Am. J. Respir. Crit. Care Med., Vol 153, No. 1, Jan 1996, 76-82.
Associations of blood group-related antigens to FEV1, wheezing, and asthma
F Kauffmann, C Frette, QT Pham, S Nafissi, JP Bertrand and R Oriol
INSERM U169, Villejuif, France.
Discordant results have been observed regarding the associations of chronic
obstructive pulmonary diseases with secretor, Lewis, and ABO histo-blood
groups, which are defined by glycosyltransferases. These enzymes build up
oligosaccharide structures that play a role in the adhesion of
environmental factors to epithelial cells. The objectives of the present
study were to assess the role of all three systems, Lewis (Le), salivary
ABH secretor (Se), and red cell blood group ABO, on lung function,
wheezing, and asthma in a cohort of 228 coal miners studied
cross-sectionally, considering the potential modifying effect of
environmental factors on these associations. Asthma was significantly
related to nonsecretor phenotype. Significantly lower lung function and
higher prevalences of wheezing and asthma were observed in Lewis-negative
or nonsecretor subjects of blood group O. Very low lung function values
were observed in the small group of Lewis- negative nonsecretors who lack
both Le and Se controlled fucoses (1% of Caucasians). Lewis-positive,
salivary ABH secretors who have these two fucoses represent 70% of
Caucasians. Among these subjects, lower lung function was observed in blood
group A, and in a lesser extent in blood group B, i.e., with terminal alpha
GaINAc or alpha Gal respectively, than in blood group O subjects. ABO,
Lewis, and secretor phenotypes did not account for the potential genetic
heterogeneity of subjects toward smoking, but alcohol consumption appeared
to exert a protective effect on lung function in Lewis-negative subjects
(10% of Caucasians). If confirmed in other populations, the magnitude of
the effects observed regarding low lung function in Lewis-negative ABH
nonsecretors, and the protective effect of Lewis negative on the
deleterious effect of alcohol, may be of clinical importance. Further
studies of the combined effects of various histo-blood group genetic
systems seem worthwhile, particularly for airflow limitation, wheezing, and
asthma, possibly with reference to susceptibility to infectious agents.
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Copyright © 1996 American Thoracic Society
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