Your search keyword '"Kajari Mondal"' showing total 4 results

1. Genetic and Transcriptomic Variation Linked to Neutrophil Granulocyte–Macrophage Colony-Stimulating Factor Signaling in Pediatric Crohn’s Disease

Author

Scott B. Snapper, Anne Dodd, Anne M. Griffiths, Michael E. Zwick, Marla Dubinsky, Wallace Crandall, Ingrid Jurickova, Jeffrey S. Hyams, David T. Okou, Yael Haberman, Aaron Linn, Stephen L. Guthery, Melvin B. Heyman, Subra Kugathasan, Lee A. Denson, Christine Stevens, David J. Cutler, Robert N. Baldassano, Rebekah Karns, Ramnik J. Xavier, Bruce J. Aronow, Anthony R. Otley, Ramona Bezold, Neal S. Leleiko, Barbara S. Kirschner, Mark J. Daly, Kajari Mondal, Kathleen Lake, Kimberly Jackson, Kelly A Shaw, Thomas D. Walters, C. Alexander Valencia, Adam Price, and Joshua D. Noe

Subjects

Adult, Male, 0301 basic medicine, Macrophage colony-stimulating factor, Adolescent, Neutrophils, Neutrophil granulocyte, medicine.medical_treatment, Mutation, Missense, STAT5B, Inflammatory bowel disease, Cytokine Receptor Common beta Subunit, Young Adult, 03 medical and health sciences, 0302 clinical medicine, Crohn Disease, medicine, Humans, Immunology and Allergy, Missense mutation, Child, STAT5, biology, business.industry, Gastroenterology, Granulocyte-Macrophage Colony-Stimulating Factor, Infant, Prognosis, medicine.disease, 030104 developmental biology, medicine.anatomical_structure, Granulocyte macrophage colony-stimulating factor, Cytokine, Receptors, Granulocyte-Macrophage Colony-Stimulating Factor, Case-Control Studies, Child, Preschool, Immunology, biology.protein, Female, 030211 gastroenterology & hepatology, Original Clinical Articles, Transcriptome, business, Follow-Up Studies, medicine.drug

Abstract

Author(s): Denson, Lee A; Jurickova, Ingrid; Karns, Rebekah; Shaw, Kelly A; Cutler, David J; Okou, David; Valencia, C Alexander; Dodd, Anne; Mondal, Kajari; Aronow, Bruce J; Haberman, Yael; Linn, Aaron; Price, Adam; Bezold, Ramona; Lake, Kathleen; Jackson, Kimberly; Walters, Thomas D; Griffiths, Anne; Baldassano, Robert N; Noe, Joshua D; Hyams, Jeffrey S; Crandall, Wallace V; Kirschner, Barbara S; Heyman, Melvin B; Snapper, Scott; Guthery, Stephen L; Dubinsky, Marla C; Leleiko, Neal S; Otley, Anthony R; Xavier, Ramnik J; Stevens, Christine; Daly, Mark J; Zwick, Michael E; Kugathasan, Subra | Abstract: BACKGROUND:Granulocyte-macrophage colony-stimulating factor auto-antibodies (GMAbs) suppress neutrophil-extrinsic GM-CSF signaling and increase risk for stricturing behavior in Crohn's disease (CD). We aimed to define clinical, genomic, and functional associations with neutrophil-intrinsic GM-CSF signaling. METHODS:Missense mutations in CSF2RA, CSF2RB, JAK2, STAT5A, and STAT5B were identified using whole-exome sequencing in 543 pediatric inflammatory bowel disease (IBD) patients. Neutrophil-intrinsic GM-CSF signaling was defined using the GM-CSF-induced STAT5 stimulation index (GMSI) in 180 pediatric IBD patients and 26 non-IBD controls. Reduced GM-CSF signaling (GMSI-Lo) was defined as the 20th percentile within the control group. Variation in neutrophil phospho-protein abundance, bacterial killing, and the global pattern of gene expression with the GMSI was determined. RESULTS:We validated 18 potentially damaging missense mutations in CSF2RA and CSF2RB. CSF2RA A17G carriage increased from 10% in those with intact neutrophil GMSI to 32% in those with low GMSI (P = 0.02). The frequency of reduced Staphylococcus aureus killing increased from 17% in those with intact neutrophil GMSI to 35% in GMSI-Lo neutrophils (P = 0.043). Crohn's disease neutrophils with low GMSI exhibited specific alterations in phospho-protein networks and genes regulating cytokine production, wound healing, and cell survival and proliferation. Stricturing behavior increased from 7% in patients with both low GMAb and intact GMSI to 64% in patients with both elevated GMAb and low GMSI (P l 0.0001). CONCLUSIONS:Low/normal neutrophil-intrinsic GM-CSF signaling is associated with CSF2RA missense mutations, alterations in gene expression networks, and higher rates of disease complications in pediatric CD.

Published

2018

2. Evolution of Pediatric Inflammatory Bowel Disease Unclassified (IBD-U): Incorporated With Serological and Gene Expression Profiles

Author

Joel R. Rosh, Anne M. Griffiths, James Markowitz, Kajari Mondal, Suresh Venkateswaran, Madeline Bertha, Marla Dubinsky, Cary G. Sauer, Shervin Rabizadeh, Joshua D. Noe, Raguraj Chandradevan, Hari K. Somineni, Nusrat Harun, Subra Kugathasan, Scott B. Snapper, Cortney R. Ballengee, Wallace Crandall, Neal S. Leleiko, Lee A. Denson, Thomas D. Walters, Jeffrey S. Hyams, Tatyana Hofmekler, and Mi-Ok Kim

Subjects

Male, 0301 basic medicine, medicine.medical_specialty, Adolescent, Disease, digestive system, Inflammatory bowel disease, Serology, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Humans, Immunology and Allergy, Prospective Studies, Child, Prospective cohort study, Irritable bowel syndrome, business.industry, Infant, Newborn, Gastroenterology, Infant, Inflammatory Bowel Diseases, Prognosis, medicine.disease, Ulcerative colitis, digestive system diseases, Natural history, 030104 developmental biology, Child, Preschool, Cohort, Female, 030211 gastroenterology & hepatology, Transcriptome, business, Biomarkers, Immunosuppressive Agents, Follow-Up Studies

Abstract

Background Inflammatory bowel disease (IBD) mainly consists of Crohn's disease (CD) and ulcerative colitis (UC). About 10%-15% of patients with IBD cannot be firmly diagnosed with CD or UC; hence, they are initially diagnosed as inflammatory bowel disease unclassified (IBD-U). Having a firm diagnosis is clearly preferred to guide treatment choices, and better understanding of the nature of IBD-U is required. Methods We performed an analysis of a subset of pediatric subjects from an inception IBD cohort of patients initially enrolled in a prospective multicenter study (the RISK study). Initial diagnosis and 2-year follow-up data from the subjects diagnosed with IBD-U were analyzed. An expert panel verified final diagnosis using predefined criteria as a guide. Serological and disease-relevant ileal and rectal tissue gene expression profiles were investigated. The use and the time to initiate anti-TNFα treatment was analyzed among the outcome groups. Results A total of 1411 subjects were enrolled with initial diagnosis of IBD, and among them, 136 subjects were initially diagnosed as IBD-U at enrollment. And 26% were reclassified as UC and 14% as CD within 2 years of diagnosis, while 60% remained as IBD-U. Of those who were reclassified, there was a 2:1 ratio, UC (n = 35) to CD (n = 19). The molecular and serological features of IBD-U at the end of follow-up were very similar to UC and very different from CD. There was less likelihood of receiving anti-TNFα agents if the diagnosis was IBD-U compared with CD (P < 0.0001). Conclusions In our cohort, 60% of the IBD-U subjects remained as unclassified at 2 years; of those subsequently classified, a higher percentage followed a course more similar to UC. Most of the IBD-U subjects at diagnosis had serological and molecular signatures that are very similar to UC. Although the atypical presentations made the clinician to make an interim diagnosis of IBD-U, results of the molecular and serological factors performed at the time of diagnosis suggests that they were very similar to UC. However, long-term studies are needed to better understand the natural history and molecular characterization of pediatric onset IBD-U. 10.1093/ibd/izy136_video1Video 1.Video 1. Watch now at https://academic.oup.com/ibd/article-lookup/doi/10.1093/ibd/izy136izy136.video15791389938001.

Published

2018

3. 27 CLINICAL AND GENOMIC CORRELATES OF NEUTROPHIL GRANULOCYTE-MACROPHAGE COLONY STIMULATING FACTOR SIGNALING IN PEDIATRIC CROHN DISEASE

Author

Thomas D. Walters, Adam Price, Kajari Mondal, Christine Stevens, Michael E. Zwick, Anne M. Griffiths, Rebekah Karns, Kathleen Lake, Jeffrey S. Hyams, Anne Dodd, Ramona Bezold, Barbara S. Kirschner, Scott B. Snapper, Bruce J. Aronow, Stephen L. Guthery, Mark J. Daly, Kimberly Jackson, Aaron Linn, David J. Cutler, Yael Haberman, Robert N. Baldassano, Anthony R. Otley, David T. Okou, Kelly A Shaw, Subra Kugathasan, Marla Dubinsky, Ramnik J. Xavier, Neal S. Leleiko, Lee A. Denson, Wallace Crandall, Ingrid Jurickova, Joshua D. Noe, and Melvin B. Heyman

Subjects

Macrophage colony-stimulating factor, medicine.anatomical_structure, Hepatology, Crohn disease, business.industry, Neutrophil granulocyte, Immunology, medicine, Gastroenterology, Immunology and Allergy, business

Published

2018

4. Excess variants in AFF2 detected by massively parallel sequencing of males with autism spectrum disorder

Author

David J. Cutler, Katie R. Hagen, Dhanya Ramachandran, Promita Bose, Viren Patel, Michael E. Zwick, and Kajari Mondal

Subjects

Male, Proband, Molecular Sequence Data, Population, Mutation, Missense, Locus (genetics), Biology, behavioral disciplines and activities, mental disorders, Genetics, medicine, Humans, Missense mutation, Child, education, 3' Untranslated Regions, Molecular Biology, Genetics (clinical), X-linked recessive inheritance, X chromosome, Chromosomes, Human, X, education.field_of_study, Base Sequence, Association Studies Articles, Genetic Variation, High-Throughput Nucleotide Sequencing, Nuclear Proteins, General Medicine, medicine.disease, Fragile X syndrome, Child Development Disorders, Pervasive, Autism spectrum disorder, Child, Preschool

Abstract

Autism spectrum disorder (ASD) is a heterogeneous disorder with substantial heritability, most of which is unexplained. ASD has a population prevalence of one percent and affects four times as many males as females. Patients with fragile X E (FRAXE) intellectual disability, which is caused by a silencing of the X-linked gene AFF2 ,d isplay an umber of ASD-like phenotypes. Duplications and deletions at theAFF2 locus have also been reported in cases with moderate intellectual disability and ASD. We hypothesized that other rare X-linked sequence variants at the AFF2 locus might contribute to ASD. We sequenced the AFF2 genomic region in 202 male ASD probands and found that 2.5% of males sequenced had missense mutations at highly conserved evolutionary sites. When compared with the frequency of missense mutations in 5545 X chromosomes from unaffected controls, we saw a statistically significant enrichment in patients with ASD (OR: 4.9; P < 0.014). In addition, we identified rare AFF2 3 " UTR variants at conserved sites which alter gene expression in a luciferase assay. These data suggest that rare variation in AFF2 may be a previously unrecognized ASD susceptibility locus and may help explain some of the male excess of ASD.

Published

2012