Glycosphingolipids(gangliosides)have been characterized as important biological molecules with a key role as regulators in many physiological processes on cellular,tissue,organ,and organism levels.The deviations in th...Glycosphingolipids(gangliosides)have been characterized as important biological molecules with a key role as regulators in many physiological processes on cellular,tissue,organ,and organism levels.The deviations in their normal amounts,production,and metabolism are very often related to the development of many multi-factor socially important diseases.GM3 ganglioside,as a small molecule,plays important roles in the cascade regulatory pathways in the pathology of many disorders like neurodegenerative diseases,autoimmune diseases,inflammation,diabetes,malignant transformation,and others.Ganglioside GM3 and its derivatives are membrane-bound glycosphingolipids composed of an oligosaccharide head structure containing one sialic acid residue.These molecules transduce signals involved in cell surface events,including the phosphorylation of transmembrane receptors.This ganglioside is the most widely distributed among tissues,and it serves as a precursor for most of the more complex ganglioside species.GM3 inhibits the function of fibroblast growth factor receptor,and cell growth is regulated by GM3-enriched microdomain.GM3 is thought to inhibit immunologic functions,such as the proliferation and production of cytokines by T cells.On the other hand,the anti-ganglioside antibodies(AGAs)are important in many acquired demyelinating immunemediated neuropathies,like Multiple sclerosis(MS),Guillain–Barrésyndrome(GBS)and its variation,Miller–Fisher syndrome(MFS)and could be suggested as important diagnostic and prognostic markers about the describe diseases and their etiology.We show that the complexes of anti-ganglioside antibodies to GM3(detected by ELISA)may be useful diagnostic and prognostic tool markers for autoimmune diseases,neurodegenerative disorders,malignancy,diabetes,and inflammation.Our pilot studies suggest increased serum IgG anti-GM3 antibodies titers in patients with secondary progressive MS(SPMS),throat cancer,elder people with diabetes(89–96 years),old Lewis rats(30–33 months),and in the serum of subjected on lead intoxication BALB/c mice treated by salinomycin.We observed no changes in the titers in healthy elder people(89–96 years),in 70-year-old woman on dialysis,in relapsing-remitting MS(RRMS)patients on long-term treatment with Glatiramer acetate,Laquinimod,and Interferons,as well as in 18–22 months old Wistar rats and subjected on lead intoxication BALB/c mice treated by monensin and dimercaptosuccinic acid(DMSA).Considerable decrease of serum GM3 in early MS correlate with early damage and severe destruction of the blood–brain barrier,which provides impetus to initiate early therapy.展开更多
A marked increase in the incidence of autoimmune diseases in the past half-a-century has been observed. MS (multiple sclerosis) is one of the most common chronic immune-mediated inflammatory diseases of the central ...A marked increase in the incidence of autoimmune diseases in the past half-a-century has been observed. MS (multiple sclerosis) is one of the most common chronic immune-mediated inflammatory diseases of the central nervous system in young adults which is characterized by inflammatory demyelination and neurodegeneration with unpredictable effects lasting for the rest of their lives. The aim of the MS treatment is to prevent the demyelination and the reduction of axonal loss. Drugs approved for use in MS which reduce the frequency of exacerbations or slow disability progression are referred as DMDs (disease-modifying drugs). Additional treatments of MS include: dietary supplementation, herbal medicine intake, vitamin D3 and vitamin B supplementation and relaxation techniques. However, little is known about the environmental factors that directly influence Th1 7 cells. Increased salt (sodium chloride) concentrations found locally under physiological conditions in vivo markedly boost the induction of murine and human Th 17 cells. Pathogenic IL-23-dependent Th 17 cells have been shown to be critical for the development of EAE (experimental autoimmune encephalomyelitis) along with some genetic risk factors.展开更多
文摘Glycosphingolipids(gangliosides)have been characterized as important biological molecules with a key role as regulators in many physiological processes on cellular,tissue,organ,and organism levels.The deviations in their normal amounts,production,and metabolism are very often related to the development of many multi-factor socially important diseases.GM3 ganglioside,as a small molecule,plays important roles in the cascade regulatory pathways in the pathology of many disorders like neurodegenerative diseases,autoimmune diseases,inflammation,diabetes,malignant transformation,and others.Ganglioside GM3 and its derivatives are membrane-bound glycosphingolipids composed of an oligosaccharide head structure containing one sialic acid residue.These molecules transduce signals involved in cell surface events,including the phosphorylation of transmembrane receptors.This ganglioside is the most widely distributed among tissues,and it serves as a precursor for most of the more complex ganglioside species.GM3 inhibits the function of fibroblast growth factor receptor,and cell growth is regulated by GM3-enriched microdomain.GM3 is thought to inhibit immunologic functions,such as the proliferation and production of cytokines by T cells.On the other hand,the anti-ganglioside antibodies(AGAs)are important in many acquired demyelinating immunemediated neuropathies,like Multiple sclerosis(MS),Guillain–Barrésyndrome(GBS)and its variation,Miller–Fisher syndrome(MFS)and could be suggested as important diagnostic and prognostic markers about the describe diseases and their etiology.We show that the complexes of anti-ganglioside antibodies to GM3(detected by ELISA)may be useful diagnostic and prognostic tool markers for autoimmune diseases,neurodegenerative disorders,malignancy,diabetes,and inflammation.Our pilot studies suggest increased serum IgG anti-GM3 antibodies titers in patients with secondary progressive MS(SPMS),throat cancer,elder people with diabetes(89–96 years),old Lewis rats(30–33 months),and in the serum of subjected on lead intoxication BALB/c mice treated by salinomycin.We observed no changes in the titers in healthy elder people(89–96 years),in 70-year-old woman on dialysis,in relapsing-remitting MS(RRMS)patients on long-term treatment with Glatiramer acetate,Laquinimod,and Interferons,as well as in 18–22 months old Wistar rats and subjected on lead intoxication BALB/c mice treated by monensin and dimercaptosuccinic acid(DMSA).Considerable decrease of serum GM3 in early MS correlate with early damage and severe destruction of the blood–brain barrier,which provides impetus to initiate early therapy.
文摘A marked increase in the incidence of autoimmune diseases in the past half-a-century has been observed. MS (multiple sclerosis) is one of the most common chronic immune-mediated inflammatory diseases of the central nervous system in young adults which is characterized by inflammatory demyelination and neurodegeneration with unpredictable effects lasting for the rest of their lives. The aim of the MS treatment is to prevent the demyelination and the reduction of axonal loss. Drugs approved for use in MS which reduce the frequency of exacerbations or slow disability progression are referred as DMDs (disease-modifying drugs). Additional treatments of MS include: dietary supplementation, herbal medicine intake, vitamin D3 and vitamin B supplementation and relaxation techniques. However, little is known about the environmental factors that directly influence Th1 7 cells. Increased salt (sodium chloride) concentrations found locally under physiological conditions in vivo markedly boost the induction of murine and human Th 17 cells. Pathogenic IL-23-dependent Th 17 cells have been shown to be critical for the development of EAE (experimental autoimmune encephalomyelitis) along with some genetic risk factors.
