Nemat Khansari scite author profile

Chronic inflammation is a pathological condition characterized by continued active inflammation response and tissue destruction. Many of the immune cells including macrophages, neutrophils and eosinophils are involved directly or by production of inflammatory cytokine production in pathology of chronic inflammation. From literatures, it is appear that there is a general concept that chronic inflammation can be a major cause of cancers and express aging processes. Moreover, many studies suggest that chronic inflammation could have serious role in wide variety of age-related diseases including diabetes, cardiovascular and autoimmune diseases. Inflammatory process induces oxidative stress and reduces cellular antioxidant capacity. Overproduced free radicals react with cell membrane fatty acids and proteins impairing their function permanently. In addition, free radicals can lead to mutation and DNA damage that can be a predisposing factor for cancer and age-related disorders. This article reviews the antioxidant defense systems, free radicals production and their role in cancer and age related diseases and also some of the recent patent relevant to the field. Study of the role of free radicals in human diseases can help the investigators to consider the antioxidants as proper agents in preventive medicine, especially for cancer and aging processes.

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Post Challenging Serum Cytokine Profile (Th1 & Th2) in the Vaccinated Mice (Balb/C) With a New Formulation of Leishmania major Antigen

Latifynia¹,

Khamisipour²,

Gharagozlou³

et al. 2014

TurkiyeParazitolDerg

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Phagocytosis of senescent erythrocytes by autologous monocytes: Requirement of membrane-specific autologous IgG for immune elimination of aging red blood cells

Khansari

Fudenberg

1983

Cellular Immunology

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Mechanisms for the removal of senescent human erythrocytes from circulation: Specificity of the membrane-bound immunoglobulin G

Khansari¹,

Springer²,

Merler³

et al. 1983

Mechanisms of Ageing and Development

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Human monocyte heterogeneity: Interleukin 1 and prostaglandin E₂ production by separate subsets

1985

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Human peripheral blood monocytes were separated into four different subpopulations by means of a discontinuous bovine serum albumin gradient. Of the least dense population, 7% were present in fraction A, 11% in fraction B, 28% in fraction C and of the most dense, 34% were in fraction D. The rest (17%) of the recovered cells sedimented as a pellet, of which 95% were dead. The monocytes of fraction D (= greater than or equal to 1.075 kg/l) were major interleukin 1 (IL 1) producers and their presence enhanced immunoglobulin synthesis in vitro. Fraction C (= greater than or equal to 1.070 kg/l) were the major prostaglandin E2 (PGE2) producers and demonstrated suppressor activity on in vitro IgG and IgM synthesis. Fractions A and B had minimal production of either IL 1 or PGE2 and lesser effects on the IgG and IgM synthesis. These data demonstrate functional heterogeneity of peripheral blood monocytes with respect to production of both IL 1 and PGE2 as well as accessory cells for immunoglobulin synthesis.

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Nemat Khansari

Chronic Inflammation and Oxidative Stress as a Major Cause of Age- Related Diseases and Cancer

Post Challenging Serum Cytokine Profile (Th1 & Th2) in the Vaccinated Mice (Balb/C) With a New Formulation of Leishmania major Antigen

Phagocytosis of senescent erythrocytes by autologous monocytes: Requirement of membrane-specific autologous IgG for immune elimination of aging red blood cells

Mechanisms for the removal of senescent human erythrocytes from circulation: Specificity of the membrane-bound immunoglobulin G

Human monocyte heterogeneity: Interleukin 1 and prostaglandin E₂ production by separate subsets

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Resources

About

Nemat Khansari

Chronic Inflammation and Oxidative Stress as a Major Cause of Age- Related Diseases and Cancer

Post Challenging Serum Cytokine Profile (Th1 & Th2) in the Vaccinated Mice (Balb/C) With a New Formulation of Leishmania major Antigen

Phagocytosis of senescent erythrocytes by autologous monocytes: Requirement of membrane-specific autologous IgG for immune elimination of aging red blood cells

Mechanisms for the removal of senescent human erythrocytes from circulation: Specificity of the membrane-bound immunoglobulin G

Human monocyte heterogeneity: Interleukin 1 and prostaglandin E2 production by separate subsets

Contact Info

Product

Resources

About

Human monocyte heterogeneity: Interleukin 1 and prostaglandin E₂ production by separate subsets