The HIV Reservoir in Monocytes and Macrophages

Wong, Michelle E.; Jaworowski, Anthony; Hearps, Anna C.

doi:10.3389/fimmu.2019.01435

Cited by 173 publications

(152 citation statements)

References 177 publications

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“…The human spleen in the BLTS-humanized mouse model recapitulates human adult spleen architecture and facilitates better reconstitution of immune cells, including human red pulp macrophages, which are poorly reconstituted in the BLT-humanized mouse model [5]. It is well established that macrophages can serve as a reservoir for HIV [106][107][108]; thus, the BLTS-humanized mouse model provides a system for investigating human splenic macrophage-HIV interactions [5]. Additionally, the spleen is a major lymphoid tissue reservoir, with B cell follicles in the white-pulp serving as an immune privilege site for anti-HIV T-cells [109].…”

Section: Bone Marrow-liver-thymus-spleen (Blts)-humanized Mouse Modelmentioning

confidence: 99%

Moving beyond the mousetrap: current and emerging humanized mouse and rat models for investigating prevention and cure strategies against HIV infection and associated pathologies

et al. 2020

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The development of safe and effective combination antiretroviral therapies for human immunodeficiency virus (HIV) infection over the past several decades has significantly reduced HIV-associated morbidity and mortality. Additionally, antiretroviral drugs have provided an effective means of protection against HIV transmission. Despite these advances, significant limitations exist; namely, the inability to eliminate HIV reservoirs, the inability to reverse lymphoid tissues damage, and the lack of an effective vaccine for preventing HIV transmission. Evaluation of the safety and efficacy of therapeutics and vaccines for eliminating HIV reservoirs and preventing HIV transmission requires robust in vivo models. Since HIV is a human-specific pathogen, that targets hematopoietic lineage cells and lymphoid tissues, in vivo animal models for HIV-host interactions require incorporation of human hematopoietic lineage cells and lymphoid tissues. In this review, we will discuss the construction of mouse models with human lymphoid tissues and/or hematopoietic lineage cells, termed, human immune system (HIS)-humanized mice. These HIS-humanized mouse models can support the development of functional human innate and adaptive immune cells, along with primary (thymus) and secondary (spleen) lymphoid tissues. We will discuss applications of HIS-humanized mouse models in evaluating the safety and efficacy of therapeutics against HIV reservoirs and associated immunopathology, and delineate the human immune response elicited by candidate HIV vaccines. In addition to focusing on how these HIS-humanized mouse models have already furthered our understanding of HIV and contributed to HIV therapeutics development, we discuss how emerging HIS-humanized rat models could address the limitations of HIS-mouse models.

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Section: Bone Marrow-liver-thymus-spleen (Blts)-humanized Mouse Modelmentioning

confidence: 99%

Moving beyond the mousetrap: current and emerging humanized mouse and rat models for investigating prevention and cure strategies against HIV infection and associated pathologies

et al. 2020

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“…Additionally, we note that most of the small molecule screens for novel LRAs (Table ), except for two small scale studies, were performed using T‐cell lines or primary cells, and there has not yet been significant effort toward identifying LRAs that may be specifically effective in monocyte‐macrophage lineages. Because these cell types represent important reservoirs for virus in patients on ART, it may be necessary to target unique aspects of provirus regulation in these cells.…”

Section: Prospective For Future Lra Identification and Developmentmentioning

confidence: 99%

Diversity of small molecule HIV‐1 latency reversing agents identified in low‐ and high‐throughput small molecule screens

Hashemi

Sadowski

2019

Medicinal Research Reviews

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The latency phenomenon produced by human immunodeficiency virus (HIV-1) prevents viral clearance by current therapies, and consequently development of a cure for HIV-1 disease represents a formidable challenge. Research over the past decade has resulted in identification of small molecules that are capable of exposing HIV-1 latent reservoirs, by reactivation of viral transcription, which is intended to render these infected cells sensitive to elimination by immune defense recognition or apoptosis. Molecules with this capability, known as latency-reversing agents (LRAs) could lead to realization of proposed HIV-1 cure strategies collectively termed "shock and kill," which are intended to eliminate the latently infected population by forced reactivation of virus replication in combination with additional interventions that enhance killing by the immune system or virus-mediated apoptosis. Here, we review efforts to discover novel LRAs via low-and high-throughput small molecule screens, and summarize characteristics and biochemical properties of chemical structures with this activity.We expect this analysis will provide insight toward further research into optimized designs for new classes of more potent LRAs.---

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“…CD14 ++ CD16 − classical monocytes presented high phagocytic activity and they are critical for initial inflammatory responses while CD14 ++ CD16 + intermediate monocytes are associated with inflammatory response, and CD14 + CD16 ++ non-classical are considered as patrolling monocytes 21 . Monocyte activation has been reported during DENV and HIV infections and they are associated with disease pathogenesis 22,40 . Our results demonstrated significant changes of monocyte subsets during DENV and DENV/HIV coinfection.…”

Section: Discussionmentioning

confidence: 99%

Apoptosis characterization in mononuclear blood leukocytes of HIV patients during dengue acute disease

Torrentes-Carvalho

Sánchez‐Arcila

Azamor

et al. 2020

Sci Rep

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Dengue virus (DenV) co-circulation in Brazil represents a challenge for treatment and vaccine development. Despite public health impact, the occurrence of coinfections with other viruses is a common event. Increased T cell activation and altered inflammatory response are found during DENV coinfection with Human Immunodeficiency Virus (HIV) impacting HIV-pathogenesis. Even with Antiretroviral therapy (ARt), HiV-treated patients had chronic immune activation and lymphocyte apoptosis. However, apoptotic mechanisms have not been investigated during coinfection with DenV. our attention was attracted to apoptotic cell markers expressions in pBMcs from DenV and DenV/ HIV coinfected patients. We found CD4/CD8 ratio inversion in most coinfected patients. CD4 T and CD8 T-cell subsets from DENV and DENV/HIV groups expressed low levels of anti-apoptotic protein Bcl-2. Furthermore, CD8 CD95 double positive cells frequency expressing low levels of Bcl-2 were significantly higher in these patients. Additionally, the density of Bcl-2 on classical monocytes (CD14 ++ CD16 − ) was significantly lower during DENV infection. Upregulation of pro-apoptotic proteins and anti-apoptotic proteins were found in DenV and DenV/HiV, while catalase, an antioxidant protein, was upregulated mainly in DENV/HIV coinfection. These findings provide evidence of apoptosis triggering during DenV/HiV coinfection, which may contribute to knowledge of immunological response during DenV acute infection in HiV-patients treated with ARt.Dengue virus (DENV) and Human Immunodeficiency Virus (HIV) infections are currently a major public health concern in Brazil. Dengue is caused by any one of four DENV (1-4) serotypes spread by mosquitoes of aedes genus. DENV causes an acute febrile illness of a broad clinical spectrum presenting both asymptomatic and symptomatic forms that can evolve with severe and potentially fatal condition 1 . The hallmark of most serious clinical conditions is the vascular permeability increase that causes plasma leakage, leading to shock and death. Acquired Immunodeficiency Sydrome (AIDS) (is still considered an important cause of morbidity and mortality in the world. HIV infects CD4 T-cells, monocytes/macrophages and to a lesser extent in dendritic cells leading to progressive CD4 T-cell depletion and consequently pronounced immunosuppression in the absence of effective antiretroviral therapy (ART) 2 .Apoptosis, also called type I cell death, is a regulated process of cell death highly conserved among mammals and comprises a controlled self-destruction process to eliminate damaged, neoplastic and virus-infected cells 3 . Apoptosis program regulation is determined by interactions of three members of B-cell lymphoma-2 family proteins (Bcl-2): Bcl-2 homologous 3 (BH3)-only proteins, Bcl-2 proteins and Bcl-2 associated X protein (Bax)/Bcl-2 homologous antagonist/killer (Bak) effectors. It can be triggered by extrinsic [death receptors like p55 tumor necrosis factor TNF receptor-TNFRI, Fas/CD95, TRAIL/APO2-L (TNF-related apoptosis-inducing li...

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The HIV Reservoir in Monocytes and Macrophages

Cited by 173 publications

References 177 publications

Moving beyond the mousetrap: current and emerging humanized mouse and rat models for investigating prevention and cure strategies against HIV infection and associated pathologies

Moving beyond the mousetrap: current and emerging humanized mouse and rat models for investigating prevention and cure strategies against HIV infection and associated pathologies

Diversity of small molecule HIV‐1 latency reversing agents identified in low‐ and high‐throughput small molecule screens

Apoptosis characterization in mononuclear blood leukocytes of HIV patients during dengue acute disease

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