Your search keyword '"Sergey Batalov"' showing total 8 results

1. An automated 13.5 hour system for scalable diagnosis and acute management guidance for genetic diseases

Author

Mallory J. Owen, Sebastien Lefebvre, Christian Hansen, Chris M. Kunard, David P. Dimmock, Laurie D. Smith, Gunter Scharer, Rebecca Mardach, Mary J. Willis, Annette Feigenbaum, Anna-Kaisa Niemi, Yan Ding, Luca Van Der Kraan, Katarzyna Ellsworth, Lucia Guidugli, Bryan R. Lajoie, Timothy K. McPhail, Shyamal S. Mehtalia, Kevin K. Chau, Yong H. Kwon, Zhanyang Zhu, Sergey Batalov, Shimul Chowdhury, Seema Rego, James Perry, Mark Speziale, Mark Nespeca, Meredith S. Wright, Martin G. Reese, Francisco M. De La Vega, Joe Azure, Erwin Frise, Charlene Son Rigby, Sandy White, Charlotte A. Hobbs, Sheldon Gilmer, Gail Knight, Albert Oriol, Jerica Lenberg, Shareef A. Nahas, Kate Perofsky, Kyu Kim, Jeanne Carroll, Nicole G. Coufal, Erica Sanford, Kristen Wigby, Jacqueline Weir, Vicki S. Thomson, Louise Fraser, Seka S. Lazare, Yoon H. Shin, Haiying Grunenwald, Richard Lee, David Jones, Duke Tran, Andrew Gross, Patrick Daigle, Anne Case, Marisa Lue, James A. Richardson, John Reynders, Thomas Defay, Kevin P. Hall, Narayanan Veeraraghavan, and Stephen F. Kingsmore

Subjects

Pediatric, Pediatric Research Initiative, Multidisciplinary, DNA Copy Number Variations, Whole Genome Sequencing, Human Genome, Infant, General Physics and Astronomy, General Chemistry, General Biochemistry, Genetics and Molecular Biology, Good Health and Well Being, Genetics, Humans, Child, Biotechnology, Retrospective Studies

Abstract

While many genetic diseases have effective treatments, they frequently progress rapidly to severe morbidity or mortality if those treatments are not implemented immediately. Since front-line physicians frequently lack familiarity with these diseases, timely molecular diagnosis may not improve outcomes. Herein we describe Genome-to-Treatment, an automated, virtual system for genetic disease diagnosis and acute management guidance. Diagnosis is achieved in 13.5 h by expedited whole genome sequencing, with superior analytic performance for structural and copy number variants. An expert panel adjudicated the indications, contraindications, efficacy, and evidence-of-efficacy of 9911 drug, device, dietary, and surgical interventions for 563 severe, childhood, genetic diseases. The 421 (75%) diseases and 1527 (15%) effective interventions retained are integrated with 13 genetic disease information resources and appended to diagnostic reports (https://gtrx.radygenomiclab.com). This system provided correct diagnoses in four retrospectively and two prospectively tested infants. The Genome-to-Treatment system facilitates optimal outcomes in children with rapidly progressive genetic diseases.

Published

2022

2. Rapid Sequencing-Based Diagnosis of Thiamine Metabolism Dysfunction Syndrome

Author

Anna-Kaisa Niemi, Kevin Hall, Meredith S. Wright, Mark Speziale, Louise Fraser, Jerica Lenberg, Shimul Chowdhury, Tim K McPhail, Sergey Batalov, Luca Van Der Kraan, Kevin K Chau, David Dimmock, Vicki S Thomson, Christian Hansen, Yan Ding, Mark Nespeca, Shyamal S Mehtalia, Sheldon Gilmer, Stephen F. Kingsmore, Mallory J Owen, Zhanyang Zhu, Gail Knight, Chris M Kunard, Charlotte A. Hobbs, Jacqueline Weir, John Reynders, Narayanan Veeraraghavan, Bryan R. Lajoie, Sebastien Lefebvre, Shareef Nahas, and Thomas Defay

Subjects

Whole genome sequencing, Infantile encephalopathy, 2019-20 coronavirus outbreak, business.industry, Thiamine Metabolism, General Medicine, Bioinformatics, Genome, Article, Neurologic injury, X ray computed, Medicine, business, Genetic diagnosis

Abstract

Speedy Genetic Diagnosis Infantile encephalopathy is associated with approximately 1500 genetic diseases. Without prompt treatment, permanent neurologic injury or death may occur. Here, the genome ...

Published

2021

3. Author Correction: Rapid whole genome sequencing impacts care and resource utilization in infants with congenital heart disease

Author

Narayanan Veeraraghavan, Michelle M. Clark, John J. Nigro, Charlotte A. Hobbs, Sara A. Caylor, David Dimmock, Nathaly M. Sweeney, Shareef Nahas, Yan Ding, Julie A. Cakici, Sergey Batalov, Stephen F. Kingsmore, and Shimul Chowdhury

Subjects

Whole genome sequencing, Heart disease, business.industry, MEDLINE, Computational biology, QH426-470, Health care economics, medicine.disease, Congenital heart defects, Genetics, medicine, Medicine, business, Author Correction, Molecular Biology, Medical genomics, Genetics (clinical), Resource utilization

Abstract

Congenital heart disease (CHD) is the most common congenital anomaly and a major cause of infant morbidity and mortality. While morbidity and mortality are highest in infants with underlying genetic conditions, molecular diagnoses are ascertained in only ~20% of cases using widely adopted genetic tests. Furthermore, cost of care for children and adults with CHD has increased dramatically. Rapid whole genome sequencing (rWGS) of newborns in intensive care units with suspected genetic diseases has been associated with increased rate of diagnosis and a net reduction in cost of care. In this study, we explored whether the clinical utility of rWGS extends to critically ill infants with structural CHD through a retrospective review of rWGS study data obtained from inpatient infants 1 year with structural CHD at a regional children's hospital. rWGS diagnosed genetic disease in 46% of the enrolled infants. Moreover, genetic disease was identified five times more frequently with rWGS than microarray ± gene panel testing in 21 of these infants (rWGS diagnosed 43% versus 10% with microarray ± gene panels, p = 0.02). Molecular diagnoses ranged from syndromes affecting multiple organ systems to disorders limited to the cardiovascular system. The average daily hospital spending was lower in the time period post blood collection for rWGS compared to prior (p = 0.003) and further decreased after rWGS results (p = 0.000). The cost was not prohibitive to rWGS implementation in the care of this cohort of infants. rWGS provided timely actionable information that impacted care and there was evidence of decreased hospital spending around rWGS implementation.

Published

2021

4. An RCT of Rapid Genomic Sequencing among Seriously Ill Infants Results in High Clinical Utility, Changes in Management, and Low Perceived Harm

Author

David Dimmock, Cinnamon S. Bloss, Yan Ding, Kiely N. James, Katarzyna A. Ellsworth, Narayanan Veeraraghavan, Matthew N. Bainbridge, Amy S. Kimball, Jaime Barea, Christina Clarke, Jerica Lenberg, Shareef Nahas, Shimul Chowdhury, Erica Sanford, Patrick Mulrooney, Nathaly M. Sweeney, Sergey Batalov, Lauge Farnaes, Jennie Le, Cynthia Cheung, Mary Gaughran, Leila Schwanemann, Daniken Orendain, Maria Ortiz-Arechiga, Charlotte A. Hobbs, Marva Evans, Kelly Watkins, Marilyn C. Jones, Joshua J.A. Braun, Meredith S. Wright, Terence C. Wong, Carlos Diaz, Mari Tokita, Miguel Del Campo, Brian Lane, Stephen F. Kingsmore, Christian Hansen, Lisa Salz, Michelle M. Clark, Nicole G. Coufal, Casey Cohenmeyer, Joe Gleeson, Seema Rego, Kristen Wigby, Jennifer Friedman, Zaira Bezares, Mark Speziale, Sara A. Caylor, Lance Prince, Richard S. Song, Jose Honold, Albert Oriol, Catherine Yamada, Annette Feigenbaum, Lucitia Van Der Kraan, Sandra Leibel, Denise Suttner, Dana Mashburn, Laurel Moyer, Julie A. Cakici, Lynne M. Bird, Charles Sauer, Daeheon Oh, Iris Reyes, Gail Knight, Michele Feddock, and Jeanne Carroll

Subjects

0301 basic medicine, Male, medicine.medical_specialty, Neonatal intensive care unit, Time Factors, Critical Illness, Clinical Decision-Making, Logistic regression, Article, law.invention, 03 medical and health sciences, 0302 clinical medicine, Randomized controlled trial, law, 030225 pediatrics, Intensive care, Internal medicine, Intensive Care Units, Neonatal, Genetics, Medicine, Humans, Genetic Testing, Prospective Studies, Genetics (clinical), Pediatric intensive care unit, Whole Genome Sequencing, business.industry, Genome, Human, Genetic Diseases, Inborn, Infant, Newborn, Chromosome Mapping, Disease Management, Infant, Odds ratio, Distress, 030104 developmental biology, Logistic Models, Etiology, Female, sense organs, business

Abstract

The second Newborn Sequencing in Genomic Medicine and Public Health (NSIGHT2) study was a randomized, controlled trial of rapid whole-genome sequencing (rWGS) or rapid whole-exome sequencing (rWES) in infants with diseases of unknown etiology in intensive care units (ICUs). Gravely ill infants were not randomized and received ultra-rapid whole-genome sequencing (urWGS). Herein we report results of clinician surveys of the clinical utility of rapid genomic sequencing (RGS). The primary end-point-clinician perception that RGS was useful- was met for 154 (77%) of 201 infants. Both positive and negative tests were rated as having clinical utility (42 of 45 [93%] and 112 of 156 [72%], respectively). Physicians reported that RGS changed clinical management in 57 (28%) infants, particularly in those receiving urWGS (p = 0.0001) and positive tests (p < 0.00001). Outcomes of 32 (15%) infants were perceived to be changed by RGS. Positive tests changed outcomes more frequently than negative tests (p < 0.00001). In logistic regression models, the likelihood that RGS was perceived as useful increased 6.7-fold when associated with changes in management (95% CI 1.8-43.3). Changes in management were 10.1-fold more likely when results were positive (95% CI 4.7-22.4) and turnaround time was shorter (odds ratio 0.92, 95% CI 0.85-0.99). RGS seldom led to clinician-perceived confusion or distress among families (6 of 207 [3%]). In summary, clinicians perceived high clinical utility and low likelihood of harm with first-tier RGS of infants in ICUs with diseases of unknown etiology. RGS was perceived as beneficial irrespective of whether results were positive or negative.

Published

2020

5. A Randomized, Controlled Trial of the Analytic and Diagnostic Performance of Singleton and Trio, Rapid Genome and Exome Sequencing in Ill Infants

Author

David Dimmock, Dorjee Tamang, Sarah White, Peter Schols, Michelle M. Clark, Zaira Bezares, Richard S. Song, Sandra Leibel, Denise Suttner, Jennie Le, Charlotte A. Hobbs, Casey Cohenmeyer, Katarzyna A. Ellsworth, Brian Lane, Amber Hildreth, Lauge Farnaes, Kelly Watkins, Kiely N. James, Terence C. Wong, Cinnamon S. Bloss, Nicole G. Coufal, Laura Puckett, Mari Tokita, Lance Prince, Amy S. Kimball, Narayanan Veeraraghavan, Shareef Nahas, Cyrielle Kint, Yan Ding, Paulina Ordonez, Jaime Barea, Erica Sanford, Kristen Wigby, Daniken Orendain, Maria Ortiz-Arechiga, Meredith S. Wright, Dana Mashburn, Sara A. Caylor, Nathaly M. Sweeney, Joshua J.A. Braun, Christina Clarke, Audra Wise, Lisa Salz, Charles Sauer, Jenni Friedman, George Chiang, Jerica Lenberg, Mark Speziale, Laurel Moyer, Michele Feddock, Jeanne Carroll, Patrick Mulrooney, Raymond Hovey, Stephen F. Kingsmore, Marva Evans, Sergey Batalov, Albert Oriol, Joe Gleeson, Jose Honold, Carlos Diaz, Mary Gaughran, Julie A. Cakici, Crystal Le, Catherine Yamada, Shimul Chowdhury, Gail Knight, Matthew N. Bainbridge, Lucitia Van Der Kraan, Daeheon Oh, and Iris Reyes

Subjects

0301 basic medicine, ultra-rapid whole-genome sequencing, Pediatrics, medicine.medical_specialty, diagnosis, precision medicine, RCIGM Investigators, Clinical Trials and Supportive Activities, 030105 genetics & heredity, Genome, intensive care unit, Medical and Health Sciences, Article, law.invention, 03 medical and health sciences, Randomized controlled trial, law, genetic disease, Clinical Research, Exome Sequencing, medicine, Genetics, Humans, Genetic Testing, whole-exome sequencing, Genetics (clinical), Exome sequencing, Whole genome sequencing, Pediatric, Genetics & Heredity, Whole Genome Sequencing, business.industry, Singleton, Human Genome, Infant, Newborn, Infant, Biological Sciences, Precision medicine, Newborn, Intensive care unit, 030104 developmental biology, genomic medicine, Good Health and Well Being, whole-genome sequencing, Etiology, business

Abstract

The second Newborn Sequencing in Genomic Medicine and Public Health study was a randomized, controlled trial of the effectiveness of rapid whole-genome or -exome sequencing (rWGS or rWES, respectively) in seriously ill infants with diseases of unknown etiology. Here we report comparisons of analytic and diagnostic performance. Of 1,248 ill inpatient infants, 578 (46%) had diseases of unknown etiology. 213 infants (37% of those eligible) were enrolled within 96h of admission. 24 infants (11%) were very ill and received ultra-rapid whole-genome sequencing (urWGS). The remaining infants were randomized, 95 to rWES and 94 to rWGS. The analytic performance of rWGS was superior to rWES, including variants likely to affect protein function, and ClinVar pathogenic/likely pathogenic variants (p < 0.0001). The diagnostic performance of rWGS and rWES were similar (18 diagnoses in 94 infants [19%] versus 19 diagnoses in 95 infants [20%], respectively), as was time to result (median 11.0 versus 11.2days, respectively). However, the proportion diagnosed by urWGS (11 of 24 [46%]) was higher than rWES/rWGS (p = 0.004) and time to result was less (median 4.6days, p < 0.0001). The incremental diagnostic yield of reflexing to trio after negative proband analysis was 0.7% (1 of 147). In conclusion, rapid genomic sequencing can be performed as a first-tier diagnostic test in inpatient infants. urWGS had the shortest time to result, which was important in unstable infants, and those in whom a genetic diagnosis was likely to impact immediate management. Further comparison of urWGS and rWES is warranted because genomic technologies and knowledge of variant pathogenicity are evolving rapidly.

Published

2019

6. Publisher Correction: Rapid whole genome sequencing impacts care and resource utilization in infants with congenital heart disease

Author

Sara A. Caylor, Shareef Nahas, David Dimmock, John J. Nigro, Shimul Chowdhury, Stephen F. Kingsmore, Michelle M. Clark, Narayanan Veeraraghavan, Julie A. Cakici, Yan Ding, Nathaly M. Sweeney, Sergey Batalov, and Charlotte A. Hobbs

Subjects

Whole genome sequencing, Heart disease, Computational biology, Biology, Health care economics, QH426-470, medicine.disease, Publisher Correction, Congenital heart defects, medicine, Genetics, Medicine, Molecular Biology, Medical genomics, Genetics (clinical), Resource utilization

Published

2021

7. Diagnosis of genetic diseases in seriously ill children by rapid whole-genome sequencing and automated phenotyping and interpretation

Author

Terence C. Wong, Marie L. Janes, John Reynders, Martin G. Reese, Brett Williams, Patrick Mulrooney, Sergey Batalov, Kristen Wigby, Brandon Camp, Lauge Farnaes, Joshua J.A. Braun, Meredith S. Wright, Narayanan Veeraraghavan, Jeremy Gore, Shareef Nahas, David Dimmock, Sheldon Gilmer, Lisa Salz, Albert Oriol, Mari Tokita, Kejia Lin, Thomas Defay, Erica Sanford, Catherine Yamada, Nathaly M. Sweeney, Stephen F. Kingsmore, Yan Ding, Christina Clarke, Laura Puckett, Katarzyna A. Ellsworth, Richard Gain, Shauna George, Luca Van Der Kraan, Margaret Bray, Mary Gaughran, Curtis Beebe, Alison Frith, Kevin Hall, Kyle McBride, Amber Hildreth, Michelle M. Clark, Haiying Li Grunenwald, Julie Ryu, Cyrielle Kint, Kelly Watkins, Mitchell Creed, Jennifer Friedman, Shimul Chowdhury, Paul D. McDonagh, Zia Rady, Peter Schols, Joseph G. Gleeson, Julie A. Cakici, Lawrence Stewart, Raymond Hovey, Jeanne Carroll, Matthew N. Bainbridge, Daeheon Oh, Calum Yacoubian, Sara A. Caylor, and Sarah White

Subjects

0301 basic medicine, medicine.medical_specialty, 030105 genetics & heredity, Phenome, Genome, DNA sequencing, Diabetic Ketoacidosis, 03 medical and health sciences, Intensive care, medicine, Electronic Health Records, Humans, Medical diagnosis, Intensive care medicine, Natural Language Processing, Retrospective Studies, Whole genome sequencing, business.industry, General Medicine, Genomics, Intensive Care Units, 030104 developmental biology, DECIPHER, Female, Precision and recall, business

Abstract

By informing timely targeted treatments, rapid whole-genome sequencing can improve the outcomes of seriously ill children with genetic diseases, particularly infants in neonatal and pediatric intensive care units (ICUs). The need for highly qualified professionals to decipher results, however, precludes widespread implementation. We describe a platform for population-scale, provisional diagnosis of genetic diseases with automated phenotyping and interpretation. Genome sequencing was expedited by bead-based genome library preparation directly from blood samples and sequencing of paired 100-nt reads in 15.5 hours. Clinical natural language processing (CNLP) automatically extracted children’s deep phenomes from electronic health records with 80% precision and 93% recall. In 101 children with 105 genetic diseases, a mean of 4.3 CNLP-extracted phenotypic features matched the expected phenotypic features of those diseases, compared with a match of 0.9 phenotypic features used in manual interpretation. We automated provisional diagnosis by combining the ranking of the similarity of a patient’s CNLP phenome with respect to the expected phenotypic features of all genetic diseases, together with the ranking of the pathogenicity of all of the patient’s genomic variants. Automated, retrospective diagnoses concurred well with expert manual interpretation (97% recall and 99% precision in 95 children with 97 genetic diseases). Prospectively, our platform correctly diagnosed three of seven seriously ill ICU infants (100% precision and recall) with a mean time saving of 22:19 hours. In each case, the diagnosis affected treatment. Genome sequencing with automated phenotyping and interpretation in a median of 20:10 hours may increase adoption in ICUs and, thereby, timely implementation of precise treatments.

Published

2018

8. Rapid whole-genome sequencing identifies a novel homozygous NPC1 variant associated with Niemann–Pick type C1 disease in a 7-week-old male with cholestasis

Author

Jaime Barea, Sergey Batalov, Amber Hildreth, Shimul Chowdhury, Stephen F. Kingsmore, Shareef Nahas, David Dimmock, Paulina Ordonez, and Kristen Wigby

Subjects

0301 basic medicine, Whole genome sequencing, congenital, hereditary, and neonatal diseases and abnormalities, business.industry, medicine.medical_treatment, Hepatosplenomegaly, nutritional and metabolic diseases, General Medicine, Disease, Neurological disorder, medicine.disease, Bioinformatics, 3. Good health, Targeted therapy, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Cholestasis, Immunology, Medicine, Neonatal cholestasis, NPC1, medicine.symptom, business, 030217 neurology & neurosurgery

Abstract

Niemann–Pick type C disease (NPC; OMIM #257220) is an inborn error of intracellular cholesterol trafficking. It is an autosomal recessive disorder caused predominantly by mutations in NPC1. Although characterized as a progressive neurological disorder, it can also cause cholestasis and liver dysfunction because of intrahepatocyte lipid accumulation. We report a 7-wk-old infant who was admitted with neonatal cholestasis, and who was diagnosed with a novel homozygous stop-gain variant in NPC1 by rapid whole-genome sequencing (WGS). WGS results were obtained 16 d before return of the standard clinical genetic test results and prompted initiation of targeted therapy.

Published

2017