4.4 Article

Relevance of the low-affinity type of the Fc gamma-receptor IIIa-polymorphism in bullous pemphigoid

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ARCHIVES OF DERMATOLOGICAL RESEARCH
卷 299, 期 3, 页码 163-164

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SPRINGER
DOI: 10.1007/s00403-007-0755-8

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Fcgamma IIIa; autoimmune; bullous pemphigoid; receptor; polymorphism

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Bullous pemphigoid (BP) is mediated by autoantibodies directed against molecules of the basement membrane zone. The biological function of antibodies involves binding to Fc-receptors expressed on human leucocytes. Recent studies suggested that a functional single-nucleotide-polymorphism of the Fc gamma-receptor IIIa (Fc gamma RIIIa = CD16) at nucleotide 559 might predispose to the development of antibody-associated autoimmune disorders. This allelic difference affects the level of receptor affinity by predicting either a phenylalanine (F 158, low-affinity) or valine (V 158, high-affinity). We investigated if inherited frequencies of the high- and low-affinity Fc gamma RIIIa polymorphism differed between patients with BP and healthy subjects. Genomic DNA from peripheral white blood cells was analyzed regarding Fc gamma RIIIa polymorphism at nucleotide 559 by an established polymerase chain reaction. Sixty-seven Caucasian patients with BP and 88 healthy controls were included into the study. There was no significant difference in the distribution of the homozygous high-affinity Fc gamma RIIIa-allotype (V/V) between BP-patients (14.9%) and healthy control subjects (20.5%). In contrast, 58.2% of the BP-patients were homozygous for the low-affinity Fc gamma RIIIa-allotype (F/F), compared to 28.4% of the healthy controls (P = 0.001, OR 3.51). The frequencies of the polymorphism in the control group were in range of formerly published frequencies for healthy Caucasian subjects. Thus, the Fc gamma RIIIa (158 F/V) polymorphism may modulate the susceptibility to acquire BP.

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