2013
DOI: 10.1016/s0140-6736(13)60104-x
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Barriers to a cure for HIV: new ways to target and eradicate HIV-1 reservoirs

Abstract: Antiretroviral therapy for HIV infection requires life-long access and strict adherence to regimens that are both expensive and associated with toxicities. There is growing recognition that a curative intervention will be needed to fully stop the epidemic. The failure to eradicate HIV infection during long-term antiretroviral therapy reflects the intrinsic stability of the viral genome in latently infected CD4+ T cells and other cells and perhaps ongoing low-level viral replication. Heterogeneity in latently i… Show more

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Cited by 269 publications
(245 citation statements)
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“…Elevated levels of inflammation and immune activation that can persist even in ART-treated HIV-infected individuals with effective viral suppression have emerged as key correlates of morbidity and mortality from non-AIDS complications such as cardiovascular disease, neurocognitive dysfunction, and kidney and bone abnormalities, among others (1,3). Furthermore, residual inflammation may contribute to HIV persistence during ART by several mechanisms, such as favoring de novo infection of activated "target" CD4 + T cells that replenish the reservoir and upregulating the expression of immune checkpoint blockers that may limit the function of HIV-specific immune responses (1,3,4). Therefore, a vicious cycle in which inflammation, poor antiviral responses, and HIV persistence are intimately connected may occur in ART-treated HIV-infected individuals.…”
Section: Introductionmentioning
confidence: 99%
“…Elevated levels of inflammation and immune activation that can persist even in ART-treated HIV-infected individuals with effective viral suppression have emerged as key correlates of morbidity and mortality from non-AIDS complications such as cardiovascular disease, neurocognitive dysfunction, and kidney and bone abnormalities, among others (1,3). Furthermore, residual inflammation may contribute to HIV persistence during ART by several mechanisms, such as favoring de novo infection of activated "target" CD4 + T cells that replenish the reservoir and upregulating the expression of immune checkpoint blockers that may limit the function of HIV-specific immune responses (1,3,4). Therefore, a vicious cycle in which inflammation, poor antiviral responses, and HIV persistence are intimately connected may occur in ART-treated HIV-infected individuals.…”
Section: Introductionmentioning
confidence: 99%
“…Therefore, treatment is required to be lifelong, with possible long-term toxicities. The cause of viral rebound and the most important obstacle to a cure for HIV infection are unclear, but it is generally believed that virus persists, in part, as long-lived latently infected cells (3)(4)(5). Since latently infected cells do not produce virus, they are unaffected by the immune system and are unresponsive to ART (6).…”
mentioning
confidence: 99%
“…9 Viral dissemination and the establishment of a viral reservoir throughout the body occurs rapidly after acquisition 9 and is the reason why ART cannot cure HIV infection. 10,11 Despite years of successful suppressive ART a latent pool of HIV-infected cells is thought to be the source of viral recrudescence on stopping therapy.…”
Section: Diagnosis Of Phimentioning
confidence: 99%