Your search keyword '"Bernier, Francois"' showing total 50 results

1. Molecular characterization of 13 patients with PIK3CA‐related overgrowth spectrum using a targeted deep sequencing approach.

Author

de Kock, Leanne, Cuillerier, Alexanne, Gillespie, Meredith, Couse, Madeline, Hartley, Taila, Mears, Wendy, Bernier, Francois P., Chudley, Albert E., Frosk, Patrick, Nikkel, Sarah M., Innes, A. Micheil, Lauzon, Julie, Thomas, Maryann, Guerin, Andrea, Armour, Christine M., Weksberg, Rosanna, Scott, James N., Watkins, Debra, Harvey, Shirley, and Cytrynbaum, Cheryl

Abstract

Activating variants in the PIK3CA gene cause a heterogeneous spectrum of disorders that involve congenital or early‐onset segmental/focal overgrowth, now referred to as PIK3CA‐related overgrowth spectrum (PROS). Historically, the clinical diagnoses of patients with PROS included a range of distinct syndromes, including CLOVES syndrome, dysplastic megalencephaly, hemimegalencephaly, focal cortical dysplasia, Klippel–Trenaunay syndrome, CLAPO syndrome, fibroadipose hyperplasia or overgrowth, hemihyperplasia multiple lipomatosis, and megalencephaly capillary malformation‐polymicrogyria (MCAP) syndrome. MCAP is a sporadic overgrowth disorder that exhibits core features of progressive megalencephaly, vascular malformations, distal limb malformations, cortical brain malformations, and connective tissue dysplasia. In 2012, our research group contributed to the identification of predominantly mosaic, gain‐of‐function variants in PIK3CA as an underlying genetic cause of the syndrome. Mosaic variants are technically more difficult to detect and require implementation of more sensitive sequencing technologies and less stringent variant calling algorithms. In this study, we demonstrated the utility of deep sequencing using the Illumina TruSight Oncology 500 (TSO500) sequencing panel in identifying variants with low allele fractions in a series of patients with PROS and suspected mosaicism: pathogenic, mosaic PIK3CA variants were identified in all 13 individuals, including 6 positive controls. This study highlights the importance of screening for low‐level mosaic variants in PROS patients. The use of targeted panels with deep sequencing in clinical genetic testing laboratories would improve diagnostic yield and accuracy within this patient population. [ABSTRACT FROM AUTHOR]

Published

2024

2. Developing a Framework of Cost Elements of Socioeconomic Burden of Rare Disease: A Scoping Review.

Author

Currie, Gillian R., Gerber, Brittany, Lorenzetti, Diane, MacDonald, Karen, Benseler, Susanne M., Bernier, Francois P., Boycott, Kym M., Carias, K. Vanessa, Hamelin, Bettina, Hayeems, Robin Z., LeBlanc, Claire, Twilt, Marinka, van Rooijen, Gijs, Wong-Rieger, Durhane, Yeung, Rae S. M., and Marshall, Deborah A.

Subjects

RARE diseases, MEDICAL economics, CHRONIC diseases, COMMUNITIES, GENETIC testing

Abstract

Background and Objective: Rare diseases place a significant burden on patients, families, the healthcare system, and society. Evidence on the socioeconomic burden of rare disease is limited and mostly reflects diseases where treatments are available. We developed a framework encompassing recommended cost elements for studies of the socioeconomic burden of rare diseases. Methods: A scoping review, conducted in five databases (Cochrane Library, EconLit, Embase, MEDLINE, and APA PsycINFO), identified English language publications from 2000 to 2021 presenting frameworks developed for determining, measuring or valuing costs for rare or chronic diseases. Cost elements were extracted and used to develop a literature-informed framework. Structured feedback was gathered from experts in rare diseases, health economics/health services, and policy research to revise the framework. Results: Of 2990 records identified, eight papers were included and informed our preliminary framework; three focused on rare disease and five on chronic disease. Following expert input, we developed a framework consisting of nine cost categories (inpatient, outpatient, community, healthcare products/goods, productivity/education, travel/accommodation, government benefits, family impacts, and other), with several cost elements within each category. Our framework includes unique costs, added from the expert feedback, including genetic testing to inform treatment, use of private laboratories or out-of-country testing, family involvement in foundations and organizations, and advocacy costs for special access programs. Conclusions: Our work is the first to identify a comprehensive list of cost elements for rare disease for use by researchers and policy makers to fully capture socioeconomic burden. Use of the framework will increase the quality and comparability of future studies. Future work should focus on measuring and valuing these costs through onset, diagnosis, and post-diagnosis. [ABSTRACT FROM AUTHOR]

Published

2023

3. Finding the sweet spot: a qualitative study exploring patients' acceptability of chatbots in genetic service delivery.

Author

Luca, Stephanie, Clausen, Marc, Shaw, Angela, Lee, Whiwon, Krishnapillai, Suvetha, Adi-Wauran, Ella, Faghfoury, Hanna, Costain, Gregory, Jobling, Rebekah, Aronson, Melyssa, Liston, Eriskay, Silver, Josh, Shuman, Cheryl, Chad, Lauren, Hayeems, Robin Z., Bombard, Yvonne, the Genetics Navigator Study Team, Bernier, Francois, Brudno, Michael, and Carroll, June C.

Subjects

CHATBOTS, PATIENT preferences, ARTIFICIAL intelligence, QUALITATIVE research, GENETIC testing, THEMATIC analysis

Abstract

Chatbots, web-based artificial intelligence tools that simulate human conversation, are increasingly in use to support many areas of genomic medicine. However, patient preferences towards using chatbots across the range of clinical settings are unknown. We conducted a qualitative study with individuals who underwent genetic testing for themselves or their child. Participants were asked about their preferences for using a chatbot within the genetic testing journey. Thematic analysis employing interpretive description was used. We interviewed 30 participants (67% female, 50% 50 + years). Participants considered chatbots to be inefficient for very simple tasks (e.g., answering FAQs) or very complex tasks (e.g., explaining results). Chatbots were acceptable for moderately complex tasks where participants perceived a favorable return on their investment of time and energy. In addition to achieving this "sweet spot," participants anticipated that their comfort with chatbots would increase if the chatbot was used as a complement to but not a replacement for usual care. Participants wanted a "safety net" (i.e., access to a clinician) for needs not addressed by the chatbot. This study provides timely insights into patients' comfort with and perceived limitations of chatbots for genomic medicine and can inform their implementation in practice. [ABSTRACT FROM AUTHOR]

Published

2023

4. Effect of Probiotic Bifidobacterium breve in Improving Cognitive Function and Preventing Brain Atrophy in Older Patients with Suspected Mild Cognitive Impairment: Results of a 24-Week Randomized, Double-Blind, Placebo-Controlled Trial.

Author

Asaoka, Daisuke, Xiao, Jinzhong, Takeda, Tsutomu, Yanagisawa, Naotake, Yamazaki, Takahiro, Matsubara, Yoichiro, Sugiyama, Hideki, Endo, Noemi, Higa, Motoyuki, Kasanuki, Koji, Ichimiya, Yosuke, Koido, Shigeo, Ohno, Kazuya, Bernier, Francois, Katsumata, Noriko, Nagahara, Akihito, Arai, Heii, Ohkusa, Toshifumi, and Sato, Nobuhiro

Subjects

CEREBRAL atrophy, OLDER patients, COGNITIVE ability, MILD cognitive impairment, PROBIOTICS, GUT microbiome, THERAPEUTIC use of probiotics, BRAIN, RESEARCH, RESEARCH methodology, COGNITION, EVALUATION research, ATROPHY, COMPARATIVE studies, RANDOMIZED controlled trials, BLIND experiment

Abstract

Background: Probiotics have been reported to ameliorate cognitive impairment.Objective: We investigated the effect of the probiotic strain Bifidobacterium breve MCC1274 (A1) in enhancing cognition and preventing brain atrophy of older patients with mild cognitive impairment (MCI).Methods: In this RCT, 130 patients aged from 65 to 88 years old with suspected MCI received once daily either probiotic (B. breve MCC1274, 2×1010 CFU) or placebo for 24 weeks. Cognitive functions were assessed by ADAS-Jcog and MMSE tests. Participants underwent MRI to determine brain atrophy changes using Voxel-based Specific Regional Analysis System for Alzheimer's disease (VSRAD). Fecal samples were collected for the analysis of gut microbiota composition.Results: Analysis was performed on 115 participants as the full analysis set (probiotic 55, placebo 60). ADAS-Jcog subscale "orientation" was significantly improved compared to placebo at 24 weeks. MMSE subscales "orientation in time" and "writing" were significantly improved compared to placebo in the lower baseline MMSE (< 25) subgroup at 24 weeks. VSRAD scores worsened in the placebo group; probiotic supplementation tended to suppress the progression, in particular among those subjects with progressed brain atrophy (VOI Z-score ≥1.0). There were no marked changes in the overall composition of the gut microbiota by the probiotic supplementation.Conclusion: Improvement of cognitive function was observed on some subscales scores only likely due to the lower sensitiveness of these tests for MCI subjects. Probiotics consumption for 24 weeks suppressed brain atrophy progression, suggesting that B. breve MCC1274 helps prevent cognitive impairment of MCI subjects. [ABSTRACT FROM AUTHOR]

Published

2022

5. A Deep Invertible 3-D Facial Shape Model for Interpretable Genetic Syndrome Diagnosis.

Author

Bannister, Jordan J., Wilms, Matthias, Aponte, J. David, Katz, David C., Klein, Ophir D., Bernier, Francois P. J., Spritz, Richard A., Hallgrimsson, Benedikt, and Forkert, Nils D.

Subjects

GENETIC disorder diagnosis, COMPUTER-aided diagnosis, GENETIC models, HUMAN facial recognition software, DEEP learning, DIAGNOSIS, COMPUTER-assisted image analysis (Medicine)

Abstract

One of the primary difficulties in treating patients with genetic syndromes is diagnosing their condition. Many syndromes are associated with characteristic facial features that can be imaged and utilized by computer-assisted diagnosis systems. In this work, we develop a novel 3D facial surface modeling approach with the objective of maximizing diagnostic model interpretability within a flexible deep learning framework. Therefore, an invertible normalizing flow architecture is introduced to enable both inferential and generative tasks in a unified and efficient manner. The proposed model can be used (1) to infer syndrome diagnosis and other demographic variables given a 3D facial surface scan and (2) to explain model inferences to non-technical users via multiple interpretability mechanisms. The model was trained and evaluated on more than 4700 facial surface scans from subjects with 47 different syndromes. For the challenging task of predicting syndrome diagnosis given a new 3D facial surface scan, age, and sex of a subject, the model achieves a competitive overall top-1 accuracy of 71%, and a mean sensitivity of 43% across all syndrome classes. We believe that invertible models such as the one presented in this work can achieve competitive inferential performance while greatly increasing model interpretability in the domain of medical diagnosis. [ABSTRACT FROM AUTHOR]

Published

2022

6. IMPACT webinars: Improving Patient Access to genetic Counselling and Testing using webinars—the Alberta experience with hypertrophic cardiomyopathy.

Author

Christian, Susan, Tagoe, Julia, Delday, Lenore, Bernier, Francois P., Kohut, Ruth, and Ferrier, Raechel

Abstract

Growing demand for genetic counselling and testing has created a need for innovative service delivery models to provide quality care in an efficient manner. The goal of this study was to develop and evaluate a patient-facing webinar providing pre-test genetic counselling to individuals with hypertrophic cardiomyopathy. A patient-facing webinar was developed and implemented between April 2019 and January 2021. It was evaluated using the Alberta Quality Matrix for Health framework, which considers the patient experience across the domains of effectiveness, appropriateness, acceptability, accessibility, and efficiency. The webinar group showed comparable scores to controls with regard to self-perceived knowledge and decisional conflict. The majority of patients reported that the webinar met their expectations and was an acceptable replacement for a 1:1 genetic counselling appointment. Finally, the webinar reduced genetic counsellor time to an average of 24 min per patient. Providing pre-test genetic counselling to index hypertrophic cardiomyopathy patients via a group webinar has achieved a high quality of care, and optimized use of provider and space resources. [ABSTRACT FROM AUTHOR]

Published

2022

7. Association of Plasma Hemoglobin A1c with Improvement of Cognitive Functions by Probiotic Bifidobacterium breve Supplementation in Healthy Adults with Mild Cognitive Impairment.

Author

Bernier, Francois, Ohno, Kazuya, Katsumata, Noriko, Shimizu, Takashi, and Xiao, Jinzhong

Subjects

COGNITIVE ability, PROBIOTICS, BIFIDOBACTERIUM, HEMOGLOBINS, COGNITION, BLIND experiment, BLOOD testing

Abstract

We demonstrated the benefit of the probiotic strain, Bifidobacterium breve MCC1274 (synonym B. breve A1), at improving cognition in our previous double-blind, placebo-controlled clinical study. Analysis of the association of blood parameters changes with the improvement of cognitive function revealed an inverse correlation of HbA1c with total RBANS score amelioration after the study only in the probiotic group (ρ= -0.4218, p = 0.0067). A stratified analysis based on baseline HbA1c with a median value showed a more remarkable benefit by the probiotic supplementation in the higher median subgroup. These data support the mechanism of anti-inflammation in improving cognition by the probiotic strain. [ABSTRACT FROM AUTHOR]

Published

2021

8. Targeting Impaired Antimicrobial Immunity in the Brain for the Treatment of Alzheimer's Disease.

Author

Fulop, Tamas, Tripathi, Shreyansh, Rodrigues, Serafim, Desroches, Mathieu, Bunt, Ton, Eiser, Arnold, Bernier, Francois, Beauregard, Pascale B, Barron, Annelise E, Khalil, Abdelouahed, Plotka, Adam, Hirokawa, Katsuiku, Larbi, Anis, Bocti, Christian, Laurent, Benoit, Frost, Eric H, and Witkowski, Jacek M

Subjects

ALZHEIMER'S disease, DISEASE risk factors, INFLAMMATION, PATHOGENESIS, CEREBRAL amyloid angiopathy, AMYLOID plaque, BRAIN diseases

Abstract

Alzheimer's disease (AD) is the most common form of dementia and aging is the most common risk factor for developing the disease. The etiology of AD is not known but AD may be considered as a clinical syndrome with multiple causal pathways contributing to it. The amyloid cascade hypothesis, claiming that excess production or reduced clearance of amyloid-beta (Aβ) and its aggregation into amyloid plaques, was accepted for a long time as the main cause of AD. However, many studies showed that Aβ is a frequent consequence of many challenges/pathologic processes occurring in the brain for decades. A key factor, sustained by experimental data, is that low-grade infection leading to production and deposition of Aβ, which has antimicrobial activity, precedes the development of clinically apparent AD. This infection is chronic, low grade, largely clinically silent for decades because of a nearly efficient antimicrobial immune response in the brain. A chronic inflammatory state is induced that results in neurodegeneration. Interventions that appear to prevent, retard or mitigate the development of AD also appear to modify the disease. In this review, we conceptualize further that the changes in the brain antimicrobial immune response during aging and especially in AD sufferers serve as a foundation that could lead to improved treatment strategies for preventing or decreasing the progression of AD in a disease-modifying treatment. [ABSTRACT FROM AUTHOR]

Published

2021

9. De novo variants in MPP5 cause global developmental delay and behavioral changes.

Author

Sterling, Noelle, Duncan, Anna R, Park, Raehee, Koolen, David A, Shi, Jiahai, Cho, Seo-Hee, Benke, Paul J, Grant, Patricia E, Genetti, Casie A, VanNoy, Grace E, Juusola, Jane, McWalter, Kirsty, Parboosingh, Jillian S, Lamont, Ryan E, Bernier, Francois P, Smith, Christopher, Harris, David J, Stegmann, Alexander P A, Innes, A Micheil, and Kim, Seonhee

Published

2020

10. Probiotic Bifidobacterium breve in Improving Cognitive Functions of Older Adults with Suspected Mild Cognitive Impairment: A Randomized, Double-Blind, Placebo-Controlled Trial.

Author

Xiao, Jinzhong, Katsumata, Noriko, Bernier, Francois, Ohno, Kazuya, Yamauchi, Yuki, Odamaki, Toshitaka, Yoshikawa, Kenji, Ito, Kumie, and Kaneko, Toshiyuki

Subjects

OLDER people, COGNITIVE ability, MILD cognitive impairment, BIFIDOBACTERIUM, SHORT-term memory, NEUROPSYCHOLOGICAL tests, COGNITION, PROBIOTICS, RANDOMIZED controlled trials, BLIND experiment, STATISTICAL sampling

Abstract

Background: Probiotics use has been associated with modulation of inflammation and considered as a possible intervention for CNS diseases such as mild cognitive impairment (MCI) and dementia.Objective: We aimed to test the effect of the probiotic strain, Bifidobacterium breve A1 (MCC1274), to restore cognition in a physically healthy, suspected MCI population.Methods: In this randomized, double-blind, placebo-controlled trial, 80 healthy older adults suffering from MCI were divided into two even groups to receive once daily either probiotic (B. breve A1, 2×1010 CFU) or placebo for 16 weeks using a computer-generated algorithm. Cognitive functions were assessed by the Repeatable Battery for the Assessment of Neuropsychological Status (RBANS) and the Japanese version of the MCI Screen (JMCIS) tests before and after the study as primary and secondary endpoints, respectively.Results: 79 participants completed the study, and no adverse events were observed. RBANS total score was significantly improved in probiotic group compared with placebo (mean between-group difference 11.3 [95% CI 6.7 to 15.8]; p < 0.0001) after 16 weeks of consumption, in particular with significant improvement in domain scores of immediate memory, visuospatial/constructional, and delayed memory (p < 0.0001), in both intention-to-treat (ITT) analysis and per-protocol (PP) analysis. JMCIS score was also improved versus placebo in ITT analysis (p = 0.052) and PP analysis (p = 0.036).Conclusion: Study results indicate B. breve A1 is a safe and effective approach for improving memory functions of suspected MCI subjects. [ABSTRACT FROM AUTHOR]

Published

2020

11. Enabling Global Clinical Collaborations on Identifiable Patient Data: The Minerva Initiative.

Author

Nellåker, Christoffer, Alkuraya, Fowzan S., Baynam, Gareth, Bernier, Raphael A., Bernier, Francois P.J., Boulanger, Vanessa, Brudno, Michael, Brunner, Han G., Clayton-Smith, Jill, Cogné, Benjamin, Dawkins, Hugh J.S., deVries, Bert B.A., Douzgou, Sofia, Dudding-Byth, Tracy, Eichler, Evan E., Ferlaino, Michael, Fieggen, Karen, Firth, Helen V., FitzPatrick, David R., and Gration, Dylan

Subjects

BIG data, FREE enterprise, RARE diseases, GENETIC disorders, PERSONALLY identifiable information, PUBLIC goods

Abstract

The clinical utility of computational phenotyping for both genetic and rare diseases is increasingly appreciated; however, its true potential is yet to be fully realized. Alongside the growing clinical and research availability of sequencing technologies, precise deep and scalable phenotyping is required to serve unmet need in genetic and rare diseases. To improve the lives of individuals affected with rare diseases through deep phenotyping, global big data interrogation is necessary to aid our understanding of disease biology, assist diagnosis, and develop targeted treatment strategies. This includes the application of cutting-edge machine learning methods to image data. As with most digital tools employed in health care, there are ethical and data governance challenges associated with using identifiable personal image data. There are also risks with failing to deliver on the patient benefits of these new technologies, the biggest of which is posed by data siloing. The Minerva Initiative has been designed to enable the public good of deep phenotyping while mitigating these ethical risks. Its open structure, enabling collaboration and data sharing between individuals, clinicians, researchers and private enterprise, is key for delivering precision public health. [ABSTRACT FROM AUTHOR]

Published

2019

12. Validation of Dried Blood Spots for Maternal Biomonitoring of Nonessential Elements in an Artisanal and Small‐Scale Gold Mining Area of Tanzania.

Author

Nyanza, Elias C., Dewey, Deborah, Bernier, Francois, Manyama, Mange, Hatfield, Jennifer, and Martin, Jonathan W.

Subjects

ENVIRONMENTAL monitoring, DRIED blood spot testing, GOLD mining, INDUCTIVELY coupled plasma mass spectrometry, LEAD

Abstract

Biomonitoring studies of vulnerable populations in low‐ and middle‐income countries are limited because traditional sampling methods are challenging to implement in low‐resource settings. The present study examined the feasibility, precision, and accuracy of dried blood spots (DBS) for human biomonitoring of nonessential elements (cadmium [Cd], mercury [Hg], and lead [Pb]) in an area of northern Tanzania with artisanal and small‐scale gold mining activities. Pregnant women (n = 44) were recruited in Geita during antenatal clinic visits, and DBS from capillary blood were collected on filter paper. As a gold‐standard comparison, venous blood was sampled from the same participants and compared with the DBS. Venous blood, DBS, and quality control samples were analyzed for chemical elements by inductively coupled plasma mass spectrometry. Field blanks were very clean for most elements, generally only twice as high as corresponding laboratory filter blanks. No significant differences were found between duplicate DBS samples taken from the same participants, with near perfect intraclass correlation coefficients (0.99) for Cd, Hg, and Pb, indicating excellent reliability. Moreover, correlation was strong (r2 > 0.9) and significant (p < 0.0001) between DBS and the quantitative venous blood, with regression line slopes close to 1.0 (0.847, 0.976, and 0.969 for Cd, Hg, and Pb, respectively), indicating high accuracy of the DBS method compared with the gold‐standard approach. The DBS method is minimally invasive and was a feasible, precise, and accurate means of measuring exposure to Cd, Hg, and Pb in pregnant women in a low‐resource setting. Environ Toxicol Chem 2019;38:1285–1293. © 2019 SETAC [ABSTRACT FROM AUTHOR]

Published

2019

13. Is PNPT1‐related hearing loss ever non‐syndromic? Whole exome sequencing of adult siblings expands the natural history of PNPT1‐related disorders.

Author

Eaton, Alison, Bernier, Francois P., Goedhart, Caitlin, Caluseriu, Oana, Lamont, Ryan E., Boycott, Kym M., Parboosingh, Jillian S., and Innes, A. Micheil

Abstract

PNPT1 is a mitochondrial RNA transport protein that has been linked to two discrete phenotypes, namely isolated sensorineural hearing loss (OMIM 614934) and combined oxidative phosphorylation deficiency (OMIM 614932). The latter has been described in multiple families presenting with complex neurologic manifestations in childhood. We describe adult siblings with biallelic PNPT1 variants identified through WES who presented with isolated severe congenital sensorineural hearing loss (SNHL). In their 40s, they each developed and then followed a nearly identical neurodegenerative course with ataxia, dystonia, and cognitive decline. Now in their 50s and 60s, all have developed the additional features of optic nerve atrophy, spasticity, and incontinence. The natural history of the condition in this family may suggest that the individuals previously reported as having isolated SNHL may be at risk of developing multisystem disease in late adulthood, and that PNPT1‐related disorders may constitute a spectrum rather than distinct phenotypes. [ABSTRACT FROM AUTHOR]

Published

2018

14. Advancing Concussion Assessment in Pediatrics (A-CAP): a prospective, concurrent cohort, longitudinal study of mild traumatic brain injury in children: protocol study.

Author

Yeates, Keith Owen, Beauchamp, Miriam, Craig, William, Doan, Quynh, Zemek, Roger, Bjornson, Bruce, Gravel, Jocelyn, Mikrogianakis, Angelo, Goodyear, Bradley, Abdeen, Nishard, Beaulieu, Christian, Dehaes, Mathieu, Deschenes, Sylvain, Harris, Ashley, Lebel, Catherine, Lamont, Ryan, Williamson, Tyler, Barlow, Karen Maria, Bernier, Francois, and Brooks, Brian L.

Abstract

Introduction Paediatric mild traumatic brain injury (mTBI) is a public health burden. Clinicians urgently need evidence-based guidance to manage mTBI, but gold standards for diagnosing and predicting the outcomes of mTBI are lacking. The objective of the Advancing Concussion Assessment in Pediatrics (A-CAP) study is to assess a broad pool of neurobiological and psychosocial markers to examine associations with postinjury outcomes in a large sample of children with either mTBI or orthopaedic injury (OI), with the goal of improving the diagnosis and prognostication of outcomes of paediatric mTBI. Methods and analysis A-CAP is a prospective, longitudinal cohort study of children aged 8.00-16.99 years with either mTBI or OI, recruited during acute emergency department (ED) visits at five sites from the Pediatric Emergency Research Canada network. Injury information is collected in the ED; follow-up assessments at 10 days and 3 and 6 months postinjury measure a variety of neurobiological and psychosocial markers, covariates/confounders and outcomes. Weekly postconcussive symptom ratings are obtained electronically. Recruitment began in September 2016 and will occur for approximately 24 months. Analyses will test the major hypotheses that neurobiological and psychosocial markers can: (1) differentiate mTBI from OI and (2) predict outcomes of mTBI. Models initially will focus within domains (eg, genes, imaging biomarkers, psychosocial markers), followed by multivariable modelling across domains. The planned sample size (700 mTBI, 300 OI) provides adequate statistical power and allows for internal cross-validation of some analyses. Ethics and dissemination The ethics boards at all participating institutions have approved the study and all participants and their parents will provide informed consent or assent. Dissemination will follow an integrated knowledge translation plan, with study findings presented at scientific conferences and in multiple manuscripts in peer-reviewed journals. [ABSTRACT FROM AUTHOR]

Published

2017

15. Mosaic trisomy 1q: a recurring chromosome anomaly that is a diagnostic challenge and is associated with a Fryns-like phenotype.

Author

Bone, Kathleen M., Chernos, Judy E., Perrier, Renee, Innes, A. Micheil, Bernier, Francois P., McLeod, Ross, and Thomas, Mary Ann

Abstract

Objective: Trisomy of the long arm of chromosome 1 is a very rare cytogenetic anomaly that is difficult to diagnose because of tissue-limited mosaicism. This study aimed to further characterize the prenatal and post-natal findings associated with this anomaly, including the first reported chromosomal microarray finding.Method: This is a retrospective study of six cases of mos 46,X,der(Y)t(Y;1)(q12;q21)/46,XY, diagnosed both prenatally and post-natally. Detailed clinical features and pregnancy outcome were documented.Results: Recurrent prenatal and post-natal features of our case series, as well as the previously reported cases, were described, suggesting a Fryns-like phenotype. A diagnosis of mosaic trisomy 1q is difficult to confirm post-natally in some cases because of the tissue provided for analysis, emphasizing the need to study multiple tissue types in cases of fetal loss with a suspected underlying chromosomal imbalance.Conclusion: The overlap of clinical features between mosaic trisomy 1q and Fryns syndrome emphasizes the need to obtain appropriate samples for genetic analysis. The present cases and a review of the literature suggest that partial trisomy of the long arm of chromosome 1 is a distinct de novo clinical entity with low recurrence risk. © 2017 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2017

16. A novel NDUFS4 frameshift mutation causes Leigh disease in the Hutterite population.

Author

Lamont, Ryan E., Beaulieu, Chandree L., Bernier, Francois P., Sparkes, Rebecca, Innes, A. Micheil, Jackel‐Cram, Candice, Ober, Carole, Parboosingh, Jillian S., and Lemire, Edmond G.

Abstract

Leigh disease is a progressive, infantile-onset, neurodegenerative disorder characterized by feeding difficulties, failure to thrive, hypotonia, seizures, and central respiratory compromise. Metabolic and neuroimaging investigations typically identify abnormalities consistent with a disorder of mitochondrial energy metabolism. Mutations in more than 35 genes affecting the mitochondrial respiratory chain encoded from both the nuclear and mitochondrial genomes have been associated with Leigh disease. The clinical presentations of five individuals of Hutterite descent with Leigh disease are described herein. An identity-by-descent mapping and candidate gene approach was used to identify a novel homozygous c.393dupA frameshift mutation in the NADH dehydrogenase (ubiquinone) Fe-S protein 4 ( NDUFS4) gene. The carrier frequency of this mutation was estimated in >1,300 Hutterite individuals to be 1 in 27. © 2017 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2017

17. OP168 Costs And Effectiveness Of Whole Exome Sequencing (WES) In Patients With Unsolved Rare Disease Through The Diagnostic Pathway.

Author

Marshall, Deborah A, Degeling, Koen, Tagimacruz, Toni, Seeger, Trevor A., Boycott, Kym M, Bernier, Francois, Mendoza-Londona, Roberto, MacDonald, Karen V., Hartley, Taila, and Hayeems, Robin Z.

Abstract

Introduction: Patients suspected of having a rare genetic disease often experience lengthy and costly diagnostic odysseys. The timing of whole exome sequencing (WES) in the testing sequence, its diagnostic yield and test costs in the sequence all factor into estimates of cost-effectiveness analysis for health technology assessment. Methods: We modeled the diagnostic pathway using a discrete event simulation model, starting with the first test result. We defined and populated the simulation based on data from the electronic medical records of n=307 from the Care-for-Rare SOLVE multi-center Canadian observational cohort. Five alternative diagnostic pathways were modeled based on the observed data: no WES, and WES as the first, second, third or fourth test in the sequence. WES as the second test in the sequence is considered standard of care in medical genetic centers in Canada. We assessed effectiveness of WES in terms of diagnostic yield, time to diagnosis, and costs as patient-level overall test costs (2020 CAD/USD) across the diagnostic pathway. Results: Compared to molecular and specialized diagnostic tests only (i.e., no WES), WES increased diagnostic yield from 5 percent to 40 percent. The shortest time to diagnosis for those with a diagnosis was 1.82 years in the diagnostic pathway with WES as the second test. Test costs for each pathway were CAD2,800 (USD2,087, no WES), CAD2,700 (USD2,013, WES as first test), CAD3,500 (USD2,609, WES as second test), CAD4,500 (USD3,354, WES as third test), and CAD5,300 (USD3,951, WES as fourth test). Conclusions: Placing WES earlier in the diagnostic pathway for patients suspected of having a rare disease is associated with an increased diagnostic yield, reduced time to diagnosis and lower overall test costs with the benefits being greater the earlier in the pathway that WES is implemented. [ABSTRACT FROM AUTHOR]

Published

2023

18. Copy-number variations are enriched for neurodevelopmental genes in children with developmental coordination disorder.

Author

Mosca, Stephen J., Langevin, Lisa Marie, Dewey, Deborah, Innes, A. Micheil, Lionel, Anath C., Marshall, Christian C., Scherer, Stephen W., Parboosingh, Jillian S., and Bernier, Francois P.

Abstract

Background Developmental coordination disorder is a common neurodevelopment disorder that frequently co-occurs with other neurodevelopmental disorders including attention-deficit hyperactivity disorder (ADHD). Copy-number variations (CNVs) have been implicated in a number of neurodevelopmental and psychiatric disorders; however, the proportion of heritability in developmental coordination disorder (DCD) attributed to CNVs has not been explored. Objective This study aims to investigate how CNVs may contribute to the genetic architecture of DCD. Methods CNV analysis was performed on 82 extensively phenotyped Canadian children with DCD, with or without co-occurring ADHD and/or reading disorder, and 2988 healthy European controls using identical genome-wide SNP microarrays and CNV calling algorithms. Results An increased rate of large and rare genic CNVs (p=0.009) was detected, and there was an enrichment of duplications spanning brain-expressed genes (p=0.039) and genes previously implicated in other neurodevelopmental disorders (p=0.043). Genes and loci of particular interest in this group included: GAP43, RBFOX1, PTPRN2, SHANK3, 16p11.2 and distal 22q11.2. Although no recurrent CNVs were identified, 26% of DCD cases, where sample availability permitted segregation analysis, were found to have a de novo rare CNV. Of the inherited CNVs, 64% were from a parent who also had a neurodevelopmental disorder. Conclusions These findings suggest that there may be shared susceptibility genes for DCD and other neurodevelopmental disorders and highlight the need for thorough phenotyping when investigating the genetics of neurodevelopmental disorders. Furthermore, these data provide compelling evidence supporting a genetic basis for DCD, and further implicate rare CNVs in the aetiology of neurodevelopmental disorders. [ABSTRACT FROM AUTHOR]

Published

2016

19. The Concept of Atypical Brain Development in Developmental Coordination Disorder (DCD)-a New Look.

Author

Dewey, Deborah and Bernier, Francois

Published

2016

20. Cerebro-costo-mandibular syndrome: Clinical, radiological, and genetic findings.

Author

Tooley, Madeleine, Lynch, Danielle, Bernier, Francois, Parboosingh, Jillian, Bhoj, Elizabeth, Zackai, Elaine, Calder, Alistair, Itasaki, Nobue, Wakeling, Emma, Scott, Richard, Lees, Melissa, Clayton‐Smith, Jill, Blyth, Moira, Morton, Jenny, Shears, Debbie, Kini, Usha, Homfray, Tessa, Clarke, Angus, Barnicoat, Angela, and Wallis, Colin

Abstract

Cerebro-Costo-Mandibular syndrome (CCMS) is a rare autosomal dominant condition comprising branchial arch-derivative malformations with striking rib-gaps. Affected patients often have respiratory difficulties, associated with upper airway obstruction, reduced thoracic capacity, and scoliosis. We describe a series of 12 sporadic and 4 familial patients including 13 infants/children and 3 adults. Severe micrognathia and reduced numbers of ribs with gaps are consistent findings. Cleft palate, feeding difficulties, respiratory distress, tracheostomy requirement, and scoliosis are common. Additional malformations such as horseshoe kidney, hypospadias, and septal heart defect may occur. Microcephaly and significant developmental delay are present in a small minority of patients. Key radiological findings are of a narrow thorax, multiple posterior rib gaps and abnormal costo-transverse articulation. A novel finding in 2 patients is bilateral accessory ossicles arising from the hyoid bone. Recently, specific mutations in SNRPB, which encodes components of the major spliceosome, have been found to cause CCMS. These mutations cluster in an alternatively spliced regulatory exon and result in altered SNRPB expression. DNA was available from 14 patients and SNRPB mutations were identified in 12 (4 previously reported). Eleven had recurrent mutations previously described in patients with CCMS and one had a novel mutation in the alternative exon. These results confirm the specificity of SNRPB mutations in CCMS and provide further evidence for the role of spliceosomal proteins in craniofacial and thoracic development. © 2016 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2016

21. A relatively mild skeletal ciliopathy phenotype consistent with cranioectodermal dysplasia is associated with a homozygous nonsynonymous mutation in WDR35.

Author

Smith, Christopher, Lamont, Ryan E., Wade, Andrew, Bernier, Francois P., Parboosingh, Jillian S., and Innes, A. Micheil

Abstract

Ciliopathies are a class of clinically and genetically heterogeneous disorders characterized by deficits of the primary cilium, an important organelle for cellular signaling and development. Here we report on a patient from a consanguineous family presenting with renal cysts, short stature, distinctive facial features, missing teeth, brachydactyly, narrow chest, and abnormal ribs. His phenotype resembled a skeletal ciliopathy and the initial clinical differential diagnosis included Jeune thoracic dystrophy and cranioectodermal dysplasia. Due to the presence of parental consanguinity, a homozygous recessive mutation was the suspected cause and homozygosity mapping was used to direct candidate gene sequencing. WDR35, an intraflagellar transport protein previously associated with cranioectodermal dysplasia, the more severe short rib polydactyly syndrome type V and recently Ellis van Creveld syndrome, is present within a region of homozygosity and sequencing of all coding exons identified a novel homozygous nonsynonymous variant, p.Trp1153Cys. This variant affects a highly conserved tryptophan residue, is predicted to be deleterious, and is the most distal mutation yet reported in WDR35. This case expands the spectrum of phenotypes caused by WDR35 mutations, which we review herein. © 2015 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2016

22. Anti‐inflammation as one of the mechanisms in the improvement of cognitive function by probiotic Bifidobacterium breve strain.

Author

Ohno, Kazuya, Bernier, Francois, Katsumata, Noriko, Shimizu, Takashi, and Xiao, Jin‐Zhong

Published

2021

23. GeneMatcher Aids in the Identification of a New Malformation Syndrome with Intellectual Disability, Unique Facial Dysmorphisms, and Skeletal and Connective Tissue Abnormalities Caused by De Novo Variants in HNRNPK.

Author

Au, P. Y. Billie, You, Jing, Caluseriu, Oana, Schwartzentruber, Jeremy, Majewski, Jacek, Bernier, Francois P., Ferguson, Marcia, Valle, David, Parboosingh, Jillian S., Sobreira, Nara, Innes, A. Micheil, and Kline, Antonie D.

Abstract

ABSTRACT We report a new syndrome due to loss-of-function variants in the heterogeneous nuclear ribonucleoprotein K gene ( HNRNPK). We describe two probands: one with a de novo frameshift (NM_002140.3: c.953+1dup), and the other with a de novo splice donor site variant (NM_002140.3: c.257G>A). Both probands have intellectual disability, a shared unique craniofacial phenotype, and connective tissue and skeletal abnormalities. The identification of this syndrome was made possible by a new online tool, GeneMatcher, which facilitates connections between clinicians and researchers based on shared interest in candidate genes. This report demonstrates that new Web-based approaches can be effective in helping investigators solve exome sequencing projects, and also highlights the newer paradigm of 'reverse phenotyping,' where characterization of syndromic features follows the identification of genetic variants. [ABSTRACT FROM AUTHOR]

Published

2015

24. Matching Two Independent Cohorts Validates DPH1 as a Gene Responsible for Autosomal Recessive Intellectual Disability with Short Stature, Craniofacial, and Ectodermal Anomalies.

Author

Loucks, Catrina M., Parboosingh, Jillian S., Shaheen, Ranad, Bernier, Francois P., McLeod, D. Ross, Seidahmed, Mohammed Z., Puffenberger, Erik G., Ober, Carole, Hegele, Robert A., Boycott, Kym M., Alkuraya, Fowzan S., and Innes, A. Micheil

Abstract

ABSTRACT Recently, Alazami et al. (2015) identified 33 putative candidate disease genes for neurogenetic disorders. One such gene was DPH1, in which a homozygous missense mutation was associated with a 3C syndrome-like phenotype in four patients from a single extended family. Here, we report a second homozygous missense variant in DPH1, seen in four members of a founder population, and associated with a phenotype initially reminiscent of Sensenbrenner syndrome. This postpublication 'match' validates DPH1 as a gene underlying syndromic intellectual disability with short stature and craniofacial and ectodermal anomalies, reminiscent of, but distinct from, 3C and Sensenbrenner syndromes. This validation took several years after the independent discoveries due to the absence of effective methods for sharing both candidate phenotype and genotype data between investigators. Sharing of data via Web-based anonymous data exchange servers will play an increasingly important role toward more efficient identification of the molecular basis for rare Mendelian disorders. [ABSTRACT FROM AUTHOR]

Published

2015

25. The clinical application of genome-wide sequencing for monogenic diseases in Canada: Position Statement of the Canadian College of Medical Geneticists.

Author

Boycott, Kym, Hartley, Taila, Adam, Shelin, Bernier, Francois, Karen Chong, Fernandez, Bridget A., Friedman, Jan M., Geraghty, Michael T., Hume, Stacey, Knoppers, Bartha M., Laberge, Anne-Marie, Majewski, Jacek, Mendoza-Londono, Roberto, Stephen Meyn, M., Michaud, Jacques L., Nelson, Tanya N., Richer, Julie, Sadikovic, Bekim, Skidmore, David L., and Stockley, Tracy

Abstract

Purpose and scope The aim of this Position Statement is to provide recommendations for Canadian medical geneticists, clinical laboratory geneticists, genetic counsellors and other physicians regarding the use of genome-wide sequencing of germline DNA in the context of clinical genetic diagnosis. This statement has been developed to facilitate the clinical translation and development of best practices for clinical genome-wide sequencing for genetic diagnosis of monogenic diseases in Canada; it does not address the clinical application of this technology in other fields such as molecular investigation of cancer or for population screening of healthy individuals. Methods of statement development Two multidisciplinary groups consisting of medical geneticists, clinical laboratory geneticists, genetic counsellors, ethicists, lawyers and genetic researchers were assembled to review existing literature and guidelines on genome-wide sequencing for clinical genetic diagnosis in the context of monogenic diseases, and to make recommendations relevant to the Canadian context. The statement was circulated for comment to the Canadian College of Medical Geneticists (CCMG) membership-at-large and, following incorporation of feedback, approved by the CCMG Board of Directors. The CCMG is a Canadian organisation responsible for certifying medical geneticists and clinical laboratory geneticists, and for establishing professional and ethical standards for clinical genetics services in Canada. Results and conclusions Recommendations include (1) clinical genome-wide sequencing is an appropriate approach in the diagnostic assessment of a patient for whom there is suspicion of a significant monogenic disease that is associated with a high degree of genetic heterogeneity, or where specific genetic tests have failed to provide a diagnosis; (2) until the benefits of reporting incidental findings are established, we do not endorse the intentional clinical analysis of disease-associated genes other than those linked to the primary indication; and (3) clinicians should provide genetic counselling and obtain informed consent prior to undertaking clinical genome-wide sequencing. Counselling should include discussion of the limitations of testing, likelihood and implications of diagnosis and incidental findings, and the potential need for further analysis to facilitate clinical interpretation, including studies performed in a research setting. These recommendations will be routinely reevaluated as knowledge of diagnostic and clinical utility of clinical genome-wide sequencing improves. While the document was developed to direct practice in Canada, the applicability of the statement is broader and will be of interest to clinicians and health jurisdictions internationally. [ABSTRACT FROM AUTHOR]

Published

2015

26. Copy number variants (CNVs) analysis in a deeply phenotyped cohort of individuals with intellectual disability (ID).

Author

Ying Qiao, Mercier, Eloi, Dastan, Jila, Hurlburt, Jane, McGillivray, Barbara, Chudley, Albert E., Farrell, Sandra, Bernier, Francois P., Lewis, M. E. Suzanne, Pavlidis, Paul, and Rajcan-Separovic, Evica

Abstract

Background: DNA copy number variants (CNVs) are found in 15% of subjects with ID but their association with phenotypic abnormalities has been predominantly studied in smaller cohorts of subjects with detailed yet non-systematically categorized phenotypes, or larger cohorts (thousands of cases) with smaller number of generalized phenotypes. Methods: We evaluated the association of de novo, familial and common CNVs detected in 78 ID subjects with phenotypic abnormalities classified using the Winter-Baraitser Dysmorphology Database (WBDD) (formerly the London Dysmorphology Database). Terminology for 34 primary (coarse) and 169 secondary (fine) phenotype features were used to categorize the abnormal phenotypes and determine the prevalence of each phenotype in patients grouped by the type of CNV they had. Results: In our cohort more than 50% of cases had abnormalities in primary categories related to head (cranium, forehead, ears, eye globes, eye associated structures, nose) as well as hands and feet. The median number of primary and secondary abnormalities was 12 and 18 per subject, respectively, indicating that the cohort consisted of subjects with a high number of phenotypic abnormalities (median De Vries score for the cohort was 5). The prevalence of each phenotypic abnormality was comparable in patients with de novo or familial CNVs in comparison to those with only common CNVs, although a trend for increased frequency of cranial and forehead abnormalities was noted in subjects with rare de novo and familial CNVs. Two clusters of subjects were identified based on the prevalence of each fine phenotypic feature, with an average of 28.3 and 13.5 abnormal phenotypes/subject in the two clusters respectively (P < 0.05). Conclusions: Our study is a rare example of using standardized, deep morphologic phenotype clustering with phenotype/CNV correlation in a cohort of subjects with ID. The composition of the cohort inevitably influences the phenotype/genotype association, and our studies show that the influence of the de novo CNVs on the phenotype is less obvious in cohorts consisting of subjects with a high number of phenotypic abnormalities. The outcome of phenotype/genotype analysis also depends on the choice of phenotypes assessed and standardized phenotyping is required to minimize variability. [ABSTRACT FROM AUTHOR]

Published

2014

27. Validation of congenital anomaly coding in Canada's administrative databases compared with a congenital anomaly registry.

Author

Metcalfe, Amy, Sibbald, Barbara, Lowry, R. Brian, Tough, Suzanne, and Bernier, Francois P.

Abstract

Background Congenital anomaly (CA) surveillance provides epidemiologic data that are necessary for health planning. Approaches to CA surveillance vary; however, an increasing number of jurisdictions rely on administrative health databases for case ascertainment. This study aimed to assess the validity of CA coding in three administrative databases compared with a CA registry. Methods A cohort of 5862 live and stillborn infants from Calgary Alberta Canada was created through linking 12 clinical and administrative databases. Diagnostic codes for all health care contacts (hospitalizations, emergency room visits, out-patient physician visits) in the first 3 months of life were examined for relevant International Classification of Disease codes. Sensitivity, positive predictive values, and kappa coefficients were calculated, and data from the Alberta Congenital Anomalies Surveillance System was used as the reference standard. Results The ability of administrative data to accurately ascertain CAs varied by data source and the specificity of the diagnosis. Consistently, hospitalization data out-performed other administrative data sources in terms of sensitivity, positive predictive values, and kappa. Kappa scores for CAs easily visible at birth ranged from moderate (0.62 for emergency room visits and 0.65 for out-patient physician claims) to good (0.83 for hospitalization data) depending on the data source. Conclusion The validity of CA coding in administrative databases compared with a CA registry varies by database used and by CA studied. This has important implications for national surveillance efforts. Condition-specific validity should be assessed locally before use of these data sources for research or planning purposes. Birth Defects Research (Part A) 100:59-66, 2014. © 2013 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2014

28. How Do Interactions Between Early Caregiving Environment and Genes Influence Health and Behavior?

Author

Letourneau, Nicole, Giesbrecht, Gerald F., Bernier, Francois P., and Joschko, Justin

Subjects

HYPOTHALAMUS physiology, ENDOCRINE gland physiology, ATTACHMENT behavior, CHILD rearing, CHILD behavior, CHILDREN'S health, GENE expression, GENES, GENETIC polymorphisms, INFANT development, PARENT-infant relationships, SYSTEMATIC reviews, HOME environment

Published

2014

29. The Alberta Pregnancy Outcomes and Nutrition (APrON) cohort study: rationale and methods.

Author

Kaplan, Bonnie J., Giesbrecht, Gerald F., Leung, Brenda M.Y., Field, Catherine J., Dewey, Deborah, Bell, Rhonda C., Manca, Donna P., O'Beirne, Maeve, Johnston, David W., Pop, Victor J., Singhal, Nalini, Gagnon, Lisa, Bernier, Francois P., Eliasziw, Misha, McCargar, Linda J., Kooistra, Libbe, Farmer, Anna, Cantell, Marja, Goonewardene, Laki, and Casey, Linda M.

Subjects

DNA analysis, ADIPOSE tissues, BODY weight, CHILD Behavior Checklist, ESSENTIAL fatty acids, FATHERS, FOLIC acid, HEMOGLOBINS, INFANT development, INTERVIEWING, IRON, LONGITUDINAL method, EVALUATION of medical care, MEDICAL history taking, MENTAL health, CLASSIFICATION of mental disorders, MOTHERS, PREGNANCY, PREGNANCY complications, PROBABILITY theory, PSYCHOLOGICAL tests, PUERPERIUM, QUESTIONNAIRES, RESEARCH funding, SKINFOLD thickness, STATISTICS, STATURE, THYROXINE, TIME, VITAMIN B6, DATA analysis, SOCIOECONOMIC factors, SYMPTOMS, EDINBURGH Postnatal Depression Scale, FOOD diaries, PHYSICAL activity, DATA analysis software, WAIST circumference, NUTRITIONAL status

Abstract

The Alberta Pregnancy Outcomes and Nutrition (APrON) study is an ongoing prospective cohort study that recruits pregnant women early in pregnancy and, as of 2012, is following up their infants to 3 years of age. It has currently enrolled approximately 5000 Canadians (2000 pregnant women, their offspring and many of their partners). The primary aims of the APrON study were to determine the relationships between maternal nutrient intake and status, before, during and after gestation, and (1) maternal mood; (2) birth and obstetric outcomes; and (3) infant neurodevelopment. We have collected comprehensive maternal nutrition, anthropometric, biological and mental health data at multiple points in the pregnancy and the post-partum period, as well as obstetrical, birth, health and neurodevelopmental outcomes of these pregnancies. The study continues to follow the infants through to 36 months of age. The current report describes the study design and methods, and findings of some pilot work. The APrON study is a significant resource with opportunities for collaboration. [ABSTRACT FROM AUTHOR]

Published

2014

30. The hutterite variant of treacher collins syndrome: A 28-year-old story solved.

Author

Caluseriu, Oana, Lowry, Brian R., McLeod, Ross, Lamont, Ryan, Parboosingh, Jillian S., Bernier, Francois P., and Innes, A. Micheil

Abstract

Treacher Collins syndrome (TCS), the best known form of mandibulofacial dysostosis (MFD) comprises a recognizable pattern of anomalies. In 1985, Lowry et al. reported on two Hutterite sisters born to apparently unaffected parents with TCS, raising the possibility of an autosomal recessive (AR) variant of TCS, subsequently given a unique Mendelian Inheritance of Man (MIM) number (248390). Recently, biallelic mutations in POLR1C were found in TCS patients, confirming AR TCS as a distinct entity. The Hutterites, an endogamous Anabaptist group, like other genetically isolated populations, provide a powerful resource for mapping AR disorders. We elected to study the molecular basis of TCS in the Hutterite population including the original kindred described in 1985, and another unrelated Hutterite patient. Prior to starting this study, a TCOF1 mutation had apparently been excluded in the original family at two outside institutions. We hypothesized that an AR variant of TCS was present in the three Hutterite patients, but homozygosity mapping did not show convincing evidence of shared regions between the affected individuals. TCOF1 analysis was undertaken and mutations were found in the three affected patients and an unaffected parent. These data show that the initial Hutterite family reported with AR TCS in fact has classic TCS due to a TCOF1 mutation, despite recent data confirming the existence of AR TCS in other populations. These results have significant counseling implications for the affected families in the Hutterite population and in the population at large. © 2013 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2013

31. Possible autosomal recessive inheritance in an infant with acrofacial dysostosis similar to nager syndrome.

Author

Nur, Banu Guzel, Bernier, Francois P., Oztekin, Osman, KardelEN, Fırat, Kalay, Salih, Parboosingh, Jillian S., and Mihci, Ercan

Abstract

The acrofacial dysostosis syndromes, which are characterized by malformations of the craniofacial region and limbs, are a clinically heterogeneous group of disorders. Based primarily on the of the pattern of limb defects two major groups have emerged: Nager syndrome with predominantly preaxial malformations plus mandibulofacial dysostosis (severe micrognathia and malar hypoplasia) and Miller syndrome with postaxial malformations plus mandibulofacial dysostosis. Among these syndromes, Nager syndrome is a rare condition but the most common form of acrofacial dysostosis. Most cases are sporadic, while autosomal dominant and autosomal recessive inheritance patterns have been reported. Recently, heterozygous mutations in the SF3B4 gene on chromosome 1q12-q21 were found to be responsible for a subset of sporadic and autosomal dominant cases. We present a female infant born to consanguineous parents with craniofacial features resembling Nager syndrome and a unilateral preaxial limb malformation. Mutation analysis of coding exons of SF3B4 did not identify any mutations. This couple also had a deceased child who had similar clinical features. We conclude that, the presence of consanguinity and absence of mutation in SF3B4, provides evidence in support of a recessive form of Nager syndrome. © 2013 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2013

32. Circulating miRNA Biomarkers for Alzheimer's Disease.

Author

Kumar, Pavan, Dezso, Zoltan, MacKenzie, Crystal, Oestreicher, Judy, Agoulnik, Sergei, Byrne, Michael, Bernier, Francois, Yanagimachi, Mamoru, Aoshima, Ken, and Oda, Yoshiya

Subjects

MICRORNA, BIOMARKERS, ALZHEIMER'S disease, EARLY diagnosis, DISEASE progression, NON-coding RNA, CLINICAL trials

Abstract

A minimally invasive diagnostic assay for early detection of Alzheimer's disease (AD) is required to select optimal patient groups in clinical trials, monitor disease progression and response to treatment, and to better plan patient clinical care. Blood is an attractive source for biomarkers due to minimal discomfort to the patient, encouraging greater compliance in clinical trials and frequent testing. MiRNAs belong to the class of non-coding regulatory RNA molecules of ∼22 nt length and are now recognized to regulate ∼60% of all known genes through post-transcriptional gene silencing (RNAi). They have potential as useful biomarkers for clinical use because of their stability and ease of detection in many tissues, especially blood. Circulating profiles of miRNAs have been shown to discriminate different tumor types, indicate staging and progression of the disease and to be useful as prognostic markers. Recently their role in neurodegenerative diseases, both as diagnostic biomarkers as well as explaining basic disease etiology has come into focus. Here we report the discovery and validation of a unique circulating 7-miRNA signature (hsa-let-7d-5p, hsa-let-7g-5p, hsa-miR-15b-5p, hsa-miR-142-3p, hsa-miR-191-5p, hsa-miR-301a-3p and hsa-miR-545-3p) in plasma, which could distinguish AD patients from normal controls (NC) with >95% accuracy (AUC of 0.953). There was a >2 fold difference for all signature miRNAs between the AD and NC samples, with p-values<0.05. Pathway analysis, taking into account enriched target mRNAs for these signature miRNAs was also carried out, suggesting that the disturbance of multiple enzymatic pathways including lipid metabolism could play a role in AD etiology. [ABSTRACT FROM AUTHOR]

Published

2013

33. Longer Term Survival of a Child With Autosomal Recessive Cutis Laxa Due to a Mutation in FBLN4.

Author

Sawyer, Sarah L., Dicke, Frank, Kirton, Adam, Rajapkse, Thilinie, Rebeyka, Ivan M., McInnes, Brenda, Parboosingh, Jillian S., and Bernier, Francois P.

Abstract

Autosomal recessive cutis laxa (ARCL) is a clinically and genetically heterogeneous group of disorders characterized by loose, inelastic skin and variable systemic involvement and severity. Mutations in the FBLN4 gene are associated with ARCL1B. Fibulin-4 is important in elastic fiber formation and smooth muscle cell differentiation. We describe herein an 8-year-old boy who presented with severe aortic root dilatation and arterial tortuosity at 1 year of age which required surgical repair. His parents were consanguineous and there was a family history of three brothers who died early in life with an unknown type of connective tissue disorder in the 1960s. Both parents of the patient reported here were related to these three boys. We used a homozygosity mapping strategy with a 900K SNP array and identified FBLN4 as a candidate gene in an extended region of homozygosity. We sequenced this gene in the patient and identified a homozygous non-synonymous mutation at c.376G>A (p.Glu126Lys) in exon 5 that was predicted to be damaging. ARCL1B has most typically been associated with early demise but our report suggests that long-term survival is possible. With this longer term survival we are learning more about the natural history of this disorder, which includes baroreceptor reflex failure and low bone mineral density in this patient. © 2013 Wiley Periodicals, Inc. [ABSTRACT FROM AUTHOR]

Published

2013

34. Impact of observed versus hypothesized service utilization on the incremental cost of first trimester screening and prenatal diagnosis for trisomy 21 in a Canadian province.

Author

Metcalfe, Amy, Currie, Gillian, Johnson, Jo‐Ann, Bernier, Francois, Lix, Lisa M., Lyon, Andrew W., and Tough, Suzanne C.

Abstract

ABSTRACT Objective The aim of this research was to determine the impact of observed versus hypothesized service utilization on the cost of first trimester screening (FTS) and prenatal diagnosis for trisomy 21 in a Canadian province. Methods A population-based pregnancy cohort was created by linking 12 clinical and administrative databases. Care trajectories were derived to examine utilization patterns for FTS, prenatal diagnosis, and pregnancy termination. A literature review was conducted to determine what utilization parameters were used in economic evaluations of FTS. Local cost data was applied to observed and hypothesized care trajectories. Results The observed mean cost per fetus with trisomy 21 detected prenatally using FTS was $129 606.04 compared with $27 021.45 for women who did not access FTS. Observed utilization of FTS and prenatal diagnosis among screen positive women and termination of pregnancy following prenatal diagnosis of trisomy 21 were substantially lower than hypothesized in existing cost effectiveness studies. Cost estimates were sensitive to hypothetical changes in utilization of prenatal screening, prenatal diagnosis, and pregnancy termination. Conclusion Literature-based estimates of the cost-effectiveness of prenatal screening may not accurately represent current local practice due to potentially unrealistic assumptions about what proportion of women will proceed to invasive testing and ultimately terminate an affected pregnancy. © 2013 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2013

35. Identification of Novel Mutations Confirms Pde4d as a Major Gene Causing Acrodysostosis.

Author

Lynch, Danielle C., Dyment, David A., Huang, Lijia, Nikkel, Sarah M., Lacombe, Didier, Campeau, Philippe M., Lee, Brendan, Bacino, Carlos A., Michaud, Jacques L., Bernier, Francois P., Consortium, FORGE Canada, Parboosingh, Jillian S., and Innes, A. Micheil

Abstract

ABSTRACT Acrodysostosis is characterized by nasal hypoplasia, peripheral dysostosis, variable short stature, and intellectual impairment. Recently, mutations in PRKAR1A were reported in patients with acrodysostosis and hormone resistance. Subsequently, mutations in a phosphodiesterase gene ( Pde4d) were identified in seven sporadic cases. We sequenced Pde4d in seven acrodysostosis patients from five families. Missense mutations were identified in all cases. Families showed de novo inheritance except one family with three affected children whose father was subsequently found to have subtle features of acrodysostosis. There were no recurrent mutations. Short stature and endocrine resistance are rare in this series; however, cognitive involvement and obesity were frequent. This last finding is relevant given Pde4d is insulin responsive and potentially involved in lipolysis. Pde4d encodes a cyclic AMP regulator and places Pde4d-related acrodysostosis within the same family of diseases as pseudohypoparathyroidism, pseudopseudohypoparathyroidism, PRKAR1A-related acrodysostosis and brachydactyly-mental retardation syndrome; all characterized by cognitive impairment and short distal extremities. [ABSTRACT FROM AUTHOR]

Published

2013

36. Increasing the quality of life from womb to grave: the importance of pregnancy and birth cohorts.

Author

Kaplan, Bonnie J., Leung, Brenda M., Giesbrecht, Gerald F., Field, Catherine J., Bernier, Francois P., Tough, Suzanne, Xinjie Cui, and Dewey, Deborah

Subjects

CHILDREN'S health, EXPERIMENTAL design, GENE expression, LONGITUDINAL method, MOTHERS, ENVIRONMENTAL exposure, FETAL development, SOCIAL history

Abstract

Copyright of Applied Physiology, Nutrition & Metabolism is the property of Canadian Science Publishing and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2013

37. Exome Sequencing Identifies SMAD3 Mutations as a Cause of Familial Thoracic Aortic Aneurysm and Dissection With Intracranial and Other Arterial Aneurysms.

Author

Regalado, Ellen S., Guo, Dong-chuan, Villamizar, Carlos, Avidan, Nili, Gilchrist, Dawna, McGillivray, Barbara, Clarke, Lorne, Bernier, Francois, Santos-Cortez, Regie L., Leal, Suzanne M., Bertoli-Avella, Aida M., Shendure, Jay, Rieder, Mark J., Nickerson, Deborah A., and Milewicz, Dianna M.

Published

2011

38. Distress and Psychosocial Needs of a Heterogeneous High Risk Familial Cancer Population.

Author

Power, Tara, Robinson, John, Bridge, Peter, Bernier, Francois, and Gilchrist, Dawna

Abstract

In order to assess the levels of distress and psychosocial support needs of a high risk population, we undertook a study to look at both the objective and subjective levels of distress and the wants and needs of individuals from a high familial cancer risk population. Three hundred and eighteen individuals (160 affected, 158 unaffected) completed several distress and psychosocial needs questionnaires (including the Brief Symptom Inventory-18). Sixty key informants were also surveyed about their perspective on the support needs of this population. In the largely female (90%), largely HBOC syndrome group (approximately 90%), 20% had significant levels of generalized distress, with no significant differences between affected and unaffected individuals. Generalized distress was also not significantly different as a function of mutation status. Individuals who received inconclusive test results, however, were more likely to indicate somatic symptoms of distress. Those individuals who did not have social support were more likely to be those who had never had cancer and who either had a mutation, received inconclusive test results, or were not tested. Key informants were most likely to indicate that patients need more support. These results provide evidence for the importance of establishing regular psychosocial distress screening, including a focus on somatic symptoms, in such high risk populations. [ABSTRACT FROM AUTHOR]

Published

2011

39. Application of Microarray-Based Comparative Genomic Hybridization in Prenatal and Postnatal Settings: Three Case Reports.

Author

Jing Liu, Bernier, Francois, Lauzon, Julie, Lowry, R. Brian, and Chernos, Judy

Abstract

Microarray-based comparative genomic hybridization (array CGH) is a newly emerged molecular cytogenetic technique for rapid evaluation of the entire genome with sub-megabase resolution. It allows for the comprehensive investigation of thousands and millions of genomic loci at once and therefore enables the efficient detection of DNA copy number variations (a.k.a, cryptic genomic imbalances). The development and the clinical application of array CGH have revolutionized the diagnostic process in patients and has provided a clue to many unidentified or unexplained diseases which are suspected to have a genetic cause. In this paper, we present three clinical cases in both prenatal and postnatal settings. Among all, array CGH played a major discovery role to reveal the cryptic and/or complex nature of chromosome arrangements. By identifying the genetic causes responsible for the clinical observation in patients, array CGH has provided accurate diagnosis and appropriate clinical management in a timely and efficient manner. [ABSTRACT FROM AUTHOR]

Published

2011

40. Developmental outcome of children who had choroid plexus cysts detected prenatally.

Author

Bernier, Francois P., Crawford, Susan G., and Dewey, Deborah

Abstract

Objective The purpose of this study was to evaluate cognitive, motor, language and adaptive behavior development in children who had isolated choroid plexus cysts (CPC) detected prenatally. Methods A retrospective double cohort design and standardized psychometric measures were used to compare the development of children who had isolated CPCs identified prenatally with a control group of children who had normal prenatal ultrasounds. Results Our study cohort ( n = 37) had a mean age of 3.88 years (SD = 0.83) and the control cohort ( n = 48) had a mean age of 4.62 years (SD = 1.03). The age difference between our cohorts was significant. There were no differences between cohorts in socioeconomic status, sex, birth weight or gestational age. Cognitive data showed no clinically significant difference in Full Scale IQ using the WISC-III or WPPSI-R (CPC = 113.97, control = 116.69). Scores on standardized measures of motor and adaptive functioning also did not show any significant group differences. Children with CPCs did score significantly lower than controls on some of the measures of verbal functioning; however, this difference was not associated with clinically significant delays. Conclusion We conclude that the presence of isolated CPCs on midtrimester ultrasound are unlikely to be associated with any significant neurocognitive delays in early childhood. Copyright © 2005 John Wiley & Sons, Ltd. [ABSTRACT FROM AUTHOR]

Published

2005

41. Cardiac features of a novel autosomal recessive dilated cardiomyopathic syndrome due to defective importation of mitochondrial protein.

Author

Sparkes, Rebecca, Patton, David, and Bernier, Francois

Published

2007

42. Correction to: 2020 CIS Annual Meeting: Immune Deficiency & Dysregulation North American Conference.

Author

Kalashnikova, Tatiana, Wright, Nicola, Midgley, Julian, Bernier, Francois, Luider, Joanne, and Murguia-Favela, Luis

Subjects

IMMUNODEFICIENCY, ANNUAL meetings, CONFERENCES & conventions

Abstract

The abstract with Submission ID#809896 has been revised due to duplicate title and the missing main author. [ABSTRACT FROM AUTHOR]

Published

2020

43. Fully Automatic Landmarking of Syndromic 3D Facial Surface Scans Using 2D Images.

Author

Bannister, Jordan J., Crites, Sebastian R., Aponte, J. David, Katz, David C., Wilms, Matthias, Klein, Ophir D., Bernier, Francois P. J., Spritz, Richard A., Hallgrímsson, Benedikt, and Forkert, Nils D.

Subjects

RECORDING & registration

Abstract

3D facial landmarks are known to be diagnostically relevant biometrics for many genetic syndromes. The objective of this study was to extend a state-of-the-art image-based 2D facial landmarking algorithm for the challenging task of 3D landmark identification on subjects with genetic syndromes, who often have moderate to severe facial dysmorphia. The automatic 3D facial landmarking algorithm presented here uses 2D image-based facial detection and landmarking models to identify 12 landmarks on 3D facial surface scans. The landmarking algorithm was evaluated using a test set of 444 facial scans with ground truth landmarks identified by two different human observers. Three hundred and sixty nine of the subjects in the test set had a genetic syndrome that is associated with facial dysmorphology. For comparison purposes, the manual landmarks were also used to initialize a non-linear surface-based registration of a non-syndromic atlas to each subject scan. Compared to the average intra- and inter-observer landmark distances of 1.1 mm and 1.5 mm respectively, the average distance between the manual landmark positions and those produced by the automatic image-based landmarking algorithm was 2.5 mm. The average error of the registration-based approach was 3.1 mm. Comparing the distributions of Procrustes distances from the mean for each landmarking approach showed that the surface registration algorithm produces a systemic bias towards the atlas shape. In summary, the image-based automatic landmarking approach performed well on this challenging test set, outperforming a semi-automatic surface registration approach, and producing landmark errors that are comparable to state-of-the-art 3D geometry-based facial landmarking algorithms evaluated on non-syndromic subjects. [ABSTRACT FROM AUTHOR]

Published

2020

44. Prenatal maternal and childhood bisphenol a exposure and brain structure and behavior of young children.

Author

Grohs, Melody N., Reynolds, Jess E., Liu, Jiaying, Martin, Jonathan W., Pollock, Tyler, Lebel, Catherine, Dewey, Deborah, the APrON Study Team, Kaplan, Bonnie J., Field, Catherine J., Bell, Rhonda C., Bernier, Francois P., Cantell, Marja, Casey, Linda M., Eliasziw, Misha, Farmer, Anna, Gagnon, Lisa, Giesbrecht, Gerald F., Goonewardene, Laksiri, and Johnston, David W.

Subjects

MATERNAL exposure, DIFFUSION magnetic resonance imaging, CHILD psychology, CHILD Behavior Checklist, NEURAL development, SECOND trimester of pregnancy, VOXEL-based morphometry, PRESCHOOL children

Abstract

Background: Bisphenol A (BPA) is commonly used in the manufacture of plastics and epoxy resins. In North America, over 90% of the population has detectable levels of urinary BPA. Human epidemiological studies have reported adverse behavioral outcomes with BPA exposure in children, however, corresponding effects on children's brain structure have not yet been investigated. The current study examined the association between prenatal maternal and childhood BPA exposure and white matter microstructure in children aged 2 to 5 years, and investigated whether brain structure mediated the association between BPA exposure and child behavior.Methods: Participants were 98 mother-child pairs who were recruited between January 2009 and December 2012. Total BPA concentrations in spot urine samples obtained from mothers in the second trimester of pregnancy and from children at 3-4 years of age were analyzed. Children participated in a diffusion magnetic resonance imaging (MRI) scan at age 2-5 years (3.7 ± 0.8 years). Associations between prenatal maternal and childhood BPA and children's fractional anisotropy and mean diffusivity of 10 isolated white matter tracts were investigated, controlling for urinary creatinine, child sex, and age at the time of MRI. Post-hoc analyses examined if alterations in white matter mediated the relationship of BPA and children's scores on the Child Behavior Checklist (CBCL).Results: Prenatal maternal urinary BPA was significantly associated with child mean diffusivity in the splenium and right inferior longitudinal fasciculus. Splenium diffusivity mediated the relationship between maternal prenatal BPA levels and children's internalizing behavior (indirect effect: β = 0.213, CI [0.0167, 0.564]). No significant associations were found between childhood BPA and white matter microstructure.Conclusions: This study provides preliminary evidence for the neural correlates of BPA exposure in humans. Our findings suggest that prenatal maternal exposure to BPA may lead to alterations in white matter microstructure in preschool aged children, and that such alterations mediate the relationship between early life exposure to BPA and internalizing problems. [ABSTRACT FROM AUTHOR]

Published

2019

45. Response to correspondence of NDUFS4-related Leigh syndrome in Hutterites.

Author

Lamont, Ryan E., Beaulieu, Chandree L., Bernier, Francois P., Sparkes, Rebecca, Innes, A. Micheil, Jackel‐Cram, Candice, Ober, Carole, Parboosingh, Jillian S., and Lemire, Edmond G.

Published

2017

46. Optimizing genotype quality metrics for individual exomes and cohort analysis.

Author

Gordon, Paul M. K., Dimnik, Leo, Lamont, Ryan, Innes, Micheil, Bernier, Francois, and Parboosingh, Jillian

Subjects

GENOMICS

Abstract

An abstract of the conference paper "Optimizing genotype quality metrics for individual exomes and cohort analysis," by Robinder Gauba and colleagues is presented.

Published

2012

47. Cover Image, Volume 170A, Number 5, May 2016.

Author

Tooley, Madeleine, Lynch, Danielle, Bernier, Francois, Parboosingh, Jillian, Bhoj, Elizabeth, Zackai, Elaine, Calder, Alistair, Itasaki, Nobue, Wakeling, Emma, Scott, Richard, Lees, Melissa, Clayton‐Smith, Jill, Blyth, Moira, Morton, Jenny, Shears, Debbie, Kini, Usha, Homfray, Tessa, Clarke, Angus, Barnicoat, Angela, and Wallis, Colin

Abstract

The cover image, by Sarah Smithson et al., is based on the Research Article Cerebro‐costo‐mandibular syndrome: Clinical, radiological, and genetic findings, DOI: 10.1002/ajmg.a.37587. [ABSTRACT FROM AUTHOR]

Published

2016

48. A single dose of the beta-secretase inhibitor, e2609, decreases CSF bace1 enzymatic activity in cynomolgus monkeys.

Author

Matijevic, Mark, Watanabe, Hideki, Sato, Yoshiaki, Bernier, Francois, McGrath, Shannon, Burns, Lynne, Yamamoto, Noboru, Ogo, Makoto, Dezso, Zoltan, Chow, Jesse, Oda, Yoshiya, Kaplow, June, and Albala, Bruce

Published

2015

49. Disrupted auto-regulation of the spliceosomal gene SNRPB causes cerebro-costo-mandibular syndrome.

Author

Lynch, Danielle C., Revil, Timothée, Schwartzentruber, Jeremy, Bhoj, Elizabeth J., Innes, A. Micheil, Lamont, Ryan E., Lemire, Edmond G., Chodirker, Bernard N., Taylor, Juliet P., Zackai, Elaine H., McLeod, D. Ross, Kirk, Edwin P., Hoover-Fong, Julie, Fleming, Leah, Savarirayan, Ravi, Majewski, Jacek, Jerome-Majewska, Loydie A., Parboosingh, Jillian S., and Bernier, Francois P.

Published

2014

50. Identification of Novel Mutations Confirms PDE4D as a Major Gene Causing Acrodysostosis.

Author

Lynch, Danielle C., Dyment, David A., Huang, Lijia, Nikkel, Sarah M., Lacombe, Didier, Campeau, Philippe M., Lee, Brendan, Bacino, Carlos A., Michaud, Jacques L., Bernier, Francois P., Consortium, FORGE Canada, Parboosingh, Jillian S., and Innes, A. Micheil

Published

2013