Your search keyword '"Lauren E Bleakley"' showing total 12 results

1. Loss‐of‐function variants in Kv11.1 cardiac channels as a biomarker for SUDEP

Author

Ming S. Soh, Richard D. Bagnall, Mark F. Bennett, Lauren E. Bleakley, Erlina S. Mohamed Syazwan, A. Marie Phillips, Mathew D. F. Chiam, Chaseley E. McKenzie, Michael Hildebrand, Douglas Crompton, Melanie Bahlo, Christopher Semsarian, Ingrid E. Scheffer, Samuel F. Berkovic, and Christopher A. Reid

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571, Neurology. Diseases of the nervous system, RC346-429

Abstract

Abstract Objective To compare the frequency and impact on the channel function of KCNH2 variants in SUDEP patients with epilepsy controls comprising patients older than 50 years, a group with low SUDEP risk, and establish loss‐of‐function KCNH2 variants as predictive biomarkers of SUDEP risk. Methods We searched for KCNH2 variants with a minor allele frequency of 20% reduction in maximal amplitude, were observed in 8.9% (8/90) SUDEP patients compared to 3.3% (11/332) epilepsy controls suggesting about threefold enrichment (nominal p = 0.04). KCNH2 variants that did not change channel function occurred at a similar frequency in SUDEP (2.2%; 2/90) and epilepsy control (2.7%; 9/332) cohorts (p > 0.99). Rare KCNH2 variants (

Published

2021

2. Retinal Dysfunction in a Mouse Model of HCN1 Genetic Epilepsy

Author

Da Zhao, Paulo Pinares-Garcia, Chaseley E. McKenzie, Lauren E. Bleakley, Ian C. Forster, Vickie H.Y. Wong, Christine T.O. Nguyen, Ingrid E. Scheffer, Christopher A. Reid, and Bang V. Bui

Subjects

General Neuroscience

Abstract

Pathogenic variants inHCN1are associated with a range of epilepsy syndromes including a developmental and epileptic encephalopathy. The recurrentde novo HCN1pathogenic variant (M305L) results in a cation leak, allowing the flux of excitatory ions at potentials where the wild-type channels are closed. The Hcn1M294Lmouse recapitulates patient seizure and behavioral phenotypes. As HCN1 channels are highly expressed in rod and cone photoreceptor inner segments, where they shape the light response, mutated channels are likely to impact visual function. Electroretinogram (ERG) recordings from male and female mice Hcn1M294Lmice revealed a significant decrease in the photoreceptor sensitivity to light, as well as attenuated bipolar cell (P2) and retinal ganglion cell responses. Hcn1M294Lmice also showed attenuated ERG responses to flickering lights. ERG abnormalities are consistent with the response recorded from a single female human subject. There was no impact of the variant on the structure or expression of the Hcn1 protein in the retina.In silicomodeling of photoreceptors revealed that the mutated HCN1 channel dramatically reduced light-induced hyperpolarization, resulting in more Ca2+flux during the response when compared with the wild-type situation. We propose that the light-induced change in glutamate release from photoreceptors during a stimulus will be diminished, significantly blunting the dynamic range of this response. Our data highlight the importance of HCN1 channels to retinal function and suggest that patients withHCN1pathogenic variants are likely to have a dramatically reduced sensitivity to light and a limited ability to process temporal information.SIGNIFICANCE STATEMENTPathogenic variants in HCN1 are emerging as an important cause of catastrophic epilepsy. HCN1 channels are ubiquitously expressed throughout the body, including the retina. Electroretinogram recordings from a mouse model ofHCN1genetic epilepsy showed a marked decrease in the photoreceptor sensitivity to light and a reduced ability to respond to high rates of light flicker. No morphologic deficits were noted. Simulation data suggest that the mutated HCN1 channel blunts light-induced hyperpolarization and consequently limits the dynamic range of this response. Our results provide insights into the role HCN1 channels play in retinal function as well as highlighting the need to consider retinal dysfunction in disease caused byHCN1variants. The characteristic changes in the electroretinogram open the possibility of using this tool as a biomarker for this HCN1 epilepsy variant and to facilitate development of treatments.

Published

2023

3. Are Variants Causing Cardiac Arrhythmia Risk Factors in Sudden Unexpected Death in Epilepsy?

Author

Lauren E. Bleakley, Ming S. Soh, Richard D. Bagnall, Lynette G. Sadleir, Samuel Gooley, Christopher Semsarian, Ingrid E. Scheffer, Samuel F. Berkovic, and Christopher A. Reid

Subjects

sudden unexpected death in epilepsy, epilepsy, cardiac arrhythmia, genetics, ion channels, common variants, Neurology. Diseases of the nervous system, RC346-429

Abstract

Sudden unexpected death in epilepsy (SUDEP) is the most common cause of premature mortality in individuals with epilepsy. Acute and adaptive changes in heart rhythm in epilepsy implicate cardiac dysfunction as a potential pathogenic mechanism in SUDEP. Furthermore, variants in genes associated with Long QT syndrome (LQTS) have been identified in patients with SUDEP. LQTS is a cardiac arrhythmia condition that causes sudden cardiac death with strong similarities to SUDEP. Here, we discuss the possibility of an additive risk of death due to the functional consequences of a pathogenic variant in an LQTS gene interacting with seizure-mediated changes in cardiac function. Extending this general concept, we propose a hypothesis that common variants in LQTS genes, which cause a subtle impact on channel function and would not normally be considered risk factors for cardiac disease, may increase the risk of sudden death when combined with epilepsy. A greater understanding of the interaction between epilepsy, cardiac arrhythmia, and SUDEP will inform our understanding of SUDEP risk and subsequent potential prophylactic treatment.

Published

2020

4. Using a Multiplex Nucleic Acid in situ Hybridization Technique to Determine HCN4 mRNA Expression in the Adult Rodent Brain

Author

Julia Oyrer, Lauren E. Bleakley, Kay L. Richards, Snezana Maljevic, A. Marie Phillips, Steven Petrou, Cameron J. Nowell, and Christopher A. Reid

Subjects

HCN4 channels, HCN1 channel, HCN2, multiplex nucleic acid in situ hybridization, Ih, quantifcation workflow, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Hyperpolarization-activated cyclic nucleotide-gated (HCN) channels carry a non-selective cationic conductance, Ih, which is important for modulating neuron excitability. Four genes (HCN1-4) encode HCN channels, with each gene having distinct expression and biophysical profiles. Here we use multiplex nucleic acid in situ hybridization to determine HCN4 mRNA expression within the adult mouse brain. We take advantage of this approach to detect HCN4 mRNA simultaneously with either HCN1 or HCN2 mRNA and markers of excitatory (VGlut-positive) and inhibitory (VGat-positive) neurons, which was not previously reported. We have developed a Fiji-based analysis code that enables quantification of mRNA expression within identified cell bodies. The highest HCN4 mRNA expression was found in the habenula (medial and lateral) and the thalamus. HCN4 mRNA was particularly high in the medial habenula with essentially no co-expression of HCN1 or HCN2 mRNA. An absence of Ih-mediated “sag” in neurons recorded from the medial habenula of knockout mice confirmed that HCN4 channels are the predominant subtype in this region. Analysis in the thalamus revealed HCN4 mRNA in VGlut2-positive excitatory neurons that was always co-expressed with HCN2 mRNA. In contrast, HCN4 mRNA was undetectable in the nucleus reticularis. HCN4 mRNA expression was high in a subset of VGat-positive cells in the globus pallidus external. The majority of these neurons co-expressed HCN2 mRNA while a smaller subset also co-expressed HCN1 mRNA. In the striatum, a small subset of large cells which are likely to be giant cholinergic interneurons co-expressed high levels of HCN4 and HCN2 mRNA. The amygdala, cortex and hippocampus expressed low levels of HCN4 mRNA. This study highlights the heterogeneity of HCN4 mRNA expression in the brain and provides a morphological framework on which to better investigate the functional roles of HCN4 channels.

Published

2019

5. Cation leak: a common functional defect causing HCN1 developmental and epileptic encephalopathy

Author

Chaseley E McKenzie, Ian C Forster, Ming S Soh, A Marie Phillips, Lauren E Bleakley, Sophie J Russ-Hall, Kenneth A Myers, Ingrid E Scheffer, and Christopher A Reid

Subjects

Cellular and Molecular Neuroscience, Psychiatry and Mental health, Neurology, Biological Psychiatry

Abstract

Pathogenic variants in HCN1 are an established cause of developmental and epileptic encephalopathy (DEE). To date, the stratification of patients with HCN1-DEE based on the biophysical consequence on channel function of a given variant has not been possible. Here, we analysed data from eleven patients carrying seven different de novo HCN1 pathogenic variants located in the transmembrane domains of the protein. All patients were diagnosed with severe disease including epilepsy and intellectual disability. The functional properties of the seven HCN1 pathogenic variants were assessed using two-electrode voltage-clamp recordings in Xenopus oocytes. All seven variants showed a significantly larger instantaneous current consistent with cation leak. The impact of each variant on other biophysical properties was variable, including changes in the half activation voltage and activation and deactivation kinetics. These data suggest that cation leak is an important pathogenic mechanism in HCN1-DEE. Furthermore, published mouse model and clinical case reports suggest that seizures are exacerbated by sodium channel blockers in patients with HCN1 variants that cause cation leak. Stratification of patients based on their ‘cation leak’ biophysical phenotype may therefore provide key information to guide clinical management of individuals with HCN1-DEE.

Published

2023

6. Efficacy of antiseizure medication in a mouse model of HCN1 developmental and epileptic encephalopathy

Author

Lauren E. Bleakley, Chaseley E. McKenzie, and Christopher A. Reid

Subjects

Neurology, Neurology (clinical)

Abstract

Acquisition of drug-sensitivity profiles is challenging in rare epilepsies. Anecdotal evidence suggests that antiseizure medications that block sodium channels as their primary mechanism of action exacerbate seizures in HCN1 developmental and epileptic encephalopathies (DEEs), whereas sodium valproate is effective for some patients. The Hcn1 M294L heterozygous knock-in (Hcn1

Published

2022

7. Loss‐of‐function variants in Kv11.1 cardiac channels as a biomarker for SUDEP

Author

Christopher A. Reid, Christopher Semsarian, Samuel F. Berkovic, A. Marie Phillips, Richard D. Bagnall, Lauren E Bleakley, Erlina S Mohamed Syazwan, Mathew D. F. Chiam, Chaseley E McKenzie, Melanie Bahlo, Mark F. Bennett, Douglas E. Crompton, Michael S. Hildebrand, Ingrid E. Scheffer, and Ming S Soh

Subjects

0301 basic medicine, Oncology, Male, ERG1 Potassium Channel, Cohort Studies, Epilepsy, Xenopus laevis, 0302 clinical medicine, Sudden Unexpected Death in Epilepsy, Child, Research Articles, Aged, 80 and over, education.field_of_study, General Neuroscience, Middle Aged, Cohort, Biomarker (medicine), Female, RC321-571, Research Article, Adult, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, Adolescent, Population, Neurosciences. Biological psychiatry. Neuropsychiatry, Maximal amplitude, 03 medical and health sciences, Young Adult, Internal medicine, medicine, Animals, Humans, RC346-429, education, Allele frequency, Loss function, Aged, business.industry, Genetic Variation, Infant, medicine.disease, Minor allele frequency, 030104 developmental biology, Neurology. Diseases of the nervous system, Neurology (clinical), business, 030217 neurology & neurosurgery, Biomarkers

Abstract

Objective To compare the frequency and impact on the channel function of KCNH2 variants in SUDEP patients with epilepsy controls comprising patients older than 50 years, a group with low SUDEP risk, and establish loss‐of‐function KCNH2 variants as predictive biomarkers of SUDEP risk. Methods We searched for KCNH2 variants with a minor allele frequency of 20% reduction in maximal amplitude, were observed in 8.9% (8/90) SUDEP patients compared to 3.3% (11/332) epilepsy controls suggesting about threefold enrichment (nominal p = 0.04). KCNH2 variants that did not change channel function occurred at a similar frequency in SUDEP (2.2%; 2/90) and epilepsy control (2.7%; 9/332) cohorts (p > 0.99). Rare KCNH2 variants (

Published

2021

8. The hyperpolarization‐activated cyclic nucleotide‐gated 4 channel as a potential anti‐seizure drug target

Author

Andreas Ludwig, Lauren E Bleakley, Christopher A. Reid, Liang Jin, Linghan Jia, Emma Morrisroe, Steven Petrou, Joseph A. Nicolazzo, Qays Kharouf, A. Marie Phillips, Julia Oyrer, M. Novella Romanelli, and Elisabetta Cerbai

Subjects

0301 basic medicine, Central nervous system, Cyclic Nucleotide-Gated Cation Channels, Biology, Mice, 03 medical and health sciences, Bursting, Epilepsy, 0302 clinical medicine, Seizures, Hyperpolarization-Activated Cyclic Nucleotide-Gated Channels, Biological neural network, medicine, Animals, Electrocorticography, Ion channel, Pharmacology, medicine.diagnostic_test, Hyperpolarization (biology), medicine.disease, Research Papers, 030104 developmental biology, medicine.anatomical_structure, Pharmaceutical Preparations, Knockout mouse, Nucleotides, Cyclic, Neuroscience, 030217 neurology & neurosurgery

Abstract

BACKGROUND AND PURPOSE: Hyperpolarization-activated Cyclic Nucleotide-gated (HCN) channels are encoded by four genes (HCN1-4) with distinct biophysical properties and functions within the brain. HCN4 channels activate slowly at robust hyperpolarizing potentials, making them more likely to be engaged during hyperexcitable neuronal network activity seen during seizures. HCN4 channels are also highly expressed in thalamic nuclei, a brain region implicated in seizure generalisation. Here we assessed the utility of targeting the HCN4 channel as an anti-seizure strategy using pharmacological and genetic approaches. EXPERIMENTAL APPROACH: The impact of reducing HCN4 channel function on seizure susceptibility and neuronal network excitability was studied using a HCN4 channel preferring blocker (EC18) and a conditional brain specific HCN4 knockout mouse model. KEY RESULTS: EC18 (10mg kg-1 ) and brain-specific HCN4 channel knockout reduced seizure susceptibility and proconvulsant-mediated cortical spiking recorded using electrocorticography, with minimal effects on other mouse behaviours. EC18 (10μM) decreased neuronal network bursting in mouse cortical cultures. Importantly, EC18 was not protective against proconvulsant-mediated seizures in the conditional HCN4 channel knockout mouse and did not reduce bursting behaviour in AAV-HCN4 shRNA infected mouse cortical cultures. CONCLUSIONS AND IMPLICATIONS: These data suggest the HCN4 channel as a potential pharmacologically relevant target for anti-seizure drugs that is likely to have a low side-effect liability in the central nervous system.

Published

2020

9. Altered EEG power spectrum, but not sleep-wake architecture, in HCN1 knockout mice

Author

Lauren E. Bleakley, Ryan J. Keenan, Rachel D. Graven, Jeremy A. Metha, Sherie Ma, Heather Daykin, Linda Cornthwaite-Duncan, Daniel Hoyer, Christopher A. Reid, and Laura H. Jacobson

Subjects

Mice, Knockout, Mice, Behavioral Neuroscience, Potassium Channels, Hyperpolarization-Activated Cyclic Nucleotide-Gated Channels, Animals, Sleep, REM, Electroencephalography, Wakefulness, Sleep

Abstract

Sleep is a complex biological state characterized by large populations of neurons firing in a rhythmic or synchronized manner. HCN channels play a critical role in generating and sustaining synchronized neuronal firing and are involved in the actions of anaesthetics. However, the role of these channels in sleep-wakefulness per se has yet to be studied. We conducted polysomnographic recordings of Hcn1 constitutive knockout (Hcn1 KO) and wild-type (WT) mice in order to investigate the potential role of HCN1 channels in sleep/wake regulation. EEG and EMG data were analysed using the Somnivore™ machine learning algorithm. Time spent in each vigilance state, bout number and duration, and EEG power spectral activity were compared between genotypes. There were no significant differences in the time spent in wake, rapid eye movement (REM) or non-REM (NREM) sleep between Hcn1 KO and WT mice. Wake bout duration during the inactive phase was significantly shorter in Hcn1 KO mice whilst no other bout parameters were affected by genotype. Hcn1 KO mice showed a reduction in overall EEG power which was particularly prominent in the theta (5-9 Hz) and alpha (9-15 Hz) frequency bands and most evident during NREM sleep. Together these data suggest that HCN1 channels do not play a major role in sleep architecture or modulation of vigilance states. However, loss of these channels significantly alters underlying neuronal activity within these states which may have functional consequences.

Published

2023

10. Loss-of-function variants in the cardiac Kv11.1 channel as a genetic biomarker for SUDEP

Author

Phillips Am, Melanie Bahlo, Lauren E Bleakley, Chaseley E McKenzie, Christopher Semsarian, Syazwan Esm, Ingrid E. Scheffer, Richard D. Bagnall, Chiam, Douglas E. Crompton, Ming S Soh, Michael S. Hildebrand, Christopher A. Reid, Mark F. Bennett, and Samuel F. Berkovic

Subjects

Oncology, medicine.medical_specialty, business.industry, Maximal amplitude, medicine.disease, Minor allele frequency, Epilepsy, Internal medicine, Cohort, medicine, Biomarker (medicine), business, Allele frequency, Loss function, Predictive biomarker

Abstract

ObjectiveTo compare the frequency and impact on channel function of KCNH2 variants in SUDEP patients with epilepsy controls comprising patients older than 50 years, a group with low SUDEP risk, and establish loss-of-function KCNH2 variants as predictive biomarkers of SUDEP risk.MethodsWe searched for KCNH2 variants with a minor allele frequency of < 5%. Functional analysis in Xenopus laevis oocytes was performed for all KCNH2 variants identified.ResultsKCNH2 variants were found in 11.1% (10/90) of SUDEP individuals compared to 6.0% (20/332) of epilepsy controls (p = 0.11). Loss-of-function KCNH2 variants, defined as causing > 20% reduction in maximal amplitude, were observed in 8.9% (8/90) SUDEP patients compared to 3.3% (11/332) epilepsy controls suggesting about three-fold enrichment (nominal p = 0.04). KCNH2 variants that did not change channel function occurred at a similar frequency in SUDEP (2.2%; 2/90) and epilepsy control (2.7%; 9/332) cohorts (p > 0.99). Rare KCNH2 variants (< 1% allele frequency) associated with greater loss of function and an ∼11-fold enrichment in the SUDEP cohort (nominal p = 0.03). In silico tools were unable to predict the impact of a variant on function highlighting the need for electrophysiological analysis.ConclusionsThese data show that loss-of-function KCNH2 variants are enriched in SUDEP patients and suggest that cardiac mechanisms contribute to SUDEP risk. We propose that genetic screening in combination with functional analysis can identify loss-of-function KCNH2 variants that could act as biomarkers of an individual’s SUDEP risk.

Published

2021

11. Cation leak underlies neuronal excitability in an HCN1 developmental and epileptic encephalopathy

Author

Ian C. Forster, Leonid Churilov, Samuel F. Berkovic, Snezana Maljevic, Ingrid E. Scheffer, Nikola Jancovski, Ming S Soh, Bina Santoro, Anirudh Kathirvel, Lauren E Bleakley, Christopher A. Reid, Alicia Sedo, Paulo Pinares-Garcia, Chaseley E McKenzie, and Steven Petrou

Subjects

0301 basic medicine, Male, Potassium Channels, Action potential, Biology, Somatosensory system, 03 medical and health sciences, Epilepsy, Mice, Xenopus laevis, 0302 clinical medicine, medicine, Hyperpolarization-Activated Cyclic Nucleotide-Gated Channels, Animals, Membrane potential, Neurons, Brain Diseases, Dentate gyrus, Pyramidal Cells, Depolarization, medicine.disease, Resting potential, Mice, Mutant Strains, Disease Models, Animal, 030104 developmental biology, Rheobase, Mutation, Female, Neurology (clinical), Neuroscience, 030217 neurology & neurosurgery

Abstract

Pathogenic variants in HCN1 are associated with developmental and epileptic encephalopathies. The recurrent de novo HCN1 M305L pathogenic variant is associated with severe developmental impairment and drug-resistant epilepsy. We engineered the homologue Hcn1 M294L heterozygous knock-in (Hcn1M294L) mouse to explore the disease mechanism underlying an HCN1 developmental and epileptic encephalopathy. The Hcn1M294L mouse recapitulated the phenotypic features of patients with the HCN1 M305L variant, including spontaneous seizures and a learning deficit. Active epileptiform spiking on the electrocorticogram and morphological markers typical of rodent seizure models were observed in the Hcn1M294L mouse. Lamotrigine exacerbated seizures and increased spiking, whereas sodium valproate reduced spiking, mirroring drug responses reported in a patient with this variant. Functional analysis in Xenopus laevis oocytes and layer V somatosensory cortical pyramidal neurons in ex vivo tissue revealed a loss of voltage dependence for the disease variant resulting in a constitutively open channel that allowed for cation ‘leak’ at depolarized membrane potentials. Consequently, Hcn1M294L layer V somatosensory cortical pyramidal neurons were significantly depolarized at rest. These neurons adapted through a depolarizing shift in action potential threshold. Despite this compensation, layer V somatosensory cortical pyramidal neurons fired action potentials more readily from rest. A similar depolarized resting potential and left-shift in rheobase was observed for CA1 hippocampal pyramidal neurons. The Hcn1M294L mouse provides insight into the pathological mechanisms underlying hyperexcitability in HCN1 developmental and epileptic encephalopathy, as well as being a preclinical model with strong construct and face validity, on which potential treatments can be tested.

Published

2020

12. Using a Multiplex Nucleic Acid in situ Hybridization Technique to Determine HCN4 mRNA Expression in the Adult Rodent Brain

Author

Lauren E Bleakley, Snezana Maljevic, Julia Oyrer, A. Marie Phillips, Christopher A. Reid, Cameron J. Nowell, Kay L. Richards, and Steven Petrou

Subjects

0301 basic medicine, HCN1 channel, Hippocampus, multiplex nucleic acid in situ hybridization, In situ hybridization, Striatum, Biology, Ih, lcsh:RC321-571, 03 medical and health sciences, Cellular and Molecular Neuroscience, 0302 clinical medicine, medicine, HCN2, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Molecular Biology, Original Research, Messenger RNA, HCN4 channels, quantifcation workflow, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Globus pallidus, Habenula, nervous system, Neuron, Nucleus, 030217 neurology & neurosurgery, Neuroscience

Abstract

Hyperpolarization-activated cyclic nucleotide-gated (HCN) channels carry a non-selective cationic conductance, I h , which is important for modulating neuron excitability. Four genes (HCN1-4) encode HCN channels, with each gene having distinct expression and biophysical profiles. Here we use multiplex nucleic acid in situ hybridization to determine HCN4 mRNA expression within the adult mouse brain. We take advantage of this approach to detect HCN4 mRNA simultaneously with either HCN1 or HCN2 mRNA and markers of excitatory (VGlut-positive) and inhibitory (VGat-positive) neurons, which was not previously reported. We have developed a Fiji-based analysis code that enables quantification of mRNA expression within identified cell bodies. The highest HCN4 mRNA expression was found in the habenula (medial and lateral) and the thalamus. HCN4 mRNA was particularly high in the medial habenula with essentially no co-expression of HCN1 or HCN2 mRNA. An absence of I h -mediated "sag" in neurons recorded from the medial habenula of knockout mice confirmed that HCN4 channels are the predominant subtype in this region. Analysis in the thalamus revealed HCN4 mRNA in VGlut2-positive excitatory neurons that was always co-expressed with HCN2 mRNA. In contrast, HCN4 mRNA was undetectable in the nucleus reticularis. HCN4 mRNA expression was high in a subset of VGat-positive cells in the globus pallidus external. The majority of these neurons co-expressed HCN2 mRNA while a smaller subset also co-expressed HCN1 mRNA. In the striatum, a small subset of large cells which are likely to be giant cholinergic interneurons co-expressed high levels of HCN4 and HCN2 mRNA. The amygdala, cortex and hippocampus expressed low levels of HCN4 mRNA. This study highlights the heterogeneity of HCN4 mRNA expression in the brain and provides a morphological framework on which to better investigate the functional roles of HCN4 channels.

Published

2019