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2. Karawun: a software package for assisting evaluation of advances in multimodal imaging for neurosurgical planning and intraoperative neuronavigation.

Author

Beare, R, Alexander, B, Warren, A, Kean, M, Seal, M, Wray, A, Maixner, W, Yang, JY-M, Beare, R, Alexander, B, Warren, A, Kean, M, Seal, M, Wray, A, Maixner, W, and Yang, JY-M

Abstract

PURPOSE: The neuroimaging research community-which includes a broad range of scientific, medical, statistical, and engineering disciplines-has developed many tools to advance our knowledge of brain structure, function, development, aging, and disease. Past research efforts have clearly shaped clinical practice. However, translation of new methodologies into clinical practice is challenging. Anything that can reduce these barriers has the potential to improve the rate at which research outcomes can contribute to clinical practice. In this article, we introduce Karawun, a file format conversion tool, that has become a key part of our work in translating advances in diffusion imaging acquisition and analysis into neurosurgical practice at our institution. METHODS: Karawun links analysis workflows created using open-source neuroimaging software, to Brainlab (Brainlab AG, Munich, Germany), a commercially available surgical planning and navigation suite. Karawun achieves this using DICOM standards supporting representation of 3D structures, including tractography streamlines, and thus offers far more than traditional screenshot or color overlay approaches. RESULTS: We show that neurosurgical planning data, created from multimodal imaging data using analysis methods implemented in open-source research software, can be imported into Brainlab. The datasets can be manipulated as if they were created by Brainlab, including 3D visualizations of white matter tracts and other objects. CONCLUSION: Clinicians can explore and interact with the results of research neuroimaging pipelines using familiar tools within their standard clinical workflow, understand the impact of the new methods on their practice and provide feedback to methods developers. This capability has been important to the translation of advanced analysis techniques into practice at our institution.

Published
2023

3. Basal ganglia dysplasia and mTORopathy: A potential cause of postoperative seizures in focal cortical dysplasia

Author

Lee, WS, Macdonald-Laurs, E, Stephenson, SEM, D'Arcy, C, MacGregor, D, Leventer, RJ, Maixner, W, Harvey, AS, Lockhart, PJ, Lee, WS, Macdonald-Laurs, E, Stephenson, SEM, D'Arcy, C, MacGregor, D, Leventer, RJ, Maixner, W, Harvey, AS, and Lockhart, PJ

Abstract

Pathogenic somatic MTOR variants in the cerebral cortex are a frequent cause of focal cortical dysplasia (FCD). We describe a child with drug and surgery-resistant focal epilepsy due to FCD type II who developed progressive enlargement and T2 signal hyperintensity in the ipsilateral caudate and lentiform nuclei. Histopathology of caudate nucleus biopsies showed dysmorphic neurons, similar to those in resected cortex. Genetic analysis of frontal and temporal cortex and caudate nucleus identified a pathogenic somatic MTOR variant [NM_004958.4:c.4375G > C (p.Ala1459Pro)] that was not present in blood-derived gDNA. The mean variant allele frequency ranged from 0.4% to 3.2% in cerebral cortex and up to 5.4% in the caudate nucleus. The basal ganglia abnormalities suggest more widespread, potentially hemispheric dysplasia in this patient, consistent with the pathogenic variant occurring in early cerebral development. This finding provides a potential explanation for persistent seizures in some patients with seemingly complete resection of FCD or disconnection of a dysplastic hemisphere.

Published
2023

4. Assessment of intraoperative diffusion EPI distortion and its impact on estimation of supratentorial white matter tract positions in pediatric epilepsy surgery

Author

Yang, JY-M, Chen, J, Alexander, B, Schilling, K, Kean, M, Wray, A, Seal, M, Maixner, W, Beare, R, Yang, JY-M, Chen, J, Alexander, B, Schilling, K, Kean, M, Wray, A, Seal, M, Maixner, W, and Beare, R

Abstract

The effectiveness of correcting diffusion Echo Planar Imaging (EPI) distortion and its impact on tractography reconstruction have not been adequately investigated in the intraoperative MRI setting, particularly for High Angular Resolution Diffusion Imaging (HARDI) acquisition. In this study, we evaluated the effectiveness of EPI distortion correction using 27 legacy intraoperative HARDI datasets over two consecutive surgical time points, acquired without reverse phase-encoded data, from 17 children who underwent epilepsy surgery at our institution. The data was processed with EPI distortion correction using the Synb0-Disco technique (Schilling et al., 2019) and without distortion correction. The corrected and uncorrected b0 diffusion-weighted images (DWI) were first compared visually. The mutual information indices between the original T1-weighted images and the fractional anisotropy images derived from corrected and uncorrected DWI were used to quantify the effect of distortion correction. Sixty-four white matter tracts were segmented from each dataset, using a deep-learning based automated tractography algorithm for the purpose of a standardized and unbiased evaluation. Displacement was calculated between tracts generated before and after distortion correction. The tracts were grouped based on their principal morphological orientations to investigate whether the effects of EPI distortion vary with tract orientation. Group differences in tract distortion were investigated both globally, and regionally with respect to proximity to the resecting lesion in the operative hemisphere. Qualitatively, we observed notable improvement in the corrected diffusion images, over the typically affected brain regions near skull-base air sinuses, and correction of additional distortion unique to intraoperative open cranium images, particularly over the resection site. This improvement was supported quantitatively, as mutual information indices between the FA and T1-weighted images w

Published
2022

5. Women in pediatric neurosurgery

Author

Ocal, E., Kim, E.E., Niquen-Jimenez, M., Salibe de Oliveira, G., Bakhti, S., Bhattacharjee, S., Coelho, G., Maixner, W., Messing-Jünger, M., Taghlit, N., and Zanon, N.

Subjects
pediatric, Woman, education, neurosurgery
Abstract

Pediatric neurosurgery is an ever-evolving field, and at the heart of it are talented and hardworking neurosurgeons who harness technology and research to enhance the standard of neurosurgical care for children. Recent studies have found that female neurosurgeons tend to choose a career focused on pediatric neurosurgery more than other subspecialties. However, the achievements and contributions of women in pediatric neurosurgery are not well known. To address this, an international working group of pediatric neurosurgeons was established from the World Federation of Neurosurgical Societies (WFNS) Women in Neurosurgery (WINS) group and Pediatric Neurosurgery Committee. The working group reviewed the current literature and collected information through personal communications with the global WINS network. Despite the increasing number of women entering neurosurgical training, the number of female pediatric neurosurgeons is still a mere handful worldwide. In this article, the authors summarize the current status of female pediatric neurosurgeons across the globe, highlighting their achievements as well as the gender bias and challenges that they face at every level of progression of their career. A better organized pediatric neurosurgery workforce, with more female representation and mentorship, would encourage future generations of diverse genders toward a career in this field.

Published
2022

7. Rationale, design, and methods of a randomized, controlled, open-label clinical trial with open-label extension to investigate the safety of vosoritide in infants, and young children with achondroplasia at risk of requiring cervicomedullary decompression surgery

Author

Savarirayan, R., Irving, M., Maixner, W., Thompson, D., Offiah, A.C., Connolly, D.J.A., Raghavan, A., Powell, J., Kronhardt, M., Jeha, G., Ghani, S., Fisheleva, E., and Day, J.R.S.

Subjects
musculoskeletal diseases
Abstract

Achondroplasia causes narrowing of the foramen magnum and the spinal canal leading to increased mortality due to cervicomedullary compression in infants and significant morbidity due to spinal stenosis later in adulthood. Vosoritide is a C-natriuretic peptide analogue that has been shown to improve endochondral ossification in children with achondroplasia. The objective of this trial is to evaluate the safety of vosoritide and whether vosoritide can improve the growth of the foramen magnum and spinal canal in children that may require decompression surgery. An Achondroplasia Foramen Magnum Score will be used to identify infants at risk of requiring decompression surgery. This is a 2-year open label randomized controlled trial of vosoritide in infants with achondroplasia ages 0 to ≤12 months. Approximately 20 infants will be randomized 1:1 to either open label once daily subcutaneous vosoritide combined with standard of care or standard of care alone. The primary and secondary aims of the study are to evaluate the safety and efficacy of vosoritide in children with cervicomedullary compression at risk of requiring decompression surgery. The trial will be carried out in specialized skeletal dysplasia treatment centers with well established multidisciplinary care pathways and standardized approaches to the neurosurgical management of cervicomedually compression. After 2 years, infants randomized to standard of care alone will be eligible to switch to vosoritide plus standard of care for an additional 3 years. This pioneering trial hopes to address the important question as to whether treatment with vosoritide at an early age in infants at risk of requiring cervicomedullary decompression surgery is safe, and can improve growth at the foramen magnum and spinal canal alleviating stenosis. This in turn may reduce compression of surrounding structures including the neuraxis and spinal cord, which could alleviate future morbidity and mortality.

Published
2021

8. Progress in neurosurgery: Contributions of women neurosurgeons in Asia and Australasia.

Author

Shrestha R., Olson S., Phusoongnern W., Yan L., Rosseau G., Drummond K.J., Kim E.E., Apuahe E., Darbar A., Kedia S., Kuo M.-F., Lewis E., Lucena L.L.N., Maixner W., Mo S.M., Shrestha R., Olson S., Phusoongnern W., Yan L., Rosseau G., Drummond K.J., Kim E.E., Apuahe E., Darbar A., Kedia S., Kuo M.-F., Lewis E., Lucena L.L.N., Maixner W., and Mo S.M.

Abstract

At the end of the first 100 years of neurosurgery as a specialty, it is appropriate to look back and then imagine the future. As neurosurgery celebrates its first century, the increasing role of women neurosurgeons is a major theme. This article documents the early women pioneers in neurosurgery in Asia and Australasia. The contributions of these trailblazers to the origins, academics, and professional organizations of neurosurgery are highlighted. The first woman neurosurgeon of the region, Dr. T.S. Kanaka of India, completed her training in 1968, not long after the trailblazers in Europe and North America. She heralded the vibrant communities of neurosurgical women that have developed in the vast and diverse nations of the region, and the many formal and informal groups of women in neurosurgery that have introduced and promoted talented women in the profession. Contributions of women neurosurgeons to academic medicine and society as a whole are briefly highlighted, as are their challenges in this male-dominated specialty. The region is home to many deeply conservative societies; in fact, some nations in the region have not yet trained their first woman neurosurgeon. The fortitude of these individuals to achieve at the highest levels of neurosurgery indicates great potential for future growth of women in the profession, but also demonstrates the need for initiatives and advocacy to reach the full potential of gender equity.Copyright © 2021 Elsevier Ltd

Published
2021

9. Cerebrospinal fluid liquid biopsy for detecting somatic mosaicism in brain

Author

Ye, Z, Chatterton, Z, Pflueger, J, Damiano, JA, McQuillan, L, Harvey, AS, Malone, S, Do, H, Maixner, W, Schneider, A, Nolan, B, Wood, M, Lee, WS, Gillies, G, Pope, K, Wilson, M, Lockhart, PJ, Dobrovic, A, Scheffer, IE, Bahlo, M, Leventer, RJ, Lister, R, Berkovic, SF, Hildebrand, MS, Ye, Z, Chatterton, Z, Pflueger, J, Damiano, JA, McQuillan, L, Harvey, AS, Malone, S, Do, H, Maixner, W, Schneider, A, Nolan, B, Wood, M, Lee, WS, Gillies, G, Pope, K, Wilson, M, Lockhart, PJ, Dobrovic, A, Scheffer, IE, Bahlo, M, Leventer, RJ, Lister, R, Berkovic, SF, and Hildebrand, MS

Abstract

Brain somatic mutations are an increasingly recognized cause of epilepsy, brain malformations and autism spectrum disorders and may be a hidden cause of other neurodevelopmental and neurodegenerative disorders. At present, brain mosaicism can be detected only in the rare situations of autopsy or brain biopsy. Liquid biopsy using cell-free DNA derived from cerebrospinal fluid has detected somatic mutations in malignant brain tumours. Here, we asked if cerebrospinal fluid liquid biopsy can be used to detect somatic mosaicism in non-malignant brain diseases. First, we reliably quantified cerebrospinal fluid cell-free DNA in 28 patients with focal epilepsy and 28 controls using droplet digital PCR. Then, in three patients we identified somatic mutations in cerebrospinal fluid: in one patient with subcortical band heterotopia the LIS1 p. Lys64* variant at 9.4% frequency; in a second patient with focal cortical dysplasia the TSC1 p. Phe581His*6 variant at 7.8% frequency; and in a third patient with ganglioglioma the BRAF p. Val600Glu variant at 3.2% frequency. To determine if cerebrospinal fluid cell-free DNA was brain-derived, whole-genome bisulphite sequencing was performed and brain-specific DNA methylation patterns were found to be significantly enriched (P = 0.03). Our proof of principle study shows that cerebrospinal fluid liquid biopsy is valuable in investigating mosaic neurological disorders where brain tissue is unavailable.

Published
2021

10. Cerebrospinal fluid liquid biopsy for detecting somatic mosaicism in brain (vol 3, fcaa235, 2021)

Author

Ye, Z, Chatterton, Z, Pflueger, J, Damiano, JA, McQuillan, L, Harvey, AS, Malone, S, Do, H, Maixner, W, Schneider, A, Nolan, B, Wood, M, Lee, WS, Gillies, G, Pope, K, Wilson, M, Lockhart, PJ, Dobrovic, A, Scheffer, IE, Bahlo, M, Leventer, RJ, Lister, R, Berkovic, SF, Hildebrand, MS, Ye, Z, Chatterton, Z, Pflueger, J, Damiano, JA, McQuillan, L, Harvey, AS, Malone, S, Do, H, Maixner, W, Schneider, A, Nolan, B, Wood, M, Lee, WS, Gillies, G, Pope, K, Wilson, M, Lockhart, PJ, Dobrovic, A, Scheffer, IE, Bahlo, M, Leventer, RJ, Lister, R, Berkovic, SF, and Hildebrand, MS

Abstract

[This corrects the article DOI: 10.1093/braincomms/fcaa235.][This corrects the article DOI: 10.1093/braincomms/fcaa235.].

Published
2021

11. Rationale, design, and methods of a randomized, controlled, open-label clinical trial with open-label extension to investigate the safety of vosoritide in infants, and young children with achondroplasia at risk of requiring cervicomedullary decompression surgery

Author

Savarirayan, R, Irving, M, Maixner, W, Thompson, D, Offiah, AC, Connolly, DJA, Raghavan, A, Powell, J, Kronhardt, M, Jeha, G, Ghani, S, Fisheleva, E, Day, JRS, Savarirayan, R, Irving, M, Maixner, W, Thompson, D, Offiah, AC, Connolly, DJA, Raghavan, A, Powell, J, Kronhardt, M, Jeha, G, Ghani, S, Fisheleva, E, and Day, JRS

Abstract

Achondroplasia causes narrowing of the foramen magnum and the spinal canal leading to increased mortality due to cervicomedullary compression in infants and significant morbidity due to spinal stenosis later in adulthood. Vosoritide is a C-natriuretic peptide analogue that has been shown to improve endochondral ossification in children with achondroplasia. The objective of this trial is to evaluate the safety of vosoritide and whether vosoritide can improve the growth of the foramen magnum and spinal canal in children that may require decompression surgery. An Achondroplasia Foramen Magnum Score will be used to identify infants at risk of requiring decompression surgery. This is a 2-year open label randomized controlled trial of vosoritide in infants with achondroplasia ages 0 to ≤12 months. Approximately 20 infants will be randomized 1:1 to either open label once daily subcutaneous vosoritide combined with standard of care or standard of care alone. The primary and secondary aims of the study are to evaluate the safety and efficacy of vosoritide in children with cervicomedullary compression at risk of requiring decompression surgery. The trial will be carried out in specialized skeletal dysplasia treatment centers with well established multidisciplinary care pathways and standardized approaches to the neurosurgical management of cervicomedually compression. After 2 years, infants randomized to standard of care alone will be eligible to switch to vosoritide plus standard of care for an additional 3 years. This pioneering trial hopes to address the important question as to whether treatment with vosoritide at an early age in infants at risk of requiring cervicomedullary decompression surgery is safe, and can improve growth at the foramen magnum and spinal canal alleviating stenosis. This in turn may reduce compression of surrounding structures including the neuraxis and spinal cord, which could alleviate future morbidity and mortality.Trial registrations: ClinicalTri

Published
2021

12. Gradient of brain mosaic RHEB variants causes a continuum of cortical dysplasia

Author

Lee, WS, Baldassari, S, Chipaux, M, Adle-Biassette, H, Stephenson, SEM, Maixner, W, Harvey, AS, Lockhart, PJ, Baulac, S, Leventer, RJ, Lee, WS, Baldassari, S, Chipaux, M, Adle-Biassette, H, Stephenson, SEM, Maixner, W, Harvey, AS, Lockhart, PJ, Baulac, S, and Leventer, RJ

Abstract

Focal cortical dysplasia (FCD) and hemimegalencephaly (HME) are related malformations with shared etiologies. We report three patients with a spectrum of cortical malformations associated with pathogenic brain-specific somatic Ras homolog enriched in brain (RHEB) variants. The somatic variant load directly correlated with the size of the malformation, with upregulated mTOR activity confirmed in dysplastic tissues. Laser capture microdissection showed enrichment of RHEB variants in dysmorphic neurons and balloon cells. Our findings support the role of RHEB in a spectrum of cortical malformations confirming that FCD and HME represent a disease continuum, with the extent of dysplastic brain directly correlated with the somatic variant load.

Published
2021

13. Pituitary function in paediatric survivors of severe traumatic brain injury

Author

Poomthavorn, P., Maixner, W., and Zacharin, M.

Subjects
Pituitary diseases -- Risk factors, Pituitary diseases -- Demographic aspects, Pituitary diseases -- Research, Pituitary-adrenal function tests -- Usage, Pituitary-adrenal function tests -- Research, Brain -- Injuries, Brain -- Patient outcomes, Brain -- Demographic aspects, Brain -- Complications and side effects, Brain -- Research
Published
2008

14. Genetic characterization identifies bottom-of-sulcus dysplasia as an mTORopathy

Author

Lee, WS, Stephenson, SEM, Pope, K, Gillies, G, Maixner, W, Macdonald-Laurs, E, MacGregor, D, D'Arcy, C, Jackson, G, Harvey, AS, Leventer, RJ, Lockhart, PJ, Lee, WS, Stephenson, SEM, Pope, K, Gillies, G, Maixner, W, Macdonald-Laurs, E, MacGregor, D, D'Arcy, C, Jackson, G, Harvey, AS, Leventer, RJ, and Lockhart, PJ

Abstract

OBJECTIVE: To determine the genetic basis of bottom-of-sulcus dysplasia (BOSD), which is a highly focal and epileptogenic cortical malformation in which the imaging, electrophysiologic, and pathologic abnormalities are maximal at the bottom of sulcus, tapering to a normal gyral crown. METHODS: Targeted panel deep sequencing (>500×) was performed on paired blood and brain-derived genomic DNA from 20 operated patients with drug-resistant focal epilepsy and BOSD. Histopathology was assessed using immunohistochemistry. RESULTS: Brain-specific pathogenic somatic variants were found in 6 patients and heterozygous pathogenic germline variants were found in 2. Somatic variants were identified in MTOR and germline variants were identified in DEPDC5 and NPRL3. Two patients with somatic MTOR variants showed a mutation gradient, with higher mutation load at the bottom of sulcus compared to the gyral crown. Immunohistochemistry revealed an abundance of dysmorphic neurons and balloon cells in the bottom of sulcus but not in the gyral crown or adjacent gyri. CONCLUSIONS: BOSD is associated with mTOR pathway dysregulation and shares common genetic etiologies and pathogenic mechanisms with other forms of focal and hemispheric cortical dysplasia, suggesting these disorders are on a genetic continuum.

Published
2020

17. Second-hit DEPDC5 mutation is limited to dysmorphic neurons in cortical dysplasia type IIA

Author

Lee, WS, Stephenson, SEM, Howell, KB, Pope, K, Gillies, G, Wray, A, Maixner, W, Mandelstam, SA, Berkovic, SF, Scheffer, IE, MacGregor, D, Harvey, AS, Lockhart, PJ, Leventer, RJ, Lee, WS, Stephenson, SEM, Howell, KB, Pope, K, Gillies, G, Wray, A, Maixner, W, Mandelstam, SA, Berkovic, SF, Scheffer, IE, MacGregor, D, Harvey, AS, Lockhart, PJ, and Leventer, RJ

Abstract

Focal cortical dysplasia (FCD) causes drug-resistant epilepsy and is associated with pathogenic variants in mTOR pathway genes. How germline variants cause these focal lesions is unclear, however a germline + somatic "2-hit" model is hypothesized. In a boy with drug-resistant epilepsy, FCD, and a germline DEPDC5 pathogenic variant, we show that a second-hit DEPDC5 variant is limited to dysmorphic neurons, and the somatic mutation load correlates with both dysmorphic neuron density and the epileptogenic zone. These findings provide new insights into the molecular and cellular correlates of FCD determining drug-resistant epilepsy and refine conceptualization of the epileptogenic zone.

Published
2019

18. Optic Radiation Tractography in Pediatric Brain Surgery Applications: A Reliability and Agreement Assessment of the Tractography Method

Author

Yang, JY-M, Beare, R, Wu, MH, Barton, SM, Malpas, CB, Yeh, C-H, Harvey, AS, Anderson, V, Maixner, W, Seal, M, Yang, JY-M, Beare, R, Wu, MH, Barton, SM, Malpas, CB, Yeh, C-H, Harvey, AS, Anderson, V, Maixner, W, and Seal, M

Abstract

BACKGROUND: Optic radiation (OR) tractography may help predict and reduce post-neurosurgical visual field deficits. OR tractography methods currently lack pediatric and surgical focus. PURPOSE: We propose a clinically feasible OR tractography strategy in a pediatric neurosurgery setting and examine its intra-rater and inter-rater reliability/agreements. METHODS: Preoperative and intraoperative MRI data were obtained from six epilepsy and two brain tumor patients on 3 Tesla MRI scanners. Four raters with different clinical experience followed the proposed strategy to perform probabilistic OR tractography with manually drawing anatomical landmarks to reconstruct the OR pathway, based on fiber orientation distributions estimated from high angular resolution diffusion imaging data. Intra- and inter-rater reliabilities/agreements of tractography results were assessed using intraclass correlation coefficient (ICC) and dice similarity coefficient (DSC) across various tractography and OR morphological metrics, including the lateral geniculate body positions, tract volumes, and Meyer's loop position from temporal anatomical landmarks. RESULTS: Good to excellent intra- and inter-rater reproducibility was demonstrated for the majority of OR reconstructions (ICC = 0.70-0.99; DSC = 0.84-0.89). ICC was higher for non-lesional (0.82-0.99) than lesional OR (0.70-0.99). The non-lesional OR's mean volume was 22.66 cm3; the mean Meyer's loop position was 29.4 mm from the temporal pole, 5.89 mm behind of and 10.26 mm in front of the temporal ventricular horn. The greatest variations (± 1.00-3.00 mm) were observed near pathology, at the tract edges or at cortical endpoints. The OR tractography were used to assist surgical planning and guide lesion resection in all cases, no patient had new visual field deficits postoperatively. CONCLUSION: The proposed tractography strategy generates reliable and reproducible OR tractography images that can be reliably implemented in the routine, non-em

Published
2019

19. Genome-wide association reveals contribution of MRAS to painful temporomandibular disorder in males

Author

Smith, S. B. (Shad B.), Parisien, M. (Marc), Bair, E. (Eric), Belfer, I. (Inna), Chabot-Dore, A.-J. (Anne-Julie), Gris, P. (Pavel), Khoury, S. (Samar), Tansley, S. (Shannon), Torosyan, Y. (Yelizaveta), Zaykin, D. (Dmitri), Bernhardt, O. (Olaf), Serrano, P. d. (Priscila de Oliveira), Gracely, R. (Richard), Jain, D. (Deepti), Järvelin, M.-R. (Marjo-Riitta), Kaste, L. (Linda), Kerr, K. (Kathleen), Kocher, T. (Thomas), Lähdesmaki, R. (Raija), Laniado, N. (Nadia), Laurie, C. (Cathy), Laurie, C. (Cecelia), Männikko, M. (Minna), Meloto, C. (Carolina), Nackley, A. (Andrea), Nelson, S. (Sarah), Pesonen, P. (Paula), Ribeiro-Dasilva, M. (Margarete), Rizzatti-Barbosa, C. (Celia), Sanders, A. (Anne), Schwahn, C. (Christian), Sipilä, K. (Kirsi), Sofer, T. (Tamar), Teumer, A. (Alexander), Mogil, J. (Jeffrey), Fillingim, R. (Roger), Greenspan, J. (Joel), Ohrbach, R. (Richard), Slade, G. (Gary), Maixner, W. (William), Diatchenko, L. (Luda), Smith, S. B. (Shad B.), Parisien, M. (Marc), Bair, E. (Eric), Belfer, I. (Inna), Chabot-Dore, A.-J. (Anne-Julie), Gris, P. (Pavel), Khoury, S. (Samar), Tansley, S. (Shannon), Torosyan, Y. (Yelizaveta), Zaykin, D. (Dmitri), Bernhardt, O. (Olaf), Serrano, P. d. (Priscila de Oliveira), Gracely, R. (Richard), Jain, D. (Deepti), Järvelin, M.-R. (Marjo-Riitta), Kaste, L. (Linda), Kerr, K. (Kathleen), Kocher, T. (Thomas), Lähdesmaki, R. (Raija), Laniado, N. (Nadia), Laurie, C. (Cathy), Laurie, C. (Cecelia), Männikko, M. (Minna), Meloto, C. (Carolina), Nackley, A. (Andrea), Nelson, S. (Sarah), Pesonen, P. (Paula), Ribeiro-Dasilva, M. (Margarete), Rizzatti-Barbosa, C. (Celia), Sanders, A. (Anne), Schwahn, C. (Christian), Sipilä, K. (Kirsi), Sofer, T. (Tamar), Teumer, A. (Alexander), Mogil, J. (Jeffrey), Fillingim, R. (Roger), Greenspan, J. (Joel), Ohrbach, R. (Richard), Slade, G. (Gary), Maixner, W. (William), and Diatchenko, L. (Luda)

Abstract

Painful temporomandibular disorders (TMDs) are the leading cause of chronic orofacial pain, but its underlying molecular mechanisms remain obscure. Although many environmental factors have been associated with higher risk of developing painful TMD, family and twin studies support a heritable genetic component as well. We performed a genome-wide association study assuming an additive genetic model of TMD in a discovery cohort of 999 cases and 2031 TMD-free controls from the Orofacial Pain: Prospective Evaluation and Risk Assessment (OPPERA) study. Using logistic models adjusted for sex, age, enrollment site, and race, we identified 3 distinct loci that were significant in combined or sex-segregated analyses. A single-nucleotide polymorphism on chromosome 3 (rs13078961) was significantly associated with TMD in males only (odds ratio = 2.9, 95% confidence interval: 2.02–4.27, P = 2.2 × 10⁻⁸). This association was nominally replicated in a meta-analysis of 7 independent orofacial pain cohorts including 160,194 participants (odds ratio = 1.16, 95% confidence interval: 1.0–1.35, P = 2.3 × 10⁻²). Functional analysis in human dorsal root ganglia and blood indicated this variant is an expression quantitative trait locus, with the minor allele associated with decreased expression of the nearby muscle RAS oncogene homolog (MRAS) gene (beta = −0.51, P = 2.43 × 10⁻⁵). Male mice, but not female mice, with a null mutation of Mras displayed persistent mechanical allodynia in a model of inflammatory pain. Genetic and behavioral evidence support a novel mechanism by which genetically determined MRAS expression moderates the resiliency to chronic pain. This effect is male-specific and may contribute to the lower rates of painful TMD in men.

Published
2019

21. S5A-03 SESSION 5A

Author

Wray, A., primary, Maixner, W., additional, Chong, D., additional, Burge, J., additional, and Holmes, A., additional

Published
2019
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23. Somatic GNAQ mutation in the forme fruste of Sturge-Weber syndrome

Author

Hildebrand, MS, Harvey, AS, Malone, S, Damiano, JA, Do, H, Ye, Z, McQuillan, L, Maixner, W, Kalnins, R, Nolan, B, Wood, M, Ozturk, E, Jones, NC, Gillies, G, Pope, K, Lockhart, PJ, Dobrovic, A, Leventer, RJ, Scheffer, IE, Berkovic, SF, Hildebrand, MS, Harvey, AS, Malone, S, Damiano, JA, Do, H, Ye, Z, McQuillan, L, Maixner, W, Kalnins, R, Nolan, B, Wood, M, Ozturk, E, Jones, NC, Gillies, G, Pope, K, Lockhart, PJ, Dobrovic, A, Leventer, RJ, Scheffer, IE, and Berkovic, SF

Abstract

OBJECTIVE: To determine whether the GNAQ R183Q mutation is present in the forme fruste cases of Sturge-Weber syndrome (SWS) to establish a definitive molecular diagnosis. METHODS: We used sensitive droplet digital PCR (ddPCR) to detect and quantify the GNAQ mutation in tissues from epilepsy surgery in 4 patients with leptomeningeal angiomatosis; none had ocular or cutaneous manifestations. RESULTS: Low levels of the GNAQ mutation were detected in the brain tissue of all 4 cases-ranging from 0.42% to 7.1% frequency-but not in blood-derived DNA. Molecular evaluation confirmed the diagnosis in 1 case in which the radiologic and pathologic data were equivocal. CONCLUSIONS: We detected the mutation at low levels, consistent with mosaicism in the brain or skin (1.0%-18.1%) of classic cases. Our data confirm that the forme fruste is part of the spectrum of SWS, with the same molecular mechanism as the classic disease and that ddPCR is helpful where conventional diagnosis is uncertain.

Published
2018

26. Genome wide association study of sleep quality identifies a new association with loci near MPP6

Author

Khoury, S., primary, Parisien, M., additional, Wang, Q.-P., additional, Neely, G., additional, Bortsov, A., additional, McLean, S., additional, Sofer, T., additional, Louie, T., additional, Kaunisto, M., additional, Kalso, E., additional, Belfer, I., additional, Slade, G., additional, Smith, S., additional, Fillingim, R., additional, Ohrbach, R., additional, Greenspan, J., additional, Maixner, W., additional, and Diatchenko, L., additional

Published
2017
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27. Large meta-analysis of genome-wide association studies identifies five loci for lean body mass.

Author

Zillikens, M.C., Demissie, S., Hsu, Y.H., Yerges-Armstrong, L.M., Chou, W.C., Stolk, L., Livshits, G., Broer, L., Johnson, T., Koller, D.L., Kutalik, Z., Luan, J., Malkin, I., Ried, J.S., Smith, A.V., Thorleifsson, G., Vandenput, L., Hua Zhao, J., Zhang, W., Aghdassi, A., Åkesson, K., Amin, N., Baier, L.J., Barroso, I., Bennett, D.A., Bertram, L., Biffar, R., Bochud, M., Boehnke, M., Borecki, I.B., Buchman, A.S., Byberg, L., Campbell, H., Campos Obanda, N., Cauley, J.A., Cawthon, P.M., Cederberg, H., Chen, Z., Cho, N.H., Jin Choi, H., Claussnitzer, M., Collins, F., Cummings, S.R., De Jager, P.L., Demuth, I., Dhonukshe-Rutten, RAM, Diatchenko, L., Eiriksdottir, G., Enneman, A.W., Erdos, M., Eriksson, J.G., Eriksson, J., Estrada, K., Evans, D.S., Feitosa, M.F., Fu, M., Garcia, M., Gieger, C., Girke, T., Glazer, N.L., Grallert, H., Grewal, J., Han, B.G., Hanson, R.L., Hayward, C., Hofman, A., Hoffman, E.P., Homuth, G., Hsueh, W.C., Hubal, M.J., Hubbard, A., Huffman, K.M., Husted, L.B., Illig, T., Ingelsson, E., Ittermann, T., Jansson, J.O., Jordan, J.M., Jula, A., Karlsson, M., Khaw, K.T., Kilpeläinen, T.O., Klopp, N., Kloth, JSL, Koistinen, H.A., Kraus, W.E., Kritchevsky, S., Kuulasmaa, T., Kuusisto, J., Laakso, M., Lahti, J., Lang, T., Langdahl, B.L., Launer, L.J., Lee, J.Y., Lerch, M.M., Lewis, J.R., Lind, L., Lindgren, C., Liu, Y., Liu, T., Ljunggren, Ö., Lorentzon, M., Luben, R.N., Maixner, W., McGuigan, F.E., Medina-Gomez, C., Meitinger, T., Melhus, H., Mellström, D., Melov, S., Michaëlsson, K., Mitchell, B.D., Morris, A.P., Mosekilde, L., Newman, A., Nielson, C.M., O'Connell, J.R., Oostra, B.A., Orwoll, E.S., Palotie, A., Parker, S., Peacock, M., Perola, M., Peters, A., Polasek, O., Prince, R.L., Räikkönen, K., Ralston, S.H., Ripatti, S., Robbins, J.A., Rotter, J.I., Rudan, I., Salomaa, V., Satterfield, S., Schadt, E.E., Schipf, S., Scott, L., Sehmi, J., Shen, J., Soo Shin, C., Sigurdsson, G., Smith, S., Soranzo, N., Stančáková, A., Steinhagen-Thiessen, E., Streeten, E.A., Styrkarsdottir, U., Swart, KMA, Tan, S.T., Tarnopolsky, M.A., Thompson, P., Thomson, C.A., Thorsteinsdottir, U., Tikkanen, E., Tranah, G.J., Tuomilehto, J., van Schoor, N.M., Verma, A., Vollenweider, P., Völzke, H., Wactawski-Wende, J., Walker, M., Weedon, M.N., Welch, R., Wichmann, H.E., Widen, E., Williams, FMK, Wilson, J.F., Wright, N.C., Xie, W., Yu, L., Zhou, Y., Chambers, J.C., Döring, A., van Duijn, C.M., Econs, M.J., Gudnason, V., Kooner, J.S., Psaty, B.M., Spector, T.D., Stefansson, K., Rivadeneira, F., Uitterlinden, A.G., Wareham, N.J., Ossowski, V., Waterworth, D., Loos, RJF, Karasik, D., Harris, T.B., Ohlsson, C., Kiel, D.P., Zillikens, M.C., Demissie, S., Hsu, Y.H., Yerges-Armstrong, L.M., Chou, W.C., Stolk, L., Livshits, G., Broer, L., Johnson, T., Koller, D.L., Kutalik, Z., Luan, J., Malkin, I., Ried, J.S., Smith, A.V., Thorleifsson, G., Vandenput, L., Hua Zhao, J., Zhang, W., Aghdassi, A., Åkesson, K., Amin, N., Baier, L.J., Barroso, I., Bennett, D.A., Bertram, L., Biffar, R., Bochud, M., Boehnke, M., Borecki, I.B., Buchman, A.S., Byberg, L., Campbell, H., Campos Obanda, N., Cauley, J.A., Cawthon, P.M., Cederberg, H., Chen, Z., Cho, N.H., Jin Choi, H., Claussnitzer, M., Collins, F., Cummings, S.R., De Jager, P.L., Demuth, I., Dhonukshe-Rutten, RAM, Diatchenko, L., Eiriksdottir, G., Enneman, A.W., Erdos, M., Eriksson, J.G., Eriksson, J., Estrada, K., Evans, D.S., Feitosa, M.F., Fu, M., Garcia, M., Gieger, C., Girke, T., Glazer, N.L., Grallert, H., Grewal, J., Han, B.G., Hanson, R.L., Hayward, C., Hofman, A., Hoffman, E.P., Homuth, G., Hsueh, W.C., Hubal, M.J., Hubbard, A., Huffman, K.M., Husted, L.B., Illig, T., Ingelsson, E., Ittermann, T., Jansson, J.O., Jordan, J.M., Jula, A., Karlsson, M., Khaw, K.T., Kilpeläinen, T.O., Klopp, N., Kloth, JSL, Koistinen, H.A., Kraus, W.E., Kritchevsky, S., Kuulasmaa, T., Kuusisto, J., Laakso, M., Lahti, J., Lang, T., Langdahl, B.L., Launer, L.J., Lee, J.Y., Lerch, M.M., Lewis, J.R., Lind, L., Lindgren, C., Liu, Y., Liu, T., Ljunggren, Ö., Lorentzon, M., Luben, R.N., Maixner, W., McGuigan, F.E., Medina-Gomez, C., Meitinger, T., Melhus, H., Mellström, D., Melov, S., Michaëlsson, K., Mitchell, B.D., Morris, A.P., Mosekilde, L., Newman, A., Nielson, C.M., O'Connell, J.R., Oostra, B.A., Orwoll, E.S., Palotie, A., Parker, S., Peacock, M., Perola, M., Peters, A., Polasek, O., Prince, R.L., Räikkönen, K., Ralston, S.H., Ripatti, S., Robbins, J.A., Rotter, J.I., Rudan, I., Salomaa, V., Satterfield, S., Schadt, E.E., Schipf, S., Scott, L., Sehmi, J., Shen, J., Soo Shin, C., Sigurdsson, G., Smith, S., Soranzo, N., Stančáková, A., Steinhagen-Thiessen, E., Streeten, E.A., Styrkarsdottir, U., Swart, KMA, Tan, S.T., Tarnopolsky, M.A., Thompson, P., Thomson, C.A., Thorsteinsdottir, U., Tikkanen, E., Tranah, G.J., Tuomilehto, J., van Schoor, N.M., Verma, A., Vollenweider, P., Völzke, H., Wactawski-Wende, J., Walker, M., Weedon, M.N., Welch, R., Wichmann, H.E., Widen, E., Williams, FMK, Wilson, J.F., Wright, N.C., Xie, W., Yu, L., Zhou, Y., Chambers, J.C., Döring, A., van Duijn, C.M., Econs, M.J., Gudnason, V., Kooner, J.S., Psaty, B.M., Spector, T.D., Stefansson, K., Rivadeneira, F., Uitterlinden, A.G., Wareham, N.J., Ossowski, V., Waterworth, D., Loos, RJF, Karasik, D., Harris, T.B., Ohlsson, C., and Kiel, D.P.

Abstract

Lean body mass, consisting mostly of skeletal muscle, is important for healthy aging. We performed a genome-wide association study for whole body (20 cohorts of European ancestry with n = 38,292) and appendicular (arms and legs) lean body mass (n = 28,330) measured using dual energy X-ray absorptiometry or bioelectrical impedance analysis, adjusted for sex, age, height, and fat mass. Twenty-one single-nucleotide polymorphisms were significantly associated with lean body mass either genome wide (p < 5 × 10(-8)) or suggestively genome wide (p < 2.3 × 10(-6)). Replication in 63,475 (47,227 of European ancestry) individuals from 33 cohorts for whole body lean body mass and in 45,090 (42,360 of European ancestry) subjects from 25 cohorts for appendicular lean body mass was successful for five single-nucleotide polymorphisms in/near HSD17B11, VCAN, ADAMTSL3, IRS1, and FTO for total lean body mass and for three single-nucleotide polymorphisms in/near VCAN, ADAMTSL3, and IRS1 for appendicular lean body mass. Our findings provide new insight into the genetics of lean body mass.Lean body mass is a highly heritable trait and is associated with various health conditions. Here, Kiel and colleagues perform a meta-analysis of genome-wide association studies for whole body lean body mass and find five novel genetic loci to be significantly associated.

Published
2017

34. GWAS Identifies New Loci for Painful Temporomandibular Disorder: Hispanic Community Health Study/Study of Latinos

Author

Sanders, A.E., primary, Jain, D., additional, Sofer, T., additional, Kerr, K.F., additional, Laurie, C.C., additional, Shaffer, J.R., additional, Marazita, M.L., additional, Kaste, L.M., additional, Slade, G.D., additional, Fillingim, R.B., additional, Ohrbach, R., additional, Maixner, W., additional, Kocher, T., additional, Bernhardt, O., additional, Teumer, A., additional, Schwahn, C., additional, Sipilä, K., additional, Lähdesmäki, R., additional, Männikkö, M., additional, Pesonen, P., additional, Järvelin, M., additional, Rizzatti-Barbosa, C.M., additional, Meloto, C.B., additional, Ribeiro-Dasilva, M., additional, Diatchenko, L., additional, Serrano, P., additional, and Smith, S.B., additional

Published
2017
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35. Genome-wide association meta-analyses to identify common genetic variants associated with hallux valgus in Caucasian and African Americans

Author

Hsu, Y-H., Liu, Y., Hannan, M. T., Maixner, W., Smith, S. B., Diatchenko, L., Golightly, Y. M., Menz, H. B., Kraus, V. B., Doherty, M., Wilson, A. G., and Jordan, J. M.

Abstract

Objective Hallux valgus (HV) affects ∼36% of Caucasian adults. Although considered highly heritable, the underlying genetic determinants are unclear. We conducted the first genome-wide association study (GWAS) aimed to identify genetic variants associated with HV.\ud \ud Methods HV was assessed in three Caucasian cohorts (n=2263, n=915 and n=1231 participants, respectively). In each cohort, a GWAS was conducted using 2.5 M imputed SNPs. Mixed-effect regression with the additive genetic model adjusted for age, sex, weight and within-family correlations was used for both sex-specific and combined analyses. To combine GWAS results across cohorts, fixed-effect inverse-variance meta-analyses were used. Following meta-analyses, top-associated findings were also examined in an African American cohort (n=327).\ud \ud Results The proportion of HV variance explained by genome-wide genotyped SNPs was 50% in men and 48% in women. A higher proportion of genetic determinants of HV were sex specific. The most significantly associated SNP in men was rs9675316 located on chr17q23-a24 near the AXIN2 gene (p=0.000000546×10−7); the most significantly associated SNP in women was rs7996797 located on chr13q14.1-q14.2 near the ESD gene (p=0.000000721×10−7). Genome-wide significant SNP-by-sex interaction was found for SNP rs1563374 located on chr11p15.1 near the MRGPRX3 gene (interaction p value =0.0000000041×10−9). The association signals diminished when combining men and women.\ud \ud Conclusions The findings suggest that the potential pathophysiological mechanisms of HV are complex and strongly underlined by sex-specific interactions. The identified genetic variants imply contribution of biological pathways observed in osteoarthritis as well as new pathways, influencing skeletal development and inflammation.

Published
2015

36. COMT Diplotype Amplifies Effect of Stress on Risk of Temporomandibular Pain

Author

Maixner, W., Greenspan, J.D., Ohrbach, R., Slade, G.D., Smith, S., Sanders, A.E., Diatchenko, L., Bair, E., and Fillingim, R.B.

Subjects
stomatognathic diseases
Abstract

When measured once, psychological stress predicts development of painful temporomandibular disorder (TMD). However, a single measurement fails to characterize the dynamic nature of stress over time. Moreover, effects of stress on pain likely vary according to biological susceptibility. We hypothesized that temporal escalation in stress exacerbates risk for TMD, and the effect is amplified by allelic variants in a gene, catechol-O-methyltransferase (COMT), regulating catechol neurotransmitter catabolism. We used data from the Orofacial Pain: Prospective Evaluation and Risk Assessment prospective cohort study of 2,707 community-dwelling adults with no lifetime history of TMD on enrollment. At baseline and quarterly periods thereafter, the Perceived Stress Scale (PSS) measured psychological stress. Genotyped DNA from blood samples determined COMT diplotypes. During follow-up of 0.25 to 5.2 y, 248 adults developed examiner-verified incident TMD. PSS scores at baseline were 20% greater (P < 0.001) in adults who developed incident TMD compared with TMD-free controls. Baseline PSS scores increased by 9% (P = 0.003) during follow-up in cases but remained stable in controls. This stress escalation was limited to incident cases with COMT diplotypes coding for low-activity COMT, signifying impaired catabolism of catecholamines. Cox regression models confirmed significant effects on TMD hazard of both baseline PSS (P < 0.001), modeled as a time-constant covariate, and change in PSS (P < 0.001), modeled as a time-varying covariate. Furthermore, a significant (P = 0.04) interaction of COMT diplotype and time-varying stress showed that a postbaseline increase of 1.0 standard deviation in PSS more than doubled risk of TMD incidence in subjects with low-activity COMT diplotypes (hazard ratio = 2.35; 95% confidence limits: 1.66, 3.32), an effect not found in subjects with high-activity COMT diplotypes (hazard ratio = 1.42; 95% confidence limits: 0.96, 2.09). Findings provide novel insights into dynamic effects of psychological stress on TMD pain, highlighting that effects are most pronounced in individuals whose genetic susceptibility increases responsiveness to catecholamine neurotransmitters.

Published
2015
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37. Familial cortical dysplasia caused by mutation in the mammalian target of rapamycin regulator NPRL3

Author

Sim, J., Scerri, T., Fanjul-Fernández, M., Riseley, J., Gillies, G., Pope, K., Van Roozendaal, H., Heng, Julian, Mandelstam, S., McGillivray, G., Macgregor, D., Kannan, L., Maixner, W., Harvey, A., Amor, D., Delatycki, M., Crino, P., Bahlo, M., Lockhart, P., Leventer, R., Sim, J., Scerri, T., Fanjul-Fernández, M., Riseley, J., Gillies, G., Pope, K., Van Roozendaal, H., Heng, Julian, Mandelstam, S., McGillivray, G., Macgregor, D., Kannan, L., Maixner, W., Harvey, A., Amor, D., Delatycki, M., Crino, P., Bahlo, M., Lockhart, P., and Leventer, R.

Abstract

© 2015 American Neurological Association. We describe first cousin sibling pairs with focal epilepsy, one of each pair having focal cortical dysplasia (FCD) IIa. Linkage analysis and whole-exome sequencing identified a heterozygous germline frameshift mutation in the gene encoding nitrogen permease regulator-like 3 (NPRL3). NPRL3 is a component of GAP Activity Towards Rags 1, a negative regulator of the mammalian target of rapamycin complex 1 signaling pathway. Immunostaining of resected brain tissue demonstrated mammalian target of rapamycin activation. Screening of 52 unrelated individuals with FCD identified 2 additional patients with FCDIIa and germline NPRL3 mutations. Similar to DEPDC5, NPRL3 mutations may be considered as causal variants in patients with FCD or magnetic resonance imaging-negative focal epilepsy.

Published
2016

38. Painful Temporomandibular Disorder

Author

Slade, G.D., primary, Ohrbach, R., additional, Greenspan, J.D., additional, Fillingim, R.B., additional, Bair, E., additional, Sanders, A.E., additional, Dubner, R., additional, Diatchenko, L., additional, Meloto, C.B., additional, Smith, S., additional, and Maixner, W., additional

Published
2016
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39. Familial cortical dysplasia type IIA caused by a germline mutation in DEPDC5

Author

Scerri, T, Riseley, JR, Gillies, G, Pope, K, Burgess, R, Mandelstam, SA, Dibbens, L, Chow, CW, Maixner, W, Harvey, AS, Jackson, GD, Amor, DJ, Delatycki, MB, Crino, PB, Berkovic, SF, Scheffer, IE, Bahlo, M, Lockhart, PJ, Leventer, RJ, Scerri, T, Riseley, JR, Gillies, G, Pope, K, Burgess, R, Mandelstam, SA, Dibbens, L, Chow, CW, Maixner, W, Harvey, AS, Jackson, GD, Amor, DJ, Delatycki, MB, Crino, PB, Berkovic, SF, Scheffer, IE, Bahlo, M, Lockhart, PJ, and Leventer, RJ

Abstract

Whole-exome sequencing of two brothers with drug-resistant, early-onset, focal epilepsy secondary to extensive type IIA focal cortical dysplasia identified a paternally inherited, nonsense variant of DEPDC5 (c.C1663T, p.Arg555*). This variant has previously been reported to cause familial focal epilepsy with variable foci in patients with normal brain imaging. Immunostaining of resected brain tissue from both brothers demonstrated mammalian target of rapamycin (mTOR) activation. This report shows the histopathological features of cortical dysplasia associated with a DEPDC5 mutation, confirms mTOR dysregulation in the malformed tissue and expands the spectrum of neurological manifestations of DEPDC5 mutations to include severe phenotypes with large areas of cortical malformation.

Published
2015

40. Sleep Apnea Symptoms and Risk of Temporomandibular Disorder: OPPERA Cohort

Author

Ohrbach, R., Fillingim, R., Diatchenko, L., Dubner, R., Slade, G.D., Essick, G.K., Maixner, W., Greenspan, J.D., Sanders, A.E., Miller, V.E., Bair, E., and Knott, C.

Subjects
stomatognathic diseases, human activities, respiratory tract diseases
Abstract

The authors tested the hypothesis that obstructive sleep apnea (OSA) signs/symptoms are associated with the occurrence of temporomandibular disorder (TMD), using the OPPERA prospective cohort study of adults aged 18 to 44 years at enrollment (n = 2,604) and the OPPERA case-control study of chronic TMD (n = 1,716). In both the OPPERA cohort and case-control studies, TMD was examiner determined according to established research diagnostic criteria. People were considered to have high likelihood of OSA if they reported a history of sleep apnea or ≥ 2 hallmarks of OSA: loud snoring, daytime sleepiness, witnessed apnea, and hypertension. Cox proportional hazards regression estimated hazard ratios (HRs) and 95% confidence limits (CL) for first-onset TMD. Logistic regression estimated odds ratios (OR) and 95% CL for chronic TMD. In the cohort, 248 individuals developed first-onset TMD during the median 2.8-year follow-up. High likelihood of OSA was associated with greater incidence of first-onset TMD (adjusted HR = 1.73; 95% CL, 1.14, 2.62). In the case-control study, high likelihood of OSA was associated with higher odds of chronic TMD (adjusted OR = 3.63; 95% CL, 2.03, 6.52). Both studies supported a significant association of OSA symptoms and TMD, with prospective cohort evidence finding that OSA symptoms preceded first-onset TMD.

Published
2013
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43. The surgically remediable syndrome of epilepsy associated with bottom-of-sulcus dysplasia

Author

Harvey, A. S., primary, Mandelstam, S. A., additional, Maixner, W. J., additional, Leventer, R. J., additional, Semmelroch, M., additional, MacGregor, D., additional, Kalnins, R. M., additional, Perchyonok, Y., additional, Fitt, G. J., additional, Barton, S., additional, Kean, M. J., additional, Fabinyi, G. C. A., additional, and Jackson, G. D., additional

Published
2015
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44. Hemispheric cortical dysplasia secondary to a mosaic somatic mutation in MTOR

Author

Leventer, R. J., primary, Scerri, T., additional, Marsh, A. P. L., additional, Pope, K., additional, Gillies, G., additional, Maixner, W., additional, MacGregor, D., additional, Harvey, A. S., additional, Delatycki, M. B., additional, Amor, D. J., additional, Crino, P., additional, Bahlo, M., additional, and Lockhart, P. J., additional

Published
2015
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46. ABSTRACT 334

Author

Lewis, P., primary, Czosnyka, M., additional, Carter, B.G., additional, Rosenfeld, J.V., additional, Maixner, W., additional, and Butt, W., additional

Published
2014
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49. Construction of a Global Pain Systems Network Highlights Phospholipid Signaling as a Regulator of Heat Nociception

Author

Neely, GG, Rao, S, Costigan, M, Mair, N, Racz, I, Milinkeviciute, G, Meixner, A, Nayanala, S, Griffin, RS, Belfer, I, Dai, F, Smith, S, Diatchenko, L, Marengo, S, Haubner, BJ, Novatchkova, M, Gibson, D, Maixner, W, Pospisilik, JA, Hirsch, E, Whishaw, IQ, Zimmer, A, Gupta, V, Sasaki, J, Kanaho, Y, Sasaki, T, Kress, M, Woolf, CJ, Penninger, JM, Neely, GG, Rao, S, Costigan, M, Mair, N, Racz, I, Milinkeviciute, G, Meixner, A, Nayanala, S, Griffin, RS, Belfer, I, Dai, F, Smith, S, Diatchenko, L, Marengo, S, Haubner, BJ, Novatchkova, M, Gibson, D, Maixner, W, Pospisilik, JA, Hirsch, E, Whishaw, IQ, Zimmer, A, Gupta, V, Sasaki, J, Kanaho, Y, Sasaki, T, Kress, M, Woolf, CJ, and Penninger, JM

Abstract

The ability to perceive noxious stimuli is critical for an animal's survival in the face of environmental danger, and thus pain perception is likely to be under stringent evolutionary pressure. Using a neuronal-specific RNAi knock-down strategy in adult Drosophila, we recently completed a genome-wide functional annotation of heat nociception that allowed us to identify α2δ3 as a novel pain gene. Here we report construction of an evolutionary-conserved, system-level, global molecular pain network map. Our systems map is markedly enriched for multiple genes associated with human pain and predicts a plethora of novel candidate pain pathways. One central node of this pain network is phospholipid signaling, which has been implicated before in pain processing. To further investigate the role of phospholipid signaling in mammalian heat pain perception, we analysed the phenotype of PIP5Kα and PI3Kγ mutant mice. Intriguingly, both of these mice exhibit pronounced hypersensitivity to noxious heat and capsaicin-induced pain, which directly mapped through PI3Kγ kinase-dead knock-in mice to PI3Kγ lipid kinase activity. Using single primary sensory neuron recording, PI3Kγ function was mechanistically linked to a negative regulation of TRPV1 channel transduction. Our data provide a systems map for heat nociception and reinforces the extraordinary conservation of molecular mechanisms of nociception across different species. © 2012 Neely et al.

Published
2012

50. Pain perception is altered by a nucleotide polymorphism in SCN9A.

Author

Reimann, F., Cox, J.J., Belfer, I., Diatchenko, L., Zaykin, D.V., McHale, D.P., Drenth, J.P.H., Dai, F., Wheeler, J., Sanders, F., Wood, L., Wu, T.X., Karppinen, J., Nikolajsen, L., Mannikko, M., Max, M.B., Kiselycznyk, C., Poddar, M., Morsche, R.H.M. te, Smith, S., Gibson, D., Kelempisioti, A., Maixner, W., Gribble, F.M., Woods, C.G., Reimann, F., Cox, J.J., Belfer, I., Diatchenko, L., Zaykin, D.V., McHale, D.P., Drenth, J.P.H., Dai, F., Wheeler, J., Sanders, F., Wood, L., Wu, T.X., Karppinen, J., Nikolajsen, L., Mannikko, M., Max, M.B., Kiselycznyk, C., Poddar, M., Morsche, R.H.M. te, Smith, S., Gibson, D., Kelempisioti, A., Maixner, W., Gribble, F.M., and Woods, C.G.

Abstract

Contains fulltext : 89837.pdf (publisher's version ) (Closed access), The gene SCN9A is responsible for three human pain disorders. Nonsense mutations cause a complete absence of pain, whereas activating mutations cause severe episodic pain in paroxysmal extreme pain disorder and primary erythermalgia. This led us to investigate whether single nucleotide polymorphisms (SNPs) in SCN9A were associated with differing pain perception in the general population. We first genotyped 27 SCN9A SNPs in 578 individuals with a radiographic diagnosis of osteoarthritis and a pain score assessment. A significant association was found between pain score and SNP rs6746030; the rarer A allele was associated with increased pain scores compared to the commoner G allele (P = 0.016). This SNP was then further genotyped in 195 pain-assessed people with sciatica, 100 amputees with phantom pain, 179 individuals after lumbar discectomy, and 205 individuals with pancreatitis. The combined P value for increased A allele pain was 0.0001 in the five cohorts tested (1277 people in total). The two alleles of the SNP rs6746030 alter the coding sequence of the sodium channel Nav1.7. Each was separately transfected into HEK293 cells and electrophysiologically assessed by patch-clamping. The two alleles showed a difference in the voltage-dependent slow inactivation (P = 0.042) where the A allele would be predicted to increase Nav1.7 activity. Finally, we genotyped 186 healthy females characterized by their responses to a diverse set of noxious stimuli. The A allele of rs6746030 was associated with an altered pain threshold and the effect mediated through C-fiber activation. We conclude that individuals experience differing amounts of pain, per nociceptive stimulus, on the basis of their SCN9A rs6746030 genotype.

Published
2010

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