Day 1 :
Keynote Forum
Horacio Kaufmann
New York University School of Medicine, USA
Keynote: Efficacy, durability and safety of ampreloxetine, a norepinephrine reuptake inhibitor, given once daily to treat neurogenic orthostatic hypotension (nOH) in subjects with primary autonomic failure
Time : 09:40-10:20
Biography:
Horacio Kaufmann is Professor of Neurology, Medicine and Pediatrics and holds the Axelrod Chair for Neurological Research at New York University School of Medicine where he also Heads the Division of Autonomic Disorders and the Dysautonomia Center at NYU Langone Health. He received his Medical Degree from the National University of Buenos Aires, Argentina. He trained in Internal Medicine and completed Neurology residency and fellowship at Mount Sinai School of Medicine in New York City. His research focuses on the autonomic nervous system and its abnormalities in neurological disorders. His research is funded by the National Institute of Health (NIH, NINDS), the US Food and Drug Administration (FDA), The Michael J. Fox Foundation,The MSA Coalition and the Dysautonomia Foundation, Inc.
Abstract:
Background: The neurogenic orthostatic hypotension (nOH) is due to failure of the autonomic nervous system to adequately increase synaptic norepinephrine to maintain upright blood pressure (BP). Norepinephrine reuptake inhibitors (NRI) could augment local synaptic concentrations of tonically released norepinephrine, resulting in increased BP and reduced symptoms of OH. Ampreloxetine is a novel NRI being investigated for the treatment of symptomatic nOH.
Methods: This was a phase 2 multicenter, single and multiple-dose study of subjects with nOH. After a single dose escalation phase, responders were enrolled in an open label phase, treated with ampreloxetine taken orally once daily for up to 20 weeks, and followed for 4 weeks thereafter. The primary endpoint was the improvement from baseline in the validated symptom questionnaire OHSA#1 on day 29.
Results: 21 subjects were enrolled (mean age 64yrs), 16(76%) completed day 29. The mean [SD] improvement from baseline in OHSA#1 was 2.4[4.5] in all subjects and 3.8[3.1] in symptomatic subjects (OSHA#1 >4 at baseline). OHSA and OHDAS composite scores improved by 1.0(2.8) and 1.1(2.9), respectively. The most frequently reported adverse events (AE) were urinary tract infection (24%), hypertension (19%) and headache (14%). 2(10%) discontinued treatment due to AE and 5(24%) reported SAEs, none considered related to the study medication.
Conclusion: In subjects with nOH, ampreloxetine demonstrated clinically meaningful improvements in OHSA#1, OHSA and OHDAS composite scores at week 4. Th e improvement in OHSA#1 was maintained through week 20, with a regression to baseline levels during the 4 week follow-up. Ampreloxetine was generally well-tolerated.
Keynote Forum
Amin Hajitou
Imperial College London, UK
Keynote: Bacteriophage: From applications in infectious diseases to targeted delivery systems for brain tumours through the blood-brain barrier
Time : 10:20-11:00
Biography:
Amin Hajitou completed his PhD at the University of Liege, Belgium, where he acquired extensive experience in delivery technologies for therapeutic nucleic acids. Then he did his Postdoctoral training in the world leading MD-Anderson Cancer Center in Texas-USA, where he gained expertise in bacteriophage
(phage)-guided gene delivery and phage display technologies in vitro and in vivo. Importantly, he designed a novel hybrid phage vector for targeted nucleic acid transfer to cancer. The hybrid phage, published in Cell 2006, showed first success of systemic gene targeting to cancer in vivo. His team and independent groups reported efficacy of intravenous cancer gene therapy in rodents and pet dogs with naturally occurring cancers. In 2008, he established his research team, as a Lecturer, at Imperial College, then became Senior Lecturer in 2013 and Reader in 2016. His research team has become a leading authority in phage-guided delivery systems to cancer including brain tumours. His leadership in the field has resulted in various awards for his research and a Royal Decoration by his Majesty the King of Morocco, in 2015.
Abstract:
Current treatments for brain tumours have faced major challenges including lack of tumour selectivity and the bloodbrain barrier (BBB). Development of a selective delivery system for brain tumours would play a major advance in the treatment of these tumours. For instance, successful exploitation of numerous therapeutic agents depends, essentially on the development of non-invasive nucleic acid delivery platforms. Indeed, gene therapy is promising in this disease and brain tumours were the first to be treated by clinical gene therapy but success has been limited by the inefficiency of vectors and by the BBB. We have used bacteriophage (phage), bacteria virus, to develop tumour targeted systemic vectors. Phages have a historic safety profile as they have been administered to human over many years to treat infectious diseases. Importantly, the filamentous M13 phage is able to traverse the BBB. However, phage has no strategies to deliver genes to human cells. We reported a bacteriophage vector, as hybrid genome between two single-stranded DNA of human adenoassociated virus (AAV) and filamentous M13 phage, termed AAV phage or AAVP, in which gene expression is under the control of AAV genome. We and independent groups reported efficacy of selective intravenous cancer gene therapy, with the RGD4C-AAVP displaying RGD4C ligand to target the tumour specifi c αvβ3 integrin receptor. To validate our systemic delivery platform for brain tumours, we showed the ability of the phage vector administered intravenously to home selectively to human glioblastoma (GBM), in preclinical models, through the BBB by binding the αvβ3 integrin, subsequently delivering a recombinant rAAV genome that delivers a suicide gene therapy in tumour cells, angiogenic endothelial cells and GBM-derived stem cells. Combination with a low dose of temozolomide (TMZ) enhanced gene delivery/therapy by using a tumour specific promoter from an endogenous gene associated with GBM resistance to TMZ chemotherapy. These findings provide evidence that bacteriophage is a promising delivery platform for use in targeted treatment in neuro-oncology.
Keynote Forum
Manoj Malhotra
Eisai Inc., USA
Keynote: Perampanel in real-world clinical care of patients with epilepsy: Retrospective phase IV study 506 – third interim analysis
Time : 11:20-12:00
Biography:
Manoj Malhotra received his Medical Degree from Wayne State University in Detroit, Michigan. He completed his Neurology residency and two fellowships at The Cleveland Clinic in Cleveland, Ohio. He is the Vice President, Head of Medical Affairs for the Neurology Business Group at Eisai Inc. He is responsible for Medical Affairs activities for the Americas and is Global Medical Lead for Epilepsy. He holds six neurology board certifications (neurology, epilepsy, sleep medicine, clinical neurophysiology, vascular neurology and electrodiagnostic medicine) and has extensive experience in neurodegenerative diseases, rare diseases and epilepsy. His industry experience includes working at Novartis, Takeda and Mallinckrodt.
Abstract:
Perampanel is a once-daily oral anti-seizure drug for partial-onset seizures and primary generalised tonic-clonic seizures. We report the second interim analysis of the multicentre, non-interventional, Phase IV retrospective Study 506 (NCT03208660), to assess retention rate, safety and dosing experience of perampanel administered to patients with epilepsy during routine clinical care. Data were obtained from medical records of patients initiating perampanel after 1 January 2014. Primary endpoint is retention rate (proportion of patients remaining on perampanel; Safety Analysis Set [SAS]). Safety, effi cacy and dosing experience are secondary objectives. Th e interim SAS comprised 605 patients (55.9% female). At data cut-off (5 March 2018), 317 (52.4%) patients remained on perampanel; 285 (47.1%) had discontinued, primarily due to adverse event (AE; n=157 [26.0%]) and inadequate therapeutic effect (n=86 [14.2%]). Mean (standard deviation [SD]) cumulative duration of exposure to perampanel was 15.4 (13.9) months. Mean (SD) maximum perampanel dose was 6.5 (3.2) mg. Retention rates at 3, 6, 12, 18 and 24 months were 80.2% (n=479/597), 69.0% (n=392/568), 58.1% (n=288/496), 52.7% (n=216/410) and 49.8% (n=154/309), respectively. At Months 22-24: median reduction in seizure frequency per 28 days was 93.3% (n=27); 50% responder rate was 77.8% (n=21/27); 40.7% (n=11/27) of patients achieved seizure freedom. Treatment-emergent AEs (TEAEs) occurred in 304 (50.2%) patients, including dizziness (10.2%), aggression (6.1%) and irritability (5.0%). Serious TEAEs occurred in 14 (2.3%) patients, including 3 (0.5%) deaths. Favourable retention rates and sustained efficacy of perampanel for ≤2 years were demonstrated in patients with epilepsy treated during routine clinical care.
- Neurology | Pediatric Neurology | Neurogenetic and Neurometabolic Disorders | Neuro Cardiology & Strokes | Clinical Trails & Case Reports | Neuropathology | Clinical Neurophysiology | Neurological Diseases
Location: London, UK
Chair
William C. L. Stewart
The Abigail Wexner Research Institute at Nationwide Children’s Hospital, USA
Co-Chair
Nihar Ranjan Haldar
Nobel Medical College Teaching Hospital, Nepal
Session Introduction
Leock Y. Ngo
Eisai Inc., USA
Title: Safety and efficacy of adjunctive perampanel in paediatric patients (aged 4 to Ë‚12 years) with partialonset seizures (POS) or primary generalised tonic-clonic seizures (PGTCS): Final results from the 311 core study
Time : 12:00-12:30
Biography:
Leock Y. Ngo has a PhD in Pharmaceutical Sciences from the University of Alberta, Canada and was a Postdoctoral Research Fellow at the University of Washington in Seattle, Washington. Stella is Director in Clinical Research at Eisai Inc., responsible for the development of new anti-epilepsy drugs. She is the International Project Lead for Fycompa® and Inovelon®, and the Clinical Lead for new chemical entities in early development for epilepsy treatment. Before joining Eisai, Stella gained 19+ years’ experience in clinical pharmacology and clinical trials across various therapeutic areas, including neurology (Alzheimer’s disease and peripheral neuropathy), oncology, pulmonology and autoimmune/infl ammatory disorders.
Abstract:
Perampanel is a once-daily oral anti-seizure drug for POS and PGTCS. Study 311 (NCT02849626) is a global, multicentre, open-label, single-arm study assessing the safety, tolerability, pharmacokinetics and efficacy of oncedaily
adjunctive perampanel oral suspension in patients aged 4 to <12 years with POS (with/without secondarily generalised seizures [SGS]) or PGTCS. We report safety, tolerability and efficacy data from the 311 Core Study. This study included a 4-week Pre-treatment Period, 23-week Treatment Period and 4-week Follow-up Period. Primary endpoints were safety and tolerability. Secondary endpoints included median percent change in seizure frequency
per 28 days from Baseline during the Treatment Period, and 50% responder and seizure-freedom rates during Maintenance (Core Study) and longer-term treatment (≤52 weeks). In total, 180 patients (POS, n=149; PGTCS, n=31) received ≥1 perampanel dose (mean age [standard deviation], 8.1 [2.09] years; female, 48.9%); 146 (81.1%) patients completed the Core Study and 34 (18.9%) discontinued. Adverse events (AEs) were the primary reason for discontinuation (n=14 [7.8%]). Median (minimum, maximum) dose of perampanel was 8.0 (2, 16) mg/day and duration of exposure was 22.9 (0, 27) weeks. Treatment-emergent AEs in ≥10% of patients were: somnolence, nasopharyngitis, dizziness, irritability, pyrexia and vomiting. Median percent reduction in seizure frequency per 28 days from Baseline, 50% responder rates and seizure-freedom rates, respectively, were: POS: 40.1%, 46.6% and 11.5%; PGTCS: 69.2%, 63.6% and 54.5%; SGS: 58.7%, 64.8% and 18.5%. Adjunctive perampanel was generally safe, well tolerated and efficacious in children aged 4 to <12 years with POS, SGS or PGTCS.
Shahid Aziz Mian
King Fahad Medical City, Saudi Arabia
Title: Clinical exome sequencing of patients from a highly consanguineous population: Novel pathogenic variants impacting neurological function
Time : 12:30-13:00
Biography:
Shahid Mian is a Consultant Clinical Research Scientist, PhD within the Department of Pathology and Clinical Laboratory Medicine (PCLM) at King Fahad Medical City (KFMC), Saudi Arabia. PCLM is a College of American Pathologists (CAP) accredited laboratory. He has responsibility for establishing bioinformatic and variant reporting pipelines for the clinical exome analysis of paediatric patients with suspected inherited disorders. He has reviewed over 500 clinical exome reports produced by third party laboratories for PCLM, independently reported over 100 patient exome results to KFMC physicians and analysed over 1300 exomes bioinformatically.
Abstract:
Saudi Arabia has a highly consanguineous population with specific geographical regions estimated to have rates exceeding greater than 80%. The downstream effect of such population dynamics is to significantly enrich the
frequency at which recessive pathogenic variants occur and consequently their associated Mendelian disorders.This is evident at both a community and a family level. King Fahad Medical City (KFMC) is a tertiary care facility that diagnoses patients with inherited disorders through exome sequence analysis of germline DNA. Many of the biological pathways negatively impacted by these pathogenic changes manifest at a neurological level. These include for example intellectual disability, ataxia, epilepsy and white matter structural changes. The Department of Pathology and Clinical Laboratory Medicine (PCLM) has sequenced the exomes of over 1100 patients. Novel pathogenic variants in genes biologically and clinically linked to specific neurological conditions have been identified. Furthermore the PCLM knowledge base has also implicated novel genes with no known function, to a variety of neurological conditions. Evidence is presented at how genetic analysis of exome sequence data derived from patients orginating within highly consanguineous populations can lead to the identification of novel genes/genetic variants linked to neurological physiology.
Nihar Ranjan Haldar
Nobel Medical College Teaching Hospital, Nepal
Title: Diagnosing leprosy at its neuritic phase
Time : 13:00-13:30
Biography:
Nihar Ranjan Haldar is 60 years old and a resident of Siliguri, Darjeeling, India. He completed his M.B.B.S from Calcutta University in 1982, MD (Medicine) in 1987 and DM (Neurology) in 1990 from PGIMER Chandigarh. He Practicing Neurology in India, Nepal, Bhutan & Bangladesh for 27 years. He presently works as a Professor in the Department of Neurology at Nobel Medical College Teaching Hospital & Research Centre, Biratnagar, Nepal. He is also Director of Tenovus Research & Diagnostic Centre and Founder Director of Mrigna Centre for Epilepsy. Nihar Ranjan Haldar engaged in patient care, neuroelectrophysiology and research work. He presented and published his work in various Conferences and Journals. He is also member of Neurology Society of India, Association of Neuroscientist of Eastern India, Indian Academy of Neurology and American Academy of Neurology.
Abstract:
Introduction: Leprosy is known to common people including medical practitioners as a disfiguring contagious disease. Patients suffering from leprosy usually have ulcers, in the extremities loss of fingers, nasal tips and ear lobule if not treated. They go to dermatologist or laporalogists. Pathophysiology says it is an illness which affects nervous system i.e. peripheral sensory and motor nerves. Ulceration and disfiguring are secondary to trauma and later involvement of skin. It is a very common infective illness of nervous system if taken worldwide statistics (>200,000 new case per year). It is neglected by neurologist when patients present initially with neurological symptoms, it becomes obvious when skin is affected. Hypertrophic neuropathy is a common type of initial association which can be detected when first they present with minor neurological symptoms. Ultrasonography of nerves as a routine investigation tool is neglected in most of the places which could have identifi ed the disease. Assessment of hypertrophy or other pathologic changes by ultrasonic examination was practiced by us to detect enlargement of any kind.
Materials & Methods: We report 1200 consecutive cases, studied in patients from Nepal, India, Bhutan and Bangladesh. Patients were from neurology and dermatology clinics. High resolution Ultrasonography machine and 12 MHz linear transducer were used for the investigation. Hypoechoic nerves were subjected to aspiration cytology for detecting acid fast bacilli. Duration of study was from 2005 to 2018.
Results: From a total of 1200 cases, 75% had thickened nerves, 20% had doubtfully thickened nerves, 11% normal nerves, 3% cases showed nodularity and nerve abscess was seen in 2% cases; 43% had hypoechoic nerves; Aspiration cytology was done in 3323 hypoechoic nerves, of which 27% had granulomatous infl ammation, 8% were AFB positive and 20% had no yield (Figures rounded).
Conclusion: It is true that all leprosy patients to start with are pure neuritic leprosy with sensory or motor symptoms. Early diagnosis is very important and obvious that doing ultrasonography of nerves is a very useful method to identify certain common group of peripheral nerves in medical practice, especially in tropical countries. Further development and practice in this regard needs to be done using high resolution ultrasonography machine and expert
personnel generation. Awareness among general physician and neurophysician are very much needed for early identifi cation of the disease.
Break: Lunch Break 13:30-14:30 @ RBG
William C. L. Stewart
The Abigail Wexner Research Institute at Nationwide Children’s Hospital, USA
Title: Malic enzyme 2 and genetic generalized epilepsy
Time : 14:30-15:00
Biography:
William C. L. Stewart has completed his PhD in Statistics from the University Washington in 2005, and finished his Postdoctoral studies in the Biostatistics Department at the University of Michigan in 2008. He is a Principal Investigator at the Abigail Wexner Research Institute of Nationwide Children’s Hospital. He is an Assistant Professor of Statistics and Pediatrics at Ohio State University. He has published more than 30 papers in peer-review journals and has served on the Editorial Board of Frontiers in Genetics for nine years.
Abstract:
Genetic generalized epilepsy (GGE) is a highly heritable condition (h2=66%) consisting of epileptic syndromes with overlapping symptoms. Previous studies (both linkage and association) identified malic enzyme 2 (ME2) as a candidate susceptibility gene for adolescent-onset GGE. To definitively test ME2’s infl uence on GGE, we used three different approaches. First, we compared a newly recruited GGE cohort with an ethnically matched reference sample from 1000 genomes, using an efficient test of association (POPFAM+). Second, in a previously collected data set, we replaced the original controls with ethnically matched reference samples to minimize the confounding effect of population stratification and we used POPFAM+ in the re-analysis. Third, in a post hoc analysis of healthy human pre-frontal cortex, we identified single nucleotide polymorphisms (SNPs) influencing ME2 messenger RNA (mRNA) expression and then, we tested those same SNPs for association with GGE in a large case control cohort. In the analysis of our newly-recruited GGE Cohort, we found a strong association between an ME2 SNP and GGE (p =0.0006 at rs608781). In the re-analysis of previously collected data, we confirmed the Greenberg et al., (2005) finding of a GGE associated ME2 risk haplotype. Finally, in the post hoc ME2 expression analysis, we found evidence for a possible link between GGE and ME2 gene expression in human brain. Overall, our research (and the research of others) provides compelling evidence that ME2 influences adolescent onset GGE susceptibility.
Abdulrahman O. Alharbi
Majmaah University, Saudi Arabia
Title: Incidence of stroke among diabetic nephropathypatients: A meta-analysis
Time : 15:00-15:30
Biography:
Abdulrahman Alharbi is currently working as an Assistant Professor of Neurology & Consultant Stroke Neurologist in the College of Medicine at Majmaah University.
Abstract:
Background and Objectives: The association of micro vascular complications (diabetic nephropathy) with the stroke is limited because it will require huge sample size of diabetic population with nephropathy and long follow-up period to see the association or development incidence of stroke among these patients. So, we conducted out this meta analysis of the existing studies to find out the incidence/ risk of stroke among diabetic nephropathy patients and, explore the association between stroke and proteinuria in a diabetic nephropathy population and to describe Does Degree of Proteinuria a Clinical Matter!! ?
Methods & Materials: We searched the existing databases from the year 1995 to August 2018 by using the MeSH terms. All cohorts, cross sectional studies were searched for, fulfilling the inclusion criteria and as per operational defi nitions. The quality assessment criterion for quality of studies was already predefined.
Study Result: Seven studies were found to be eligible for inclusion in the meta- analysis. The hazards or risk of stroke development among diabetic patients was 3.25 times higher in patients with nephropathy as compared to patients without nephropathy.
The pooled hazards ratio of 1.46 (95% CI=0.81-2.60) and of 1.65 (95% CI=0.53-5.11) among diabetic patients with micro albuminuria and macro albuminuria respectively.
Conclusion: Diabetic nephropathy patients have a higher incidence and risk of stroke compared to diabetic patients without nephropathy. This is the first meta-analysis which has included studies from January 1995 to August 2018 to the best of our knowledge which has tried to compare the risk/ hazard of stroke among diabetic patients with and with out nephropathy and sub-group analysis for micro and macro albuminuria.
Biography:
Manoj Malhotra received his Medical Degree from Wayne State University in Detroit, Michigan. He completed his Neurology residency and two fellowships at The Cleveland Clinic in Cleveland, Ohio. He is the Vice President, Head of Medical Affairs for the Neurology Business Group at Eisai Inc. He is responsible for Medical Affairs activities for the Americas and is Global Medical Lead for Epilepsy. He holds six neurology board certifications (neurology, epilepsy, sleep medicine, clinical neurophysiology, vascular neurology and electrodiagnostic medicine) and has extensive experience in neurodegenerative diseases, rare diseases and epilepsy. His industry experience includes working at Novartis, Takeda and Mallinckrodt.
Abstract:
Perampanel is given daily once orally as anti-seizure drug for partial-onset seizures (POS) and primary generalised tonic clonic seizures. We report second interim results for paediatric patients from the multicentre, non-interventional, Phase IV, retrospective study 506 (NCT03208660), to assess retention rate, safety and dosing experience of perampanel administered to patients with epilepsy during routine clinical care. Data were obtained from medical records of patients initiating perampanel after 1 January 2014. Primary endpoint is retention rate (proportion of patients in Safety Analysis Set [SAS] remaining on perampanel). Safety, efficacy and dosing experience are secondary objectives. Interim SAS comprised 605 patients; 68 were aged <12 years (mean age [standard deviation (SD)], 6.7[3.0] years). Seizure types included: complex partial, n=33 (48.5%); POS with secondary generalization, n=11(16.2%); generalized tonic-clonic, n=21 (30.9%). Mean (SD) cumulative duration of exposure to perampanel was 14.3(11.5) months and mean (SD) maximum perampanel dose was 5.4(3.2) mg. At data cut-off (5 March 2018),
34(50.0%) paediatric patients remained on perampanel 33(48.5%) had discontinued, primarily due to adverse event (AE; n=15 [22.1%]) and inadequate therapeutic effect (n=11 [16.2%]). Retention rates at 3, 6, 12, 18 and 24 months were 82.4% (n=56/68), 66.2% (n=43/65), 61.0% (n=36/59), 53.2% (n=25/47) and 48.6% (n=17/35), respectively. Treatment emergent AEs occurred in 39.7% of patients; most common were abnormal behavior, aggression and irritability (all 5.9%). This subgroup analysis suggests that daily oral doses of adjunctive perampanel are generally well tolerated, with favorable retention rates for ≤2 years in pediatric patients (<12 years) with epilepsy.
Break: Networking & Refreshments 16:00-16:20 @ Foyer
- Special Session
Location: London, UK
Session Introduction
Ann Ali Abdelkader Hanafy
Cairo University, Egypt
Title: Basics of electrophysiological assessments of enterapement neuropathies
Time : 16:20-17:20
Biography:
Ann Ali Abdelkader Hanafy has completed her MD at the age of 30 years from Cairo University and postdoctoral studies from Cairo University School of Medicine. She is a Professor of Clinical neurophysiology & the President of Egyptian Clinical Neurophysiology Society. She has published more than 100 papers in local and international journals.
Abstract:
Nerve compression syndrome or compression neuropathy, is a medical condition caused by direct pressure on a nerve. It is known colloquially as a trapped nerve, though this may also refer to nerve root compression (by a herniated disc, for example). Its symptoms include pain, tingling, numbness and muscle weakness. I will discuss the clinical presentation of various entrapment nerve sites and the value of nerve conductions and electromyography in the diagnosis of each one.