Activation of skeletal muscle FAPs by LPA requires the Hippo signaling via the FAK pathway

Meilyn Cruz-Soca; Jennifer Faundez-Contreras; Adriana Córdova-Casanova; Felipe S Gallardo; Alexia Bock-Pereda; Jerold Chun; Juan Carlos Casar; Enrique Brandan

doi:10.1016/j.matbio.2023.03.010

Activation of skeletal muscle FAPs by LPA requires the Hippo signaling via the FAK pathway

Matrix Biol. 2023 May:119:57-81. doi: 10.1016/j.matbio.2023.03.010. Epub 2023 Apr 3.

Authors

Meilyn Cruz-Soca¹, Jennifer Faundez-Contreras¹, Adriana Córdova-Casanova¹, Felipe S Gallardo¹, Alexia Bock-Pereda¹, Jerold Chun², Juan Carlos Casar³, Enrique Brandan⁴

Affiliations

¹ Facultad de Ciencias Biológicas, Centro de Envejecimiento y Regeneración (CARE), Pontificia Universidad Católica de Chile, Santiago 8330025, Chile; Centro Científico y Tecnológico de Excelencia Ciencia & Vida, Santiago, Chile.
² Sanford Burnham Prebys Medical Discovery Institute, La Jolla, CA, United States.
³ Departamento de Neurología, Pontificia Universidad Católica de Chile, Santiago, Chile.
⁴ Facultad de Ciencias Biológicas, Centro de Envejecimiento y Regeneración (CARE), Pontificia Universidad Católica de Chile, Santiago 8330025, Chile; Centro Científico y Tecnológico de Excelencia Ciencia & Vida, Santiago, Chile; Facultad de Medicina y Ciencia, Universidad San Sebastián, Santiago, Chile. Electronic address: ebrandan@cienciavida.org.

PMID: 37137584
DOI: 10.1016/j.matbio.2023.03.010

Abstract

Lysophosphatidic acid (LPA) is a lysophospholipid that signals through six G-protein coupled receptors (LPARs), LPA₁ to LPA₆. LPA has been described as a potent modulator of fibrosis in different pathologies. In skeletal muscle, LPA increases fibrosis-related proteins and the number of fibro/adipogenic progenitors (FAPs). FAPs are the primary source of ECM-secreting myofibroblasts in acute and chronic damage. However, the effect of LPA on FAPs activation in vitro has not been explored. This study aimed to investigate FAPs' response to LPA and the downstream signaling mediators involved. Here, we demonstrated that LPA mediates FAPs activation by increasing their proliferation, expression of myofibroblasts markers, and upregulation of fibrosis-related proteins. Pretreatment with the LPA₁/LPA₃ antagonist Ki16425 or genetic deletion of LPA₁ attenuated the LPA-induced FAPs activation, resulting in decreased expression of cyclin e1, α-SMA, and fibronectin. We also evaluated the activation of the focal adhesion kinase (FAK) in response to LPA. Our results showed that LPA induces FAK phosphorylation in FAPs. Treatment with the P-FAK inhibitor PF-228 partially prevented the induction of cell responses involved in FAPs activation, suggesting that this pathway mediates LPA signaling. FAK activation controls downstream cell signaling within the cytoplasm, such as the Hippo pathway. LPA induced the dephosphorylation of the transcriptional coactivator YAP (Yes-associated protein) and promoted direct expression of target pathway genes such as Ctgf/Ccn2 and Ccn1. The blockage of YAP transcriptional activity with Super-TDU further confirmed the role of YAP in LPA-induced FAPs activation. Finally, we demonstrated that FAK is required for LPA-dependent YAP dephosphorylation and the induction of Hippo pathway target genes. In conclusion, LPA signals through LPA₁ to regulate FAPs activation by activating FAK to control the Hippo pathway.

Keywords: Fibro/adipogenic progenitors; Fibrosis; LPARs; Lysophosphatidic acid; Myofibroblasts.

Publication types

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

MeSH terms

Fibrosis
Focal Adhesion Protein-Tyrosine Kinases / metabolism
Hippo Signaling Pathway*
Humans
Lysophospholipids* / metabolism
Lysophospholipids* / pharmacology
Muscle, Skeletal / metabolism

Substances

lysophosphatidic acid
Focal Adhesion Protein-Tyrosine Kinases
Lysophospholipids