Chromosome 11q13 and atopic asthma

Adra, Chaker N.; Mao, Xiao-Quan; Kawada, H.; Gao, Peisong; Korzycka, B.; Donate, J. L.; Shaldon, S. R.; Coull, P.; Dubowitz, M.; Enomoto, Tadao; Ozawa, A.; Syed, Salam A.; Horiuchi, T; Khaeraja, R.; Khan, Rafsa; Lin, Shiquan; Flinter, Frances; Beales, Philip L.; Hagihara, Akihito; Inoko, Hidetoshi; Shirakawa, Taro; Hopkin, Julian M.

doi:10.1034/j.1399-0004.1999.550606.x

Cited by 44 publications

(46 citation statements)

References 53 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…This fact makes it more reliable that the association found reflects a common biological mechanism since there are more alleles transmitted (73) and non-transmitted (40) with the disease phenotype. Our results support those obtained earlier (Adra et al 1999;Collee et al 1993;Cox et al 1998;Folster-Holst et al 1998;Shirakawa et al 1994Shirakawa et al , 1996van Herwerden et al 1995) indicating that the locus on 11q13 contributes to the development of atopic diseases. Association in non-inbred populations is usually only seen over small distances.…”

Section: Discussionsupporting

confidence: 96%

“…Chromosome 11q13 was the first region to which a putative atopy gene was localised (Cookson et al 1989) and members of the same group later identified the β-subunit of the high-affinity IgE receptor as a candidate gene for atopic diseases (Sandford et al 1993). Other groups (Adra et al 1999;Collee et al 1993;Cox et al 1998;FolsterHolst et al 1998;Hizawa et al 1998;Shirakawa et al 1994Shirakawa et al , 1996van Herwerden et al 1995) have confirmed genetic linkage to the 11q13 region, whereas other groups have not detected linkage to atopic disease (Amelung et al 1992;Brereton et al 1994;Coleman et al 1993;Deichmann et al 1999;Hizawa et al 1992;Lympany et al 1992;Rich et al 1992). We have found only weak evidence in favour of linkage for 11q13 to raised allergenspecific serum IgE levels.…”

Section: Discussionmentioning

confidence: 98%

See 1 more Smart Citation

Linkage and association to candidate regions in Swedish atopic dermatitis families

et al. 2001

View full text Add to dashboard Cite

We have studied, in 406 families with at least two siblings affected with atopic dermatitis (in total 1514 individuals) from the Swedish population, linkage and association to five chromosomal regions (2q35, 5q31-33, 6p21, 11q13 and 14q11) previously implicated in atopic diseases. The region on 14q11 gave evidence for linkage to atopic dermatitis (NPL-score: 2.36, P<0.009). In the 11q13 region, there was a clear association to an intragenic marker in the beta-subunit of the high-affinity IgE receptor for raised allergen-specific serum IgE levels (P<0.009). When a quantitative variable for the severity of atopic dermatitis was studied, evidence was found in favour of linkage to the 5q31-33 region, with the highest Z-score (2.06) close to the marker D5S458 (P<0.005).

show abstract

Section: Discussionsupporting

confidence: 96%

Section: Discussionmentioning

confidence: 98%

Linkage and association to candidate regions in Swedish atopic dermatitis families

et al. 2001

View full text Add to dashboard Cite

show abstract

“…Because the competitive antagonist MK571 interfered with calcium flux in response to both cys-LTs and to UDP, it is likely that the respective binding sites for the two agonists are in close proximity to one another. The genes encoding the P2Y6 receptor and the P2Y2 receptor, which also binds uridine nucleotides, are closely linked on human chromosome 11q13 (29), a region containing genes linked to the inheritance of asthma (30,31). The respective genes encoding the CysLT1 receptor and the P2Y4 receptor, both of which are expressed by hMCs, are closely linked on human chromosome Xq13-21, another region containing candidate asthma genes (19).…”

Section: Resultsmentioning

confidence: 99%

Cysteinyl leukotriene receptor 1 is also a pyrimidinergic receptor and is expressed by human mast cells

Mellor

Maekawa

Austen

et al. 2001

Proc. Natl. Acad. Sci. U.S.A.

160

162

View full text Add to dashboard Cite

show abstract

“…Regarding the chromosome 11q some studies have confirmed the linkage of atopy and bronchial hyperresponsiveness to markers on 11q13 (Adra et al 1999;Collée et al 1993;Daniels et al 1996;van Herwerden et al 1995;Mao et al 1997;Shirakawa et al 1994a;Young et al 1992), while others have failed to find the linkage (Amelung et al 1992; Collaborative Study on the Genetics of Asthma 1997; Hizawa et al 1992;Lympany et al 1992;Malerba et al 1999;Ober et al 1998;Rich et al 1992;Wjst et al 1999;Yokouchi et al 2000). Meanwhile, the gene for the β-chain of the high-affinity receptor for IgE (FcεRIβ) has been identified as a candidate gene for this linkage between atopy and 11q13 (Sandford et al 1993), and two coding variants in exon 6 of FcεRIβ, Ile181Leu/Ile183Val and Ile181Leu, are reported to be associated with atopy in British subjects (Shirakawa et al 1994b).…”

Section: Introductionmentioning

confidence: 93%

Association between nasal allergy and a coding variant of the Fc ε RI β gene Glu237Gly in a Japanese population

et al. 2001

View full text Add to dashboard Cite

The gene for the beta-chain of the high-affinity receptor for IgE (Fc epsilon RI beta) has been proposed as a candidate gene for atopy. A coding variant Glu237Gly has been studied in various populations with asthma and atopy, and the results were controversial for association of the variant with atopy/asthma. Because nasal allergy is a more common atopic disease and shows less remission than asthma, we analyzed whether the Glu237Gly variant is correlated with nasal allergy. The study enrolled 233 patients with nasal allergy and 100 control subjects. Further, three subgroups were selected: patients with perennial nasal allergy (n=149), Japanese cedar pollinosis (n=189), and allergy to multiple allergens (n=45). The allele frequency of Gly237 in the controls and patients was 0.14 and 0.20, and the frequency of Gly237-positive subjects was 0.23 and 0.356, respectively. There was a significant association between Gly237-positivity and nasal allergy, perennial nasal allergy, Japanese cedar pollinosis, and allergy to multiple allergens. Among all 333 subjects we observed a significant relationship between Gly237 and elevated levels of serum total IgE (>250 IU/ml) and very high IgE (>1000 IU/ml). Among patients positive for a specific IgE, Gly237 was significantly associated with high IgE for house dust, mite, and Japanese cedar pollen. These results suggest that the Glu237Gly variant of the Fc epsilon RI beta gene is involved in the development of nasal allergy through the process for the production of both specific and nonspecific IgE antibodies.

show abstract

Chromosome 11q13 and atopic asthma

Cited by 44 publications

References 53 publications

Linkage and association to candidate regions in Swedish atopic dermatitis families

Linkage and association to candidate regions in Swedish atopic dermatitis families

Cysteinyl leukotriene receptor 1 is also a pyrimidinergic receptor and is expressed by human mast cells

Association between nasal allergy and a coding variant of the Fc ε RI β gene Glu237Gly in a Japanese population

Contact Info

Product

Resources

About