Aptamer Neutralization of Beta1-Adrenoceptor Autoantibodies Isolated From Patients With Cardiomyopathies

Haberland, Annekathrin; Wallukat, Gerd; Dahmen, Claudia; Kage, Andreas; Schimke, Ingolf

doi:10.1161/circresaha.111.253849

Cited by 63 publications

(41 citation statements)

References 26 publications

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“…11 Our previously selected aptamer using the Monolex technology 12 bound β1-AABs isolated from patients with DCM, Chagas' cardiomyopathy, or peripartum cardiomyopathy and neutralized their pathogenic functions, which we demonstrated in vitro by reducing β1-AAB-induced chronotropy and apoptosis. 1 However, as recently discussed, 13 the relationship between the selected aptamer and β1-AABs must be consolidated in vivo using animal models.…”

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confidence: 99%

The First Aptamer-Apheresis Column Specifically for Clearing Blood of β1-Receptor Autoantibodies

Wallukat

Haberland

Berg

et al. 2012

Circ J

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Circulation Journal Official Journal of the Japanese Circulation Society http://www. j-circ.or.jp e present here for the first time in vitro and animal experiments demonstrating aptamer-based clearing from blood of pathogenic autoantibodies targeting the second extracellular loop of the β1-receptor using apheresis technology.We recently published the selection and identification of a novel ssDNA aptamer that targets autoantibodies directed against the second extracellular loop of the adrenergic β1-receptor (β1-AABs). 1 As recently summarized, 2,3 autoantibodies directed against the first or second extracellular loop of the adrenergic β1-receptor (ie, β1-AABs) have been found in patients with cardiomyopathies, with evidence that mainly β1-AABs directed at the second loop are related to disease pathogenesis. 4 Up to 80% of patients with dilated cardiomyopathy (DCM) are positive for either first-or second-loop β1-AABs; approximately one-half of the patients present with first-loop β1-AABs, the other half with second-loop β1-AABs. As demonstrated in a Bolivian cohort, nearly 100% of patients with Chagas' cardiomyopathy are positive for second-loop β1-AABs. 5 A first indication exists that exclusively second-loop β1-AABs were found also in patients with peripartum cardiomyopathy. 6 Consequently, technologies have been developed to clear β1-AABs from the blood of β1-AAB-positive DCM patients via immunoapheresis. In addition, β1-AAB immunoapheresis has been suggested for the treatment of Chagas' patients. Background: Application of immunoapheresis to eliminate pathogenic autoantibodies targeting the second extracellular loop of the β1-receptor (β1-AABs) is currently investigated in patients with cardiomyopathy. Aptamers (single short DNA or RNA strands) are a new class of molecules that bind to a specific target molecule. This property qualifies aptamers for potential use in the apheresis technique. We recently identified an aptamer that specifically binds to β1-AABs, so in the present study we tested whether this aptamer could be used as a binder to prepare an apheresis column suitable for clearing β1-AABs from rat's blood.

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The First Aptamer-Apheresis Column Specifically for Clearing Blood of β1-Receptor Autoantibodies

Wallukat

Haberland

Berg

et al. 2012

Circ J

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“…Novel therapy-modalities specifically directed against cardio-noxious β 1 AR-autoantibodies comprise extracorporeal IgG-absorption [14][15][16] and neutralisation/clearance of β 1 AR-autoantibodies by systemic administration of synthetic epitope mimics [17][18][19][20]. DCM patients with reduced cardiac function are considered to benefit from therapies selective for β 1 AR-autoantibodies only when they are positive for β 1 AR-autoantibodies [14,15].…”

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A standardised FACS assay based on native, receptor transfected cells for the clinical diagnosis and monitoring of β1-adrenergic receptor autoantibodies in human heart disease

Bornholz

Benninghaus

Reinke

et al. 2016

Clinical Chemistry and Laboratory Medicine (CCLM)

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“…To be useful in the clinical setting, such a treatment must be conveniently administered and be relatively free of adverse events. In the current issue of Circulation Research, Haberland et al 19 demonstrate that a singlestrand DNA aptamer could be such a therapeutic compound.…”

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“…In the current article, Haberland et al 19 use MonoLEX technology, 35 a variant of SELEX, to generate aptamers that neutralize and inactivate ␤ 1 -AR AAbs. Interestingly, the 21 nucleotide DNA sequence investigated, aptamer 110, markedly attenuated ␤ 1 -AR AAb-mediated increases in heart rate and apoptosis in cultured cardiac myocytes.…”

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Aptamer Therapy for Heart Failure?

Port

Bristow

2011

Circulation Research

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Aptamer Neutralization of Beta1-Adrenoceptor Autoantibodies Isolated From Patients With Cardiomyopathies

Cited by 63 publications

References 26 publications

The First Aptamer-Apheresis Column Specifically for Clearing Blood of β1-Receptor Autoantibodies

The First Aptamer-Apheresis Column Specifically for Clearing Blood of β1-Receptor Autoantibodies

A standardised FACS assay based on native, receptor transfected cells for the clinical diagnosis and monitoring of β1-adrenergic receptor autoantibodies in human heart disease

Aptamer Therapy for Heart Failure?

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