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Entry inhibitor

September 02, 2023

Entry inhibitors, also known as fusion inhibitors, are a class of antiviral drugs that prevent a virus from entering a cell, for example, by blocking a receptor. Entry inhibitors are used to treat conditions such as HIV and hepatitis D.

HIV entry Edit

 
An illustration of HIV entry mechanism and mechanisms of action (MOA) of two entry inhibitor, 5-Helix and C37.
 
An HIV virion binds to a CD4+ human cell. The two bottom pictures depict two proposed models of HIV fusion with the cell.

They are used in combination therapy for the treatment of HIV infection. This class of drugs interferes with the binding, fusion and entry of an HIV virion to a human cell. By blocking this step in HIV's replication cycle, such agents slow the progression from HIV infection to AIDS.[1]

Proteins Edit

There are several key proteins involved in the HIV entry process.[citation needed]

  • CD4, a protein receptor found on the surface of helper T cells in the human immune system, also called CD4+ T cells
  • gp120, a protein on HIV surface that binds to the CD4 receptor
  • CCR5, a second receptor found on the surface of CD4+ cells and macrophages, called a chemokine co-receptor
  • CXCR4, another chemokine co-receptor found on CD4+ cells
  • gp41, an HIV protein, closely associated with gp120, that penetrates the cell membrane

Binding, fusion, entry sequence Edit

HIV entry into a human cell requires the following steps in sequence.[2][3]

  1. The binding of HIV surface protein gp120 to the CD4 receptor
  2. A conformational change in gp120, which both increases its affinity for a co-receptor and exposes gp41
  3. The binding of gp120 to a co-receptor either CCR5 or CXCR4
  4. The penetration of the cell membrane by gp41, which approximates the membrane of HIV and the T cell and promotes their fusion
  5. The entry of the viral core into the cell

Entry inhibitors work by interfering with one aspect of this process.

Approved agents Edit

  • Maraviroc binds to CCR5, preventing an interaction with gp120. It is also referred to as a "chemokine receptor antagonist" or a "CCR5 inhibitor."[4]
  • Enfuvirtide binds to gp41 and interferes with its ability to approximate the two membranes. It is also referred to as a "fusion inhibitor."
  • Ibalizumab, a monoclonal antibody that binds to domain 2 of CD4 and interferes with post-attachment steps required for the entry of HIV-1 virus particles into host cells and prevents the viral transmission that occurs via cell-cell fusion.
  • Fostemsavir, an attachment inhibitor that interferes with the interaction of CD4 and gp120 by binding with gp120.

Investigational agents Edit

Other agents are under investigation for their ability to interact with the proteins involved in HIV entry and the possibility that they may serve as entry inhibitors.[5]

  • Leronlimab, a monoclonal antibody that binds CCR5
  • Plerixafor was being developed to interfere with interaction between HIV and CXCR4, but showed little useful antiviral activity in recent trials.
  • Epigallocatechin gallate, a substance found in green tea, appears to interact with gp120 as do several other theaflavins.[6]
  • Vicriviroc, similar to maraviroc, is currently undergoing clinical trials for FDA approval.
  • Aplaviroc, an agent similar to maraviroc and vicriroc. Clinical trials were halted in 2005 over concerns about the drug's safety.
  • b12 is an antibody against HIV found in some long-term nonprogressors. It has been found to bind to gp120 at the exact region, or epitope, where gp120 binds to CD4. b12 seems to serve as a natural entry inhibitor in some individuals. It is hoped that further study of b12 may lead to an effective HIV vaccine.
  • Griffithsin, a substance derived from algae, appears to have entry inhibitor properties.[7]
  • DCM205, is a small molecule based on L-chicoric acid, an integrase inhibitor. DCM205 has been reported to inactivate HIV-1 particles directly in vitro and is thought to act primarily as an entry inhibitor.[8]
  • CD4 specific Designed Ankyrin Repeat Proteins (DARPins) potently block viral entry of diverse strains and are being developed and studied as potential microbicide candidates [9]
  • A polyclonal caprine antibody is in phase II human clinical trials that targets, among others sites, the GP41 transmembrane glycoprotein. The trials are being conducted by Virionyx, a New Zealand Company.[10]
  • VIR-576 is a synthesized peptide which binds to gp41, preventing fusion of the virus with a cell membrane.
  • ITX5061 for hepatitis C.[11]

References Edit

  1. ^ Biswas P, Tambussi G, Lazzarin A (May 2007). "Access denied? The status of co-receptor inhibition to counter HIV entry". Expert Opinion on Pharmacotherapy. 8 (7): 923–33. doi:10.1517/14656566.8.7.923. PMID 17472538. S2CID 32675897.
  2. ^ Xiao, Tianshu; Cai, Yongfei; Chen, Bing (2021). "HIV-1 entry and membrane fusion inhibitors". Viruses. 13 (5): 735. doi:10.3390/v13050735. PMC 8146413. PMID 33922579.
  3. ^ Wilen, Craig B.; Tilton, John C.; Doms, Robert W. (2012). "HIV: cell binding and entry". Cold Spring Harb Perspect Med. 2 (8): a006866. doi:10.1101/cshperspect.a006866. PMC 3405824. PMID 22908191. Retrieved 2021-08-11.
  4. ^ Pugach P, Ketas TJ, Michael E, Moore JP (August 2008). "Neutralizing antibody and anti-retroviral drug sensitivities of HIV-1 isolates resistant to small molecule CCR5 inhibitors". Virology. 377 (2): 401–7. doi:10.1016/j.virol.2008.04.032. PMC 2528836. PMID 18519143.
  5. ^ Merck Manual.com Human Immunodeficiency Virus (HIV) Infection Table 4 [1]
  6. ^ Williamson MP, McCormick TG, Nance CL, Shearer WT (December 2006). "Epigallocatechin gallate, the main polyphenol in green tea, binds to the T-cell receptor, CD4: Potential for HIV-1 therapy". The Journal of Allergy and Clinical Immunology. 118 (6): 1369–74. doi:10.1016/j.jaci.2006.08.016. PMID 17157668.
  7. ^ Emau P, Tian B, O'keefe BR, Mori T, McMahon JB, Palmer KE, et al. (August 2007). "Griffithsin, a potent HIV entry inhibitor, is an excellent candidate for anti-HIV microbicide". Journal of Medical Primatology. 36 (4–5): 244–53. doi:10.1111/j.1600-0684.2007.00242.x. PMID 17669213. S2CID 22539115.
  8. ^ Duong YT, Meadows DC, Srivastava IK, Gervay-Hague J, North TW (May 2007). "Direct inactivation of human immunodeficiency virus type 1 by a novel small-molecule entry inhibitor, DCM205". Antimicrobial Agents and Chemotherapy. 51 (5): 1780–6. doi:10.1128/AAC.01001-06. PMC 1855571. PMID 17307982.
  9. ^ Schweizer A, Rusert P, Berlinger L, Ruprecht CR, Mann A, Corthésy S, et al. (July 2008). "CD4-specific designed ankyrin repeat proteins are novel potent HIV entry inhibitors with unique characteristics". PLOS Pathogens. 4 (7): e1000109. doi:10.1371/journal.ppat.1000109. PMC 2453315. PMID 18654624.
  10. ^ "virionyx.com". Retrieved 2007-08-26.
  11. ^ Sulkowski MS, Kang M, Matining R, Wyles D, Johnson VA, Morse GD, et al. (March 2014). "Safety and antiviral activity of the HCV entry inhibitor ITX5061 in treatment-naive HCV-infected adults: a randomized, double-blind, phase 1b study". The Journal of Infectious Diseases. 209 (5): 658–67. doi:10.1093/infdis/jit503. PMC 3923538. PMID 24041792.

External links Edit

September 02, 2023
entry, inhibitor, this, article, needs, updated, please, help, update, this, reflect, recent, events, newly, available, information, 2020, also, known, fusion, inhibitors, class, antiviral, drugs, that, prevent, virus, from, entering, cell, example, blocking, . This article needs to be updated Please help update this to reflect recent events or newly available information May 2020 Entry inhibitors also known as fusion inhibitors are a class of antiviral drugs that prevent a virus from entering a cell for example by blocking a receptor Entry inhibitors are used to treat conditions such as HIV and hepatitis D Contents 1 HIV entry 1 1 Proteins 1 2 Binding fusion entry sequence 2 Approved agents 3 Investigational agents 4 References 5 External linksHIV entry Edit nbsp An illustration of HIV entry mechanism and mechanisms of action MOA of two entry inhibitor 5 Helix and C37 nbsp An HIV virion binds to a CD4 human cell The two bottom pictures depict two proposed models of HIV fusion with the cell They are used in combination therapy for the treatment of HIV infection This class of drugs interferes with the binding fusion and entry of an HIV virion to a human cell By blocking this step in HIV s replication cycle such agents slow the progression from HIV infection to AIDS 1 Proteins Edit There are several key proteins involved in the HIV entry process citation needed CD4 a protein receptor found on the surface of helper T cells in the human immune system also called CD4 T cells gp120 a protein on HIV surface that binds to the CD4 receptor CCR5 a second receptor found on the surface of CD4 cells and macrophages called a chemokine co receptor CXCR4 another chemokine co receptor found on CD4 cells gp41 an HIV protein closely associated with gp120 that penetrates the cell membraneBinding fusion entry sequence Edit HIV entry into a human cell requires the following steps in sequence 2 3 The binding of HIV surface protein gp120 to the CD4 receptor A conformational change in gp120 which both increases its affinity for a co receptor and exposes gp41 The binding of gp120 to a co receptor either CCR5 or CXCR4 The penetration of the cell membrane by gp41 which approximates the membrane of HIV and the T cell and promotes their fusion The entry of the viral core into the cellEntry inhibitors work by interfering with one aspect of this process Approved agents EditMaraviroc binds to CCR5 preventing an interaction with gp120 It is also referred to as a chemokine receptor antagonist or a CCR5 inhibitor 4 Enfuvirtide binds to gp41 and interferes with its ability to approximate the two membranes It is also referred to as a fusion inhibitor Ibalizumab a monoclonal antibody that binds to domain 2 of CD4 and interferes with post attachment steps required for the entry of HIV 1 virus particles into host cells and prevents the viral transmission that occurs via cell cell fusion Fostemsavir an attachment inhibitor that interferes with the interaction of CD4 and gp120 by binding with gp120 Investigational agents EditOther agents are under investigation for their ability to interact with the proteins involved in HIV entry and the possibility that they may serve as entry inhibitors 5 Leronlimab a monoclonal antibody that binds CCR5 Plerixafor was being developed to interfere with interaction between HIV and CXCR4 but showed little useful antiviral activity in recent trials Epigallocatechin gallate a substance found in green tea appears to interact with gp120 as do several other theaflavins 6 Vicriviroc similar to maraviroc is currently undergoing clinical trials for FDA approval Aplaviroc an agent similar to maraviroc and vicriroc Clinical trials were halted in 2005 over concerns about the drug s safety b12 is an antibody against HIV found in some long term nonprogressors It has been found to bind to gp120 at the exact region or epitope where gp120 binds to CD4 b12 seems to serve as a natural entry inhibitor in some individuals It is hoped that further study of b12 may lead to an effective HIV vaccine Griffithsin a substance derived from algae appears to have entry inhibitor properties 7 DCM205 is a small molecule based on L chicoric acid an integrase inhibitor DCM205 has been reported to inactivate HIV 1 particles directly in vitro and is thought to act primarily as an entry inhibitor 8 CD4 specific Designed Ankyrin Repeat Proteins DARPins potently block viral entry of diverse strains and are being developed and studied as potential microbicide candidates 9 A polyclonal caprine antibody is in phase II human clinical trials that targets among others sites the GP41 transmembrane glycoprotein The trials are being conducted by Virionyx a New Zealand Company 10 VIR 576 is a synthesized peptide which binds to gp41 preventing fusion of the virus with a cell membrane ITX5061 for hepatitis C 11 References Edit Biswas P Tambussi G Lazzarin A May 2007 Access denied The status of co receptor inhibition to counter HIV entry Expert Opinion on Pharmacotherapy 8 7 923 33 doi 10 1517 14656566 8 7 923 PMID 17472538 S2CID 32675897 Xiao Tianshu Cai Yongfei Chen Bing 2021 HIV 1 entry and membrane fusion inhibitors Viruses 13 5 735 doi 10 3390 v13050735 PMC 8146413 PMID 33922579 Wilen Craig B Tilton John C Doms Robert W 2012 HIV cell binding and entry Cold Spring Harb Perspect Med 2 8 a006866 doi 10 1101 cshperspect a006866 PMC 3405824 PMID 22908191 Retrieved 2021 08 11 Pugach P Ketas TJ Michael E Moore JP August 2008 Neutralizing antibody and anti retroviral drug sensitivities of HIV 1 isolates resistant to small molecule CCR5 inhibitors Virology 377 2 401 7 doi 10 1016 j virol 2008 04 032 PMC 2528836 PMID 18519143 Merck Manual com Human Immunodeficiency Virus HIV Infection Table 4 1 Williamson MP McCormick TG Nance CL Shearer WT December 2006 Epigallocatechin gallate the main polyphenol in green tea binds to the T cell receptor CD4 Potential for HIV 1 therapy The Journal of Allergy and Clinical Immunology 118 6 1369 74 doi 10 1016 j jaci 2006 08 016 PMID 17157668 Emau P Tian B O keefe BR Mori T McMahon JB Palmer KE et al August 2007 Griffithsin a potent HIV entry inhibitor is an excellent candidate for anti HIV microbicide Journal of Medical Primatology 36 4 5 244 53 doi 10 1111 j 1600 0684 2007 00242 x PMID 17669213 S2CID 22539115 Duong YT Meadows DC Srivastava IK Gervay Hague J North TW May 2007 Direct inactivation of human immunodeficiency virus type 1 by a novel small molecule entry inhibitor DCM205 Antimicrobial Agents and Chemotherapy 51 5 1780 6 doi 10 1128 AAC 01001 06 PMC 1855571 PMID 17307982 Schweizer A Rusert P Berlinger L Ruprecht CR Mann A Corthesy S et al July 2008 CD4 specific designed ankyrin repeat proteins are novel potent HIV entry inhibitors with unique characteristics PLOS Pathogens 4 7 e1000109 doi 10 1371 journal ppat 1000109 PMC 2453315 PMID 18654624 virionyx com Retrieved 2007 08 26 Sulkowski MS Kang M Matining R Wyles D Johnson VA Morse GD et al March 2014 Safety and antiviral activity of the HCV entry inhibitor ITX5061 in treatment naive HCV infected adults a randomized double blind phase 1b study The Journal of Infectious Diseases 209 5 658 67 doi 10 1093 infdis jit503 PMC 3923538 PMID 24041792 External links EditFusion Inhibitor Resource Center HIV Fusion Inhibitors at the U S National Library of Medicine Medical Subject Headings MeSH Retrieved from https en wikipedia org w index php title Entry inhibitor amp oldid 1153923131, wikipedia, wiki, book, books, library,

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