Isolation and identification in human blood serum of the proteins possessing the ability to bind with 48 kDa form of unconventional myosin 1c and their possible diagnostic and prognostic value

Starykovych, M.; Antonyuk, V.; Nehrych, T.; Negrych, N.; Horák, Daniel; Souchelnytskyi, S.; Kit, O.; Stoika, R.; Kit, Y.

doi:https://dx.doi.org/10.1002/bmc.5029

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Isolation and identification in human blood serum of the proteins possessing the ability to bind with 48 kDa form of unconventional myosin 1c and their possible diagnostic and prognostic value

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0540994 - ÚMCH 2022 RIV GB eng J - Článek v odborném periodiku
Starykovych, M. - Antonyuk, V. - Nehrych, T. - Negrych, N. - Horák, Daniel - Souchelnytskyi, S. - Kit, O. - Stoika, R. - Kit, Y.
Isolation and identification in human blood serum of the proteins possessing the ability to bind with 48 kDa form of unconventional myosin 1c and their possible diagnostic and prognostic value.
Biomedical Chromatography. Roč. 35, č. 4 (2021), č. článku e5029. ISSN 0269-3879. E-ISSN 1099-0801
Institucionální podpora: RVO:61389013
Klíčová slova: human blood serum * 48/Myo1C protein * magnetic microparticles
Obor OECD: Polymer science
Impakt faktor: 1.911, rok: 2021
Způsob publikování: Omezený přístup
https://analyticalsciencejournals.onlinelibrary.wiley.com/doi/10.1002/bmc.5029

We firstly identified 48 kDa molecular form of the unconventional myosin 1c (p48/Myo1C), and isolated it from blood serum of multiple sclerosis patients. The amount of p48/Myo1C in human blood serum correlated with some autoimmune, hemato‐oncological and neurodegenerative diseases and thus may serve as a potential molecular biomarker. The biological functions of this protein in human blood remain unknown. Previously, we used the monodisperse magnetic poly (glycidyl methacrylate)(mag‐PGMA–NH2) microspheres with immobilized 48/Myo1C and western‐blot analysis, which allowed us to identify IgM and IgG immunoglobulins presenting an affinity to this protein. Here, we used mass spectrometry followed by the western blotting in order to identify other blood serum proteins with affinity to 48/Myo1C. The obtained data demonstrate that 48/Myo1C binds to component 3 of the complement and the antithrombin‐III proteins. A combination of magnetic microparticle‐based affinity chromatography with MALDI–TOF mass spectrometry and an in silico analysis provided an opportunity to identify the partners of interaction of 48/Myo1C with other proteins, in particular those participating in complement and coagulation cascades.
Trvalý link: http://hdl.handle.net/11104/0319047

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