Some new aspects of molecular mechanisms of cyclosporin A effect on immune response. NLM AIDSLINE Important note: Information in this article was accurate in 1996. The state of the art may have changed since the publication date.

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Some new aspects of molecular mechanisms of cyclosporin A effect on immune response.

APMIS. 1995 Jun;103(6):401-15. Unique Identifier : AIDSLINE MED/96028031
Zav'yalov VP; Denesyuk AI; Lundell J; Korpela T; Institute of Immunology, Lyubuchany, Moscow Region, Russia.

Abstract: A few protein targets were found to display a specific high-affinity interaction with the immunosuppressant cyclosporin A (CsA): cytosolic cyclophilins (CyP)A, B, C, D, E containing from 122 to 174 amino acid residues in a polypeptide chain, and secreted forms of CyP; CyP-40, 40-kDa CsA-binding polypeptide complexed with steroid receptor (SR); CyP-related 150-kDa receptor of natural killer (NK) cells; interleukin 8 (IL-8); actin; a family of molecular chaperones hsp70 and P-glycoprotein (P-GP). All CyPs possess peptidyl-prolyl cis-trans isomerase activity (PPIase) and may serve as ATP-independent molecular chaperone proteins. The CsA-CyP complexes are specific inhibitors of Ca(2+)-and calmodulin-dependent protein phosphatase calcineurin (CaN). The inhibition of CaN blocks the activation of genes of IL-2, IL-2R, IL-4, etc. in T cells. In addition, immunosuppressive and/or antiinflammatory activity of CsA can be executed via CyP-40 and hsp 70 complexed with SR, and following the interaction with CyP-related receptor of NK and with IL-8. CsA binding to CyPC, P-GP and actin may throw light on the biochemical events leading to nephrotoxicity and graft vessel disease, two major side effects produced by CsA. The discovery of the interaction of human immunodeficiency virus type 1 (HIV-1) Gag protein with CyP and effective disruption of this interaction by CsA may be important for our understanding of the pathology caused by this immunosuppressive virus and will inspire therapeutic strategies to nip HIV in the bud. Bacterial immunophilins (ImPs) contribute to the virulence of pathogenic microorganisms. Elucidation of molecular mechanisms of microbial ImPs' action in the pathogenesis of bacterial infections may lead to new strategies for designing antibacterial drugs.
Keywords: Actins/METABOLISM Calmodulin-Binding Proteins/METABOLISM Carrier Proteins/METABOLISM Cyclosporine/*METABOLISM/PHARMACOLOGY DNA-Binding Proteins/METABOLISM Heat-Shock Proteins/METABOLISM Heat-Shock Proteins 70/METABOLISM Human Immunity/*DRUG EFFECTS Immunosuppressive Agents/*PHARMACOLOGY Interleukin-8/METABOLISM P-Glycoprotein/METABOLISM Phosphoprotein Phosphatase/METABOLISM JOURNAL ARTICLE REVIEW REVIEW, TUTORIAL

KWDactins/metabolismcalmodulin-bindingproteins/metabolismcarrierproteins/metabolismcyclosporine/KWDmetabolism/pharmacologydna-bindingproteins/metabolismheat-shockproteins/metabolismheat-shockproteins70/metabolismhumanimmunity/KWDdrugeffectsimmunosuppressiveagents/KWDpharmacologyinterleukin-8/metabolismp-glycoprotein/metabolismphosphoproteinphosphatase/metabolismjournalarticlereviewreview,tutorial
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M9610764

Copyright © 1996 - National Library of Medicine. Reproduced under license with the National Library of Medicine, Bethesda, MD.

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