The Relevance of Thimet Oligopeptidase in the Regulation of Energy Metabolism and Diet-Induced Obesity

Mayara C F Gewehr; Alexandre A S Teixeira; Bruna A C Santos; Luana A Biondo; Fábio C Gozzo; Amanda M Cordibello; Rosangela A S Eichler; Patrícia Reckziegel; Renée N.O. Da Silva; Nilton B Dos Santos; Niels O S Camara; Angela Castoldi; Maria L M Barreto-Chaves; Camila S Dale; Nathalia Senger; Joanna D C C Lima; Marilia C L Seelaender; Aline C Inada; Eliana H Akamine; Leandro M Castro; Alice C Rodrigues; José C Rosa Neto; Emer S Ferro

doi:10.3390/biom10020321

The Relevance of Thimet Oligopeptidase in the Regulation of Energy Metabolism and Diet-Induced Obesity

Biomolecules. 2020 Feb 17;10(2):321. doi: 10.3390/biom10020321.

Authors

Mayara C F Gewehr¹, Alexandre A S Teixeira², Bruna A C Santos¹, Luana A Biondo², Fábio C Gozzo³, Amanda M Cordibello³, Rosangela A S Eichler¹, Patrícia Reckziegel⁴, Renée N.O. Da Silva¹, Nilton B Dos Santos¹, Niels O S Camara⁵, Angela Castoldi⁵, Maria L M Barreto-Chaves⁶, Camila S Dale⁶, Nathalia Senger⁶, Joanna D C C Lima², Marilia C L Seelaender², Aline C Inada¹, Eliana H Akamine¹, Leandro M Castro⁷, Alice C Rodrigues¹, José C Rosa Neto², Emer S Ferro¹

Affiliations

¹ Department of Pharmacology, Biomedical Sciences Institute, University of São Paulo, 05508-900 São Paulo, SP, Brazil.
² Department of Cell Biology and Development, Biomedical Sciences Institute, University of São Paulo, 05508-900 São Paulo, SP, Brazil.
³ Institute of Chemistry, State University of Campinas, 13083-862 Campinas, SP, Brazil.
⁴ Department of Pharmacology, Federal University of São Paulo, 04023-062 São Paulo, SP, Brazil.
⁵ Department of Immunology, Biomedical Sciences Institute, University of São Paulo, 05508-900 São Paulo, SP, Brazil.
⁶ Department of Anatomy, Biomedical Sciences Institute, University of São Paulo, 05508-900 São Paulo, SP, Brazil.
⁷ Biosciences Institute, São Paulo State University, 11330-900 São Vicente, SP, Brazil.

Abstract

Thimet oligopeptidase (EC 3.4.24.15; EP24.15; THOP1) is a potential therapeutic target, as it plays key biological functions in processing biologically functional peptides. The structural conformation of THOP1 provides a unique restriction regarding substrate size, in that it only hydrolyzes peptides (optimally, those ranging from eight to 12 amino acids) and not proteins. The proteasome activity of hydrolyzing proteins releases a large number of intracellular peptides, providing THOP1 substrates within cells. The present study aimed to investigate the possible function of THOP1 in the development of diet-induced obesity (DIO) and insulin resistance by utilizing a murine model of hyperlipidic DIO with both C57BL6 wild-type (WT) and THOP1 null (THOP1^-/-) mice. After 24 weeks of being fed a hyperlipidic diet (HD), THOP1^-/- and WT mice ingested similar chow and calories; however, the THOP1^-/- mice gained 75% less body weight and showed neither insulin resistance nor non-alcoholic fatty liver steatosis when compared to WT mice. THOP1^-/- mice had increased adrenergic-stimulated adipose tissue lipolysis as well as a balanced level of expression of genes and microRNAs associated with energy metabolism, adipogenesis, or inflammation. Altogether, these differences converge to a healthy phenotype of THOP1^-/- fed a HD. The molecular mechanism that links THOP1 to energy metabolism is suggested herein to involve intracellular peptides, of which the relative levels were identified to change in the adipose tissue of WT and THOP1^-/- mice. Intracellular peptides were observed by molecular modeling to interact with both pre-miR-143 and pre-miR-222, suggesting a possible novel regulatory mechanism for gene expression. Therefore, we successfully demonstrated the previously unanticipated relevance of THOP1 in energy metabolism regulation. It was suggested that intracellular peptides were responsible for mediating the phenotypic differences that are described herein by a yet unknown mechanism of action.

Keywords: diet-induced obesity; insulin resistance; mass spectrometry; obesity; peptidases; peptidome; proteases; proteasome.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Adipogenesis
Adipose Tissue / metabolism
Animals
Diet, High-Fat / adverse effects
Energy Metabolism*
Female
Gene Deletion
Insulin Resistance
Lipolysis
Male
Metalloendopeptidases / genetics
Metalloendopeptidases / metabolism*
Mice
Mice, Inbred C57BL
Obesity / etiology
Obesity / genetics
Obesity / metabolism*

Substances

Metalloendopeptidases
thimet oligopeptidase

Abstract

Publication types

MeSH terms

Substances

Grants and funding