Abstract
Vascular endothelial cells (ECs) play central roles in physiologically important functions of blood vessels and contribute to the maintenance of vascular integrity. Therefore, it is considered that the impairment of EC functions leads to the development of vascular diseases. However, the molecular mechanisms of the EC dysfunctions that accompany senescence and aging have not yet been clarified. The carbohydrate antigens carried by glycoconjugates (e.g. glycoproteins, glycosphingolipids, and proteoglycans) mainly present on the cell surface serve not only as marker molecules but also as functional molecules. In this study, we have investigated the abundance and functional roles of glycosphingolipids in human ECs during senescence and aging. Among glycosphingolipids, ganglioside GM1 was highly expressed in abundance on the surface of replicatively and prematurely senescent ECs and also of ECs derived from an elderly subject. Insulin signaling, which regulates important functions of ECs, is impaired in senescent and aged ECs. Actually, by down-regulating GM1 on senescent ECs and overloading exogenous GM1 onto non-senescent ECs, we showed that an increased abundance of GM1 functionally contributes to the impairment of insulin signaling in ECs. Taken together, these findings provide the first evidence that GM1 increases in abundance on the cell surface of ECs under the conditions of cellular senescence and aging and causes insulin resistance in ECs. GM1 may be an attractive target for the detection, prevention, and therapy of insulin resistance and related vascular diseases, particularly in older people.
Highlights
The roles of gangliosides in senescent endothelial cells (ECs) were unknown
We revealed for the first time that monosialotetrahexosylganglioside (GM1) among the several gangliosides species was increased in abundance on the cell surface of ECs with cellular senescence and aging and that the increased abundance of GM1 resulted in a state of insulin resistance in senescent ECs
Ganglioside GM1 Is Increased in Abundance on Senescent ECs—It is well known that the amount and composition of gangliosides in the cell membrane can change depending on the cellular condition, such as the developmental and pathological state [9]
Summary
The roles of gangliosides in senescent endothelial cells (ECs) were unknown. Results: Ganglioside GM1 increased on senescent and aged ECs. It has been speculated that senescence and aging produce insulin resistance in ECs, but until now, the molecular mechanisms of the insulin resistance that occurs with senescence and aging have been unclear To investigate these mechanisms, we focused on glycosphingolipids (GSLs). We focused on gangliosides of ECs, and we hypothesized that changes in the abundance of cell surface gangliosides with senescence and aging contribute to EC dysfunctions such as insulin resistance. We revealed for the first time that monosialotetrahexosylganglioside (GM1) among the several gangliosides species was increased in abundance on the cell surface of ECs with cellular senescence (replicative and premature) and aging and that the increased abundance of GM1 resulted in a state of insulin resistance in senescent ECs
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