups, in particular Rettsyndrome.com, which should help to facilitate recruitment of patients into the planned study. Given the study start date of July 2016 and allowing around six months for recruitment, top-line primary endpoint data (based on 24 weeks of treatment) could become available during the second half of 2017.
Given there is already a substantial safety database accumulated with prior development in PD, the planned 129-patient study could be sufficient to obtain regulatory approvals, particularly given the lack of available treatments in this indication. Our forecasts assume first approval in the US during H218, with launch shortly thereafter, with sarizotan potentially eligible for accelerated review given the unmet medical need.
Given the small size of the indication, we continue to assume that Newron will commercialise sarizotan alone in key markets, including the US and major European countries. We have made no changes to our €260m peak sales forecast, which is based on pricing of €60,000 a year, reflecting the ultra-orphan indication and assumes a 40% penetration of the targeted patients (which we assume is a quarter of the overall market). Pricing and penetration will ultimately depend on sarizotan’s magnitude of benefit; if it can command pricing of €80,000 a year with 70% penetration of our assumed target market (one quarter of RS patients) this would suggest peak sales of around €600m.
