HIV/AIDS is a chronic well manageable disease. HAART improves the quality of life of people living with HIV/AIDS, but the treatment has to be continued life long, as the total cure has not been established. Cost of treatment, drug toxicities, interaction with other drugs and persistence of inflammation and acceleration of ageing process, all put together, warrant an urgent need for a total cure. Even though two cases had been proved to be cured, still a practical cure is far beyond the reach. Numerous approaches and strategies had been put forth to achieve a cure; still they are to be proved with human studies. This article reviews the major approaches, recent advances in the venture of HIV cure and the safety concerns involved.

Keywords: HAART Improve, Interaction with other drugs, Venture of HIV cure, Safety concerns

INTRODUCTION

HAART revolutionized the management of HIV disease into a well manageable one. The longevity of the people living with HIV/AIDS is in no way inferior to that of those without HIV, their quality of life also improved a lot and the incidence of AIDS defining diseases have declined considerably. Newer molecules are introduced regularly which can suit individual’s needs and newer FDC (Fixed dose combination) are made it easy to adhere to treatment. The dose of Efavirenz was reduced and found equally effective with lesser side effects. Many newer molecules are on the pipeline. But in spite of all these, the long awaiting sterilized cure is getting delayed. The sterilized cure would no doubt be beneficial as it will certainly reduce morbidity, mortality, new infections, economic burden of the individuals and their countries, adverse effects due to the lifelong exposure to drugs, acceleration of ageing etc. The main barrier to a sterilizing cure is the presence of a ‘latent reservoir’; a population of HIV infected cells that persist for the lifetime of the individual despite ART and the HIV specific immune response [1,2]. So, the identification of various sources of viral reservoirs like Latent CD4 cells, CNS-microglial cells, macrophages, monocytes- (Peripheral Blood Mononuclear cells), reproductive system, lymph nodes, spleen and gut tissues get the prime importance in the research [3].

The Types of “Cure”

The FDA defines HIV cure research as “any investi­gation that evaluates [1] a therapeutic intervention or approach that controls or eliminates HIV infection to the point where no further medical interventions are needed to maintain health and [2] preliminary scientific concepts that might ultimately lead to such a therapeutic intervention” [4].

To be considered cured; an infected person would need to meet three criteria

1. Be able to live a normal, healthy lifespan
2. Be off antiretroviral therapy or any other HIV-related medications
3. Be incapable of transmitting the virus to others

STRATEGIES AVAILABLE

Genetic approach

• Hit early Hit hard: Early starting the treatment before the establishment of latent reservoir.
• Kick and kill or Shock and Kill: Flushing the reservoir cells into the blood stream and made the virus susceptible for ART or immune mechanism.
• Keep the reservoir to be inactive and remain dormant for ever.

  INTRODUCTION

  HAART revolutionized the management of HIV disease into a well manageable one. The longevity of the people living with HIV/AIDS is in no way inferior to that of those without HIV, their quality of life also improved a lot and the incidence of AIDS defining diseases have declined considerably. Newer molecules are introduced regularly which can suit individual’s needs and newer FDC (Fixed dose combination) are made it easy to adhere to treatment. The dose of Efavirenz was reduced and found equally effective with lesser side effects. Many newer molecules are on the pipeline. But in spite of all these, the long awaiting sterilized cure is getting delayed. The sterilized cure would no doubt be beneficial as it will certainly reduce morbidity, mortality, new infections, economic burden of the individuals and their countries, adverse effects due to the lifelong exposure to drugs, acceleration of ageing etc. The main barrier to a sterilizing cure is the presence of a ‘latent reservoir’; a population of HIV infected cells that persist for the lifetime of the individual despite ART and the HIV specific immune response [1,2]. So, the identification of various sources of viral reservoirs like Latent CD4 cells, CNS-microglial cells, macrophages, monocytes- (Peripheral Blood Mononuclear cells), reproductive system, lymph nodes, spleen and gut tissues get the prime importance in the research [3].

  The Types of “Cure”

  The FDA defines HIV cure research as “any investi­gation that evaluates [1] a therapeutic intervention or approach that controls or eliminates HIV infection to the point where no further medical interventions are needed to maintain health and [2] preliminary scientific concepts that might ultimately lead to such a therapeutic intervention” [4].

  To be considered cured; an infected person would need to meet three criteria

  1. Be able to live a normal, healthy lifespan
  2. Be off antiretroviral therapy or any other HIV-related medications
  3. Be incapable of transmitting the virus to others

  STRATEGIES AVAILABLE

  Genetic approach

  • Hit early Hit hard: Early starting the treatment before the establishment of latent reservoir.
  • Kick and kill or Shock and Kill: Flushing the reservoir cells into the blood stream and made the virus susceptible for ART or immune mechanism.
  • Keep the reservoir to be inactive and remain dormant for ever.

1. Be able to live a normal, healthy lifespan
2. Be off antiretroviral therapy or any other HIV-related medications
3. Be incapable of transmitting the virus to others

• Hit early Hit hard: Early starting the treatment before the establishment of latent reservoir.
• Kick and kill or Shock and Kill: Flushing the reservoir cells into the blood stream and made the virus susceptible for ART or immune mechanism.
• Keep the reservoir to be inactive and remain dormant for ever.

• Now they identified an enzyme called as Histone Deacetylase (HDAC) which is responsible to keep up latency. Several companies are looking into HDAC-Inhibitors. Some in vitro HDAC studies seemed to be promising but yet to be confirmed by clinical studies. Flush these latent CD4 HIV infected cells with drugs like Vorinostat and Panobinostat (HDAC inhibitors) into the circulation. Make susceptible for ART after expressed out of these reservoirs [10].
• Histone Deacetylase Inhibitors (HDI) have a broad spectrum of epigenetic activities. Vorinostat is marketed under the name Zolinza for the treatment of cutaneous T cell lymphoma (CTCL) when the disease persists, gets worse, or comes back during or after treatment with other medicines [11].

1. Chun TW, Finzi D, Margolick J, Chadwick K, Schwartz D, et al. (1995) In vivo fate of HIV-1 infected T cells: Quantitative analysis of transition to stable latency. Nat Med 1: 1284-1290.
2. Finzi D, Hermankova M, Pierson T, Carruth LM, Buck C, et al. (1997) Identification of a reservoir for HIV-1 in patients on highly active antiretroviral therapy. Science 278: 1295-1300.
3. Alexaki A, Liu Y, Wighdahl B (2008) Cellular reservoirs of HIV-1 and their role in viral persistence. Curr HIV Res 6: 388-400.
4. Saloman L (2018) A Cure for HIV? An Update One Year Later. Contagion 2: 2.
5. Hayden EC (2013) Weak statistical standards implicated in scientific irreproducibility. Nature.
6. Mississippi Baby (2020) Available online at: https://en.wikipedia.org/wiki/Mississippi_baby.
7. Tebas P, Stein D, Tang WW, Frank I, Wang SQ, et al. (2014) Gene editing of CCR5 in analogues CD4 T cells of persons infected with HIV. N Eng J Med 28: 839-847.
8. Ebina H, Miswa N, Kanemura Y, Koyanagi Y (2013) Harnessing the CRISPR/Cas9 system to disrupt latent HIV-1 provirus. Sci Rep 3: 2510.
9. Liu L, Patel B, Ghanem MH, Bundoc V, Zheng Z, et al. (2015) Novel CD4-Based bispecific chimeric antigen receptor designed for enhanced anti-HIV potency and absence of hiv entry receptor activity. J Virol 89: 6685-6694.
10. Shirakawa K, Chavez L, Hakre S, Calvanese V, Verdin E (2013) Reactivation of latent HIV by histone deacetylase inhibitors. Trends Microbiol 21: 277-285.
11. Vorinostat (2020) Available online at: https://en.wikipedia.org/wiki/Vorinostat
12. Mediouni S, Jablonski J, Paris JJ, Clementz MA, Thenin-Houssier S, et al. (2015) Didehydro-cortistatin A inhibits HIV-1 Tat mediated neuroinflammation and prevents potentiation of cocaine reward in Tat transgenic mice. Curr HIV Res 13: 64-79.
13. Pebody R (2020) Top 5 HIV cure and vaccine stories from AIDS 2020. HIV & AIDS. Available online at: https://www.aidsmap.com/news/jul-2020/top-5-hiv-cure-and-vaccine-stories-aids-2020
14. Kuriakose S (2018) Ibalizumab Effective for Multidrug-Resistant HIV-1 Infection. Contagion 3: 6.

1. Chun TW, Finzi D, Margolick J, Chadwick K, Schwartz D, et al. (1995) In vivo fate of HIV-1 infected T cells: Quantitative analysis of transition to stable latency. Nat Med 1: 1284-1290.
2. Finzi D, Hermankova M, Pierson T, Carruth LM, Buck C, et al. (1997) Identification of a reservoir for HIV-1 in patients on highly active antiretroviral therapy. Science 278: 1295-1300.
3. Alexaki A, Liu Y, Wighdahl B (2008) Cellular reservoirs of HIV-1 and their role in viral persistence. Curr HIV Res 6: 388-400.
4. Saloman L (2018) A Cure for HIV? An Update One Year Later. Contagion 2: 2.
5. Hayden EC (2013) Weak statistical standards implicated in scientific irreproducibility. Nature.
6. Mississippi Baby (2020) Available online at: https://en.wikipedia.org/wiki/Mississippi_baby.
7. Tebas P, Stein D, Tang WW, Frank I, Wang SQ, et al. (2014) Gene editing of CCR5 in analogues CD4 T cells of persons infected with HIV. N Eng J Med 28: 839-847.
8. Ebina H, Miswa N, Kanemura Y, Koyanagi Y (2013) Harnessing the CRISPR/Cas9 system to disrupt latent HIV-1 provirus. Sci Rep 3: 2510.
9. Liu L, Patel B, Ghanem MH, Bundoc V, Zheng Z, et al. (2015) Novel CD4-Based bispecific chimeric antigen receptor designed for enhanced anti-HIV potency and absence of hiv entry receptor activity. J Virol 89: 6685-6694.
10. Shirakawa K, Chavez L, Hakre S, Calvanese V, Verdin E (2013) Reactivation of latent HIV by histone deacetylase inhibitors. Trends Microbiol 21: 277-285.
11. Vorinostat (2020) Available online at: https://en.wikipedia.org/wiki/Vorinostat
12. Mediouni S, Jablonski J, Paris JJ, Clementz MA, Thenin-Houssier S, et al. (2015) Didehydro-cortistatin A inhibits HIV-1 Tat mediated neuroinflammation and prevents potentiation of cocaine reward in Tat transgenic mice. Curr HIV Res 13: 64-79.
13. Pebody R (2020) Top 5 HIV cure and vaccine stories from AIDS 2020. HIV & AIDS. Available online at: https://www.aidsmap.com/news/jul-2020/top-5-hiv-cure-and-vaccine-stories-aids-2020
14. Kuriakose S (2018) Ibalizumab Effective for Multidrug-Resistant HIV-1 Infection. Contagion 3: 6.