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Detection and isolation of cell-derived microparticles are compromised by protein complexes resulting from shared biophysical parameters

Authors :
Krisztina Pálóczi
Petra Misják
Anna Polgár
György Nagy
Kálmán Tóth
Bence György
Anikó Szalai
Maria Pasztoi
István Voszka
Mária A. Deli
Edit I. Buzás
Mária Csete
Ágnes Kittel
Áron Sipos
Károly Módos
Éva Pállinger
András Falus
Source :
Blood. 117(4)
Publication Year :
2010

Abstract

Numerous diseases, recently reported to associate with elevated microvesicle/microparticle (MP) counts, have also long been known to be characterized by accelerated immune complex (IC) formation. The goal of this study was to investigate the potential overlap between parameters of protein complexes (eg, ICs or avidin-biotin complexes) and MPs, which might perturb detection and/or isolation of MPs. In this work, after comprehensive characterization of MPs by electron microscopy, atomic force microscopy, dynamic light-scattering analysis, and flow cytometry, for the first time, we drive attention to the fact that protein complexes, especially insoluble ICs, overlap in biophysical properties (size, light scattering, and sedimentation) with MPs. This, in turn, affects MP quantification by flow cytometry and purification by differential centrifugation, especially in diseases in which IC formation is common, including not only autoimmune diseases, but also hematologic disorders, infections, and cancer. These data may necessitate reevaluation of certain published data on patient-derived MPs and contribute to correct the clinical laboratory assessment of the presence and biologic functions of MPs in health and disease.

Details

ISSN :
15280020
Volume :
117
Issue :
4
Database :
OpenAIRE
Journal :
Blood
Accession number :
edsair.doi.dedup.....a4d26a5256aab4be47726bbe8c74a8ac