Your search keyword '"Kanchan, Kanika"' showing total 13 results

1. Incorporating genetics in identifying peanut allergy risk and tailoring allergen immunotherapy: A perspective on the genetic findings from the LEAP trial.

Author

Huffaker, Michelle F., Kanchan, Kanika, Bahnson, Henry T., Baloh, Carolyn, Lack, Gideon, Nepom, Gerald T., and Mathias, Rasika A.

Abstract

Examining the genetics of peanut allergy (PA) in the context of clinical trial interventions and outcomes provides an opportunity to not only understand gene-environment interactions for PA risk but to also understand the benefit of allergen immunotherapy. A consistent theme in the genetics of food allergy is that in keeping with the dual allergen exposure hypothesis, barrier- and immune-related genes are most commonly implicated in food allergy and tolerance. With a focus on PA, we review how genetic risk factors across 3 genes (FLG , MALT1 , and HLA-DQA1) have helped delineate distinct allergic characteristics and outcomes in the context of environmental interventions in the Learning Early about Peanut Allergy (LEAP) study and other clinical trials. We specifically consider and present a framework for genetic risk prediction for the development of PA and discuss how genetics, age, and oral consumption intertwine to predict PA outcome. Although there is some promise in this proposed framework, a better understanding of the mechanistic pathways by which PA develops and persists is needed to develop targeted therapeutics for established disease. Only by understanding the mechanisms by which PA develops, persists, and resolves can we identify adjuvants to oral immunotherapy to make older children and adults immunologically similar to their younger, more malleable counterparts and thus more likely to achieve long-term tolerance. [ABSTRACT FROM AUTHOR]

Published

2023

2. Omics-oriented research illustrated with the LEAP study and the OASIS bioinformatics tool.

Author

Baloh, Carolyn H., Kanchan, Kanika, Shankar, Gautam, Nepom, Gerald T., Mathias, Rasika A., and Perry, James A.

Published

2023

3. Genome-wide association study of asthma, total IgE, and lung function in a cohort of Peruvian children.

Author

Akenroye, Ayobami T., Brunetti, Tonya, Romero, Karina, Daya, Michelle, Kanchan, Kanika, Shankar, Gautam, Chavan, Sameer, Preethi Boorgula, Meher, Ampleford, Elizabeth A., Fonseca, Héllen Freitas, Hawkins, Gregory A., Pitangueira Teixeira, Helena Mariana, Campbell, Monica, Rafaels, Nicholas, Winters, Alexandra, Bleecker, Eugene R., Cruz, Alvaro A., Barreto, Mauricio L., Meyers, Deborah A., and Ortega, Victor E.

Abstract

Genetic ancestry plays a role in asthma health disparities. Our aim was to evaluate the impact of ancestry on and identify genetic variants associated with asthma, total serum IgE level, and lung function. A total of 436 Peruvian children (aged 9-19 years) with asthma and 291 without asthma were genotyped by using the Illumina Multi-Ethnic Global Array. Genome-wide proportions of indigenous ancestry populations from continental America (NAT) and European ancestry from the Iberian populations in Spain (IBS) were estimated by using ADMIXTURE. We assessed the relationship between ancestry and the phenotypes and performed a genome-wide association study. The mean ancestry proportions were 84.7% NAT (case patients, 84.2%; controls, 85.4%) and 15.3% IBS (15.8%; 14.6%). With adjustment for asthma, NAT was associated with higher total serum IgE levels (P <.001) and IBS was associated with lower total serum IgE levels (P <.001). NAT was associated with higher FEV 1 percent predicted values (P <.001), whereas IBS was associated with lower FEV 1 values in the controls but not in the case patients. The HLA-DR/DQ region on chromosome 6 (Chr6) was strongly associated with total serum IgE (rs3135348; P = 3.438 × 10–10) and was independent of an association with the haplotype HLA-DQA1 ∼ HLA-DQB1 :04.01∼04.02 (P = 1.55 × 10–05). For lung function, we identified a locus (rs4410198; P = 5.536 × 10–11) mapping to Chr19, near a cluster of zinc finger interacting genes that colocalizes to the long noncoding RNA CTD-2537I9.5. This novel locus was replicated in an independent sample of pediatric case patients with asthma with similar admixture from Brazil (P =.005). This study confirms the role of HLA in atopy, and identifies a novel locus mapping to a long noncoding RNA for lung function that may be specific to children with NAT. [ABSTRACT FROM AUTHOR]

Published

2021

4. Gene and protein expression in human megakaryocytes derived from induced pluripotent stem cells

Author

Kammers, Kai, Taub, Margaret A., Mathias, Rasika A., Yanek, Lisa R., Kanchan, Kanika, Venkatraman, Vidya, Sundararaman, Niveda, Martin, Joshua, Liu, Senquan, Hoyle, Dixie, Raedschelders, Koen, Holewinski, Ronald, Parker, Sarah, Dardov, Victoria, Faraday, Nauder, Becker, Diane M., Cheng, Linzhao, Wang, Zack Z., Leek, Jeffrey T., Van Eyk, Jennifer E., and Becker, Lewis C.

Abstract

There is interest in deriving megakaryocytes (MKs) from pluripotent stem cells (iPSC) for biological studies. We previously found that genomic structural integrity and genotype concordance is maintained in iPSC‐derived MKs.

Published

2021

5. Gene and protein expression in human megakaryocytes derived from induced pluripotent stem cells

Author

Kammers, Kai, Taub, Margaret A., Mathias, Rasika A., Yanek, Lisa R., Kanchan, Kanika, Venkatraman, Vidya, Sundararaman, Niveda, Martin, Joshua, Liu, Senquan, Hoyle, Dixie, Raedschelders, Koen, Holewinski, Ronald, Parker, Sarah, Dardov, Victoria, Faraday, Nauder, Becker, Diane M., Cheng, Linzhao, Wang, Zack Z., Leek, Jeffrey T., Van Eyk, Jennifer E., and Becker, Lewis C.

Abstract

There is interest in deriving megakaryocytes (MKs) from pluripotent stem cells (iPSC) for biological studies. We previously found that genomic structural integrity and genotype concordance is maintained in iPSC‐derived MKs. To establish a comprehensive dataset of genes and proteins expressed in iPSC‐derived MKs. iPSCs were reprogrammed from peripheral blood mononuclear cells (MNCs) and MKs were derived from the iPSCs in 194 healthy European American and African American subjects. mRNA was isolated and gene expression measured by RNA sequencing. Protein expression was measured in 62 of the subjects using mass spectrometry. MKs expressed genes and proteins known to be important in MK and platelet function and demonstrated good agreement with previous studies in human MKs derived from CD34+ progenitor cells. The percent of cells expressing the MK markers CD41 and CD42a was consistent in biological replicates, but variable across subjects, suggesting that unidentified subject‐specific factors determine differentiation of MKs from iPSCs. Gene and protein sets important in platelet function were associated with increasing expression of CD41/42a, while those related to more basic cellular functions were associated with lower CD41/42a expression. There was differential gene expression by the sex and race (but not age) of the subject. Numerous genes and proteins were highly expressed in MKs but not known to play a role in MK or platelet function; these represent excellent candidates for future study of hematopoiesis, platelet formation, and/or platelet function.

Published

2021

6. Transcriptional profile of platelets and iPSC-derived megakaryocytes from whole-genome and RNA sequencing

Author

Kammers, Kai, Taub, Margaret A., Rodriguez, Benjamin, Yanek, Lisa R., Ruczinski, Ingo, Martin, Joshua, Kanchan, Kanika, Battle, Alexis, Cheng, Linzhao, Wang, Zack Z., Johnson, Andrew D., Leek, Jeffrey T., Faraday, Nauder, Becker, Lewis C., and Mathias, Rasika A.

Abstract

Genome-wide association studies have identified common variants associated with platelet-related phenotypes, but because these variants are largely intronic or intergenic, their link to platelet biology is unclear. In 290 normal subjects from the GeneSTAR Research Study (110 African Americans [AAs] and 180 European Americans [EAs]), we generated whole-genome sequence data from whole blood and RNA sequence data from extracted nonribosomal RNA from 185 induced pluripotent stem cell-derived megakaryocyte (MK) cell lines (platelet precursor cells) and 290 blood platelet samples from these subjects. Using eigenMT software to select the peak single-nucleotide polymorphism (SNP) for each expressed gene, and meta-analyzing the results of AAs and EAs, we identify (q-value < 0.05) 946 cis-expression quantitative trait loci (eQTLs) in derived MKs and 1830 cis-eQTLs in blood platelets. Among the 57 eQTLs shared between the 2 tissues, the estimated directions of effect are very consistent (98.2% concordance). A high proportion of detected cis-eQTLs (74.9% in MKs and 84.3% in platelets) are unique to MKs and platelets compared with peak-associated SNP-expressed gene pairs of 48 other tissue types that are reported in version V7 of the Genotype-Tissue Expression Project. The locations of our identified eQTLs are significantly enriched for overlap with several annotation tracks highlighting genomic regions with specific functionality in MKs, including MK-specific DNAse hotspots, H3K27-acetylation marks, H3K4-methylation marks, enhancers, and superenhancers. These results offer insights into the regulatory signature of MKs and platelets, with significant overlap in genes expressed, eQTLs detected, and enrichment within known superenhancers relevant to platelet biology.

Published

2021

7. Transcriptional profile of platelets and iPSC-derived megakaryocytes from whole-genome and RNA sequencing

Author

Kammers, Kai, Taub, Margaret A., Rodriguez, Benjamin, Yanek, Lisa R., Ruczinski, Ingo, Martin, Joshua, Kanchan, Kanika, Battle, Alexis, Cheng, Linzhao, Wang, Zack Z., Johnson, Andrew D., Leek, Jeffrey T., Faraday, Nauder, Becker, Lewis C., and Mathias, Rasika A.

Abstract

Genome-wide association studies have identified common variants associated with platelet-related phenotypes, but because these variants are largely intronic or intergenic, their link to platelet biology is unclear. In 290 normal subjects from the GeneSTAR Research Study (110 African Americans [AAs] and 180 European Americans [EAs]), we generated whole-genome sequence data from whole blood and RNA sequence data from extracted nonribosomal RNA from 185 induced pluripotent stem cell-derived megakaryocyte (MK) cell lines (platelet precursor cells) and 290 blood platelet samples from these subjects. Using eigenMT software to select the peak single-nucleotide polymorphism (SNP) for each expressed gene, and meta-analyzing the results of AAs and EAs, we identify (q-value < 0.05) 946 cis-expression quantitative trait loci (eQTLs) in derived MKs and 1830 cis-eQTLs in blood platelets. Among the 57 eQTLs shared between the 2 tissues, the estimated directions of effect are very consistent (98.2% concordance). A high proportion of detected cis-eQTLs (74.9% in MKs and 84.3% in platelets) are unique to MKs and platelets compared with peak-associated SNP-expressed gene pairs of 48 other tissue types that are reported in version V7 of the Genotype-Tissue Expression Project. The locations of our identified eQTLs are significantly enriched for overlap with several annotation tracks highlighting genomic regions with specific functionality in MKs, including MK-specific DNAse hotspots, H3K27-acetylation marks, H3K4-methylation marks, enhancers, and superenhancers. These results offer insights into the regulatory signature of MKs and platelets, with significant overlap in genes expressed, eQTLs detected, and enrichment within known superenhancers relevant to platelet biology.

Published

2021

8. Advancing Food Allergy Through Omics Sciences

Author

Irizar, Haritz, Kanchan, Kanika, Mathias, Rasika A., and Bunyavanich, Supinda

Abstract

Since the publication of the first draft of the human genome, there has been an explosion of new technologies with increasing power to interrogate the totality of biological molecules (eg, DNA, RNA, proteins, metabolites) and their modifications (eg, DNA methylation, histone modifications). These technologies, collectively called omics, have been widely applied in the last 2 decades to study biological systems to gain deeper insight into mechanisms driving the physiology and pathophysiology of human health and disease. Because of its complex, multifactorial nature, food allergy is especially well suited to be investigated using omics approaches. In this rostrum, we review how omic technologies have been applied to explore diverse aspects of food allergy, including adaptive and innate immune processes in food-allergic responses, the role of the microbiome in food allergy risk, metabolic changes in the gut and blood associated with food allergy, and the identification of biomarkers and potential therapeutic targets for the condition. We discuss the strengths and limitations of the studies performed thus far and the need to adopt systems biology approaches that integrate data from multiple omics to fully leverage the potential of these technologies to advance food allergy research and care.

Published

2021

9. Epidermal differentiation complex genetic variation in atopic dermatitis and peanut allergy.

Author

Huffaker, Michelle F., Kanchan, Kanika, Bahnson, Henry T., Ruczinski, Ingo, Shankar, Gautam, Leung, Donald Y.M., Baloh, Carolyn, Du Toit, George, Lack, Gideon, Nepom, Gerald T., and Mathias, Rasika A.

Abstract

Deleterious variation in the epidermal differentiation complex (EDC) on chromosome 1 is a well-known genetic determinant of atopic dermatitis (AD) and has been associated with risk of peanut allergy (PA) in population-based studies. Our aim was to determine the effect of genetic variation in the EDC on AD trajectory and risk of PA in early life. Genome sequencing was used to measure genetic variation in the EDC in the Learning Early about Peanut Allergy (LEAP) study participants. Association tests were done to identify gene- and variant-level predicted deleterious variation associated with AD severity by using the Scoring Atopic Dermatitis (SCORAD) tool (n = 559) at baseline and each follow-up visit, as well as PA and food allergy in peanut avoiders (n = 275). Predicted deleterious variants included missense variants that were frameshift insertions, frameshift deletions, stop-gain mutations, or stop-loss mutations. Associations between variant load, SCORAD score, and PA were tested by using linear and generalized linear regression models. The genes FLG , FLG2 , HRNR , and TCHH1 harbored the most predicted deleterious variation (30, 6, 3, and 1 variant, respectively). FLG variants were associated with SCORAD score at all time points; 4 variants (R1798X, R501X, S126X, and S761fs) drove the association with SCORAD score at each time point, and higher variant load was associated with greater AD severity over time. There was an association between these variants and PA, which remained significant independent of baseline AD severity (odds ratio = 2.63 [95% CI = 1.11-6.01] [ P =.02]). Variation in FLG predicted to be deleterious is associated with AD severity at baseline and longitudinally and has an association with PA independent of baseline severity. [ABSTRACT FROM AUTHOR]

Published

2023

10. Translating lessons learned on the role of HLA in immunological responses in LEAP to peanut OIT Trials: IMPACT and POISED.

Author

Kanchan, Kanika, Shankar, Gautam, Huffaker, Michelle, Bahnson, Henry, Chinthrajah, R Sharon, Sanda, Srinath, Manohar, Monali, Du Toit, George, Ruczinski, Ingo, Lack, Gideon, Nadeau, Kari, Jones, Stacie, Nepom, Gerald, and Mathias, Rasika

Published

2022

11. Multiple FLG variants drive eczema severity in the LEAP study participants.

Author

Huffaker, Michelle, Kanchan, Kanika, Bahnson, Henry, Ruczinski, Ingo, Shankar, Gautam, Leung, Donald, Baloh, Carolyn, Du Toit, George, Lack, Gideon, Nepom, Gerald, and Mathias, Rasika

Published

2022

12. Genomic integrity of human induced pluripotent stem cells across nine studies in the NHLBI NextGen program.

Author

Kanchan, Kanika, Iyer, Kruthika, Yanek, Lisa R, Carcamo-Orive, Ivan, Taub, Margaret A, Malley, Claire, Baldwin, Kristin, Becker, Lewis C, Broeckel, Ulrich, Cheng, Linzhao, Cowan, Chad, D'Antonio, Matteo, Frazer, Kelly A, Quertermous, Thomas, Mostoslavsky, Gustavo, Murphy, George, Rabinovitch, Marlene, Rader, Daniel J, Steinberg, Martin H, and Topol, Eric

Abstract

• NextGen: A collection of publicly available hiPSCs from more than 1,500 individuals. • Determined genomic structural integrity of 506 lines, 71% show no detectable CNVs. • Enrichment of cancer related biological processes in regions of acquired CNVs. • Recurrent aberrant regions on five chromosomes encompass cancer associated loci. • Amplification on chr20 includes transcriptomic signatures for known cancer gene HCK. Human induced pluripotent stem cell (hiPSC) lines have previously been generated through the NHLBI sponsored NextGen program at nine individual study sites. Here, we examined the structural integrity of 506 hiPSC lines as determined by copy number variations (CNVs). We observed that 149 hiPSC lines acquired 258 CNVs relative to donor DNA. We identified six recurrent regions of CNVs on chromosomes 1, 2, 3, 16 and 20 that overlapped with cancer associated genes. Furthermore, the genes mapping to regions of acquired CNVs show an enrichment in cancer related biological processes (IL6 production) and signaling cascades (JNK cascade & NFκB cascade). The genomic region of instability on chr20 (chr20q11.2) includes transcriptomic signatures for cancer associated genes such as ID1, BCL2L1, TPX2, PDRG1 and HCK. Of these HCK shows statistically significant differential expression between carrier and non-carrier hiPSC lines. Overall, while a low level of genomic instability was observed in the NextGen generated hiPSC lines, the observation of structural instability in regions with known cancer associated genes substantiates the importance of systematic evaluation of genetic variations in hiPSCs before using them as disease/research models. [ABSTRACT FROM AUTHOR]

Published

2020

13. Genetic Determinants of Peanut-Specific IgG4 in The Learning Early About Peanut Allergy (LEAP) Study.

Author

Kanchan, Kanika, Ruczinski, Ingo, Bahnson, Henry, Boorgula, Meher Preethi, Chavan, Sameer, Larson, David, Cerosaletti, Karen, DuToit, George, Lack, Gideon, Barnes, Kathleen, Nepom, Gerald, and Mathias, Rasika

Published

2020