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Asthma Genetics^*

^* From the Department of Human Genetics, University of Oxford, Oxford, UK.

Correspondence to: William Osmond Charles Cookson, MA, DPhil, MD, Wellcome Trust Centre for Human Genetics, Roosevelt Dr, Headington, Oxford OX3 7BN, UK; e-mail: wocc{at}well.ox.ac.uk

	Abstract

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 
Asthma is the most common chronic childhood disease in developed nations and is a complex disease that has high social and economic costs. Asthma and its associated intermediate phenotypes are under a substantial degree of genetic control. Identifying the genes underlying asthma offers a means of better understanding its pathogenesis, with the promise of improving preventive strategies, diagnostic tools, and therapies. A number of chromosomal regions containing genes influencing asthma and atopy have been identified consistently by different groups, and a role for several candidate genes has been established.

Asthma has become an epidemic, affecting 155 million individuals in the world. One child in seven in the United Kingdom wheezes,¹ and similar numbers suffer from the related disorder of eczema (atopic dermatitis).^{2 3} Asthma is due to a combination of strong genetic and environmental factors. It has risen in prevalence over the past 30 years in all Westernized societies,⁴ perhaps as a result of the loss of childhood infections.^{5 6 7}

Many candidate gene and positional cloning studies of asthma have now been carried out. Although the number of candidate gene studies in asthma is growing rapidly, many contain small numbers of subjects and give equivocal results that do not subsequently replicate. This review will, therefore, concentrate on regions identified consistently through genetic linkage, because these by and large represent the strongest genetic effects, and candidates studied within these regions will be discussed in detail.

	Genome Screens

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 
The first genome-wide screen for linkages to quantitative traits underlying asthma identified significant evidence for linkage on chromosomes 4q, 6 (near the major histocompatibility complex [MHC]), 7, 11q (containing FcRI-ß), 13q and 16. A replication sample of families in the same study confirmed linkage to chromosomes 4, 11, 13, and 16.⁸ A two-stage screen in Hutterite families from the United States found suggestive evidence for linkage and replication for loci on chromosome 5q, 12q, 19q, and 21q.⁹ A screen in German families identified suggestive evidence for linkage to asthma on chromosomes 2q (near the interleukin-1 cluster), 6p (near the MHC), 9, and 12q.¹⁰ A genome screen for responsiveness to the house dust mite (HDM) allergen found suggestive linkages to chromosomes 2q, 6p (near the MHC), and 13q, as well as chromosome 8p.¹¹ A genome screen in American families from three racial groups found a weak linkage to broad regions that might match other studies on chromosomes 2q, 5q, 6p, 12q, 13q, and 14q.¹² A two-stage genome screen in French families found replicated linkages on chromosomes 1p, 12q, and 17q.¹³

Thus, the loci most consistently and robustly identified by these screens are on chromosomes 5, 6, 12, and 13.

	Chromosome 5

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 
Chromosome 5q31 has been studied by many groups following an original observation of genetic linkage to total serum IgE concentrations in extended Amish pedigrees¹⁴ and the confirmation of linkage to the same region.¹⁵ The region also has been linked to eosinophil levels¹⁶ and to schistosomiasis resistance.¹⁷ The region contains several genes that modulate atopic responses, including interleukin (IL)-4, IL-13, IL-5, CD14, and granulocyte macrophage-colony-stimulating factor.

Humans (and different strains of mice) seem to exhibit a constitutional preference for either cellular or humoral immune responses,^{5 18} which are associated with distinct cytokine profiles in T-helper cells (Ths). The profiles are classified as Th-1 or Th-2 responses, respectively. Th-2 responses are characterized by high levels of secretion of IL-4, IL-13, and IL-5, and are associated with atopy.

A number of polymorphisms have been identified in IL-13 and are convincingly associated with a variation in IgE levels in large population samples.¹⁹ IL-13 enhances bronchial mucus secretion and up-regulates IgE production.²⁰ It is in close proximity to IL-4 and is highly homologous to that gene. Polymorphisms within IL-4 have been less securely related to IgE levels or atopic disease than IL-13.^{21 22} Functionally important polymorphisms within the IL-4 receptor gene (on chromosome 16) are associated with atopy and asthma,^{23 24} although positive findings are not universal.²⁵

CD14 is found on the surface of monocytes and macrophages, as well as in a soluble form. CD14 acts as a high-affinity ligand for bacterial lipopolysaccharide (LPS) [endotoxin], and initiates the nonspecific innate immune response to bacterial infection. A polymorphism upstream of the transcription start site for CD14 is associated with high levels of soluble CD14 and low levels of IgE.²⁶ The prevalence of asthma correlates inversely with a rural lifestyle and high ambient levels of LPS, so it has been suggested that the CD14 interaction with LPS may be protective against allergic disease.²⁶

The level of variation in IgE associated with any of the chromosome-5 polymorphisms is of the order of 1% or 2%, and the polymorphisms so far identified cannot be considered to have major influences on the allergic process. Genetic linkage maps of the region suggest the presence of a least two genes influencing atopy.²⁷ Localizations within the region have been imprecise, and the overall impression is that of a weak linkage to a number of adjoining loci.

However, the coincidence of nonhomologous cytokine genes within a limited interval suggests that the region is involved in the coordinate regulation of cytokine responses. Sequence comparison between human and mouse of 1 megabase of the proximal cluster, including interleukins 4, 13, and 5, found 90 noncoding highly conserved sequences.²⁸ Fifteen of these elements were found to be present in other mammals.²⁸ The characterization of the largest element in yeast artificial chromosome transgenic mice revealed it to be a coordinate regulator of IL-4, IL-13, and IL-5.²⁹ This work, therefore, has begun to unpick at a structural level the mechanisms for T-cell commitment to a particular cytokine profile. It also has identified a high level of conservation of controlling elements of gene expression between species. It will be of interest to see whether this level of conservation is observed in other genomic regions.

	Chromosome 6

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 
The MHC region on chromosome 6 has shown consistent linkage to asthma-associated phenotypes in several studies^{8 9 10 11 12} and may be considered to be a major locus influencing allergic diseases.

The MHC contains many molecules involved in innate and specific immunity. At the same time, the asthma phenotype is complex, containing inflammatory and allergic components. An investigation of the effects of the MHC on asthma and its related phenotypes, therefore, poses a methodological and statistical challenge.

The class II genes of the MHC have recognized influences on the ability to respond to particular allergens.^{30 31 32 33 34 35} Asthma and bronchial hyperresponsiveness are associated primarily with an allergy to the HDM and to a lesser degree with allergy to cat dander and molds,^{36 37} so that genetic control of specific IgE responses is of relevance to clinical disease. The T-cell receptor (TCR) genes, on chromosomes 7q and 14q, are also important potential genetic modifiers of the specific IgE response. Genetic linkage and allelic association have been reported between specific IgE responses and the TCR / locus on chromosome 14q.^{38 39}

The class I genes of the MHC may have important effects on atopic responses, but these have not yet been adequately investigated. Similarly, the class III complement genes contain polymorphisms that may be of relevance to inflammatory or immune diseases, but which have not yet been tested in asthmatic subjects.

Nonclassical MHC genes also may have an impact on asthma through nonallergic pathways, and a polymorphism in the control elements of inflammatory cytokines and their receptors is an important mechanism for flexibility in the immunoregulatory machinery.⁴⁰ Tumor necrosis factor (TNF) is a potent proinflammatory cytokine that is found in excess in asthmatic airways. A polymorphism in the TNF complex is associated with variation on the expression of TNF- and with the presence of asthma.^{41 42 43} These results emphasize the inflammatory nature of the asthmatic response, as distinct from its allergic basis.

	Chromosome 11Q

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 
The linkage of atopy to a VNTR (ie, variable number of tandem repeats) polymorphism on chromosome 11q13 was first reported in 1989⁴⁴ and was at first disputed.⁴⁵ The ß-chain of the high-affinity receptor for IgE (FcRI-ß) was subsequently localized to the region. The FcRI receptor acts as the allergic trigger on mast cells and other types of cells, and is central to the allergic response.⁴⁶ The ß-chain is not essential for FcRI function, but it both stabilizes the surface expression of the receptor and acts as an amplifying element within it.⁴⁷ Any variation in the level of the ß-chain expression may therefore modify receptor function.

A polymorphism in FcRI-ß has been related to atopy,⁴⁸ asthma,⁴⁹ bronchial hyperresponsiveness,^{50 51} and severe atopic dermatitis.⁵² A polymorphism within the gene also has been associated with levels of IgE in heavily parasitized Australian aborigines, implying a protective role for the gene in helminth infestation.⁵³

Although coding changes have been identified within FcRI-ß,^{54 55} they are conservative and do not seem to alter gene function.⁵⁶ The Ile181Leu polymorphisms identified by Shirakawa et al⁵⁴ have not been found in several other studies^{57 58 59} but have been found in association with asthma in Kuwaiti Arabs⁶⁰ and black South Africans.⁶¹ The difficulty in their identification nevertheless suggests that they are artifactual or in homologous sequences out of the FcRI-ß gene. The structural variation that causes the effect of this gene on patients with asthma, therefore, has not yet been identified.

The genetic linkage and association of atopy to the locus both have been typified by a strong maternal effect,^{52 62 63} with preferential linkage and the transmission of maternal alleles to affected children. Maternal effects are well-recognized in allergic disorders, and asthma, eczema, elevated serum IgE concentrations, and skin prick test positivity in children all have been accompanied by an increased prevalence of asthma or atopy in mothers.⁶⁴ The preferential transmission of or linkage to alleles from either the maternal or paternal sides also has been observed for other loci influencing allergic disease, including those identified on chromosomes 13 and 16.⁸

Parent-of-origin effects have been noted in other immunologic disorders, including type I diabetes,⁶⁵ rheumatoid arthritis,⁶⁶ inflammatory bowel disease,⁶⁷ and selective IgA deficiency.⁶⁸ Parent-of-origin linkages also have been observed in the same diseases, so that the preferential linkage of paternal alleles is seen from the insulin locus and type I diabetes,⁶⁹ and HLA alleles for selective IgA deficiency.⁶⁸ These findings suggest a common underlying mechanism for parent-of-origin effects in immune disorders. The monoallelic expression of cytokines and cell-signaling molecules is recognized^{70 71 72} and mediated by methylation,⁷³ providing a potential mechanism for these effects.

	Chromosome 12

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 
The initial demonstration of the genetic linkage of asthma to chromosome 12q⁷⁴ was followed by single-locus confirmatory studies^{75 76} and by several general genome screens.^{9 10 12 13} In addition, a genome screen in a mouse model of asthma found a linkage to bronchial hyperresponsiveness on mouse chromosome 10 in the region of syntenic homology to human chromosome 12q.⁷⁷ The facility with which many groups have identified a linkage to this region suggests that it is a true major atopy locus. Interferon- does not seem to be responsible for the linkage. High-density mapping of the region has been begun,⁷⁸ and it is likely that positional cloning of the gene will be possible.

	Chromosome 13Q14

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 
A linkage of the total serum IgE to the esterase D protein polymorphism on chromosome 13q14 was reported in 1985.⁷⁹ The linkage of chromosome 13q to atopy was confirmed by a genome-wide scan⁸ and by a single-locus study of Japanese families.⁸⁰ The same study identified potential linkage disequilibrium (LD) between disease and D13S153.⁸⁰ A two-stage screen in Hutterite families from the United States found a linkage of asthma to chromosome 13q21.3⁹ in the first-stage families but not in the second-stage families. A linkage of chromosome 13q14 to HDM allergy in children with asthma also has been observed,⁸¹ as has a linkage to children with atopic dermatitis.⁸²

These results suggest that chromosome 13q14 also contains a major atopy locus. The same chromosomal region has been shown to be linked to total serum IgA concentrations.⁸³ Low levels of serum IgA occur much more frequently in atopic children than in healthy children,⁸⁴ and salivary IgA deficiency is more common in infants with atopic parents.⁸⁵ Ig production is known to be under the control of many genes (reviewed by Corrigan⁸⁶ ), none of which have been mapped to chromosome 13q14. The gene of interest may encode a regulatory component of the humoral immune system but, alternatively, might influence both IgA levels and atopic status by influencing the mucosal handling of allergens.

	Sharing of Loci With Other Disorders

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 
Genetic studies of other disorders also may have an impact on asthma and atopy. Crohn’s disease and ulcerative colitis are inflammatory bowel diseases of unknown etiology that show familial clustering.^{87 88 89} Genome-wide screens have implicated loci on chromosomes 3, 7, 12, and 16.^{90 91 92} The regions on chromosomes 7 and 12 may coincide with the asthma and atopy loci on the same chromosomes. Polymorphism in the IL-1 cluster on chromosome 2 also has been shown to influence the severity of the disease.^{93 94} A genome-wide screen in families with rheumatoid arthritis similarly has shown linkage near the asthma locus on chromosome 2 and the TCR- locus on chromosome 14.⁹⁵ Linkage to type I diabetes is found near FcRI-ß on chromosome 11q13.⁹⁶ These findings suggest that important genes or gene families may be common to several inflammatory and immune disorders.

	Mendelian Disorders

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 
Asthma, eczema, and allergic diseases are associated with a number of mendelian disorders. The identification of genes causing such disorders is much easier than the positional cloning of complex disease genes. These mendelian disorders may therefore be extremely helpful in identifying genes influencing asthma and allergy. They include Netherton’s syndrome,^{97 98} Job syndrome (also known as hyper-IgE syndrome or Buckley’s syndrome),⁹⁹ thymic hypoplasia (DiGeorge syndrome), cellular deficiency with Igs (Nezelof syndrome),¹⁰⁰ selective IgA deficiency, and Wiskott-Aldrich syndrome.

Netherton’s syndrome is a rare recessive disease in which children are born with a severe ichthyotic dermatosis.⁹⁷ Severe symptomatic atopy is a universal accompaniment of the disease.⁹⁸ The gene for Netherton’s syndrome has recently been located distal to the chromosome 5 cytokine cluster,¹⁰¹ and the gene underlying the disorder has been identified as SPINK5.¹⁰² SPINK5 codes a multidomain serine protease inhibitor LEKTI, which is expressed in the epithelium, mucosa, and thymus.¹⁰³ Common coding polymorphisms have been identified in the gene by our group, and these show associations with atopy, asthma, and eczema in children without Netherton’s syndrome. These findings therefore define a new pathway for allergic disorders.

Other mendelian disorders localize to regions that may be relevant to common allergic diseases. Selective IgA deficiency has been localized to the MHC.⁶⁸ Hypereosinophilia syndrome has been localized to the distal part of the chromosome 5 cytokine cluster,¹⁰⁴ and it is of interest that acquired hypereosinophilia is associated consistently with translocations on chromosome 5q35.^{105 106} Hyper-IgE syndrome has been linked to the distal arm of chromosome 4q.¹⁰⁷ A small chromosomal deletion in one child with the disease may have limited this localization to a 20-megabase interval.¹⁰⁷ A linkage of the total serum IgE to this region has been seen in at least one genome scan (http://www.well.ox.ac.uk/asthma/public/GenomeScan/index.html),⁸ suggesting that this locus also may have an affect on the normal regulation of IgE levels.

	Conclusion

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 
The positional cloning of the genes underlying asthma and allergic disorders is becoming increasingly tractable. Agreed-on regions of strong genetic linkage have emerged, some of which coincide with linkages to single-gene disorders or to other immunologic diseases. The completion of the human genomic sequence and the availability of the deep public expressed sequence tag databases mean that laborious physical mapping of these loci may not be necessary. The key element in gene discovery will be the identification of robust patterns of LD between markers and disease. LD mapping of at least one atopy locus has shown that LD is irregularly distributed,¹⁰⁸ and the challenge is to develop statistical as well as genotyping methods to handle dense local single-nucleotide polymorphism maps.

	Footnotes

 
Abbreviations: HDM = house dust mite; IL = interleukin; LD = linkage disequilibrium; LPS = lipopolysaccharide; MHC =major histocompatibility complex; TCR = T-cell receptor; Th = T-helper cell; TNF = tumor necrosis factor

	References

TOP Abstract Genome Screens Chromosome 5 Chromosome 6 Chromosome 11q Chromosome 12 Chromosome 13q14 Sharing of Loci With... Mendelian Disorders Conclusion References

 

1. Strachan, DP, Anderson, HR, Limb, ES, et al (1994) A national survey of asthma prevalence, severity, and treatment in Great Britain. Arch Dis Child 70,174-178[Abstract]
2. Sampson, HA (1990) Pathogenesis of eczema. Clin Exp Allergy 20,459-467[CrossRef][ISI][Medline]
3. Schulz-Larsen, F (1993) A genetic-epidemiologic study in a population-based twin sample. J Am Acad Dermatol 28,719-723[ISI][Medline]
4. von Mutius, E, Fritzsch, C, Weiland, SK, et al (1992) Prevalence of asthma and allergic disorders among children in united Germany: a descriptive comparison. BMJ 305,1395-1399
5. Shirakawa, T, Enomoto, T, Shimazu, S, et al (1997) The inverse association between tuberculin responses and atopic disorder. Science 275,77-79[Abstract/Free Full Text]
6. Cookson, WO, Moffatt, MF (1997) Asthma: an epidemic in the absence of infection? Science 275,41-42[Free Full Text]
7. Rook, GA, Stanford, JL (1998) Give us this day our daily germs. Immunol Today 19,113-116[CrossRef][ISI][Medline]
8. Daniels, SE, Bhattacharrya, S, James, A, et al (1996) A genome-wide search for quantitative trait loci underlying asthma. Nature 383,247-250[CrossRef][Medline]
9. Ober, C, Cox, NJ, Abney, M, et al (1998) Genome-wide search for asthma susceptibility loci in a founder population: the Collaborative Study on the Genetics of Asthma. Hum Mol Genet 7,1393-1398[Abstract/Free Full Text]
10. Wjst, M, Fischer, G, Immervoll, T, et al (1999) A genome-wide search for linkage to asthma: German Asthma Genetics Group. Genomics 58,1-8[CrossRef][ISI][Medline]
11. Hizawa, N, Freidhoff, L, Chiu, Y, et al (1998) Genetic regulation of Dermatophagoides pteronyssinus-specific IgE responsiveness: a genome-wide multipoint linkage analysis in families recruited through 2 asthmatic sibs; Collaborative Study on the Genetics of Asthma (CSGA). J Allergy Clin Immunol 102,436-442[CrossRef][ISI][Medline]
12. . The Collaborative Study on the Genetics of Asthma (1997) A genome-wide search for asthma susceptibility loci in ethnically diverse populations. Nat Genet 15,389-392[CrossRef][ISI][Medline]
13. Dizier, MH, Besse-Schmittler, C, Guilloud-Bataille, M, et al (1999) Genome screen for asthma and related phenotypes in the French EGEA study [abstract]. Am J Respir Crit Care Med 159,A649
14. Marsh, DG, Neely, JD, Breazeale, DR, et al (1994) Linkage analysis of IL4 and other chromosome 5q31.1 markers and total serum immunoglobulin E concentrations Science 264,1152-1156[Abstract/Free Full Text]
15. Meyers, DA, Postma, DS, Panhuysen, CI, et al (1994) Evidence for a locus regulating total serum IgE levels mapping to chromosome 5. Genomics 23,464-470[CrossRef][ISI][Medline]
16. Martinez, F, Solomon, S, Holberg, C, et al (1998) Linkage of circulating eosinophils to markers on chromosome 5q. Am J Respir Crit Care Med 158,1739-1744[Abstract/Free Full Text]
17. Marquet, S, Abel, L, Hillaire, D, et al (1996) Genetic localization of a locus controlling the intensity of infection by Schistosoma mansoni on chromosome 5q31–q33. Nat Genet 14,181-184[CrossRef][ISI][Medline]
18. Kelso, A (1995) Th1 and Th2 subsets: paradigms lost? Immunol Today 16,374-379[CrossRef][ISI][Medline]
19. Graves, PE, Kabesch, M, Halonen, M, et al (2000) A cluster of seven tightly linked polymorphisms in the IL-13 gene is associated with total serum IgE levels in three populations of white children. J Allergy Clin Immunol 105,506-513[CrossRef][ISI][Medline]
20. Wills-Karp, M, Luyimbazi, J, Xu, X, et al (1998) Interleukin-13: central mediator of allergic asthma. Science 282,2258-2261[Abstract/Free Full Text]
21. Rosenwasser, LJ, Klemm, DJ, Dresback, JK, et al (1995) Promoter polymorphisms in the chromosome 5 gene cluster in asthma and atopy. Clin Exp Allergy 25,74-78
22. Walley, AJ, Cookson, WO (1996) Investigation of an interleukin-4 promoter polymorphism for associations with asthma and atopy. J Med Genet 33,689-692[Abstract/Free Full Text]
23. Shirakawa, I, Deichmann, KA, Izuhara, I, et al (2000) Atopy and asthma: genetic variants of IL-4 and IL-13 signalling. Immunol Today 21,60-64[CrossRef][ISI][Medline]
24. Ober, C, Leavitt, SA, Tsalenko, A, et al (2000) Variation in the interleukin 4-receptor alpha gene confers susceptibility to asthma and atopy in ethnically diverse populations. Am J Hum Genet 66,517-526[CrossRef][ISI][Medline]
25. Noguchi, E, Shibasaki, M, Arinami, T, et al (1999) No association between atopy/asthma and the ILe50Val polymorphism of IL-4 receptor. Am J Respir Crit Care Med 160,342-345[Abstract/Free Full Text]
26. Baldini, M, Lohman, I, Halonen, M, et al (1999) A polymorphism in the 5' flanking region of the CD14 gene is associated with circulating soluble CD14 levels and with total serum immunoglobulin E. Am J Respir Cell Mol Biol 20,976-983[Abstract/Free Full Text]
27. Xu, J, Levitt, RC, Panhuysen, CI, et al (1995) Evidence for two unlinked loci regulating total serum IgE levels. Am J Hum Genet 57,425-430[ISI][Medline]
28. Loots, GG, Locksley, RM, Blankespoor, CM, et al (2000) Identification of a coordinate regulator of interleukins 4, 13, and 5 by cross-species sequence comparisons. Science 288,136-140[Abstract/Free Full Text]
29. Lacy, DA, Wang, ZE, Symula, DJ, et al (2000) Faithful expression of the human 5q31 cytokine cluster in transgenic mice. J Immunol 164,4569-4574[Abstract/Free Full Text]
30. Marsh, DG, Meyers, DA, Bias, WB (1981) The epidemiology and genetics of atopic allergy. N Engl J Med 305,1551-1559[ISI][Medline]
31. Young, RP, Dekker, JW, Wordsworth, BP, et al (1994) HLA-DR and HLA-DP genotypes and immunoglobulin E responses to common major allergens. Clin Exp Allergy 24,431-439[CrossRef][ISI][Medline]
32. Fischer, GF, Pickl, WF, Fae, I, et al (1992) Association between IgE response against Bet v I, the major allergen of birch pollen, and HLA-DRB alleles. Hum Immunol 33,259-265[CrossRef][ISI][Medline]
33. Sparholt, SH, Georgsen, J, Madsen, HO, et al (1994) Association between HLA- DRB3^* 0101 and immunoglobulin-E responsiveness to Bet v I. Hum Immunol 39,76-78[CrossRef][ISI][Medline]
34. . et alD’Amato, M, Scotto d’Abusco, A, Maggi, E (1996) Association of responsiveness to the major pollen allergen of Parietaria officinalis with HLA-DRB1^* alleles: a multicenter study. Hum Immunol 46,100-106[CrossRef][ISI][Medline]
35. Donfack, J, Tsalenko, A, Hoki, DM, et al (2000) HLA-DRB1^* 01 alleles are associated with sensitization to cockroach allergens. J Allergy Clin Immunol 105,960-966[CrossRef][ISI][Medline]
36. Sears, MR, Herbison, GP, Holdaway, MD, et al (1989) The relative risks of sensitivity to grass pollen, house dust mite and cat dander in the development of childhood asthma. Clin Allergy 18,419-424
37. Cookson, WOCM, De Klerk, NH, Ryan, GR, et al (1991) Relative risks of bronchial hyper-responsiveness associated with skin-prick test responses to common antigens in young adults. Clin Exp Allergy 21,473-479[CrossRef][ISI][Medline]
38. Moffatt, MF, Hill, MR, Cornelis, F, et al (1994) Genetic linkage of T cell receptor / complex to specific IgE responses Lancet 343,1597-1600[CrossRef][ISI][Medline]
39. Moffatt, MF, Schou, C, Faux, JA, et al (1997) Germline TCR-A restriction of immunoglobulin E responses to allergen. Immunogenetics 46,226-230[CrossRef][ISI][Medline]
40. Daser, A, Mitchison, H, Mitchison, A, et al (1996) Non-classical-MHC genetics of immunological disease in man and mouse: the key role of pro-inflammatory cytokine genes. Cytokine 8,593-597[CrossRef][ISI][Medline]
41. Moffatt, MF, Cookson, WO (1997) Tumour necrosis factor haplotypes and asthma. Hum Mol Genet 6,551-554[Abstract/Free Full Text]
42. Li Kam Wa, TC, Mansur, AH, Britton, J, et al (1999) Association between -308 tumour necrosis factor promoter polymorphism and bronchial hyperreactivity in asthma Clin Exp Allergy 29,1204-1208[CrossRef][ISI][Medline]
43. Chagani, T, Pare, PD, Zhu, S, et al (1999) Prevalence of tumor necrosis factor-alpha and angiotensin converting enzyme polymorphisms in mild/moderate and fatal/near-fatal asthma. Am J Respir Crit Care Med 160,278-282[Abstract/Free Full Text]
44. Cookson, WOCM, Sharp, PA, Faux, J, et al (1989) Linkage between immunoglobulin E responses underlying asthma and rhinitis and chromosome 11q. Lancet 1,1292-1295[CrossRef][ISI][Medline]
45. Morton, NE (1992) Major loci for atopy? [editorial]. Clin Exp Allergy 22,1041-1043[CrossRef][ISI][Medline]
46. Turner, H, Kinet, JP (1999) Signalling through the high-affinity IgE receptor Fc epsilonRI. Nature 402,B24-B30[CrossRef][Medline]
47. Lin, S, Cicala, C, Scharenberg, A, et al (1996) The Fc(epsilon)RIbeta subunit functions as an amplifier of Fc(epsilon)RIgamma-mediated cell activation signals. Cell 85,985-995[CrossRef][ISI][Medline]
48. Hill, MR, James, AL, Faux, JA, et al (1995) FcRI-ß polymorphism and risk of atopy in a general population sample. BMJ 311,776-779[Abstract/Free Full Text]
49. Shirakawa, T, Mao, XQ, Sasaki, S, et al (1996) Association between Fc epsilon RI beta and atopic disorder in a Japanese population [letter]. Lancet 347,394-395[CrossRef][ISI][Medline]
50. van Herwerden, L, Harrap, SB, Wong, ZY, et al (1995) Linkage of high-affinity IgE receptor gene with bronchial hyperreactivity, even in absence of atopy. Lancet 346,1262-1265[CrossRef][ISI][Medline]
51. Trabetti, E, Cusin, V, Malerba, G, et al (1998) Association of the FcepsilonRIbeta gene with bronchial hyper-responsiveness in an Italian population. J Med Genet 35,680-681[Abstract/Free Full Text]
52. Cox, HE, Moffatt, MF, Faux, JA, et al (1998) Association of atopic dermatitis to the beta subunit of the high affinity immunoglobulin E receptor. Br J Dermatol 138,182-187[CrossRef][ISI][Medline]
53. Palmer, LJ, Pare, PD, Faux, JA, et al (1997) Fc epsilon R1-beta polymorphism and total serum IgE levels in endemically parasitized Australian aborigines. Am J Hum Genet 61,182-188[ISI][Medline]
54. Shirakawa, T, Li, A, Dubowitz, M, et al (1994) Association between atopy and variants of the ß subunit of the high affinity immunoglobulin E receptor. Nat Genet 7,125-129[CrossRef][ISI][Medline]
55. Hill, MR, Cookson, WOCM (1996) A new variant of the ß subunit of the high affinity receptor for immunoglobulin E (FcRI-E237G): associations with measures of atopy and bronchial hyper-responsiveness. Hum Mol Genet 5,959-962[Abstract/Free Full Text]
56. Donnadieu, E, Cookson, WO, Jouvin, MH, et al (2000) Allergy-associated polymorphisms of the FcepsilonRIbeta subunit do not impact its two amplification functions. J Immunol 165,3917-3922[Abstract/Free Full Text]
57. Duffy, D, Healey, S, Chenevix-Trench, G, et al (1995) Atopy in Australia [letter]. Nat Genet 10,260[ISI][Medline]
58. Rohrbach, M, Kraemer, R, Liechti-Gallati, S (1998) Screening of the Fc epsilon RI-beta-gene in a Swiss population of asthmatic children: no association with E237G and identification of new sequence variations. Dis Markers 14,177-186[ISI][Medline]
59. Dickson, P, Wong, Z, Harrap, S, et al (1999) Mutational analysis of the high affinity immunoglobulin E receptor beta subunit gene in asthma. Thorax 54,409-412[Abstract/Free Full Text]
60. Haider, M, Hijazi, Z (1998) Prevalence of high affinity IgE receptor [Fc epsilon RI beta] gene polymorphisms in Kuwaiti Arabs with asthma [letter]. Clin Genet 54,166-167[ISI][Medline]
61. Green, S, Gaillard, M, Song, E, et al (1998) Polymorphisms of the beta chain of the high-affinity immunoglobulin E receptor (Fcepsilon RI-beta) in South African black and white asthmatic and nonasthmatic individuals. Am J Respir Crit Care Med 158,1487-1492[Abstract/Free Full Text]
62. Cookson, WO, Young, RP, Sandford, AJ, et al (1992) Maternal inheritance of atopic IgE responsiveness on chromosome 11q. Lancet 340,381-384[CrossRef][ISI][Medline]
63. Shirakawa, T, Hashimoto, T, Furuyama, J, et al (1994) Linkage between severe atopy and chromosome 11q13 in Japanese families. Clin Genet 46,228-232[ISI][Medline]
64. Moffatt, M, Cookson, W (1998) The genetics of asthma: maternal effects in atopic disease. Clin Exp Allergy 28(suppl),56-61
65. Warram, JH, Krolewski, AS, Gottlieb, MS, et al (1984) Differences in risk of insulin-dependent diabetes in offspring of diabetic mothers and diabetic fathers. N Engl J Med 311,149-152[Abstract]
66. Koumantaki, Y, Giziaki, E, Linos, A, et al (1997) Family history as a risk factor for rheumatoid arthritis: a case-control study. J Rheumatol 24,1522-1526[ISI][Medline]
67. Akolkar, PN, Gulwani-Akolkar, B, Heresbach, D, et al (1997) Differences in risk of Crohn’s disease in offspring of mothers and fathers with inflammatory bowel disease. Am J Gastroenterol 92,2241-2244[ISI][Medline]
68. Vorechovsky, I, Webster, AD, Plebani, A, et al (1999) Genetic linkage of IgA deficiency to the major histocompatibility complex: evidence for allele segregation distortion, parent-of-origin penetrance differences, and the role of anti-IgA antibodies in disease predisposition. Am J Hum Genet 64,1096-1109[CrossRef][ISI][Medline]
69. Bennett, S, Todd, J (1996) Human type 1 diabetes and the insulin gene: principles of mapping polygenes. Annu Rev Genet 30,343-370[CrossRef][ISI][Medline]
70. Bix, M, Locksley, RM (1998) Independent and epigenetic regulation of the interleukin-4 alleles in CD4+ T cells. Science 281,1352-1354[Abstract/Free Full Text]
71. Hollander, G, Zuklys, S, Morel, C, et al (1998) Monoallelic expression of the interleukin-2 locus. Science 279,2118-2121[Abstract/Free Full Text]
72. Held, W, Raulet, D (1997) Expression of the Ly49A gene in murine natural killer cell clones is predominantly but not exclusively mono-allelic. Eur J Immunol 27,2876-2884[ISI][Medline]
73. Young, HA, Ghosh, P, Ye, J, et al (1994) Differentiation of the T helper phenotypes by analysis of the methylation state of the IFN-gamma gene. J Immunol 153,3603-3610[Abstract]
74. Barnes, KC, Neely, JD, Duffy, DL, et al (1996) Linkage of asthma and total serum IgE concentration to markers on chromosome 12q: evidence from Afro-Caribbean and caucasian populations. Genomics 37,41-50[CrossRef][ISI][Medline]
75. Nickel, R, Wahn, U, Hizawa, N, et al (1997) Evidence for linkage of chromosome 12q15–q24.1 markers to high total serum IgE concentrations in children of the German Multicenter Allergy Study Genomics 46,159-162[CrossRef][ISI][Medline]
76. Wilkinson, J, Thomas, NS, Morton, N, et al (1999) Candidate gene and mutational analysis in asthma and atopy. Int Arch Allergy Immunol 118,265-267[CrossRef][ISI][Medline]
77. Zhang, Y, Lefort, J, Kearsey, V, et al (1999) A genome-wide screen for asthma-associated quantitative trait loci in a mouse model of allergic asthma. Hum Mol Genet 8,601-605[Abstract/Free Full Text]
78. Barnes, KC, Freidhoff, LR, Nickel, R, et al (1999) Dense mapping of chromosome 12q13.12-q23.3 and linkage to asthma and atopy J Allergy Clin Immunol 104,485-491[CrossRef][ISI][Medline]
79. Eiberg, H, Lind, P, Mohr, J, et al (1985) Linkage relationship between the human immunoglobulin E polymorphism and marker systems [abstract]. Cytogenet Cell Genet 40,622
80. Kimura, K, Noguchi, E, Shibasaki, M, et al (1999) Linkage and association of atopic asthma to markers on chromosome 13 in the Japanese population. Hum Mol Genet 8,1487-1490[Abstract/Free Full Text]
81. Hizawa, N, Freidhoff, L, Ehrlich, E, et al (1998) Genetic influences of chromosomes 5q31–q33 and 11q13 on specific IgE responsiveness to common inhaled allergens among African American families: Collaborative Study on the Genetics of Asthma (CSGA). J Allergy Clin Immunol 102,449-453[CrossRef][ISI][Medline]
82. Beyer, KWU, Freidhoff, L, Nickel, R, et al (1998) Evidence for linkage of chromosome 5q31–q33 and 13q12–q14 markers to atopic dermatitis [abstract]. J Allergy Clin Immunol 101,152[CrossRef]
83. Wiltshire, S, Bhattacharyya, S, Faux, JA, et al (1998) A genome scan for loci influencing total serum immunoglobulin levels: possible linkage of IgA to the chromosome 13 atopy locus. Hum Mol Genet 7,27-31[Abstract/Free Full Text]
84. Ludviksson, BR, Eiriksson, TH, Ardal, B, et al (1992) Correlation between serum immunoglobulin A concentrations and allergic manifestations in infants. J Pediatr 121,23-27[CrossRef][ISI][Medline]
85. van Asperen, PP, Gleeson, M, Kemp, AS, et al (1985) The relationship between atopy and salivary IgA deficiency in infancy. Clin Exp Immunol 62,753-757[ISI][Medline]
86. Corrigan, CJ (1997) T and B lymphocytes and the development of allergic reactions. Kay, AB eds. Allergy and allergic diseases ,36-57 Blackwell Science Ltd Oxford, UK.
87. Rioux, JD, Silverberg, MS, Daly, MJ, et al (2000) Genome-wide search in Canadian families with inflammatory bowel disease reveals two novel susceptibility loci. Am J Hum Genet 66,1863-1870[CrossRef][ISI][Medline]
88. Duerr, RH, Barmada, MM, Zhang, L, et al (2000) High-density genome scan in Crohn disease shows confirmed linkage to chromosome 14q11–12. Am J Hum Genet 66,1857-1862[CrossRef][ISI][Medline]
89. Ma, Y, Ohmen, JD, Li, Z, et al (1999) A genome-wide search identifies potential new susceptibility loci for Crohn’s disease. Inflamm Bowel Dis 5,271-278[ISI][Medline]
90. Satsangi, J, Parkes, M, Louis, E, et al (1996) Two stage genome-wide search in inflammatory bowel disease provides evidence for susceptibility loci on chromosomes 3, 7 and 12. Nat Genet 14,199-202[CrossRef][ISI][Medline]
91. Hugot, JP, Thomas, G (1998) Genome-wide scanning in inflammatory bowel diseases. Dig Dis 16,364-369[CrossRef][ISI][Medline]
92. Duerr, RH, Barmada, MM, Zhang, L, et al (1998) Linkage and association between inflammatory bowel disease and a locus on chromosome 12. Am J Hum Genet 63,95-100[CrossRef][ISI][Medline]
93. Mansfield, J, Holden, H, Tarlow, J, et al (1994) Novel genetic association between ulcerative colitis and the anti-inflammatory cytokine interleukin-1 receptor antagonist. Gastroenterology 106,637-642[ISI][Medline]
94. Parkes, M, Satsangi, J, Jewell, D (1998) Contribution of the IL-2 and IL-10 genes to inflammatory bowel disease (IBD) susceptibility. Clin Exp Immunol 113,28-32[CrossRef][ISI][Medline]
95. Hardwick, L, Walsh, S, Butcher, S, et al (1998) Genetic mapping of susceptibility loci in the genes involved in rheumatoid arthritis. J Rheumatol 24,197-198
96. Nakagawa, Y, Kawaguchi, Y, Twells, R, et al (1998) Fine mapping of the diabetes-susceptibility locus, IDDM4, on chromosome 11q13. Am J Hum Genet 63,547-556[CrossRef][ISI][Medline]
97. Netherton, EW (1958) A unique case of trichorrhexis nodosa, "Bamboo hairs." Arch Dermatol 78,483-487[Abstract/Free Full Text]
98. Judge, MR, Morgan, G, Harper, JI (1994) A clinical and immunological study of Netherton’s syndrome. Br J Dermatol 131,615-621[CrossRef][ISI][Medline]
99. Davis, SD, Schaller, J, Wedgwood, RJ (1966) Job’s syndrome: recurrent, cold, staphylococcal abscesses. Lancet 1,1013-1015[ISI][Medline]
100. Knutsen, AP, Wall, D, Mueller, KR, et al (1996) Abnormal in vitro thymocyte differentiation in a patient with severe combined immunodeficiency-Nezelof’s syndrome. J Clin Immunol 16,151-158[CrossRef][ISI][Medline]
101. Chavanas, S, Garner, C, Bodemer, C, et al (2000) Localization of the Netherton syndrome gene to chromosome 5q32, by linkage analysis and homozygosity mapping. Am J Hum Genet 66,914-921[CrossRef][ISI][Medline]
102. Chavanas, S, Bodemer, C, Rochat, A, et al (2000) Mutations in SPINK5, encoding a serine protease inhibitor, cause Netherton syndrome. Nat Genet 25,141-142[CrossRef][ISI][Medline]
103. Mägert, HJ, Standker, L, Kreutzmann, P, et al (1999) LEKTI, a novel 15-domain type of human serine proteinase inhibitor. J Biol Chem 274,21499-21502[Abstract/Free Full Text]
104. Rioux, J, Stone, V, Daly, M, et al (1998) Familial eosinophilia maps to the cytokine gene cluster on human chromosomal region 5q31–q33. Am J Hum Genet 63,1086-1094[CrossRef][ISI][Medline]
105. Jani, K, Kempski, H, Reeves, B (1994) A case of myelodysplasia with eosinophilia having a translocation t(5; 12) (q31; q13) restricted to myeloid cells but not involving eosinophils. Br J Haematol 87,57-60[ISI][Medline]
106. Sato, H, Saito, H, Ikebuchi, K, et al (1995) Biological characteristics of chronic eosinophilic leukemia cells with a t(2; 5)(p23; q35) translocation. Leuk Lymphoma 19,499-505[ISI][Medline]
107. Grimbacher, B, Schaffer, AA, Holland, SM, et al (1999) Genetic linkage of hyper-IgE syndrome to chromosome 4. Am J Hum Genet 65,735-744[CrossRef][ISI][Medline]
108. Moffatt, MF, Traherne, JA, Abecasis, GR, et al (2000) Single nucleotide polymorphism and linkage disequilibrium within the TCR alpha/delta locus. Hum Mol Genet 9,1011-1019[Abstract/Free Full Text]

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