HIV-1 suppression and durable control by combining single broadly neutralizing antibodies and antiretroviral drugs in humanized mice

Horwitz, Joshua A.; Halper-Stromberg, Ariel; Mouquet, Hugo; Gitlin, Alexander D.; Tretiakova, Anna P.; Eisenreich, Thomas; Malbec, Marine; Gravemann, S.; Billerbeck, Eva; Dorner, Marcus; Büning, Hildegard; Schwartz, Olivier; Knops, Elena; Kaiser, Rolf; Seaman, Michael S.; Wilson, James M.; Rice, Charles M.; Ploß, Alexander; Björkman, Pamela J.; Klein, Florian; Nussenzweig, Michel C.

doi:10.1073/pnas.1315295110

Cited by 243 publications

(252 citation statements)

References 51 publications

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“…Recently, a human leukocyte reconstituted mouse model was developed to assess antibody mediated protection by neutralisation [43] and activating FcγR-dependent mechanisms [44]. The full potency of bNAbs in protection and control of viremia has been shown in this model to require FcγR-dependent extra-neutralising activity [44].…”

Section: In Vivo Studies I: Macaque and Mouse Modelsmentioning

confidence: 99%

Antibody functional assays as measures of Fc receptor-mediated immunity to HIV - new technologies and their impact on the HIV vaccine field.

Wines¹,

Billings²,

Mcleand³

et al. 2017

CHR

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Background:There is now intense interest in the role of HIV-specific antibodies and the engagement of FcγR functions in the control and prevention of HIV infection. The analyses of the RV144 vaccine trial, natural progression cohorts, and macaque models all point to a role for Fc-dependent effector functions, such as cytotoxicity (ADCC) or phagocytosis (ADCP), in the control of HIV. However, reliable assays that can be reproducibly used across different laboratories to measure Fcdependent functions, such as antibody dependent cellular cytotoxicity (ADCC) are limited. Method: This brief review highlights the importance of Fc properties for immunity to HIV, particularly via FcγR diversity and function. We discuss assays used to study FcR mediated functions of HIV-specific Ab, including our recently developed novel cell-free ELISA using homo-dimeric FcγR ectodomains to detect functionally relevant viral antigen-specific antibodies. Results: The binding of these dimeric FcγR ectodomains, to closely spaced pairs of IgG Fc, mimics the engagement and cross-linking of Fc receptors by IgG opsonized virions or infected cells as the essential prerequisite to the induction of Ab-dependent effector functions. The dimeric FcγR ELISA reliably correlates with ADCC in patient responses to influenza. The assay is amenable to high throughput and could be standardized across laboratories. Conclusion: We propose the assay has broader implications for the evaluation of the quality of antibody responses in viral infections and for the rapid evaluation of responses in vaccine development campaigns for HIV and other viral infections.

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Section: In Vivo Studies I: Macaque and Mouse Modelsmentioning

confidence: 99%

Antibody functional assays as measures of Fc receptor-mediated immunity to HIV - new technologies and their impact on the HIV vaccine field.

Wines¹,

Billings²,

Mcleand³

et al. 2017

CHR

View full text Add to dashboard Cite

show abstract

“…The human cells present in these animals have been shown to induce both innate and adaptive immune responses (46,53,(58)(59)(60)(61). In addition, HIV infection in these models responds to the same drugs used in humans (62)(63)(64)(65)(66)(67)(68). Like all animal models for biomedical research, there are limitations to their use in HIV research.…”

Section: Strengths and Limitations Of Current Humanized Mouse Modelsmentioning

confidence: 99%

In vivo platforms for analysis of HIV persistence and eradication

García

2016

Journal of Clinical Investigation

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“…Likewise, recent animal studies have shown that broadly neutralizing antibodies are indeed effective therapeutically. [78][79][80][81] In a human primate study, 3 out of 18 monkeys that exhibited the lowest viral loads prior to treatment exhibited prolonged virological control after the animals were treated with a PGT121-containing mAb cocktail and virus was cleared from the blood. However, while these mAbs cleared systemic virus transiently, the mAbs were unable to eradicate the reservoir in the majority of animals.…”

Section: Engineering Monoclonal Functionmentioning

confidence: 99%

Exploring the Potential of Monoclonal Antibody Therapeutics for HIV-1 Eradication

Euler

Alter

2015

AIDS Research and Human Retroviruses

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The HIV field has seen an increased interest in novel cure strategies. In particular, new latency reversal agents are in development to reverse latency to flush the virus out of its hiding place. Combining these efforts with immunotherapeutic approaches may not only drive the virus out of latency, but allow for the rapid elimination of these infected cells in a ''shock and kill'' approach. Beyond cell-based approaches, growing interest lies in the potential use of functionally enhanced ''killer'' monoclonal therapeutics to purge the reservoir. Here we discuss prospects for a monoclonal therapeutic-based ''shock and kill'' strategy that may lead to the permanent elimination of replication-competent virus, making a functional cure a reality for all patients afflicted with HIV worldwide.

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HIV-1 suppression and durable control by combining single broadly neutralizing antibodies and antiretroviral drugs in humanized mice

Cited by 243 publications

References 51 publications

Antibody functional assays as measures of Fc receptor-mediated immunity to HIV - new technologies and their impact on the HIV vaccine field.

Antibody functional assays as measures of Fc receptor-mediated immunity to HIV - new technologies and their impact on the HIV vaccine field.

In vivo platforms for analysis of HIV persistence and eradication

Exploring the Potential of Monoclonal Antibody Therapeutics for HIV-1 Eradication

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