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Autoimmune Disease Related Molecular and Cellular Mechanisms | 94647

International Journal of Collaborative Research on Internal Medicine & Public Health

ISSN - 1840-4529

Abstract

Autoimmune Disease Related Molecular and Cellular Mechanisms

Robert Wellington*

Several autoimmune illnesses are becoming more common in the United States, according to evidence. As a result, the expense of clinical management of autoimmune disorders to the public health is increasing. Both genetic and environmental variables play a role in the onset and course of autoimmune disorders. Autoantibodies can be caused by deficiencies in key proteins that are normally involved in maintaining the internal environment's checks and balances. Autoimmunity has been linked to structural anomalies or a decrease in normal levels of the pentraxins (serum amylase P protein, acute phase proteins, complement, and C-reactive proteins). The quality and amount of subsequent immune responses are determined by the type of ligand/receptor interactions that promote physical recruitment of various signals within the cell. CD95, also known as Fas/Apo-1, and its ligand CD95L regulate lymphocyte populations, influencing different aspects of immune responses. Mutations in the apoptotic pathways may occur from aberrant protein

synthesis by CD95 and/or its receptor CD95L. Apoptosis can be prevented fully, triggered partially, or partially stimulated. Apoptosis modulation may result in the buildup of selfantigens. Through lymphatic hyperplasia, the immune system may be prompted to react to self-molecules. Proliferative diseases and increased vulnerability to autoimmune syndromes may result from this process. The mechanisms of auto immune pathogenesis at the cellular and molecular levels are discussed in this research. The importance of T and B cell receptor/ligand interactions, functions, and malfunctions as a result of structural and quantitative changes in the T-B-cell cluster of antigen determinants is highlighted. The etiological factors implicated in the initiation and subsequent dissemination of autoimmune disorders is reviewed in genetically sensitive patients who acquire spontaneous autoimmune diseases.

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