Your search keyword '"Perkey, Katherine"' showing total 14 results

1. Defining total-body AIDS-virus burden with implications for curative strategies

Author

Estes, Jacob D, Kityo, Cissy, Ssali, Francis, Swainson, Louise, Makamdop, Krystelle Nganou, Del Prete, Gregory Q, Deeks, Steven G, Luciw, Paul A, Chipman, Jeffrey G, Beilman, Gregory J, Hoskuldsson, Torfi, Khoruts, Alexander, Anderson, Jodi, Deleage, Claire, Jasurda, Jacob, Schmidt, Thomas E, Hafertepe, Michael, Callisto, Samuel P, Pearson, Hope, Reimann, Thomas, Schuster, Jared, Schoephoerster, Jordan, Southern, Peter, Perkey, Katherine, Shang, Liang, Wietgrefe, Stephen W, Fletcher, Courtney V, Lifson, Jeffrey D, Douek, Daniel C, McCune, Joseph M, Haase, Ashley T, and Schacker, Timothy W

Subjects

Medical Microbiology, Biomedical and Clinical Sciences, Immunology, HIV/AIDS, Infectious Diseases, Sexually Transmitted Infections, 2.2 Factors relating to the physical environment, Infection, Good Health and Well Being, Anti-HIV Agents, DNA, Viral, HIV, HIV Infections, Humans, Lymphoid Tissue, RNA, Viral, Viral Load, Medical and Health Sciences, Biomedical and clinical sciences, Health sciences

Abstract

In the quest for a functional cure or the eradication of HIV infection, it is necessary to know the sizes of the reservoirs from which infection rebounds after treatment interruption. Thus, we quantified SIV and HIV tissue burdens in tissues of infected nonhuman primates and lymphoid tissue (LT) biopsies from infected humans. Before antiretroviral therapy (ART), LTs contained >98% of the SIV RNA+ and DNA+ cells. With ART, the numbers of virus (v) RNA+ cells substantially decreased but remained detectable, and their persistence was associated with relatively lower drug concentrations in LT than in peripheral blood. Prolonged ART also decreased the levels of SIV- and HIV-DNA+ cells, but the estimated size of the residual tissue burden of 108 vDNA+ cells potentially containing replication-competent proviruses, along with evidence of continuing virus production in LT despite ART, indicated two important sources for rebound following treatment interruption. The large sizes of these tissue reservoirs underscore challenges in developing 'HIV cure' strategies targeting multiple sources of virus production.

Published

2017

2. Impact of Integrase Inhibition compared to non-nucleoside inhibition on HIV reservoirs in Lymphoid Tissues

Author

Rothenberger, Meghan, Nganou-Makamdop, Krystelle, Kityo, Cissy, Ssali, Francis, Chipman, Jeffrey G, Beilman, Gregory J, Hoskuldsson, Torfi, Anderson, Jodi, Jasurda, Jake, Schmidt, Thomas E, Calisto, Samuel P, Pearson, Hope, Reimann, Thomas, David, Caitlin, Perkey, Katherine, Southern, Peter, Wietgrefe, Steve, Helgeson, Erika, Reilly, Cavan, Haase, Ashley T, Douek, Daniel C, Fletcher, Courtney V, and Schacker, Timothy W

Published

2019

3. Impact of Integrase Inhibition Compared With Nonnucleoside Inhibition on HIV Reservoirs in Lymphoid Tissues

Author

Rothenberger, Meghan, Nganou-Makamdop, Krystelle, Kityo, Cissy, Ssali, Francis, Chipman, Jeffrey G., Beilman, Gregory J., Hoskuldsson, Torfi, Anderson, Jodi, Jasurda, Jake, Schmidt, Thomas E., Calisto, Samuel P., Pearson, Hope, Reimann, Thomas, David, Caitlin, Perkey, Katherine, Southern, Peter, Wietgrefe, Steve, Helgeson, Erika, Reilly, Cavan, Haase, Ashley T., Douek, Daniel C, Fletcher, Courtney V., and Schacker, Timothy W.

Published

2019

4. Large number of rebounding/founder HIV variants emerge from multifocal infection in lymphatic tissues after treatment interruption

Author

Rothenberger, Meghan K., Keele, Brandon F., Wietgrefe, Stephen W., Fletcher, Courtney V., Beilman, Gregory J., Chipman, Jeffrey G., Khoruts, Alexander, Estes, Jacob D., Anderson, Jodi, Callisto, Samuel P., Schmidt, Thomas E., Thorkelson, Ann, Reilly, Cavan, Perkey, Katherine, Reimann, Thomas G., Utay, Netanya S., Makamdop, Krystelle Nganou, Stevenson, Mario, Douek, Daniel C., Haase, Ashley T., and Schacker, Timothy W.

Published

2015

5. Persistent HIV-1 replication is associated with lower antiretroviral drug concentrations in lymphatic tissues

Author

Fletcher, Courtney V., Staskus, Kathryn, Wietgrefe, Stephen W., Rothenberger, Meghan, Reilly, Cavan, Chipman, Jeffrey G., Beilman, Greg J., Khoruts, Alexander, Thorkelson, Ann, Schmidt, Thomas E., Anderson, Jodi, Perkey, Katherine, Stevenson, Mario, Perelson, Alan S., Douek, Daniel C., Haase, Ashley T., and Schacker, Timothy W.

Published

2014

6. Humanized Mouse Model of HIV-1 Latency with Enrichment of Latent Virus in PD-1 + and TIGIT + CD4 T Cells

Author

Llewellyn, George N., primary, Seclén, Eduardo, additional, Wietgrefe, Stephen, additional, Liu, Siyu, additional, Chateau, Morgan, additional, Pei, Hua, additional, Perkey, Katherine, additional, Marsden, Matthew D., additional, Hinkley, Sarah J., additional, Paschon, David E., additional, Holmes, Michael C., additional, Zack, Jerome A., additional, Louie, Stan G., additional, Haase, Ashley T., additional, and Cannon, Paula M., additional

Published

2019

7. Defining total-body AIDS-virus burden with implications for curative strategies.

Author

Estes, Jacob, Estes, Jacob, Kityo, Cissy, Ssali, Francis, Swainson, Louise, Makamdop, Krystelle, Del Prete, Gregory, Chipman, Jeffrey, Beilman, Gregory, Hoskuldsson, Torfi, Khoruts, Alexander, Anderson, Jodi, Deleage, Claire, Jasurda, Jacob, Schmidt, Thomas, Hafertepe, Michael, Callisto, Samuel, Pearson, Hope, Reimann, Thomas, Schuster, Jared, Schoephoerster, Jordan, Southern, Peter, Perkey, Katherine, Shang, Liang, Wietgrefe, Stephen, Fletcher, Courtney, Lifson, Jeffrey, Douek, Daniel, McCune, Joseph, Haase, Ashley, Schacker, Timothy, Deeks, Steven, Luciw, Paul, Estes, Jacob, Estes, Jacob, Kityo, Cissy, Ssali, Francis, Swainson, Louise, Makamdop, Krystelle, Del Prete, Gregory, Chipman, Jeffrey, Beilman, Gregory, Hoskuldsson, Torfi, Khoruts, Alexander, Anderson, Jodi, Deleage, Claire, Jasurda, Jacob, Schmidt, Thomas, Hafertepe, Michael, Callisto, Samuel, Pearson, Hope, Reimann, Thomas, Schuster, Jared, Schoephoerster, Jordan, Southern, Peter, Perkey, Katherine, Shang, Liang, Wietgrefe, Stephen, Fletcher, Courtney, Lifson, Jeffrey, Douek, Daniel, McCune, Joseph, Haase, Ashley, Schacker, Timothy, Deeks, Steven, and Luciw, Paul

Abstract

In the quest for a functional cure or the eradication of HIV infection, it is necessary to know the sizes of the reservoirs from which infection rebounds after treatment interruption. Thus, we quantified SIV and HIV tissue burdens in tissues of infected nonhuman primates and lymphoid tissue (LT) biopsies from infected humans. Before antiretroviral therapy (ART), LTs contained >98% of the SIV RNA+ and DNA+ cells. With ART, the numbers of virus (v) RNA+ cells substantially decreased but remained detectable, and their persistence was associated with relatively lower drug concentrations in LT than in peripheral blood. Prolonged ART also decreased the levels of SIV- and HIV-DNA+ cells, but the estimated size of the residual tissue burden of 108 vDNA+ cells potentially containing replication-competent proviruses, along with evidence of continuing virus production in LT despite ART, indicated two important sources for rebound following treatment interruption. The large sizes of these tissue reservoirs underscore challenges in developing HIV cure strategies targeting multiple sources of virus production.

Published

2017

8. Defining HIV and SIV Reservoirs in Lymphoid Tissues

Author

Deleage, Claire, primary, Wietgrefe, Stephen W., additional, Del Prete, Gregory, additional, Morcock, David R., additional, Hao, Xing-Pei, additional, Piatak, Jr., Michael, additional, Bess, Julian, additional, Anderson, Jodi L., additional, Perkey, Katherine, additional, Reilly, Cavan, additional, McCune, Joseph M., additional, Haase, Ashley T., additional, Lifson, Jeffrey D., additional, Schacker, Timothy W., additional, and Estes, Jacob D., additional

Published

2016

9. Live Simian Immunodeficiency Virus Vaccine Correlate of Protection: Immune Complex–Inhibitory Fc Receptor Interactions That Reduce Target Cell Availability

Author

Smith, Anthony J., primary, Wietgrefe, Stephen W., additional, Shang, Liang, additional, Reilly, Cavan S., additional, Southern, Peter J., additional, Perkey, Katherine E., additional, Duan, Lijie, additional, Kohler, Heinz, additional, Müller, Sybille, additional, Robinson, James, additional, Carlis, John V., additional, Li, Qingsheng, additional, Johnson, R. Paul, additional, and Haase, Ashley T., additional

Published

2014

10. NK Cell Responses to Simian Immunodeficiency Virus Vaginal Exposure in Naive and Vaccinated Rhesus Macaques

Author

Shang, Liang, primary, Smith, Anthony J., additional, Duan, Lijie, additional, Perkey, Katherine E., additional, Qu, Lucy, additional, Wietgrefe, Stephen, additional, Zupancic, Mary, additional, Southern, Peter J., additional, Masek-Hammerman, Katherine, additional, Reeves, R. Keith, additional, Johnson, R. Paul, additional, and Haase, Ashley T., additional

Published

2014

11. Targeted Cytotoxic Therapy Kills Persisting HIV Infected Cells During ART

Author

Denton, Paul W., primary, Long, Julie M., additional, Wietgrefe, Stephen W., additional, Sykes, Craig, additional, Spagnuolo, Rae Ann, additional, Snyder, Olivia D., additional, Perkey, Katherine, additional, Archin, Nancie M., additional, Choudhary, Shailesh K., additional, Yang, Kuo, additional, Hudgens, Michael G., additional, Pastan, Ira, additional, Haase, Ashley T., additional, Kashuba, Angela D., additional, Berger, Edward A., additional, Margolis, David M., additional, and Garcia, J. Victor, additional

Published

2014

12. Targeted Cytotoxic Therapy Kills Persisting HIV Infected Cells During ART

Author

Sykes, Craig, Yang, Kuo, Snyder, Olivia D., Margolis, David M., Kashuba, Angela D., Denton, Paul W., Haase, Ashley T., Wietgrefe, Stephen W., Berger, Edward A., Perkey, Katherine, Archin, Nancie M., Pastan, Ira, Choudhary, Shailesh K., Hudgens, Michael G., Garcia, J. Victor, Spagnuolo, Rae Ann, and Long, Julie M.

Subjects

3. Good health

Abstract

Antiretroviral therapy (ART) can reduce HIV levels in plasma to undetectable levels, but rather little is known about the effects of ART outside of the peripheral blood regarding persistent virus production in tissue reservoirs. Understanding the dynamics of ART-induced reductions in viral RNA (vRNA) levels throughout the body is important for the development of strategies to eradicate infectious HIV from patients. Essential to a successful eradication therapy is a component capable of killing persisting HIV infected cells during ART. Therefore, we determined the in vivo efficacy of a targeted cytotoxic therapy to kill infected cells that persist despite long-term ART. For this purpose, we first characterized the impact of ART on HIV RNA levels in multiple organs of bone marrow-liver-thymus (BLT) humanized mice and found that antiretroviral drug penetration and activity was sufficient to reduce, but not eliminate, HIV production in each tissue tested. For targeted cytotoxic killing of these persistent vRNA+ cells, we treated BLT mice undergoing ART with an HIV-specific immunotoxin. We found that compared to ART alone, this agent profoundly depleted productively infected cells systemically. These results offer proof-of-concept that targeted cytotoxic therapies can be effective components of HIV eradication strategies.

13. A humanized mouse model of HIV-1 latency with enrichment of latent virus in PD-1+ and TIGIT+ CD4 T cells.

Author

Llewellyn, George N., Seclèn, Eduardo, Wietgrefe, Stephen, Siyu Liu, Chateau, Morgan, Hua Pei, Perkey, Katherine, Marsden, Matthew D., Hinkley, Sarah J., Paschon, David E., Holmes, Michael C., Zack, Jerome A., Louie, Stan G., Haase, Ashley T., and Cannon, Paula M.

Subjects

*T cells, *COMBINATION drug therapy, *MICE, *LYMPHOID tissue, *HUMAN T cells

Abstract

Combination anti-retroviral drug therapy (ART) potently suppresses HIV-1 replication but does not result in virus eradication or a cure. A major contributing factor is the long-term persistence of a reservoir of latently infected cells. To study this reservoir, we established a humanized mouse model of HIV-1 infection and ART suppression based on an oral ART regimen. Similar to humans, HIV-1 levels in the blood of ART-treated animals were frequently suppressed below the limits of detection. However, the limited timeframe of the mouse model and the small volume of available samples makes it a challenging model with which to achieve full viral suppression and to investigate the latent reservoir. We therefore used an ex vivo latency reactivation assay that allows a semiquantitative measure of the latent reservoir that establishes in individual animals, regardless of whether they are treated with ART. Using this assay, we found that latently infected human CD4 T cells can be readily detected in mouse lymphoid tissues and that latent HIV-1 was enriched in populations expressing markers of T cell exhaustion, PD-1 and TIGIT. In addition, we were able to use the ex vivo latency reactivation assay to demonstrate that HIV-specific TALENs can reduce the fraction of reactivatable virus in the latently infected cell population that establishes in vivo, supporting the use of targeted nuclease-based approaches for an HIV-1 cure. [ABSTRACT FROM AUTHOR]

Published

2019

14. NK Cell Responses to Simian Immunodeficiency Virus Vaginal Exposure in Naive and Vaccinated Rhesus Macaques.

Author

Liang Shang, Smith, Anthony J., Duan, Lijie, Perkey, Katherine E., Lucy Qu, Wietgrefe, Stephen, Zupancic, Mary, Southern, Peter J., Masek-Hammerman, Katherine, Reeves, R. Keith, Johnson, R. Paul, and Haase, Ashley T.

Subjects

*KILLER cells, *SIMIAN immunodeficiency virus diseases, *IMMUNOSUPPRESSION, *RETROVIRUS diseases -- Immunological aspects, *MACAQUES, *PHYSIOLOGY, *IMMUNOLOGY

Abstract

NK cell responses to HIV/SIV infection have been well studied in acute and chronic infected patients/monkeys, but little is known about NK cells during viral transmission, particularly in mucosal tissues. In this article, we report a systematic study of NK cell responses to high-dose vaginal exposure to SIVmac251 in the rhesus macaque female reproductive tract (FRT). Small numbers of NK cells were recruited into the FRT mucosa following vaginal inoculation. The influx of mucosal NK cells preceded local virus replication and peaked at 1 wk and, thus, was in an appropriate time frame to control an expanding population of infected cells at the portal of entry. However, NK cells were greatly outnumbered by recruited target cells that fuel local virus expansion and were spatially dissociated from SIV RNA+ cells at the major site of expansion of infected founder populations in the transition zone and adjoining endocervix. The number of NK cells in the FRT mucosa decreased rapidly in the second week, while the number of SIV RNA+ cells in the FRT reached its peak. Mucosal NK cells produced IFN-γ and MIP-1a/CCL3 but lacked several markers of activation and cytotoxicity, and this was correlated with inoculum-induced upregulation of the inhibitory ligand HLA-E and downregulation of the activating receptor CD122/IL-2Rß. Examination of SIVΔnef-vaccinated monkeys suggested that recruitment of NK cells to the genital mucosa was not involved in vaccine-induced protection from vaginal challenge. In summary, our results suggest that NK cells play, at most, a limited role in defenses in the FRT against vaginal challenge. [ABSTRACT FROM AUTHOR]

Published

2014