The Content Presented at the 13th Clinical Trials on Alzheimer’s Disease (CTAD) Conference

 

Sysmex Corporation (HQ: Kobe, Japan; Chairman and CEO: Hisashi Ietsugu; “Sysmex”) and Eisai Co., Ltd. (HQ: Tokyo, Japan; CEO: Haruto Naito; “Eisai”) announced that the most recent data from the project to develop a method of diagnosing Alzheimer’s disease (AD) using blood plasma was presented at the 13th Clinical Trials on Alzheimer’s Disease (CTAD) conference, held virtually from November 4 to 7, 2020. Sysmex demonstrated on behalf of the two companies the performance of the amyloid beta (Aβ) in plasma measured on Sysmex’s HISCL^TM?fully automated immunoassay analyzers in predicting amyloid pathology as defined by amyloid positron emission tomography (PET) imaging on the centiloid scale.¹

 

The total number of those living with dementia across the world is projected to reach 82 million in 2030 and 152 million in 2050, with the total global societal cost of dementia stemming from direct medical and social care costs and lower productivity being estimated to reach 2 trillion USD in 2030.⁶?In Japan, the number of those with dementia is thought to have reached approximately 4.62 million in 2012 and is projected to grow to 7.30 million in 2025⁷, with the total societal cost of this disease being estimated to be equivalent to 4.1%⁸?of the gross domestic product (GDP) in 2025 (25.8 trillion yen⁹). Of these sufferers, those living with AD are thought to account for more than 60% of those living with dementia.⁷

It is conceivable that AD is a disease that results in synaptic dysfunction and neuronal cell death due to tau deposition in neurons triggered by Aβ aggregation on the outside of neurons. These brain changes cause cognitive impairment and psychological and behavioral symptoms, suggesting that the Aβ aggregation and accumulation inside the brain is caused by AD before the presence of cognitive impairment appears, thus, it is believed that early diagnosis and early intervention is more effective in therapies targeting Aβ. Currently, amyloid PET and Aβ ratio in cerebrospinal fluid (CSF) are used for detecting amyloid aggregates in the brain, but this puts significant burden on patients in terms of access, costs, and their physical wellbeing.¹⁰

Sysmex and Eisai are working to create new diagnostic technologies for the prevention and treatment of dementia. Accordingly, the overarching aim is to contribute to the advancement of healthcare and improve the quality of life for those living with the disease and their families.

 

Terminology
1. A standardization scale for integration analysis of PET SUVR values as measured by different amyloid PET imaging probes.
2. Trained doctors qualitatively distinguish amyloid PET positive from amyloid negative subjects by visually reading images.
3. Klunk WE?et al, Alzheimer’s Dementia (2014)
4. Assesses how correlated two sets of data are based on two quantitative data distributions. For the purpose of this analysis, Spearman’s rank correlation coefficient (rs), which is a correlation index as determined by the rankings of the two variables, was calculated.
5. Schindler SE?et al, Neurology (2019)
6. World Alzheimer Report 2018
7. Promotion of Comprehensive Measures against Dementia, Ministry of Health, Labour and Welfare
8. Study on Economic Impact of Dementia in Japan, 2014 Health Labour Sciences Research Grant Annual Report
9. Estimated by Sysmex based on Japan’s Medium-term Economic Outlook (February 2018), Daiwa Institute of Research
10. Aβ is a peptide made of amino-acid residues removed from amyloid precursor protein. Many of them are Aβ_1-40, which is comprised of 40-residues, and the Aβ_1-40?level does not fluctuate significantly as AD progresses. Comprised of 42-residues, Aβ_1-42, on the other hand, is highly cohesive and decreases in cerebrospinal fluid (CSF) from the early stages of AD. It is believed that Aβ’s absolute values show individual and intrinsic variability but that the plasma Aβ_1-42/Aβ_1-40?ratio remains unchanged. It has also been reported that the plasma Aβ_1-42/Aβ_1-40?ratio in CSF shows a high correlation with amyloid PET.

About the collaboration between Sysmex and Eisai

In February 2016, Sysmex and Eisai signed a comprehensive non-exclusive agreement aimed at the development of new diagnostic tests in the field of dementia. By leveraging each other’s technologies and knowledge, the objective has been to discover next-generation diagnostic reagents that will enable early diagnosis of dementia, selection of the most appropriate treatment options, and regular monitoring of the effects of such treatments. At the 12th CTAD held in December 2019, the two companies reported on the performance of the plasma Aβ ratio measured on a fully automated immunoassay system HISCL in predicting the amyloid PET scan results (sensitivity: 73%, specificity: 71% [AUC = 0.74]), thus demonstrating the potential to predict amyloid pathology in the brain using the plasma Aβ ratio.^*?This finding was expected to lead to the development of a simple method of diagnosing Alzheimer’s disease using blood.
^*https://www.sysmex.co.jp/en/news/2019/191209.html

https://www.eisai.com/news/2019/news201990.html

 

Contacts for inquiries
Sysmex Corporation
IR & Corporate Communication
Tel：078-265-0500

Eisai Co., Ltd.
Public Relations Department
Tel：03-3817-5120

Information contained in the press release is current as of the date of the announcement but may be subject to change without prior notice.

Eisai Co., Ltd. (Headquarters: Tokyo, CEO: Haruo Naito, “Eisai”) announced today that the latest information on its in-house discovered and developed eribulin mesylate (halichondrin class microtubule dynamics inhibitor, product name: HALAVEN^?, “eribulin”) will be presented during the 42nd San Antonio Breast Cancer Symposium (SABCS2019). The symposium will be held from December 10 through 14, 2019, in San Antonio, Texas in the United States.

A total of five poster presentations will be given at this year’s SABCS including the study results evaluating absolute lymphocyte count at the baseline with eribulin as a predictor of overall survival from the post-hoc analysis of two Phase III clinical studies of eribulin in patients with advanced or metastatic breast cancer.

Eisai positions oncology as a key therapeutic area, and is aiming to discover revolutionary new medicines with the potential to cure cancer. Eisai will continue to create innovation in the development of new drugs based on cutting-edge cancer research, as it seeks to contribute further to addressing the diverse needs of, and increasing the benefits provided to, patients with cancer, their families, and healthcare providers.

Major poster presentations at SABCS2019:

Product, Poster No.	Title and scheduled presentation date (local time: Central Standard Time)
Eribulin Poster no.: P2-15-13	A Time-and-Motion Study of Chemotherapy Administration in Metastatic Breast Cancer December 12 (Thu), 7:00-9:00AM
Eribulin Poster no.: P4-10-08	Absolute lymphocyte count (ALC) is a predictor of eribulin benefit in advanced or metastatic breast cancer (MBC) December 13 (Fri), 7:00-9:00AM
Eribulin Poster no.: P5-05-03	Eribulin treatment activates type 1 IFNs to promote a gene expression signature associated with antitumor immunity December 13 (Fri), 5:00-7:00PM
Eribulin Poster no.: P6-07-02	Evaluating the effects of eribulin and paclitaxel on exosome formation and release from triple negative breast cancer cells December 14 (Sat), 7:00-9:00AM
Eribulin Poster no.: OT2-09-01	A multicenter, randomized, phase II trial evaluating the efficacy of eribulin monotherapy and eribulin plus endocrine therapy in locally-recurrent or metastatic breast cancer patients after progression on endocrine therapy (REVERT study) December 12 (Thu), 5:00-7:00PM

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Eisai Co., Ltd.
+81-(0)3-3817-5120

Eisai Co., Ltd. (Headquarters: Tokyo, CEO: Haruo Naito, “Eisai”) has announced that LENVIMA (generic name: lenvatinib), the orally available kinase inhibitor discovered by Eisai, has been accepted by the National Medical Products Administration of China for an application for the additional indication of differentiated thyroid cancer. This application for additional indication marks the second in China following the indication for hepatocellular carcinoma, which was approved in September 2018.

This application was mainly based on the results of the SELECT Study (Study 303)¹conducted globally for patients with radioactive iodine-refractory differentiated thyroid cancer. In the SELECT study, LENVIMA demonstrated a statistically significant extension in progression-free survival (PFS), which is the primary endpoint, compared to placebo (median PFS in the LENVIMA group: 18.3 months, median PFS in the placebo group: 3.6 months; Hazard Ratio 0.21 [99% CI: 0.14-0.31]; p<0.001). ?Eisai could submit this application earlier by utilizing the results of SELECT study, while local Phase III clinical trial (Study 308) evaluating LENVIMA in patients with radioactive iodine-refractory differentiated thyroid cancer is ongoing in China.

In China, approximately 190,000 new cases of thyroid cancer are diagnosed each year, and approximately 8,600 are likely to die annually.²?Although treatment is possible for most types of thyroid cancer, there are few treatment options available once thyroid cancer has progressed, therefore it remains a disease with significant unmet medical needs.

Eisai positions oncology as a key therapeutic area, and is aiming to discover revolutionary new medicines with the potential to cure cancer. Eisai is committed to exploring the potential clinical benefits of LENVIMA, as it seeks to contribute further to addressing the diverse needs of, and increasing the benefits provided to, cancer patients, their families, and healthcare providers.

* In March 2018, Eisai and Merck & Co., Inc., Kenilworth, N.J., U.S.A. (known as MSD outside the United States and Canada), through an affiliate, entered into a strategic collaboration for the worldwide co-development and co-commercialization of LENVIMA.

Eisai China Inc. (hereinafter referred to as “Eisai China”) successfully held the launch meeting of Fycompa? (perampanel) in China on December 1, 2019, which marks the official launch of the new third-generation antiepileptic drug of Fycompa^??in China. This means that the first non-competitive AMPA receptor antagonist is officially ushered in the field of epilepsy treatment in China, which will bring new treatment methods and means for the majority of patients with epilepsy and their families.

At the Fycompa? launch meeting in China, Mr. Okada Yasushi, the Executive Officer of Eisai Co., Ltd., the Chairman of Eisai China Holdings Ltd. and Eisai China Inc., said, “First of all, I would like to welcome the experts and scholars who are here and teachers from nearly 200 epilepsy centers who are watching this meeting online to participate in the launching meeting of Fycompa in China and the following academic discussion. Eisai regards neuroscience, including epilepsy, as a key therapeutic area. With the approval and official launch of Fycompa^??in China, Eisai China will also officially enter the antiepileptic market from now on, benefiting epilepsy patients in China. In keeping with the mission of freeing numerous epilepsy patients from epilepsy, Eisai is committed to meeting the diverse needs of epilepsy patients and their families, and improving their well-being.”

Mr. Okada Yasushi delivered a welcome speech

It is learned that Fycompa^??has been granted priority status by the National Medical Products Administration since the application for new drug listing was submitted in September 2018 on the basis that it has significant clinical benefits compared with existing treatment methods. About 12 months later, namely on September 29, 2019, the National Medical Products Administration approved the import license of the new drug of Eisai, Fycompa?, which is applicable to additional treatment of partial onset seizures (with or without secondary generalized seizures) in epilepsy adults and children aged 12 and above.

Fycompa^??launching ceremony

Epilepsy is a chronic non-communicable disease of the brain that affects approximately 50 million people worldwide, making it one of the most common neurological diseases around the world. The disease is characterized by recurrent attacks. During an epileptic seizure, patients present a temporary involuntary convulsion of a part or whole of the body (i.e., partial or general seizure), and sometimes accompanied by loss of consciousness and incontinence. About 9 million people in China suffer from epilepsy, 60% of whom are affected by partial seizures, and 40% of those require additional treatment. In addition, the disease of about 30% of epilepsy patients can’t be controlled with existing antiepileptic drugs. Epilepsy is a disease with great medical needs which have not yet been met.?

Fycompa^??is an innovative antiepileptic drug developed by the Eisai Tsukuba Research Institute, with dosage and administration of oral administration, once daily. This drug is a highly selective, non-competitive AMPA-type receptor antagonist that can reduce the over-excitation of neurons associated with epilepsy attack via targeted inhibition of glutamate activity of the post-synaptic membrane AMPA receptor. Fycompa? has currently received Class A recommendation for the combination therapy of refractory epilepsy with partial seizures (TRAFE) for adults in the 2018 AAN / AES guidelines.

Venue of Fycompa^??launch meeting in China

Fycompa^??has been approved in more than 60 countries worldwide for the additional treatment of partial onset seizures (with or without secondary generalized seizures) in epilepsy patients aged 12 and above. In addition, Fycompa? has been approved in 55 countries worldwide for the additional treatment of primary generalized tonic-clonic seizures in epilepsy patients aged 12 years and above. In the United States, Fycompa? has been approved for monotherapy and additional treatment of partial onset seizures (with or without secondary generalized seizures) in children aged 4 and above.

With the launch of Fycompa? in China, Eisai China will further strengthen the leadership position in the field of neuroscience based on more than 35 years of drug development experience in neuroscience and the philosophy of “human health care (hhc)” aiming at “giving first thought to patients and their families, and increasing the benefits health care provides”, which has been rooted in China for more than 25 years.

While continuously introducing new drugs and providing disease solutions, we also provide long-term communication and learning platforms to medical professionals, build bridges for the latest medical information exchange at home and abroad, and present rich disease management experience and cutting-edge academic progress. Eisai China is willing to join hands with all walks of life to promote the attention and development of the entire Chinese society in the field of neuroscience.

Eisai Co., Ltd. (Headquarters: Tokyo, CEO: Haruo Naito, “Eisai”) announced today that the latest data on its antiepileptic drug (AED) perampanel (product name: Fycompa^?) will be presented at the 73rd American Epilepsy Society Annual Meeting (AES 2019) to be held from December 6 to December 10, 2019 in Baltimore, Maryland in the United States.

Thirty-Eight poster presentations will be given by Eisai at AES 2019, including results of a Phase III clinical study (FREEDOM / Study 342) to assess efficacy and safety of perampanel monotherapy for untreated patients from 12 to 74 years of age with partial onset seizures and results of a retrospective Phase IV study (Study 506) of perampanel in real-world clinical care of patients with epilepsy. Including Investigator Initiated Studies, more than 40 scientific posters on perampanel will be presented at AES 2019.

Perampanel is a first-in-class AED and a once-daily tablet discovered at Eisai’s Tsukuba Research Laboratories. In the United States and Europe, a new oral suspension formulation has been approved and is being marketed. The agent is a highly selective, noncompetitive AMPA receptor antagonist that reduces neuronal hyperexcitation by targeting glutamate activity at AMPA receptors on postsynaptic membranes. Perampanel is currently approved in countries around the world as an adjunctive therapy for the treatment of partial-onset seizures (with or without secondarily generalized seizures) and primary generalized tonic-clonic seizures in patients with epilepsy 12 years of age and older. Furthermore, perampanel is also indicated for monotherapy and adjunctive use in the treatment of partial-onset seizures (with or without secondarily generalized seizures) in patients with epilepsy 4 years of age and older in the United States.

Eisai considers neurology including epilepsy, a therapeutic area of focus, and strives to deliver perampanel throughout the world in pursuit of our mission to provide “seizure freedom” to a greater number of patients living with epilepsy. Eisai seeks to address the diverse needs of, as well as increasing the benefits provided to, patients with epilepsy and their families.

 

Major Poster Presentations for perampanel:

 

Media Inquiries:
Public Relations Department,
Eisai Co., Ltd.
+81-(0)3-3817-5120

 

[Notes to editors]
1. About Fycompa (perampanel)
Fycompa is a first-in-class AED discovered and developed by Eisai. With epileptic seizures being mediated by the neurotransmitter glutamate, the agent is a highly selective, noncompetitive AMPA receptor antagonist that reduces neuronal hyperexcitation associated with seizures by targeting glutamate activity at AMPA receptors on postsynaptic membranes. Fycompa is available in tablet form to be taken once daily orally at bedtime. In addition, an oral suspension formulation has been approved and marketed in the United States and in Europe. To date, Fycompa has been used to treat more than 270,000 patients worldwide across all indications.

Fycompa is currently approved in more than 65 countries and territories, including the United States, Japan, China, in Europe and in Asia as adjunctive treatment for partial-onset seizures (with or without secondarily generalized seizures) in patients with epilepsy 12 years of age and older. In addition, Fycompa has been approved in more than 60 countries, including the United States, Japan, in Europe and in Asia for treatment as an adjunctive therapy for primary generalized tonic clonic seizures in patients with epilepsy 12 years of age and older. In the United States, Fycompa is also indicated for monotherapy and adjunctive use in the treatment of partial-onset seizures (with or without secondarily generalized seizures) in patients with epilepsy 4 years of age and older.

In Japan, a supplementary new drug application has been filed seeking approval of Fycompa for use as monotherapy for partial-onset seizures, treatment for partial-onset seizures in pediatric patients aged 4 years and older, as well as a fine granule formulation. In Europe, an application has been submitted seeking the additional approval of Fycompa for adjunctive use in the treatment of partial-onset seizures (with or without secondarily generalized seizures) or primarily generalized tonic-clonic seizures in pediatric patients with epilepsy.

Furthermore, Eisai is conducting a global Phase III clinical study (Study 338) for the agent in patients with seizures associated with Lennox-Gastaut syndrome.