IQUIBICEN   23947
INSTITUTO DE QUIMICA BIOLOGICA DE LA FACULTAD DE CIENCIAS EXACTAS Y NATURALES
Unidad Ejecutora - UE
artículos
Título:
MODIFICATION OF ERYTHROPOIETIN STRUCTURE BY N-HOMOCYSTEINYLATION AFFECTS ITS ANTIAPOPTOTIC AND PROLIFERATIVE FUNCTIONS
Autor/es:
SCHIAPPACASSE A; NESSE A; CHAMORRO MARIA E; VITTORI D; MALTANERI R; WETZLER D
Revista:
FEBS JOURNAL
Editorial:
WILEY-BLACKWELL PUBLISHING, INC
Referencias:
Lugar: Londres; Año: 2018 vol. 285 p. 3801 - 3814
ISSN:
1742-464X
Resumen:
Many patients under therapy with recombinant human erythropoietin (rhuEPO) show resistance to the treatment, an effect likely associated with the accumulation of tissue factors, especially in renal and cardiovascular diseases. Hyperhomocysteinemia due to high serum levels of homocysteinehas been suggested among the risk factors in those pathologies. Its main effect is the N-homocysteinylation of proteins due to the interaction between the highly reactive homocysteine thiolactone (HTL) and lysine residues. The aim of this study was to evaluate the effect of N-homocysteinylation on the erythropoietic and antiapoptotic abilities of EPO, which can be aconsequence of structural changes in the modified protein. We found that both cellular functions were altered in the presence of HTL-EPO. A decreased net positive charge of HTL-EPO was detected by capillary zone electrophoresis, while analysis of polyacrylamide gel electropherogramssuggested formation of aggregates. Far-UV spectra, obtained by Circular Dichroism Spectroscopy, indicated a switch of the protein?s secondary structure from a-helix to b-sheet structures. Results of Congo red and Thioflavin T assays confirm the formation of repetitive b-sheet structures, which may account for aggregates. Accordingly, Dynamic Light Scatteringanalysis showed a markedly larger radius of the HTL-EPO structures, supporting the formation of soluble oligomers. These structural changes might interfere with the conformational adaptations necessary for efficient ligandreceptor interaction, thus affecting the proliferative and antiapoptoticfunctions of EPO. The present findings may contribute to explain the resistance exhibited by patients with cardio-renal syndrome to treatment with rhuEPO, as a consequence of structural modifications due to protein N-homocysteinylation.