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Modification of Cholinergic-Mediated Cellular Transmembrane Signals by the Interaction of Human Chagasic IgG with Cardiac Muscarinic Receptors

 

作者: Juan Carlos Goin,   Claudia Pérez Leirós,   Enri Borda,   Leonor Sterin-Borda,  

 

期刊: Neuroimmunomodulation  (Karger Available online 1994)
卷期: Volume 1, issue 5  

页码: 284-291

 

ISSN:1021-7401

 

年代: 1994

 

DOI:10.1159/000097178

 

出版商: S. Karger AG

 

关键词: Chagas' disease;cAMP;cGMP;Immunoprecipitation;Contractility;Muscarinic cholinergic receptors

 

数据来源: Karger

 

摘要:

The possible role of altered humoral immunity in cardiac Chagas'' disease was examined by analyzing the interaction of IgG and the corresponding F(ab′)2 from Trypanosoma cruzi-infected patients with cardiac muscarinic cholinergic receptors (mAchR). Human chagasic IgG and its F(ab′)2 simulated the agonist amons triggering the biological effects associated with cholinergic-mediated cellular transmembrane signals, i.e. stimulation of cGMP, inhibition of cAMP and a decrease in atrial contractility. Atropine blunted all of these effects while pertussis toxin prevented the inhibition of cAMP and contractility confirming the G-regulatory-protein-mediated response in the interaction of chagasic antibodies with cardiac mAchR. In addition, chagasic IgG and its F(ab′)2 behaved as partial agonists activating the specific receptor and inhibiting in a noncompetitive manner the activity of an exogenous agonist (pilocarpine). Moreover, chagasic IgG immunoprecipitated the mAchR solu-bilized from cardiac membrane in a concentration-dependent fashion. By means of SDS-PAGE and immunoblotting analysis, chagasic serum was shown to recognize a band of approximately 75 kD. The electrophoretic studies of prelabeled immunoprecipitated proteins revealed a peak of [3H] propyl-benzilylcholine mustard with an apparent molecular weight similar to that of mAchR, which disappeared in the presence of atropine. The presence of these antibodies in the serum of chagasic patients could explain the progressive receptor blockade in the parasympathetic branch of the cardiac autonomic nervous system associated with the cardioneuromyopathy described in the course of Chagas'' di

 

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