LOXL2-A New Target in Antifibrogenic Therapy?

Angela Puente; Jose Ignacio Fortea; Joaquin Cabezas; Maria Teresa Arias Loste; Paula Iruzubieta; Susana Llerena; Patricia Huelin; Emilio Fábrega; Javier Crespo

doi:10.3390/ijms20071634

LOXL2-A New Target in Antifibrogenic Therapy?

Int J Mol Sci. 2019 Apr 2;20(7):1634. doi: 10.3390/ijms20071634.

Authors

Angela Puente^{1

2}, Jose Ignacio Fortea^{3

4}, Joaquin Cabezas^{5

6}, Maria Teresa Arias Loste^{7

8}, Paula Iruzubieta^{9

10}, Susana Llerena^{11

12}, Patricia Huelin^{13

14}, Emilio Fábrega^{15

16}, Javier Crespo^{17

18}

Affiliations

¹ Digestive Disease Department, Marqués de Valdecilla University Hospital, Cantabria University, 39008 Santander, Spain. anpuente@humv.es.
² Health Research Institute Marques de Valdecilla (IDIVAL), 39008 Santander, Spain. anpuente@humv.es.
³ Digestive Disease Department, Marqués de Valdecilla University Hospital, Cantabria University, 39008 Santander, Spain. joseignacio.fortea@scsalud.es.
⁴ Health Research Institute Marques de Valdecilla (IDIVAL), 39008 Santander, Spain. joseignacio.fortea@scsalud.es.
⁵ Digestive Disease Department, Marqués de Valdecilla University Hospital, Cantabria University, 39008 Santander, Spain. joaquin.cabezas@scsalud.es.
⁶ Health Research Institute Marques de Valdecilla (IDIVAL), 39008 Santander, Spain. joaquin.cabezas@scsalud.es.
⁷ Digestive Disease Department, Marqués de Valdecilla University Hospital, Cantabria University, 39008 Santander, Spain. mteresa.arias@scsalud.es.
⁸ Health Research Institute Marques de Valdecilla (IDIVAL), 39008 Santander, Spain. mteresa.arias@scsalud.es.
⁹ Digestive Disease Department, Marqués de Valdecilla University Hospital, Cantabria University, 39008 Santander, Spain. paula.iruzubieta@scsalud.es.
¹⁰ Health Research Institute Marques de Valdecilla (IDIVAL), 39008 Santander, Spain. paula.iruzubieta@scsalud.es.
¹¹ Digestive Disease Department, Marqués de Valdecilla University Hospital, Cantabria University, 39008 Santander, Spain. susana.llerena@scsalud.es.
¹² Health Research Institute Marques de Valdecilla (IDIVAL), 39008 Santander, Spain. susana.llerena@scsalud.es.
¹³ Digestive Disease Department, Marqués de Valdecilla University Hospital, Cantabria University, 39008 Santander, Spain. patricia.huelin@scsalud.es.
¹⁴ Health Research Institute Marques de Valdecilla (IDIVAL), 39008 Santander, Spain. patricia.huelin@scsalud.es.
¹⁵ Digestive Disease Department, Marqués de Valdecilla University Hospital, Cantabria University, 39008 Santander, Spain. emilio.fabrega@scsalud.es.
¹⁶ Health Research Institute Marques de Valdecilla (IDIVAL), 39008 Santander, Spain. emilio.fabrega@scsalud.es.
¹⁷ Digestive Disease Department, Marqués de Valdecilla University Hospital, Cantabria University, 39008 Santander, Spain. javier.crespo@scsalud.es.
¹⁸ Health Research Institute Marques de Valdecilla (IDIVAL), 39008 Santander, Spain. javier.crespo@scsalud.es.

Abstract

The concept of liver fibrosis and cirrhosis being static and therefore irreversible is outdated. Indeed, both human and animal studies have shown that fibrogenesis is a dynamic and potentially reversible process that can be modulated either by stopping its progression and/or by promoting its resolution. Therefore, the study of the molecular mechanisms involved in the pathogenesis of liver fibrosis is critical for the development of future antifibrotic therapies. The fibrogenesis process, common to all forms of liver injury, is characterized by the increased deposition of extracellular matrix components (EMCs), including collagen, proteoglycans, and glycoproteins (laminin and fibronectin 2). These changes in the composition of the extracellular matrix components alter their interaction with cell adhesion molecules, influencing the modulation of cell functions (growth, migration, and gene expression). Hepatic stellate cells and Kupffer cells (liver macrophages) are the key fibrogenic effectors. The antifibrogenic mechanism starts with the activation of Ly6C^high macrophages, which can differentiate into macrophages with antifibrogenic action. The research of biochemical changes affecting fibrosis irreversibility has identified lysyl oxidase-like 2 (LOXL2), an enzyme that promotes the network of collagen fibers of the extracellular matrix. LOXL2 inhibition can decrease cell numbers, proliferation, colony formations, and cell growth, and it can induce cell cycle arrest and increase apoptosis. The development of a new humanized IgG4 monoclonal antibody against LOXL2 could open the window of a new antifibrogenic treatment. The current therapeutic target in patients with liver cirrhosis should focus (after the eradication of the causal agent) on the development of new antifibrogenic drugs. The development of these drugs must meet three premises: Patient safety, in non-cirrhotic phases, down-staging or at least stabilization and slowing the progression to cirrhosis must be achieved; whereas in the cirrhotic stage, the objective should be to reduce fibrosis and portal pressure.

Keywords: LOXL2; fibrosis; hepatic stellate cells; portal hypertension; regression cirrhosis.

Publication types

Review

MeSH terms

Animals
Humans
Liver Cirrhosis / drug therapy*
Models, Biological
Molecular Targeted Therapy*
Protein-Lysine 6-Oxidase / antagonists & inhibitors*
Protein-Lysine 6-Oxidase / metabolism

Substances

Protein-Lysine 6-Oxidase