Genetic Architectures of Childhood- and Adult-Onset Asthma Are Partly Distinct

Ferreira, Manuel A. R.; Mathur, Riddhima; Vonk, Judith M.; Szwajda, Agnieszka; Brumpton, Ben; Granell, Raquel; Brew, Bronwyn K.; Ullemar, Vilhelmina; Lu, Yi; Jiang, Yunxuan; Magnusson, Patrik K. E.; Karlsson, Robert; Hinds, David A.; Paternoster, Lavinia; Koppelman, Gerard H.; Almqvist, Catarina

doi:10.1016/j.ajhg.2019.02.022

Cited by 202 publications

(257 citation statements)

References 90 publications

(83 reference statements)

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“…Dupuytren's disease, which has a prevalence of more than 30% in some Northern European ethnicities, although it is lower in most of the world by 1-3 levels of magnitude, is an interesting example that was examined in this research. The alleles were randomly distributed throughout the model genome; these results are consistent with GWAS findings for asthma [53,98], schizophrenia [99], and other diseases [4].…”

Section: Allele Genetic Architecturesupporting

confidence: 82%

Future Preventive Gene Therapy of Polygenic Diseases from a Population Genetics Perspective

Oliynyk

2019

Preprint

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With the accumulation of scientific knowledge of the genetic causes of common diseases and continuous advancement of gene-editing technologies, gene therapies to prevent polygenic diseases may soon become possible. This study endeavored to assess population genetics consequences of such therapies. Computer simulations were used to evaluate the heterogeneity in causal alleles for polygenic diseases that could exist among geographically distinct populations. The results show that although heterogeneity would not be easily detectable by epidemiological studies following population admixture, even significant heterogeneity would not impede the outcomes of preventive gene therapies. Preventive gene therapies designed to correct causal alleles to a naturally-occurring neutral state of nucleotides would lower the prevalence of polygenic early-to middle-age-onset diseases in proportion to the decreased population relative risk attributable to the edited alleles. The outcome would manifest differently for late-onset diseases, for which the therapies would result in a delayed disease onset and decreased lifetime risk, however the lifetime risk would increase again with prolonging population life expectancy, which is a likely consequence of such therapies. If gene therapies that prevent heritable diseases were to be applied on a large scale, the decreasing frequency of risk alleles in populations would reduce the disease risk or delay the age of onset, even with a fraction of the population receiving such therapies. With ongoing population admixture, all groups would benefit over generations.

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Section: Allele Genetic Architecturesupporting

confidence: 82%

Future Preventive Gene Therapy of Polygenic Diseases from a Population Genetics Perspective

Oliynyk

2019

Preprint

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“…The association between asthma and the 17q12-21 locus was first established in childhood asthma 6 and was then confirmed to be mainly driven by individuals with the early-onset form of the disease. 13,14 Using a familial cohort with a mean age of onset of seven and 22 years old for probands and other family members respectively can be considered a caveat for the study of this locus, principally since gene expression counts and DNA methylation levels are changing over time. However, the genetic association was replicated in a previous study performed with the SLSJ asthma cohort 11 and analyses using the imputed data in this study show similar results when taking account of all samples or only those with age of onset under 17 years old.…”

Section: Discussionmentioning

confidence: 99%

“…Since the association between genetic variants and the disease occurring at the 17q12-21 locus is mainly driven by individuals with early-onset asthma, 13,14 correlation analyses were performed with DNA methylation levels from different mother-child duos for the two CpGs included in the significant mQTLs at GSDMA TSS. Analyses were between unaffected mother and affected child duos, all asthma status mother and affected child duos and affected mother and affected child duos to demonstrate the possible heritability of these DNA methylation levels.…”

Section: Locus In Naïve Cd4 + T Cellsmentioning

confidence: 99%

“…[1][2][3][4][5][6][7][8][9][10][11][12] Even though this locus was associated with this disease without considering any specific age of onset as it was done using the Saguenay-Lac-Saint-Jean (SLSJ) asthma familial cohort before, 11 it is principally with the condition of childhood. 13,14 Several studies explored the complex interactions between SNPs, gene expressions and epigenetic modifications at this locus, primarily focusing on the levels of expressed ORMDL3 and GSDMB. 12,[15][16][17][18][19][20][21][22][23][24][25] Given that DNA methylation and gene expression signals are cell-type specific, 26,27 isolated materials such as lymphocytes from blood [17][18][19][20][21] and, to a lesser extent, bronchial epithelial cells from biopsies of bronchi or bronchoalveolar lavages 15,16 have been used in a number of studies to investigate such interactions.…”

Section: Introductionmentioning

confidence: 99%

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GSDMAdrives the most replicated association with asthma in naïve CD4⁺T cells

Madore

Pain

Boucher-Lafleur

et al. 2019

Preprint

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Background The 17q12-21 locus is the most replicated association with asthma. However, no study had described the genetic mechanisms underlying this association considering all genes of the locus in immune cell samples isolated from asthmatic and non-asthmatic individuals. Objective This study takes benefit of samples from naïve CD4 + T cells and eosinophils isolated from the same 200 individuals to describe specific interactions between genetic variants, gene expression and DNA methylation levels for the 17q12-21 asthma locus. Methods and Results After isolation of naïve CD4 + T cells and eosinophils from blood samples, next generation sequencing was used to measure DNA methylation levels and gene expression counts. Genetic interactions were then evaluated considering genetic variants from imputed genotype data. In naïve CD4 + T cells but not eosinophils, 20 SNPs in the fourth and fifth haplotype blocks modulated both GSDMA expression and methylation levels,showing an opposite pattern of allele frequencies and expression counts in asthmatics compared to controls. Moreover, negative correlations have been measured between methylation levels of CpG sites located within the 1.5 kb region from the transcription start site of GSDMA and its expression counts. Conclusion Availability of sequencing data from two key cell types isolated from asthmatic and non-asthmatic individuals allowed identifying a new gene in naïve CD4 + T cells that drives the association with the 17q12-21 locus, leading to a better understanding of the genetic mechanisms taking place in it.

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“…Consistent with this notion, estimates for the heritability of asthma have ranged between 35% and 95% 3 , although those based on twin studies have been lower 4 . Genome-wide association studies (GWAS) have confirmed the contribution of genetic factors to risk of asthma, with over 140 susceptibility loci having been identified thus far [5][6][7][8][9][10][11][12][13] . However, the risk alleles, most of which are common in the population, still only explain a small fraction of the overall heritability for asthma [5][6][7] .…”

mentioning

confidence: 99%

Genome-wide analysis highlights contribution of immune system pathways to the genetic architecture of asthma

et al. 2020

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Asthma is a chronic and genetically complex respiratory disease that affects over 300 million people worldwide. Here, we report a genome-wide analysis for asthma using data from the UK Biobank and the Trans-National Asthma Genetic Consortium. We identify 66 previously unknown asthma loci and demonstrate that the susceptibility alleles in these regions are, either individually or as a function of cumulative genetic burden, associated with risk to a greater extent in men than women. Bioinformatics analyses prioritize candidate causal genes at 52 loci, including CD52, and demonstrate that asthma-associated variants are enriched in regions of open chromatin in immune cells. Lastly, we show that a murine anti-CD52 antibody mimics the immune cell-depleting effects of a clinically used human anti-CD52 antibody and reduces allergen-induced airway hyperreactivity in mice. These results further elucidate the genetic architecture of asthma and provide important insight into the immunological and sex-specific relevance of asthma-associated risk variants.

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Genetic Architectures of Childhood- and Adult-Onset Asthma Are Partly Distinct

Cited by 202 publications

References 90 publications

Future Preventive Gene Therapy of Polygenic Diseases from a Population Genetics Perspective

Future Preventive Gene Therapy of Polygenic Diseases from a Population Genetics Perspective

GSDMAdrives the most replicated association with asthma in naïve CD4⁺T cells

Genome-wide analysis highlights contribution of immune system pathways to the genetic architecture of asthma

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Genetic Architectures of Childhood- and Adult-Onset Asthma Are Partly Distinct

Cited by 202 publications

References 90 publications

Future Preventive Gene Therapy of Polygenic Diseases from a Population Genetics Perspective

Future Preventive Gene Therapy of Polygenic Diseases from a Population Genetics Perspective

GSDMAdrives the most replicated association with asthma in naïve CD4+T cells

Genome-wide analysis highlights contribution of immune system pathways to the genetic architecture of asthma

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GSDMAdrives the most replicated association with asthma in naïve CD4⁺T cells