The clinical and molecular cardiometabolic fingerprint of an exploratory psoriatic arthritis cohort is associated with the disease activity and differentially modulated by methotrexate and apremilast

Arias de la Rosa, Iván; López-Montilla, María Dolores; Román-Rodríguez, Cristobal; Pérez Sánchez, Carlos; Gómez-García, Ignacio; López Medina, Eloísa Clementina; Ladehesa-Pineda, Lourdes; Ábalos-Aguilera, María del Carmen; Ruiz, Desireé; Patiño-Trives, Alejandra Mª; Luque-Tévar, María; Añón-Oñate, Isabel; Pérez-Galán, María José; Guzmán Ruiz, R.; Malagón, María M.; López-Pedrera, Ch.; Escudero Contreras, Alejandro; Collantes Estévez, Eduardo; Barbarroja, Nuria

View/Open

the_clinical_and_molecular_cardiometabolic_fingerprin.pdf (2.521Mb)

Author

Arias de la Rosa, Iván

López-Montilla, María Dolores

Román-Rodríguez, Cristobal

Pérez Sánchez, Carlos

Gómez-García, Ignacio

López Medina, Eloísa Clementina

Ladehesa-Pineda, Lourdes

Ábalos-Aguilera, María del Carmen

Ruiz, Desireé

Patiño-Trives, Alejandra Mª

Luque-Tévar, María

Añón-Oñate, Isabel

Pérez-Galán, María José

Guzmán Ruiz, R.

Malagón, María M.

López-Pedrera, Ch.

Escudero Contreras, Alejandro

Collantes Estévez, Eduardo

Barbarroja, Nuria

Publisher

Wiley

Date

2022

Subject

Apremilast
Cardiometabolic profile
Cardiovascular risk
Insulin resistance
Methotrexate
Obesity and disease activity
Psoriatic arthritis

Abstract

Objectives: (1) To evaluate clinical and molecular cardiovascular disease (CVD) signs and their relationship with psoriatic arthritis (PsA) features and (2) to identify a clinical patient profile susceptible to benefit from methotrexate (MTX) and/or apremilast regarding CVD risk. Methods: This cross-sectional study included 100 patients with PsA and 100 age-matched healthy donors. In addition, an exploratory cohort of 45 biologically naïve patients treated for 6 months with apremilast, MTX or combined therapy according to routine clinical practice was recruited. Extensive clinical and metabolic profiles were obtained. Ninety-nine surrogate CVD-related molecules were analysed in plasma and peripheral blood mononuclear cells (PBMCs). Hard cluster analysis was performed to identify the clinical and molecular phenotypes. Mechanistic studies were performed on adipocytes. Results: Cardiometabolic comorbidities were associated with disease activity and long-term inflammatory status. Thirty-five CVD-related proteins were altered in the plasma and PBMCs of PsA patients and were associated with the key clinical features of the disease. Plasma levels of some of the CVD-related molecules might distinguish insulin-resistant patients (MMP-3, CD163, FABP-4), high disease activity (GAL-3 and FABP-4) and poor therapy outcomes (CD-163, LTBR and CNTN-1). Hard cluster analysis identified two phenotypes of patients according to the rates of cardiometabolic comorbidities with distinctive clinical and molecular responses to each treatment. Conclusions: (1) Novel CVD-related proteins associated with clinical features could be emerging therapeutic targets in the context of PsA and (2) the pleiotropic action of apremilast could make it an excellent choice for the management of PsA patients with high CVD risk, targeting metabolic alterations and CVD-related molecules.

URI

http://hdl.handle.net/10396/22939

Fuente

Journal of Internal Medicine 291, 676-693 (2022)

Versión del Editor

https://doi.org/10.1111/joim.13447