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Dive into the research topics where Bruce L. Levine is active.

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Featured researches published by Bruce L. Levine.


Science | 1996

Antiviral effect and ex vivo CD4+ T cell proliferation in HIV-positive patients as a result of CD28 costimulation.

Bruce L. Levine; Joseph D. Mosca; James L. Riley; Richard G. Carroll; Maryanne Vahey; Linda L. Jagodzinski; Kenneth F. Wagner; Douglas L. Mayers; Donald S. Burke; Owen S. Weislow; Daniel C. St. Louis; Carl H. June

Because stimulation of CD4+ lymphocytes leads to activation of human immunodeficiency virus-type 1 (HIV-1) replication, viral spread, and cell death, adoptive CD4+ T cell therapy has not been possible. When antigen and CD28 receptors on cultured T cells were stimulated by monoclonal antibodies (mAbs) to CD3 and CD28 that had been immobilized, there was an increase in the number of polyclonal CD4+ T cells from HIV-infected donors. Activated cells predominantly secreted cytokines associated with T helper cell type 1 function. The HIV-1 viral load declined in the absence of antiretroviral agents. Moreover, CD28 stimulation of CD4+ T cells from uninfected donors rendered these cells highly resistant to HIV-1 infection. Immobilization of CD28 mAb was crucial to the development of HIV resistance, as cells stimulated with soluble CD28 mAb were highly susceptible to HIV infection. The CD28-mediated antiviral effect occurred early in the viral life cycle, before HIV-1 DNA integration. These data may facilitate immune reconstitution and gene therapy approaches in persons with HIV infection.


Immunological Reviews | 1997

Tales of tails: regulation of telomere length and telomerase activity during lymphocyte development, differentiation, activation, and aging.

Nan-ping Weng; Larry D. Palmer; Bruce L. Levine; H. Clifford Lane; Carl H. June; Richard J. Hodes

Summary: Telomerase activity and the regulation of telomere length are factors which have been implicated in the control of cellular replication. These variables have been examined during human lymphocyte development, differentiation, activation, and aging. It was found that telomere length of peripheral blood CD4+ T cells decreases with age as well as with differentiation from naive to memory cells in vivo, and decreases with cell division in vitro. These results provide evidence that telomere length correlates with lymphocyte replicative history and residual replicative potential. In contrast, telomere length appears to increase during tonsil B‐cell differentiation and germinal center (GC) formation in vivo. It was also found that telomerase activity is highly regulated during T‐cell development and B‐cell differentiation in vivo, with high levels of telomerase activity expressed in thymocytes and GC B cells, and low levels of telomerase activity in resting mature peripheral blood lymphocytes. Finally, resting lymphocytes retain the ability to upregulate telomerase activity upon activation, and this capacity does not appear to decline with age. Although the precise role of telomerase in lymphocyte function remains to be elucidated, telomerase may contribute to protection from telomere shortening in T and B lymphocytes, and may thus play a critical role in lymphocyte development, differentiation and activation. The future study of study telomerase and its regulation of telomere length may enhance our understanding of bow the replicative lifespan is regulated in lymphocytes.


International Immunology | 1995

Both CD28 ligands CD80 (B7-1) and CD86 (B7-2) activate phosphatidylinositol 3-kinase, and wortmannin reveals heterogeneity in the regulation of T cell IL-2 secretion

Yuji Ueda; Bruce L. Levine; Mark L. Huang; Gordon J. Freeman; Lee M. Nadler; Carl H. June; Stephen G. Ward


Archive | 2002

Generation of use of tc1 and tc2 cells

Daniel H. Fowler; Unsu Jung; Jeffrey A. Medin; Ronald E. Gress; Andreas Erdmann; Bruce L. Levine; Carl H. June


Clinical Immunology | 1999

Increases in T cell telomere length in HIV infection after antiretroviral combination therapy for HIV-1 infection implicate distinct population dynamics in CD4+ and CD8+ T cells.

Sumesh Kaushal; Alan Landay; Michael M. Lederman; Elizabeth Connick; John Spritzler; Daniel R. Kuritzkes; Harold A. Kessler; Bruce L. Levine; Daniel C. St. Louis; Carl H. June


Archive | 2002

Methods of generating human cd4+ th2 cells and uses thereof

Daniel H. Fowler; Jeanne Hou; Unsu Jung; Ronald E. Gress; Michael Bishop; Carl H. June; Bruce L. Levine


Archive | 2002

Methods of generating human cd4+ th1 cells

Daniel H. Fowler; Jeannie Hou; Unsu Jung; Ronald E. Gress; Bruce L. Levine; Carl H. June


Archive | 2006

Methods for modulating expression of an HIV-1 fusion cofactor

Carl H. June; Richard G. Carroll; James L. Riley; Daniel C. Louis St.; Bruce L. Levine


Archive | 2017

METHODS OF MAKING CHIMERIC ANTIGEN RECEPTOR -EXPRESSING CELLS

Felipe Bedoya; Saba Ghassemi; Carl H. June; Bruce L. Levine; Jan J. Melenhorst; Michael C. Milone; Daniel J. Powell; Zoe Zheng


Archive | 1998

Methods for downregulating CCR5 in T cells with anti-CD3 antibodies and anti-CD28 antibodies

Carl H. June; Richard G. Carroll; James L. Riley; Daniel C. St. Louis; Bruce L. Levine

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Carl H. June

National Marrow Donor Program

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James L. Riley

University of Pennsylvania

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Daniel C. St. Louis

Henry M. Jackson Foundation for the Advancement of Military Medicine

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David L. Porter

University of Pennsylvania

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Stephen G. Emerson

Children's Hospital of Philadelphia

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Wayne R. Godfrey

University of Pennsylvania

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