Direct evidence for a β1-adrenergic receptor–directed autoimmune attack as a cause of idiopathic dilated cardiomyopathy
Roland Jahns, Valérie Boivin, Lutz Hein, Sven Triebel, Christiane E. Angermann, Georg Ertl, Martin J. Lohse
Roland Jahns, Valérie Boivin, Lutz Hein, Sven Triebel, Christiane E. Angermann, Georg Ertl, Martin J. Lohse
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Article Autoimmunity

Direct evidence for a β1-adrenergic receptor–directed autoimmune attack as a cause of idiopathic dilated cardiomyopathy

Abstract

Today, dilated cardiomyopathy (DCM) represents the main cause of severe heart failure and disability in younger adults and thus is a challenge for public health. About 30% of DCM cases are genetic in origin; however, the large majority of cases are sporadic, and a viral or immune pathogenesis is suspected. Following the established postulates for pathogenesis of autoimmune diseases, here we provide direct evidence that an autoimmune attack directed against the cardiac β1-adrenergic receptor may play a causal role in DCM. First, we immunized inbred rats against the second extracellular β1-receptor loop (β1-ECII; 100% sequence identity between human and rat) every month. All these rats developed first, receptor-stimulating anti–β1-ECII Ab’s and then, after 9 months, progressive severe left ventricular dilatation and dysfunction. Second, we transferred sera from anti–β1-ECII–positive and Ab-negative animals every month to healthy rats of the same strain. Strikingly, all anti–β1-ECII–transferred rats also developed a similar cardiomyopathic phenotype within a similar time frame, underlining the pathogenic potential of these receptor Ab’s. As a consequence, β1-adrenergic receptor–targeted autoimmune DCM should now be categorized with other known receptor Ab-mediated autoimmune diseases, such as Graves disease or myasthenia gravis. Although carried out in an experimental animal model, our findings should further encourage the development of therapeutic strategies that combat harmful anti–β1-ECII in receptor Ab–positive DCM patients.

Authors

Roland Jahns, Valérie Boivin, Lutz Hein, Sven Triebel, Christiane E. Angermann, Georg Ertl, Martin J. Lohse

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β1-AR/β2-AR subtypes and urine catecholamines. (A) Immunization and (B) ...
β1-AR/β2-AR subtypes and urine catecholamines. (A) Immunization and (B) transfer experiment. Columns represent total β-AR density and the amount of β1-AR and β2-AR subtypes (femtomoles per milligram of protein) in cardiac membranes of β1-ECII–injected (n = 15, aged 18 months) or anti–β1-ECII-transferred rats (n = 10, aged 15 months), and corresponding control animals at the end of each experiment (n = 20 or n = 10, respectively). Error bars indicate mean values plus or minus SEM. **P < 0.01; ***P < 0.001. The inset in A depicts a representative radioligand displacement curve using the β1-selective antagonist CGP 20712A (immunization experiment). (C) Immunization and (D) transfer experiment. Columns correspond to urine catecholamine concentrations determined at study end. Error bars indicate mean values plus or minus SEM.