Your search keyword '"monomeric ubiquitin"' showing total 4 results

1. Almost 50 Years of Monomeric Extracellular Ubiquitin (eUb).

Author

Mendoza-Salazar, Ivette, Fragozo, Ana, González-Martínez, Aneth P., Trejo-Martínez, Ismael, Arreola, Rodrigo, Pavón, Lenin, Almagro, Juan C., Vallejo-Castillo, Luis, Aguilar-Alonso, Francisco A., and Pérez-Tapia, Sonia M.

Subjects

*UBIQUITIN, *POST-translational modification

Abstract

Monomeric ubiquitin (Ub) is a 76-amino-acid highly conserved protein found in eukaryotes. The biological activity of Ub first described in the 1970s was extracellular, but it quickly gained relevance due to its intracellular role, i.e., post-translational modification of intracellular proteins (ubiquitination) that regulate numerous eukaryotic cellular processes. In the following years, the extracellular role of Ub was relegated to the background, until a correlation between higher survival rate and increased serum Ub concentrations in patients with sepsis and burns was observed. Although the mechanism of action (MoA) of extracellular ubiquitin (eUb) is not yet well understood, further studies have shown that it may ameliorate the inflammatory response in tissue injury and multiple sclerosis diseases. These observations, compounded with the high stability and low immunogenicity of eUb due to its high conservation in eukaryotes, have made this small protein a relevant candidate for biotherapeutic development. Here, we review the in vitro and in vivo effects of eUb on immunologic, cardiovascular, and nervous systems, and discuss the potential MoAs of eUb as an anti-inflammatory, antimicrobial, and cardio- and brain-protective agent. [ABSTRACT FROM AUTHOR]

Published

2024

2. Almost 50 Years of Monomeric Extracellular Ubiquitin (eUb)

Author

Ivette Mendoza-Salazar, Ana Fragozo, Aneth P. González-Martínez, Ismael Trejo-Martínez, Rodrigo Arreola, Lenin Pavón, Juan C. Almagro, Luis Vallejo-Castillo, Francisco A. Aguilar-Alonso, and Sonia M. Pérez-Tapia

Subjects

extracellular ubiquitin, monomeric ubiquitin, immunomodulatory drugs, sepsis, biotherapeutic proteins, Medicine, Pharmacy and materia medica, RS1-441

Abstract

Monomeric ubiquitin (Ub) is a 76-amino-acid highly conserved protein found in eukaryotes. The biological activity of Ub first described in the 1970s was extracellular, but it quickly gained relevance due to its intracellular role, i.e., post-translational modification of intracellular proteins (ubiquitination) that regulate numerous eukaryotic cellular processes. In the following years, the extracellular role of Ub was relegated to the background, until a correlation between higher survival rate and increased serum Ub concentrations in patients with sepsis and burns was observed. Although the mechanism of action (MoA) of extracellular ubiquitin (eUb) is not yet well understood, further studies have shown that it may ameliorate the inflammatory response in tissue injury and multiple sclerosis diseases. These observations, compounded with the high stability and low immunogenicity of eUb due to its high conservation in eukaryotes, have made this small protein a relevant candidate for biotherapeutic development. Here, we review the in vitro and in vivo effects of eUb on immunologic, cardiovascular, and nervous systems, and discuss the potential MoAs of eUb as an anti-inflammatory, antimicrobial, and cardio- and brain-protective agent.

Published

2024

3. Sequencing Analysis and Identification of the Primary Peptide Component of the Dialyzable Leukocyte Extract 'Transferon Oral': The Starting Point to Understand Its Mechanism of Action

Author

Luis Vallejo-Castillo, Liliana Favari, Said Vázquez-Leyva, Gabriela Mellado-Sánchez, Zaira Macías-Palacios, Leonardo E. López-Juárez, Luis Valencia-Flores, Emilio Medina-Rivero, Rommel Chacón-Salinas, Lenin Pavón, and Sonia Mayra Pérez-Tapia

Subjects

Transferon, human dialyzable leukocyte extracts, MS sequencing, immunomodulatory drugs, oral peptides, monomeric ubiquitin, Therapeutics. Pharmacology, RM1-950

Abstract

“Transferon Oral” is a peptide-derived product with immunomodulatory properties obtained from the lysis and dialysis of human buffy coat. Its active pharmaceutical ingredient, generically known as Dialyzable Leucocyte Extract, is a mixture of peptide populations with reproducible proportions among batches. “Transferon Oral” modulates IFN-γ, TNF-α, and IL-6 and increases the survival rate in a herpes infection murine model when oropharyngeally (ORO) administered, which correlate with clinical observations where “Transferon Oral” is used as a therapeutic auxiliary in inflammatory diseases. Notwithstanding, how a peptide-derived product elicits systemic modulation of cytokines when ORO administered remains unclear. To shed light on the pharmacology of “Transferon Oral” its peptide components must be known. Ten “Transferon Oral” batches were sequenced by mass spectrometry and the intact peptides were identified. The most abundant peptides were the monomeric human Ubiquitin (Ub), a globular low-molecular mass protein, and an Ub variant which lacks the two-terminal Gly (Ub-GG). Recombinant Ub prevented murine death when ORO administered in a herpes infection murine model. Besides, the percentage of survival increased in groups treated with Transferon Oral+Ub and decreased in groups treated with Ub-depleted “Transferon Oral” respect to the group treated with “Transferon Oral” only. Our findings indicate that the biological properties of “Transferon Oral” are partially associated to the Ub content. They suggest that Ub may activate its extracellular receptor (CXCR-4) in the stomach eliciting systemic immunomodulatory effects via vagus nerve. This is the first report that identifies an active component of “Transferon Oral” with the potential for the development of oral peptide immunomodulators.

Published

2020

4. Sequencing Analysis and Identification of the Primary Peptide Component of the Dialyzable Leukocyte Extract "Transferon Oral": The Starting Point to Understand Its Mechanism of Action.

Author

Vallejo-Castillo, Luis, Favari, Liliana, Vázquez-Leyva, Said, Mellado-Sánchez, Gabriela, Macías-Palacios, Zaira, López-Juárez, Leonardo E., Valencia-Flores, Luis, Medina-Rivero, Emilio, Chacón-Salinas, Rommel, Pavón, Lenin, and Pérez-Tapia, Sonia Mayra

Subjects

SEQUENCE analysis, LEUCOCYTES, VAGUS nerve, UBIQUITIN, MASS spectrometry

Abstract

"Transferon Oral" is a peptide-derived product with immunomodulatory properties obtained from the lysis and dialysis of human buffy coat. Its active pharmaceutical ingredient, generically known as Dialyzable Leucocyte Extract, is a mixture of peptide populations with reproducible proportions among batches. "Transferon Oral" modulates IFN-γ, TNF-α, and IL-6 and increases the survival rate in a herpes infection murine model when oropharyngeally (ORO) administered, which correlate with clinical observations where "Transferon Oral" is used as a therapeutic auxiliary in inflammatory diseases. Notwithstanding, how a peptide-derived product elicits systemic modulation of cytokines when ORO administered remains unclear. To shed light on the pharmacology of "Transferon Oral" its peptide components must be known. Ten "Transferon Oral" batches were sequenced by mass spectrometry and the intact peptides were identified. The most abundant peptides were the monomeric human Ubiquitin (Ub), a globular low-molecular mass protein, and an Ub variant which lacks the two-terminal Gly (Ub-GG). Recombinant Ub prevented murine death when ORO administered in a herpes infection murine model. Besides, the percentage of survival increased in groups treated with Transferon Oral+Ub and decreased in groups treated with Ub-depleted "Transferon Oral" respect to the group treated with "Transferon Oral" only. Our findings indicate that the biological properties of "Transferon Oral" are partially associated to the Ub content. They suggest that Ub may activate its extracellular receptor (CXCR-4) in the stomach eliciting systemic immunomodulatory effects via vagus nerve. This is the first report that identifies an active component of "Transferon Oral" with the potential for the development of oral peptide immunomodulators. [ABSTRACT FROM AUTHOR]

Published

2020