Resumen de Sodium transport systems in human chondrocytes I. Morphological and functional expression of the Na+,K+-ATPase a and β subunit isoforms in healthy and arthritic chondrocytes

E. Trujillo, Diego Álvarez de la Rosa Rodríguez, A. Mobasheri, J. Ávila, T. González, Pablo Martín Vasallo

• The chondrocyte is the cell responsible for the maintenance of the articular cartilage matrix. The negative charges of proteoglycans of the matrix draw cations, principally Na+, into the matrix to balance the negative charge distribution. The Na+,Kf -ATPase is the plasma membrane enzyme that maintains the intracellular Na+ and K+ concentrations. The enzyme is composed of an a and a l3 subunit, so far, 4 a and 3 B isoforms have been identified in mammals. Chondrocytes are sensitive to their ionic and osmotic environment and are capable of adaptive responses to ionic environmental perturbations particularly changes to extracellular [Na+]. In this article we show that human fetal and adult chondrocytes express three a ( a l , a 2 and the neural form of a3) and the three l3 isoforms (131, l32 and 83) of the Na+,K+-ATPase. The presence of multiple Na+,K+-ATPase isoforms in the plasma membrane of chondrocytes suggests a variety of kinetic properties that reflects a cartilage specific and very fine specialization in order to maintain the Na+/K+ gradients. Changes in the ionic and osmotic environment of chondrocytes occur in osteoarthritis and rheumatoid arthritis as result of tissue hydration and proteoglycan loss leading to a fall in tissue Na+ and K+ content. Although the expression levels and cellular distribution of the proteins tested do not vary, we detect changes in p-nitrophenylphosphatase activity "in situ" between control and pathological samples. This change in the sodium pump enzymatic activity suggests that the chondrocyte responds to these cationic environmental changes with a variation of the active isozyme types present in the plasma membrane.