Literature DB >> 18555269

Comparison of non-digitalis binding properties of digoxin-specific Fabs using direct binding methods.

Mark A Pullen1, Mark R Harpel, Theodore M Danoff, David P Brooks.   

Abstract

Digibind and DigiFab are commercial formulations of polyclonal, ovine, digoxin-specific Fabs in clinical use for treatment of digoxin intoxication. Of interest for extending its use to other clinical indications, Digibind has also been reported to neutralize the effect of endogenous digoxin-like molecules, including ouabain, that are linked to clinical disorders ranging from preeclampsia to congestive heart failure. Although Digibind and DigiFab are equivalent in their digoxin-binding activity, the antigens used to produce these Fabs are different. We therefore explored, using native (3)H-digoxin and (3)H-ouabain in four different types of solution-phase binding methods, whether they might exhibit different profiles with respect to ouabain and other digoxin-like factors. Consistent with previous results, both Fab preparations bound digoxin with the same affinities and capacities. However, (3)H-ouabain was found to bind with high affinity only to Fab sub-populations present in both products. Interestingly, this sub-population was twice as large for Digibind compared to DigiFab. Competition experiments also showed differences in specificity within Fab sub-populations. Therefore, the equivalence in digoxin-binding activity of the two Fab preparations does not extend to ouabain-binding capacity and Fab specificity, with implications for clinical differentiation between the preparations in treatment of disorders related to control of non-digoxin cardenolides. The existence of a small but perhaps clinically relevant sub-population of antibodies was detected using specific radioligands. This sub-population could not have been detected nor quantified using standard cross-reactivity in an ELISA assay.

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Year:  2008        PMID: 18555269     DOI: 10.1016/j.jim.2008.05.005

Source DB:  PubMed          Journal:  J Immunol Methods        ISSN: 0022-1759            Impact factor:   2.303


  8 in total

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Authors:  Mordecai P Blaustein
Journal:  Am J Physiol Heart Circ Physiol       Date:  2017-07-21       Impact factor: 4.733

4.  Central and peripheral slow-pressor mechanisms contributing to Angiotensin II-salt hypertension in rats.

Authors:  Jiao Lu; Hong-Wei Wang; Monir Ahmad; Marzieh Keshtkar-Jahromi; Mordecai P Blaustein; John M Hamlyn; Frans H H Leenen
Journal:  Cardiovasc Res       Date:  2018-02-01       Impact factor: 10.787

Review 5.  The pump, the exchanger, and the holy spirit: origins and 40-year evolution of ideas about the ouabain-Na+ pump endocrine system.

Authors:  Mordecai P Blaustein
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6.  Interaction of Digibind with endogenous cardiotonic steroids from preeclamptic placentae.

Authors:  Olga V Fedorova; Natalia I Tapilskaya; Anton M Bzhelyansky; Elena V Frolova; Elena R Nikitina; Vitaly A Reznik; Vladimir A Kashkin; Alexei Y Bagrov
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7.  The cardiac glycoside binding site on the Na,K-ATPase alpha2 isoform plays a role in the dynamic regulation of active transport in skeletal muscle.

Authors:  T L Radzyukevich; J B Lingrel; J A Heiny
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Review 8.  Endogenous digitalis-like factors: an overview of the history.

Authors:  Vardaman M Buckalew
Journal:  Front Endocrinol (Lausanne)       Date:  2015-04-13       Impact factor: 5.555

  8 in total

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